NON-INVASIVE SAMPLING OF INNER-COLONIC MICROBIOME

BACKGROUND OF THE INVENTION
Technical Field

The present invention relates to the field of gastroenterological systems, and more particularly, to sampling large intestine contents.

Discussion of Related Art

Colonoscopy procedures, carried out routinely on a large number of patients, require a prior cleansing of the large intestine, which may be carried out by various means.

U.S. Pat. No. 9,775,865, incorporated herein by reference in their entirety, teaches Systems, kits and methods are provided, which analyze the large intestine content and utilize acoustic signals detected during delivery of water into the large intestine and drained large intestine contents to derive large intestine characteristics such as microbial analyses. Systems may include a water delivery unit including a water supply and a nozzle connected thereto, configured to introduce water controllably into a patient's large intestine, and an analysis unit that provides information about the drained contents using optical examination or biological assays. The information may be related to acoustic analysis of signals from acoustic sensors that are attachable to a patient's abdomen. A variety of sensor configurations, positioning options, analysis strategies and large intestine characteristics are presented.

SUMMARY OF THE INVENTION

The following summary does not necessarily identify key elements nor limit the scope of the invention, but merely serves as an introduction to the following description.

One embodiment of the present invention provides a non-invasive sampling system of inner-colonic microbiome, operable in fluid communication with a large intestine cleansing system, the sampling system comprising: an electromechanical sampling device configured to collect at least a part of large intestine contents drained by the cleansing system, the sampling device comprising: a collection unit configured to collect at least one sample from the contents, and a robotic unit configured to move the collection unit to and from a sampling position that is in fluid communication with the drained contents.

One embodiment of the present invention provides a method comprising: introducing water controllably into a patient's large intestine, draining the introduced water with contents of the patient's large intestine, optically monitoring the drained content, characterizing the optically monitored drained content to determine sampling times, and sampling the drained contents according to the characterization.

These, additional, and/or other aspects and/or advantages of embodiments the present invention are set forth in the detailed description which follows; possibly inferable from the detailed description; and/or learnable by practice of the present invention.

BRIEF DESCRIPTION OF THE DRAWINGS

For a better understanding of embodiments of the invention and to show how the same may be carried into effect, reference will now be made, purely by way of example, to the accompanying drawings in which like numerals designate corresponding elements or sections throughout.

In the accompanying drawings:

FIGS. 1A-1E are high-level schematic illustrations of a large bowel cleansing systems, according to some embodiments of the invention.

FIGS. 2A-2C are high-level schematic illustrations of a system, according to some embodiments of the invention.

FIGS. 3A-3D are high-level schematic flowcharts and illustrations of methods of deriving large intestine characteristics from acoustic signals, according to some embodiments of the invention.

FIGS. 4A and 4B are high-level flowcharts illustrating methods, according to some embodiments of the invention.

FIG. 5 is a high-level schematic illustration of draining and separating multiple samples of large intestine content, according to some embodiments of the invention.

FIGS. 6A, 6B, 7-10, 11A and 11B illustrate the significant difference of microbiota samples from more proximal portions of the large intestine, with respect to prior art stool samples, according to some embodiments of the invention.

FIG. 12 is a high-level flowchart illustrating methods, according to some embodiments of the invention.

FIG. 13A is a high-level schematic illustration of a sampling system with enlarged views of a collection unit thereof, according to some embodiments of the invention.

FIG. 13B a high-level control schematic illustrating the operation of the sampling system, according to some embodiments of the invention.

FIGS. 14A and 14B are high-level schematic illustrations of configurations of the sampling system with respect to the cleansing system, according to some embodiments of the invention.

FIGS. 15A-15C schematically illustrate stages in the operation of sampling system, according to some embodiments of the invention.

FIG. 16 is a high-level schematic flowchart of a sampling method, according to some embodiments of the invention.

DETAILED DESCRIPTION

Prior to the detailed description being set forth, it may be helpful to set forth definitions of certain terms that will be used hereinafter.

The term “large intestine characteristics” as used in this application refers to any feature that may be used to relate to the large intestine, such as its shape, length, diameter, position in the abdomen, any related structures, such as appendages and pouches, the large intestine may have, any changes in the form of the large intestine, features of the large intestine wall and its muscular activity, as well as features that are related to measured acoustic signals, such as signal levels, signal frequencies, temporal and/or spatial distribution of the signals and relation of the signals to any external or internal event such as introduction of water into the large intestine and the cleansing of the large intestine. The term “large bowel” is used interchangeably with the term “large intestine”.

The term “microbiota transplant” or “MT” as used in this application refers to any introduced sample of intestinal bacteria such as fecal transplants (fecal microbiota transplants—FMT) from autologous (self) sources or from donors, as well as any probiotic infusions and/or rationally designed microbial consortia.

In the following description, various aspects of the present invention are described. For purposes of explanation, specific configurations and details are set forth in order to provide a thorough understanding of the present invention. However, it will also be apparent to one skilled in the art that the present invention may be practiced without the specific details presented herein. Furthermore, well known features may have been omitted or simplified in order not to obscure the present invention. With specific reference to the drawings, it is stressed that the particulars shown are by way of example and for purposes of illustrative discussion of the present invention only, and are presented in the cause of providing what is believed to be the most useful and readily understood description of the principles and conceptual aspects of the invention. In this regard, no attempt is made to show structural details of the invention in more detail than is necessary for a fundamental understanding of the invention, the description taken with the drawings making apparent to those skilled in the art how the several forms of the invention may be embodied in practice.

Before at least one embodiment of the invention is explained in detail, it is to be understood that the invention is not limited in its application to the details of construction and the arrangement of the components set forth in the following description or illustrated in the drawings. The invention is applicable to other embodiments that may be practiced or carried out in various ways as well as to combinations of the disclosed embodiments. Also, it is to be understood that the phraseology and terminology employed herein is for the purpose of description and should not be regarded as limiting.

Unless specifically stated otherwise, as apparent from the following discussions, it is appreciated that throughout the specification discussions utilizing terms such as “processing”, “computing”, “calculating”, “determining”, “enhancing” or the like, refer to the action and/or processes of a computer or computing system, or similar electronic computing device, that manipulates and/or transforms data represented as physical, such as electronic, quantities within the computing system's registers and/or memories into other data similarly represented as physical quantities within the computing system's memories, registers or other such information storage, transmission or display devices. Any of the disclosed modules or units may be at least partially implemented by a computer processor.

Systems, kits and methods are provided, which analyze the large intestine content and may utilize acoustic signals detected during delivery of water into the large intestine and drained large intestine contents to derive large intestine characteristics. Systems may include a water delivery unit including a water supply and a nozzle connected thereto, configured to introduce water controllably into a patient's large intestine, and an analysis unit that provides information about the drained contents using optical examination or biological assays. The information may be related to acoustic analysis of signals from acoustic sensors that are attachable to a patient's abdomen. A variety of sensor configurations, positioning options, analysis strategies and large intestine characteristics are presented.

Additionally, sampling systems and methods for non-invasive sampling of inner-colonic microbiome and its potential derivatives are provided. The sampling systems may operate in fluid communication with a large intestine cleansing system and comprise an electromechanical sampling device configured to collect at least a part of large intestine contents drained by the cleansing system. The electromechanical sampling device may comprise a collection unit configured to collect at least one sample from the contents, and an electromechanical robotic unit configured to move the collection unit to and from a sampling position and to manipulate the collection unit into a respective casing, to deposit the sample(s). Sampling methods may comprise optically monitoring drained contents of the large intestine, characterizing the optically-monitored (and possibly spectrally analyzed) drained contents to determine sampling times, and sampling the drained contents according to the characterization.

Moreover, methods and systems are provided for diagnosis and possibly treatment of the large intestine, using samples from at least three portions of the large intestine, including sampling the ascending portion thereof. Methods and systems are provided for diagnosis and possibly treatment of the large intestine, using samples from at least three portions of the large intestine, including sampling the ascending colon portion thereof. Samples from the ascending portions of the large intestine were found to differ in their microbial characteristics significantly from prior art stool samples and from samples taken from the descending and transverse parts of the large intestine—enabling more accurate diagnosis and possibly more effective treatment of diseases of the large intestine, such as inflammatory bowel diseases, colorectal cancer, irritable bowel disease, diabetes, and/or chronic constipation, as non-limiting examples.

Advantageously, as the gut microbiome is increasingly reported to relate to a variety of medical conditions (e.g., risk for cancer, inflammatory bowel disease (IBD), obesity, nonalcoholic fatty liver disease, arterial condition, allergies and asthma, “reset” of the gut microbiome community (e.g., such as caused by dietary changes, antibiotics, apnea, therapies, diseases, jetlag etc.), and the ability to diagnose and transplant the microbiome is expected to provide substantial benefits in many fields of medicine.

In certain embodiments, the systems, kits and methods may be integrated within a system or a procedure of large intestine cleansing prior to colonoscopy, to provide additional information in form of the large intestine characteristics to the practitioner of the upcoming colonoscopy procedure. It is noted however, that sampling and/or treatment may be carried out as a separate procedure, irrespective of colonoscopy.

Moreover, systems and methods are provided to limit abdominal distension and limit and/or alleviate uncomfortable side effects related to it—in patients treated in hydrocolonic preparation units. Systems may comprise a water delivery unit comprising a controllable water supply, configured to introduce water controllably into the patient's large intestine, a drainage configured to drain the introduced water with contents of the patient's large intestine and a controller. The drainage comprises a drainage pipe and sensor(s) such as camera(s) configured to continuously measure the amount of drained water drained by the drainage pipe. The controller is configured to control the water introduction with respect to the measured amount of drained water, keeping an amount of water retained in the patient below a specified water retention threshold to reduce uncomfortable side effects of abdominal distension.

It is noted that hydrocolonic preparation units that cleanse the patient's large intestine generally cause abdominal distension in the sense that the water introduction unfolds the normally collapsed intestine to a certain extent. In various embodiments, disclosed systems and methods provide control over the extent of distension that limits the abdominal distension to alleviate, limit or even avoid uncomfortable side effects of abdominal distension. As the extent of uncomfortable side effects is both patient specific and process-specific, disclosed embodiments provide ways to control the cleansing process with respect to limit or reduce side effects in relation to predefined thresholds and/or patient indications during the treatment.

FIGS. 1A-1E are high-level schematic illustrations of a large bowel (large intestine) cleansing systems 100, according to some embodiments of the invention. FIG. 1A illustrates schematically a part of system 100 with a corresponding block diagram, FIGS. 1B and 1C illustrate schematically perspective views of systems 100, with and without the treated patient, respectively, FIG. 1D illustrates schematically a processor in system 100 and FIG. 1E illustrated schematically large intestine cleansing system 100. Systems 100 are used with a hydrocolonic preparation unit 80 that is designed ergonomically to receive the patient in a comfortable posture and apply large intestine cleansing procedures to the patient.

Systems 100 comprise a water delivery unit 130 comprising a controllable water supply 131, configured to introduce water (132) controllably into the patient's large intestine, a drainage 151 configured to drain (possibly by gravity, or by other means) the introduced water with contents of the patient's large intestine (139), e.g., stool and/or effluent. Drainage 151 typically comprises a drainage basin 154 below the patient, one or more drainage pipe 138 within unit 80 that removes drained contents 139. Drainage pipe 138 may be connected to draining basin 154 of unit 80 and/or of cleansing system 100, and drain the accumulating water and drained content therefrom, e.g., by gravity or by other means, such as pumping, suction etc. Drainage 151 may be monitored by at least one sensor 161 configured to continuously measure an amount of drained water drained into basin 154 and through drainage pipe(s) 138. It is noted that contents 139 includes mostly water that was introduced and then drained form the patient's large intestine, as well as an amount of contents (e.g., stool and/or effluent) that originated in the patient's large intestine and is rinsed and drained by the introduced water. In certain embodiments, a pipe 134A may be configured to deliver water from an external pressurized source, such as a faucet, to the top of water delivery unit 130 (see, e.g., FIG. 1C, and FIG. 1B illustrating schematically water supply 131 with a gauge 136) from which water can be introduced (132, via pipe 134) by gravity into the patient's large intestine, and then drained (139, via pipe 138) from the patient, e.g., by gravity and/or using mechanical means such as pumping or suction.

Systems 100 further comprise a controller 141 (e.g., as part of a control unit 140, see below, and/or as part of water delivery unit 130) that is configured to control water introduction 132 (via pipe 134) with respect to the measured amount of drained water 139, keeping an amount of water retained in the patient below a specified water retention threshold to limit abdominal distension and reduce uncomfortable side effects thereof. It is noted that abdominal distension, resulting from excessive accumulation of water during the cleansing procedure, may be inconvenient to the patient to a degree that can hinder the cleansing procedure. Systems 100 and controller 141 may be configured to limit abdominal distension and reduce uncomfortable side effects thereof by avoiding excessive introduction of water into the patient's large intestine, in respect to the amount of water that was previously introduced into the large intestine and to the amount of water that was already drained therefrom. In particular, systems 100 may be configured to monitor the amount of liquid (denoted R(t)) retained in the patient's colon and to control the flow of water to the colon in such a way as to steer away from, e.g., the trigger point of nausea and uneasiness due to abdominal distension, where the process needs to be stopped to allow recovery of the patient.

In various embodiments, the specified water retention threshold may be defined in different ways, such as relying on typical and/or patient specific values or indications. Typical distended bowel (large intestine) volumes are between 0.7 liter and 4.4 liter, averaging 2.1 liter. Typical lengths of large intestines range between 118 cm and 285 cm, averaging 197 cm. The specified water retention threshold for avoiding uneasiness due to abdominal distention may be determined as a value that is lower than the average of 2.1 liter, e.g., 2 liters, 1.8 liters, 1.5 liter or other values. Thresholds for limiting abdominal distension and reducing the related side effects may be set as a specified percentage of the typical and/or patient-specific distended bowel volume—e.g., any of 50%, 25-50%, 50-75%, 10-30% or any other intermediate values or ranges. In certain embodiments, patient indications of uneasiness may be used to calibrate the threshold or the percentage of the estimated patient's bowel volume, e.g., lower thresholds may be set for sensitive patients while higher threshold may be set for less sensitive patients, in either case possibly in relation to estimated physical dimensions of the patient's large intestine. For example, the patient may be asked to mark once (e.g., by an appropriate “event” button) when uneasiness starts, and the marked value of water retention may be used as a reference for defining the threshold during the procedure for this patient.

In certain embodiments, variability among patients may be taken into account, by correlating the specified water retention threshold with various measures of the patient such as height, weight, circumference of the abdomen, body mass index etc. Typically, thresholds may be larger for larger patients. In certain embodiments, an estimation of initial bowel contents may be taken into account, lowering the threshold at the start of the cleansing procedure. The estimation may be received from the patient, or be derived from initial drained contents during the cleansing procedure (e.g., the threshold may be raised after initial cleansing). In certain embodiments, the specified water retention threshold may be determined individually, e.g., following previous imaging data of the large intestine. In certain embodiments, the specified water retention threshold may be determined individually, e.g., by patient indication of initial discomfort that may be used to set the specified water retention threshold below the amount of retained water at the time of the patient indication. Accordingly, the specified water retention threshold may be adjusted according to feedback from the patient.

Limiting abdominal distention and reducing uncomfortable side effects thereof may be carried out in various ways. For example, controller 141 may be adjusted manually 142, e.g., by supervising personnel such as a nurse, via a console 144, and/or controller 141 may be associated with a processor 143, such as a computing device 143 disclosed in FIG. 1D below. Manual adjustment 142 and/or control by computing device 143 may be carried out with respect to patient feedback, e.g., adjustments of the specified water retention threshold may be made in case the patient indicates initial uneasiness or other indication of commencing symptoms of abdominal distension.

In certain embodiments, measurements of sensor(s) 161 may be transferred to controller 141 per wire and/or via a wireless communication link 99. When associated with processor 143, controller 141 and/or processor 143 may be configured to calculate the amount of water retained in the patient as R(t)=I(t)−O(t), with I(t) denoting an amount of the introduced water at any given time t and O(t) denoting an amount of the drained water at any given time t. The continuous estimation of the amount of retained water may be used to provide a risk assessment for abdominal distension and enable to avoid reaching that state.

The amount I(t) of introduced water 132 may be integrated by controller 141 and/or be displayed or visually estimated using gauge 136 (see FIG. 1B), e.g., by the personnel operating system 100 and/or electronically. The amount O(t) of drained water 139 may be integrated by processor 143 and/or controller 141 as explained below, and/or be displayed or visually estimated using a window 152 (e.g., above pipe 138, possibly with illumination 164 to improve visibility, see, e.g., FIG. 1C) and a mirror 153 configured to enable the estimation of the amount and characteristics of drained water by the personnel operating system 100 (and see FIG. 1E below).

Processor 143 may be further configured to estimate O(t) by integrating over time a liquid height h(t) in drainage pipe 138. For example, sensor(s) 161 may comprise one or more camera(s) 161 having a field of view (FoV) covering a part of transparent drainage pipe 138 and configured to image that part externally, to determine the amount of drained water flowing by in pipe 138. A background 163 may be set in the FoV behind transparent pipe 138, to provide contrast for camera(s) 161. In a non-limiting example, sensor(s) 161 may comprise one or more video camera(s) 161 that records transparent pipe 138 against a white background 163 and associated with transmitter 162 configured to communicate the video stream to processor 143. In certain embodiments, illumination source 164 (illustrated schematically in FIG. 1C) may be used to enhance visibility and/or improve measurements by sensor(s) 161. In certain embodiments, sensor(s) 161 may be directly associated with processor 143 configured to pre-process the sensor measurements and derive data pertaining to the amount of drained water, which may then be transmitted to processor 143 associated with controller 141 and/or directly to controller 141. For example, sensor measurements (e.g., direct measurements, images and/or video streams) may be processed to measure over time a liquid height h(t) (indicated schematically) in drainage pipe 138.

In certain embodiments, camera(s) 161, sensor(s) 161 and/or an optical inspection unit 150 associated therewith may be configured to apply spectral analysis (e.g., in the visual infrared and/or ultraviolet ranges, see example below) to the drained contents, e.g., to detect blood in the drained contents, characterize the drained contents according to its color and/or consistence to detect specific compounds in the drained contents, and/or to distinguish between yellowish mucous effluent and brownish solid contents. The latter may be used in relation to the estimated location along the large intestine to define sampling (see below) from respective portions of the contents. Specifically, mucous effluent may be sampled as characterizing the ascending colon, as distinguished from more distal parts of the large intestine (e.g., the descending colon). In certain embodiments, spectral analysis results may be correlated with the estimation of the position along the large intestine (as derived, e.g., from drainage duration and contents consistence), e.g., by an analysis module 160 to increase the accuracy of sampling and of large intestine characteristics, including the spatial distribution of its microbiome and/or related clinical issues.

In certain embodiments, drained contents 139 may be assumed to include only water delivered by water delivery unit 130, ignoring added large intestine content for the purpose of monitoring the amount of liquid (R(t)). Such assumption is reasonable as the amount of introduced water is typically much larger than the amount of large intestine contents removed in the cleansing process. In certain embodiments, the amount of large intestine contents added to drained water to yield drained contents (O(t)) may be estimated in various ways, such as a fixed estimation or an estimation from the measurements by sensor(s) 161. Denoting drained contents O(t)=W(t)+C(t), with W(t) denoting drained water which was previously introduced into the large intestine and C(t) denoting contents of the large intestine that was drained with the water for cleansing the large intestine, both as expressed time-dependent amounts—various embodiments may comprise any of the following: (i) ignoring C(t), assuming O(t)=W(t); (ii) assuming a fixed or time-dependent estimation C′(t) for C(t), assuming O(t)=W(t)+C′(t); (iii) estimating C(t) from the sensor measurements, for example in relation to the level of cleanliness of drained contents 139 as measured by the optical density or any other measure of the relative amount of material originating from the large intestine in drained contents 139. In certain embodiments, illumination source 164 may be configured to enhance the measurement of W(t) and/or C(t), e.g., by using one or more appropriate wavelengths for the measurements, with sensor(s) 161 and processor(s) 143 possibly being configured to distinguish introduced water from contents of the large intestine that was drained with the water, e.g., spectrally by comparing measurements at different wavelengths.

In certain embodiments, sensor(s) 161 may be further configured to extract over time diagnostic parameters of drained contents 139 from the measurements. For example, measured diagnostic parameters may comprise the color and/or consistency of drained contents 139 over time, optionally relating the diagnostic parameters to the timing of drainage and correlating them with an estimated source location in the patient's large intestine, as disclosed below.

In certain embodiments, as disclosed below, water delivery unit 130 may be further configured to modify a pressure of 132 introduced water, e.g., in relation to drained contents 139 and properties thereof, such as its amount over time and/or the measured diagnostic parameters. Pressure modification may be used to enhance the cleaning process, the derived diagnostic parameters and/or the correlation to the location in the large intestine, while disclosed monitoring of the amount of drained water may be used as disclosed, to limit abdominal distension and alleviate uncomfortable side effects related to it.

In various embodiments, as disclosed below (see, e.g., FIG. 1E), systems 100 may further comprise an analysis module 160 configured to determine a large intestine cleanliness level according to drained contents 139 of the patient's large intestine and/or to derive large intestine characteristics by analyzing at least one portion of drained contents 139, possible with the deriving being carried out using at least most of drained contents 139.

FIG. 1D is a high-level block diagram of exemplary computing device 143, which may be used with embodiments of the present invention. Computing device 143 may include a controller or processor 173 that may be or include, for example, one or more central processing unit processor(s) (CPU), one or more Graphics Processing Unit(s) (GPU or general-purpose GPU-GPGPU), a chip or any suitable computing or computational device, an operating system 171, a memory 172, a storage 175, input devices 176 and output devices 177. Any of system 100, processing unit 120, water delivery unit 130, control unit 140 and/or controller 141, processor 143, optical inspection unit 150, analysis module 160 or other system modules may be or include a computer system as shown for example in FIG. 1D.

Operating system 171 may be or may include any code segment designed and/or configured to perform tasks involving coordination, scheduling, arbitration, supervising, controlling or otherwise managing operation of computing device 143, for example, scheduling execution of programs. Memory 172 may be or may include, for example, a Random Access Memory (RAM), a read only memory (ROM), a Dynamic RAM (DRAM), a Synchronous DRAM (SD-RAM), a double data rate (DDR) memory chip, a Flash memory, a volatile memory, a non-volatile memory, a cache memory, a buffer, a short term memory unit, a long term memory unit, or other suitable memory units or storage units. Memory 172 may be or may include a plurality of, possibly different memory units. Memory 172 may store for example, instructions to carry out a method (e.g., code 174), and/or data such as user responses, interruptions, etc.

Executable code 174 may be any executable code, e.g., an application, a program, a process, task or script. Executable code 174 may be executed by controller 173 possibly under control of operating system 171. For example, executable code 174 may when executed cause the production or compilation of computer code, or application execution such as VR execution or inference, according to embodiments of the present invention. Executable code 174 may be code produced by methods described herein. For the various modules and functions described herein, one or more computing devices 143 or components of computing device 143 may be used. Devices that include components similar or different to those included in computing device 143 may be used, and may be connected to a network and used as a system. One or more processor(s) 173 may be configured to carry out embodiments of the present invention by for example executing software or code.

Storage 175 may be or may include, for example, a hard disk drive, a floppy disk drive, a Compact Disk (CD) drive, a CD-Recordable (CD-R) drive, a universal serial bus (USB) device or other suitable removable and/or fixed storage unit. Data such as instructions, code, VR model data, parameters, etc. may be stored in a storage 175 and may be loaded from storage 175 into a memory 172 where it may be processed by controller 173. In some embodiments, some of the components shown in FIG. 1D may be omitted.

Input devices 176 may be or may include for example a mouse, a keyboard, a touch screen or pad or any suitable input device. It will be recognized that any suitable number of input devices may be operatively connected to computing device 143 as shown by block 176. Output devices 177 may include one or more displays, speakers and/or any other suitable output devices. It will be recognized that any suitable number of output devices may be operatively connected to computing device 143 as shown by block 177. Any applicable input/output (I/O) devices may be connected to computing device 143, for example, a wired or wireless network interface card (NIC), a modem, printer or facsimile machine, a universal serial bus (USB) device or external hard drive may be included in input devices 176 and/or output devices 177.

Embodiments of the invention may include one or more article(s) (e.g., memory 172 or storage 175) such as a computer or processor non-transitory readable medium, or a computer or processor non-transitory storage medium, such as for example a memory, a disk drive, or a USB flash memory, encoding, including or storing instructions, e.g., computer-executable instructions, which, when executed by a processor or controller, carry out methods disclosed herein.

Aspects of the present invention are described above with reference to flowchart illustrations and/or portion diagrams of methods, apparatus (systems) and computer program products according to embodiments of the invention. It will be understood that each portion of the flowchart illustrations and/or portion diagrams, and combinations of portions in the flowchart illustrations and/or portion diagrams, can be implemented by computer program instructions. These computer program instructions may be provided to a processor of a general-purpose computer, special purpose computer, or other programmable data processing apparatus to produce a machine, such that the instructions, which execute via the processor of the computer or other programmable data processing apparatus, create means for implementing the functions/acts specified in the flowchart and/or portion diagram or portions thereof.

These computer program instructions may also be stored in a computer readable medium that can direct a computer, other programmable data processing apparatus, or other devices to function in a particular manner, such that the instructions stored in the computer readable medium produce an article of manufacture including instructions which implement the function/act specified in the flowchart and/or portion diagram or portions thereof.

The computer program instructions may also be loaded onto a computer, other programmable data processing apparatus, or other devices to cause a series of operational steps to be performed on the computer, other programmable apparatus or other devices to produce a computer implemented process such that the instructions which execute on the computer or other programmable apparatus provide processes for implementing the functions/acts specified in the flowchart and/or portion diagram or portions thereof.

The aforementioned flowchart and diagrams illustrate the architecture, functionality, and operation of possible implementations of systems, methods and computer program products according to various embodiments of the present invention. In this regard, each portion in the flowchart or portion diagrams may represent a module, segment, or portion of code, which comprises one or more executable instructions for implementing the specified logical function(s). It should also be noted that, in some alternative implementations, the functions noted in the portion may occur out of the order noted in the figures. For example, two portions shown in succession may, in fact, be executed substantially concurrently, or the portions may sometimes be executed in the reverse order, depending upon the functionality involved. It will also be noted that each portion of the portion diagrams and/or flowchart illustration, and combinations of portions in the portion diagrams and/or flowchart illustration, can be implemented by special purpose hardware-based systems that perform the specified functions or acts, or combinations of special purpose hardware and computer instructions.

FIG. 1E is a high-level schematic illustration of large bowel cleansing system 100, according to some embodiments of the invention. Embodiments of large bowel cleansing system 100 may be integrated with embodiments of kit 101 for acoustic sensing as described below.

System 100 may include water delivery unit 130 (also see FIG. 2A below) including water supply 131 and nozzle 135 connected thereto, configured to introduce water controllably into the patient's large intestine, drainage 151 configured to drain the introduced water with contents of the patient's large intestine (denoted by numeral 139), and analysis module 160 configured to determine a large intestine cleanliness level according to drained contents 139 of the patient's large intestine. Analysis module 160 may be further configured to derive patient diagnostics by analyzing drained contents 139 of the patient's large intestine. For example, the analyzing may be carried out using a biological assay of drained contents 139, such as an application of cancer markers thereto. Advantageously, the analysis may be carried out using at least most of drained contents 139 or all of drained contents 139, thus providing a sample having a large volume that may enable efficient and sensitive diagnosis.

In certain embodiments, the drained large intestine's contents may be separated after its original location in the large intestine, e.g., contents of the left colon, the central colon and the right colon may be separated from each other and be characterized independently (physically, optically, chemically and/or biologically). Specific sections of the large intestine may be separated from the rest of the large intestine's content, according to specified definitions that may relate to the patient's possible medical conditions. A sequence of sections of the large intestine may be diagnosed independently, both in respect to contents as well as acoustically. The acoustic measurements may be used as indicators for the splitting of the large intestine into sections and/or may provide additional data for the analysis of the large intestine's contents from each section. The spatial information concerning the contents of the large intestine may be utilized to provide more effective medical diagnosis, as certain conditions may be location-specific, and isolating the contents from a specific section of the large intestine may provide more concentrated samples for analysis than the whole bowel contents. The possibility provided by the system to register the position of each portion of the contents opens up a new dimension in the ability to pinpoint the origins of various large intestine medical conditions. It is known, for example, that certain conditions originate from very specific locations in the large intestine, and that the microbiota and relevant secreted products or related cellular metabolites may vary significantly along the large intestine. Non-limiting examples for secreted products or related cellular metabolites include any of peptides, gas molecule such as nitric oxide (NO), primary and/or secondary metabolites such as amino acids, bile acids and short and/or long chain fatty acids. System 100, e.g., via analysis module 160, may be configured to diagnosis respective conditions from detected microbiota and/or relevant secreted products or related cellular metabolites in sample portions from specific locations along the large intestine, such as different ecological niches or different biogeographic locations in the colon. It is noted that microbiome characteristics may include the microbiota organisms and/or secreted products or related cellular metabolites.

In certain embodiments, drained contents 139 may flow from the system's basin 154 via one or more transparent drainage pipe(s) 138 as part of drainage 151 and the analyzing may be carried out optically through transparent drainage pipe 138, e.g., as disclosed above. For example, a light source (below window 152) may be located next to the transparent drainage pipe and analysis module 160 may employ optical analysis methods using camera(s) 161 and image processing software, possibly as part of optical inspection unit 150 (illustrated in FIG. 2A). It is noted that camera 161 may be the same as the one used to estimate the amount of drained water 139 (see, e.g., FIG. 1A above) or may be set in addition thereto, depending on the spatial configuration of system 100. Camera 161 may be used to record effluent 139 seen in viewing tube 138 for monitoring progress of cleanliness of the bowel from a control center external to the room where the patient is located, and an analytical tool in analysis module 160 may be configured to perform analysis of pathological indicators e.g., excretion of red blood, black stool, indicators of diverticula (such as corresponding pellets of stool). Image processing may be carried out locally or by a remote service and diagnosis of the images may be carried out automatically (e.g., by the analytical tool), manually, e.g., by a local or remote expert or by a combination thereof. The analytical tool may comprise algorithms configured to generate corresponding alerts once finding suggest any type of abnormality.

Analysis module 160 may be further configured to relate at least two, or at least three portions of the drained contents with at least two, or at least three sections of the large intestine. The relation may be carried out e.g., according to the time of drainage of the portions, according to characteristics of the drained content (e.g., consistence, shape, color, etc. related to diagnosed conditions in the large intestine sections), according to spectral analysis of signals, images and/or video streams from sensor(s)/camera(s)/video 161, according to acoustic measurements of the large intestine section and the drainage and/or according to modifications in the pressure of the introduced water and drained contents, which may be related to positional information along the large intestine. It is noted that any one of these methods, or a combination of two or more of these methods may be used to relate two, three or more portions of the drained contents with respective sections of the large intestine, and to sample these portions as disclosed herein.

Analysis module 160 may be further configured to derive microbiome characteristics of the at least two, or at least three sections of the large intestine by analyzing the corresponding at least two, or at least three portions of the drained contents. Analysis module 160 may be further configured to derive microbiome characteristics of the at least three sections of the large intestine including an ascending part thereof, by analyzing the corresponding at least three portions of the drained contents, including at least one portion from the ascending part of the large intestine. For example, a diversity, an abundance, and chemical and/or genetic characteristics of the microbiome may be derived from analyzing different portions of the contents. The microbiome characterization may be used to reinstate the original microbiome after a treatment, or be modified under spatial analysis of a present and a specified microbiome composition and/or community and/or ensemble. In certain embodiments, the drained contents may be used to provide a FMT for transplantation after a treatment as an auto-FMT. Any type of microbiotic infusion may be used as microbiota transplant (MT) to enhance or replace the characterized microbiome, at least on one section of the large intestine. For example, MTs may comprise any kind of FMT or microbiome related transplant, possibly with the source of the inserted material being from stool, from colon effluent and/or comprising a rationally-designed bacterial consortium or various biochemical compositions.

Advantageously, system 100 enables use of most or all of the drained contents for characterizing the microbiome of the patient, thus providing an exhaustive and reliable analysis. Alternatively or complementarily, system 100 enables sampling contents and/or effluent from specific regions of the large intestine and/or with respect to specific contents characteristics (e.g., following spectral analysis)—in a non-invasive manner.

For example, the microbiotic diagnosis and transplant may be used to diagnose and treat Clostridium difficile (C. Diff) infections. The combined treatment of cleansing the large intestine and transplanting a MT may be combined using system 100, thus becoming cleansing and transplantation system 100. Moreover, system 100 may be used to provide a healthy donor-based stool bank and/or to create a biobank, which stores large intestine contents and/or effluents, isolated bacteria, strains, and/or related compounds from healthy subjects (e.g., with samples from cleansing system 100 from any subject and/or from subjects being prepared for colonoscopy examinations) or subjects with any clinical indication that may be used for research and treatment. Biobank samples may comprise inner cellular metabolites and/or peptides and/or samples of secreted compounds. Biobank samples may comprise isolated strains, metabolites and/or molecules, and be stored as solid, liquid and or gaseous samples. Data relating to any of the stored materials, such as data characterizing any of the large intestine contents and/or effluents, isolated bacteria, strains, and/or related compounds and molecules, may be part of the biobank, and/or used independently of using the actual samples. Moreover, donors to the stool bank and/or biobank may utilize the stored samples (e.g., as autologous FMTs) and/or any of isolated bacteria, strains, related compounds and/or data related thereto—for microbiome rehabilitation after deterioration, thus treating, resetting or healing imbalances related to the large intestine, such as caused by dietary changes, antibiotics, apnea, therapies, diseases, and jetlag.

In some embodiments, whole stool sampling may be used to overcome the inherent patchiness of the microbiome and patchiness patterns may be analyzed using the accumulating contents from many patients. In some embodiments, samples of colon effluent, with or without stool sampling, correlated with one, two, three or more locations along the large intestine—may be used to characterize the inherent patchiness of the microbiome and used to directly analyze patchiness patterns and related symptoms. As shown below, both stool and effluent may be used to derive unique information, as does spatial analysis of the large intestine contents, which may include stool and/or effluent.

Certain embodiments comprise using system 100 to drain and to store a plurality of the drained contents' samples from a plurality of the patients, in association with the derived microbiome characteristics of the drained contents samples. Moreover, system 100 may be utilized to establish a stool bank and/or biobank for storing and providing drained contents' samples, isolated strains and/or compounds related thereto. Certain embodiments comprise a stool bank and/or biobank with the plurality of drained large intestine contents' samples and/or compounds related thereto from the plurality of patients, associated with derived microbiome characteristics of the drained large intestine contents samples, wherein the drained large intestine contents' samples are drained after controllable water introduction into the patients' large intestines. Biobank samples may comprise inner cellular metabolites and/or peptides and/or samples of secreted compounds. Biobank samples may comprise isolated strains, metabolites and/or molecules, and be stored as solid, liquid and or gaseous samples. Data relating to any of the stored materials, such as data characterizing any of the large intestine contents and/or effluents, isolated bacteria, strains, and/or related compounds and molecules, may be part of the biobank, and/or used independently of using the actual samples.

In certain embodiments, the stool bank and/or biobank storage may comprise samples, compounds and/or data related to the samples from at least part of the ascending portion of the large intestine, as disclosed below, providing access to microbiota and/or relevant secreted products or related cellular metabolites. Secreted products and/or cellular metabolites may include, but are not limited to—peptides, gas molecule such as nitric oxide (NO), primary and secondary metabolites such as amino acids, bile acids and short and/or long chain fatty acids (SCFA, LCFA). It is noted that microbiome characteristics are shown herein to be distinct from prior art stool samples, and moreover, microbiome characteristics of the ascending part of the large intestine are shown here to be clearly distinguishable from the microbiome characteristics of the descending and even the transverse parts of the large intestine—including unique species and possibly microbiota that is essential for the health of the large intestine (see, e.g., FIGS. 6A-11B). It is further noted that the stool bank and/or biobank may comprise any part of the collected effluent (e.g., inner cellular metabolites and/or peptides and/or samples of secreted compounds), possibly associated with the related sampling location along the large intestine, such as whole samples (e.g., stool and/or colon effluent), isolated strains and/or isolated metabolites and molecules, stored as solid, liquid and/or gas, as well as data related thereto.

The samples may be used in different ways, e.g., for infusion (transplantation) of certain pre-screened stool samples and/or of related microbiome infusions; for administering of specific bacteria, probiotics, antibiotics and/or therapeutics related to the derived microbiome characteristics; for infusion (transplantation) of autologous samples; for prescribing food additives, food supplements, medications and/or therapies related to the derived microbiome characteristics. Any of the above may be related to specific patients and/or to specific patient groups.

Returning to FIG. 1E, in certain embodiments, mirror 153 above transparent drainage pipe 138 may reflect drained contents 139 to a camera and an image processing unit, and/or to a staff person to determine the consistency of drained contents 139, specific diagnostic appearances (e.g., color, objects etc.) and eventually the cleanliness level of the patient's large intestine by noting the amount of drained content 139 flowing through drainage 151. It is noted that mirror 153 may also be used by the patient and/or by a staff member to simplify the process of inserting nozzle 135 into patient's anus 96. Alternatively or complementarily, a utensil 185 including two mirrors 153A, 153B mounted on a handle 186 may be configured to enable visualization of the nozzle insertion by the patient and/or by the physician. Utensil 185 may be designed or be configurable to enable easy self-insertion of nozzle 135 into anus 96 by the patient, or simplify the insertion procedure when carried out by a physician or other medical personnel.

System 100 may include a support 180 configured to support the patient's legs to help the patient maintain an appropriate posture during the procedure. For example, support 180 may have two interconnected hooks 180A, one for supporting each leg or knee. Hooks 180A may be interconnected by any connecting member 180B such as a flexible or rigid strap or bar, a band etc. Support 180 may be configured to anchor the legs of the patient on hydrocolonic preparation system 100, allowing the legs to fall sideways while supporting them against each other (the force applied by each leg on respective hook 180A are balanced and maintained by connecting member 180B) to maintain a required posture conveniently, as water flows through the nozzle into the rectum. Support 180 may be configured to allow the patient to sit comfortably in the required position for an extended period of time as may be required by the procedure.

In certain embodiments, analysis module 160 may be further configured to derive large intestine characteristics by analyzing parameters of drained water and contents 139. For example, an exceptionally large amount of contents 139 may signify a large volume of large intestine, or contents 139 with specific features may be used to indicate specific large intestine features (e.g., small hard round clumps may signify large intestine diverticula). Certain large intestine characteristics may be corroborated by deriving them from both the acoustic signals and the contents analysis.

In certain embodiments, system 100 may further include a MT unit 170 configured to transplant a microbiota transplant (MT) such as a fecal microbiota transplant (FMT) or into the patient's large intestine after a predetermined cleanliness level thereof is determined. MT transplantation may be carried out e.g., via water supply, before or after cleansing and/or colonoscopy. For example, MTs may comprise any kind of FMT or microbiome related transplant, possibly with the source of the inserted material being from stool, from colon effluent and/or comprising a rationally-designed bacterial consortium or various biochemical or chemical compositions.

In certain embodiments, water delivery unit 130 may be further configured to modify a pressure of introduced water 132 and analysis module 160 may be further configured to measure a pressure of drained water and contents 139, and derive large intestine characteristics by correlating the measured drainage pressure with the pressure of introduced water according to a specified model. The reaction of the large intestine to different pressures may indicate certain characteristics thereof, such as peristaltic parameters of the large intestine and possibly certain anomalies. Measuring the difference in pressure between the water flowing into the anus (132) and the effluent flowing out of the anus (139) may be used to provide new information regarding the effectiveness of the peristaltic waves created by the muscles of the colon. Acoustic signals relating to the introduction of pressurized water may also be analyzed to derive additional information about the large intestine, so that the analysis of the acoustic signals and the analysis of the contents of the large intestine may be combined synergistically.

Certain embodiments may include any combination of acoustic signal sensing and large intestine content analysis. For example, system 100 may include water delivery unit 130 including water supply 131 and nozzle 135 connected thereto, configured to introduce water controllably into the patient's large intestine, drainage 151 configured to drain the introduced water with contents of the patient's large intestine, acoustic sensor(s) 110 that are attachable to the patient's abdomen, and processing unit 120, possibly incorporating analysis unit 160, configured to determine a large intestine cleanliness level according to drained contents 139 of the patient's large intestine as well as to derive large intestine characteristics by analyzing and correlating acoustic signals received from acoustic sensors 110, to which processing unit 120 is connected, with parameters of the drained water and contents.

FIGS. 2A-2C are high level schematic illustrations of a system 100, according to some embodiments of the invention. It is noted that elements of system 100 from FIGS. 1 and 2A may be combined to various embodiments of system 100. System 100 may be used to calculate or derive information about a patient's large intestine by processing acoustic signals received by sensors placed on the patient's abdomen. The information may be provided to physician, e.g., as preparation for colonoscopy procedures. It is noted that the illustrated elements of the patient's digestive tract 90, namely stomach 91, small intestine 92, large intestine 93, sigmoid colon 94 (being the last part of large intestine 93), rectum 95 and anus 96 are shown schematically, in a non-limiting manner. FIG. 2A schematically illustrates system 100 while FIGS. 2B and 2C schematically illustrate sensor configurations, according to some embodiments of the invention. System 100 may be configured to cleanse the patient's large intestine, e.g., as a preparation for a colonoscopy procedure.

The inventors have found out that the acoustic signals, e.g., ones generated during the cleansing of the large intestine, may be used to derive significant information about the large intestine, such as indications whether the structure and position of the large intestine are normal or abnormal, simple or complex, and/or adequate or not for performing colonoscopy (abnormalities and complexity may be of different kinds); and various large intestine characteristics such as geometric parameters thereof and flow characteristics therethrough. The derivation of the large intestine characteristics may be carried out experimentally, by relating measured acoustic signals to known large intestine characteristics in a calibration process, utilizing theoretical or empirical models describing flow properties through the large intestine and by comparing acoustic signals from different parts of the abdomen and/or from different measurement times to derive differences that are indicative of large intestine characteristics or progress of the water flow and cleansing into the proximal large intestine (closer to the cecum and distal to the anus). As a simple example, the measurement of flow noise may be used to indicate the location and general form of the large intestine. In another example, modifying water flow through the large intestine and correlation thereof with the changing acoustic signals may be used to refine the measurement of geometrical parameters of the large intestine and furthermore provide information about flow patterns therethrough (e.g., indicate the resistance of the large intestine to flow, enable as evaluation of intestine wall thickness, relate to the peristaltic movements of the large intestine etc.). Large intestine characteristics may be measured spatially, relating to specific sections of the large intestine.

System 100 may include a water delivery unit 130 including a water supply 131 (e.g., a container with a controlled outflow valve) and a nozzle 135 connected thereto, configured to introduce water through nozzle 135 controllably (as explained below) into a patient's large intestine 93, a plurality of acoustic sensors 110 (e.g., microphones) that are attachable to a patient's abdomen, and a processing unit 120 which is connected to acoustic sensors 110 and is configured to calculate or derive large intestine characteristics by analyzing acoustic signals that are related to noise received from acoustic sensors 110, the noises resulting from movements of water, large bowel content and/or air bubbles through the large intestine, that are initiated through the water introduction. Sounds of water flow introduced into the large intestine may allow diagnosing structural features of large intestine 93 such as its shape and layout, dimensions of its various section, width along its length and presence of specific features such as pouches (diverticula), redundant loops, irregular geometrical and/or positional features etc.

In certain embodiments, acoustic sensors 110 may be configured to communicate with processing unit 120 over wires or wirelessly, the latter via transmitters attached to acoustic sensors 110 which do not have a galvanic connection to the patient's body.

System 100 may include a control unit 140 configured to control water delivery unit 130 according to instructions or control signals received from processing unit 120 which relate to the acoustic signals analysis. For example, water delivery may be stopped, increased, enhanced, made periodic or any parameters of water delivery may be modified in order, e.g., to verify or improve analysis initial findings.

Processing unit 120 may be configured to compare acoustic signals emanating from the large intestine with acoustic signals emanating from other regions, e.g., the small intestine, to identify and remove background acoustic noise. For example, one or more sensors 110 may be positioned away from large intestine 93 (see e.g., central sensor 110 in FIG. 2A or four central sensors in FIG. 2B) and their signals may be used as characterizing the background noise. Processing unit 120 may receive multiple channels from sensors 110, convert the analog audio signals into digital signals (by analog to digital converter, ADC 121) and further process the digital signals.

Processing unit 120 may be configured to compare acoustic signals (from large intestine noises) received before the water introduction with acoustic signals received after the water introduction and/or processing unit 120 may be configured to compare acoustic signals received before the introduced water reaches at least one specified region with acoustic signals received after the introduced water reaches the at least one specified region. In certain embodiments, signals received from sensors 110 positioned along large intestine 93 (see e.g., FIG. 2C and the corresponding sensors in FIGS. 2A and 2B) and sampled sequentially to track water reaching the corresponding large intestine sections positioned below sensors 110. The sequential sampling may include sampling sensors 110 according to the position along the large intensity, sampling one or more sensors 110 sequentially over a specified period of time (e.g., over the time it takes to fill and/or empty the large intestine) and/or any combination of these sampling approaches. In certain embodiments, water delivery unit 130 may be configured to introduce air bubbles of different sizes into the large intestine (e.g., air bubbles of different sizes maybe introduced simultaneously or bubbles of uniform but selectable size may be introduced at one or several times), and processing unit 120 may be configured to calculate or derive information from acoustic signals emitted due to the bubble introduction and bubble behavior in the large intestine. For example, bubble-induced noises may be used to improve the delineation of the large intestine, to derive information about the diameter of the large intestine at different portions thereof and/or to indicate pressure levels that characterize different sections of the large intestine (varying the pressure of introduced water, which is described below, may be applied to achieve this end together with the introduction of bubbles). Processing unit 120 may be configured to utilize and/or analyze any type of water-flow and air-flow modulations and the progress along the large intestine of flow noise resulting from the introduction. Sensors 110 may be placed accordingly along the nominal location of the large intestine, and/or at additional locations for reference and/or for detecting abnormalities or exceptional features in the large intestine, especially ones relating to the performance of a subsequent colonoscopy procedure (see FIGS. 3A-3D below for more details on the acoustic signal analysis).

In certain embodiments, acoustic sensors 110 may be attached along an expected position of the patient's large intestine (see e.g., FIG. 2C), additional sensors 110 may be attached at at least one location aside from or not at the expected position of the patient's large intestine (see e.g., FIGS. 2A and 2B) and/or acoustic sensors 110 may be attached at an array covering the patient's abdomen (see e.g., FIG. 2B). The positioning of sensors 110 may be optimized over a large number of patients and water delivery schemes and/or may be personalized according to each patient's specific characteristics and possibly modified in view of accumulating analysis results.

In certain embodiments, sensors 110 may be connected to a frame or framework 112 configured or adapted to an expected form of the patient's large intestine. Framework 112 may be stiff or flexible, and may allow accommodation to the shape and dimensions of the patient's abdomen. Sensors 110 may be attached to the patient's abdomen by various means such as suction, adhesion (e.g., stickers), structural conformity to the patient's abdomen and/or by the configuration of framework 112 to yield effective transfer of acoustic waves from the patient's body to sensors 110. In certain embodiments, framework 112 may be wearable, e.g., sensors 110 may be incorporated in a vest as framework 112, configured to facilitate correct positioning of sensors 110.

In certain embodiments, the water introduction may include at least one time period of continuous water introduction and at least one period of a pulsated or intermittent water introduction, and processing unit 120 may be configured to analyze acoustic signals received during the at least two periods.

In certain embodiments, the sensed acoustic signals and/or the calculated or derived large intestine characteristics may be used to derive an alert or indication concerning a consequent colonoscopy procedure and/or an indication of large intestine anomaly, exceptional features or adequacy for colonoscopy. The alert or indication may be delivered as any type of output, such as a textual indication, a visual or an auditory signal and so forth, and by any medium (e.g., a display, a speaker, a medical record etc.). In certain embodiments, the calculated or derived large intestine characteristics may include for example: an indication of large intestine anomaly, a categorization of the patient's large intestine (e.g., into medically significant classes), at least one geometric parameter of at least one region of the large intestine (e.g., length, width, position, wall thickness, etc.) and at least one parameter of water flow through the large intestine (such as throughput, speed of flow, regions which receive little or no flow, etc.).

Certain embodiments include a kit 101 (FIG. 2A) including acoustic sensors 110 that are attachable to a patient's abdomen, and processing unit 120 connected to acoustic sensors 110 and configured to derive large intestine characteristics by analyzing acoustic signals received therefrom, which are associated with water introduction to the patient's large intestine. The placing of sensors 110, configurations of processing unit 120 and derived large intestine characteristics may be similar to the one described above for system 100. Kit 101 may comprise the parts of system 100 which handle the acoustic sensing and processing, such as acoustic sensors 110 and elements of processing unit 120 and related units. Kit 101 may include placing instructions for acoustic sensors 110 and/or diagnostic flow(s) that relate processing results with the large intestine characteristics and/or with corresponding medical conditions.

In certain embodiments, system 100 may further include a drainage 151 configured to drain introduced water with contents of the patient's large intestine 139 and an analysis module 160 (which may be part of, integrated with or include processing unit 120) that is configured to determine a large intestine cleanliness level according to the drained contents of the patient's large intestine. Further details were provided above concerning FIGS. 1A-1E. Analysis module 160 may comprise a separation unit 165 such as a mesh apparatus, configured to separate contents of the large intestine such as feces from the water in drained contents 139.

System 100 may be configured to cleanse the patient's large intestine, e.g., as a preparation for a colonoscopy procedure. Water delivery unit 130 may be further configured to introduce at least one additive 133 with introduced water 132. Additive(s) 133 selected to enhance cleansing of the patient's large intestine. For example, at least one additive 133 may include biological detergents that can be shown to be acceptable for use in large intestine cleansing procedures.

Analysis of drained material 139 may be carried out, for example optically, by an optical inspection unit 150 (e.g., implementing spectral analysis) and/or using a biological assay, such as one including various markers, e.g., cancer markers. Processing unit 120 may be configured to determine existence of specific diseases based on analyzing biochemical and/or biological (e.g., genetic, taxonomic, and/or phylogenetic as non-limiting examples) characteristics of the contents of the patients' large intestine to markers for such diseases. It is emphasized that the analysis may be carried out with respect to most or all of the large bowel contents, thus providing significant diagnostic advantages over prior art diagnosis that is based on partial sampling of the large bowel content. The biological assay may be carried out as part of system 100 or at least partially by external labs. The biological assay may be carried out in real-time, or at least partially a certain period after the contents has been drained.

Processing unit 120 and/or control unit 140 and/or analysis module 160 may be configured to carry out methods according to embodiments of the present invention by for example executing software or code (for example stored in memory 125) and/or by including dedicated circuitry.

FIGS. 3A-3D are high level schematic flowcharts and illustrations of methods 242 of deriving large intestine characteristics from acoustic signals, according to some embodiments of the invention. Methods 242 may commence with acquiring or obtaining the acoustic signals (stage 221), denoted by P(x_i, t)-P for the signals, x_ifor the respective location of the i^thsensor 110 and t for the time from the beginning of the measurements, inputting or receiving a start time t₁and an end time t₂(stage 222) and determining a noise pattern {tilde over (P)} (x, t₁, t₂) (stage 223, and see FIG. 3D below). Then, FIG. 3A exemplifies an option of displaying {tilde over (P)}(x, t₁,t₂) (stage 226A) for further visual analysis or for deriving certain alerts or indications that are based on the appearance of the noise pattern, and then enabling determining the noise pattern {tilde over (P)}(x, t₁, t₂) for another interval (t₁, t₂) (stage 222A). Alternatively or complementarily, FIG. 3B exemplifies an option of deriving a ridge of {tilde over (P)}(x, t₁, t₂) (stage 231), the ridge representing the line of the smallest gradient of {tilde over (P)}(x, t₁, t₂) (alternatively or complementarily, the ridge may represent a central line of the noise pattern that exhibits the highest noise values in a set of cross sections of the pattern), and then displaying the ridge of {tilde over (P)}(x, t₁, t₂) (stage 226B) for further visual analysis or for deriving certain alerts or indications that are based on the appearance and location of the ridge and then enabling determining the ridge of the noise pattern {tilde over (P)}(x, t₁, t₂) for another interval (t₁, t₂) (stage 231A). As illustrated in FIG. 3D, a noise pattern 113 may expand beyond large intestine 93, depending on the sensitivity of sensors 110, their density and locations, the propagation of noise through the patient's abdomen and possible pre-processing algorithms applied to the sensor data. FIG. 3D illustrates schematically noise pattern 113 ({tilde over (P)}) which is centered along large intestine 93 and exhibits a central ridge, i.e., a substantially linear region exhibiting the lowest gradient (and optionally the highest noise level along the cross section) of noise pattern 113. FIG. 3D further illustrates schematically changes in noise intensity along the ridge in graph 122 and the cross section of the pattern's intensity, topping at the ridge, in graph 124. Clearly, the wider pattern 113 is, more refined algorithms are required in order to detect the ridge. Sensors 110, their positions and/or the sound processing algorithms may be adjusted to optimize the detection of a clear ridge in pattern 113. FIG. 3C exemplifies another option, of building a source model around an initial skeleton, which is a two-dimensional projection of the ridge (e.g., onto the plane of the large intestine), then constructing a tubular noise source model around the skeleton and refining skeleton to yield the closest noise pattern {tilde over (P)}(x, t₁, t₂) that fits the measured noise map (stage 233), deriving a skeleton (as estimation of the central line of the large intestine) of the refined noise source model (stage 235), i.e., estimating the outline of the large intestine, and displaying the skeleton as an approximation to the location of the large intestine (stage 226C). The skeleton may then be determined for another interval (t₁, t₂) (stage 235A), and the subsequent skeletons may be used for refinements until a final, most accurate skeleton is reached and used for display. In certain embodiments, the dimensions and layout of the large intestine may be approximated by estimating the distribution of water flow noise sources in the abdomen by means of estimating the skeleton and dimensions of the noise source model that gives rise to the measured and interpolated noise map. Comparisons of the noise source model at different times, or of developing noise source models over time (progress of water flow in the large bowel over time), or of different noise sources (with or without bubbles) or with and without water flow are possibly based on the schemes illustrated in FIGS. 3A-3C. Using the noise source model may improve the derivation of the location of the large intestine by taking into account models for noise propagation within the patient's abdomen, thus removing some of the spatial ambiguity in the acoustic signals depicted by sensors 110.

FIGS. 4A and 4B are high-level flowcharts illustrating methods 200, according to some embodiments of the invention. Method 200 may be carried out using system 100, kit 101 and/or equivalent devices, or other equipment. Other operations or steps may be included. Method 200 may be at least partially implemented by at least one computer processor. Certain embodiments comprise computer program products comprising a computer readable storage medium having computer readable program embodied therewith and configured to carry out of the relevant stages of method 200, e.g., by processor 143. Method 200 may comprise the following stages, from either or both FIGS. 4A and 4B, irrespective of their order.

As illustrated in FIG. 4A, method 200 may comprise introducing water controllably into a patient's large intestine (stage 210), draining the introduced water with contents of the patient's large intestine, e.g., with the large bowel contents (stage 220), relating at least two, or at least three portions of the drained contents with at least two, or at least three sections of the large intestine (stage 222) and deriving microbiome characteristics of the at least two, or at least three sections of the large intestine by analyzing the corresponding at least two, or at least three portions of the drained contents (stage 224). Method 200 may further comprise selecting a microbiota transplant (MT) such as a fecal microbiota transplant (FMT), probiotic infusions, rationally designed microbial consortia or any microbiotic transfusion—according to the derived microbiome characteristics of the at least two, or at least three sections of the large intestine (stage 226) and transplanting the MT, possibly into a specified location related to the characterized section(s) of the large intestine (stage 228). The MT may comprise an autologous FMT, e.g., extracted prior to a treatment and transplanted after the treatment, or any donor FMT or artificial microbiota. Alternatively or complementarily, MTs may comprise colon effluent and/or rationally-designed bacterial consortia or various biochemical or chemical compositions related to the samples.

Method 200 may comprise introducing water controllably into a patient's large intestine (stage 210), sensing acoustic signals at a patient's abdomen (stage 240) and deriving large intestine characteristics by analyzing the sensed acoustic signals associated with the water introduction (stage 242). In certain embodiments, method 200 may further include introducing at least one additive with the water to enhance cleansing of the patient's large intestine (stage 212), for example, additive(s) may comprise biological and/or bio-compatible detergents that are acceptable for use for cleansing the large intestine.

Method 200 may further include identifying local maxima in the sensed noise and deriving an estimated mid-line, or ridge, therefrom (stage 244). In certain embodiments, method 200 may include modelling noise generation in the large intestine and deriving model parameters from the measured noise patterns (stage 246).

Method 200 may include controlling the water introduction according to results of the acoustic signals analysis (stage 248), e.g., to improve sensor readings, analysis and/or derivation of large intestine characteristics.

Method 200 may include for example comparing acoustic signals that are sensed before and after the water introduction (stage 250), comparing acoustic signals from different locations on the patient's abdomen (stage 255), and comparing acoustic signals that are sensed before and after the introduced water reaches at least specified one region (stage 260).

Method 200 may include introducing the water continuously and/or in a pulsated manner (stage 215) and/or introducing air bubbles of different sizes into the intestine (stage 217). Method 200 may include supporting the patient's legs to help the patient maintain an appropriate posture (stage 218), e.g., by a utensil that has two interconnected hooks, one for supporting each leg or knee. Method 200 may further include comparing acoustic signals sensed during continuous and/or pulsated water introduction and/or bubble introduction (stage 265).

Method 200 may further include deriving at least one of: an alert concerning a consequent colonoscopy procedure, an indication of a large intestine anomaly, a categorization of the patient's large intestine, geometric parameter(s) of region(s) of the large intestine and parameter(s) of water flow through the large intestine (stage 270).

In certain embodiments, method 200 may include introducing water controllably into a patient's large intestine (stage 210), draining the introduced water with contents of the patient's large intestine, e.g., with the large bowel contents (stage 220), and determining a large intestine cleanliness level according to the drained contents of the patient's large intestine (stage 290).

Method 200 may further include deriving patient diagnostics by analyzing the drained contents of the patient's large intestine (stage 230). For example, the analyzing may be carried out optically, e.g., through a transparent drainage pipe. Additionally or alternatively, the analyzing may be carried out using a biological assay (e.g., by application of cancer markers) of the drained contents (stage 232). In certain embodiments, most or all of the drained contents may be used for the analyzing (stage 235), improving thereby significantly the diagnostic power of the analysis with respect to prior art methods which are based on small samples of large bowel content.

Method 200 may further include deriving large intestine characteristics by analyzing parameters of the drained water and contents (stage 300). Examples for deriving large intestine characteristics include geometric measures of the large intestine (e.g., volume, length, diameter), physiological measures and anomalies of the large intestine relating to parameters of the drained contents, and so forth. The derivations of large intestine characteristics by analyzing the sensed acoustic signals associated with the water introduction (stage 242) and by analyzing parameters of the drained water and contents (stage 230) may be combined to verify findings and/or to derive compound large intestine characteristics. Moreover, the timing of the received acoustic signals may be correlated with the timing of content drainage to identify causes for specific or generic types of acoustic noise received by the sensors. These analyses may be combined to derive or enhance the derivation of temporal parameters of water and large bowel content flow through the large intestine.

In certain embodiments, method 200 may further include transplanting a microbiota transplant (MT, the term is used as a generalized term to include fecal transplants, probiotic infusions and/or rationally designed microbial consortia) into the patient's large intestine after a predetermined cleanliness level thereof is determined (stage 310). MT/FMT transplantation may be carried out before or after colonoscopy, or as a separate procedure. The location for FMT transplantation may be determined or evaluate according to the derived large intestine characteristics, e.g., with reference to specific structures, locations or abnormalities in the large intestine. The efficiency of MT transplantation may be enhanced by selecting a location with predefined flow parameters which are conducive to successful MT transplantation. MT transplantation may be carried out according to the derived patient diagnostics, e.g., upon detection of certain large intestine infections, and responsive thereto.

Method 200 may further comprise storing drained contents' samples from multiple patients, associated with their derived microbiome characteristics (stage 320) and establishing a stool bank and/or biobank for storing and providing drained contents' samples, isolated strains and/or compounds related thereto (stage 325), e.g., for self and/or foreign FMT transplantation or other treatment and diagnostic options.

In certain embodiments, method 200 may include modifying a pressure or flow of the introduced water (stage 216), measuring a pressure or flow of the drained water and contents (stage 280), and deriving large intestine characteristics by correlating the measured drainage pressure or flow with the pressure or flow of introduced water according to a specified model (stage 285). Exemplary large intestine characteristics may comprise characteristics of different sections in the large intestine, relating e.g., to an ascending part, to a transverse part and to a descending part of the large intestine. The spatial characterization of the large intestine's contents may be enhanced by the acoustic spatial characterization described above. Method 200 may comprise analyzing the large intestine's contents with respect to at least one, at least two, or at least three portion(s) of the contents which correspond to a respective derived at least one, at least two, or at least three section(s) of the large intestine. The derivation of the specific section may be carried out physically, e.g., with respect to the volume of outflowing contents, or acoustically, simultaneously with the acoustic sensing described above.

As illustrated in FIG. 4B, method 200 may comprise introducing water controllably into a patient's large intestine (stage 210), draining the introduced water with contents of the patient's large intestine (stage 220), measuring, continuously, an amount of the drained water (stage 330), and controlling the water introduction with respect to the measured amount of drained water, keeping an amount of water retained in the patient below a specified water retention threshold to limit abdominal distension and reduce uncomfortable side effects thereof (stage 340).

Method 200 may comprise continuously measuring of the amount of the drained water 330 by capturing images of the drained water, optically through a transparent drainage pipe (stage 332). Method 200 may further comprise calculating the amount of water retained in the patient as I(t)−O(t), with I(t) denoting an amount of the introduced water at any given time t and O(t) denoting an amount of the drained water at any given time t (stage 350). For example, method 200 may comprise estimating O(t) by integrating over time a liquid height h(t) in the drainage pipe (stage 352). In certain embodiments, calculating 350 may be carried out over changing water introduction parameters (stage 355). Method 200 may further comprise analyzing at least one portion of the drained contents to derive diagnostic parameters of the drained contents (stage 230), a large intestine cleanliness level (stage 290) and/or the structural and functional characteristics of the large intestine (stage 300). Method 200 may further comprise any stage disclosed with relation to systems 100.

FIG. 5 is a high-level schematic illustration of draining and separating multiple samples of large intestine content 139, according to some embodiments of the invention. FIG. 12 is a high-level flowchart illustrating methods 200, according to some embodiments of the invention. Method 200 may be carried out using system 100, kit 101 and/or equivalent devices, or other equipment. Other operations or steps may be included. Method 200 may be at least partially implemented by at least one computer processor. Certain embodiments comprise computer program products comprising a computer readable storage medium having computer readable program embodied therewith and configured to carry out of the relevant stages of method 200, e.g., by processor 143. Method 200 may comprise the following stages, as well as any of the stages from FIGS. 4A and/or 4B, irrespective of their order.

Certain embodiments comprise methods 200 and systems (or apparatuses) 100 which introduce water controllably into a patient's large intestine (stage 210), drain the introduced water with contents of the patient's large intestine (stage 220), relate at least three portions 139A, 139B, 139C of drained contents 139 with respective at least three sections 93A, 93B, 93C of large intestine 93 (stage 400), during and/or after the draining and according to at least one of: time of drainage of the portions, and characteristics of the drained content, wherein at least one of the at least three sections comprises at least a part of an ascending portion 93C of the large intestine (stage 410), and derive microbiome characteristics of at least three sections 93A, 93B, 93C of large intestine 93 (stage 420) by analyzing corresponding at least three portions 139A, 139B, 139C of drained contents 139 (stage 425), e.g., with respect to their microbiota. In systems 100, analysis module 160 may be configured to relate at least three different portions 139A, 139B, 139C of drained contents 139 with at least three sections 93A, 93B, 93C of large intestine 93 and to derive microbiome characteristics of at least three sections 93A, 93B, 93C of the large intestine by analyzing corresponding at least three different portions 139A, 139B, 139C of drained contents 139, wherein at least one of at least three sections 93A, 93B, 93C comprises at least a part of ascending portion 93C of large intestine 93. For example, as illustrated schematically in a non-limiting manner in FIG. 5, different portions 139A, 139B, 139C of drained contents 139 may comprise at least parts of drained contents of descending (left) colon 93A, transverse colon 93B and ascending (right) colon 93C, respectively.

Advantageously, separating contents 139 into at least three portions, and specifically draining and separating contents of at least part of descending colon 93A may provide new and important diagnostic information and possibly may be used to provide effective treatment—especially with respect to descending colon 93A which is not separately accessible in a non-invasive manner using prior art methods (which are typically invasive, e.g., taking a biopsy). The following experimental results demonstrate the effectiveness of disclosed methods 200 and systems (or apparatuses) 100 to separate among at least three different portions 139A, 139B, 139C of drained contents 139, the different characteristics derived therefrom, particularly with respect to the different microbiota and/or secreted products or related cellular metabolites, and the distinctness of the results from prior art stool samples 70, taken without use of disclosed cleansing systems 100.

The experimental conditions included gravity-fed high volume colonic lavage with induced defecation, and collection of the colon effluent excreted by the patient over time, reflecting the different ecological niches of the colon, from the sigmoid and descending colon, to the ascending colon moving towards the cecum. The procedure was performed by trained personnel under stringent standard operating procedures (SOPs) when medically indicated, such as before colonoscopy. The method has proved safe, effective, and well tolerated in patients with a 97% adequacy in over 17,000 colonoscopy preparations (see, e.g., Hogan et al., 2021, Open-system colon irrigation bowel prep for colonoscopy is a safe and effective alternative to oral prep, JSM Gastroenterol Hepatol 8(1): 1098, and Godell et al., 2021, Colon irrigation bowel preparation supports multiple clinical benefits in over 8,000 patients, Open Journal of Gastroenterology and Hepatology 4:48). Clinical adequacy remains high even in patients with predictors of poor bowel oral preparation such as age, male sex, and co-morbidities. Study participants collected home stool samples for comparison, using a standardized DNA Genotek OMNIgene® stool microbiome collection kit. Colon effluent samples were collected continuously during the gravity-fed high-volume (e.g., >35 liter) colonic lavage procedure described herein. Samples were collected at the beginning, middle, and end of the procedure (approximately 1 hour) to allow for an approximate representation of the descending, transverse, and ascending colon. The last sample collected (from the ascending colon) was characterized by a diluted, mucoid consistency and white-yellowish color, as expected from the ascending colon. The home-collected stool samples were collected by the participants up to 48 hours before their high-volume colon irrigation bowel prep. All samples were immediately preserved in DNA Genotek OMNIGene tubes with a preservation buffer. Overall, up to 20 stool samples and 62 colon effluent samples were collected and sent for either 16S rRNA amplicon sequencing at Microbiome Insights Inc. or for whole genome sequencing (WGS) at SeqMatic LLC.

FIGS. 6A, 6B, 7-10, 11A and 11B illustrate the significant differences of microbiota samples from more proximal portions 93B, 93C of the large intestine, with respect to prior art stool samples 70, according to some embodiments of the invention. It is noted that the following results are related to a prospective Institutional Review Board (IRB)-approved clinical study. It is further noted that these results demonstrate the ability of disclosed systems and methods to sample large intestine contents and effluent non-invasively, even from the ascending portion of the large intestine.

FIGS. 6A-6E illustrate the experimentally measured phylogenetic diversity of the microbiota in three different portions 139A, 139B, 139C of drained contents 139, according to some embodiments of the invention, and compared to prior art stool samples 70.

FIGS. 6A and 6B illustrate the alpha (within-sample) diversity of the stool sample and of the three colon effluent samples in terms of the Shannon index. The diagram provides the individual sampling points and the four quartiles of their distribution. FIGS. 6A and 6B provide data for two different analyses of partially overlapping samples, with the differences in the phylogenetic diversity between all three samples (effluent) 139A, 139B, 139C and prior art stool samples 70 being statistically significant, as calculated for samples 139A, 139B, 139C versus stool samples 70 of FIG. 6B. FIGS. 6A and 6B therefore illustrate the significant difference of microbiota samples from more proximal (and less accessible in a non-invasive manner) portions 93B, 93C of the large intestine, with respect to prior art stool samples 70. Advantageously, disclosed methods and systems provide non-invasive sampling of the ascending and transverse colon.

FIG. 7 illustrates the beta diversity (between samples) using principal coordinates analysis (PCoA) and Bray-Curtis dissimilarity between samples (effluent) 139A, 139B, 139C and prior art stool samples 70 using WGS data. FIG. 7 clearly illustrates the dissimilarity of samples 139A, 139B, 139C from stool samples 70, which is particularly accentuated with respect to samples 139B, 139C from remoter (more proximal) large intestine sections 93B, 93C. FIG. 7 therefore further illustrates the significant difference of microbiota samples from more proximal (and less accessible in a non-invasive manner) portions 93B, 93C of the large intestine, with respect to prior art stool samples 70.

FIG. 8 illustrates the phylogenetic species beta diversity between samples, represented by UniFrac PCoA analysis (unweighted, and weighted by the relative abundances)—comparing samples (effluent) 139A (n=13), 139B (n=11), 139C (n=11) versus stool samples 70 (n=11) (data corresponding to FIG. 6A). In both types of analysis samples 139A, 139B, 139C were found to be clearly distinct from prior art stool samples 70.

FIG. 9 provides a differential abundance analysis derived from whole metagenome shotgun (WGS) sequencing, comparing respective samples (effluent) 139A, 139B, 139C to stool samples 70 (n=20). FIG. 9 is a volcano plot that clearly illustrates the genotypic differences between samples 139A, 139B, 139C and stool samples 70, which increase as samples are taken from remoter (more proximal) parts of the large intestine, reaching the highest values for samples 139C from ascending colon 93C.

FIG. 10 provides a Venn diagram of the presence and absence of species in samples (colon effluent) 139A, 139B, 139C and in stool samples 70—indicating the common and unique numbers and proportions of species among the samples—samples 139A (n=13), 139B (n=11), 139C (n=11) and stool samples 70 (n=11). Overall, out of 1099 species, 579 species were found in both samples 139 (any of samples 139A, 139B, 139C) and stool 70, 179 species were unique to stool samples 70 and 344 species were unique to effluent samples 139. The more detailed analysis is presented, e.g., in FIGS. 9 and 10, showing that samples 139C from ascending colon 93C are especially distinct from stool samples 70, having about double the number of unique species with respect to samples 139A, 139B from descending and transverse colon sections 93A, 93B, respectively.

FIGS. 11A and 11B illustrates the divergent taxonomical distribution of microbiota species in more proximal (and less accessible in a non-invasive manner) portions 93B, 93C of the large intestine, with respect to prior art stool samples 70, according to some embodiments of the invention.

As illustrated in FIG. 11A, the taxonomic distribution of the species was found to differ with respect to the sampled portion of the large intestine, specifically, the species abundance of firmicutes decreases and the species abundance of proteobacteria increases from stool samples 70 to samples 139, without a significant change in number of bacteroidetes species and with species of other phyla being more abundant in the inner-colonic samples 139B, 139C—indicating the distinct characteristics of microbiota from different portions of the large intestine. Overall, disclosed samples 139A, 139B, 139C differ in many ways from prior art stool samples 70, indicating the advantages of disclosed methods 200 and system 100 in providing accurate diagnosis and possibly treatment of the large intestine and its microbiota.

FIG. 11B provides results of an analysis of the biosynthetic gene clusters (BGCs, were identified by the VBx1 analysis pipeline from VastBiome™) derived from whole genome sequencing (WGS) of stool samples 70 and colon effluent samples 139A, 139B, 139C, unique BGCs were found in samples 139A, 139B, 139C overall and specifically within the different colon effluent samples 139A, 139B, 139C—indicating the unique functional biodiversity of sections 93A, 93B, 93C of the large intestine, as reflected by samples 139A, 139B, 139C. Specifically, of 74 BGCs found in stool samples 70 (n=20) and 174 BGCs found in samples 139 (n=62), only 15 BGCs were common, while 159 BGCs were unique to samples 139 and not found in stool samples 70. With respect to samples 139A (n=24), 139B (n=22), 139C (n=22)—58 BGCs, 49 BGCs and 26 BGCs were unique to the respective sample—further indicating the high diagnostic and possibly treatment value of sampling specific portions of the large intestine, and specifically remoter (more proximal) portions thereof such as transverse colon 93B and ascending colon 93C.

It is further noted that ascending colon effluent 139C was clearly distinguishable from descending colon effluent 139A in its appearance, e.g., in its consistency and color being more mucus-like and yellow, or of lighter color. The gradient in consistency and color of effluent as sampling moves to more distal parts of the large intestine further emphasize the differences in the microbiota and/or secreted compounds, indicating possible differential diagnostic capabilities and treatment options associated therewith.

Summarizing the experimental results, bacterial communities detected in inner-colonic samples were significantly different that those of stool samples. Of all bacterial strains detected, a third of the strains (n=344) were unique to the inner-colonic samples, with a unique contribution from the different colon biogeographic locations. A decrease in the species abundance of firmicutes and an increase in proteobacteria was detected when comparing stool to inner-colonic samples, without a significant change in number of bacteroidetes species. Species of other phyla were more abundant in the inner-colonic samples. There was a clear biogeography gradient of bacteria along the colon, where the overall microbial alpha diversity in each sample decreased towards the proximal colon. The phylogeny of the microbiota community in all stool samples was relatively similar regardless of the patient. Moreover, there were distinctive and large differences between stool and inner-colonic samples. For most patients there was a detectable phylogenetic progression with a predictable, yet personal, trajectory. The phylogenetic spread in the multivariance space of the weighted PCoA analysis explained approximately 50% of the population diversity of the inner-colonic samples diversity (n=35) and was much wider than the phylogenetic difference of the stool samples. It is noted that the disclosed process of collection of microbial samples using a high-volume colon irrigation is currently the only way of obtaining microbiome information from within the colon, non-invasively, and without the effects of oral prep purgatives. Obtaining information from inner-colonic microbiota communities may be imperative for developing personalized medicine.

Returning to FIG. 12, method 200 may further comprise deriving a diagnosis of the large intestine according to the derived microbiome characteristics from at least one of the at least three sections and possibly adjusting the diagnosis with respect to the derived microbiome characteristics of the at least a part of an ascending portion of the large intestine (stage 430). Method 200 may further comprise applying a treatment to the large intestine according to the derived microbiome characteristics from at least one of the at least three sections, and possibly adjusting the treatment with respect to the derived microbiome characteristics of the at least part of the ascending portion of the large intestine (stage 440). For example, the treatment may comprise transplanting a microbiota transplant (MT) into the patient's large intestine, the MT selected according to the derived microbiome characteristics of the at least three sections of the large intestine and/or possibly according to the derived microbiome characteristics of the at least part of the ascending portion of the large intestine (stage 450). The MT may be derived at least partly from prior drainage of the at least three sections of the large intestine and/or partly from prior drainage of the at least part of the ascending portion of the large intestine (stage 460).

FIGS. 13A, 13B, 14A, 14B and 15A-15C are high-level schematic illustrations of non-invasive sampling systems 190 of inner-colonic microbiome and its derivatives (e.g., effluent, mucosa and related compounds such as produced by the microbiome), according to some embodiments of the invention. FIG. 13A is a high-level schematic illustration of sampling system 190 with enlarged views of a collection unit 192 thereof, FIG. 13B a high-level control schematic illustrating the operation of sampling system 190, FIGS. 14A and 14B illustrate schematically configurations of sampling system 190 with respect to cleansing system 100 and FIGS. 15A-15C schematically illustrate stages in the operation of sampling system, according to some embodiments of the invention. Sampling system 190 may be operable in fluid communication with large intestine cleansing system 100, e.g., to sample large intestine contents 139 drained by system 100. Sampling system 190 comprises an electromechanical sampling device 191 configured to collect at least a part of large intestine contents 139 drained by cleansing system 100. Disclosed sampling systems 190 may be configured to provide scalable access to unique and personalized gut microbiota, in association with other procedures (e.g., large intestine cleansing prior to colonoscopy) or independently therefrom, e.g., as a dedicated procedure.

Sampling device 191 comprises collection unit 192 configured to collect at least one sample from contents 139, and a robotic unit 195 configured to move collection unit 192 to and from a sampling position 192A to collect the sample. Optionally, robotic unit 195 may be further configured to manipulate collection unit 192 to deposit the at least one sample into at least one corresponding collection utensil and/or into a casing to minimize or prevent contamination. Robotic unit 195 may comprise a clasping arm 195B configured to clasp and release collection unit 192 (e.g., actuating a clamp 195C) and a telescopic arm 195A configured to lower and raise clasping arm 195B, as illustrated schematically in FIGS. 15A-15C.

For example, collection unit 192 may comprise one or more perforated container (e.g., a disposable cup) having a perforated or meshed bottom 194 and possibly a funnel-shaped opening 194A configured to fit into (or onto a part of) a pipe section of drainage 151 (e.g., drain outlet 137, see FIGS. 15A-15C) and/or into or onto a drainage opening of basin 154 of cleansing system 100. Funnel-shaped opening 194A may be configured to provide the fitting, e.g., in a fluid-tight manner. One or more filters (not shown) with any of a range of pore sizes may be used to control the particle sizes of the collected samples, possibly in relation to the location along the large intestine from which the respective sample is taken. For example, finer meshes may be used to collect samples from finer forms of effluent (e.g., from ascending colon) which larger ore sizes of the mesh and/or filter may be used to sample coarser contents.

In certain embodiments, sampling device 191 may be set within a module 193 that may fit into drainage basin 154 (as part of overall drainage 151 of cleansing system 100, see, e.g., schematic illustrations in FIGS. 1A-1E as the covered region beneath the patient's legs, and in FIG. 14A). Sampling system 190 may hence be integrated within cleansing system 100. Alternatively or complementarily, sampling device 191 and/or module 193 may be set with fluid communication to the drained contents along drainage 151, e.g., within a container configured to enable sampling the drained contents, e.g., from drainage pipe(s) 138. In certain embodiments, sampling system 190 may be configured to sample drained contents after it exits cleansing system 100 (see, e.g., FIG. 14B) and before the drained contents is disposed of.

Sampling device 191 may be configured to be operated by one or more sensors 161 (e.g., one or more camera 161) of cleansing system 100. Alternatively or complementarily, sampling system 190 may comprise one or more sensors or cameras 196 (shown schematically in FIG. 14B), configured to monitor one or more locations along drainage 151 to time the activation of electromechanical sampling device 191 and/or to monitor the interior of module 193, e.g., to guide the operation of robotic unit 195.

As illustrated schematically in FIG. 13B, sampling system 190 may comprise a control unit 140A, which may be part of control unit 140 or in communication therewith, and may be implemented by computing device 143. Control unit 140A may be configured to operate robotic unit 195 with telescopic arm 195A, clasping arm 195B and clamp 195C, e.g., as illustrated schematically in FIGS. 15A-15C. Control unit 140A may be powered by cleansing system 100 or possibly powered independently by power source based on a rechargeable battery (illustrated schematically), or optionally on external power supply. Control unit 140A may be activated by cleansing system 100 or possibly activated independently by a switch operated manually or electronically (illustrated schematically).

Automatic operation of sampling system 190 may be implemented by a near-real-time algorithm operated by control unit 140 with respect to input from sensor(s) 161. For example, referring to FIGS. 1D and 1E as a non-limiting example, drained contents 139 may flow via a transparent drainage pipe 138 as part of drainage 151 and the analyzing may be carried out optically through transparent drainage pipe 138, e.g., through window 152.

Analysis module 160 may employ optical analysis methods using camera(s) 161 and image/video/spectral processing software, possibly as part of optical inspection unit 150—to derive a timing for sampling contents 139 by sampling system 190. Camera(s) 161 of cleansing system 100, or possibly dedicated camera(s) of sampling system 190 may be configured as a video monitoring system (see, e.g., schematic sensor(s) 196 in FIG. 14B) to monitor colon effluent drainage and indicate times for operating sampling system 190 according to specified criteria (e.g., time lapsed or amount of contents expelled since start of the cleansing procedure, optical characteristics or consistency of the effluent, e.g., segment blobs, color, count, size, and texture features, etc.). The video monitoring system may be configured to analyze and tag the captured images and apply neural networks to detect instances of required sampling to operate sampling system 190 at. For example, the video monitoring system and/or control unit 140 (e.g., being in communication with the monitoring system) may be configured to create a colon irrigation effluent phase classification system that may be configured to classify (e.g., algorithmically, in a non-limiting example, using a classifier or any other algorithm) the captured frames into colon segments (descending/transverse/ascending) and relate the sampling thereto. It is noted that for data storage, specific images from the video stream and/or specific characteristics of the video streams (e.g., analyzed image parameters) may be stored, rather than the full video sequences. Video monitoring may be optional, while monitoring may be carried out using non-continuous imaging methods.

Optical inspection of the contents may comprise deriving parameters such as color or other spectral analysis parameters, used to characterize the drained content with respect to characteristics such as appearance of blood in the drained content, the color of the effluent, etc. Sampling may be carried out with respect to such spectral characteristics, e.g., sampling may be aimed at portions of the drained contents that include hues of red, or sampling of mucosa effluent may be carried out upon detection of yellowish color, or mucosa-like spectral parameters. Machine learning may also be applied to correlate the type of drained contents with the respective spectral signatures, to improve the accuracy of the sampling. It is noted that detection of blood (or corresponding spectral components) may also be used to generate a stop alert for stopping the cleansing and/or sampling procedure.

Inspection may further comprise analyzing volatile compounds from the drained contents, such as volatile amino acids (e.g., mycosporine-like amino acids, MAAs) which may be characterized by their ultraviolet (UV) signatures, e.g., in the UVA, UVB and/or UVC ranges (ultraviolet A, UVA, ranges between 320-400 nm, ultraviolet B, UVB, ranges between 280-320 nm and ultraviolet C, UVC, ranges between 200-280 nm). Disclosed sampling may be carried out according to detected volatile amino acids, e.g., above specific threshold(s), which may indicate certain medical conditions—yield functional sampling of the contents, in addition or instead of spatial sampling of the large intestine. In certain embodiments, the samples may be spectrally analyzed, e.g., for UV signatures to detect volatile amino acids for diagnostic purposes. Spectral analysis may be implemented to detect specific compounds in any of the infrared, visible or ultraviolet ranges, e.g., using the spectral signatures of the compounds.

FIGS. 14A and 14B are high-level schematic illustrations of configurations of sampling system 190 with respect to cleansing system 100, according to some embodiments of the invention. In certain embodiments, illustrated in as a non-limiting example in FIG. 14A, sampling system 190 may be integrated in cleansing system 100, e.g., be mounted above drainage pipe 138 (see, e.g., FIG. 1A) possibly under or over a splash protection part (splash guard between the patient's legs) of cleansing system 100—to directly sample drained contents 139. Alternatively or complementarily, in certain embodiments, sampling system 190 may be used to sample drained contents 139 that exit cleansing system 100 via drainage 151, as illustrated in as a non-limiting example in FIG. 14B. In either case, sampling cups 142 may be deposited and/or removed from sampling system 190 in a sterile manner, manually and/or automatically. In either case, activation of the sampling process by sampling system 190 may be carried out by sensor(s) 161 of cleansing system 100 and/or by sensor(s) 196 of sampling system 190 (shown in a highly schematic manner), configured to monitor the drained contents and possibly apply image and/or spectral analysis. In either case, sampling system 190 may be operated using an energy storage device such as a battery or by power from an external source such as the electric grid. Power supply to sampling system 190 and cleansing system 100 may be related (e.g., power from cleansing system 100 may be delivered to sampling system 190) or separate.

FIG. 15A schematically illustrates a position 192B of collection unit 192 in which it is loaded into sampling system 190, e.g., into a dedicated casing, or compartment 198 in module 193. In certain embodiments, sampling system 190 may be configured to receive collection unit 192 within casing 198, e.g., within a clean and/or sterile resealable casing 198. In other embodiments, a technician may insert collection unit 192 into compartment 198. Accordingly, in some embodiments, casing 198 may be inserted into module 193 together with collection unit 192, while in other embodiments collection unit 192 may be inserted into compartment 198 in module 193. Possibly, collection unit 192 with casing 198 may be inserted into a compartment (not shown, but similar to compartment 198) in module 193.

Robotic unit 195 may be configured to remove collection unit 192 from casing 198, optionally opening casing 198 prior to removing collection unit therefrom 192. Casing 198 may be used to keep collection unit clean or sterile while it is handled outside sampling unit 190 and until briefly before it is used to collect the sample.

Clasping arm 195B is configured to clasp collection unit 192, possibly free it from a package thereof (e.g., a plastic cover, possibly at least partly sterile, such as casing 198) and move collection unit 192 by telescopic arm 195A, as illustrated schematically in FIG. 15B, to a drain outlet 137 along drainage 151 (illustrated schematically, e.g., drainage basin 154 and/or drainage pipe 138). Once positioned in drain outlet 137, as illustrated schematically in FIG. 15C, collection unit 192 may sieve contents 139 flowing through drainage 151 to collect a sample of contents 139 for a specified time or until a specified amount of sample is collected. Following the sampling, telescopic arm 195A may be configured to move collection unit 192 (as illustrated schematically in FIG. 15B) back to casing 198, compartment 198 and/or to collection utensil 198, which may be positioned in the same or in a different compartment 198—depending on the exact configuration of sampling system 190 as disclosed herein. Any of collection unit 192, casing 198 and/or compartment 198 may be configured to be sealable to prevent odor from the sample during its handling inside and outside sampling system 190.

For example, when casing 198 is resealable, robotic unit 195 may be configured, to seal casing 198 after returning collection unit 192 with the sample thereto, e.g., further using clasping arm 195B to seal casing 198. Following the returning of collection unit 192 with the sample, collection unit 192 (e.g., within casing 198, which may be resealed) may be stored at a designated sample preservation station.

In another example, in case of using separate collection utensil 198, robotic unit 195 may be configured to manipulate collection unit 192 to deposit the sample into collection utensil 198. Following the transfer of the sample, collection unit 192 may be disposed of and collection utensil 198 may be stored at a designated sample preservation station.

Sampling system 190 may be configured to smoothly lower, position and retrieve collection unit 192 for viewing and further handling of the samples collected thereby. In various embodiments, the sample may be preserved within collection unit 192 until it is stored, e.g., utilizing cooling means such as ice, dry ice or any other mechanism. In certain embodiments, a cooling unit (not shown) may be part of module 193, e.g., as part of or in association with compartment or casing 198.

FIG. 16 is a high-level schematic flowchart of a sampling method 500, according to some embodiments of the invention. Sampling method 500 may be part of method 200 disclosed herein and comprise introducing water controllably into a patient's large intestine (stage 210), draining the introduced water with contents of the patient's large intestine (stage 220), as well as optically monitoring the drained content (stage 232A), characterizing the optically monitored drained content to determine sampling times (stage 510), and sampling the drained contents according to the characterization (stage 520). Characterization 510 may be carried out with respect to at least one of: time lapsed or amount of contents expelled since start of the draining, optical characteristics or consistency of the drained content, and an estimated section of the large intestine. Sampling 520 may be carried out by moving a collection unit into a flow path of the drained content and removing sampled content from the collection unit (stage 525), as disclosed herein.

Method 500 and/or sampling 525 may further comprise receiving a collection unit for the sampling (stage 530), which may enclosed within a casing, optionally opening the casing prior to the removing of the collection unit therefrom (stage 535), removing the collection unit from the casing prior to the sampling (stage 537), returning the collection unit with the sample to the casing (stage 540), and optionally sealing the casing after returning the collection unit with the sample thereto (stage 545), when the casing is resealable—for example, as illustrated schematically in FIGS. 15A-15C.

Advantageously, sampling system 190 provides a clean and safe mechanism for collecting effluent samples from the large intestine. When integrated within cleansing system 100, sampling system 190 is configured to operate in a way that does not interrupt or interfere with the operation of cleansing system 100. Advantageously, using cleansing system 100 enables sampling large intestine microbiota in a comfortable procedure, without prior disturbance to the microbiota by oral purgatives, and moreover, enables differentiation of sampling from different parts of the large intestine. In a non-limiting example, sampling system 190 may be configured to collect one or more samples of different effluent portions 139A, 139B, 139C of drained contents 139, from descending colon 93A, transverse colon 93B and ascending colon 93C, respectively, as disclosed herein.

The aforementioned flowchart and diagrams illustrate the architecture, functionality, and operation of possible implementations of systems, methods and computer program products according to various embodiments of the present invention. In this regard, each portion in the flowchart or portion diagrams may represent a module, segment, or portion of code, which comprises one or more executable instructions for implementing the specified logical function(s). It should also be noted that, in some alternative implementations, the functions noted in the figure portion may occur out of the order noted in the figures. For example, two portions shown in succession may, in fact, be executed substantially concurrently, or the portions may sometimes be executed in the reverse order, depending upon the functionality involved. It will also be noted that each portion of the portion diagrams and/or flowchart illustration, and combinations of portions in the portion diagrams and/or flowchart illustration, can be implemented by special purpose hardware-based systems that perform the specified functions or acts, or combinations of special purpose hardware and computer instructions.

In the above description, an embodiment is an example or implementation of the invention. The various appearances of “one embodiment”, “an embodiment”, “certain embodiments” or “some embodiments” do not necessarily all refer to the same embodiments. Although various features of the invention may be described in the context of a single embodiment, the features may also be provided separately or in any suitable combination. Conversely, although the invention may be described herein in the context of separate embodiments for clarity, the invention may also be implemented in a single embodiment. Certain embodiments of the invention may include features from different embodiments disclosed above, and certain embodiments may incorporate elements from other embodiments disclosed above. The disclosure of elements of the invention in the context of a specific embodiment is not to be taken as limiting their use in the specific embodiment alone. Furthermore, it is to be understood that the invention can be carried out or practiced in various ways and that the invention can be implemented in certain embodiments other than the ones outlined in the description above.

The invention is not limited to those diagrams or to the corresponding descriptions. For example, flow need not move through each illustrated box or state, or in exactly the same order as illustrated and described. Meanings of technical and scientific terms used herein are to be commonly understood as by one of ordinary skill in the art to which the invention belongs, unless otherwise defined. While the invention has been described with respect to a limited number of embodiments, these should not be construed as limitations on the scope of the invention, but rather as exemplifications of some of the preferred embodiments. Other possible variations, modifications, and applications are also within the scope of the invention. Accordingly, the scope of the invention should not be limited by what has thus far been described, but by the appended claims and their legal equivalents.

	Number	Date	Country
	62208995	Aug 2015	US
	62289944	Feb 2016	US

	Number	Date	Country
Parent	15138594	Apr 2016	US
Child	15688877		US

	Number	Date	Country
Parent	15688877	Aug 2017	US
Child	16362660		US

	Number	Date	Country
Parent	17406136	Aug 2021	US
Child	17494958		US
Parent	16842294	Apr 2020	US
Child	17406136		US
Parent	16362660	Mar 2019	US
Child	16842294		US

NON-INVASIVE SAMPLING OF INNER-COLONIC MICROBIOME

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CROSS-REFERENCE TO RELATED APPLICATIONS

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