The present disclosure relates to systems and methods to integrate an out-patient site with a healthcare provider site using remote wireless communication with a health care provider (HCP).
Healthcare is undergoing a paradigm shift from reactive, in-hospital treatment to proactive, community-based care. Today's healthcare systems must deliver improved patient outcomes while reducing costs. Hospital overcapacity and the pressure to deliver patient care in the community is driving pent-up demand for care at home. Until recently, health care systems have lacked the technology to satisfy this demand. Various aspects of telemedicine are becoming more common. However, the Health Insurance Portability and Accountability Act (HIPPA), among other health care related laws and rules, place limits on patient-specific health information access, transmission, storage, etc.
As patient desire for out-patient care increases, the need for remote patient health monitoring apparatuses, systems, and methods increases. This increased need for remote patient health monitoring is further increased due to a desire for improved patient outcomes, particularly with regard to higher risk patients (e.g., complete out-patient treatment of patients having residual amounts of leukemia cells in their system, a likelihood of experiencing treatment-emergent adverse events (TEAE), such as, for example, cytokine release syndrome (CRS) and/or neurotoxicity (NT), a likelihood of experiencing other serious adverse events (SAEs) requiring hospitalization during the mandatory device monitoring period (MDMP), etc.).
Apparatuses, systems, and methods are needed for improving out-patient healthcare outcomes. Apparatuses, systems, and methods are also needed for improving out-patient healthcare having improved communication between a patient and associated healthcare provider(s).
A system for out-patient treatment may include an infusion pump for delivering a therapeutic to a patient. The system may also include a wearable device configured to be worn by the patient before, during, and/after delivery of the therapeutic. The wearable device may include one or more sensors configured to acquire sensor data related to detection of patient vital signs. The system may further include a wireless communication module disposed on the wearable device and configured for remote wireless communication with a healthcare provider based on the acquired sensor data.
In another embodiment, a computer-readable medium may include computer-readable instructions stored thereon that, when executed by a processor, may cause the processor to monitor health of a patient. The computer-readable medium may include a sensor data receiving module that, when executed by a processor, may cause the processor to receive sensor data. The computer-readable medium may also include a warning data generation module that, when executed by a processor, may cause the processor to generate at least one warning based on the sensor data. A content of the sensor data may be based on an out-patient treatment that includes an immunotherapy that activates T cells of the patient.
In a further embodiment, a computer-implemented method for out-patient treatment with immunotherapy that activates T cells of a patient to kill cancer cells may include receiving, at a processor, sensor data in response to the processor executing a sensor data receiving module. The method may also include generating, using a processor, warning data, based on the sensor data, in response to the processor executing a warning data generation module. A content of the sensor data may be based on a likelihood that the immunotherapy will trigger increased risk factors of cytokine release syndrome.
It is believed that the disclosure will be more fully understood from the following description taken in conjunction with the accompanying drawings. Some of the drawings may have been simplified by the omission of selected elements for the purpose of more clearly showing other elements. Such omissions of elements in some drawings are not necessarily indicated of the presence or absence of particular elements in any of the exemplary embodiments, except as may be explicitly delineated in the corresponding written description. Also, none of the drawings are necessarily to scale.
Skilled artisans will appreciate that elements in the figures are illustrated for simplicity and clarity and have not necessarily been drawn to scale. For example, the dimensions and/or relative positioning of some of the elements in the figures may be exaggerated relative to other elements to help to improve understanding of various embodiments of the present invention. Also, common but well-understood elements that are useful or necessary in a commercial feasible embodiment are often not depicted in order to facilitate a less obstructed view of these various embodiments. It will further be appreciated that certain actions and/or steps may be described or depicted in a particular order of occurrence while those skilled in the art will understand that such specificity with respect to sequence is not actually required. It will further be appreciated that certain actions and/or steps may be described or depicted in a particular order of occurrence while those skilled in the art will understand that such specificity with respect to sequence is not actually required. It will also be understood that the terms and expressions used herein have the ordinary technical meaning as is accorded to such terms and expressions by persons skilled in the technical field as set forth above except where different specific meanings have otherwise been set forth herein.
Reliable, continuous patient monitoring, as described herein, may enable early intervention in the event of patient deterioration, a better experience for patients, fewer unnecessary hospital re-admissions, customers have been able to shorten hospital stays, reduce hospital readmission rates, and deliver better patient outcomes. Apparatuses, systems, and methods are provided for improving out-patient healthcare outcomes. Apparatuses, systems, and methods are also provided for improving out-patient healthcare having improved communication between a patient and associated healthcare provider(s). In a specific embodiment (described herein as an “EXAMPLE STUDY”), a system is provided for out-patient treatment with immunotherapy that activates T cells of a patient to fight cancer. The system may include an infusion pump (e.g., blinatumomab infusion, Blincyto® as described in international patent application WO2020/221792, the entire content of the disclosure of which is incorporated herein by reference). In another embodiment, a system may be provided for out-patient treatment with acapatamab (AMG 160) as described in international patent application WO 2017/134158, the entire content of the disclosure of which is incorporated herein by reference, a product that contains a half-life extended (HLE) anti-prostate-specific membrane antigen (PSMA)×anti-CD3 BiTE® (bispecific T cell engager), etc.). As described in more detail herein,
In any event, a patient wearable device configured to acquire sensor data (e.g., patient vital signs data, respiratory rate data, heart rate data, oxygen data, blood pressure data, temperature data, patient motion data, patient orientation data, etc.) related to detection of symptoms that may result from the administered medication (e.g., cytokines released by the patient in response to the patient receiving immunotherapy that activates T cells, etc.). The system may also include remote wireless communication between the patient and a healthcare provider based on the acquired sensor data.
As described in detail herein, apparatuses, systems, and methods are provided that may acquire sensor data based on a type of therapy being administered (e.g., based on a type of medication; for AMG 160, a wearable device may monitor patient vital signs for 3 days after a 60 min infusion, etc.) to a respective patient. As also described in detail herein, apparatuses, systems, and methods are provided that generate warning data based on the acquired sensor data. As further described in detail herein, apparatuses, systems, and methods are provided that facilitate audio/video communication between a patient and a respective healthcare provider, along with transmission of sensor data and warning data to a healthcare provider.
Turning to
With further reference to
The out-patient treatment system 100 may also include a patient wearable device 115 (e.g., a wearable device as available from Current Health device (https://currenthealth.com/), a wearable device as available from Bio Beat device (https://www.bio-beat.com/), or any suitable/required remote and/or wearable monitor, etc.). The patient wearable device 115 may include a lithium ion battery with, for example, a battery life of 36 hours. The battery may be charged using, for example, wireless Qi induction charging, with a charge time of 3 hours. While not shown in
A patient wearable device assembly may be provided to a patient 105 that includes, for example, at least three components: 1) reusable cradle, 2) a fabric single-use strap (in 5 sizes), and 3) a reusable sensor. The sensor may be inserted into the cradle, and may power on through detection of magnets in the cradle. The strap may be inserted into the cradle on both sides. The patient wearable device 115 may be, for example, slid up an arm of the patient like a tourniquet, and then tightened such that the patient wearable device 115 closely moves with the skin. The reusable sensor may include a battery having a battery life of, for example, 36 hours, and the patient 105, may be instructed to swap the sensor every 24 hours, 1 on the charger, and 1 on their arm. The reusable sensor may be charged wirelessly by placing the reusable sensor on top of the charging plate.
The out-patient treatment system 100 may also include a blood pressure monitor 140 (e.g., an Evolv blood pressure monitor as available from Omron, etc.). The blood pressure monitor 140 may be, for example, an upper-arm worn wireless device that uses an optical sensor, thermistor, accelerometer and gyroscope to measure a subject's heart rate (HR), respiratory rate (RR), axillary temperature, and oxygen saturation. Associated “vital signs” may be measured, for example, every 2 seconds and transmitted every 30 seconds over WiFi. The BP monitor 140 may be, for example, a brachial or radial artery oscillometric BP monitor. It is self-applied by the subject like a tourniquet and, after pressing the start button, will transmit the subject's systolic and diastolic BP over Bluetooth to the subject “tablet app” (e.g., module 253a of
The out-patient treatment system 100 may also include an auxiliary temperature sensor 141 (e.g., a Fever Scout auxiliary temperature sensor as available from VivaLNK, etc.). The axillary temperature sensor 141 may be attached to the patient 105 via, for example, an adhesive to the axilla of the patient. An auxiliary temperature sensor 141 may be attached to the patient's axilla for, for example, a duration of an associated mandatory monitoring period. The axillary temperature sensor 141 may, for example, measure axillary temperature of the patient 105 continuously, and may broadcasts the data, via Bluetooth, to the patient wearable device 115. The axillary temperature sensor 141 may be, for example, a single subject use, and may include a battery having a battery life that is longer than the mandatory device monitoring period. As described herein, an auxiliary temperature sensor 141 may be attached to the patient's axilla for, for example, a duration of an associated mandatory monitoring period (e.g., days, weeks, months, etc.).
While the patient wearable device 115, the blood pressure monitor 140, and the auxiliary temperature sensor 141 are shown in
The out-patient treatment system 100 may also include a patient device 150 (e.g., a tablet computer w/ePro software, a smart phone, etc.) and a network device 195 (e.g., a home hub, etc.). The network device 195 may, for example, provide WiFi signal within a subject home and transmits data out over the cellular network to CH's software platform. The network device 195 may be, for example, plugged into a standard home power outlet. The network device 195 may not require any patient configuration. Similarly, the network device 195 may not include any buttons (e.g., patient inputs, etc.). The patient 105 may plug the network device 195 into a standard home 110V power outlet. While not shown in
As described in detail herein, a user interface displayed on, for example, a display (e.g., display 254a of
The out-patient treatment system 100 may also include a “Software Platform” (e.g., a combination of modules 253a and 268a of
The module 253a may be configured as a “Subject Tablet App” pre-installed on, for example, the patient device 150. The patient device 150 may be provided to a patient 105 in, for example, a “kiosk mode” (i.e., a mode where module 253a is the only “application” that can be accessed by the patient 105). As described in detail herein, execution of the module 253a by processor 251a may, for example, cause the processor 251a to capture electronic patient-reported outcomes (ePRO) data, capture BP data from the integrated BP monitor 140 and initiate a video call between the patient 105 and the healthcare provider 106.
The software platform 253a, 268a may, for example, further include a “healthcare provider (HCP) App” (e.g., module 283a of
As described in detail herein, the out-patient treatment system 100 may include two independent communication links between the patient site 101 and the healthcare provider site 102. A first communication link 103 (e.g., similar to a combination of communication links 290a, 292a, and 293a of
Clinical dashboards (e.g., as illustrated in displays 500a-h,j-l of
An associated “kit” assembly, may be contained within, for example, a soft case that is easily transportable to the patient's home. A kit assembly may include: at least one infusion pump 110, at least one sensor device 140, 141, at least one patient wearable device 115, at least one patient device 150, and at least one network device 195. While not shown in
With reference to
While not shown in
As described in detail herein, the server 260a may, for example, host at least a portion of the “Software Platform” (e.g., module 268a, etc.) including interfaces to the “Subject Tablet App” 253a and the “healthcare provider (HCP) App” 283a. Thereby, the server 260a may, for example: acquire sensor data: acquire patient-initiate call input data; generate alarm data based on the sensor data and/or the patient-initiate call input data; receive audio/video data; transmit audio/video data; generate user interface displays based on the sensor data, the patient-initiate call input data, the warning data, and the audio/video data. Additionally, the server 260a may, for example, store the sensor data, the patient-initiate call input data, the warning data, and/or the audio/video data in a patient health related database 269a.
For clarity, only two sensor devices 240a, 241a, one patient wearable device 215a, one patient device 250a, one server 265a, one healthcare provider device 280a, and one network device 290a are depicted in
A patient wearable device 215a may include a memory 217a and a processor 216a for storing and executing, respectively, a module 218a. The module 218a, stored in the memory 217a as a set of computer-readable instructions, may be related to an application for implementing at least a portion of the out-patient treatment system 200a. As described in detail herein, the processor 216a may execute the module 218a to, among other things, cause the processor 216a to receive, generate, and/or transmit data (e.g., sensor data, patient-initiated call data, warning data, audio/video data, etc.) with the sensor device 241a, the network device 290a, the patient device 250a, the server 265a, and/or the healthcare provider device 280a.
The patient wearable device 215a may also include a user interface 219a which may be any type of electronic display device, such as touch screen display, a liquid crystal display (LCD), a light emitting diode (LED) display, a plasma display, a cathode ray tube (CRT) display, or any other type of known or suitable electronic display along with a user input device. A user interface 219a may exhibit a user interface display (e.g., any user interface 500a-h,j-l of
The patient wearable device 215a may also include a patient-initiated call button 210a, a warning device 221a, a network interface 222a, and a Bluetooth interface 223a. The network interface 222a may be configured to facilitate communications, for example, between the patient wearable device 215a and the network device 290a via any wireless communication network 291a, including for example: a wireless LAN, MAN or WAN, WiFi, TLS v1.2 WiFi, the Internet, or any combination thereof. Moreover, a patient wearable device 215a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
The Bluetooth interface 223a may be configured to facilitate communications, for example, between the patient wearable device 215a and the sensor device 241a via any wireless communication network 224a, including for example: a Bluetooth link, a wireless LAN, MAN or WAN, WiFi, TLS v1.2 WiFi, the Internet, or any combination thereof. Additionally, or alternatively, a patient wearable device 215a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
The sensor device 241a may be similar to, for example, the sensor device 141 of
The sensor device 241a may also include a Bluetooth interface 248a. The Bluetooth interface 248a may be configured to facilitate communications, for example, between the sensor device 241a and the patient wearable device 215a via any wireless communication network 224a, including for example: a Bluetooth link, a wireless LAN, MAN or WAN, WiFi, TLS v1.2 WiFi, the Internet, or any combination thereof. Additionally, or alternatively, a sensor device 241a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
A patient device 250a may include a memory 252a and a processor 251a for storing and executing, respectively, a module 253a. The module 253a, stored in the memory 252a as a set of computer-readable instructions, may be related to an application for implementing at least a portion of the out-patient treatment system 200a (e.g., a “Subject Tablet App”, etc.). As described in detail herein, the processor 251a may execute the module 253a to, among other things, cause the processor 251a to receive, generate, and/or transmit data (e.g., sensor data, patient-initiated call data, warning data, audio/video data, etc.) with the sensor device 240a, the network device 290a, the patient wearable device 215a, the server 265a, and/or the healthcare provider device 280a.
The patient device 250a may also include a user interface 254a which may be any type of electronic display device, such as touch screen display, a liquid crystal display (LCD), a light emitting diode (LED) display, a plasma display, a cathode ray tube (CRT) display, or any other type of known or suitable electronic display along with a user input device. A user interface 254a may exhibit a user interface display (e.g., any user interface 500a-h,j-l of
The patient device 250a may also include a microphone 255a, a speaker 256a, a camera 260a, a network interface 257a, a Bluetooth interface 258a, and a cellular interface 289a. The network interface 257a may be configured to facilitate communications (e.g., sensor data, warning data, patient-initiated call data, etc.), for example, between the patient device 250a and the network device 290a via any wireless communication network 292a, including for example: TLS v1.2 WiFi, a wireless LAN, MAN or WAN, WiFi, the Internet, or any combination thereof. Moreover, a patient device 250a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
While the patient device 250a is illustrated in
The Bluetooth interface 258a may be configured to facilitate communications, for example, between the patient device 250a and the sensor device 240a via any wireless communication network 259a, including for example: a Bluetooth link, a wireless LAN, MAN or WAN, WiFi, TLS v1.2 WiFi, the Internet, or any combination thereof. Additionally, or alternatively, a patient wearable device 215a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
The cellular interface 261a may be configured to facilitate communications (e.g., audio data, video data, etc.), for example, between the patient device 250a and the healthcare provide device 280a via any wireless communication network 296a, including for example: TLS v1.2 Cellular, a wireless LAN, MAN or WAN, WiFi, TLS v1.2 WiFi, the Internet, or any combination thereof. Moreover, a patient device 250a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
The sensor device 240a may be similar to, for example, the sensor device 140 of
The sensor device 240a may also include a Bluetooth interface 244a. The Bluetooth interface 244a may be configured to facilitate communications, for example, between the sensor device 240a and the patient device 250a via any wireless communication network 259a, including for example: a Bluetooth link, a wireless LAN, MAN or WAN, WiFi, TLS v1.2 WiFi, the Internet, or any combination thereof. Additionally, or alternatively, a sensor device 240a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
A server 260a may include a memory 267a and a processor 266a for storing and executing, respectively, a module 268a. The module 268a, stored in the memory 267a as a set of computer-readable instructions, may be related to an application for implementing at least a portion of the out-patient treatment system 200a (e.g., a “Software Platform”, etc.). As described in detail herein, the processor 266a may execute the module 268a to, among other things, cause the processor 266a to receive, generate, and/or transmit data (e.g., sensor data, patient-initiated call data, warning data, audio/video data, etc.) with the network device 290a, the patient device 250a, the patient wearable device 215a, and/or the healthcare provider device 280a.
The server 260a may also include a user interface (not shown in
The server 260a may also include a patient health related database 269a and a network interface 270a. The patient health related database 269a may, for example, store sensor data, patient-initiated call data, warning data, audio/video data, etc. The network interface 270a may be configured to facilitate communications, for example, between the server 260a and the network device 290a via any wireless communication network 294a, including for example: TLS v1.2 Cellular, CSV/JSON Output, TLS v1.2 REST API, a wireless LAN, MAN or WAN, WiFi, TLS v1.2 WiFi, the Internet, or any combination thereof. Moreover, a server 260a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
A healthcare provider device 280a may include a memory 282a and a processor 281a for storing and executing, respectively, a module 283a. The module 283a, stored in the memory 282a as a set of computer-readable instructions, may be related to an application for implementing at least a portion of the out-patient treatment system 200a (e.g., a “healthcare provider (HCP) App”, etc.). As described in detail herein, the processor 281a may execute the module 283a to, among other things, cause the processor 281a to receive, generate, and/or transmit data (e.g., sensor data, patient-initiated call data, warning data, audio/video data, etc.) with the network device 290a, the patient wearable device 215a, the patient device 250a, and/or the server 265a.
The healthcare provider device 280a may also include a user interface 284a which may be any type of electronic display device, such as touch screen display, a liquid crystal display (LCD), a light emitting diode (LED) display, a plasma display, a cathode ray tube (CRT) display, or any other type of known or suitable electronic display along with a user input device. A user interface 284a may exhibit a user interface display (e.g., any user interface 500a-h,j-l of
While the healthcare provider device 280a is illustrated in
The healthcare provider device 280a may also include a microphone 285a, a speaker 286a, a camera 288a, a network interface 287a, and a cellular interface 289a. The network interface 287a may be configured to facilitate communications (e.g., sensor data, warning data, patient-initiated call data, etc.), for example, between the healthcare provider device 280a and the network device 290a via any wireless communication network 293a, including for example: TLS v1.2 REST API, TLS v1.2 Cellular, CSV/JSON Output, TLS v1.2 REST API, a wireless LAN, MAN or WAN, WiFi, TLS v1.2 WiFi, the Internet, or any combination thereof. Moreover, a healthcare provider device 280a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
The cellular interface 289a may be configured to facilitate communications (e.g., audio data, video data, etc.), for example, between the healthcare provide device 280a and the patient device via any wireless communication network 296a, including for example: TLS v1.2 Cellular, a wireless LAN, MAN or WAN, WiFi, TLS v1.2 WiFi, the Internet, or any combination thereof. Moreover, a healthcare provider device 280a may be communicatively connected to any other device via any suitable communication system, such as via any publicly available or privately owned communication network, including those that use wireless communication structures, such as wireless communication networks, including for example, wireless LANs and WANs, satellite and cellular telephone communication systems, etc.
Each of the sensor devices 240a, 241a, the patient wearable device 215a, the patient device 250a, the healthcare provider device 280a, and/or the network device 295a may be, for example, configured such that any given device will store data (e.g., sensor data, patient-initiated call data, warning data, audio data, video data, etc.) within a respective memory 246a, 242a, 217a, 252a, etc. when the given device is unable to communicate data to another device as when fully functional within the out-patient treatment system 200a.
Turning to
With reference to
The processor 245a may execute the sensor data acquisition module 244b to cause the processor 245b to, for example, receive sensor data (block 244c). The processor 245a may execute the sensor data transmission module 245b to cause the processor 245b to, for example, transmit sensor data (block 245c). The processor 245a may execute the patient-initiation call button input receiving module 246b to cause the processor 245b to, for example, receive a patient-initiation call button input (block 246c). The processor 245a may execute the patient call initiation button input transmission module 247b to cause the processor 245b to, for example, transmit a patient call initiation button input (block 247c). The processor 245a may execute the warning data generation module 248b to cause the processor 245b to, for example, generate warning data (block 248c). The warning data may be based on, for example, the sensor data and/or the warning data.
Turning to
With reference to
The processor 216a may execute the sensor data acquisition module 219d to cause the processor 216a to, for example, acquire sensor data from the sensor device 241a (block 219e). The processor 216a may execute the sensor data transmission module 220d to cause the processor 216a to, for example, transmit sensor data (block 220e). The processor 216a may execute the patient-initiation call button input receiving module 221d to cause the processor 216a to, for example, receive a patient-initiation call button input (block 221e). The processor 216a may execute the patient call initiation button input transmission module 222d to cause the processor 216a to, for example, transmit a patient call initiation button input (block 222e). The processor 216a may execute the warning data generation module 223d to cause the processor 216a to, for example, generate warning data (block 223e). The warning data may be, for example, based on the sensor data and/or the patient call initiation button input. The processor 216a may execute the warning data transmission module 224d to cause the processor 216a to, for example, transmit warning data (block 224e).
Turning to
With reference to
The processor 251a may execute the sensor data acquisition module 254f to cause the processor 251a to, for example, acquire sensor data from sensor device 240a (block 254g). The processor 251a may execute the sensor data transmission module 255f to cause the processor 251a to, for example, transmit sensor data (block 255g). The processor 251a may execute the patient-initiation call button input receiving module 256f to cause the processor 251a to, for example, receive a patient-initiation call button input (block 256g). The processor 251a may execute the patient call initiation button input transmission module 257f to cause the processor 251a to, for example, transmit a patient-initiation call button input (block 257g).
The processor 251a may execute the warning data generation module 258f to cause the processor 251a to, for example, generate warning data (block 258g). The warning data may be, for example, based on the sensor data and the patient-initiation call button input. The processor 251a may execute the warning data transmission module 259f to cause the processor 251a to, for example, transmit warning data (block 259g). The processor 251a may execute the audio/video data receiving module 260f to cause the processor 251a to, for example, receive audio/video data from a healthcare provider device 180, 280a (block 260g). The processor 251a may execute the audio/video data transmission module 261f to cause the processor 251a to, for example, transmit audio/video data to a healthcare provider device 180, 280a (block 261g).
Turning to
With reference to
The processor 281a may execute the warning data receiving module 284h to cause the processor 281a to, for example, receive warning data (block 284j). The processor 281a may execute the patient-initiated call button input receiving module 285h to cause the processor 281a to, for example, receive a patient-initiated call button input (block 285j). The processor 281a may execute the audio/video data receiving module 286h to cause the processor 281a to, for example, receive audio/video data from a patient device 150, 250a (block 286j). The processor 281a may execute the audio/video data transmission module 287h to cause the processor 281a to, for example, transmit audio/video data to the patient device 150, 250a (block 287j). The processor 281a may execute the warning data generation module 288h to cause the processor 281a to, for example, generate warning data (block 288j). The warning data may be based on, for example, the sensor data and/or the patient-initiated call button input.
With reference to Turning to
With reference to
The processor 266a may execute the sensor data storage module 269k to cause the processor 266a to, for example, store sensor data in the in the patient health related database 269a (block 2691). The processor 266a may execute the sensor data transmission module 270k to cause the processor 266a to, for example, transmit sensor data (block 2701). The processor 266a may execute the warning data receiving module 271k to cause the processor 266a to, for example, receive warning data (block 2711). The processor 266a may execute the warning data storage module 272k to cause the processor 266a to, for example, store warning data in the patient health related database 269a (block 272l). The processor 266a may execute the warning data transmission module 273k to cause the processor 266a to, for example, transmit warning data (block 273l).
Turning to
With reference to
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With reference to
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A patient wearable device assembly 300a-c may be designed for in-clinic and remote patient monitoring applications. For example, a multi-function cardiac patch may generate live stream multiple parameters to a mobile device or the cloud. A patient wearable device assembly 300a-c may be reusable, rechargeable, and can record data even in the event of a network disruption.
The patient wearable device assembly 300a-c may be powerful cardiac patch has been used in multiple studies including AF detection, coronary artery disease, stress and depression, and more. A patient wearable device assembly 300a-c may include: up to 96 hour rechargeable; 24 hour cache; IP25 water resistant; BLE network; size—90×20×7.9 mm; weight: 7.5 grams; 128 Hz ECG sensor; heart hate sensor 40 to 300 bpm; respiratory 5 to 35 brpm; 3-Axis ACC 5 Hz; FDA/NMPA-ECG; heart rate; and CE-ECG, heart rate, and respiratory rate.
A patient wearable device assembly 300a-c may include a SpO2 sensor that may provide continuous updates of a patient's oxygen saturation levels without the need for the patient to manually initiate a reading. With a secure design that wraps around the thumb of a patient, the sensor may be to stay on the patient even in ambulatory situations. Advantages of any given patient wearable device assembly 300a-c may include: live stream or recording; reusable/rechargeable; IoT enabled; secure thumb strap; data including oxygen saturation, pulse, up to 16 hours rechargeable; 10 hour cache; IP 22; BLE network; weight: 47.5 grams; SpO2—70% to 100%; pulse: 30 to 250 bpm; and FDA/CE/NMPA.
With reference to
Turning to
Medications or factors related to hepatic injury/dysfunction and cholestasis or biliary obstruction may cause liver enzyme elevations above normal levels even in otherwise healthy individuals. An associated patient wearable device 115 and/or sensor device 140, 141 may generate a detailed serum chemistry, including, for example: liver enzymes such as alkaline phosphatase (AP), alanine aminotransferase (ALT), aspartate aminotransferase (AST), lactate dehydrogenase (LDH), and C-reactive protein (CRP), total bilirubin, gamma-glutamyl transferase (GGT), D-Dimer, a combination thereof, or any sub-combination thereof. Corresponding sensor data may, thereby, provide important information related to a respective patient's liver function in response to drug treatment, and may reveal drug induced hepatocellular, cholestatic or mixed liver injury. In any event, a content of the sensor data may be based on a respective medication and/or patient related bio-information. In general, an associated patient wearable device 115 and/or sensor device 140, 141 may be configured to sense body chemistry parameters that are pre-determined to be likely representative of a patient's reaction to a particular treatment and/or medication.
With reference to
With reference to
The example study included a first sub-study 600a having: a patient examination stage 601a, a patient screening stage 602a, a first medication administration stage 603a, a medication administration stage end 604a, a second medication administration stage 605a, and an end of first sub-study 606a. The example study included a second sub-study 600b having: a patient examination stage 601b, a patient screening stage 602b, a first medication administration stage 603b, a second medication administration stage 604b, a medication administration stage end 605b, a third medication administration stage 606b, and an end of second sub-study 607b. The example study included patient 105 monitoring 600c having a plurality of patient monitoring requirements 610c.
The phase 4 indication included adult subjects with MRD of B-precursor ALL. Rationale for this example study was to determine the safety and feasibility of complete outpatient blinatumomab administration for subjects with MRD of B-precursor ALL. Blinatumomab administration had been demonstrated to be efficacious in the respective population for converting subjects to MRD negative status (MRD<0.1%). However, the mechanism of action (MOA) of T cell activation and cytokine production can result in potentially severe toxicity, specifically cytokine release syndrome (CRS) and/or neurotoxicity (NT). The incidence of these potentially severe side effects had been shown to be low. In the BLAST study, 3% and 13% of subjects had severe CRS and NT respectively (e.g., Gökbuget et al, 2018).
The objective of this example study was to determine the safety and feasibility of complete outpatient blinatumomab administration for subjects with MRD of B-precursor ALL. The example study used mobile electronic devices (e.g., a tablet, a smartphone, a personal electronic device, etc.) to electronically communicate with an associated healthcare provider (HCP), and a Wi-Fi enabled platform for real-time constant transfer of data and communication between subject and HCP to detect clinically important changes. The data provided to the HCP may enable the HCP to identify subjects at risk of developing grade 3 or 4 CRS, NT, or other serious adverse events (SAEs) requiring hospitalization during the mandatory device monitoring period (MDMP). In circumstances where the subject experiences a SAE, the HCP can then direct such subjects to the appropriate medical facility for hospitalization if needed.
aTherapeutic intervention is any measurable action taken by the subject or performed on the subject as a result of the onset of the clinical parameters described. Such actions may include: Advice from HCP to immediately call EMS or dial 911, discontinuation of the blinatumomab infusion, subject taking an oral medication, subiect receiving a medication or intervention by any emergency or hospital medical services, intervention such as administering any medication (IV or PO or PR) or IV fluids or oxygen etc Time to therapeutic intervention (TTI) is the measured time between the delivery of the device alert or unscheduled contact with HCP by subject/CG to report a change to the time of initiation of the therapeutic intervention as defined.
The example study determined the safety and feasibility of complete outpatient blinatumomab administration. Blinatumomab is a novel bispecific T-cell engaging (BiTE®) single-chain bispecific binding molecule construct that links CD3+T lymphocytes with CD19+ B cells. This treatment may result in a significant degree of T cell-mediated immune activation in subjects, which has correlated with efficacy but also with notable toxicity. The result of the example study included a heightened T-cell activation and release of pro-inflammatory cytokines and the clinical manifestation of CRS. Along with CRS, another potentially severe toxicity observed is NT. It was anticipated that some subjects may show signs of encephalopathy with varying degrees of severity and may experience delirium, aphasia, lethargy, difficulty concentrating, agitation, tremor, seizures, and, rarely, cerebral edema.
Minimal residual disease (MRD) is defined as the presence of leukemic cells not detectable by microscopy (<5%) with a sensitivity of 0.1%, measured either by polymerase chain reaction (PCR) or flow cytometry. After achieving hematologic remission, the presence of MRD portends a poor prognosis for patients. In an associated Amgen trial (i.e., MT103-203 (BLAST)), 78% of subjects with MRD of B-precursor ALL achieved a complete MRD response to blinatumomab therapy. In this trial, 4 subjects (3%) had CRS (Common Terminology Criteria for Adverse Events [CTCAE] v4 grade 1, n=2; grade 3, n=2), all during cycle 1. Twelve (10%) and 3 subjects (3%) had grade 3 and 4 NT, respectively. Moreover, subjects with relapsed/refractory B-precursor ALL treated with blinatumomab in the Amgen trial 00103311 (TOWER) similarly had a low incidence of CRS and NT. In the 00103311 study the incidence of grade 3 CRS and NT were 4.9% and 9.4%, respectively with 1% and 4.9% of subjects having their treatment discontinued due to CRS and NT, respectively (i.e., Kantarjian et al, 2017).
At the time of the study, the current recommendation for blinatumomab treatment for subjects with MRD of B-precursor ALL was continuous intravenous infusion (CiVI) for 28 days, with the first 3 days in cycle 1 and the first 2 days in cycle 2 administered in the inpatient setting. This recommendation for hospitalization is primarily for safety concerns of CRS, NT, or other severe AEs.
Implementing the apparatuses, systems, and methods of the present disclosure, this example study determined the safety and feasibility of complete outpatient blinatumomab administration for subjects with MRD of B-precursor ALL. A patient (e.g., patient 105 of
Additionally, each patient 105 wore at least one sensor device (e.g., a patient wearable sensor device 140 of
Each patient was provided, a Wifi hub (e.g., network 250a of
Additionally, each patient was provided a patient device (e.g., a tablet device 150 of
Each healthcare provided was provided a mobile phone (e.g., smartphone 450g,j,k of
This example study included the following: 1) remote monitoring to measure vital signs (e.g., sensor data) and mobile electronic devices (e.g., a patient device 250a with module 253a) to electronically communicate the sensor data with the HCP (e.g., 280a of
During screening within the example study, subjects and caregivers were trained on the patient wearable device 115, and were assessed for compliance. Subjects receive 2 cycles of blinatumomab completely in the outpatient setting in accordance with the monitoring and intervention guidelines 510c of
After the end of cycle 2 clinical assessment visit, some subjects may continue to receive 2 additional (optional) cycles of blinatumomab. There is no health management system (HMS) 270a 270a outpatient monitoring during the optional cycles 3 and 4. For the purpose of this study, the MDMP is defined as the first 3 days of cycle 1 (72 hours) and the first 2 days of cycle 2 (48 hours) of blinatumomab infusion for subjects with MRD of B precursor ALL.
The end of study visit occurs 30 days (3 days) after the last dose of blinatumomab is given. The end of study visit occurs after cycle 3 or 4 for subjects who chose these optional cycles. During the MDMP, the health management system (HMS) 270a 270a measures vital signs. These vital signs include heart rate (HR), axillary temperature, and oxygen saturation. The health management system (HMS) 270a measures respiratory rate (RR) intermittently (sampling every 30 seconds). The subjects take intermittent blood pressure (BP) measurements (using a subject-usable BP device) every 3 hours during the MDMP. The schedule for BP measurements could have been extended by HCP (up to but not exceeding every 6 hours) after the first 24 hours of MDMP. The BP device 140 be provided and directly transmits the BP reading via the monitoring platform to the HCP device 270a.
Threshold vital sign values were established, and an immediate alert was generated, and transmitted to the HCP device 280a once the preset threshold values were surpassed and sustained for at least 10 minutes. In addition, subject and caregiver were trained on the usual side effects of blinatumomab infusion (fever, erythematous skin rash, chills, confusion, headache, tremor, myalgia, lethargy, somnolence, seizure), and have direct (phone and video) contact with HCP or emergency services if any expected or unexpected side effects occur. The caregiver is expected to be a spouse or close relative such as a child but included any adult (18 years) willing and able to participate in the subject's care. The caregiver remains in the home with the subject for the entire MDMP. The caregiver is trained to use and have access to the patient device (e.g., tablet 150 of
The HCP and the staff were trained on the infusion 110, usual side effects and response algorithm. The HCP (or designee) is a physician with experience in the treatment of patients with ALL and the use of blinatumomab. The HCP (or designee) carries the smart phone 480h device at all times during the MDMP. The smart phone 480h includes a cellular connection to the subject's tablet 150 and the health management system (HMS) 270a 170 and receives vital signs (i.e., sensor data) refreshed every 30 seconds for the entire MDMP. Blood pressure is performed manually by the subject (or caregiver) every 3 hours and the result electronically delivered to the HCP smart phone 480h. In addition to the continuous feed of vital signs, an audible alarm sounds every time the vital signs exceed the preset threshold and is consistent for at least 10 minutes. In addition, an audible alarm sounds if there is no data transfer for 15 minutes.
It is not intended that the health management system (HMS) 270a 170 allows the HCP to identify patients experiencing neurotoxicity. The health management system (HMS) 270a is intended to provide remote monitoring of vital signs. Knowing a subject's vital signs provide the HCP an overall picture of the subject's disposition. In addition to vital signs monitoring, the health management system (HMS) 270a includes the functionality for video calling between the physician and the subject. This allows the HCP to visually assess the patient for early symptoms of mild neurotoxicity such as kinetic tremor (assessed by finger-nose test), ataxia, appearance of disorientation to time or place, impaired attention or short-term memory with preserved alertness, impaired naming, paraphasic errors, or verbal perseveration. The HCP also tests the patient's ability to name objects, follow simple commands, and communicate their needs. The HCP evaluates expressive aphasia by evaluating the subjects' ability to communicate spontaneously (for example HCP may instruct subject to “look directly on the video screen and tell me how you are feeling today”) or in naming a common household object provided by caregiver. HCP evaluates apraxia by the subject's ability to write a standard sentence (for example “Today is Tuesday Jan. 1, 2001”). HCP tests receptive aphasia by the subject's ability to follow a simple command (for example “Lift your right hand and touch your nose”).
In addition, the caregiver is present with the patient for the entire MDMP and is able to communicate and participate with the HCP during the video call assessment. The HCP uses the video call assessment to determine if the patient's symptoms (as defined for neurotoxicity) necessitate immediate transfer to hospital. The HCP schedules video calls with the patients a minimum of every 12 hours (e.g., 8 am and 8 pm) daily during the MDMP. The frequency was increased when there were any concerns by the HCP.
The monitoring system also provides the functionality for the patient or caregiver to activate an “I don't feel well” button 320b on the device tablet 170 in the event of the subject experiencing any neurological symptoms. Activating the button 320b immediately generates an alarm and notifies the HCP and allows for an immediate video call assessment to be initiated. HCP advises transfer to an inpatient facility if any of the neurological symptoms were greater than mild in severity. In addition, as part of screening, patients and caregivers were trained to activate the “I don't feel well” button 320b for any moderate symptoms of speech disorders, disturbances in consciousness, deterioration of hand writing, confusion or disorientation, hypotension, hypoxia, transaminitis, hypertension, vomiting, diarrhea, or other symptoms that may be associated with a CRS.
Subjects were trained to resend the “I don't feel well” signal if no response from the HCP is received in 5 minutes. If there is still no response after another 5 minutes, 10 minutes total from the initial alarm, then the subject was to call emergency medical service (EMS) or dial 911 immediately. Likewise, when the HCP responded to any alarm generated from the subject and the subject or caregiver did not answer within 10 minutes, then the HCP made 1 attempt to call the subject's personal phone. If the subject or caregiver was still not reachable, the HCP had EMS dispatched to the subject's location immediately. The HCP phone is configured so that a loud audible alarm is made and repeated every 5 minutes until the HCP responds or if no data is transferred for 15 minutes. The HCP then used the compendium of vital sign's absolute value and/or deviation from baseline (provided by the health management system (HMS) 270a) and the subject's clinical status (provided by direct subject/caregiver telephone and video contact), to make decisions on urgency of response, appropriate intervention and subject disposition.
During MDMP any device malfunction (e.g., a patient wearable device malfunction, a sensor device malfunction, an axillary temperature patch malfunction, a blood pressure sensor malfunction, a communication network malfunction, an in-home hub malfunction, etc.) that is detected within 15 minutes generated an alarm to the HCP. The HCP contacts the patient immediately via the video calling functionality to assess the patient's safety, clinical status, and any specific circumstances associated with the device malfunction (e.g., device inadvertently dislodged, low battery charge, intermittent loss of signal transmission etc.) If the HCP has any concern of patient safety, HCP advises the patient to immediately go to the hospital.
Patients were provided with a full set of replacement devices to be used in case of a malfunction. In addition, a manual oral thermometer is provided to the patients, as needed or directed by the HCP. In the case of a device malfunction and the HCP decides that the patient is safe via the video conference, the HCP directs the patient to switch to the replacement device(s) immediately. In addition, HCP may contact a health monitoring platform 270a (e.g., Current Health's 24/7 hotline, etc.) for device support and troubleshooting for assistance. It is recommended that the HCP remain in contact with the subject until device malfunction is resolved. If these interventions by HCP fail to resolve the device malfunction, then HCP advises the patient to proceed immediately to the hospital. Only United States (US) Food and Drug Administration (FDA) cleared vital sign monitoring devices and platform 270m used. During the MDMP, subjects were required to live no more than 1-hour transportation by car from an advanced medical care facility. An advanced medical care facility included staff trained to manage acutely ill patients such as those who may have developed CRS. Subjects were allowed to stay at a hotel or other outpatient hospital housing facilities to fulfil the 1-hour transportation requirement. Subjects were trained to call emergency medical services for any concerns or for any delay in communication with the HCP.
Subjects were provided with duplicate devices (e.g., BP monitor, axillary temperature patch, Current Health wearable device) of the health management system (HMS) 270a 270m in case of unexpected device malfunction (see above). In addition, subjects were provided with a dedicated in-house Wi-Fi device (home hub 295m,n) for the sole purpose of uninterrupted transmission of vital signs and for communication including video contact with the HCP. Subjects, caregivers, and HCP have access to a 24/7 helpline for any technical issues relating to the home digital monitoring devices, platform or communication.
Alternative monitoring devices may be used, such as a Biobeat monitoring device (https://www.bio-beat.com/), which may be used to measure pulse pressure, continuous blood pressure, blood saturation, pulse rate, respiratory rate, systematic vascular resistance, heart rate variability, arterial pressure, skin temperature, heart stroke volume, cardiac output, and cardiac index. The Biobeat device may be able to communicate with smart devices or otherwise provide continuous or semi-continuous wireless monitoring features. The device may be self-adhesive and may have disposable chest patches and/or a cuff accessory.
With further reference to
Non-investigational Product Dosage and Administration included: Dexamethasone-Premedication with dexamethasone (or prednisone): Dexamethasone 16 mg (or equivalent prednisone 100 mg) intravenously (IV): up to 6 hours before start of treatment in each treatment cycle. Subjects 45 kg had 2 additional 8 mg doses (subjects <45 kg receive 2 doses of 5 mg/m2 rounded to the nearest mg) of oral dexamethasone to use as needed for treatment of CRS symptoms only if instructed by HCP. It was recommended that hospitalization was strongly considered for subjects who required interruption of blinatumomab for >4 hours.
Written informed consent was obtained from all subjects before any study-specific screening procedures were performed. Study-specific procedures occurred according to the Schedule of Assessments
Descriptive statistics for demographic and safety were summarized as appropriate. For categorical variables, the number and percentage of subjects in each category were summarized. Continuous variables were summarized by n, mean, standard deviation, median, Q1 (25th percentile), Q3 (75th percentile), minimum, and maximum values.
The example study determined the safety and feasibility of complete outpatient blinatumomab administration for subjects with minimal residual disease (MRD) of B-precursor acute lymphoblastic leukemia (ALL). Blinatumomab administration has been demonstrated to be efficacious in this population for converting subjects to MRD negative status (MRD <0.1%). However, the mechanism of action (MOA) of T cell activation and cytokine production can result in potentially severe toxicity, specifically cytokine release syndrome (CRS) and/or neurotoxicity (NT). The incidence of these potentially severe side effects has been shown to be low. In the BLAST study, 3% and 13% of subjects had severe CRS and NT respectively (i.e., Gökbuget et al, 2018).
The objective of the example study was to determine the safety and feasibility of complete outpatient blinatumomab administration for subjects with MRD of B-precursor ALL. The study used mobile electronic devices (tablet 170) to electronically communicate with the HCP, and a Wi-Fi enabled platform 200a for the real-time constant transfer of data and communication between subject and HCP 250a to detect clinically important changes. The data provided to the HCP enabled the HCP to identify subjects at risk of developing grade 3 or 4 CRS, NT, or other serious adverse events (SAEs) requiring hospitalization during the mandatory device monitoring period (MDMP). The HCP then directed such subjects to the appropriate medical facility for hospitalization when needed. The population for this study (MRD of B-precursor ALL) had a low incidence of severe CRS and NT and a reasonable target population to evaluate the feasibility of complete outpatient blinatumomab administration.
The example study used a Current Health (CH) system 270m and platform for outpatient monitoring. Subjects who were in a high-acuity environment, such as an operating room (OR) or intensive care unit (ICU), or those who were acutely ill and that developed immediate and life-threatening arrhythmias were excluded from the CH platform and not enrolled into the example study. As illustrated in
B-precursor ALL is a malignant disease of lymphatic progenitor cells in the bone marrow or sites of lymphatic system. Immature lymphoblasts proliferate in the bone marrow and may infiltrate other organs. As a consequence, the normal hematopoiesis in the bone marrow is suppressed. Acute lymphoblastic leukemia is a rare malignant disease with an overall incidence of 1.1/100,000 per year. Acute lymphoblastic leukemia has a bimodal distribution with an early peak at 4 to 5 years of age (incidence of 4.5/100,000 per year) followed by a second gradual increase at 50 years (incidence of 2/100,000 per year). It represents 80% of acute childhood leukemia and 20% of acute leukemia cases in adults (i.e., Pui and Evans 1998; Jabbour et al, 2005; Larson 2005; Howlader et al, 2012).
Seventy-5 percent of adult subjects with ALL is of B-cell lineage and approximately 25% is derived from T-cell lineage. The majority of subjects with B-cell lineage ALL have an immature immunophenotype and were classified as B-precursor ALL. CD19 is expressed in all subtypes of B-ALL (Bassan et al, 2004). The Philadelphia chromosome (Ph) represents the most frequent cytogenetic aberration in adult ALL and is found in 20-30% of subjects with B-precursor ALL. Adult ALL can be stratified into risk groups that were the basis for risk adapted treatment strategies. A selection of prognostic factors in B-precursor ALL: Prognostic Factors for Risk Stratification of Adult B-precursor ALL.
A white blood cell count (WBC) of <30,000/1 at diagnosis and younger age were favorable factors in adult ALL. Additionally, a short interval until achievement of a complete remission (CR) and a complete molecular remission following induction (MRD negative; <1 leukemic cell in 104 bone marrow cells is detectable) were favorable factors. Outcome of therapy in adult patients with ALL has improved substantially over the last 10 years with CR rates of 85 to 90% and overall survival (OS) rates of 40 to 50% (Gökbuget and Hoelzer, 2010). Pediatric protocols have been the guideline to develop treatment regimens for adult ALL. These regimens consist of 3 phases: induction, consolidation, and maintenance therapy. Generally, the therapeutic “state of the art” modalities for adult leukemia can be summarized (Gökbuget and Hoelzer, 2011). 4- to 5 drug induction regimens using vincristine and prednisone, adding anthracyclines, cyclophosphamide, asparaginase (or a combination of these agents) to achieve CR. Intensified consolidation therapy based on cyclical administration of cytarabine, anthracyclines, methotrexate, asparaginase and repeated induction to reduce the level of MRD.
Protracted maintenance therapy (about 2 years) using methotrexate combined with mercaptopurine; allogeneic stem cell transplantation in first CR in high-risk patients: Allogeneic hematopoietic stem cell transplantation (HSCT) is the most intensive option of consolidation in first CR of high-risk patients. Progress in therapy and optimized risk stratification, which enabled patient-tailored treatment, were important factors contributing to improvement of treatment outcome. In spite of the success in upfront treatment, the outcome in most adults with recurring disease irrespective of their prior treatment is dismal, as they cannot be rescued using currently available therapy (Fielding et al, 2007). Thus, prevention of relapse is the major treatment goal in patients resistant or intolerant to chemotherapy.
The platform illustrated in
In the context of the example study, the health management system (HMS) 270a was intended for intermittent or spot-check monitoring, in adults, of: respiratory rate (RR) (every 30 secs); non-invasive blood pressure (BP); lung function & spirometry (not collected for this study); and weight (not collected for this study). The health management system (HMS) 270a generated intermittent respiration rates by sampling sensor data every 30 seconds. This meant that every 30 seconds new respiration rates were available for use in the alarm system and for presentation on an associated dashboard. This functionality was assessed using physician-underscored end tidal CO2 in CH 510(k) K182453. The health management system (HMS) 270a functioned as a hub with seamless, wireless integrations. Data flows directly through the CH wearable via integrated third-party devices such as: the axillary temperature monitor and the BP monitor. For the example study, the following was monitored and collected: heart rate (HR), axillary temperature respiratory rate (RR), oxygen saturation, and blood pressure (BP). The health management system (HMS) 270a was not intended for use in high-acuity environments, such as ICUs or ORs, or for use on acutely ill cardiac patients with the potential to develop life threatening arrhythmias eg, very fast atrial fibrillation and is not intended for peripheral capillary oxygen saturation (SpO2) monitoring in conditions of high motion or low perfusion. These excluded patients and conditions were not be eligible for this example study.
Additional detail related to the health management system (HMS) 270a and integrated platform is described herein. Blinatumomab is a CD19-directed bispecific single-chain bispecific binding molecule construct designed to link B cells and T cells resulting in T-cell activation and a cytotoxic T-cell response against CD19 expressing cells. As stated previously blinatumomab is approved for the treatment of MRD of B-precursor ALL and has shown efficacy in the recently completed BLAST trial (Gökbuget et al, 2018). The approval for blinatumomab recommends that the initiation of cycle 1 (first 3 days) and of cycle 2 (first 2 days) be given while patients are admitted to hospital. In this investigational study we are testing the hypothesis that blinatumomab can be given as an outpatient for the entire 28 days if subjects are monitored during the initiation days. The blinatumomab infusion, doses, and indication for use were consistent with an associated FDA approved label.
Results from previously conducted pivotal Study M103-203 and supportive Study M103-202 showed similar high (up to 80%) MRD response rates after blinatumomab treatment in subjects with ALL in complete hematologic remission (<5% bone marrow blasts) who were MRD positive at the start of blinatumomab treatment baseline. Minimal residual disease response is a strong prognostic factor for relapse after achieving CR regardless of treatment choice or risk classification system (Lussana et al, 2016; van Dongen et al, 2015; Gökbuget et al, 2012; Gökbuget and Hoelzer, 2011; Bassan et al, 2009; Brüggemann et al, 2006). At the time of relapse, the strongest prognostic factors for OS are duration of initial remission and age (i.e., Oriol et al, 2010; Fielding et al, 2007; Thomas et al, 1999).
A published meta-analysis of 16 studies in adults with ALL solidified the association between MRD-negative status and improved clinical outcomes (event-free survival [EFS] and OS) that has up to this point been based largely on reports of individual studies with variable sample sizes. Of particular interest, EFS and OS for subjects who are MRD negative (MRD <0.1%) were shown to be remarkably consistent across a variety of subgroups (eg, MRD detection by flow cytometry vs polymerase chain reaction (PCR), MRD assessment after induction vs after consolidation, definition of MRD positivity, Ph status, and B-cell or T-cell phenotype) (i.e., Berry et al, 2017).
Key safety factors, that had been identified in clinical trials, were (and are) NT, CRS, and medication errors. Most AEs occurred within the first few weeks of the first cycle and were mitigated by appropriate measures such as temporary interruption without negatively affecting therapeutic benefit. Based on the short half-life of blinatumomab, in the presence of an AE, blinatumomab can be rapidly discontinued and cleared, which may enhance the ability to manage the AE effectively. In addition, the rate of severe AEs, in particular, CRS, are low enough to warrant the evaluation of complete outpatient administration of blinatumomab. This is particularly so in the MRD positive population, who by definition have low tumor burden. Moreover, the CH system is FDA cleared to accurately assess vitals and transmit vital signs efficiently to an HCP. In addition to benefit of MRD treatment, full outpatient blinatumomab is anticipated to be more convenient for patients.
The above benefit risk assessment supports the conduct of this clinical trial (i.e., the example study). Reference was made to an Investigator's Brochure for further data on blinatumomab. Training material was provided by CH with further information on the digital devices used in the study. The example study determined the safety and feasibility of complete outpatient blinatumomab administration for subjects with MRD of B-precursor ALL using health management system (HMS) 270a to measure vital signs and transmit the vital signs to the HCP, mobile electronic devices (e.g., a tablet 150 of
During screening, subjects and caregivers were trained on the health management system (HMS) 270a and assessed for compliance. Once enrolled, subjects received 2 complete cycles of blinatumomab in the outpatient setting in accordance with the monitoring and intervention guidelines. After the end of cycle 2 clinical assessment visit, some subjects may continue to receive 2 additional (optional) cycles of outpatient blinatumomab. The end of study visit occurred 30 days (3 days) after the last dose of blinatumomab 506a, 507b. The end coincided with the end of cycle 2 clinical assessment for subjects ending after cycle 2 or after cycle 3 or 4 if subjects and PI's chose to receive the optional consolidation cycles 3 and/or 4 as illustrated in
The overall study design was described by the study schema of
Therapeutic intervention is any measurable action taken by the subject or performed on the subject as a result of the onset of the clinical parameters described. Such actions may include: Advice from HCP to immediately call EMS or dial 911, discontinuation of the blinatumomab infusion, subject taking an oral medication, subject receiving a medication or intervention by any emergency or hospital medical services, intervention such as administering any medication (IV or PO or PR) or IV fluids or oxygen etc Time to therapeutic intervention (TTI) is the measured time between the delivery of the device alert or unscheduled contact with HP by subject/CG to report a change to the time of initiation of the therapeutic intervention as defined.
aBlinatumomab will be manufactured and packaged by Amgen and distributed using Amgen clinical study drug distribution procedures.
The medical devices provided by Amgen for use in this study include: infusion pump and infusion line (e.g., infusion 110 of
In at least part, infusion pumps 110, IV bags and tubing, and ancillary materials (e.g., syringes, sterile needles, alcohol prep pads, etc.) were provided by Amgen when the site was unable to provision. Additional non-investigational medical devices that were commercially available and were not provided or reimbursed by Amgen. The investigator overseeing the conduct of the example study at each respective institution were responsible for obtaining these supplies. When site supplies were used, the Investigator was responsible for obtaining and maintaining these supplies.
A central component of the health management system (HMS) 270a was a patient wearable device 115, 215a, 315a-c (i.e., as available from Current Health, Biobeat, etc.). In any event, the patient wearable device 115, 215a, 315a-c worn on the upper arm. The wearable device 115 monitored a subject's HR, RR, skin temperature, oxygen saturation, step count and activity levels at a maximum rate of every 2 seconds. For this example study, the following vital signs were collected and evaluated: HR, RR, axillary temperature, and oxygen saturation.
The patient wearable device 115 was also integrated with the axillary temperature sensor (e.g., auxiliary temperature sensor 241m of
Sites administered blinatumomab as per the FDA-approved guidelines. Common Terminology Criteria for Adverse Events (CTCAE) v 5.0 will be used to grade toxicities. grade 1 and grade 2 events will be managed symptomatically with temporary discontinuation of the blinatumomab (if considered necessary by the investigator). The investigator will intervene in accordance with the alert algorithm for other AEs.
aObtain brain MRI and perform cerebrospinal fluid (CSF) analysis, if indicated, and if there are no contraindications.
Compliance with using the devices 110, 115, 140, 150, 200a, 200m, 200n was determined from the data transmitted by the device. Device alerts confirmed when data was not being transmitted from the devices (i.e., the patient wearable device 115, the auxiliary temperature monitor 241m, and the blood pressure monitor 240m). The subject was instructed to call HCP immediately when alert was received that data was not being transmitted from the devices 115, 240m, 241m. The HCP or designee were advised to contact the subject immediately if data was not being received. Assessing compliance with blinatumomab therapy per protocol and per IPIM was performed by study centers and clinical research associates. When a subject failed to comply with the instructions for use of the device, the subject received re-education/re-training on use of the device. When the subject failed to comply a second time, the subject was removed from the study and the subject was recommended for admission to a hospital for the remainder of the MDMP as per the product FDA label.
Digital health device monitoring of vital signs of patients during the mandatory monitoring period was conducted. During the MDMP, subjects wore a patient wearable device 115 continuously 24 hours a day. After the first 24 hours, subjects were allowed to remove one or all of the devices for a maximum of 1 hour per day. This allowed subjects to attend to personal activities such as taking a bath or shower. Subject was clinically stable with normal vitals and no evidence of NT prior to the start of the 60-minute period. The breaks were coordinated with the HCP, as no data was transmitted during this period. It was recommended that subjects use this time to change the device(s) and place it (them) in the charger (e.g., charger 442a of
Vital signs (HR, RR, oxygen saturation, and axillary temperature) were measured continuously using health management system (HMS) 270a, as specified in a schedule of activities. There was no data transmission to HCP while subjects were transported to home from the outpatient facility. Vital sign data (i.e., sensor data) was stored but not transmitted in real time. Non-invasive BP was performed as specified in the schedule of activities. Vital signs were available as a constant live feed to the HCP or designee for the entire MDMP. Alarms/alerts were generated, and indicated when a vital sign was outside of the preset parameters. Details of the data that was monitored using the devices 115, 140 is described in detail herein.
The digital health tools used in this example study collected data beyond what was specified for analysis in this protocol. Digital Health is capable of collecting HR, RR, axillary temperature, skin temperature, oxygen saturation, step count and activity levels, and noninvasive BP. The patient device 150 also supported collection of subject responses in accordance with QLQ-C30.
The above description describes various devices, assemblies, components, subsystems and methods for use related to a drug delivery device such as a pre-filled syringe. The devices, assemblies, components, subsystems, methods or drug delivery devices (i.e., prefilled syringe) can further comprise or be used with a drug including but not limited to those drugs identified below as well as their generic and biosimilar counterparts. The term drug, as used herein, can be used interchangeably with other similar terms and can be used to refer to any type of medicament or therapeutic material including traditional and non-traditional pharmaceuticals, nutraceuticals, supplements, biologics, biologically active agents and compositions, large molecules, biosimilars, bioequivalents, therapeutic antibodies, polypeptides, proteins, small molecules and generics. Non-therapeutic injectable materials are also encompassed. The drug may be in liquid form, a lyophilized form, or in a reconstituted from lyophilized form. The following example list of drugs should not be considered as all-inclusive or limiting.
The drug will be contained in a reservoir within the pre-filled syringe for example. In some instances, the reservoir is a primary container that is either filled or pre-filled for treatment with the drug. The primary container can be a vial, a cartridge or a pre-filled syringe. In some embodiments, the reservoir of the drug delivery device may be filled with or the device can be used with colony stimulating factors, such as granulocyte colony-stimulating factor (G-CSF). Such G-CSF agents include but are not limited to Neulasta® (pegfilgrastim, pegylated filgastrim, pegylated G-CSF, pegylated hu-Met-G-CSF) and Neupogen® (filgrastim, G-CSF, hu-MetG-CSF), UDENYCA® (pegfilgrastim-cbqv), Ziextenzo® (LA-EP2006; pegfilgrastim-bmez), or FULPHILA (pegfilgrastim-bmez).
In other embodiments, the drug delivery device may contain or be used with an erythropoiesis stimulating agent (ESA), which may be in liquid or lyophilized form. An ESA is any molecule that stimulates erythropoiesis. In some embodiments, an ESA is an erythropoiesis stimulating protein. As used herein, “erythropoiesis stimulating protein” means any protein that directly or indirectly causes activation of the erythropoietin receptor, for example, by binding to and causing dimerization of the receptor. Erythropoiesis stimulating proteins include erythropoietin and variants, analogs, or derivatives thereof that bind to and activate erythropoietin receptor; antibodies that bind to erythropoietin receptor and activate the receptor; or peptides that bind to and activate erythropoietin receptor. Erythropoiesis stimulating proteins include, but are not limited to, Epogen® (epoetin alfa), Aranesp® (darbepoetin alfa), Dynepo® (epoetin delta), Mircera® (methyoxy polyethylene glycol-epoetin beta), Hematide®, MRK-2578, INS-22, Retacrit® (epoetin zeta), Neorecormon® (epoetin beta), Silapo® (epoetin zeta), Binocrit® (epoetin alfa), epoetin alfa Hexal, Abseamed® (epoetin alfa), Ratioepo® (epoetin theta), Eporatio® (epoetin theta), Biopoin® (epoetin theta), epoetin alfa, epoetin beta, epoetin iota, epoetin omega, epoetin delta, epoetin zeta, epoetin theta, and epoetin delta, pegylated erythropoietin, carbamylated erythropoietin, as well as the molecules or variants or analogs thereof.
Among particular illustrative proteins are the specific proteins set forth below, including fusions, fragments, analogs, variants or derivatives thereof: OPGL specific antibodies, peptibodies, related proteins, and the like (also referred to as RANKL specific antibodies, peptibodies and the like), including fully humanized and human OPGL specific antibodies, particularly fully humanized monoclonal antibodies; Myostatin binding proteins, peptibodies, related proteins, and the like, including myostatin specific peptibodies; IL-4 receptor specific antibodies, peptibodies, related proteins, and the like, particularly those that inhibit activities mediated by binding of IL-4 and/or IL-13 to the receptor; Interleukin 1-receptor 1 (“IL1-R1”) specific antibodies, peptibodies, related proteins, and the like; Ang2 specific antibodies, peptibodies, related proteins, and the like; NGF specific antibodies, peptibodies, related proteins, and the like; CD22 specific antibodies, peptibodies, related proteins, and the like, particularly human CD22 specific antibodies, such as but not limited to humanized and fully human antibodies, including but not limited to humanized and fully human monoclonal antibodies, particularly including but not limited to human CD22 specific IgG antibodies, such as, a dimer of a human-mouse monoclonal hLL2 gamma-chain disulfide linked to a human-mouse monoclonal hLL2 kappa-chain, for example, the human CD22 specific fully humanized antibody in Epratuzumab, CAS registry number 501423-23-0; IGF-1 receptor specific antibodies, peptibodies, and related proteins, and the like including but not limited to anti-IGF-1R antibodies; B-7 related protein 1 specific antibodies, peptibodies, related proteins and the like (“B7RP-1” and also referring to B7H2, ICOSL, B7h, and CD275), including but not limited to B7RP-specific fully human monoclonal IgG2 antibodies, including but not limited to fully human IgG2 monoclonal antibody that binds an epitope in the first immunoglobulin-like domain of B7RP-1, including but not limited to those that inhibit the interaction of B7RP-1 with its natural receptor, ICOS, on activated T cells; IL-15 specific antibodies, peptibodies, related proteins, and the like, such as, in particular, humanized monoclonal antibodies, including but not limited to HuMax IL-15 antibodies and related proteins, such as, for instance, 145c7; IFN gamma specific antibodies, peptibodies, related proteins and the like, including but not limited to human IFN gamma specific antibodies, and including but not limited to fully human anti-IFN gamma antibodies; TALL-1 specific antibodies, peptibodies, related proteins, and the like, and other TALL specific binding proteins; Parathyroid hormone (“PTH”) specific antibodies, peptibodies, related proteins, and the like; Thrombopoietin receptor (“TPO-R”) specific antibodies, peptibodies, related proteins, and the like; Hepatocyte growth factor (“HGF”) specific antibodies, peptibodies, related proteins, and the like, including those that target the HGF/SF:cMet axis (HGF/SF:c-Met), such as fully human monoclonal antibodies that neutralize hepatocyte growth factor/scatter (HGF/SF); TRAIL-R2 specific antibodies, peptibodies, related proteins and the like; Activin A specific antibodies, peptibodies, proteins, and the like; TGF-beta specific antibodies, peptibodies, related proteins, and the like; Amyloid-beta protein specific antibodies, peptibodies, related proteins, and the like; c-Kit specific antibodies, peptibodies, related proteins, and the like, including but not limited to proteins that bind c-Kit and/or other stem cell factor receptors; OX40L specific antibodies, peptibodies, related proteins, and the like, including but not limited to proteins that bind OX40L and/or other ligands of the OX40 receptor; Activase® (alteplase, tPA); Aranesp® (darbepoetin alfa) Erythropoietin [30-asparagine, 32-threonine, 87-valine, 88-asparagine, 90-threonine], Darbepoetin alfa, novel erythropoiesis stimulating protein (NESP); Epogen® (epoetin alfa, or erythropoietin); GLP-1, Avonex® (interferon beta-1a); Bexxar® (tositumomab, anti-CD22 monoclonal antibody); Betaseron® (interferon-beta); Campath® (alemtuzumab, anti-CD52 monoclonal antibody); Dynepo® (epoetin delta); Velcade® (bortezomib); MLN0002 (anti-α4ß7 mAb); MLN1202 (anti-CCR2 chemokine receptor mAb); Enbrel® (etanercept, TNF-receptor/Fc fusion protein, TNF blocker); Eprex® (epoetin alfa); Erbitux® (cetuximab, anti-EGFR/HER1/c-ErbB-1); Genotropin® (somatropin, Human Growth Hormone); Herceptin® (trastuzumab, anti-HER2/neu (erbB2) receptor mAb); Kanjinti™ (trastuzumab-anns) anti-HER2 monoclonal antibody, biosimilar to Herceptin®, or another product containing trastuzumab for the treatment of breast or gastric cancers; Humatrope® (somatropin, Human Growth Hormone); Humira® (adalimumab); Vectibix® (panitumumab), Xgeva® (denosumab), Prolia® (denosumab), Immunoglobulin G2 Human Monoclonal Antibody to RANK Ligand, Enbrel® (etanercept, TNF-receptor/Fc fusion protein, TNF blocker), Nplate® (romiplostim), rilotumumab, ganitumab, conatumumab, brodalumab, insulin in solution; Infergen® (interferon alfacon-1); Natrecor® (nesiritide; recombinant human B-type natriuretic peptide (hBNP); Kineret® (anakinra); Leukine® (sargamostim, rhuGM-CSF); LymphoCide® (epratuzumab, anti-CD22 mAb); Benlysta™ (lymphostat B, belimumab, anti-BlyS mAb); Metalyse® (tenecteplase, t-PA analog); Mircera® (methoxy polyethylene glycol-epoetin beta); Mylotarg® (gemtuzumab ozogamicin); Raptiva® (efalizumab); Cimzia® (certolizumab pegol, CDP 870); Soliris™ (eculizumab); pexelizumab (anti-C5 complement); Numax® (MEDI-524); Lucentis® (ranibizumab); Panorex® (17-1A, edrecolomab); Trabio® (lerdelimumab); TheraCim hR3 (nimotuzumab); Omnitarg (pertuzumab, 2C4); Osidem® (IDM-1); OvaRex® (B43.13); Nuvion® (visilizumab); cantuzumab mertansine (huC242-DM1); NeoRecormon® (epoetin beta); Neumega® (oprelvekin, human interleukin-11); Orthoclone OKT3® (muromonab-CD3, anti-CD3 monoclonal antibody); Procrit® (epoetin alfa); Remicade® (infliximab, anti-TNFα monoclonal antibody); Reopro® (abciximab, anti-GP lib/Ilia receptor monoclonal antibody); Actemra® (anti-IL6 Receptor mAb); Avastin® (bevacizumab), HuMax-CD4 (zanolimumab); Mvasi™ (bevacizumab-awwb); Rituxan® (rituximab, anti-CD20 mAb); Tarceva® (erlotinib); Roferon-A®-(interferon alfa-2a); Simulect® (basiliximab); Prexige® (lumiracoxib); Synagis® (palivizumab); 145c7-CHO (anti-IL15 antibody, see U.S. Pat. No. 7,153,507); Tysabri® (natalizumab, anti-α4integrin mAb); Valortim® (MDX-1303, anti-B. anthracis protective antigen mAb); ABthrax™; Xolair® (omalizumab); ETI211 (anti-MRSA mAb); IL-1 trap (the Fc portion of human IgG1 and the extracellular domains of both IL-1 receptor components (the Type I receptor and receptor accessory protein)); VEGF trap (Ig domains of VEGFR1 fused to IgG1 Fc); Zenapax® (daclizumab); Zenapax® (daclizumab, anti-IL-2Rα mAb); Zevalin® (ibritumomab tiuxetan); Zetia® (ezetimibe); Orencia® (atacicept, TACI-Ig); anti-CD80 monoclonal antibody (galiximab); anti-CD23 mAb (lumiliximab); BR2-Fc (huBR3/huFc fusion protein, soluble BAFF antagonist); CNTO 148 (golimumab, anti-TNFα mAb); HGS-ETR1 (mapatumumab; human anti-TRAIL Receptor-1 mAb); HuMax-CD20 (ocrelizumab, anti-CD20 human mAb); HuMax-EGFR (zalutumumab); M200 (volociximab, anti-α5β1 integrin mAb); MDX-010 (ipilimumab, anti-CTLA-4 mAb and VEGFR-1 (IMC-18F1); anti-BR3 mAb; anti-C. difficile Toxin A and Toxin B C mAbs MDX-066 (CDA-1) and MDX-1388); anti-CD22 dsFv-PE38 conjugates (CAT-3888 and CAT-8015); anti-CD25 mAb (HuMax-TAC); anti-CD3 mAb (NI-0401); adecatumumab; anti-CD30 mAb (MDX-060); MDX-1333 (anti-IFNAR); anti-CD38 mAb (HuMax CD38); anti-CD40L mAb; anti-Cripto mAb; anti-CTGF Idiopathic Pulmonary Fibrosis Phase I Fibrogen (FG-3019); anti-CTLA4 mAb; anti-eotaxin1 mAb (CAT-213); anti-FGF8 mAb; anti-ganglioside GD2 mAb; anti-ganglioside GM2 mAb; anti-GDF-8 human mAb (MYO-029); anti-GM-CSF Receptor mAb (CAM-3001); anti-HepC mAb (HuMax HepC); anti-IFNα mAb (MEDI-545, MDX-198); anti-IGF1R mAb; anti-IGF-1R mAb (HuMax-Inflam); anti-IL12 mAb (ABT-874); anti-IL12/IL23 mAb (CNTO 1275); anti-IL13 mAb (CAT-354); anti-IL2Rα mAb (HuMax-TAC); anti-IL5 Receptor mAb; anti-integrin receptors mAb (MDX-018, CNTO 95); anti-IP10 Ulcerative Colitis mAb (MDX-1100); BMS-66513; anti-Mannose Receptor/hCGβ mAb (MDX-1307); anti-mesothelin dsFv-PE38 conjugate (CAT-5001); anti-PD1mAb (MDX-1106 (ONO-4538)); anti-PDGFRα antibody (IMC-3G3); anti-TGFß mAb (GC-1008); anti-TRAIL Receptor-2 human mAb (HGS-ETR2); anti-TWEAK mAb; anti-VEGFR/Flt-1 mAb; and anti-ZP3 mAb (HuMax-ZP3).
In some embodiments, the drug delivery device may contain or be used with a sclerostin antibody, such as but not limited to romosozumab, blosozumab, BPS 804 (Novartis), Evenity™ (romosozumab-aqqg), another product containing romosozumab for treatment of postmenopausal osteoporosis and/or fracture healing and in other embodiments, a monoclonal antibody (IgG) that binds human Proprotein Convertase Subtilisin/Kexin Type 9 (PCSK9). Such PCSK9 specific antibodies include, but are not limited to, Repatha® (evolocumab) and Praluent® (alirocumab). In other embodiments, the drug delivery device may contain or be used with rilotumumab, bixalomer, trebananib, ganitumab, conatumumab, motesanib diphosphate, brodalumab, vidupiprant or panitumumab. In some embodiments, the reservoir of the drug delivery device may be filled with or the device can be used with IMLYGIC® (talimogene laherparepvec) or another oncolytic HSV for the treatment of melanoma or other cancers including but are not limited to OncoVEXGALV/CD; OrienX010; G207, 1716; NV1020; NV12023; NV1034; and NV1042. In some embodiments, the drug delivery device may contain or be used with endogenous tissue inhibitors of metalloproteinases (TIMPs) such as but not limited to TIMP-3. In some embodiments, the drug delivery device may contain or be used with Aimovig® (erenumab-aooe), anti-human CGRP-R (calcitonin gene-related peptide type 1 receptor) or another product containing erenumab for the treatment of migraine headaches. Antagonistic antibodies for human calcitonin gene-related peptide (CGRP) receptor such as but not limited to erenumab and bispecific antibody molecules that target the CGRP receptor and other headache targets may also be delivered with a drug delivery device of the present disclosure.
Additionally, the sensors, devices, systems and methods of the present disclosure may be particularly advantageous in regard to out-patient treatments that may be associated with particular adverse side effects caused by similar molecules having a specific mechanism of action (MOA). For example, a bispecific T cell engager (BiTE®) molecules such as, but not limited to, BLINCYTO® (blinatumomab) can be used in or with the drug delivery device of the present disclosure. In some embodiments, the drug delivery device may contain or be used with AMG 160, or another product that contains a half-life extended (HLE) anti-prostate-specific membrane antigen (PSMA)×anti-CD3 BiTE® (bispecific T cell engager) construct. In some embodiments, the drug delivery device may contain or be used with AMG 199 or another product containing a half-life extended (HLE) bispecific T cell engager construct (BiTE®). In some embodiments, the drug delivery device may contain or be used with AMG 330 or another product containing an anti-CD33×anti-CD3 BiTE® (bispecific T cell engager) construct. In some embodiments, the drug delivery device may contain or be used with AMG 427 or another product containing a half-life extended (HLE) anti-fms-like tyrosine kinase 3 (FLT3)×anti-CD3 BiTE® (bispecific T cell engager) construct. In some embodiments, the drug delivery device may contain or be used with AMG 509 or another product containing a bivalent T-cell engager and is designed using XmAb® 2+1 technology. In some embodiments, the drug delivery device may contain or be used with AMG 562 or another product containing a half-life extended (HLE) CD19×CD3 BiTE® (bispecific T cell engager) construct. In some embodiments, the drug delivery device may contain or be used with AMG 596 or another product containing a CD3×epidermal growth factor receptor vIII (EGFRvIII) BiTE® (bispecific T cell engager) molecule. In some embodiments, the drug delivery device may contain or be used with AMG 673 or another product containing a half-life extended (HLE) anti-CD33×anti-CD3 BiTE® (bispecific T cell engager) construct. In some embodiments, the drug delivery device may contain or be used with AMG 701 or another product containing a half-life extended (HLE) anti-B-cell maturation antigen (BCMA)×anti-CD3 BiTE® (bispecific T cell engager) construct. In some embodiments, the drug delivery device may contain or be used with AMG 757 or another product containing a half-life extended (HLE) anti-delta-like ligand 3 (DLL3)×anti-CD3 BiTE® (bispecific T cell engager) construct. In some embodiments, the drug delivery device may contain or be used with AMG 910 or another product containing a half-life extended (HLE) epithelial cell tight junction protein claudin 18.2×CD3 BiTE® (bispecific T cell engager) construct.
In some embodiments, the drug delivery device may contain or be used with an APJ large molecule agonist such as but not limited to apelin or analogues thereof. In some embodiments, a therapeutically effective amount of an anti-thymic stromal lymphopoietin (TSLP) or TSLP receptor antibody is used in or with the drug delivery device of the present disclosure. In some embodiments, the drug delivery device may contain or be used with Avsola™ (infliximab-axxq), anti-TNF a monoclonal antibody, biosimilar to Remicade® (infliximab) (Janssen Biotech, Inc.) or another product containing infliximab for the treatment of autoimmune diseases. In some embodiments, the drug delivery device may contain or be used with Kyprolis® (carfilzomib), (2S)-N-((S)-1-((S)-4-methyl-1-((R)-2-methyloxiran-2-yl)-1-oxopentan-2-ylcarbamoyl)-2-phenylethyl)-2-((S)-2-(2-morpholinoacetamido)-4-phenylbutanamido)-4-methylpentanamide, or another product containing carfilzomib for the treatment of multiple myeloma. In some embodiments, the drug delivery device may contain or be used with Otezla® (apremilast), N-[2-[(15)-1-(3-ethoxy-4-methoxyphenyl)-2-(methylsulfonyl)ethyl]-2,3-dihydro-1,3-dioxo-1H-isoindol-4-yl]acetamide, or another product containing apremilast for the treatment of various inflammatory diseases. In some embodiments, the drug delivery device may contain or be used with Parsabiv™ (etelcalcetide HCl, KAI-4169) or another product containing etelcalcetide HCl for the treatment of secondary hyperparathyroidism (sHPT) such as in patients with chronic kidney disease (KD) on hemodialysis. In some embodiments, the drug delivery device may contain or be used with ABP 798 (rituximab), a biosimilar candidate to Rituxan®/MabThera™, or another product containing an anti-CD20 monoclonal antibody. In some embodiments, the drug delivery device may contain or be used with a VEGF antagonist such as a non-antibody VEGF antagonist and/or a VEGF-Trap such as aflibercept (Ig domain 2 from VEGFR1 and Ig domain 3 from VEGFR2, fused to Fc domain of IgG1). In some embodiments, the drug delivery device may contain or be used with ABP 959 (eculizumab), a biosimilar candidate to Soliris®, or another product containing a monoclonal antibody that specifically binds to the complement protein C5. In some embodiments, the drug delivery device may contain or be used with Rozibafusp alfa (formerly AMG 570) is a novel bispecific antibody-peptide conjugate that simultaneously blocks ICOSL and BAFF activity. In some embodiments, the drug delivery device may contain or be used with Omecamtiv mecarbil, a small molecule selective cardiac myosin activator, or myotrope, which directly targets the contractile mechanisms of the heart, or another product containing a small molecule selective cardiac myosin activator. In some embodiments, the drug delivery device may contain or be used with Sotorasib (formerly known as AMG 510), a KRASG12C small molecule inhibitor, or another product containing a KRASG12C small molecule inhibitor. In some embodiments, the drug delivery device may contain or be used with Tezepelumab, a human monoclonal antibody that inhibits the action of thymic stromal lymphopoietin (TSLP), or another product containing a human monoclonal antibody that inhibits the action of TSLP. In some embodiments, the drug delivery device may contain or be used with AMG 714, a human monoclonal antibody that binds to Interleukin-15 (IL-15) or another product containing a human monoclonal antibody that binds to Interleukin-15 (IL-15). In some embodiments, the drug delivery device may contain or be used with AMG 890, a small interfering RNA (siRNA) that lowers lipoprotein(a), also known as Lp(a), or another product containing a small interfering RNA (siRNA) that lowers lipoprotein(a). In some embodiments, the drug delivery device may contain or be used with ABP 654 (human IgG1 kappa antibody), a biosimilar candidate to Stelara®, or another product that contains human IgG1 kappa antibody and/or binds to the p40 subunit of human cytokines interleukin (IL)-12 and IL-23. In some embodiments, the drug delivery device may contain or be used with Amjevita™ or Amgevita™ (formerly ABP 501) (mab anti-TNF human IgG1), a biosimilar candidate to Humira®, or another product that contains human mab anti-TNF human IgG1. In some embodiments, the drug delivery device may contain or be used with AMG 119, or another product containing a delta-like ligand 3 (DLL3) CART (chimeric antigen receptor T cell) cellular therapy. In some embodiments, the drug delivery device may contain or be used with AMG 119, or another product containing a delta-like ligand 3 (DLL3) CAR T (chimeric antigen receptor T cell) cellular therapy. In some embodiments, the drug delivery device may contain or be used with AMG 133, or another product containing a gastric inhibitory polypeptide receptor (GIPR) antagonist and GLP-1R agonist. In some embodiments, the drug delivery device may contain or be used with AMG 171 or another product containing a Growth Differential Factor 15 (GDF15) analog. In some embodiments, the drug delivery device may contain or be used with AMG 176 or another product containing a small molecule inhibitor of myeloid cell leukemia 1 (MCL-1). In some embodiments, the drug delivery device may contain or be used with AMG 256 or another product containing an anti-PD-1×IL21 mutein and/or an IL-21 receptor agonist designed to selectively turn on the Interleukin 21 (IL-21) pathway in programmed cell death-1 (PD-1) positive cells. In some embodiments, the drug delivery device may contain or be used with AMG 404 or another product containing a human anti-programmed cell death-1 (PD-1) monoclonal antibody being investigated as a treatment for patients with solid tumors. In some embodiments, the drug delivery device may contain or be used with AMG 430 or another product containing an anti-Jagged-1 monoclonal antibody. In some embodiments, the drug delivery device may contain or be used with AMG 506 or another product containing a multi-specific FAP×4-1BB-targeting DARPin® biologic under investigation as a treatment for solid tumors. In some embodiments, the drug delivery device may contain or be used with Efavaleukin alfa (formerly AMG 592) or another product containing an IL-2 mutein Fc fusion protein.
Although the drug delivery devices, assemblies, components, subsystems and methods have been described in terms of exemplary embodiments, they are not limited thereto. The detailed description is to be construed as exemplary only and does not describe every possible embodiment of the present disclosure. Numerous alternative embodiments could be implemented, using either current technology or technology developed after the filing date of this patent that would still fall within the scope of the claims defining the invention(s) disclosed herein.
Those skilled in the art will recognize that a wide variety of modifications, alterations, and combinations can be made with respect to the above described embodiments without departing from the spirit and scope of the invention(s) disclosed herein, and that such modifications, alterations, and combinations are to be viewed as being within the ambit of the inventive concept(s).
Priority is claimed to U.S. Patent Application No. 63/181,002, filed Apr. 28, 2021, the entire contents of which are hereby incorporated by reference herein.
Filing Document | Filing Date | Country | Kind |
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PCT/US22/26426 | 4/27/2022 | WO |
Number | Date | Country | |
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63181002 | Apr 2021 | US |