Hybrid drape having a gel-coated perforated mesh

Description

FIELD

The present disclosure relates generally to dressings for adhering to a wound or tissue site, and more particularly, but without limitation, to a hybrid drape having a gel-coated perforated mesh.

BACKGROUND

Clinical studies and practice have shown that reducing pressure in proximity to a tissue site can augment and accelerate growth of new tissue at the tissue site. The applications of this phenomenon are numerous, but it has proven particularly advantageous for treating wounds. Regardless of the etiology of a wound, whether trauma, surgery, or another cause, proper care of the wound is important to the outcome. Treatment of wounds or other tissue with reduced pressure may be commonly referred to as “negative-pressure therapy,” but is also known by other names, including “negative pressure wound therapy,” “reduced-pressure therapy,” “vacuum therapy,” and “vacuum assisted closure,” for example. Negative-pressure therapy may provide a number of benefits, including migration of epithelial and subcutaneous tissues, improved blood flow, and micro-deformation of tissue at a wound site. Together, these benefits can increase development of granulation tissue and reduce healing times.

While the clinical benefits of negative-pressure therapy are widely known, the cost and complexity of negative-pressure therapy can be a limiting factor in its application, and the development and operation of negative-pressure systems, components, and processes continues to present significant challenges to manufacturers, healthcare providers, and patients.

SUMMARY

According to an illustrative, non-limiting embodiment, a dressing for treating a tissue site with negative pressure is described. The dressing may include a tissue interface configured to be positioned adjacent to the tissue site; and a sealing member configured to be positioned over the tissue interface and the tissue site to form a sealed environment. The sealing member may include a film layer, a layer of a bonding adhesive coupled to the film layer, and a mesh coupled to the layer of the bonding adhesive. The mesh may have a coating of a sealing adhesive and one or more bonding apertures.

According to another illustrative embodiment, a system for treating a tissue site with negative-pressure is described. The system may include a manifold configured to be positioned adjacent to the tissue site and a drape configured to be positioned over the tissue site and the manifold to form a sealed space. The system may also include a negative-pressure source configured to provide negative-pressure to the sealed space. The drape may include a film layer, a layer of a bonding adhesive coupled to the film layer, and a mesh coupled to the layer of the bonding adhesive. The mesh may have a coating of a sealing adhesive and one or more bonding apertures.

According to another illustrative embodiment, a method for manufacturing a drape for a negative-pressure system is described. A film layer may be provided, and a layer of a bonding adhesive may be coupled to the film layer. A mesh may be formed and coated with a sealing adhesive. One or more bonding apertures may be formed in the mesh, and the mesh may be coupled to the layer of the bonding adhesive.

Other aspects, features, and advantages of the illustrative embodiments will become apparent with reference to the drawings and detailed description that follow.

BRIEF DESCRIPTION OF THE DRAWINGS

Illustrative embodiments are described in detail below with reference to the attached drawings, which are incorporated by reference herein, and wherein:

FIG. 1 is a schematic diagram of an illustrative embodiment of a system for treating a tissue site with negative pressure;

FIG. 2 is an exploded perspective view of a drape that may be used with some embodiments of the systems of FIG. 1;

FIG. 3A is a plan view of a mesh that may be used with some embodiments of the drape of FIG. 2;

FIG. 3B is a perspective view of a portion of the mesh of FIG. 3A;

FIG. 3C is a side elevation view of a portion of the mesh of FIG. 3A;

FIG. 4 is a sectional view illustrating additional details that may be associated with some embodiments of the drape of FIG. 2 in a first state; and

FIG. 5 is a sectional view of the portion of the drape of FIG. 4 in a second state.

DETAILED DESCRIPTION

The following description of example embodiments provides information that enables a person skilled in the art to make and use the subject matter set forth in the appended claims, but may omit certain details already well-known in the art. The following detailed description is, therefore, to be taken as illustrative and not limiting.

The example embodiments may also be described herein with reference to spatial relationships between various elements or to the spatial orientation of various elements depicted in the attached drawings. In general, such relationships or orientation assume a frame of reference consistent with or relative to a patient in a position to receive treatment. However, as should be recognized by those skilled in the art, this frame of reference is merely a descriptive expedient rather than a strict prescription.

FIG. 1 is a sectional view of an example embodiment of a negative-pressure therapy system 100 illustrating details that may be associated with some embodiments for treating a tissue site 102 with negative pressure. As shown in the illustrative embodiment of FIG. 1, the negative-pressure therapy system 100 may include a dressing 104 fluidly coupled to a negative-pressure source 106. In some embodiments, the negative-pressure source 106 may be fluidly coupled to the dressing 104 by a conduit, such as a tube 112, and a connector, such as a connector 114. The dressing 104 may generally include a drape, such as a drape 108, and a tissue interface, such as a manifold 110. The drape 108 may have a film layer 124, a layer of a bonding adhesive 126, and a mesh 128. The drape 108 may be attached to an epidermis 116.

In general, components of the negative-pressure therapy system 100 may be coupled directly or indirectly to each other. For example, the negative-pressure source 106 may be directly coupled to the connector 114 and indirectly coupled to the manifold 110 through the connector 114. Components may be fluidly coupled to each other to provide a path for transferring fluids (such as, liquid, gas, or both liquid and gas) between the components.

In some embodiments, components may be fluidly coupled with a tube, such as the tube 112, for example. A “tube,” as used herein, broadly refers to a tube, pipe, hose, conduit, or other structure with one or more lumina adapted to convey fluids between two ends. Typically, a tube is an elongated, cylindrical structure with some flexibility, but the geometry and rigidity may vary. In some embodiments, components may additionally or alternatively be coupled by virtue of physical proximity, being integral to a single structure, or being formed from the same piece of material. Coupling may also include mechanical, thermal, electrical, or chemical coupling (such as a chemical bond) in some contexts.

In operation, a tissue interface, such as the manifold 110, may be placed within, over, on, against, or otherwise adjacent to a tissue site. For example, the manifold 110 may be placed against the tissue site 102, and the drape 108 may be placed over the manifold 110 and sealed to tissue proximate to the tissue site 102. Tissue proximate to a tissue site is often undamaged epidermis peripheral to the tissue site. Thus, the drape 108 can provide a sealed therapeutic environment 118 proximate to the tissue site 102. The sealed therapeutic environment 118 may be substantially isolated from the external environment, and the negative-pressure source 106 can reduce the pressure in the sealed therapeutic environment 118. Negative pressure applied uniformly through a tissue interface in the sealed therapeutic environment 118 can induce macrostrain and microstrain in the tissue site 102, as well as remove exudates and other fluids from the tissue site. The removed exudates and other fluids can be collected in a container and disposed of properly.

The fluid mechanics of using a negative-pressure source to reduce pressure in another component or location, such as within a sealed therapeutic environment 118, can be mathematically complex. However, the basic principles of fluid mechanics applicable to negative-pressure therapy are generally well-known to those skilled in the art, and the process of reducing pressure may be described illustratively herein as “delivering,” “distributing,” or “generating” negative pressure, for example.

In general, exudates and other fluids flow toward lower pressure along a fluid path. This orientation is generally presumed for purposes of describing various features and components of negative-pressure therapy systems herein. Thus, in the context of negative-pressure therapy, the term “downstream” typically implies something in a fluid path relatively closer to a negative-pressure source, and conversely, the term “upstream” implies something relatively further away from a negative-pressure source. Similarly, it may be convenient to describe certain features in terms of fluid “inlet” or “outlet” in such a frame of reference. However, a fluid path may also be reversed in some applications, such as by substituting a positive-pressure source, and this descriptive convention should not be construed as a limiting convention.

The term “tissue site” in this context broadly refers to a wound or defect located on or within tissue, including but not limited to, bone tissue, adipose tissue, muscle tissue, neural tissue, dermal tissue, vascular tissue, connective tissue, cartilage, tendons, or ligaments. A wound may include chronic, acute, traumatic, subacute, and dehisced wounds, partial-thickness burns, ulcers (such as diabetic, pressure, or venous insufficiency ulcers), flaps, and grafts, for example. The term “tissue site” may also refer to areas of tissue that are not necessarily wounded or defective, but are instead areas in which it may be desired to add or promote the growth of additional tissue. For example, negative pressure may be used in certain tissue areas to grow additional tissue that may be harvested and transplanted to another tissue location. In an illustrative embodiment, the tissue site 102 may be a wound that extends through the epidermis 116, through a dermis 120, and into subcutaneous tissue 122.

“Negative pressure” generally refers to a pressure less than a local ambient pressure, such as the ambient pressure in a local environment external to a sealed therapeutic environment 118 provided by the drape 108. In many cases, the local ambient pressure may also be the atmospheric pressure in a patient's vicinity. Alternatively, the pressure may be less than a hydrostatic pressure associated with tissue at the tissue site. Unless otherwise indicated, values of pressure stated herein are gauge pressures. Similarly, references to increases in negative pressure typically refer to a decrease in absolute pressure, while decreases in negative pressure typically refer to an increase in absolute pressure.

A negative-pressure source, such as the negative-pressure source 106, may be a reservoir of air at a negative pressure, or may be a manual or electrically-powered device that can reduce the pressure in a sealed volume, such as a vacuum pump, a suction pump, a wall-suction port available at many healthcare facilities, or a micro-pump, for example. A negative-pressure source may be housed within or used in conjunction with other components, such as sensors, processing units, alarm indicators, memory, databases, software, display devices, or operator interfaces that further facilitate negative-pressure therapy. While the amount and nature of negative pressure applied to a tissue site may vary according to therapeutic requirements, the pressure typically ranges between −5 millimeters of mercury (mm Hg) (−667 Pa) and −500 mm Hg (−66.7 kPa). Common therapeutic ranges are between −75 mm Hg (−9.9 kPa) and −300 mm Hg (−39.9 kPa).

A tissue interface, such as the manifold 110, can generally be adapted to contact a tissue site or other layers of a dressing. A tissue interface may be partially or fully in contact with a tissue site. If a tissue site is a wound, for example, a tissue interface may partially or completely fill the wound, or may be placed over the wound. A tissue interface may take many forms, and may be many sizes, shapes, or thicknesses depending on a variety of factors, such as the type of treatment being implemented or the nature and size of a tissue site. For example, the size and shape of a tissue interface may be adapted to the contours of deep and irregular shaped tissue sites.

In some embodiments, a tissue interface may be a manifold, such as the manifold 110. A “manifold” in this context generally includes any substance or structure providing a plurality of pathways adapted to collect or distribute fluid across a tissue site under negative pressure. For example, a manifold may be adapted to receive negative pressure from a source and distribute the negative pressure through multiple apertures across a tissue site, which may have the effect of collecting fluid from across a tissue site and drawing the fluid toward the source. In some embodiments, the fluid path may be reversed or a secondary fluid path may be provided to facilitate delivering fluid across a tissue site.

In some illustrative embodiments, the pathways of a manifold may be channels interconnected to improve distribution or collection of fluids across a tissue site. For example, cellular foam, open-cell foam, reticulated foam, porous tissue collections, and other porous material such as gauze or felted mat generally include pores, edges, and/or walls adapted to form interconnected fluid pathways. Liquids, gels, and other foams may also include or be cured to include apertures and flow channels. In some illustrative embodiments, a manifold may be a porous foam material having interconnected cells or pores adapted to uniformly (or quasi-uniformly) distribute negative pressure to a tissue site. The foam material may be either hydrophobic or hydrophilic. In one non-limiting example, a manifold may be an open-cell, reticulated polyurethane foam such as GranuFoam® dressing available from Kinetic Concepts, Inc. of San Antonio, Tex.

In some embodiments, such as embodiments in which the manifold 110 may be made from a hydrophilic material, the manifold 110 may also wick fluid away from a tissue site while continuing to distribute negative pressure to the tissue site. The wicking properties of the manifold 110 may draw fluid away from a tissue site by capillary flow or other wicking mechanisms. An example of a hydrophilic foam is a polyvinyl alcohol, open-cell foam such as V.A.C. WhiteFoam® dressing available from Kinetic Concepts, Inc. of San Antonio, Tex. Other hydrophilic foams may include those made from polyether. Other foams that may exhibit hydrophilic characteristics include hydrophobic foams that have been treated or coated to provide hydrophilicity.

A tissue interface may further promote granulation at a tissue site if pressure within the sealed therapeutic environment 118 is reduced. For example, any or all of the surfaces of the manifold 110 may have an uneven, coarse, or jagged profile that can induce microstrains and stresses at a tissue site if negative pressure is applied through the manifold 110.

In some example embodiments, a tissue interface may be constructed from bioresorbable materials. Suitable bioresorbable materials may include, without limitation, a polymeric blend of polylactic acid (PLA) and polyglycolic acid (PGA). The polymeric blend may also include without limitation polycarbonates, polyfumarates, and capralactones. The tissue interface may further serve as a scaffold for new cell-growth, or a scaffold material may be used in conjunction with the tissue interface to promote cell-growth. In general, a scaffold material may be a biocompatible or biodegradable substance or structure used to enhance or promote the growth of cells or formation of tissue, such as a three-dimensional porous structure that provides a template for cell growth. Illustrative examples of scaffold materials include calcium phosphate, collagen, PLA/PGA, coral hydroxy apatites, carbonates, or processed allograft materials.

In some embodiments, the drape 108 may provide a bacterial barrier and protection from physical trauma. The drape 108 may also be constructed from a material that can reduce evaporative losses and provide a fluid seal between two components or two environments, such as between a therapeutic environment and a local external environment. The drape 108 may be, for example, an elastomeric film or membrane that can provide a seal adequate to maintain a negative pressure at a tissue site for a given negative-pressure source. In some example embodiments, the drape 108 may be a polymer drape, such as a polyurethane film, that is permeable to water vapor but impermeable to liquid. Such drapes typically have a thickness in the range of about 25 microns to about 50 microns. For permeable materials, the permeability generally should be low enough that a desired negative pressure may be maintained.

An attachment device may be used to attach the drape 108 to an attachment surface, such as undamaged epidermis, a gasket, or another cover. The attachment device may take many forms. For example, an attachment device may be a medically-acceptable, pressure-sensitive adhesive that extends about a periphery, a portion, or an entire sealing member. In some embodiments, for example, some or all of the drape 108 may be coated with an acrylic adhesive having a coating weight between about 25 grams per square meter (gsm) to about 65 gsm. Thicker adhesives, or combinations of adhesives, may be applied in some embodiments to improve the seal and reduce leaks. Other example embodiments of an attachment device may include a double-sided tape, paste, hydrocolloid, hydrogel, silicone gel, or organogel.

A “container” broadly includes a canister, pouch, bottle, vial, or other fluid collection apparatus. A container, for example, can be used to manage exudates and other fluids withdrawn from a tissue site. In many environments, a rigid container may be preferred or required for collecting, storing, and disposing of fluids. In other environments, fluids may be properly disposed of without rigid container storage, and a re-usable container could reduce waste and costs associated with negative-pressure therapy. In some embodiments, a container may be a component of a negative-pressure source, such as the negative-pressure source 106.

A “connector,” such as the connector 114, may be used to fluidly couple a tube to a sealed therapeutic environment. The negative pressure developed by a negative-pressure source may be delivered through a tube to a connector. In one illustrative embodiment, a connector may be a T.R.A.C.® Pad or Sensa T.R.A.C.® Pad available from Kinetic Concepts, Inc. of San Antonio, Tex. In one exemplary embodiment, the connector 114 may allow the negative pressure generated by the negative-pressure source 106 to be delivered to the sealed therapeutic environment 118. In other exemplary embodiments, a connector may also be a tube inserted through a drape.

Negative-pressure therapy is increasingly being performed with smaller devices that use battery power rather than a connection to an electrical outlet. Use of battery power decreases the total power supply available to a device. As a result, power drains that would be considered negligible in a device powered through an electrical outlet connection may significantly reduce the performance of a battery-powered device. Power drains may be caused by low-level dressing leaks, for example, which can drain power by repeatedly triggering operation of the a negative-pressure source to maintain a therapeutic negative pressure at the tissue site. Power drains can shorten the useful life of a device by draining the device battery faster, requiring more frequent disposal of the device, recharging of the battery, or battery replacement. Leak detection techniques may help to identify some leaks that may be sealed by the user; however, low-level leaks can challenge the most sensitive leak detection systems and may often go undetected.

Low-level dressing leaks may occur between a drape and epidermis surrounding a tissue site if the drape fails to completely seal to the epidermis. Generally, a drape suitable for covering a tissue site for negative-pressure therapy may comprise a film having a thickness between about 25 microns and about 50 microns that is water-vapor permeable and formed of a polymer. The film, often formed of polyurethane, may be coated with an adhesive having a coating weight between about 25 gsm and about 65 gsm. The adhesive may often be acrylic-based and pressure sensitive. A standard acrylic adhesive may have a bond strength between about 1.8 Newton/centimeter (N/cm) and about 3.8 N/cm on stainless steel substrate at 23° C. at 50% relative humidity based on the American Society for Testing and Materials (“ASTM”) standard ASTM D3330. A pressure-sensitive adhesive increases in bond strength when pressed against the surface to which the adhesive is being bonded. In some applications, a pressure-sensitive adhesive may undergo a physical change when compressed against a surface. In other applications, a pressure-sensitive adhesive may flow into crevices of a surface when compressed, increasing the bond strength without undergoing a physical change. A drape using a standard acrylic adhesive as described above is generally suitable for a dressing where a negative-pressure source powered by a continuous power supply is available to compensate for a dressing leak.

Some drapes may use a bonding adhesive instead of the standard acrylic adhesive. A bonding adhesive may be an adhesive having a bond strength that is greater than the bond strength of a standard acrylic adhesive. In some embodiments, a bonding adhesive may be a type of acrylic adhesive. A bonding adhesive may be better for sealing, but the increased bond strength may cause significantly more discomfort if the drape is removed. In addition, removing a drape having a bonding adhesive may cause significant damage to delicate or damaged skin.

A drape that has a sealing adhesive can fill gaps between the drape and the epidermis to limit leaks and can be easy to remove with low discomfort to the patient. Generally, a sealing adhesive may have a lower bond strength than a standard acrylic adhesive and a bonding adhesive. Generally, a sealing adhesive may flow into gaps and crevices more readily than a standard acrylic adhesive or a bonding adhesive. Various sealing, gap-filling adhesives, such as silicone, hydrocolloids, and hydrogels, have been used but each can have drawbacks. For example, hydrogel adhesives are usually low tack and prone to swelling, creep, and mobility when used with fluid systems. Available hydrogels and hydrocolloids may not adhere well and may move when anchored. In another example, silicone adhesives can fill gaps and seal, but are not breathable and may lose mechanical bonding strength as the silicone adhesives interact with moisture during use. To counter these problems, silicone adhesives may require additional materials to secure the silicone adhesive to a patient. For example, a low-leak drape may be formed from two adhesive layers: a thick sealing adhesive, perhaps in the shape of a gasket or ring, and a thinner bonding adhesive layer used to keep the sealing adhesive in place. Low-leak drapes constructed in this way can be more complex than a drape using a single adhesive, increasing the complexity of manipulation and operation.

A hybrid drape having a thick sealing layer that is perforated and laminated over an adhesive-coated film can overcome many of these challenges. For example, a hybrid drape may include a film layer having a bonding adhesive applied directly to the film layer, and a sealing adhesive applied directly to the bonding adhesive. The sealing adhesive can be perforated to expose the bonding adhesive. When the drape is applied to a patient, the bonding adhesive can be pushed through the perforations of the sealing adhesive to secure the sealing adhesive to the patient. This laminated configuration may provide the benefits of the sealing adhesive and the bonding adhesive over the entire drape area. For example, the laminated configuration may be conformable and of sufficient strength to ensure an initial seal, can inhibit the development of typical low-level leaks, and can mechanically affix to an epidermis without secondary processes. The laminated configuration may also minimize application care by a user and can be removable with minimal trauma to a patient.

However, construction of a laminated configuration can require additional assembly steps and can increase an amount of materials that may be needed for drape construction, which can also significantly increase costs. In addition, as two layers of adhesive are applied to the film layer, the total thickness of the drape can significantly increase, reducing breathability of the drape. Still further, as two full layers of adhesive are applied, significantly more adhesive material is needed to construct the drape.

Other hybrid drapes may register a bonding adhesive and a sealing adhesive. These hybrid drapes apply both a bonding adhesive and a sealing adhesive directly to a film layer. The bonding adhesive and the sealing adhesive may each cover different portions of a film layer to reduce the overall thickness of a hybrid drape and decrease the amount of adhesive needed to construct the hybrid drape. However, the complexity of the manufacturing process may also increase costs relative to other drapes. While using less adhesive than the laminated hybrid drapes, registered hybrid drapes may still use more adhesive in construction than standard drapes.

Some hybrid drapes may use a gel coated mesh having mesh apertures with a diameter between about 5 millimeters (mm) and about 15 mm. However, a gel-coated mesh having apertures of this size may be unable to form a seal with a tissue site. The sealing properties of the gel-coated mesh may be improved by increasing an average diameter of the fibers used to form the mesh; however, the increased diameter of the fibers may also increase a prominence of a mesh where two fibers intersect. A prominence may be a relative height of a feature compared to surrounding features. If two fibers intersect so that a first fiber overlaps a second fiber, a prominence may be a distance between a top of a first fiber and the top of the second fiber. Generally, the prominence at an intersection of two fibers may be the diameter of the largest of the two intersecting fibers. Consequently, if the diameters of the fibers are increased to increase the sealing properties of a gel-coated mesh, the raised contours associated with fiber cross-over may create leaks that are difficult to seal.

As disclosed herein, the negative-pressure therapy system 100 can overcome these challenges and others by providing a substantially flat mesh coated with a sealing adhesive. In some embodiments, for example, the drape 108 may comprise a layer of a bonding adhesive coupled to a film layer, and a mesh layer coupled to the layer of bonding adhesive. The mesh layer may be a mesh formed of small diameter fibers and can be perforated to form bonding apertures. The mesh may be coated with a sealing adhesive.

FIG. 2 is an exploded perspective view, illustrating details that may be associated with some embodiments of the drape 108. The film layer 124 may be liquid-impermeable and vapor-permeable, allowing vapor to egress and inhibiting liquid from exiting. The film layer 124 may be a flexible film that is breathable and may have a high moisture-vapor transfer rate (MVTR). For example, in some embodiments, the MVTR may be greater than or equal to about 300 g/m²/24 hours. The film layer 124 may be formed from a range of medically approved films that typically range in thickness from about 15 microns (μm) to about 50 microns (μm). In other embodiments, a drape having a low MVTR or that allows no vapor transfer may be used. The film layer 124 can also function as a barrier to liquids and microorganisms.

The film layer 124 may be formed from numerous materials, such as one or more of the following: hydrophilic polyurethane (PU), cellulosics, hydrophilic polyamides, polyvinyl alcohol, polyvinyl pyrrolidone, hydrophilic acrylics, hydrophilic silicone elastomers, and copolymers of these. In an illustrative embodiment, the film layer 124 may be formed from a breathable cast matt polyurethane film sold by Expopack Advanced Coatings of Wrexham, United Kingdom, under the name INSPIRE 2301. The illustrative film may have an MVTR (inverted cup technique) of 14400 g/m²/24 hours and may be approximately 30 microns thick.

The bonding adhesive 126 may be coupled directly to the film layer 124. The bonding adhesive 126 may be a medically-acceptable, pressure-sensitive adhesive. For example, the bonding adhesive 126 may be formed from an acrylic adhesive, rubber adhesive, high-tack silicone adhesive, polyurethane, or other substance. In some illustrative embodiments, the bonding adhesive 126 may be formed from an acrylic adhesive with a coating weight of about 15 gsm to about 70 gsm. The bonding adhesive 126 may also be a high-bond strength acrylic adhesive, patterrubber adhesive, high-tack silicone adhesive, or polyurethane, for example. In some embodiments, the bonding adhesive 126 may have a peel adhesion or resistance to being peeled from a stainless steel material between about 6N/25 mm to about 10N/25 mm on stainless steel substrate at 23° C. at 50% relative humidity based on the ASTM D3330.

The bonding adhesive 126 may be a continuous layer of material or may be a layer with apertures (not shown). The apertures may be formed after application of the bonding adhesive 126 or may be formed by coating the bonding adhesive 126 in patterns on a carrier layer. The apertures may be sized to help control the resultant tackiness of the bonding adhesive 126. The apertures may also be sized to enhance the MVTR of the drape 108. The bonding adhesive 126 may couple the film layer 124 to the mesh 128.

In some embodiments, the mesh 128 may be a polymeric mesh, such as Mepitel® produced by Molnlycke Health Care, Adaptic® produced by Systagenix, and Noveface produced by Zodiac Aerospace Group. In some embodiments, the mesh 128 may be substantially flat. For example, the mesh 128 may have a thickness 129, and individual portions of the mesh 128 may have a minimal tolerance from the thickness 129. In some embodiments, the thickness 129 of the mesh 128 may be about 1 mm, and the tolerance of the thickness 129 may be less than about 2 mm. In another exemplary embodiment, a tolerance of the thickness 129 of the mesh 128 may be less than about 1 mm. In other embodiments, a tolerance of the thickness 129 of the mesh 128 may be less than about 0.5 mm. In some embodiments, the mesh 128 may be formed with bonding apertures 134. The bonding apertures 134 may be numerous shapes, for example, circles, squares, stars, ovals, polygons, slits, complex curves, rectilinear shapes, triangles, or other shapes.

FIG. 3A is a plan view, illustrating details that may be associate with some embodiments of the mesh 128. Generally, a mesh may include a structure of connected strands of metal, fiber, or other flexible or ductile material having openings between the strands. In some embodiments, a mesh may have evenly spaced openings between adjacent strands. In some embodiments, the mesh 128 may have a plurality of fibers 136. In some embodiments, the fibers 136 may be formed from a monofilament, a plurality of twisted monofilaments, a plurality of filaments, or a plurality of staple fibers. A filament may be a fiber that is formed in a continuous or near-continuous length. A monofilament may be a single filament. In some embodiments, a monofilament may be made from a single synthetic fiber of plastic, for example. Monofilaments may have a tensile strength related to a diameter of the monofilament and the type of material from which the monofilament is formed. A staple fiber may be a fiber of a selected standardized length, and the staple fiber may be formed of a suitable composition for used with a medical device. Each of the fibers 136 may have a diameter 127. In some embodiments, the diameter 127 may be no greater than about 1 mm. The fibers 136 may be formed from a range of materials including, but not limited to, silicone, cellulose acetate, and other similar materials.

In some embodiments, antimicrobial agents may be added to the mesh 128. In other embodiments, the fibers 136 may have antimicrobial properties. For example, in some embodiments, silver ions may be added to the fibers 136. In still other embodiments, the fibers 136 may be formed from elastomers to permit easier coverage of complex contours.

The plurality of fibers 136 may be woven, knitted, knotted, linked or otherwise connected to form a regular pattern of mesh apertures. In some embodiments, each of the plurality of fibers 136 may be separated from adjacent fibers 136 to form mesh apertures 139. In some embodiments, the fibers 136 may be separated a distance 138 from adjacent fibers, which may be between about 0.5 mm and about 4 mm. In some embodiments, each of the fibers 136 may be separated from adjacent fibers in a second direction by a distance 140. In some embodiments, the distance 140 may be between about 0.5 mm and about 4 mm. In some embodiments, the first direction of the distance 138 and the second direction of the distance 140 may be perpendicular. In some embodiments, the distance 138 and the distance 140 may be the same. In other embodiments, the first direction of the distance 138 and the second direction of the distance 140 may be other angles, and the distance 138 and the distance 140 may not be the same.

In some embodiments, the mesh apertures 139 may have an average effective diameter of about 1 mm. An effective diameter of a non-circular area may be a diameter of a circular area having the same surface area as the non-circular area. For example, the surface area of a mesh aperture 139 where the distance 138 is 0.5 mm and the distance 140 is 0.5 mm may be 0.25 mm². The diameter of a circular area having a 0.25 mm²surface area is about 0.56 mm; consequently, the effective diameter of the exemplary mesh aperture 139 is about 0.56 mm. Similarly, if the distance 138 is about 4 mm and the distance 140 is about 4 mm, the effective diameter of the mesh aperture 139 may be about 4.51 mm.

In some embodiments, the mesh 128 may include the bonding apertures 134. The bonding apertures 134 may have a uniform pattern or may be randomly distributed on the mesh 128. The bonding apertures 134 may be formed through one or more fibers 136. In some embodiments, the bonding apertures 134 may extend into the mesh apertures 139. Each bonding aperture 134 of the plurality of bonding apertures 134 may have an effective diameter. The average effective diameter of each bonding aperture 134 may be in the range of about 5 mm to about 15 mm.

In some embodiments, the mesh 128 may be coated with a gel, such as a sealing adhesive 144. In some embodiments, the sealing adhesive 144 may have a coating weight of about 100 gsm to about 500 gsm. In other embodiments, the sealing adhesive 144 may have a coating weight greater than about 200 gsm. The coating of the mesh 128 with the sealing adhesive 144 may fill in a portion of each mesh aperture 139. In some embodiments, the mesh apertures 139 may remain at least partially open after the coating of the mesh 128 with the sealing adhesive 144.

A sealing adhesive may be a soft material that provides a good seal with the tissue site 102. A sealing adhesive may be formed of a silicone gel (or soft silicone), hydrocolloid, hydrogel, polyurethane gel, polyolefin gel, hydrogenated styrenic copolymer gels, or foamed gels with compositions as listed, or soft closed cell foams (polyurethanes, polyolefins) coated with an adhesive (for example, 30 gsm-70 gsm acrylic), polyurethane, polyolefin, or hydrogenated styrenic copolymers. In some embodiments, a sealing adhesive may have a stiffness between about 5 Shore OO and about 80 Shore OO. A sealing adhesive may be hydrophobic or hydrophilic. A sealing adhesive may be an adhesive having a low to medium tackiness, for example, a silicone polymer, polyurethane, or an additional acrylic adhesive. In some embodiments, a sealing adhesive may a bond strength between about 0.5N/25 mm and about 1.5N/25 mm on a stainless steel substrate at 23° C. at 50% relative humidity based on ASTM D3330. A sealing adhesive may have a tackiness such that the sealing adhesive may achieve the bond strength above after a contact time of less than 60 seconds. Tackiness may be considered a bond strength of an adhesive after a very low contact time between the adhesive and a substrate. In an illustrative embodiment, a sealing adhesive may have a tackiness that may be about 30% to about 50% of the tackiness of a bonding adhesive.

In some embodiments, the bonding apertures 134 may be formed prior to coating of the mesh 128 with the sealing adhesive 144. In other embodiments, the bonding apertures 134 may be formed in the mesh 128 following coating of the mesh 128 with the sealing adhesive 144.

In some embodiments, the fibers 136 of the mesh 128 may form a plurality of intersections 142. In some embodiments, an intersection 142 may be a location of the mesh 128 where at least two fibers 136 overlap, cross-over, or meet, for example.

FIG. 3B is a perspective view, illustrating additional details that may be associated with some embodiments of the mesh 128 of FIG. 3A. In some embodiments, the mesh 128 may be formed so that at each intersection 142, the intersecting fibers 136 may be fused so that the intersection 142 is planar. In some embodiments, the mesh 128 may be molded, extruded, or expanded to form the mesh 128. In embodiments where the mesh 128 is molded, extruded, or expanded, the fibers 136 at an intersection 142 may be fused or joined so that a prominence at the intersection 142 is less than about 1 mm. In some embodiments, the prominence at an intersection 142 may be about 0 mm. In some embodiments, a substantially flat mesh may have a thickness at the intersections 142 that may be substantially the same as a thickness of the mesh 128 surrounding the intersections 142.

FIG. 3C is a side elevation view, illustrating additional details that may be associated with some embodiments of the mesh 128. In some embodiments, the mesh 128 may be formed by weaving or knitting the fibers 136. If the fibers 136 are woven or knitted, the intersections 142 may have a prominence 141. In some embodiments, the prominence 141 of the fibers 136 at the intersections 142 may be equal to the diameter 127 of the fibers 136. In some embodiments, the prominence 141 may be reduced by compressing the mesh 128 following weaving or knitting the fibers 136. The prominences 141 of the fibers 136 may also be reduced by passing the mesh 128 through a calender, which may apply pressure to the mesh 128 to smooth out the mesh 128. In some embodiments, the prominence 141 may be less than about 1 mm.

FIG. 4 is a sectional view, illustrating additional details that may be associated with some embodiments of the drape 108. In the assembled state, the bonding adhesive 126 may be coupled to the film layer 124, and the mesh 128 may be coupled to the bonding adhesive 126. If the mesh 128 is placed proximate to or in contact with the epidermis 116, the sealing adhesive 144 coating the mesh 128 may form sealing couplings 146 with the epidermis 116. In some embodiments, the diameter 127 of the fibers 136, the thickness of the sealing adhesive 144, and the bonding apertures 134 may create a gap 148 between the bonding adhesive 126 and the epidermis 116.

FIG. 5 is a sectional view, illustrating additional details that may be associated with some embodiments of the drape 108 of FIG. 4 in a second position. If the drape 108 is in a desired location, pressure may be applied to the film layer 124. The pressure may cause the bonding adhesive 126 to be pressed at least partially into contact with the epidermis 116 to form bonding couplings 150. The bonding couplings 150 may provide secure, releasable mechanical fixation to the epidermis 116. The sealing couplings 146 between the sealing adhesive 144 and the epidermis 116 may be sufficient to seal the film layer 124 to the epidermis 116. The sealing couplings 146 may not be as mechanically strong as the bonding couplings 150 between the bonding adhesive 126 and the epidermis 116. The bonding couplings 150 may also anchor the drape 108 to the epidermis 116, inhibiting migration of the drape 108 and the sealing adhesive 144.

The average effective diameter of the bonding apertures 134 of the sealing adhesive 144 may be varied as one control of the tackiness or adhesion strength of the drape 108. In this regard, there may be an interplay between three main variables for each embodiment: the diameter 127 of the fibers 136, the average effective diameter of the plurality of bonding apertures 134, and the tackiness of the bonding adhesive 126. The more bonding adhesive 126 that extends through the bonding apertures 134, the stronger the bonding coupling 150. The smaller the diameter 127 of the fibers 136, the more the bonding adhesive 126 generally extends through the bonding apertures 134 and the greater the bonding coupling 150. As an example of the interplay, if a very tacky bonding adhesive 126 is used and the diameter 127 of the fibers 136 of the mesh 128 is small, the average effective diameter of the plurality of bonding apertures 134 may be relatively smaller to maintain a same adhesion strength of the drape 108.

In other embodiments, the mesh 128 may be formed from a perforated film which is then coated with the sealing adhesive 144 and laminated to the film layer 124 or the bonding adhesive 126. In other embodiments, the mesh 128 may be coated with the bonding adhesive 126 and then pattern-coated with the sealing adhesive 144. The mesh 128 may then be laminated directly to the film layer 124. The bonding adhesive 126 may be exposed through the areas of the mesh 128 that were not pattern-coated with the sealing adhesive 144.

In some embodiments, the adhesives may be mixed with blowing or expanding agents, for example organic and inorganic low temperature boiling point liquids. The blowing or expanding agents allow for the adhesives to expand under the application of heat or light to increase the thickness of the adhesive following deposition by one of the above described processes. The blowing or expanding agents may reduce the amount of adhesive needed and decrease the cost of production. In some embodiments, the application of heat or light may be delayed until application of the drape 108 to the epidermis 116 so that the contact area with the epidermis 116 may increase as the bonding adhesive 126 and the sealing adhesive 144 warm by contact with the epidermis 116. The application of light or heat following application of the drape 108 to the epidermis 116 can provide a better seal for some embodiments of the drape 108 to the epidermis 116.

A drape having a coated mesh may provide a lower cost solution that makes more efficient use of a sealing adhesive. The increase in efficiency of the use of a sealing adhesive may be accomplished without the complication of adding extruders and pattern coaters that may be required for pattern printing of adhesives. A drape having a coated mesh may have a higher MVTR than other drapes as the inclusion of mesh apertures can permit greater passage of moisture without interfering with sealing.

Although certain features and their advantages have been disclosed in the context of certain illustrative, non-limiting embodiments, it should be understood that various changes, substitutions, permutations, and alterations can be made without departing from the scope of the appended claims. It will be appreciated that features that may be described in connection to one embodiment may also be applicable to other embodiments. It will also be understood that the benefits and advantages described above may relate to one embodiment or may relate to several embodiments. It will further be understood that reference to “an” item refers to one or more of those items.

The steps of the methods described herein may be carried out in a suitable order, or simultaneously where appropriate.

Where appropriate, aspects of the embodiments described above may be combined with aspects of the other embodiments described to form further examples having comparable or different properties and addressing the same or different problems.

It will be understood that the embodiments described herein are given by way of example only and that various modifications may be made by those skilled in the art. The above specification, examples and data provide a complete description of the structure and use of exemplary embodiments. Although various embodiments have been described above with a certain degree of particularity, or with reference to one or more individual illustrations, those skilled in the art could make numerous alterations to the example embodiments without departing from the scope of the claims.

Claims

1. A dressing for treating a tissue site with negative pressure, the dressing comprising: a manifold configured to be positioned adjacent to the tissue site, the manifold having a plurality of pathways configured to distribute negative pressure across the tissue site; anda sealing member configured to be positioned over the tissue interface and the tissue site to form a sealed environment, the sealing member comprising: a film layer having a first side and a second side,a layer of a bonding adhesive having a first side coupled to the second side of the film layer and a second side, anda mesh coupled to the second side of the layer of the bonding adhesive, the mesh having a coating of a sealing adhesive and one or more bonding apertures,wherein the film layer, the layer of the bonding adhesive, and the mesh are congruent layers and the layer of the bonding adhesive separates the film layer from the mesh.
2. The dressing of claim 1, wherein the mesh comprises a plurality of fibers connected to form intersections.
3. The dressing of claim 2, wherein each intersection of the fibers is substantially flat.
4. The dressing of claim 2, wherein a prominence of the fibers at each intersection is less than about 1 millimeter.
5. The dressing of claim 2, wherein the fibers are woven.
6. The dressing of claim 2, wherein the fibers are knitted.
7. The dressing of claim 2, wherein the fibers are extruded and are substantially planar at each intersection.
8. The dressing of claim 2, wherein a diameter of each fiber of the plurality of fibers is less than about 1 millimeter.
9. The dressing of claim 2, wherein each fiber of the plurality of fibers is a monofilament.
10. The dressing of claim 2, wherein each fiber of the plurality of fibers is a plurality of twisted monofilaments.
11. The dressing of claim 2, wherein each fiber of the plurality of fibers is a plurality of staple fibers.
12. The dressing of claim 1, wherein the mesh has a plurality of mesh apertures.
13. The dressing of claim 12, wherein an effective diameter of each mesh aperture is between about 0.5 millimeters and about 4 millimeter.
14. The dressing of claim 1, wherein a coating weight of the coating of the sealing adhesive is between about 100 grams per square meter and about 500 grams per square meter.
15. The dressing of claim 1, wherein an effective diameter of each bonding aperture is between about 5 millimeter and about 15 millimeter.
16. The dressing of claim 1, wherein the mesh comprises a polymeric mesh.
17. The dressing of claim 1, wherein: the film layer comprises a polyurethane film having a thickness between about 15 microns and about 50 microns;the bonding adhesive comprises an acrylic adhesive having a coating weight between about 15 grams per square meter and about 70 grams per square meter;the mesh comprises a silicone mesh having mesh apertures with an effective diameter between about 0.5 millimeters and about 4.5 millimeters; andthe sealing adhesive comprises a silicone gel adhesive having a coating weight between about 100 grams per square meter and about 500 grams per square meter.
18. A system for treating a tissue site with negative-pressure, the system comprising: a manifold configured to be positioned adjacent to the tissue site, the manifold having a plurality of pathways configured to distribute negative pressure across the tissue site;a drape configured to be positioned over the tissue site and the manifold to form a sealed space; anda negative-pressure source configured to provide negative-pressure to the sealed space;wherein the drape comprises: a film layer having a first side and a second side,a layer of a bonding adhesive having a first side coupled to the film layer and a second side,a mesh coupled to the second side of the layer of the bonding adhesive, the mesh having a coating of a sealing adhesive and one or more bonding apertures,wherein the film layer, the layer of the bonding adhesive, and the mesh are congruent layers and the layer of the bonding adhesive separates the film layer from the mesh.
19. The system of claim 18, wherein the mesh comprises a plurality of fibers connected to form intersections.
20. The system of claim 19, wherein each intersection of the fibers is substantially flat.
21. The system of claim 19, wherein a prominence of the fibers at each intersection is less than about 1 millimeter.
22. The system of claim 19, wherein the fibers are woven.
23. The system of claim 19, wherein the fibers are knitted.
24. The system of claim 19, wherein the fibers are extruded and are substantially planar at each intersection.
25. The system of claim 19, wherein a diameter of each fiber of the plurality of fibers is less than about 1 millimeter.
26. The system of claim 19, wherein each fiber of the plurality of fibers is a monofilament.
27. The system of claim 19, wherein each fiber of the plurality of fibers is a plurality of twisted monofilaments.
28. The system of claim 19, wherein each fiber of the plurality of fibers is a plurality of staple fibers.
29. The system of claim 18, wherein the mesh has a plurality of mesh apertures.
30. The system of claim 29, wherein an effective diameter of each mesh aperture is between about 0.5 millimeter and about 4 millimeter.
31. The system of claim 18, wherein a coating weight of the coating of the sealing adhesive is between about 100 grams per square meter and about 500 grams per square meter.
32. The system of claim 18, wherein an effective diameter of each bonding aperture is between about 5 millimeter and about 15 millimeter.
33. The system of claim 18, wherein the mesh comprises a polymeric mesh.
34. The system of claim 18, wherein: the film layer comprises a polyurethane film having a thickness between about 15 microns and about 50 microns;the bonding adhesive comprises an acrylic adhesive having a coating weight between about 15 grams per square meter and about 70 grams per square meter;the mesh comprises a silicone mesh having mesh apertures with an effective diameter between about 0.5 millimeters and about 4.5 millimeters; andthe sealing adhesive comprises a silicone gel adhesive having a coating weight between about 100 grams per square meter and about 500 grams per square meter.

CROSS-REFERENCE TO RELATED APPLICATIONS

This application claims priority to and the benefit of U.S. Provisional Patent Application No. 61/945,882, filed Feb. 28, 2014, entitled “HYBRID DRAPE HAVING A GEL-COATED PERFORATED MESH,” to Christopher Brian Locke and Timothy Mark Robinson, which is hereby incorporated by reference.

US Referenced Citations (407)

Number	Name	Date	Kind
1355846	Rannells	Oct 1920	A
1944834	Bennett	Jan 1934	A
2547758	Keeling	Apr 1951	A
2552664	Burdine	May 1951	A
2632443	Lesher	Mar 1953	A
2682873	Evans et al.	Jul 1954	A
2860081	Eiken	Nov 1958	A
2910763	Lauterbach	Nov 1959	A
2969057	Simmons	Jan 1961	A
3066672	Crosby, Jr. et al.	Dec 1962	A
3172808	Baumann et al.	Mar 1965	A
3183116	Schaar	May 1965	A
3367332	Groves	Feb 1968	A
3376868	Mondiadis	Apr 1968	A
3520300	Flower, Jr.	Jul 1970	A
3568675	Harvey	Mar 1971	A
3648692	Wheeler	Mar 1972	A
3682180	McFarlane	Aug 1972	A
3742952	Magers et al.	Jul 1973	A
3774611	Tussey et al.	Nov 1973	A
3777016	Gilbert	Dec 1973	A
3779243	Tussey et al.	Dec 1973	A
3826254	Mellor	Jul 1974	A
3852823	Jones	Dec 1974	A
3903882	Augurt	Sep 1975	A
3967624	Milnamow	Jul 1976	A
3983297	Ono et al.	Sep 1976	A
4060081	Yannas et al.	Nov 1977	A
4080970	Miller	Mar 1978	A
4096853	Weigand	Jun 1978	A
4139004	Gonzalez, Jr.	Feb 1979	A
4141361	Snyder	Feb 1979	A
4163822	Walter	Aug 1979	A
4165748	Johnson	Aug 1979	A
4184510	Murry et al.	Jan 1980	A
4233969	Lock et al.	Nov 1980	A
4245630	Lloyd et al.	Jan 1981	A
4256109	Nichols	Mar 1981	A
4261363	Russo	Apr 1981	A
4275721	Olson	Jun 1981	A
4284079	Adair	Aug 1981	A
4297995	Golub	Nov 1981	A
4333468	Geist	Jun 1982	A
4360015	Mayer	Nov 1982	A
4373519	Errede et al.	Feb 1983	A
4382441	Svedman	May 1983	A
4392853	Muto	Jul 1983	A
4392858	George et al.	Jul 1983	A
4414970	Berry	Nov 1983	A
4419097	Rowland	Dec 1983	A
4465485	Kashmer et al.	Aug 1984	A
4475909	Eisenberg	Oct 1984	A
4480638	Schmid	Nov 1984	A
4525166	Leclerc	Jun 1985	A
4525374	Vaillancourt	Jun 1985	A
4529402	Weilbacher et al.	Jul 1985	A
4540412	Van Overloop	Sep 1985	A
4543100	Brodsky	Sep 1985	A
4548202	Duncan	Oct 1985	A
4551139	Plaas et al.	Nov 1985	A
4569348	Hasslinger	Feb 1986	A
4600146	Ohm	Jul 1986	A
4605399	Weston et al.	Aug 1986	A
4608041	Nielsen	Aug 1986	A
4617021	Leuprecht	Oct 1986	A
4640688	Hauser	Feb 1987	A
4655754	Richmond et al.	Apr 1987	A
4664652	Weilbacher	May 1987	A
4664662	Webster	May 1987	A
4710165	McNeil et al.	Dec 1987	A
4715857	Juhasz et al.	Dec 1987	A
4733659	Edenbaum et al.	Mar 1988	A
4743232	Kruger	May 1988	A
4753230	Carus et al.	Jun 1988	A
4753232	Ward	Jun 1988	A
4758220	Sundblom et al.	Jul 1988	A
4787888	Fox	Nov 1988	A
4826494	Richmond et al.	May 1989	A
4832008	Gilman	May 1989	A
4838883	Matsuura	Jun 1989	A
4840187	Brazier	Jun 1989	A
4848364	Bosman	Jul 1989	A
4863449	Therriault et al.	Sep 1989	A
4871611	LeBel	Oct 1989	A
4872450	Austad	Oct 1989	A
4878901	Sachse	Nov 1989	A
4897081	Poirier et al.	Jan 1990	A
4906233	Moriuchi et al.	Mar 1990	A
4906240	Reed et al.	Mar 1990	A
4919654	Kalt et al.	Apr 1990	A
4930997	Bennett	Jun 1990	A
4941882	Ward et al.	Jul 1990	A
4953565	Tachibana et al.	Sep 1990	A
4961493	Kaihatsu	Oct 1990	A
4969880	Zamierowski	Nov 1990	A
4981474	Bopp et al.	Jan 1991	A
4985019	Michelson	Jan 1991	A
4995382	Lang et al.	Feb 1991	A
4996128	Aldecoa et al.	Feb 1991	A
5010883	Rawlings et al.	Apr 1991	A
5018515	Gilman	May 1991	A
5025783	Lamb	Jun 1991	A
5028597	Kodama et al.	Jul 1991	A
5037397	Kalt et al.	Aug 1991	A
5086170	Luheshi et al.	Feb 1992	A
5092323	Riedel et al.	Mar 1992	A
5092858	Benson et al.	Mar 1992	A
5100396	Zamierowski	Mar 1992	A
5112323	Winkler et al.	May 1992	A
5134994	Say	Aug 1992	A
5149331	Ferdman et al.	Sep 1992	A
5151314	Brown	Sep 1992	A
5152757	Eriksson	Oct 1992	A
5167613	Karami et al.	Dec 1992	A
5176663	Svedman et al.	Jan 1993	A
5180375	Feibus	Jan 1993	A
5215522	Page et al.	Jun 1993	A
5232453	Plass et al.	Aug 1993	A
5246775	Loscuito	Sep 1993	A
5261893	Zamierowski	Nov 1993	A
5266372	Arakawa et al.	Nov 1993	A
5270358	Asmus	Dec 1993	A
5278100	Doan et al.	Jan 1994	A
5279550	Habib et al.	Jan 1994	A
5298015	Komatsuzaki et al.	Mar 1994	A
5342329	Croquevielle	Aug 1994	A
5342376	Ruff	Aug 1994	A
5344415	DeBusk et al.	Sep 1994	A
5356386	Goldberg et al.	Oct 1994	A
5358494	Svedman	Oct 1994	A
5384174	Ward et al.	Jan 1995	A
5387207	Dyer et al.	Feb 1995	A
5419769	Devlin et al.	May 1995	A
5423778	Eriksson et al.	Jun 1995	A
5429590	Saito et al.	Jul 1995	A
5437622	Carion	Aug 1995	A
5437651	Todd et al.	Aug 1995	A
5445604	Lang	Aug 1995	A
5447492	Cartmell	Sep 1995	A
5458938	Nygard et al.	Oct 1995	A
5501212	Psaros	Mar 1996	A
5522808	Skalla	Jun 1996	A
5527293	Zamierowski	Jun 1996	A
5549584	Gross	Aug 1996	A
5549585	Maher et al.	Aug 1996	A
5556375	Ewall	Sep 1996	A
5585178	Calhoun et al.	Dec 1996	A
5599292	Yoon	Feb 1997	A
5607388	Ewall	Mar 1997	A
5611373	Ashcraft	Mar 1997	A
5634893	Rishton	Jun 1997	A
5636643	Argenta et al.	Jun 1997	A
5641506	Talke et al.	Jun 1997	A
5645081	Argenta et al.	Jul 1997	A
5653224	Johnson	Aug 1997	A
5678564	Lawrence et al.	Oct 1997	A
5710233	Meckel et al.	Jan 1998	A
5714225	Hansen et al.	Feb 1998	A
5736470	Schneberger et al.	Apr 1998	A
5759570	Arnold	Jun 1998	A
5776119	Bilbo et al.	Jul 1998	A
5807295	Hutcheon et al.	Sep 1998	A
5830201	George et al.	Nov 1998	A
5878971	Minnema	Mar 1999	A
5902439	Pike et al.	May 1999	A
5919476	Fischer et al.	Jul 1999	A
5941863	Guidotti et al.	Aug 1999	A
5964252	Simmons et al.	Oct 1999	A
5981822	Addison	Nov 1999	A
5998561	Jada	Dec 1999	A
6071267	Zamierowski	Jun 2000	A
6086995	Smith	Jul 2000	A
6135116	Vogel et al.	Oct 2000	A
6174306	Fleischmann	Jan 2001	B1
6191335	Robinson	Feb 2001	B1
6201164	Wulff et al.	Mar 2001	B1
6238762	Friedland et al.	May 2001	B1
6241747	Ruff	Jun 2001	B1
6262329	Brunsveld et al.	Jul 2001	B1
6287316	Agarwal et al.	Sep 2001	B1
6345623	Heaton et al.	Feb 2002	B1
6458109	Henley et al.	Oct 2002	B1
6488643	Tumey et al.	Dec 2002	B1
6493568	Bell et al.	Dec 2002	B1
6495229	Carte et al.	Dec 2002	B1
6503855	Menzies et al.	Jan 2003	B1
6548727	Swenson	Apr 2003	B1
6553998	Heaton et al.	Apr 2003	B2
6566575	Stickels et al.	May 2003	B1
6566577	Addison et al.	May 2003	B1
6626891	Ohmstede	Sep 2003	B2
6627215	Dale	Sep 2003	B1
6648862	Watson	Nov 2003	B2
6680113	Lucast et al.	Jan 2004	B1
6685681	Lockwood et al.	Feb 2004	B2
6693180	Lee et al.	Feb 2004	B2
6695823	Lina et al.	Feb 2004	B1
6752794	Lockwood et al.	Jun 2004	B2
6787682	Gilman	Sep 2004	B2
6814079	Heaton et al.	Nov 2004	B2
6855135	Lockwood et al.	Feb 2005	B2
6856821	Johnson	Feb 2005	B2
6979324	Bybordi et al.	Dec 2005	B2
7070584	Johnson et al.	Jul 2006	B2
7154017	Sigurjonsson et al.	Dec 2006	B2
7402721	Sigurjonsson et al.	Jul 2008	B2
7569742	Haggstrom et al.	Aug 2009	B2
7645269	Zamierowski	Jan 2010	B2
7846141	Weston	Dec 2010	B2
8062273	Weston	Nov 2011	B2
8216198	Heagle et al.	Jul 2012	B2
8251979	Malhi	Aug 2012	B2
8257327	Blott et al.	Sep 2012	B2
8298197	Eriksson et al.	Oct 2012	B2
8398614	Blott et al.	Mar 2013	B2
8449509	Weston	May 2013	B2
8529532	Pinto	Sep 2013	B2
8529548	Blott et al.	Sep 2013	B2
8535296	Blott et al.	Sep 2013	B2
8551060	Schuessler et al.	Oct 2013	B2
8568386	Malhi	Oct 2013	B2
8632523	Eriksson et al.	Jan 2014	B2
8679081	Heagle et al.	Mar 2014	B2
8764732	Hartwell	Jul 2014	B2
8834451	Blott et al.	Sep 2014	B2
8920830	Mathies	Dec 2014	B2
8926592	Blott et al.	Jan 2015	B2
9017302	Vitaris et al.	Apr 2015	B2
9192444	Locke et al.	Nov 2015	B2
9198801	Weston	Dec 2015	B2
9211365	Weston	Dec 2015	B2
9289542	Blott et al.	Mar 2016	B2
9877873	Coulthard et al.	Jan 2018	B2
9956120	Locke	May 2018	B2
20010030304	Kohda et al.	Oct 2001	A1
20010051178	Blatchford et al.	Dec 2001	A1
20020009568	Bries et al.	Jan 2002	A1
20020016346	Brandt et al.	Feb 2002	A1
20020065494	Lockwood et al.	May 2002	A1
20020077661	Saadat	Jun 2002	A1
20020090496	Kim et al.	Jul 2002	A1
20020115951	Norstrem et al.	Aug 2002	A1
20020119292	Venkatasanthanam et al.	Aug 2002	A1
20020120185	Johnson	Aug 2002	A1
20020130064	Adams et al.	Sep 2002	A1
20020143286	Tumey	Oct 2002	A1
20020150270	Werner	Oct 2002	A1
20020150720	Howard et al.	Oct 2002	A1
20020161346	Lockwood et al.	Oct 2002	A1
20020164346	Nicolette	Nov 2002	A1
20020183702	Henley et al.	Dec 2002	A1
20020198504	Risk et al.	Dec 2002	A1
20030014022	Lockwood et al.	Jan 2003	A1
20030109855	Solem et al.	Jun 2003	A1
20030158577	Ginn et al.	Aug 2003	A1
20030212357	Pace	Nov 2003	A1
20030225347	Argenta et al.	Dec 2003	A1
20030225355	Butler	Dec 2003	A1
20040002676	Siegwart et al.	Jan 2004	A1
20040030304	Hunt et al.	Feb 2004	A1
20040064132	Boehringer et al.	Apr 2004	A1
20040077984	Worthley	Apr 2004	A1
20040082925	Patel	Apr 2004	A1
20040099268	Smith et al.	May 2004	A1
20040118401	Smith et al.	Jun 2004	A1
20040127836	Sigurjonsson et al.	Jul 2004	A1
20040127862	Bubb et al.	Jul 2004	A1
20040133143	Burton et al.	Jul 2004	A1
20040186239	Qin et al.	Sep 2004	A1
20040219337	Langley et al.	Nov 2004	A1
20040230179	Shehada	Nov 2004	A1
20050034731	Rousseau et al.	Feb 2005	A1
20050054998	Poccia et al.	Mar 2005	A1
20050059918	Sigurjonsson et al.	Mar 2005	A1
20050065484	Watson	Mar 2005	A1
20050070858	Lockwood et al.	Mar 2005	A1
20050101940	Radl et al.	May 2005	A1
20050113732	Lawry	May 2005	A1
20050124925	Scherpenborg	Jun 2005	A1
20050131327	Lockwood et al.	Jun 2005	A1
20050137539	Biggie et al.	Jun 2005	A1
20050143694	Schmidt et al.	Jun 2005	A1
20050159695	Cullen et al.	Jul 2005	A1
20050161042	Fudge et al.	Jul 2005	A1
20050163978	Strobech et al.	Jul 2005	A1
20050214376	Faure et al.	Sep 2005	A1
20050233072	Stephan et al.	Oct 2005	A1
20050256437	Silcock et al.	Nov 2005	A1
20050261642	Weston	Nov 2005	A1
20050261643	Bybordi et al.	Nov 2005	A1
20050277860	Jensen	Dec 2005	A1
20060014030	Langen et al.	Jan 2006	A1
20060020235	Siniaguine	Jan 2006	A1
20060079852	Bubb et al.	Apr 2006	A1
20060083776	Bott	Apr 2006	A1
20060154546	Murphy et al.	Jul 2006	A1
20060236979	Stolarz et al.	Oct 2006	A1
20060241542	Gudnason et al.	Oct 2006	A1
20060271020	Huang et al.	Nov 2006	A1
20070027414	Hoffman et al.	Feb 2007	A1
20070078366	Haggstrom et al.	Apr 2007	A1
20070161937	Aali	Jul 2007	A1
20070185426	Ambrosio et al.	Aug 2007	A1
20070225663	Watt et al.	Sep 2007	A1
20070265585	Joshi et al.	Nov 2007	A1
20070265586	Joshi et al.	Nov 2007	A1
20080009812	Riesinger	Jan 2008	A1
20080027366	Da Silva Macedo	Jan 2008	A1
20080090085	Kawate et al.	Apr 2008	A1
20080119802	Riesinger	May 2008	A1
20080138591	Graham et al.	Jun 2008	A1
20080149104	Eifler	Jun 2008	A1
20080173389	Mehta et al.	Jul 2008	A1
20080195017	Robinson et al.	Aug 2008	A1
20080225663	Smith et al.	Sep 2008	A1
20080243044	Hunt et al.	Oct 2008	A1
20080269657	Brenneman et al.	Oct 2008	A1
20080271804	Biggie et al.	Nov 2008	A1
20090025724	Herron, Jr.	Jan 2009	A1
20090088719	Driskell	Apr 2009	A1
20090093779	Riesinger	Apr 2009	A1
20090124988	Coulthard	May 2009	A1
20090177172	Wilkes	Jul 2009	A1
20090216168	Eckstein	Aug 2009	A1
20090216170	Robinson et al.	Aug 2009	A1
20090216204	Bhavaraju et al.	Aug 2009	A1
20090227969	Jaeb et al.	Sep 2009	A1
20090234306	Vitaris	Sep 2009	A1
20090234307	Vitaris	Sep 2009	A1
20090264807	Haggstrom et al.	Oct 2009	A1
20090292264	Hudspeth et al.	Nov 2009	A1
20090312662	Colman et al.	Dec 2009	A1
20090326487	Vitaris	Dec 2009	A1
20090326488	Budig et al.	Dec 2009	A1
20100028390	Cleary et al.	Feb 2010	A1
20100030170	Keller et al.	Feb 2010	A1
20100063467	Addison et al.	Mar 2010	A1
20100106106	Heaton et al.	Apr 2010	A1
20100106118	Heaton et al.	Apr 2010	A1
20100125259	Olson	May 2010	A1
20100159192	Cotton	Jun 2010	A1
20100185163	Heagle	Jul 2010	A1
20100226824	Ophir et al.	Sep 2010	A1
20100262090	Riesinger	Oct 2010	A1
20100267302	Kantner et al.	Oct 2010	A1
20100268144	Lu et al.	Oct 2010	A1
20100286582	Simpson et al.	Nov 2010	A1
20100305490	Coulthard et al.	Dec 2010	A1
20100305524	Vess et al.	Dec 2010	A1
20100318072	Johnston et al.	Dec 2010	A1
20100324516	Braga et al.	Dec 2010	A1
20110046585	Weston	Feb 2011	A1
20110137271	Andresen et al.	Jun 2011	A1
20110160686	Ueda et al.	Jun 2011	A1
20110171480	Mori et al.	Jul 2011	A1
20110172617	Riesinger	Jul 2011	A1
20110201984	Dubrow et al.	Aug 2011	A1
20110224631	Simmons et al.	Sep 2011	A1
20110229688	Cotton	Sep 2011	A1
20110244010	Doshi	Oct 2011	A1
20110257612	Locke et al.	Oct 2011	A1
20110257617	Franklin	Oct 2011	A1
20110282309	Adie et al.	Nov 2011	A1
20120016322	Coulthard et al.	Jan 2012	A1
20120019031	Bessert	Jan 2012	A1
20120036733	Dehn	Feb 2012	A1
20120040131	Speer	Feb 2012	A1
20120059339	Gundersen	Mar 2012	A1
20120123359	Reed	May 2012	A1
20120143157	Riesinger	Jun 2012	A1
20120258271	Maughan	Oct 2012	A1
20120310186	Moghe et al.	Dec 2012	A1
20130030394	Locke et al.	Jan 2013	A1
20130053746	Roland	Feb 2013	A1
20130066285	Locke et al.	Mar 2013	A1
20130096518	Hall et al.	Apr 2013	A1
20130150763	Mirzaei et al.	Jun 2013	A1
20130152945	Locke et al.	Jun 2013	A1
20130172843	Kurata	Jul 2013	A1
20130189339	Vachon	Jul 2013	A1
20130261585	Lee	Oct 2013	A1
20140039423	Riesinger	Feb 2014	A1
20140039424	Locke	Feb 2014	A1
20140058309	Addison et al.	Feb 2014	A1
20140107561	Dorian et al.	Apr 2014	A1
20140107562	Dorian et al.	Apr 2014	A1
20140141197	Hill et al.	May 2014	A1
20140155849	Heaton et al.	Jun 2014	A1
20140163491	Schuessler et al.	Jun 2014	A1
20140171851	Addison	Jun 2014	A1
20140178564	Patel	Jun 2014	A1
20140309574	Cotton	Oct 2014	A1
20140336557	Durdag et al.	Nov 2014	A1
20140350494	Hartwell et al.	Nov 2014	A1
20140352073	Goenka	Dec 2014	A1
20150030848	Goubard	Jan 2015	A1
20150057625	Coulthard	Feb 2015	A1
20150080788	Blott et al.	Mar 2015	A1
20150080815	Chakravarthy et al.	Mar 2015	A1
20150119830	Luckemeyer et al.	Apr 2015	A1
20150119833	Coulthard et al.	Apr 2015	A1
20150141941	Allen et al.	May 2015	A1
20150190286	Allen et al.	Jul 2015	A1
20150290041	Richard	Oct 2015	A1
20160000610	Riesinger	Jan 2016	A1
20160067107	Cotton	Mar 2016	A1
20160144084	Collinson et al.	May 2016	A1

Foreign Referenced Citations (131)

Number	Date	Country
550575	Mar 1986	AU
550575	Mar 1986	AU
745271	Apr 1999	AU
755496	Feb 2002	AU
745271	Mar 2002	AU
755496	Dec 2002	AU
2009200608	Oct 2009	AU
2005436	Jun 1990	CA
2005436	Jun 1990	CA
87101823	Aug 1988	CN
26 40 413	Mar 1978	DE
43 06 478	Sep 1994	DE
29 504 378	Sep 1995	DE
202014100383	Feb 2015	DE
097517	Jan 1984	EP
0100148	Feb 1984	EP
0117632	Sep 1984	EP
0147119	Jul 1985	EP
0161865	Nov 1985	EP
0251810	Jan 1988	EP
0275353	Jul 1988	EP
0358302	Mar 1990	EP
0538917	Apr 1993	EP
0630629	Dec 1994	EP
0659390	Jun 1995	EP
0633758	Oct 1996	EP
1002846	May 2000	EP
1018967	Jul 2000	EP
1018967	Aug 2004	EP
2578193	Apr 2013	EP
692578	Jun 1953	GB
1386800	Mar 1975	GB
2 195 255	Apr 1988	GB
2 197 789	Jun 1988	GB
2 220 357	Jan 1990	GB
2 235 877	Mar 1991	GB
2 329 127	Mar 1999	GB
2 329 127	Mar 1999	GB
2 333 965	Aug 1999	GB
2377939	Jan 2003	GB
2392836	Mar 2004	GB
2393655	Apr 2004	GB
2425487	Nov 2006	GB
2452720	Mar 2009	GB
2496310	May 2013	GB
4129536	Apr 1992	JP
2005205120	Aug 2005	JP
2007254515	Oct 2007	JP
2008080137	Apr 2008	JP
4129536	Aug 2008	JP
71559	Apr 2002	SG
8002182	Oct 1980	WO
8704626	Aug 1987	WO
8707164	Dec 1987	WO
9010424	Sep 1990	WO
9309727	May 1993	WO
9420041	Sep 1994	WO
9605873	Feb 1996	WO
9622753	Aug 1996	WO
9718007	May 1997	WO
9913793	Mar 1999	WO
9965542	Dec 1999	WO
01019306	Mar 2001	WO
0136188	May 2001	WO
0160296	Aug 2001	WO
0168021	Sep 2001	WO
0185248	Nov 2001	WO
0185248	Nov 2001	WO
0190465	Nov 2001	WO
01085248	Nov 2001	WO
0243743	Jun 2002	WO
02062403	Aug 2002	WO
03045294	Jun 2003	WO
03045492	Jun 2003	WO
03053484	Jul 2003	WO
2004024197	Mar 2004	WO
2004037334	May 2004	WO
2004112852	Dec 2004	WO
2005002483	Jan 2005	WO
2005062896	Jul 2005	WO
2005105176	Nov 2005	WO
2005123170	Dec 2005	WO
2007022097	Feb 2007	WO
2007030601	Mar 2007	WO
2007070269	Jun 2007	WO
2007085396	Aug 2007	WO
2007087811	Aug 2007	WO
2007113597	Oct 2007	WO
2007133618	Nov 2007	WO
2008026117	Mar 2008	WO
2008041926	Apr 2008	WO
2008048527	Apr 2008	WO
2008054312	May 2008	WO
2008082444	Jul 2008	WO
2008100440	Aug 2008	WO
2008104609	Sep 2008	WO
2008131895	Nov 2008	WO
2009002260	Dec 2008	WO
2008149107	Dec 2008	WO
2009066105	May 2009	WO
2009066106	May 2009	WO
2009081134	Jul 2009	WO
2009089016	Jul 2009	WO
2009124100	Oct 2009	WO
2009126103	Oct 2009	WO
2010016791	Feb 2010	WO
2010032728	Mar 2010	WO
2010056977	May 2010	WO
2010129299	Nov 2010	WO
2011008497	Jan 2011	WO
2011049562	Apr 2011	WO
2011043786	Apr 2011	WO
2011115908	Sep 2011	WO
2011121127	Oct 2011	WO
2011130570	Oct 2011	WO
2011162862	Dec 2011	WO
2012112204	Aug 2012	WO
2012104584	Aug 2012	WO
2012140378	Oct 2012	WO
2012143665	Oct 2012	WO
2013009239	Jan 2013	WO
2013090810	Jun 2013	WO
2014022400	Feb 2014	WO
2014039557	Mar 2014	WO
2014078518	May 2014	WO
2014113253	Jul 2014	WO
2014140608	Sep 2014	WO
2014143488	Sep 2014	WO
2015065615	May 2015	WO
2015130471	Sep 2015	WO
2017048866	Mar 2017	WO

Non-Patent Literature Citations (116)

Entry
European Search Report for corresponding Application No. 15194949.2.
European Search Report for corresponding EPSN 15157408.4 published on Sep. 30, 2015.
International Search Report and Written Opinion for PCT/US2015/034289 dated Aug. 21, 2015.
International Search Report and Written Opinion for PCT/US2015/065135 dated Apr. 4, 2016.
International Search Report and Written Opinion for PCT/GB2012/050822 dated Aug. 8, 2012.
International Search Report and Written Opinion for PCT/US2015/029037 dated Sep. 4, 2015.
International Search Report and Written Opinion dated Jun. 1, 2011 for PCT International Application No. PCT/US2011/028344.
European Search Report for EP 11714148.1, dated May 2, 2014.
European Search Report for corresponding Application No. 15192606.0 dated Feb. 24, 2016.
International Search Report and Written Opinion for corresponding PCT/US2014/048081 dated Nov. 14, 2014.
International Search Report and Written Opinion for corresponding PCT/US2014/010704 dated Mar. 25, 2014.
European Examination Report dated Jun. 29, 2016, corresponding to EP Application No. 16173614.5.
International Search Report and Written Opinion for PCT/GB2008/003075 dated Mar. 11, 2010.
International Search Report and Written Opinion for PCT/GB2008/004216 dated Jul. 2, 2009.
International Search Report and Written Opinion for PCT/GB2012/000099 dated May 2, 2012.
EP Examination Report dated May 22, 2014 for EP.
International Search Report and Written Opinion for PCT/US2012/069893 dated Apr. 8, 2013.
International Search Report and Written Opinion for PCT/US2013/070070 dated Jan. 29, 2014.
International Search Report and Written Opinion for PCT/US2014/056566 dated Dec. 5, 2014.
International Search Report and Written Opinion for PCT/US2014/056508 dated Dec. 9, 2014.
International Search Report and Written Opinion for PCT/US2014/056524 dated Dec. 11, 2014.
International Search Report and Written Opinion for PCT/US2014/056594 dated Dec. 2, 2014.
Partial Internationl Search Report dated Jul. 31, 2009; PCT Internationl Application No. PCT/US2009/036222.
International Search Report and Written opinion dated Dec. 15, 2009; PCT Internation Application No. PCT/US2009/036222.
International Search Report and Written Opinion dated Feb. 24, 2010; PCT/US2009/057182.
International Search Report and Written Opinion dated Jan. 5, 2010; PCT International Application No. PCT/US2009/057130.
Response filed Oct. 20, 2011 for U.S. Appl. No. 12/398,904.
Interview Summary dated Oct. 27, 2011 for U.S. Appl. No. 12/398,904.
Non-Final Office Action dated Jul. 20, 2011 for U.S. Appl. No. 12/398,904.
V.A. Solovev et al., Guidelines, The Method of Treatment of Immagure External Fistulas in the Upper Gastrointestinal Tract, editor-in-chief Prov. V.I. Parahonyak (S.M. Kirov Gorky State Medican Institute, Gorky, U.S.S.R. 1987) (“Solovev Guidelines”).
V.A. Kuznetsov & N.a. Bagautdinov, “Vacuum and Vacuum-Sorption Treatement of Open Septic Wounds,” in All-Union Conference on Wounds and Wound Infections: Presentation Abstracts, edited by B.M. Kostyuchenok et al. (Mosco, U.S.S.R. Oct. 28-29, 1986) pp. 91-92 (“Bagautdinov II”).
V.A. Solovev, Dissertation Abstract, Treatement and Prevention of Suture Failures after Gastric Resection (S.M. Kirov Gorky State Medical Institute, Gorky, U.S.S.R. 1998 (“Solovev Abstract”).
NDP 1000 Negative Pressure Wound Terapy System, Kalypto Medical, pp. 1-4.
Partial International Search Report dated Jul. 31, 2009 for PCT International Application No. PCT/US2009/036217.
International Search Report and Written Opinion dated May 31, 2010 for PCT Application No. PCT/US2009/064364.
Examination report for AU2009221772 dated Apr. 4, 2013.
Response filed Oct. 21, 2011 for U.S. Appl. No. 12/398,891.
Interview Summary dated Oct. 27, 2011 for U.S. Appl. No. 12/398,891.
Restriction Requirement dated Jun. 13, 2011 for U.S. Appl. No. 12/398,891.
Response filed Jun. 24, 2011 for U.S. Appl. No. 12/398,891.
Non-Final Office Action dated Jul. 21, 2011 for U.S. Appl. No. 12/398,891.
International Search Report and Written Opinion dated Oct. 19, 2010; PCT International Application No. PCT/US2009/036217.
International Search Report and Written Opinion dated Feb. 24, 2010; PCT International Application No. PCT/US2009/057182.
NPD 1000 Negative Pressure Would Therapy System, Kalypto Medical, pp. 1-4.
Partial International Search Report dated Jul. 31, 2009; PCT Internationl Application No. PCT/US2009/036222.
Non-Final Rejection for U.S. Appl. No. 12/398,904 dated Mar. 14, 2012.
International Search Report and Written Opinion for PCT/US2014/061251 dated May 8, 2015.
International Search Report and Written Opinion for PCT/IB2013/060862 dated Jun. 26, 2014.
International Search Report and Written Opinion for corresponding PCT application PCT/US2016/051768 dated Dec. 15, 2016.
International Search Report and Written Opinion for PCT/US2015/015493 dated May 4, 2015.
N.A. Bagautdinov, “Variant of External Vacuum Aspiration in the Treatment of Purulent Diseases of the Soft Tissues,” Current Problems in Modern Clinical Surgery: Interdepartmental Collection, edited by V. Ye Volkov et al. (Chuvashia State University, Cheboksary, U.S.S.R. 1986);pp. 94-96 (certified translation).
Louis C. Argenta, MD and Michael J. Morykwas, PhD; “Vacuum-Assisted Closure: A New Method for Wound Control and Treatment: Animal Studies & Basic Foundation”; Annals of Plastic Surgery, vol. 38, No. 6, Jun. 1997; pp. 553-562.
Susan Mendez-Eastmen, RN; “When Wounds Won't Heal” RN Jan. 1998, vol. 61 (1); Medical Economics Company, Inc., Montvale, NJ, USA; pp. 20-24.
James H. Blackburn, II, MD, et al; “Negative-Pressure Dressings as a Bolster for Skin Grafts”; Annals of Plastic Surgery, vol. 40, No. 5, May 1998, pp. 453-457.
S.E. Greer, et al “The Use of Subatmospheric Pressure Dressing Therapy to Close Lymphocutaneous Fistulas of the Groin” British Journal of Plastic Surgery (2000), vol. 53, pp. 484-487.
George V. Letsou, MD., et al; “Stimulation of Adenylate Cyclase Activity in Cultured Endothelial Cells Subjected to Cyclic Stretch”; Journal of Cardiovascular Surgery, vol. 31, 1990, pp. 634-639.
Orringer, Jay, et al; “Management of Wounds in Patients with Complex Enterocutaneous Fistulas”; Surgery, Gynecology & Obstetrics, Jul. 1987, vol. 165, pp. 79-80.
International Search Report for PCT International Application PCT/GB95/01983; dated Nov. 23, 1995.
PCT International Examination and Search Report, PCT International Application PCT/GB96/02802; dated Jan. 15, 1998 & Apr. 29, 1997.
PCT Written Opinion, PCT International Application PCT/GB96/02802; dated Sep. 3, 1997.
Dattilo, Philip P., Jr., et al; “Medical Textiles: Application of an Absorbable Barbed Bi-directional Surgical Suture”; Journal of Textile and Apparel, Technology and Management, vol. 2, Issue 2, Spring 2002, pp. 1-5.
Kostyuchenok, B.M., et al; “Vacuum Treatment in the Surgical Management of Purulent Wounds”; Vestnik Khirurgi, Sep. 1986, pp. 18-21 and 6 page English translation thereof.
Davydov, Yu. A., et al; “Vacuum Therapy in the Treatment of Purulent Lactation Mastitis”; Vestnik Khirurgi, May 14, 1986, pp. 66-70, and 9 page English translation thereof.
Yusupov. Yu. N., et al; “Active Wound Drainage”, Vestnik Khirurgi, vol. 138, Issue 4, 1987, and 7 page English translation thereof.
Davydov, Yu. A., et al; “Bacteriological and Cytological Assessment of Vacuum Therapy for Purulent Wounds”; Vestnik Khirurgi, Oct 1988, pp. 48-52, and 8 page English translation thereof.
Davydov, Yu. A., et al; “Concepts for the Clinical-Biological Management of the Wound Process in the Treatment of Purulent Wounds by Means of Vacuum Therapy”; Vestnik Khirurgi, Jul. 7, 1980, pp. 132-136, and 8 page English translation thereof.
Chariker, Mark E., M.D., et al; “Effective Management of incisional and cutaneous fistulae with closed suction wound drainage”; Contemporary Surgery, vol. 34, Jun. 1989, pp. 59-63.
Egnell Minor, Instruction Book, First Edition, 300 7502, Feb. 1975, pp. 24.
Egnell Minor: Addition to the Users Manual Concerning Overflow Protection—Concerns all Egnell Pumps, Feb. 3, 1983, p. 1.
Svedman, P.: “Irrigation Treatment of Leg Ulcers”, The Lancet, Sep. 3, 1983, pp. 532-534.
Chinn, Steven D. et al.: “Closed Wound Suction Drainage”, The Journal of Foot Surgery, vol. 24, No. 1, 1985, pp. 76-81.
Arnljots, Björn et al.: “Irrigation Treatment in Split-Thickness Skin Grafting of Intractable Leg Ulcers”, Scand J. Plast Reconstr. Surg., vol. 19, 1985, pp. 211-213.
K.F. Jeter, T.E. Tintle, and M. Chariker, “Managing Draining Wounds and Fistulae: New and Established Methods,” Chronic Wound Care, edited by D. Krasner (Health Management Publications, Inc., King of Prussia, PA 1990), pp. 240-246.
G. {hacek over (Z)}ivadinovic, V. ukić, {hacek over (Z)}. Maksimović, . Radak, and P. Pe{hacek over (s)}ka, “Vacuum Therapy in the Treatment of Peripheral Blood Vessels,” Timok Medical Journal 11 (1986), pp. 161-164 (certified translation).
F.E. Johnson, “An Improved Technique for Skin Graft Placement Using a Suction Drain,” Surgery, Gynecology, and Obstetrics 159 (1984), pp. 584-585.
M. Schein, R. Saadia, J.R. Jamieson, and G.A.G. Decker, “The ‘Sandwich Technique’ in the Management of the Open Abdomen,” British Journal of Surgery 73 (1986), pp. 369-370.
Selections from W. Meyer and V. Schmieden, Bier's Hyperemic Treatment in Surgery, Medicine, and the Specialties: A Manual of Its Practical Application, (W.B. Saunders Co., Philadelphia, PA 1909), pp. 17-25, 44-64, 90-96, 167-170, and 210-211.
V.A. Solovev et al., Guidelines, The Method of Treatment of Immature External Fistulas in the Upper Gastrointestinal Tract, editor-in-chief Prov. V.I. Parahonyak (S.M. Kirov Gorky State Medical Institute, Gorky, U.S.S.R. 1987) (“Solovev Guidelines”).
V.A. Kuznetsov & N.A. Bagautdinov, “Vacuum and Vacuum-Sorption Treatment of Open Septic Wounds,” in II All-Union Conference on Wounds and Wound Infections: Presentation Abstracts, edited by B.M. Kostyuchenok et al. (Moscow, U.S.S.R. Oct. 28-29, 1986) pp. 91-92 (“Bagautdinov II”).
V.A. Solovev, Dissertation Abstract, Treatment and Prevention of Suture Failures after Gastric Resection (S.M. Kirov Gorky State Medical Institute, Gorky, U.S.S.R. 1988) (“Solovev Abstract”).
V.A.C.® Therapy Clinical Guidelines: A Reference Source for Clinicians (Jul. 2007).
European Search Report for corresponding EP Application 171572787 dated Jun. 6, 2017.
International Search Report and Written Opinion for corresponding application PCT/US2016/031397, dated Aug. 8, 2016.
European Search Report for corresponding application 17167872.5, dated Aug. 14, 2017.
John Masters; “Reliable, Inexpensive and Simple Suction Dressings”; Letter to the Editor, British Journal of Plastic Surgery, 1998, vol. 51 (3), p. 267; Elsevier Science/The British Association of Plastic Surgeons, UK.
Svedman, P.: “A Dressing Allowing Continuous Treatment of a Biosurface”, IRCS Medical Science: Biomedical Technology, Clinical Medicine, Surgery and Transplantation, vol. 7, 1979, p. 221.
Svedman, P. et al: “A Dressing System Providing Fluid Supply and Suction Drainage Used for Continuous of Intermittent Irrigation”, Annals of Plastic Surgery, vol. 17, No. 2, Aug. 1986, pp. 125-133.
A.A. Safronov, Dissertation Abstract, Vacuum Therapy of Trophic Ulcers of the Lower Leg with Simultaneous Autoplasty of the Skin (Central Scientific Research Institute of Traumatology and Orthopedics, Moscow, U.S.S.R. 1967) (certified translation).
D.E. Tribble, An improved Sump Drain-Irrigation Device of Simple Construction, Archives of Surgery 105 (1972) pp. 511-513.
C.E. Tennants, “The Use of Hyperemia in the Postoperative Treatment of Lesions of the Extremities and Thorax,” Journal of the American Medical Association 64 (1915), pp. 1548-1549.
International Search Report and Written Opinion for PCT/US2014/016320 dated Apr. 15, 2014.
M. Waring et al., “Cell attachment to adhesive dressing: qualitative and quantitative analysis”, Wounds, UK, (2008), vol. 4, No. 3, pp. 35-47.
R. White, “Evidence for atraumatic soft silicone wound dressing use”. Wound, UK (2005), vol. 3, pp. 104-108, Mepilex Border docs, (2001).
European Search Report for corresponding application 17183683.6, dated Sep. 18, 2017.
European Search Report for corresponding application 17164033.7, dated Oct. 13, 2017.
Extended European Search Report for corresponding application 17191970.7, dated Oct. 26, 2017.
Office Action for related U.S. Appl. No. 13/982,650, dated Dec. 14, 2017.
Australian Office Action for related application 2013344686, dated Nov. 28, 2017.
Office Action for related U.S. Appl. No. 14/517,521, dated Dec. 12, 2017.
Office Action for related U.S. Appl. No. 14/490,898, dated Jan. 4, 2018.
International Search Report and Written Opinion for related application PCT/US2017/058209, dated Jan. 10, 2018.
Office Action for related U.S. Appl. No. 14/965,675, dated Jan. 31, 2018.
International Search Report and Written Opinion for related application PCT/US2016/047351, dated Nov. 2, 2016.
Extended European Search Report for related application 17177013.4, dated Mar. 19, 2018.
Extended European Search Report for related application 16793298.7, dated Mar. 27, 2018.
Office Action for related U.S. Appl. No. 14/965,675, dated Aug. 9, 2018.
Office Action for related U.S. Appl. No. 15/307,472, dated Oct. 18, 2018.
Office Action for related U.S. Appl. No. 14/965,675, dated Dec. 12, 2018.
Office Action for related U.S. Appl. No. 14/630,290, dated Jan. 11, 2019.
Office Action for related U.S. Appl. No. 15/265,718, dated Feb. 7, 2019.
Extended European Search Report for related application 18193559.4, dated Dec. 17, 2018.
Office Action for related U.S. Appl. No. 14/080,348, dated Apr. 12, 2019.
Japanese Notice of Rejection for related application 2016-570333, dated Feb. 26, 2019.
Office Action for related U.S. Appl. No. 15/410,991, dated May 2, 2019.
Office Action for U.S. Appl. No. 15/314,426, dated Aug. 29, 2019.
Office Action for related U.S. Appl. No. 15/600,451, dated Nov. 27, 2019.

Related Publications (1)

	Number	Date	Country
	20150245949 A1	Sep 2015	US

Provisional Applications (1)

	Number	Date	Country
	61945882	Feb 2014	US

Hybrid drape having a gel-coated perforated mesh

Information

Patent Number

Date Filed

Date Issued

Inventors

Original Assignees

Examiners

CPC

Field of Search

CPC

International Classifications

Term Extension

Abstract