Body fluid sampling arrangements

Description

FIELD

The present invention relates to devices, arrangements and methods involving body fluid sampling with the assistance of a catalyst. In certain embodiments, the present invention is directed to integrated monitoring and body fluid sampling and monitoring devices and methods that permit both digital and alternative-site body fluid sampling and analysis.

BACKGROUND

In the discussion that follows, reference is made to certain structures and/or methods. However, the following references should not be construed as an admission that these structures and/or methods constitute prior art. Applicants expressly reserve the right to demonstrate that such structures and/or methods do not qualify as prior art.

According to the American Diabetes Association, diabetes is the fifth-deadliest disease in the United States and kills more than 213,000 people a year, the total economic cost of diabetes in 2002 was estimated at over $132 billion dollars. One out of every 10 health care dollars is spent on diabetes and its complications. The risk of developing type I juvenile diabetes is higher than virtually all other chronic childhood diseases. Since 1987 the death rate due to diabetes has increased by 45 percent, while the death rates due to heart disease, stroke, and cancer have declined.

A critical component in managing diabetes is frequent blood glucose monitoring. Currently, a number of systems exist for self-monitoring by the patient. Most fluid analysis systems, such as systems for analyzing a sample of blood for glucose content, comprise multiple separate components such as separate lancing, transport, and quantification portions. These systems are bulky, and often confusing and complicated for the user. The systems require significant user intervention.

Technology development in the field of self-monitoring of blood glucose has placed the burden of acquiring sufficient blood for conducting a test on the user of the technology. Historically, diabetics have been taught to lance their finger tips to produce blood for conducting the test. Ironically, the fingers are not only one of the most sensitive body parts to pain, but they also are among the areas of skin that are most highly perfused with blood. Earlier versions of consumer-oriented self-monitoring products usually required many microliters of blood, and the finger tips provided a reasonably convenient area to lance that would be most likely to produce the required volume of blood.

More recently, some self-monitoring systems offer the option to the user to test at alternate sites such as the palm, forearm, or thigh. While these sites are generally known to be significantly less sensitive to the pain associated with lancing, the adoption of alternate site testing has been limited for at least four reasons: (1) only a few meter products have been approved by the FDA for testing at alternate sites at this time; (2) many testers do not know that they can use their device at the alternate sites; (3) many testers find it relatively difficult to express sufficient blood at the alternate sites to perform a test; (4) data published in medical literature on some of the meters shows that there may be a distinct difference between glucose levels measured at alternate sites relative to the finger, particularly when glucose levels are falling and/or the subject may be hypoglycemic. Consequently, there is a perception by the medical community that there may be an increased risk for delayed or improper treatment by the diabetic if they act only on the basis of glucose levels measured from alternate sites. Thus, the finger lancing site remains the most frequently used test site by far.

Lancing devices and the lancets themselves have also evolved somewhat over the past few decades. Some lancing mechanisms may produce relatively less pain by either (1) projecting the lancet in and out of the skin in a more straight path and thus reducing stimulation of percutaneous nerves which provide the pain stimulus; and (2) offering depth control in the lancing device so that the user may balance the expression of sufficient blood against the level of pain. Furthermore, lancet manufacturers offer a variety of lancet sizes, lengths, and tip bevel patterns with some companies claiming that their lancet is less painful than others.

What remains clear is that the most testers, when lancing at the finger, often must put down the lancing device and apply pressure near the finger tip in order to produce sufficient blood for the test strip in the meter. Many instructions for use with conventional meter systems specifically prescribe that the user perform this “milking” process because without it, many will not spontaneously produce the required volume. Applicants have observed this phenomenon in the use of commonly available commercial sampling and meter systems. In a recent study, when a trained professional lanced the finger tips of 16 volunteer diabetic subjects at the maximum depth setting on commercially available device under controlled conditions, only 15% of lanced sites spontaneously produced sufficient blood for the meter to accurately measure glucose levels.

Attempts have been made in the past to take steps toward automation of the testing process at alternate sites. Specifically, the Sof-Tact® System offered by Medisense in the early 2000s had the capability to test automatically at alternate sites without any user intervention, but only after each lancet and test strip had been manually loaded into the device. This meter is no longer available on the market.

A device similar to the Soft-Tact® device is disclosed in U.S. Patent Application Publication No. 2004/0138588 A1. This device attempts to integrate all the functions required to complete a glucose test into one device. This device however still requires the user to load a lancet and a test strip prior to each individual testing event, and fails to describe a catalyst (i.e.—mechanism to stimulate or enhance expression of blood from the lanced wound site) that ensures that a sufficient sample is expressed from the wound.

The device is described in U.S. Patent Application Publication No. 2005/0010134 A1, and U.S. Pat. No. 6,793,633 B2 uses a spring, or motor driven mechanism, to apply pressure around the target wound area. From the description it appears that the user must insert a new lancet and test strip assembly for each test.

Another disadvantage with conventional arrangements such as the ones referenced above is that they involve complex and sometimes ineffective mechanisms for transferring blood or body fluid from the wound to a remote location for analysis. For example, many conventional arrangements and techniques utilize a solid lancet for creating a wound in the surface of the skin. After piercing the skin the lancet is retracted and a separate member, such as a tube, is positioned to transfer the blood or body fluid. Alternatively, an absorbent test strip is moved into position, manually or in an automated fashion, so that it absorbs the sample of blood or body fluid from the wound site. These arrangements and techniques are overly complex, and clearly rely upon the precise positioning of the tube or test strip to transfer the sample of blood or body fluid. When seeking to automate the sampling process, this precise positioning requires rather complex mechanical arrangements and controls that must operate under close tolerances. Such complex systems and arrangements are either costly, unreliable, or both.

Thus, conventional sampling devices and methods are overly reliant upon user intervention, such as milking, in order to consistently express a sufficient quantity of blood from the wound site, or are overly complex and/or lack reliability.

Moreover, while many diabetics continue to test their blood glucose levels with blood from the finger, testing at the alternate sites offers the advantage of significantly less pain when lancing the palm, forearm, etc. Thus, it would be advantageous to have an automatic and fully integrated meter constructed for sampling and/or testing at either the finger and the alternate sites.

SUMMARY OF THE INVENTION

According to the present invention, there are provided body fluid sampling and monitoring devices and methods that may address one or more of the shortcomings noted above associated with conventional systems and devices. According to the present invention, there may also be provided improved body fluid sampling and monitoring devices and methods that enable both digital and alternative-site body fluid sampling without significant user intervention.

As used herein “digital” means fingers or toes. “Digital body fluid” means expression of body fluid from a wound created on the fingers or toes, and encompasses lancing sites on the dorsal or palm side of the distal finger tips.

As used herein “alternate site” means a location on the body other than the digits, for example, the palm, forearm or thigh. “Alternate-site body fluid sampling” means expression of body fluid from the lancing site on a surface of the body other than the fingers or toes, and encompasses lancing sites on the palm, forearm, and thigh.

As used herein, “body fluid” encompasses whole blood, intestinal fluid, and mixtures thereof.

As used herein “integrated device” or “integrated meter” means a device or meter that includes all components necessary to perform sampling of body fluid, transport of body fluid, quantification of an analyte, and display of the amount of analyte contained in the sample of body fluid.

As used herein, the term “obstructed opening” means that the needle or skin piercing element is not retracted prior to extracting the body fluid from the wound created thereby. Thus, for example, the portion of the opening or wound on or just below the surface of the skin is at least partially obstructed by the skin piercing member or needle which will be located at the wound opening entrance on or just below the surface of the skin upon extraction of body fluid. This aspect of the present invention is believed to run counter to the conventional wisdom in the art. See, for example, U.S. Pat. No. 6,063,039.

According to one aspect, the present invention is directed to an arrangement for producing a sample of body fluid from a wound opening created in a skin surface at a sampling site, the arrangement comprising: at least one skin-penetration member having a first end configured to pierce the surface of the skin, and a inner lumen in communication with the first end; at least one actuator operatively associated with the at least one skin-penetration member; and at least one catalyst device configured to enhance perfusion of body fluid at the sampling site;

wherein the at least one actuator is configured to locate the at least one skin-penetration member so as to obstruct the wound opening while transporting body fluid through the inner lumen.

According to another aspect, the present invention is directed to a method of sampling body fluid from a wound opening created in a skin surface at a sampling site, the method comprising: automatically or manually initiating a testing sequence; applying a catalyst to the sampling site; actuating a skin-piercing member so as to drive the member into the surface of the skin thereby creating the wound opening; allowing the at least one skin-penetration member to obstruct the wound opening; and transporting body fluid through an inner lumen of the skin-penetration member; wherein the catalyst is applied to the sampling site at one or more of the following times: prior to actuating the skin-piercing member, during actuation of the skin-piercing member, or after actuating the skin-penetration member.

BRIEF DESCRIPTION OF THE DRAWING FIGURES

The following description of preferred embodiments can be read in connection with the accompanying drawings in which like numerals designate like elements and in which:

FIG. 1 is a partial perspective view of an arrangement constructed according to the present invention.

FIG. 2 is a partial cut away side view of the arrangement of FIG. 1.

FIG. 3 is a partial cut away side view of the arrangement of FIG. 1, with an activated catalyst.

FIG. 4 is a partial cut away magnified side view of the arrangement of FIG. 1, with an activated catalyst and illustrating a mechanism of body fluid collection and transport according to the present invention.

FIG. 5 is a perspective view of a portion of an arrangement, including an actuator, constructed according to the present invention.

FIG. 6 is a perspective view of an integrated device formed according to one embodiment of the present invention.

FIG. 7 is a partial side view of the integrated device of FIG. 6.

FIG. 8 is a perspective view of a component of the integrated device of FIG. 6.

FIG. 9 is a partial perspective view of various components of the integrated device of FIG. 6.

FIG. 10 is a side view illustrating various additional components of the device of FIG. 6.

FIG. 11 is a perspective view of an integrated device formed according to an alternative embodiment of the present invention.

DETAILED DESCRIPTION

According to a first aspect of the present invention, there are provided arrangements and techniques for reliably expressing body fluid from a digit or from an alternate site. For example, according to the present invention, arrangements and techniques are provided which consistently and reliably express an amount of body fluid that is sufficient to perform an analysis to quantify the amount of an analyte (e.g., glucose, bilirubin, alcohol, controlled substances, toxins, hormones, proteins, etc.) contained therein.

One embodiment of an arrangement 10 of the type described above is illustrated in FIGS. 1-4. As illustrated therein, the arrangement 10 may include a housing 12. The housing 12 may have any suitable shape or configuration, and is not limited to the shape and configuration illustrated. The housing 12 can be constructed of any suitable material. For example, the housing 12 may be constructed of a polymeric or metallic material.

The arrangement 10 may further include a catalyst to assist in the sample acquisition process by enhancing perfusion of blood or body fluid at a sampling site. At least one of several catalysts may be utilized or included in the arrangement of the present invention. Possible catalysts include, lancing velocity, heat, pressure, vacuum, vibration, and topical drugs (which induce vasodilatation and increases the blood or body fluid available at the lancing site). These catalysts may be applied before, during, after lancing, or in combination with some or all three to facilitate expression of sufficient quantity of body fluid for determination of the concentration of an analyte contained therein (e.g., glucose).

Lancing velocity refers to the speed at which the skin piercing member is driven. Velocities ranging from ˜0-22 m/s are possible. Both pain and blood production may increase as velocity increases. Attempts to balance pain and blood have led to a preferred range of about 3-20 m/s, 3-10 m/s, or 10-12 m/s.

Pressure is another possible catalyst. Footprint contact pressure can be varied by a number of possible techniques. One such technique is to vary the size of the opening of the footprint. Another form of pressure catalyst can take the form of a pressure-applying member that circumferentially surrounds and squeezes the digit or other body part from which a sample is to be acquired. One illustrative example of this form of catalyst is a pressure-applying cuff-like member of the type described in U.S. patent application Ser. No. 11/510,784, entitled BODY FLUID MONITORING AND SAMPLING DEVICES AND METHODS, the entire content of which is incorporated herein by reference. The above-described pressure catalyst can be utilized alone, or in combination with other catalysts such as vacuum pressure.

Heat is another optional catalyst. Increasing heat, thereby increasing the skin temperature at the wound site, increases blood production. Possible implementations of heat include IR lights, or resistive elements to heat the skin.

Another catalyst is vacuum pressure. According to certain embodiments, a light vacuum (e.g., 3-8 in. Hg) is applied to the wound site before, during, and/or after lancing. Several embodiments for applying vacuum to the wound site are contemplated. One embodiment uses a motor driven pump to apply vacuum. Alternative embodiments include using individually packaged vacuum chambers to apply vacuum, or using a rigid syringe like mechanism to apply vacuum. Other systems use motor driven pumps and syringes.

According to the principles of the present invention, one or more of the above-described catalysts can be used in combination with each other, either concurrently or sequentially.

In certain specific embodiments of the arrangement 10, a catalyst device 14 can be included which comprises a member or combination of members for applying pressure to a surface of the skin S disposed at a location which is proximate to an area from which a sample of body fluid is to be expressed (i.e., sampling site 28). The catalyst device 14 may cause the area of the skin from which the sample of body fluid is to be expressed to become perfused with blood and/or body fluid. This effect facilitates expression of body fluid from a wound opening 30. According to the illustrated embodiment, the catalyst device 14 comprises a member or combination of members, such as the illustrated pump 16 and related controller 18.

The arrangement 10 further comprises a footprint 20 which is attached to the housing 12. According to the illustrated embodiment, a digit D is placed on the footprint 20 at the sampling site. However, it should be understood that the footprint may also be applied to the surface of the skin at an alternate site. The footprint 20 has a central opening and may optionally have an annular in shape. However, the footprint is not limited to this shape or configuration. Numerous shapes or configurations may satisfy the function of providing a footprint around the site from which body fluid is to be expressed. The footprint can have an opening of any suitable diameter or major dimension 21. According to an illustrative example, the diameter or major dimension is at least about 3-8 mm. According to certain embodiments, the footprint 20 is constructed from a material which facilitates the formation of a seal between the digit D and the footprint 20. For example, suitable materials for this purpose include a relatively soft elastomeric material, such as a silicone rubber.

The arrangement 10 further includes at least one skin penetration member 22. The at least one skin penetration member 22 can take any suitable form. For example, the at least one skin penetration member can comprise a solid lancet or a hollow needle. Conventional arrangements often require separate mechanisms for drawing a sample of blood to the surface of the skin and for transporting the sample to a reaction chamber. The device of the present invention can use a skin-piercing element in the form of a hollow needle to both create and transport the sample, thereby greatly simplifying and improving the effectiveness of the arrangement 10. According to one optional embodiment, the skin-penetration member(s) 22 can be in the form of a so-called “microneedle.” As the name implies, microneedles are characterizable by their relatively small outer diameters. For example, a microneedle, as the term is utilized herein, may encompass a skin-penetration member having an outside diameter which is on the order of 40-200 μm. The inside diameter can vary, for example, having an inside diameter on the order of 25-160 μm. Needles are also characterizable in the art by reference to the “gage.” By way of illustration, and consistent with the above description, microneedles having a gage ranging from 26-36 are clearly comprehended by the present invention. Certain advantages may be gleaned from the use of such microneedles as the skin-penetration member. In particular, due to their small size, the size of the wound left upon entry into the skin is relatively small, thereby minimizing the pain associated with such needle insertions and allowing for a quicker healing process. However, the present invention is certainly not limited to the use of such microneedles. Thus, for example, according to one possible alternative embodiment, the skin penetration member(s) comprise hollow needles having a gage of about 20-25, or comprising hollow needles having an inner diameter of about 0.007 inches and an outer diameter of about 0.020 inches.

The at least one skin-penetration member 22 can be formed of any suitable material, such as metal, plastic, glass, etc. Optionally, the at least one skin penetration member can be mounted to a hub 24. In further alternative embodiments, the hub 24 may contain an assay pad 34 comprising a reagent that changes color upon reaction with a target analyte, as known per se to those skilled in the art. As illustrated, for example, in FIG. 2, the skin-penetration member 22 and hub 24 may be located within a chamber 25. The chamber 25 is in communication with pump 16 so that vacuum pressure can be applied within the chamber 25. The arrangement 10 can comprise a plurality of skin penetration members 22. According to certain embodiments, the plurality of skin penetration members 22 can be provided in the form of a replaceable cartridge. The at least one skin penetration member 22, and/or the hub 24 are attached to an actuation element 26. The actuation element 26 can take any suitable form. For example, the actuation element 26 may comprise a mechanical, electrical or pneumatic element. According to the illustrated embodiment, the actuation element 26 is in the form of a mechanical spring, more specifically, in the form of a torsional spring.

According to certain embodiments of the present invention, the catalyst device 14 operates in an automatic or semi-automatic manner. For example, a user may place the footprint 20 over a surface of the skin on a digit D, or at an alternate site. When the user is ready to produce a sample of body fluid, the button B is pressed. This can initiate a programmed sequence of events in the device including actuation of the catalyst device 14, thereby applying vacuum pressure to the skin an area proximate the tip region of digit D or alternate sampling site (FIG. 3) for a predetermined period of time. The skin-penetration member 22 can then be driven into the skin (FIG. 4). At a predetermined time, the catalyst device 14 is deactivated. This mode of operation can be characterized as “semi-automatic” in that sequence of events must be manually initiated by the user via pressing the button B.

According to one alternative, the mode of operation can be fully automatic. For example, the user places a tip region of digit D on the footprint 20, or places the footprint over an alternate site. The arrangement 10 can be provided with one or more sensors 27 that detect and verify that the footprint is properly located and ready for the sampling procedure to begin. Once this state has been sensed, the device automatically activates the catalyst 14 which is applied to the skin at the sampling site 28 (FIG. 3) for a predetermined period of time. Subsequently, the at least one skin penetration member 22 is driven into the skin (FIG. 4). At a subsequent predetermined time, the catalyst device 14 is deactivated. The catalyst device can be deactivated before, during or after the skin-piercing member is driven into the skin.

The arrangement 10 can form at least part of a device which functions only to sample body fluid. For example, the arrangement 10 can be used to express body fluid from the skin in the form of a drop of blood which pools on the surface of the skin of the user. This drop of blood can then be transferred to another separate device which then transports and/or analyzes the sample for a target analyte. Alternatively, the arrangement 10 may express a sample of body fluid from the skin, and then transport the sample to a location which can then be accessed for further analysis by a separate device. For instance, the sample body fluid can be transported to a reagent-containing pad 34, also contained within the arrangement 10. The sample then reacts with the reagent to produce a detectable spot or signal. The reagent pad can then be analyzed by a separate meter using photochemical, electrochemical, or other suitable techniques known per se to those skilled in the art. The reagent pad can remain within the arrangement 10 during the aforementioned analysis. According to an alternative embodiment, the reagent pad 34 can be analyzed by a detector 36 that forms part of the arrangement 10. Alternatively, the reagent pad can be removed from the arrangement 10 and inserted into a separate device, such as an electrochemical or photometric meter.

As illustrated, for example, in FIG. 4, according to this optional aspect of the present invention a skin-piercing member 22 in the form of a needle having a first end 22e configured to pierce the skin and an inner lumen 22l is driven into the skin to create a wound opening 30 therein for producing a sample of body fluid 32, preferably blood. The needle is not retracted right away, instead it is allowed to dwell and obstruct the opening 30 created in the surface of the skin. Blood or body fluid 32 is then extracted and flows through the inner lumen 22l of the needle, and is eventually transported to a site within the arrangement 10 for further analysis. The blood or body fluid 32 is drawn though the inner lumen by any suitable mechanism, such as capillary action, vacuum, or a combination of both. The needle 22 may be caused to dwell at the desired location via any of the mechanisms described herein. The skin-piercing member 22 is eventually retracted (see, e.g., FIG. 2). It has been surprisingly observed that an adequate sample volume can be extracted by the above-described arrangement/technique, especially when utilizing a vacuum catalyst. This arrangement and technique is advantageous in that a skin piercing member 22 may be used for wound creation and sample transport. Complex mechanisms and arrangements for repositioning a transport member or assay pad to a location that does not obstruct the opening can be avoided. Other advantages of obstructed opening sampling is realizing a reduction in the required sample volume, and improving the reliability of obtaining an adequate sample. When the needle is located so as to obstruct the wound opening, the end of the needle is closer to the source of body fluid, thus smaller drops of sample are more likely to reach the inner lumen of the needle and be successfully transported as the needle rests on or in the skin. By contrast, when the needle is withdrawn away from the surface of the skin, as in conventional arrangements and techniques, the droplet of blood or body fluid must be significantly larger/taller to reach the end of the needle and lumen, thereby elevating the risk that an insufficient sample is obtained.

As illustrated in FIG. 5, each individual skin-piercing element 22 is provided with its own actuation element or torsional spring 26. The torsional spring elements 26 may be provided to the user in a pre-cocked position. The acceleration path of the skin-piercing element or needle 22 may begin up to 180 degrees from the angle of impact with the skin S of the user. According to one beneficial aspect, the pivot point of the torsional spring elements can be provided as close as possible to the plane lying on the surface of the skin S in order to ensure that the skin piercing element 22 strikes the skin at an angle which is as close to 90 degrees as possible. The torsional spring element 26 can act as a guide for the skin-piercing element or needle 22 to that locates the tip 22e thereof so as to obstruct the wound opening 30 so as to draw the blood 32 into the lumen 22l of the needle. In this regard, the torsional spring element 26 may be designed such that its neutral position R_owill locate the needle so as to obstruct the wound opening 30 created by the skin piercing operation.

Another advantage of this optional aspect of the present invention is that the torsional spring elements 26 do not require a positive stop to limit the penetration depth of the skin-piercing element 22. It has been observed that elimination of a hard stop may provide certain beneficial effects. Namely, it has been observed that devices that include a hard stop experience a shock and resulting vibration and/or stirring action when the stop is impacted. It is theorized that this motion may increase the observable wound and/or the perceived pain associated with sampling. According to this embodiment, the depth of penetration of the skin-penetrating member 22 is determined by a number of factors, including the design of the sharp, the actuation force and the skin's resistance to penetration at the chosen sampling site. The lack of a positive stop has not been observed as increasing pain in clinical studies.

An exemplary body fluid sampling method or technique which may be used in conjunction with any of the above-described arrangements, but is not necessarily limited thereto, is described as follows.

A footprint is placed over a sampling site located on a digit or at an alternate site. The footprint has an opening therein which defines the sampling site. A sequence of events is then initiated. The events can be initiated manually, for example, by pressing a button or other triggering mechanism. Alternatively, the events can be automatically triggered, for example, through the use of sensors which determine when the footprint has been property positioned over a sampling site on the surface of the skin. A catalyst is then applied to the sampling site. The catalyst can comprise one or more of lancing velocity, heat, pressure, vacuum, vibration, topical drugs, or combinations thereof. These catalysts can be applied concurrently or sequentially relative to one another. According to one embodiment, a catalyst in the form of vacuum pressure is applied to the sampling site via a suitable mechanism, such as a pump capable of creating vacuum pressure. The catalyst can be applied for a set period of time, and then removed or terminated. For example, the catalyst can be removed before, during, or after penetration of the skin. Next, at least one skin penetration member is actuated or driven into the surface of the skin. The skin penetration member can take any suitable form, such as a solid lancet or hollow needle (e.g., a microneedle). According to one embodiment, at least one skin penetration member comprises a hollow needle having a first end configured to pierce the surface of the skin, and an inner lumen. The at least one skin penetration member can be actuated via any suitable mechanism, such as a mechanical spring. According to one optional embodiment, the actuating mechanism comprises a torsional spring. The at least skin penetration member is caused to dwell at or below the surface of the skin in the vicinity of the wound opening in order to obstruct the same. The skin penetration member can be caused to dwell at this location via any suitable mechanism. According to one embodiment, the actuator is provided in the form of a torsional spring having a resting position which can be utilized to cause the first end of the at least one skin penetration member to obstruct the wound opening subsequent to piercing the surface of the skin. During the period of time in which the at least one skin penetration member is caused to dwell at the wound opening, body fluid is transported away from the wound site via a suitable mechanism. According to one embodiment, the body fluid, or blood, is transported via the inner lumen of a hollow skin-penetration member via capillary action, vacuum, or a combination of both. According to one optional embodiment of the present invention, a mechanism can be provided which estimates the acquired sample volume, and compares this measured sample volume with a target sample volume. The information acquired by this analysis can be used to control the catalyst such that it is automatically removed once the target sample volume has been acquired. Any suitable mechanism can be utilized to analyze the acquired sample volume. For example, the body fluid can be transported to an assay pad which contains a chemical reagent impregnated therein. Upon exposure to the body fluid, a target analyte contained therein causes a chemical reaction producing a color change in the assay pad. This color change can in turn be detected by a suitable detection element. One such detection element utilizes colorimetric optical analysis of the assay pad. More specifically, an array of such detection elements can be provided along a longitudinal length of the assay pad. The number of detection elements contained along the length of the assay pad that detect the presence of the sample can be correlated to the acquired sample volume. For example, the further the sample volume travels along the length of the assay pad the greater the acquired sample volume. Once it has been determined that a target sample volume has been acquired, the catalyst can then be terminated. This can be accomplished by the use of a controller in signal communication with a pump. The controller operates based on signals derived from the analysis of the sample volume in the manner described above. Some advantages of monitoring volume to actively control the application of the catalyst include reduction in expression of excess blood or body fluid thereby reducing mess, preventing damage to skin (bruising, etc) due to prolonged catalyst application, and reduction in power consumption.

According to a further optional aspect of the present invention, the above-described arrangements and methods can form at least part of an integrated device or integrated meter. As previously noted, as used herein, the term “integrated device” or “integrated meter” means a device or meter that includes all components necessary to perform sampling of the body fluid, transport of the body fluid, quantification of an analyte, and display of the amount of analyte contained in the sample of body fluid. Thus, according to the principles of the present invention, an integrated device or meter can comprise one or more, or any combination, of the features previously described herein. According to further aspects of the present invention, and integrated meter or device can comprise components and/or features in addition to those specifically described herein.

An exemplary integrated meter is illustrated in detail in FIGS. 6-10. As illustrated therein, the integrated meter 100 generally comprises a housing 112 and a catalyst device 114 (e.g., FIG. 10). The catalyst device 114 may take any suitable form and can comprise any of the previously described alternative catalyst devices. The integrated meter 100 may further comprise a footprint 120 of the type previously described. A door 123 can be provided on the housing 112. The door 123 is connected via a hinge 125 to the housing 112. As described in further detail below, the door 123 can be opened to reveal a cartridge 131 containing a plurality of skin-piercing elements 122. In the illustrated embodiment, the integrated meter 100 further includes a display 127 for communicating the results of the analysis on the sample body fluid for the presence and/or concentration of an analyte contained therein. The integrated meter 100 may further include one or more buttons 129 which can be pressed by the user to engage various functions and interfaces of the integrated meter 100.

FIG. 7 is an illustration of the integrated meter 100 with the door 123 opened to reveal further details of the interior components of the exemplary integrated meter 100. As illustrated therein, the housing 112 contains a cartridge 131 therein. In the illustrated embodiment, the cartridge 131 is circular and contains a plurality of skin-piercing elements as further described herein. The cartridge 131 is mounted about a hub 133 and is rotatable. Thus, upon sampling a skin-piercing element 22 is driven through an opening in the housing in registry with the footprint 120 and pierces the skin of the user. Once the test has been completed, the cartridge 131 can be rotated such that an unused skin-piercing element now comes into registry with the opening in the housing and the corresponding opening in the footprint 120 in preparation for the next sampling event. It should be understood that the present invention is not limited to the illustrated circular cartridge having the particular configuration depicted in the drawing figures. To the contrary, a number of alternative cartridge configurations are possible, such as a slidable linear or polygonal configuration (not shown). Also illustrated in FIG. 7 is the presence of a light source 139 disposed on the back of the door 123. The light source 139 can take any suitable form, such as a light emitting diode. It should be understood that alternative light sources may also be utilized. The function of the light source 139 will be described in further detail below.

Further details of the optical assembly 135, the light source 139, and the replaceable cartridge 131 are illustrated in FIGS. 8-9. As illustrated therein, the replaceable cartridge 131 generally may comprise a plurality of compartments defining a plurality of body fluid sampling and analysis sites 132. Contained in each sampling and analysis site 132 is a skin penetration member 122. Each skin penetration member 122 can take any suitable form. According to the illustrated embodiment, each skin penetration member 122 is in the form of a hollow needle. It should be understood that alternative skin penetration members may also be utilized consistent with the principles of the present invention (e.g., solid lancets, etc.) each skin-penetration member can be attached to a needle hub 124. Each needle hub 124 is, in turn, attached to an actuation element 126. It should be understood that a number of different actuation elements may be utilized according to the principles of the present invention. The actuation elements can be mechanical, electrical, pneumatic, etc. According to the illustrated embodiment, the actuation element 126 is in the form of a torsional spring and may have those features and characteristics previously described herein. Upon activation, the torsional spring drives the needle hub 124 and the attached skin penetration member 122 into the skin of the user disposed on the footprint 120. According to certain embodiments, each sampling/analysis site 132 further contains a signaling mechanism which produces a detectable signal when contacted with a target analyte contained in a sample of body fluid expressed from the skin. A number of suitable mechanisms are envisioned. The mechanisms may be based on technologies such as photometric or electrochemical analysis. According to the illustrated embodiment, each needle hub 124 contains a reagent pad 129 which generally comprises an absorbent material containing a chemical reagent which, upon reaction with a target analyte, produces a chemical reaction that results in a detectable signal. The reagent pad 129 is in fluid communication with the inner lumen of the skin piercing element 122. As noted above, the signal can be detected optically, electrochemically, or by other suitable means. According to one embodiment, the reagent pad 129, upon reaction with the target analyte, produces a spot which is optically detected by the optical assembly 135 in a manner generally known to those skilled in the art. The spot produced by the above-mentioned reaction can be observed optically through a window 143 formed along the interior region of the illustrated cartridge 131 by the optical assembly 135. In this regard, light emitted from the light source 139 is incident upon the reagent pad 129, and reflects off the surface thereof. Upon formation of a reaction spot on the surface of the reagent pad 129, the amount of light reflected off the reaction spot differs from the light reflected off of other portions of the reagent pad 129 containing no such reaction spot. This reflected light is picked up by the optical assembly, first through the lens 137 (FIG. 7), and eventually is incident upon an optical detector element 142 (FIG. 9).

The optical detector element 142 generally comprises one or more detector elements. According to one alternative construction, the detector element 142 comprises a plurality of detector elements formed in an array. The array can take any suitable configuration, and can be a linear array or an area array according to one nonlimiting example. The detector elements can comprise any suitable construction. For example, the detector elements 142 can comprise a photo diode, CCD, or CMOS based detector element. The signals transmitted to the detector element 142 are passed on to suitable electronics contained within the housing 112 (see, e.g., FIG. 10) via suitable electrical connectors, such as flexible ribbons 141. The specifics of the electronics and signal interpretation being familiar to those of ordinary skill in the art. While not necessary to enable practice of the presently claimed invention, further details concerning the structure, function, and arrangement of the optical assembly 135, and the components contained therein, can be gleaned from the disclosure contained in U.S. Patent Application Publication No. 2006/0281187, entitled ANALYTE DETECTION DEVICES AND METHODS WITH HEMATOCRIT/VOLUME CORRECTION AND FEEDBACK CONTROL, the entire content of which is incorporated herein by reference.

Additional components of an integrated meter 100 are illustrated in FIG. 10. The view depicted in FIG. 10 is that of an integrated meter 100 with the back panel removed to reveal the above-referenced additional components. For example, as illustrated in FIG. 10, the integrated meter 100 may further include a plurality of rollers 147 which cooperate with the cartridge 131 and a motor drive 149 thereby enabling the rotation of the cartridge 131 about the hub 133, and indexing of the analysis sites 132 with the footprint 120. The integrated meter 100 may also include a catalyst device 114 comprising a pressure pump 151 which, according to certain embodiments, comprises a pump capable of producing at least a negative or vacuum pressure at the surface of the skin located over the footprint 120. The integrated meter 100 may further include appropriate electronics, as embodied in the circuit board 153 of the illustrated embodiment. Preferably, the circuit board contains conventional electronic components capable of controlling the various functions of the integrated meter 100 in the desired manner, including the pump 151. The particulars of the circuit board 153 and electronic components disposed thereon, being well-known to those of ordinary skill in the art. The integrated meter 100 may further comprise a suitable power supply 155, such as the illustrated batteries.

As evident from FIGS. 6-10, the integrated meter 100 is configured for handheld use. However, the invention is not limited to handheld devices. For example, the present invention is also directed to integrated meters that are wearable. An example of such a wearable device is illustrated in FIG. 11. The wearable integrated device 200 illustrated therein can be generally composed of a functional portion 202 and a body-attachment portion 204. The functional portion can comprise an arrangement 10 of the type described herein. The functional portion can also have one or more of the features and elements of the handheld integrated meter described above.

According to further aspects of the present invention, modified devices and techniques are provided which permit both digital body fluid sampling and analysis as well as alternate-site body fluid sampling and analysis, which may be performed at the election of the user. In the description that follows, it should be understood that the integrated meters described herein may have any of the features and/or modes of operation than that of the previously described embodiments. For example, the integrated meter that incorporate arrangements of the present invention can include features that facilitate use on digits as well as alternate sites, at the election of the user. Such features are described in U.S. patent application Ser. No. 11/510,784, entitled BODY FLUID MONITORING AND SAMPLING DEVICES AND METHODS, the entire content of which is incorporated herein by reference.

An exemplary body fluid sampling and analysis methodology or technique, which may be utilized in conjunction with any of the above-mentioned catalyst devices or integrated meters, but is not necessarily limited thereto, is described as follows.

A user loads a fresh disposable cartridge containing a plurality of skin penetration members and analysis sites into an integrated meter. The integrated meter then reads calibration data contained in or on the cartridge. This data can be read in any suitable manner. For example, a bar code may be placed on the cartridge which can be optically read by the optical assembly contained within the meter. The integrated meter then selects the proper lookup table or algorithm to calculate an aggregate glucose measurement taking into consideration the calibration data. The meter may then place itself in a ready mode waiting for a trigger to initiate sampling and testing. The user then either manually presses a button or trigger to initiate sampling and analysis, or the device verifies that it is properly positioned on the skin of the user and ready to begin the sampling and analysis procedure. Suitable sensors to accomplish this include optical, capacitive or pressure sensors. The device then initiates a catalyst which acts to facilitate the expression of body fluid. Alternatively, the catalyst is vacuum pressure which generates suction at the sampling site. Optional sensors present in the meter may be used to monitor and control the positive or negative pressure of the catalyst. After achieving a target pressure for a desired period of time, the skin penetration member (e.g., a hollow needle) is actuated and driven into the skin of the user to create a wound site. The skin penetration member comes to rest in or directly on the wound opening created at the sampling site where it obstructs the wound opening and is in the desired position for collecting a sample of body fluid expressed from the wound. The integrated meter may further include a mechanism for detecting a whether a sufficient amount of sample has been expressed. Details of such suitable detection techniques are described in detail in U.S. Pat. No. 7,052,652, entitled ANALYTE CONCENTRATION DETECTION DEVICES AND METHODS, the entire content of which is incorporated herein by reference. Once the desired amount of body fluid has been obtained, the catalyst is deactivated. A sample of body fluid is in fluid communication with a device or mechanism which creates a detectable signal upon reaction within analyte present in the sample body fluid. For example, one such suitable mechanism is an absorbent pad containing a chemical reagent which, upon reaction with the analyte produces a reaction spot which can be optically detected. An optical assembly which is in optical communication with the above described signal generating mechanism is utilized to detect the signal created via reaction with the analyte and communicate the signals to supporting electronics contained within the meter. The concentration of a target analyte (e.g., glucose) can then be calculated using these signals as a basis. Additional factors may be considered during these calculations, such as the sample size, levels of other substances contained in the sample (e.g. hematocrit), etc. Such optional calculation techniques are described in further detail in U.S. Patent Application Publication No. 2006/0281187, entitled ANALYTE DETECTION DEVICES AND METHODS WITH HEMATOCRIT/VOLUME CORRECTION AND FEEDBACK CONTROL, the entire content of which is incorporated herein by reference. These calculations quantify the amount of analyte contained in the sample body fluid. This quantity is displayed on a suitable display contained within the meter which can be easily read by the user. The integrated meter then automatically may retract the skin-penetration member and indexes the disposable cartridge to present a fresh unused skin penetration member which will be utilized to perform the next sampling and analysis event.

EXAMPLE

A prototype was constructed using a torsional Spring actuator and a needle designed to position the needle on or in the wound (i.e., to obstruct the wound opening). A vacuum catalyst was also utilized. Results of an evaluation of this prototype are summarized in the following table.

Population
Camino Medical
Camino Medical

Experiment Name
PAMF1
PAMF2

Actuator
Beam
Torsional

Actuator Version
2.1
5.0 (w/dwell)

# of Subjects
21
19

Probability BV >250 nl
94%
93%

Probability BV >300 nl
90%
91%

Probability BV >350 nl
85%
85%

Average BV (nl)
985
1137

The table shows two experiments for which the lancet design, footprint design and footprint contact force were identical. Experiment PAMF1 used a cantilevered beam actuator; this actuator did not allow the needle to remain in or on the wound. Experiment PAMF2 used a torsional coil actuator, this actuator caused the needle to dwell the needle in or on the skin. Surprisingly, the performance of the torsional coil was comparable in blood volume (BV) probabilities to the cantilevered beam. Even more surprising was the observation that the torsional coil actually produced a slightly higher average blood volume.

Numbers expressing quantities of ingredients, constituents, reaction conditions, and so forth used in this specification are to be understood as being modified in all instances by the term “about”. Notwithstanding that the numerical ranges and parameters setting forth, the broad scope of the subject matter presented herein are approximations, the numerical values set forth are indicated as precisely as possible. Any numerical value, however, inherently contains certain errors necessarily resulting from the standard deviation found in their respective measurement techniques. None of the elements recited in the appended claims should be interpreted as invoking 35 U.S.C. §112, ¶6, unless the term “means” is explicitly used.

Although the present invention has been described in connection with preferred embodiments thereof, it will be appreciated by those skilled in the art that additions, deletions, modifications, and substitutions not specifically described may be made without departing from the spirit and scope of the invention as defined in the appended claims.

Claims

1. An arrangement for producing a sample of body fluid from a wound opening created in a skin surface at a sampling site, the arrangement comprising: a cartridge comprising a plurality of compartments and a plurality of sampling sites, wherein each of the sampling sites comprises: a skin-penetration member having a first end configured to pierce the surface of the skin, and an inner lumen in communication with the first end;a spring actuator operatively associated with the skin-penetration member; anda needle hub connecting the skin-penetration member and the spring actuator, wherein the needle hub comprises a reagent pad and wherein the spring actuator is configured to drive the skin-penetration member to form the wound opening,wherein each of the compartments at least partially encloses the skin-penetration member, spring actuator, and needle hub of a respective sampling site of the plurality of sampling sites.
2. The arrangement of claim 1, wherein the spring actuator drives the skin penetration member in an arcuate path.
3. The arrangement of claim 1, further comprising at least one catalyst device comprising a means for applying vacuum pressure, positive pressure, or heat to the sampling site.
4. The arrangement of claim 3, wherein the catalyst device comprises a pump, and wherein the pump is configured and arranged to apply a vacuum to the sampling site.
5. The arrangement of claim 4, further comprising a controller operatively associated with the pump.
6. The arrangement of claim 1, further comprising a housing, and wherein a footprint is disposed on the housing to be applied to the sampling site on the skin of a user.
7. The arrangement of claim 6, wherein the footprint has an opening, and wherein the opening has a diameter of 3-8 mm.
8. The arrangement of claim 6, wherein the footprint comprises an elastomeric seal.
9. The arrangement of claim 1, wherein the skin-penetration member comprises a microneedle.
10. An arrangement for producing a sample of body fluid from a wound opening created in a skin surface at a sampling site, the arrangement comprising: a cartridge comprising a plurality of compartments and a plurality of sampling sites, wherein each of the sampling sites comprises: a skin-penetration member having a first end configured to pierce the surface of the skin;a spring actuator operatively associated with the skin-penetration member; anda needle hub connecting the skin-penetration member and the spring actuator, wherein the needle hub comprises a reagent pad and wherein the spring actuator is configured to drive the skin-penetration member to form the wound opening; anda detector assembly in communication with the reagent pad of a sampling site,wherein each of the compartments at least partially encloses the skin-penetration member, spring actuator, and needle hub of a respective sampling site of the plurality of sampling sites.
11. The arrangement of claim 10, wherein the spring actuator drives the skin penetration member in an arcuate path.
12. The arrangement of claim 10, further comprising at least one catalyst device comprising a means for applying vacuum pressure, positive pressure, or heat to the sampling site.
13. The arrangement of claim 12, wherein the catalyst device comprises a pump, and wherein the pump is configured to apply a vacuum to the sampling site.
14. The arrangement of claim 13, further comprising a controller operatively associated with the pump.
15. The arrangement of claim 10, further comprising a housing, and wherein a footprint is disposed on the housing to be applied to the sampling site on the skin of a user.
16. The arrangement of claim 15, wherein the footprint has an opening, and wherein the opening has a diameter of 3-8 mm.
17. The arrangement of claim 15, wherein the footprint comprises an elastomeric seal.
18. The arrangement of claim 10, wherein the detector assembly comprises at least one CMOS-based detector element.
19. The arrangement of claim 18, wherein the detector assembly comprises a linear or area array of CMOS-based detector elements.
20. The arrangement of claim 10, wherein the skin-penetration member comprises a microneedle.
21. An arrangement for producing a sample of body fluid from a wound opening created in a skin surface at a sampling site, the arrangement comprising: a cartridge comprising a plurality of compartments and a plurality of sampling sites, wherein each of the sampling sites comprises: a skin-penetration member having a first end configured to pierce the surface of the skin;a spring actuator operatively associated with the skin-penetration member; anda needle hub connecting the skin-penetration member and the spring actuator, wherein the needle hub comprises a reagent pad and wherein the spring actuator is configured to drive the skin-penetration member to form the wound opening,wherein each of the compartments at least partially encloses the skin-penetration member, spring actuator, and needle hub of a respective sampling site of the plurality of sampling sites.
22. The arrangement of claim 21, wherein the spring actuator drives the skin penetration member in an arcuate path.
23. The arrangement of claim 21, further comprising at least one catalyst device comprising a means for applying vacuum pressure, positive pressure, or heat to the sampling site.
24. The arrangement of claim 23, wherein the catalyst device comprises a pump, and wherein the pump is configured and arranged to apply a vacuum to the sampling site.
25. The arrangement of claim 24, further comprising a controller operatively associated with the pump.
26. The arrangement of claim 21, further comprising a housing, and wherein a footprint is disposed on the housing to be applied to the sampling site on the skin of a user.
27. The arrangement of claim 26, wherein the footprint has an opening, and wherein the opening has a diameter or major dimension of 3-8 mm.
28. The arrangement of claim 26, wherein the footprint comprises an elastomeric seal.
29. The arrangement of claim 21, wherein the skin-penetration member comprises a microneedle.

CROSS-REFERENCE TO RELATED APPLICATIONS

The present application is a Continuation of and claims priority to U.S. patent application Ser. No. 14/446,262, filed Jul. 29, 2014, which issued as U.S. Pat. No. 9,060,723 on Jun. 23, 2015, which is a Continuation of and claims priority to U.S. patent application Ser. No. 13/752,261, filed Jan. 28, 2013, which issued as U.S. Pat. No. 8,795,201 on Aug. 5, 2014, which is a Continuation of and claims priority to U.S. patent application Ser. No. 13/197,592, filed Aug. 3, 2011, which issued as U.S. Pat. No. 8,360,993 on Jan. 29, 2013, which is a Continuation of, and claims priority pursuant to 35 U.S.C. §120 to, U.S. patent application Ser. No. 11/941,403, filed Nov. 16, 2007, which issued as U.S. Pat. No. 8,012,104 on Sep. 6, 2011, which is a Divisional of, and claims priority under 35 U.S.C. §120 to, U.S. patent application Ser. No. 11/529,613, filed Sep. 29, 2006, which issued as U.S. Pat. No. 8,012,103 on Sep. 6, 2011, which claims priority pursuant to 35 U.S.C. §119 to U.S. Patent Application No. 60/721,966 filed Sep. 30, 2005. The entire contents of each of these applications are hereby incorporated by reference in this application.

US Referenced Citations (585)

Number	Name	Date	Kind
842690	Oswalt	Jan 1907	A
D137874	Partridge	May 1944	S
2749797	Harks	Mar 1950	A
3092465	Adams, Jr.	Jun 1963	A
3310002	Wilburn	Mar 1967	A
3620209	Kravitz	Nov 1971	A
3623475	Sanz et al.	Nov 1971	A
3626929	Sanz et al.	Dec 1971	A
3630957	Rey	Dec 1971	A
D223165	Komendat	Mar 1972	S
3723064	Liotta	Mar 1973	A
3741197	Sanz et al.	Jun 1973	A
3961898	Neeley et al.	Jun 1976	A
3992158	Przybylowicz et al.	Nov 1976	A
4014328	Cluff et al.	Mar 1977	A
4042335	Clement	Aug 1977	A
4057394	Genshaw	Nov 1977	A
4109655	Chacornac	Aug 1978	A
4253083	Imamura	Feb 1981	A
4254083	Columbus	Mar 1981	A
4258001	Pierce et al.	Mar 1981	A
4260257	Neeley et al.	Apr 1981	A
4289459	Neeley et al.	Sep 1981	A
4321397	Nix et al.	Mar 1982	A
4350762	DeLuca et al.	Sep 1982	A
4394512	Batz	Jul 1983	A
4414975	Ryder et al.	Nov 1983	A
4416279	Lindner et al.	Nov 1983	A
4418037	Katsuyama et al.	Nov 1983	A
4422941	Vaughan, Jr. et al.	Dec 1983	A
4429700	Thees et al.	Feb 1984	A
4627445	Garcia et al.	Dec 1986	A
4637403	Garcia et al.	Jan 1987	A
4637406	Guinn et al.	Jan 1987	A
4653513	Dombrowski	Mar 1987	A
4661319	Lape	Apr 1987	A
4702261	Cornell et al.	Oct 1987	A
4711250	Gilbaugh, Jr. et al.	Dec 1987	A
4737458	Batz et al.	Apr 1988	A
4767415	Duffy	Aug 1988	A
4774192	Terminiello et al.	Sep 1988	A
4787398	Garcia et al.	Nov 1988	A
4790979	Terminiello et al.	Dec 1988	A
4794926	Munsch et al.	Jan 1989	A
4815843	Tiefenthaler et al.	Mar 1989	A
4829470	Wang	May 1989	A
4844095	Chiodo et al.	Jul 1989	A
4846785	Cassou et al.	Jul 1989	A
4887306	Hwang et al.	Dec 1989	A
4920977	Haynes	May 1990	A
4929426	Bodai et al.	May 1990	A
4930525	Palestrant	Jun 1990	A
4935346	Phillips	Jun 1990	A
4953552	De Marzo	Sep 1990	A
4966646	Zdeblick	Oct 1990	A
4983178	Schnell	Jan 1991	A
4995402	Smith	Feb 1991	A
5029583	Meserol	Jul 1991	A
5035704	Lambert et al.	Jul 1991	A
5049487	Phillips et al.	Sep 1991	A
5050617	Columbus et al.	Sep 1991	A
5059394	Phillips et al.	Oct 1991	A
5077199	Basagni et al.	Dec 1991	A
5094943	Siedel et al.	Mar 1992	A
5110724	Hewett	May 1992	A
5114350	Hewett	May 1992	A
5116759	Klainer et al.	May 1992	A
5131404	Neeley et al.	Jul 1992	A
5141868	Shanks et al.	Aug 1992	A
5145565	Kater et al.	Sep 1992	A
5146437	Boucheron	Sep 1992	A
5153416	Neeley	Oct 1992	A
5164575	Neeley et al.	Nov 1992	A
5166498	Neeley	Nov 1992	A
5174291	Schoonen et al.	Dec 1992	A
5176632	Bernardi	Jan 1993	A
5179005	Phillips et al.	Jan 1993	A
5183741	Arai et al.	Feb 1993	A
5196302	Kidwell	Mar 1993	A
5208163	Charlton et al.	May 1993	A
5213966	Vuorinen et al.	May 1993	A
5217480	Habar et al.	Jun 1993	A
5218966	Yamasawa	Jun 1993	A
5223219	Subramanian et al.	Jun 1993	A
5228972	Osaka et al.	Jul 1993	A
5234818	Zimmermann et al.	Aug 1993	A
5241969	Carson et al.	Sep 1993	A
5251126	Kahn et al.	Oct 1993	A
D341848	Bigelow et al.	Nov 1993	S
5269800	Davis, Jr.	Dec 1993	A
5275159	Griebel	Jan 1994	A
5278079	Gubinski et al.	Jan 1994	A
5288646	Lundsgaard et al.	Feb 1994	A
5299571	Mastrototaro	Apr 1994	A
5301686	Newman	Apr 1994	A
5302513	Miike et al.	Apr 1994	A
5304468	Phillips et al.	Apr 1994	A
5306623	Kiser et al.	Apr 1994	A
5308767	Terashima	May 1994	A
5314441	Cusack et al.	May 1994	A
5320607	Ishibashi	Jun 1994	A
5354537	Moreno	Oct 1994	A
5360595	Bell et al.	Nov 1994	A
5368047	Suzuki et al.	Nov 1994	A
5383512	Jarvis	Jan 1995	A
5390671	Lord et al.	Feb 1995	A
5395388	Schraga	Mar 1995	A
5399316	Yamada	Mar 1995	A
5401110	Neeley	Mar 1995	A
5402798	Swierczek et al.	Apr 1995	A
5426032	Phillips et al.	Jun 1995	A
5441513	Roth	Aug 1995	A
5451350	Macho et al.	Sep 1995	A
5458140	Eppstein et al.	Oct 1995	A
5460777	Kitajima et al.	Oct 1995	A
5460968	Yoshida et al.	Oct 1995	A
5482473	Lord et al.	Jan 1996	A
5506200	Hirschkoff et al.	Apr 1996	A
5507288	Böcker et al.	Apr 1996	A
5508200	Tiffany et al.	Apr 1996	A
5510266	Bonner et al.	Apr 1996	A
5514152	Smith	May 1996	A
5525518	Lundsgaard et al.	Jun 1996	A
5527892	Borsotti et al.	Jun 1996	A
5563042	Phillips et al.	Oct 1996	A
5568806	Cheney, II et al.	Oct 1996	A
5569287	Tezuka et al.	Oct 1996	A
5575403	Charlton et al.	Nov 1996	A
5577499	Teves	Nov 1996	A
5582184	Erickson et al.	Dec 1996	A
5586553	Halili et al.	Dec 1996	A
5591139	Lin et al.	Jan 1997	A
5593838	Zanzucchi et al.	Jan 1997	A
5611809	Marshall et al.	Mar 1997	A
5624458	Lipscher	Apr 1997	A
5630986	Charlton et al.	May 1997	A
5632410	Moulton et al.	May 1997	A
5636632	Bommannan et al.	Jun 1997	A
5647851	Pokras	Jul 1997	A
5658515	Lee et al.	Aug 1997	A
5660791	Brenneman et al.	Aug 1997	A
5670031	Hintsche et al.	Sep 1997	A
5676850	Reed et al.	Oct 1997	A
5680858	Hansen et al.	Oct 1997	A
5681484	Zanzucchi et al.	Oct 1997	A
5682233	Brinda	Oct 1997	A
5697901	Eriksson	Dec 1997	A
5700695	Yassinzadeh et al.	Dec 1997	A
5701181	Boiarski et al.	Dec 1997	A
5701910	Powles et al.	Dec 1997	A
D389761	Thomas	Jan 1998	S
5705018	Hartley	Jan 1998	A
5708247	McAleer	Jan 1998	A
5708787	Nakano et al.	Jan 1998	A
5715417	Gardien et al.	Feb 1998	A
5730753	Morita	Mar 1998	A
5735273	Kurnik et al.	Apr 1998	A
5736103	Pugh	Apr 1998	A
5741211	Renirie et al.	Apr 1998	A
5746217	Erickson et al.	May 1998	A
5746720	Stouder, Jr.	May 1998	A
5757666	Schreiber et al.	May 1998	A
5759364	Charlton et al.	Jun 1998	A
5766066	Ranniger	Jun 1998	A
5771890	Tamada	Jun 1998	A
5797693	Jaeger	Aug 1998	A
5800420	Gross et al.	Sep 1998	A
5801057	Smart et al.	Sep 1998	A
5807375	Gross et al.	Sep 1998	A
5820570	Erickson et al.	Oct 1998	A
5827183	Kurnik et al.	Oct 1998	A
5840020	Heinonen et al.	Nov 1998	A
5841126	Fossum et al.	Nov 1998	A
5843692	Phillips et al.	Dec 1998	A
5846837	Thym et al.	Dec 1998	A
5851215	Mawhirt et al.	Dec 1998	A
5854074	Charlton et al.	Dec 1998	A
D403975	Douglas et al.	Jan 1999	S
5855801	Lin et al.	Jan 1999	A
5856195	Charlton et al.	Jan 1999	A
5858194	Bell	Jan 1999	A
5866281	Guckel et al.	Feb 1999	A
5871494	Simons et al.	Feb 1999	A
5879310	Sopp et al.	Mar 1999	A
5879326	Godshall et al.	Mar 1999	A
5879367	Latterell et al.	Mar 1999	A
5885839	Lingane et al.	Mar 1999	A
5891053	Sesekura	Apr 1999	A
5893870	Talen et al.	Apr 1999	A
D411621	Eisenbarth et al.	Jun 1999	S
5911711	Pelkey	Jun 1999	A
5911737	Lee et al.	Jun 1999	A
5912139	Iwata et al.	Jun 1999	A
5925021	Castellano et al.	Jul 1999	A
5928207	Pisano et al.	Jul 1999	A
5930873	Wyser	Aug 1999	A
5938679	Freeman et al.	Aug 1999	A
5945678	Yanagisawa	Aug 1999	A
5951492	Douglas et al.	Sep 1999	A
5951493	Douglas et al.	Sep 1999	A
5951521	Mastrototaro et al.	Sep 1999	A
5954685	Tierney	Sep 1999	A
5962215	Douglas et al.	Oct 1999	A
5968760	Phillips et al.	Oct 1999	A
5968765	Grage et al.	Oct 1999	A
5968836	Matzinger et al.	Oct 1999	A
5971941	Simons et al.	Oct 1999	A
5972294	Smith et al.	Oct 1999	A
5986754	Harding	Nov 1999	A
5989409	Kurnik et al.	Nov 1999	A
5993189	Mueller et al.	Nov 1999	A
D417504	Love et al.	Dec 1999	S
6001067	Shults et al.	Dec 1999	A
6005545	Nishida et al.	Dec 1999	A
6010463	Lauks et al.	Jan 2000	A
6010519	Mawhirt et al.	Jan 2000	A
6014135	Fernandes	Jan 2000	A
6014577	Henning et al.	Jan 2000	A
6023629	Tamada	Feb 2000	A
6027459	Shain et al.	Feb 2000	A
6030827	Davis et al.	Feb 2000	A
6032059	Henning et al.	Feb 2000	A
6036924	Simons et al.	Mar 2000	A
6041253	Kost et al.	Mar 2000	A
6045753	Loewy et al.	Apr 2000	A
6048352	Douglas et al.	Apr 2000	A
6050988	Zuck	Apr 2000	A
6056701	Duchon et al.	May 2000	A
6056734	Jacobsen et al.	May 2000	A
6058321	Swayze et al.	May 2000	A
6059815	Lee et al.	May 2000	A
6061128	Zweig et al.	May 2000	A
6063039	Cunningham et al.	May 2000	A
6071251	Cunningham et al.	Jun 2000	A
6071294	Simons et al.	Jun 2000	A
6077660	Wong et al.	Jun 2000	A
6080116	Erickson et al.	Jun 2000	A
6083196	Trautman et al.	Jul 2000	A
6086544	Hibner et al.	Jul 2000	A
6090790	Eriksson	Jul 2000	A
6091975	Daddona et al.	Jul 2000	A
6093156	Cunningham et al.	Jul 2000	A
6097831	Wieck et al.	Aug 2000	A
6099484	Douglas et al.	Aug 2000	A
6100107	Lei et al.	Aug 2000	A
6102933	Lee et al.	Aug 2000	A
6103033	Say et al.	Aug 2000	A
6103197	Werner	Aug 2000	A
6106751	Talbot et al.	Aug 2000	A
6118126	Zanzucchi	Sep 2000	A
6120676	Heller et al.	Sep 2000	A
6123861	Santini, Jr. et al.	Sep 2000	A
6126899	Woudenberg et al.	Oct 2000	A
6132449	Lum et al.	Oct 2000	A
6139562	Mauze et al.	Oct 2000	A
6142939	Eppstein et al.	Nov 2000	A
6152942	Brenneman et al.	Nov 2000	A
6162639	Douglas	Dec 2000	A
6172743	Kley et al.	Jan 2001	B1
6175752	Say et al.	Jan 2001	B1
6176865	Mauze et al.	Jan 2001	B1
6183434	Eppstein et al.	Feb 2001	B1
6183489	Douglas et al.	Feb 2001	B1
6187210	Lebouiz et al.	Feb 2001	B1
6192891	Gravel et al.	Feb 2001	B1
6193873	Ohara et al.	Feb 2001	B1
6200296	Dibiasi et al.	Mar 2001	B1
6206841	Cunningham et al.	Mar 2001	B1
6214626	Meller et al.	Apr 2001	B1
6219574	Cormier et al.	Apr 2001	B1
6228100	Schraga	May 2001	B1
6230051	Cormier et al.	May 2001	B1
6231531	Lum et al.	May 2001	B1
6241862	McAleer et al.	Jun 2001	B1
6242207	Douglas et al.	Jun 2001	B1
6245215	Douglas et al.	Jun 2001	B1
6251083	Yum et al.	Jun 2001	B1
6251260	Heller et al.	Jun 2001	B1
6254586	Mann et al.	Jul 2001	B1
6255061	Mori et al.	Jul 2001	B1
6256533	Yuzhakov et al.	Jul 2001	B1
6268162	Phillips et al.	Jul 2001	B1
6271045	Douglas et al.	Aug 2001	B1
6272364	Kurnik	Aug 2001	B1
6283926	Cunningham et al.	Sep 2001	B1
6289230	Chaiken et al.	Sep 2001	B1
6298254	Tamada	Oct 2001	B2
6299578	Kurnik et al.	Oct 2001	B1
6306104	Cunningham et al.	Oct 2001	B1
6309351	Kurnik et al.	Oct 2001	B1
D450711	Istvan et al.	Nov 2001	S
6312612	Sherman et al.	Nov 2001	B1
6312888	Wong et al.	Nov 2001	B1
6315738	Nishikawa et al.	Nov 2001	B1
6322808	Trautman et al.	Nov 2001	B1
6329161	Heller et al.	Dec 2001	B1
6331266	Powell et al.	Dec 2001	B1
6332871	Douglas et al.	Dec 2001	B1
6334856	Allen et al.	Jan 2002	B1
6350273	Minagawa et al.	Feb 2002	B1
6352514	Douglas et al.	Mar 2002	B1
6356776	Berner et al.	Mar 2002	B1
6358265	Thorne, Jr. et al.	Mar 2002	B1
6364890	Lum et al.	Apr 2002	B1
6375626	Allen et al.	Apr 2002	B1
6375627	Mauze et al.	Apr 2002	B1
6379969	Mauze et al.	Apr 2002	B1
6391005	Lum et al.	May 2002	B1
6391645	Huang et al.	May 2002	B1
6402704	McMorrow	Jun 2002	B1
6409679	Pyo	Jun 2002	B2
6428664	BhulLar et al.	Aug 2002	B1
6449608	Morita et al.	Sep 2002	B1
6455324	Douglas	Sep 2002	B1
6493069	Nagashimada et al.	Dec 2002	B1
6500134	Cassone	Dec 2002	B1
6520973	McGarry	Feb 2003	B1
6530892	Kelly	Mar 2003	B1
6537243	Henning et al.	Mar 2003	B1
6540675	Aceti et al.	Apr 2003	B2
6544475	Douglas et al.	Apr 2003	B1
6549796	Sohrab	Apr 2003	B2
6555061	Leong et al.	Apr 2003	B1
6558624	Lemmon et al.	May 2003	B1
6579690	Bonnecaze et al.	Jun 2003	B1
6589260	Schmelzeisen-Redeker et al.	Jul 2003	B1
6591125	Buse et al.	Jul 2003	B1
6602205	Erickson et al.	Aug 2003	B1
6612111	Hodges et al.	Sep 2003	B1
6616616	Fritz et al.	Sep 2003	B2
6626874	Duchamp	Sep 2003	B1
6656167	Numao et al.	Dec 2003	B2
6679852	Schmelzeisen-Redeker et al.	Jan 2004	B1
6706000	Perez et al.	Mar 2004	B2
6706049	Moerman	Mar 2004	B2
6706159	Moerman et al.	Mar 2004	B2
6740800	Cunningham	May 2004	B1
6748275	Lattner et al.	Jun 2004	B2
6753187	Cizdziel et al.	Jun 2004	B2
6766817	da Silva	Jul 2004	B2
6793633	Douglas et al.	Sep 2004	B2
6830669	Miyazaki et al.	Dec 2004	B2
6836678	Tu	Dec 2004	B2
6837858	Cunningham et al.	Jan 2005	B2
6847451	Pugh	Jan 2005	B2
6849052	Uchigaki et al.	Feb 2005	B2
6896850	Subramanian et al.	May 2005	B2
6918404	Da Silva	Jul 2005	B2
6919960	Hansen et al.	Jul 2005	B2
6923764	Aceti et al.	Aug 2005	B2
6936476	Anderson et al.	Aug 2005	B1
D511214	Sasano et al.	Nov 2005	S
6988996	Roe et al.	Jan 2006	B2
7004928	Aceti et al.	Feb 2006	B2
7011630	Desai et al.	Mar 2006	B2
7025774	Freeman et al.	Apr 2006	B2
D519868	Sasano et al.	May 2006	S
7052652	Zanzucchi et al.	May 2006	B2
7066586	Da Silva	Jun 2006	B2
7066890	Lam et al.	Jun 2006	B1
7141058	Briggs et al.	Nov 2006	B2
7156809	Quy	Jan 2007	B2
7163616	Vreeke et al.	Jan 2007	B2
7192061	Martin	Mar 2007	B2
D540343	Cummins	Apr 2007	S
7223365	Von Der Goltz	May 2007	B2
7225008	Ward et al.	May 2007	B1
7226461	Boecker et al.	Jun 2007	B2
7258673	Racchini et al.	Aug 2007	B2
D551243	Young	Sep 2007	S
7270970	Anderson et al.	Sep 2007	B2
7297151	Boecker et al.	Nov 2007	B2
7299081	Mace et al.	Nov 2007	B2
7343188	Sohrab	Mar 2008	B2
7344507	Briggs et al.	Mar 2008	B2
7379167	Mawhirt et al.	May 2008	B2
7427377	Zanzucchi et al.	Sep 2008	B2
D580068	Shigesada et al.	Nov 2008	S
D580558	Shigesada et al.	Nov 2008	S
D599373	Kobayashi et al.	Sep 2009	S
D601257	Berlninger et al.	Sep 2009	S
7585278	Aceti et al.	Sep 2009	B2
D601444	Jones et al.	Oct 2009	S
D601578	Poulet et al.	Oct 2009	S
7682318	Alden et al.	Mar 2010	B2
D622393	Gatrall et al.	Aug 2010	S
7780631	Lum et al.	Aug 2010	B2
7803123	Perez et al.	Sep 2010	B2
7879058	Ikeda	Feb 2011	B2
7887494	Emery et al.	Feb 2011	B2
D642191	Barnett et al.	Jul 2011	S
7988644	Freeman et al.	Aug 2011	B2
8012103	Escutia et al.	Sep 2011	B2
8012104	Escutia et al.	Sep 2011	B2
8105849	McDevitt et al.	Jan 2012	B2
D654926	Lipman et al.	Feb 2012	S
8173439	Petrich et al.	May 2012	B2
8184273	Dosmann et al.	May 2012	B2
8231832	Zanzucchi et al.	Jul 2012	B2
8251920	Vreeke et al.	Aug 2012	B2
8298255	Conway et al.	Oct 2012	B2
8303518	Aceti et al.	Nov 2012	B2
8360993	Escutia et al.	Jan 2013	B2
8360994	Escutia et al.	Jan 2013	B2
8372015	Escutia et al.	Feb 2013	B2
8376959	Deck	Feb 2013	B2
8382681	Escutia et al.	Feb 2013	B2
8391940	Matzinger et al.	Mar 2013	B2
D691174	Lipman et al.	Oct 2013	S
8574168	Freeman et al.	Nov 2013	B2
8702624	Alden	Apr 2014	B2
8795201	Escutia et al.	Aug 2014	B2
8801631	Escutia et al.	Aug 2014	B2
8919605	Lipman et al.	Dec 2014	B2
8969097	Emery et al.	Mar 2015	B2
9060723	Escutia et al.	Jun 2015	B2
9060727	Saikley et al.	Jun 2015	B2
9095292	Zanzucchi et al.	Aug 2015	B2
9149215	Werner et al.	Oct 2015	B2
9366636	Emery et al.	Jun 2016	B2
9380974	Litherland et al.	Jul 2016	B2
20010001034	Douglas	May 2001	A1
20010027277	Klitmose	Oct 2001	A1
20010027328	Lum et al.	Oct 2001	A1
20010053891	Ackley	Dec 2001	A1
20020002326	Causey, III et al.	Jan 2002	A1
20020002344	Douglas et al.	Jan 2002	A1
20020004640	Conn et al.	Jan 2002	A1
20020006355	Whitson	Jan 2002	A1
20020016568	Lebel et al.	Feb 2002	A1
20020020688	Sherman et al.	Feb 2002	A1
20020022934	Vogel et al.	Feb 2002	A1
20020023852	Mcivor et al.	Feb 2002	A1
20020042594	Lum et al.	Apr 2002	A1
20020052618	Haar et al.	May 2002	A1
20020087056	Aceti et al.	Jul 2002	A1
20020136667	Subramanian et al.	Sep 2002	A1
20020137998	Smart et al.	Sep 2002	A1
20020160520	Orloff et al.	Oct 2002	A1
20020168290	Yuzhakov et al.	Nov 2002	A1
20020169394	Eppstein et al.	Nov 2002	A1
20020169411	Sherman et al.	Nov 2002	A1
20020177761	Orloff et al.	Nov 2002	A1
20020177764	Sohrab	Nov 2002	A1
20020183102	Withers et al.	Dec 2002	A1
20020188223	Perez et al.	Dec 2002	A1
20020198444	Uchigaki et al.	Dec 2002	A1
20030012693	Otillar et al.	Jan 2003	A1
20030028087	Yuzhakov et al.	Feb 2003	A1
20030028125	Yuzhakov et al.	Feb 2003	A1
20030039587	Niermann	Feb 2003	A1
20030060730	Perez	Mar 2003	A1
20030083685	Freeman et al.	May 2003	A1
20030083686	Freeman et al.	May 2003	A1
20030105961	Zatloukal et al.	Jun 2003	A1
20030116596	Terasawa	Jun 2003	A1
20030135166	Gonnelli	Jul 2003	A1
20030135333	Aceti	Jul 2003	A1
20030143746	Sage	Jul 2003	A1
20030153844	Smith et al.	Aug 2003	A1
20030153900	Aceti et al.	Aug 2003	A1
20030175987	Verdonk et al.	Sep 2003	A1
20030206302	Pugh	Nov 2003	A1
20030207441	Eyster et al.	Nov 2003	A1
20030208113	Mault et al.	Nov 2003	A1
20030211619	Olson et al.	Nov 2003	A1
20030212344	Yuzhakov et al.	Nov 2003	A1
20030212345	McAllister et al.	Nov 2003	A1
20030212347	Sohrab	Nov 2003	A1
20030216628	Bortz et al.	Nov 2003	A1
20040010207	Flaherty et al.	Jan 2004	A1
20040030353	Schmelzeisen-redeker et al.	Feb 2004	A1
20040039303	Wurster et al.	Feb 2004	A1
20040049219	Briggs et al.	Mar 2004	A1
20040059256	Perez	Mar 2004	A1
20040072357	Stiene et al.	Apr 2004	A1
20040073140	Douglas	Apr 2004	A1
20040092842	Boecker et al.	May 2004	A1
20040092995	Boecker et al.	May 2004	A1
20040094432	Neel et al.	May 2004	A1
20040096959	Stiene et al.	May 2004	A1
20040097796	Berman et al.	May 2004	A1
20040098009	Boecker et al.	May 2004	A1
20040102803	Boecker et al.	May 2004	A1
20040122339	Roe et al.	Jun 2004	A1
20040132167	Rule et al.	Jul 2004	A1
20040138588	Saikley et al.	Jul 2004	A1
20040155084	Brown	Aug 2004	A1
20040157339	Burke et al.	Aug 2004	A1
20040178218	Schomakers et al.	Sep 2004	A1
20040186394	Roe et al.	Sep 2004	A1
20040191119	Zanzucchi et al.	Sep 2004	A1
20040202576	Aceti et al.	Oct 2004	A1
20040230216	Levaughn et al.	Nov 2004	A1
20040236251	Roe et al.	Nov 2004	A1
20040238675	Banaszkiewicz et al.	Dec 2004	A1
20040242982	Sakata et al.	Dec 2004	A1
20040249253	Racchini et al.	Dec 2004	A1
20040259180	Burke et al.	Dec 2004	A1
20050004494	Perez et al.	Jan 2005	A1
20050010134	Douglas et al.	Jan 2005	A1
20050015020	LeVaughn et al.	Jan 2005	A1
20050027182	Siddiqui et al.	Feb 2005	A1
20050038680	McMahon	Feb 2005	A1
20050070819	Poux et al.	Mar 2005	A1
20050096686	Allen	May 2005	A1
20050106713	Phan et al.	May 2005	A1
20050109386	Marshall	May 2005	A1
20050159678	Taniike et al.	Jul 2005	A1
20050187532	Thurau et al.	Aug 2005	A1
20050192492	Cho et al.	Sep 2005	A1
20050202567	Zanzucchi et al.	Sep 2005	A1
20050202733	Yoshimura et al.	Sep 2005	A1
20050209518	Sage, Jr. et al.	Sep 2005	A1
20050215872	Berner et al.	Sep 2005	A1
20050215923	Wiegel	Sep 2005	A1
20050245844	Mace et al.	Nov 2005	A1
20050255001	Padmaabhan et al.	Nov 2005	A1
20050277972	Wong et al.	Dec 2005	A1
20060008389	Sacherer et al.	Jan 2006	A1
20060036134	Tarassenko et al.	Feb 2006	A1
20060052724	Roe	Mar 2006	A1
20060064035	Wang et al.	Mar 2006	A1
20060094985	Aceti et al.	May 2006	A1
20060117616	Jones et al.	Jun 2006	A1
20060122536	Haar et al.	Jun 2006	A1
20060135873	Karo et al.	Jun 2006	A1
20060155317	List	Jul 2006	A1
20060161078	Schraga	Jul 2006	A1
20060178600	Kennedy et al.	Aug 2006	A1
20060189908	Kennedy	Aug 2006	A1
20060204399	Freeman et al.	Sep 2006	A1
20060229533	Hoenes et al.	Oct 2006	A1
20060241517	Fowler et al.	Oct 2006	A1
20060257993	Mcdevitt et al.	Nov 2006	A1
20060259102	Slatkine	Nov 2006	A1
20060281187	Emery et al.	Dec 2006	A1
20070016104	Jansen et al.	Jan 2007	A1
20070017824	Rippeth et al.	Jan 2007	A1
20070078313	Emery et al.	Apr 2007	A1
20070078358	Escutia et al.	Apr 2007	A1
20070083131	Escutia et al.	Apr 2007	A1
20070112281	Olson	May 2007	A1
20070179404	Escutia et al.	Aug 2007	A1
20070179405	Emery et al.	Aug 2007	A1
20070253531	Okuzawa et al.	Nov 2007	A1
20070255181	Alvarez-icaza et al.	Nov 2007	A1
20070255302	Koeppel et al.	Nov 2007	A1
20080046831	Imai et al.	Feb 2008	A1
20080077048	Escutia et al.	Mar 2008	A1
20080139910	Mastrototaro	Jun 2008	A1
20080194934	Ray et al.	Aug 2008	A1
20080269625	Halperin et al.	Oct 2008	A1
20090054810	Zanzucchi et al.	Feb 2009	A1
20090156923	Power et al.	Jun 2009	A1
20090292489	Burke et al.	Nov 2009	A1
20090301899	Hodges et al.	Dec 2009	A1
20100010374	Escutia et al.	Jan 2010	A1
20100021947	Emery et al.	Jan 2010	A1
20100021948	Lipman et al.	Jan 2010	A1
20100095229	Dixon et al.	Apr 2010	A1
20100174211	Frey et al.	Jul 2010	A1
20100185120	Sacherer et al.	Jul 2010	A1
20100217155	Poux et al.	Aug 2010	A1
20100331650	Batman et al.	Dec 2010	A1
20110098599	Emery et al.	Apr 2011	A1
20110105872	Chickering, III et al.	May 2011	A1
20110201909	Emery et al.	Aug 2011	A1
20110294152	Lipman et al.	Dec 2011	A1
20120166090	Lipman et al.	Jun 2012	A1
20120296179	Zanzucchi et al.	Nov 2012	A1
20130110516	Abulhaj et al.	May 2013	A1
20130158430	Aceti et al.	Jun 2013	A1
20130158432	Escutia et al.	Jun 2013	A1
20130172698	Reynolds et al.	Jul 2013	A1
20130274568	Escutia et al.	Oct 2013	A1
20130274579	Richter et al.	Oct 2013	A1
20140316301	Escutia et al.	Oct 2014	A1
20140336480	Escutia et al.	Nov 2014	A1
20140376762	Lipman et al.	Dec 2014	A1
20150037898	Baldus et al.	Feb 2015	A1
20150153351	Lipman et al.	Jun 2015	A1
20150212006	Emery et al.	Jul 2015	A1
20160038066	Escutia et al.	Feb 2016	A1
20160367178	Emery et al.	Dec 2016	A1

Foreign Referenced Citations (199)

Number	Date	Country
2 201 530	Sep 1997	CA
2 513 465	Aug 2004	CA
197 05 091	Feb 1999	DE
199 22 413	Nov 2000	DE
103 02-501	Aug 2004	DE
0 103 426	Mar 1984	EP
0 256 806	Feb 1988	EP
0 396-016	Nov 1990	EP
0 396-016	Nov 1990	EP
0 397 424	Nov 1990	EP
0 255-338	Feb 1998	EP
0 849 584	Jun 1998	EP
1 266-607	Dec 2002	EP
1 266-607	Dec 2002	EP
1 369 688	Oct 2003	EP
1 369 688	Oct 2003	EP
1 360-934	Nov 2003	EP
1 360-934	Nov 2003	EP
1 486-766	Dec 2004	EP
1 486-766	Dec 2004	EP
1 529-489	May 2005	EP
1 529-489	May 2005	EP
1 769-735	Apr 2007	EP
63-305841	Dec 1988	JP
3-63570	Mar 1991	JP
03093189	Apr 1991	JP
7-67861	Mar 1995	JP
7-213925	Aug 1995	JP
9-168530	Jun 1997	JP
9-313465	Sep 1997	JP
9-266889	Oct 1997	JP
9-294737	Nov 1997	JP
10-024028	Jan 1998	JP
10-505258	May 1998	JP
10-508518	Aug 1998	JP
10-318970	Dec 1998	JP
11-056822	Mar 1999	JP
11-281779	Oct 1999	JP
2000-116629	Apr 2000	JP
2000-126161	May 2000	JP
2000-168754	Jun 2000	JP
2000-254111	Sep 2000	JP
2001-159618	Jun 2001	JP
2001-515203	Sep 2001	JP
2001-305096	Oct 2001	JP
2001-330581	Nov 2001	JP
2002-502045	Jan 2002	JP
2002-085384	Mar 2002	JP
2002-514453	May 2002	JP
2002-168862	Jun 2002	JP
2003-507719	Feb 2003	JP
2003-108679	Apr 2003	JP
2003-180417	Jul 2003	JP
2004-000598	Jan 2004	JP
2004-500948	Jan 2004	JP
2004-117339	Apr 2004	JP
2004-202256	Jul 2004	JP
2004-209266	Jul 2004	JP
2004-519302	Jul 2004	JP
2004-522500	Jul 2004	JP
2004-528936	Sep 2004	JP
2005-503538	Feb 2005	JP
2005-087613	Apr 2005	JP
2006-512969	Apr 2005	JP
3638958	Apr 2005	JP
2005-525149	Aug 2005	JP
2005-237938	Sep 2005	JP
2005-525846	Sep 2005	JP
2005-527254	Sep 2005	JP
2006-506185	Feb 2006	JP
2006-512974	Apr 2006	JP
2006-516723	Jul 2006	JP
2006-521555	Sep 2006	JP
2006-527013	Nov 2006	JP
2007-014381	Jan 2007	JP
2007-054407	Mar 2007	JP
2007-067698	Mar 2007	JP
2007-136198	Jun 2007	JP
2007-521031	Aug 2007	JP
2007-311196	Nov 2007	JP
2007-537804	Dec 2007	JP
2008-125813	Jun 2008	JP
WO-8605966	Oct 1986	WO
WO-8800812	Feb 1988	WO
WO-8807666	Oct 1988	WO
WO-9114212	Sep 1991	WO
WO-9413203	Jun 1994	WO
WO-9510223	Apr 1995	WO
WO-9510223	Apr 1995	WO
WO-9604857	Feb 1996	WO
WO-9607907	Mar 1996	WO
WO-9614026	May 1996	WO
WO-9625088	Aug 1996	WO
WO-9704707	Feb 1997	WO
WO-9715227	May 1997	WO
WO-9729847	Aug 1997	WO
WO-9730344	Aug 1997	WO
WO-9741421	Nov 1997	WO
WO-9742885	Nov 1997	WO
WO-9742888	Nov 1997	WO
WO-9743962	Nov 1997	WO
WO-9800193	Jan 1998	WO
WO-9831275	Jul 1998	WO
WO-9835225	Aug 1998	WO
WO-9912008	Mar 1999	WO
WO-9923492	May 1999	WO
WO-9944508	Sep 1999	WO
WO-9956954	Nov 1999	WO
WO-9958051	Nov 1999	WO
WO-0009184	Feb 2000	WO
WO-0013573	Mar 2000	WO
WO-0014269	Mar 2000	WO
WO-0014535	Mar 2000	WO
WO-0018449	Apr 2000	WO
WO-0018449	Apr 2000	WO
WO-0036400	Jun 2000	WO
WO-0042422	Jul 2000	WO
WO-0074763	Dec 2000	WO
WO-0074763	Dec 2000	WO
WO-0078208	Dec 2000	WO
WO-0113795	Mar 2001	WO
WO-0116575	Mar 2001	WO
WO-0152727	Jul 2001	WO
WO-0164105	Sep 2001	WO
WO-0164105	Sep 2001	WO
WO-0172220	Oct 2001	WO
WO-0180728	Nov 2001	WO
WO-0185233	Nov 2001	WO
WO-0185233	Nov 2001	WO
WO-0191634	Dec 2001	WO
WO-0191634	Dec 2001	WO
WO-0200101	Jan 2002	WO
WO-0200101	Jan 2002	WO
WO-0249507	Jun 2002	WO
WO-0249509	Jun 2002	WO
WO-0249509	Jun 2002	WO
WO-02078533	Oct 2002	WO
WO-02078533	Oct 2002	WO
WO-02082052	Oct 2002	WO
WO-02082052	Oct 2002	WO
WO-02093144	Nov 2002	WO
WO-02100251	Dec 2002	WO
WO-02100251	Dec 2002	WO
WO-02101359	Dec 2002	WO
WO-02101359	Dec 2002	WO
WO-03030984	Apr 2003	WO
WO-03066128	Aug 2003	WO
WO-03066128	Aug 2003	WO
WO-03070099	Aug 2003	WO
WO-03071940	Sep 2003	WO
WO-03071940	Sep 2003	WO
WO-2004045375	Jun 2004	WO
WO-2004045375	Jun 2004	WO
WO-2004062499	Jul 2004	WO
WO-2004062500	Jul 2004	WO
WO-2004062500	Jul 2004	WO
WO-2004064636	Aug 2004	WO
WO-2004091693	Oct 2004	WO
WO-2004091693	Oct 2004	WO
WO-2004105827	Dec 2004	WO
WO-2004105827	Dec 2004	WO
WO-2005006939	Jan 2005	WO
WO-2005006939	Jan 2005	WO
WO-2005009238	Feb 2005	WO
WO-2005013824	Feb 2005	WO
WO-2005018709	Mar 2005	WO
WO-2005018709	Mar 2005	WO
WO-2005018710	Mar 2005	WO
WO-2005018710	Mar 2005	WO
WO-2005084543	Sep 2005	WO
WO-2005084546	Sep 2005	WO
WO-2005084546	Sep 2005	WO
WO-2005085995	Sep 2005	WO
WO-2005112763	Dec 2005	WO
WO-2006138226	Dec 2006	WO
WO-2006138226	Dec 2006	WO
WO-2007041062	Apr 2007	WO
WO-2007041062	Apr 2007	WO
WO-2007041063	Apr 2007	WO
WO-2007041063	Apr 2007	WO
WO-2007041244	Apr 2007	WO
WO-2007041244	Apr 2007	WO
WO-2007041287	Apr 2007	WO
WO-2007041287	Apr 2007	WO
WO-2007041355	Apr 2007	WO
WO-2007041355	Apr 2007	WO
WO-2007108519	Sep 2007	WO
WO-2007112034	Oct 2007	WO
WO-2007112034	Oct 2007	WO
WO-2008027319	Mar 2008	WO
WO-2008027319	Mar 2008	WO
WO-2008062648	May 2008	WO
WO-2009145920	Dec 2009	WO
WO-2009148624	Dec 2009	WO
WO-2009148626	Dec 2009	WO
WO-2011065981	Jun 2011	WO
WO-2011162823	Dec 2011	WO
WO-2013020103	Feb 2013	WO
WO-2014205412	Dec 2014	WO

Non-Patent Literature Citations (172)

Entry
Advisory Action dated Feb. 2, 2009, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 3 pages.
Advisory Action dated Apr. 8, 2010, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 3 pages.
Extended European Search Report dated Jan. 22, 2013, for EP Application No. 12182900.6, filed on Sep. 29, 2006, 6 pages.
Final Office Action dated Jul. 9, 2008, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 19 pages.
Final Office Action dated Nov. 23, 2009, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 20 pages.
Final Office Action dated Jan. 21, 2011, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 7 pages.
International Search Report dated Aug. 16, 2007 for PCT Application No. PCT/US2006/038163, filed on Sep. 29, 2006, 1 page.
Interview Summary dated Jan. 13, 2009, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 4 pages.
Interview Summary dated Nov. 1, 2010, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 3 pages.
Interview Summary dated May 17, 2012, for U.S. Appl. No. 13/197,592, filed Aug. 3, 2011, 3 pages.
Interview Summary dated May 17, 2012, for U.S. Appl. No. 13/197,603, filed Aug. 3, 2011, 3 pages.
Interview Summary dated Aug. 27, 2012, for U.S. Appl. No. 13/197,592, filed Aug. 3, 2011, 3 pages.
Interview Summary dated Aug. 27, 2012, for U.S. Appl. No. 13/197,603, filed Aug. 3, 2011, 3 pages.
Non-Final Office Action dated Dec. 12, 2007, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 13 pages.
Non-Final Office Action dated Apr. 28, 2009, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 21 pages.
Non-Final Office Action dated Jun. 4, 2010, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 23 pages.
Non-Final Office Action dated Mar. 23, 2012, for U.S. Appl. No. 13/197,592, filed Aug. 3, 2011, 7 pages.
Non-Final Office Action dated Mar. 23, 2012, for U.S. Appl. No. 13/197,603, filed Aug. 3, 2011, 6 pages.
Notice of Allowance dated May 3, 2011, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 12 pages.
Request for Continued Examination filed on Feb. 4, 2009, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 2 pages.
Request for Continued Examination filed on Apr. 23, 2010, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 2 pages.
Response to Non-Final Office Action filed on Apr. 11, 2008, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 18 pages.
Response to Non-Final Office Action filed on Jul. 28, 2009, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 27 pages.
Response to Non-Final Office Action filed on Nov. 4, 2010 for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 18 pages.
Response to Non-Final Office Action filed on Aug. 23, 2012 for U.S. Appl. No. 13/197,592, filed Aug. 3, 2011, 7 pages.
Response to Non-Final Office Action filed on Aug. 23, 2012 for U.S. Appl. No. 13/197,603, filed Aug. 3, 2011, 7 pages.
Response to Final Office Action filed on Jan. 9, 2009, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 23 pages.
Response to Final Office Action filed on Mar. 23, 2010, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 25 pages.
Response to Final Office Action filed on Apr. 12, 2011, for U.S. Appl. No. 11/529,613, filed Sep. 29, 2006, 11 pages.
Written Opinion dated Aug. 16, 2007 for PCT Application No. PCT/US2006/038163, filed on Sep. 29, 2006, 4 pages.
ADA Consensus Development Panel. (Jan.-Feb. 1987). “Consensus Statement on Self-Monitoring of Blood Glucose,” Diabetes Care 10(1):95-99.
ADA (Jan. 1994). “Self-Monitoring of Blood Glucose,” Consensus Statement Diabetes Care 17(1):81-86.
Anonymous. (Sep. 30, 1993). “The Effect of Intensive Treatment of Diabetes on the Development and Progression of Long-Term Complications in Insulin-Dependent Diabetes Mellitus.” The New England Journal of Medicine 329(14):977-986.
Anonymous. (Jun. 23, 1998). “Taking the “Ouch” Out of Needles: Arrays of Microneedles” Offer New Techniques for Drug Delivery, Science Daily, located at <http:www.sciencedaily.com/releases/1998/06/980623045850.htm>, last visited Jan. 14, 2014, 3 pages.
Beregszàszi, M. et al. (Jul. 1997). “Nocturnal Hypoglycemia in Children and Adolescents with Insulin-Dependent Diabetes Mellitus: Prevalence and Risk Factors,” J. Pediatrics 131(1 Pt. 1):27-33.
Chase, H.P. et al. (Feb. 2001). “Continuous Subcutaneous Glucose Monitoring in Children with Type 1 Diabetes,” Pediatrics 107(2):222-226.
Clarke, W.L. et al. (Sep.-Oct. 1987). “Evaluating Clinical Accuracy of Systems for Self-Monitoring of Blood Glucose,” Diabetes Care 10(5):622-628.
Collison, M.E. et al. (Sep. 1999). “Analytical Characterization of Electrochemical Biosensor Test Strips for Measurement of Glucose in Low-Volume Interstitial Fluid Samples,” Clinical Chemistry 45(9):1665-1673.
Cox, D.J. et al. (Jun. 1997). “Understanding Error Grid Analysis,” Diabetes Care 20(6):911-912.
D'Arrigo, T.D. (Mar. 2000). “GlucoWatch Monitor Poised for Approval,” Diabetes Forecast, 53(3):43-44.
Feldman, B. et al. (2000). “FreeStyle™: A Small-Volume Electrochemical Glucose Sensor for Home Blood Glucose Testing,” Diabetes Technology and Therapeutics, 2(2):221-229.
Johnson, R.N. et al. (Jan. 1998). “Accuracy of Devices Used for Self-Monitoring of Blood Glucose,” Annals of Clinical Biochemistry 35(1):68-74.
Johnson, R.N. et al. (Jan. 1999). “Analytical Error of Home Glucose Monitors: A Comparison of 18 Systems,” Annals of Clinical Biochemistry 36(1):72-79.
Johnson, R.N. et al. (2001). “Error Detection and Measurement in Glucose Monitors,” Clinica Chimica Acta 307:61-67.
Kumetrix, Inc. (Dec. 1999). “Painless Blood Glucose Monitoring, Courtesy of the Mosquito,” Start-Up pp. 27-28.
Lee, S-C. (Jun. 1999). “Light Scattering by Closely Spaced Parallel Cylinders Embedded in a Finite Dielectric Slab,” Journal of the Optical Society of America A 16(6):1350-1361.
Mahler, R.J. et al. (1999). “Clinical Review 102, Type 2 Diabetes Melitus: Update on Diagnosis Pathophysiology, and Treatment,” The Journal of Clinical Endocrinology and Metabolism 84(4):1165-1171.
McGarraugh, G. et al. (2001). “Physiological Influences on Off-Finger Glucose Testing,” Diabetes Technology & Therapeutics 3(3):367-376.
McNichols, R.J. et al. (Jan. 2000). “Optical Glucose Sensing in Biological Fluids: An Overview,” Journal of Biomedical Optics, 5(1):5-16.
Medline Plus. (Jun. 17, 2008). , Medical Encyclopedia, Monitor Blood Glucose-Series: Part 1-4, 6 pages.
Neeley, W.E. et al. (1981). “An Instrument for Digital Matrix Photometry,” Clinical Chemistry 27(10):1665-1668.
Neeley, W.E. (1983). “Reflectance Digital Matrix Photometry,” Clinical Chemistry 29(6):1038-1041.
Neeley, W.E. (1983). “Multilayer Film Analysis for Glucose in 1-μL Samples of Plasma,” Clinical Chemistry 29(12):2103-2105.
Neeley, W.E. (1988). “A Reflectance Photometer with a Square Photodiode Array Detector for Use on Multilayer Dry-Film Slides,” Clinical Chemistry 34(11):2367-2370.
Otto, E. et al. (2000). “An Intelligent Diabetes Software Prototype: Predicting Blood Glucose Levels and Recommending Regimen Changes,” Diabetes Technology and Therapeutics 2(4):569-576.
Pfohl, M. et al. (2000). “Spot Glucose Measurement in Epidermal Interstitial Fluid—An Alternative to Capillary Blood Glucose Estimation,” Experimental and Clinical Endocrinology & Diabetes 108(1):1-4.
Princen, H.M. (May 1969). “Capillary Phenomena in Assemblies of Parallel Cylinders, I. Capillary Rise Between Two Cylinders,” Journal of Colloid and Interface Science 30(1):69-75.
Princen, H.M. (Jul. 1969). “Capillary Phenomena in Assemblies of Parallel Cylinders, II. Capillary Rise in Systems with More Than Two Cylinders,” Journal of Colloid and Interface Science 30(3):359-371.
Rebrin, K. et al. (Sep. 1999). “Subcutaneous Glucose Predicts Plasma Glucose Independent of Insulin: Implications for Continuous Monitoring,” American Journal of Physiology 277(3):E561-E571.
Smart, W.H. et al. (2000). “The Use of Silicon Microfabrication Technology in Painless Glucose Monitoring,” Diabetes Technology & Therapeutics 2(4):549-559.
Svedman, C. et al. (Apr. 1999). “Skin Mini-Erosion Technique for Monitoring Metabolites in Interstitial Fluid: Its Feasibility Demonstrated by OGTT Results in Diabetic and Non-Diabetic Subjects,” Scand. J. Clin. Lab. Invest. 59(2):115-123.
Trinder, P. (1969). “Determination of Glucose in Blood Using Glucose Oxidase with an Alternate Oxygen Acceptor,” Annals of Clinical Biochemistry 6:24-28.
Yum, S. I. et al. (Nov. 1, 1999). “Capillary Blood Sampling for Self-Monitoring of Blood Glucose,” Diabetes Technology & Therapeutics, 1(1):29-37.
Brazzle, J. et al. Active Microneedles with Integrated Functionality, Solid-State Sensor and Actuator Workshop, Hilton Head Island, South Carolina, Jun. 4-8, 2000, Technical Digest, 199-202.
Burge, M.R., (Aug. 2001). “Lack of Compliance with Home Blood Glucose Monitoring Predicts Hospitalization in Diabetes”, Diabetes Care 24(8): 1502-1503.
Clarke, W.L. et al. (Sep.-Oct. 1981). “Evaluation of a New Reflectance Photometer for Use in Home Blood Glucose Monitoring,” Diabetes Care, 4(5):547-550.
Coster, S. et al. (2000). “Monitoring Blood Glucose Control in Diabetes Mellitus: A Systematic Review.” Health Technology Assessment 4(12):1-93.
Extended European Search Report dated Feb. 22, 2012, for EP Application No. EP 10 18 1155.2, filed Sep. 28, 2010, six pages.
Extended European Search Report dated Jul. 18, 2013, for EP Application No. 06 772 943.4, filed on Jun. 13, 2006, 7 pages.
Extended European Search Report dated Nov. 8, 2016, for EP Application No. 16 167 087.2, filed on Aug. 3, 2012, 6 pages.
Extended European Search Report dated Apr. 19, 2011, for EP Application No. 10 18 0848.3 filed Sep. 28, 2010, 5 pages.
Written Opinion dated Aug. 20, 2007 for PCT Application No. PCT/US2006/37245, filed on Sep. 26, 2006, 7 pages.
Extended European Search Report dated Apr. 29, 2013 for EP Patent Application No. 12192620.8, filed on Nov. 14, 2012, 8 pages.
Extended European Search Report dated Feb. 2, 2016 for European Patent Application No. 15187274.4, filed on Sep. 29, 2015, 5 pages.
Final Office Action dated Aug. 15, 2013 for U.S. Appl. No. 13/562,129, filed Jul. 30, 2012, 12 pages.
Final Office Action dated Apr. 13, 2016, for U.S. Appl. No. 13/669,366, filed Nov. 5, 2012, 31 pages.
Final Office Action dated Aug. 28, 2014, for U.S. Appl. No. 13/562,129, filed Jul. 30, 2012, 11 pages.
Final Office Action dated Dec. 26, 2014, for U.S. Appl. No. 13/669,366, filed Nov. 5, 2012, 9 pages.
Final Office Action dated Jan. 22, 2014, for U.S. Appl. No. 13/669,366, filed Nov. 5, 2012, 8 pages.
Final Office Action dated Jun. 30, 2010, for U.S. Appl. No. 11/529,612, filed Sep. 29, 2006, 11 pages.
Final Office Action dated May 30, 2007, for U.S. Appl. No. 11/125,107, filed May 10, 2005, 11 pages.
Final Office Action dated Nov. 1, 2010, for U.S. Appl. No. 11/311,667, filed Dec. 20, 2005, 9 pages.
Final Office Action dated Nov. 21, 2011, for U.S. Appl. No. 11/311,667, filed Dec. 20, 2005, 8 pages.
Final Office Action dated Jun. 11, 2010, for U.S. Appl. No. 11/529,614, filed Sep. 29, 2006, 16 pages.
Final Office Action dated Mar. 10, 2015, for U.S. Appl. No. 11/529,614, filed Sep. 29, 2006, 24 pages.
Final Office Action dated Oct. 15, 2009, for U.S. Appl. No. 11/239,122, filed Sep. 30, 2005, 13 pages.
Final Office Action dated Aug. 14, 2012, for U.S. Appl. No. 13/037,089, filed Feb. 28, 2011, 14 pages.
Final Office Action dated Sep. 23, 2013, for U.S. Appl. No. 13/037,089, filed Feb. 28, 2011, 14 pages.
Final Office Action dated Mar. 5, 2009, for U.S. Appl. No. 11/239,123, filed Sep. 30, 2005, 17 pages.
Final Office Action dated Mar. 3, 2011, for U.S. Appl. No. 11/239,123, filed Sep. 30, 2005, 25 pages.
Final Office Action dated Jan. 6, 2016, for U.S. Appl. No. 14/321,631, filed Jul. 1, 2014, 9 pages.
Hemmerich, K.J. et al. (Apr. 1995).“Guide to Engineering Thermoplastics,” Medical Devices and Diagnostic Industry pp. 39-59.
International Search Report dated Dec. 3, 2004, for PCT Application No. PCT/US2004/08798, filed on Mar. 24, 2004, 3 pages.
International Search Report dated May 2, 2007, for PCT Application No. PCT/US2006/37923, filed on Sep. 9, 2006, 1 page.
International Search Report dated Aug. 17, 2007 for PCT/US2006/38049, filed on Sep. 29, 2006, 1 page.
International Search Report dated Oct. 19, 2012 for PCT Application No. PCT/US2012/049629, filed on Aug. 3, 2012, 4 pages.
International Search Report dated Jan. 16, 2008, for PCT Application No. PCT/US2006/022840, filed on Jun. 13, 2006, 1 page.
Written Opinion of the International Searching Authority dated Jan. 16, 2008, for PCT Application No. PCT/US2006/022840, filed on Jun. 13, 2006, 3 pages.
International Search Report dated Aug. 20, 2007 for PCT Application No. PCT/US2006/37245, filed on Sep. 26, 2006, 1 page.
INTEG. (2000). “LifeGuide™ Glucose Meter. No Lancets. No Blood,” located at <http://www.integonline.com>, last visited May 1, 2000, 10 pages.
Ishii H. et al., (Aug. 2001). “Seasonal Variation of Glycemic Control in Type 2 Diabetic Patients”, Diabetes Care 24(8):1503.
Massey V. et al. (Aug. 1960). “Studies on the Reaction Mechanism of Lipoyl Dehydrogenase” Biochim. Biophys. Acta 48: 33-47.
Non-Final Office Action dated Nov. 26, 2012 for U.S. Appl. No. 13/562,129, filed Jul. 30, 2012, 9 pages.
Non Final Office Action dated Apr. 8, 2015, for U.S. Appl. No. 13/566,886, filed Aug. 3, 2012, 11 pages.
Non-Final Office Action dated Mar. 19, 2009, for U.S. Appl. No. 11/239,122, filed Sep. 30, 2005, 15 pages.
Non-Final Office Action dated Sep. 1, 2010, for U.S. Appl. No. 11/239,122, filed Sep. 30, 2005, 15 pages.
Non Final Office Action dated Apr. 12, 2011, for U.S. Appl. No. 11/311,667, filed Dec. 20, 2005, 7 pages.
Non-Final Office Action dated Sep. 13, 2011, for U.S. Appl. No. 13/037,089, filed Feb. 28, 2011, 14 pages.
Non-Final Office Action dated Feb. 28, 2013, for U.S. Appl. No. 13/037,089, filed Feb. 28, 2011, 12 pages.
Non-Final Office Action dated Apr. 10, 2014, for U.S. Appl. No. 13/037,089, filed Feb. 28, 2011, 14 pages.
Non-Final Office Action dated May 29, 2015, for U.S. Appl. No. 14/614,177, filed Feb. 4, 2015, 13 pages.
Non Final Office Action dated Aug. 5, 2014, for U.S. Appl. No. 13/669,366, filed Nov. 5, 2012, 8 pages.
Non Final Office Action dated Dec. 5, 2014, for U.S. Appl. No. 13/562,129, filed Jul. 30, 2012, 7 pages.
Non Final Office Action dated Jan. 12, 2009, for U.S. Appl. No. 11/529,612, filed Sep. 29, 2006, 9 pages.
Non Final Office Action dated Jan. 21, 2011, for U.S. Appl. No. 11/529,612, filed Sep. 29, 2006, 9 pages.
Non Final Office Action dated Jul. 13, 2010, for U.S. Appl. No. 12/222,724, filed Aug. 14, 2008, 11 pages.
Non Final Office Action dated Jul. 31, 2015, for U.S. Appl. No. 13/669,366, filed Nov. 5, 2012, 16 pages.
Non Final Office Action dated Mar. 21, 2014, for U.S. Appl. No. 13/562,129, filed Jul. 30, 2012, 12 pages.
Non Final Office Action dated Mar. 25, 2011, for U.S. Appl. No. 12/222,724, filed Aug. 14, 2008, 13 pages.
Non Final Office Action dated Mar. 5, 2010, for U.S. Appl. No. 11/311,667, filed Dec. 20, 2005, 8 pages.
Non Final Office Action dated May 14, 2008, for U.S. Appl. No. 11/529,612, filed Sep. 29, 2006, 9 pages.
Non Final Office Action dated May 16, 2013, for U.S. Appl. No. 13/669,366, filed Nov. 5, 2012, 8 pages.
Non Final Office Action dated May 5, 2005, for U.S. Appl. No. 10/131,268, filed Apr. 23, 2002, 8 pages.
Non Final Office Action dated Nov. 2, 2006, for U.S. Appl. No. 11/125,107, filed May 10, 2005, 10 pages.
Non Final Office Action dated Oct. 14, 2009, for U.S. Appl. No. 11/529,612, filed Sep. 29, 2006, 10 pages.
Non Final Office Action dated Oct. 3, 2008, for U.S. Appl. No. 10/722,074, filed Nov. 24, 2003, 10 pages.
Non-Final Office Action dated Dec. 17, 2015, for U.S. Appl. No. 11/529,614, filed Sep. 29, 2006, 6 pages.
Non Final Office Action dated Dec. 2, 2004, for U.S. Appl. No. 10/347,620, filed Jan. 22, 2003, 8 pages.
Non-Final Office Action dated Jan. 27, 2009, for U.S. Appl. No. 11/529,614, filed Sep. 29, 2006, 17 pages.
Non-Final Office Action dated Jan. 6, 2014, for U.S. Appl. No. 11/529,614, filed Sep. 29, 2006, 12 pages.
Non-Final Office Action dated Jun. 21, 2013, for U.S. Appl. No. 13/752,261, filed Jan. 28, 2013, 12 pages.
Non-Final Office Action dated Jun. 6, 2008, for U.S. Appl. No. 11/529,614, filed Sep. 29, 2006, 17 pages.
Non-Final Office Action dated Oct. 9, 2014, for U.S. Appl. No. 14/446,262, filed Jul. 29, 2014, 15 pages.
Non Final Office Action dated Sep. 29, 2004, for U.S. Appl. No. 10/394,230, filed Mar. 24, 2003, 10 pages.
Non-Final Office Action dated Nov. 1, 2007, for U.S. Appl. No. 11/239,123, filed Sep. 30, 2005, 15 pages.
Non-Final Office Action dated Apr. 15, 2010, for U.S. Appl. No. 11/239,123, filed Sep. 30, 2005, 19 pages.
Non-Final Office Action dated Sep. 19, 2013, for U.S. Appl. No. 11/239,123, filed Sep. 30, 2005, 24 pages.
Non-Final Office Action dated Aug. 8, 2014, for U.S. Appl. No. 14/321,631, filed Jul. 1, 2014, 11 pages.
Notice of Allowance dated Apr. 3, 2014, for U.S. Appl. No. 11/239,123, filed Sep. 30, 2005, 6 pages.
Notice of Allowance dated Apr. 18, 2012, for U.S. Appl. No. 11/529,612, filed Sep. 29, 2006, 8 pages.
Notice of Allowance dated Apr. 19, 2010, for U.S. Appl. No. 29/338,117, filed Jun. 4, 2009, 4 pages.
Notice of Allowance dated Aug. 3, 2012, for U.S. Appl. No. 11/529,612, filed Sep. 29, 2006, 5 pages.
Notice of Allowance dated Jan. 14, 2010, for U.S. Appl. No. 29/338,117, filed Jun. 4, 2009, 4 pages.
Notice of Allowance dated Jun. 29, 2012, for U.S. Appl. No. 11/311,667, filed Dec. 20, 2005, 5 pages.
Notice of Allowance dated Mar. 14, 2012, for U.S. Appl. No. 12/222,724, filed Aug. 14, 2008, 7 pages.
Notice of Allowance dated Mar. 31, 2005, for U.S. Appl. No. 10/394,230, filed Mar. 24, 2003, 10 pages.
Notice of Allowance dated May 15, 2008, for U.S. Appl. No. 11/125,107, filed May 10, 2005, 7 pages.
Notice of Allowance dated May 18, 2009, for U.S. Appl. No. 29/300,934, filed May 30, 2008, 4 pages.
Notice of Allowance dated May 28, 2009, for U.S. Appl. No. 29/300,933, filed May 30, 2008, 6 pages.
Notice of Allowance dated Nov. 23, 2011, for U.S. Appl. No. 12/222,724, filed Aug. 14, 2008, 7 pages.
Notice of Allowance dated Nov. 27, 2012, for U.S. Appl. No. 11/529,612, filed Sep. 29, 2006, 5 pages.
Notice of Allowance dated Nov. 29, 2005, for U.S. Appl. No. 10/131,268, filed Apr. 23, 2002, 6 pages.
Notice of Allowance dated Oct. 12, 2011, for U.S. Appl. No. 11/529,612, filed Sep. 29, 2006, 8 pages.
Notice of Allowance dated Feb. 23, 2015, for U.S. Appl. No. 14/446,262, filed Jul. 29, 2014, 8 pages.
Notice of Allowance dated Feb. 5, 2014, for U.S. Appl. No. 13/752,261, filed Jan. 28, 2013, 9 pages.
Notice of Allowance dated Jun. 15, 2009, for U.S. Appl. No. 10/722,074, filed Nov. 24, 2003, 6 pages.
Notice of Allowance dated Mar. 2, 2016, for U.S. Appl. No. 11/529,614, filed Sep. 29, 2006, 12 pages.
Notice of Allowance dated Mar. 28, 2005, for U.S. Appl. No. 10/347,620, filed Jan. 22, 2003, 6 pages.
Notice of Allowance dated Sep. 18, 2014, for U.S. Appl. No. 13/037,089, filed Feb. 28, 2011, 9 pages.
Notice of Allowance dated Feb. 16, 2016, for U.S. Appl. No. 14/614,177, filed Feb. 4, 2015, 7 pages.
Notice of Allowance dated Mar. 27, 2015, for U.S. Appl. No. 13/562,129, filed Jul. 30, 2012, 7 pages.
Rosen, S. (1999). “Road to New-Age Glucose Monitoring Still Rocky,” Diagnostic Insight, pp. 4-5, 12-13, 16.
Spielman, A. et al. (2001). Mosquito: A Natural History of Our Most Persistent and Deadly Foe, First Edition, Hyperion, New York, NY, 3 pages. (Table of Contents Only).
Sonntag, O. (1993). Ektachem. Dry Chemistry, Analysis With Carrier-Bound Reagents, Elsevier Science Publishers, 57 pages.
Straub F.B. (Mar. 1939). “Isolation and Properties of a flavoprotien from Heart Muscle Tissue”, Biochemical Journal 33: 787-792.
Tietz, N.W. (1986). Textbook of Clinical Chemistry, W.B. Saunders Company, pp. 1533 and 1556.
U.S. Precision Lens, Inc. (1983).The Handbook of Plastic Optics.
Wikipedia (2016). “Capillary action,” 7 pages.
Written Opinion dated Dec. 3, 2004, for PCT Application No. PCT/US2004/08798, filed on Mar. 24, 2004, 4 pages.
Written Opinion dated May 2, 2007, for PCT Application No. PCT/US2006/37923, filed on Sep. 9, 2006, 5 pages.
Written Opinion dated Aug. 17, 2007 for PCT/US2006/38049, filed on Sep. 29, 2006, 6 pages.
Written Opinion dated Oct. 19, 2012 for PCT Application No. PCT/US2012/049629, filed on Aug. 3, 2012, 7 pages.

Related Publications (1)

	Number	Date	Country
	20160038066 A1	Feb 2016	US

Provisional Applications (1)

	Number	Date	Country
	60721966	Sep 2005	US

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	Number	Date	Country
Parent	11529613	Sep 2006	US
Child	11941403		US

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	Number	Date	Country
Parent	14446262	Jul 2014	US
Child	14743867		US
Parent	13752261	Jan 2013	US
Child	14446262		US
Parent	13197592	Aug 2011	US
Child	13752261		US
Parent	11941403	Nov 2007	US
Child	13197592		US

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