The present invention relates to hemostatic wound dressings, more specifically, a flexible hemostatic patch comprising a knitted fabric of oxidized cellulose and a porous water-soluble or water-swellable polymeric matrix, and to a process of making such fabrics and wound dressings.
The control of bleeding is essential and critical in surgical procedures to minimize blood loss, postsurgical complication and to shorten the duration of the surgery in the operation room. Oxidized cellulose, due to its bioresorable, bactericidal and hemostatic properties, has long been used as a topical hemostatic wound dressing in a variety of surgical procedures, including neurosurgery, abdominal surgery, cardiovascular surgery, thoracic surgery, head and neck surgery, pelvic surgery, and skin and subcutaneous tissue procedures. Examples of hemostatic oxidized regenerated cellulose absorbable hemostats commercially available include Surgicel® absorbable hemostat, a knitted fabric of oxidized regenerated cellulose (ORC), Surgicel Nu-Knit® absorbable hemostat, a dense ORC fabric and Surgicel® Fibrillar absorbable hemostat, mircrofibrils of ORC, all available from Johnson & Johnson Wound Management Worldwide, a division of Ethicon, Inc., Somerville, N.J., a Johnson & Johnson Company.
Although the absorbency of body fluid and the hemostatic action of currently available oxidized cellulose hemostats are adequate for applications where mild to moderate bleeding is encountered, they are not known to be effective to prevent or stop severe bleeding where a relatively high volume of blood is lost at a relatively high rate. In such instances, e.g. arterial puncture, liver resection, blunt liver trauma, blunt spleen trauma, aortic aneurysm, bleeding from patients with over-anticoagulation, or patients with coagulopathies, such as hemophilia, etc., a higher degree of hemostasis is required quickly.
In an effort to achieve enhanced hemostatic properties additional chemical moieties, such as calcium, or biologics, such as fibrinogen, thrombin and fibrin, have been bound to oxidized cellulose fabrics. These biologics-bound combination products require the use of proteins derived from human or animal blood or tissue. This imposes a risk of blood-borne pathogen or zoonotic disease transmission by the products. Hemostatic wound dressings containing hemostatic agents are known. Woven or nonwoven fibrous materials are prepared by coating the materials with solutions containing ammonium salts of cellulose derivatives, e.g. free acid cellulose glycolic acid ether and free acid hydroxyproprionic acid ether. The coated material then is dried and preferably heated at elevated temperatures, e.g. 175-350° C., to obtain surgical dressings having insoluble hemostatic agent impregnant.
Medical sealants and adhesives, such as cyanoacrylate-based medical adhesives, function as hemostats only in very slowly diffusing bleeding. Sealant systems, usually involving chemical cross-linking steps, are not effective hemostatic agents on actively oozing or severely bleeding wound sites. The mobility of liquid sealants also makes it hard to apply manual or digital compression to help achieve hemostasis.
Currently available oxidized cellulose hemostats noted above are knitted fabrics having a porous structure. They exhibit good tensile and compressive strength and are flexible such that a physician can effectively place the hemostat in position and maneuver same during the particular procedure being performed.
While the various noted hemostatic materials and agents are known for use with respect to providing hemostasis for low to normal bleeding, to date none of the noted hemostats, or combinations thereof, have been shown to be effective in providing hemostasis in cases of severe bleeding, e.g. high volume and high rate of bleeding. The present invention provides such a hemostat that provides hemostasis in cases of severe bleeding.
The present invention is directed to wound dressings comprising a fabric having a wound-contacting surface and a top surface opposing the wound-contacting surface, the fabric comprising biocompatible fibers and having flexibility, strength and porosity effective for use as a hemostat; and a porous, polymeric matrix applied at least to the wound-contacting surface of the fabric and dispersed at least partially through said fabric in an amount effective to provide and maintain hemostasis for severe bleeding, wherein the polymeric matrix comprises a biocompatible, water-soluble or water-swellable polymer; and methods of making such wound dressings and fabrics.
The present invention is directed to hemostatic fabrics and wound dressings fabricated at least in part from such fabrics, each of which provides and maintains effective hemostasis in cases of severe bleeding, where a relatively high volume of blood is lost at a relatively high rate. Examples of severe bleeding include, without limitation, arterial puncture, liver resection, blunt liver trauma, blunt spleen trauma, aortic aneurysm, bleeding from patients with over-anticoagulation, or bleeding from patients with coagulopathies, such as hemophilia. The present invention allows a patient to ambulate quicker than the current standard of care following, e.g. a diagnostic or interventional endovascular procedure.
Wound dressings of the present invention comprise a fabric having a wound-contacting surface and a top surface opposing the wound-contacting surface. The fabric comprises fibers and possesses physical properties suitable for use as a hemostat. Such properties include flexibility, strength and porosity. Dispersed at least on the wound contacting surface, and preferable through the fabric, is a porous polymeric matrix comprising a biocompatible, water-soluble or water-swellable polymer, in amounts effective to provide and maintain hemostasis in cases of severe bleeding.
The fabrics utilized in the present invention may be woven or nonwoven, provided that the fabric possesses the physical properties necessary for hemostasis. A preferred woven fabric has dense and knitted structure that provides form and shape for the hemostat.
The fibers comprise a biocompatible polymer. The fibers may be fabricated from any biocompatible polymer known for use in medical wound dressings. Such polymers include, without limitation, collagen, calcium alginate, chitin, polyester, polypropylene and cellulose. Preferred fibers comprise oxidized regenerated cellulose.
In preferred embodiments of the present invention, the absorbable hemostatic fabrics comprising the porous polymeric matrix dispersed there through are warp knitted tricot fabrics constructed of bright rayon yarn which is subsequently oxidized by known techniques. The fabrics are characterized by having a single ply thickness of at least about 0.5 mm, a density of at least about 0.03 g/cm2, air porosity of less than about 150 cm3/sec/cm2 and liquid absorption capacity of at least about 3 times the dry weight of the fabric and at least about 0.1 g water per cm2 of the fabric.
The knitted fabrics have good bulk without undue weight, are soft and drapable, conforming well to the configuration of the surface to which they are applied. The fabric may be cut into suitable sizes without running or fraying along the cut edge. Fabric strength after oxidation is more than adequate for use as a surgical hemostat.
Preferred hemostatic fabrics used in the present invention comprise oxidized cellulose and are best characterized by their physical properties of thickness, bulk, porosity and liquid absorption capacity as recited above. Suitable fabrics having these properties may be constructed by knitting 60 denier, 18-filament bright rayon yarn on a 32-gauge machine at a knit quality of 12. A suitable tricot fabric construction is front-bar 1-0, 10-11; back-bar 2-3, 1-0. The extended shog movement imparted to the front bar results in a 188 inch runner compared to a 70 inch runner for the back guide bar and increases the fabric bulk and density. The ratio of front to back bar runners in this particular construction is 1:2.68.
Typical physical and hemostatic properties of preferred fabrics produced as described above are noted in Table 1.
(1)tensile strength determined at 2 in/min extension md/cd = machine direction/cross direction.
(2)Elongation, machine direction/cross direction.
(3)Absorption based on weight of water absorbed by fabric.
(4)Hemostasis evaluation on incised porcine splenic wounds, time to stop bleeding.
The tricot fabrics utilized in the present invention may be constructed from bright rayon yarns of from about 40 to 80 total denier. Each yarn may contain from 10 to 25 individual filaments, although each individual filament is preferably less than 5 denier to avoid extended absorption times. The high bulk and fabric density are obtained by knitting at 28 gauge or finer, preferably at 32 gauge, with a fabric quality of about 10 or 12 (40 to 48 courses per inch). A long guide bar shog movement of at least 6 needle spaces, and preferably 8 to 12 spaces, further increases fabric thickness and density.
Other warp knit tricot fabric constructions which produce equivalent physical properties may, of course, be utilized in the manufacture of the improved hemostatic fabrics and wound dressings of the present invention, and such constructions will be apparent to those skilled in the art.
The polymer used to prepare fabrics and wound dressings of the present invention is a biocompatible, water-soluble or water-swellable polymer. The water-soluble or water-swellable polymer rapidly absorbs blood or other body fluids and forms a tacky or sticky gel adhered to tissue when placed in contact therewith. The fluid-absorbing polymer, when in a dry or concentrated state, interacts with body fluid through a hydration process. Once applied in a bleeding site, the polymer interacts with the water component in the blood via the hydration process. The hydration force provides an adhesive interaction that aids the hemostat adhere to the bleeding site. The adhesion creates a sealing layer between the hemostat and the bleeding site to stop the blood flow.
Polymers useful in preparing fabrics and wound dressings of the present invention include, without limitation, polysaccharides, polymethacrylic acids, polyamines, polyimines, polyamides, polyesters, polyethers, polynucleotides, polynucleic acids, polypeptides, proteins, poly (alkylene oxide), polythioesters, polythioethers, polyvinyls and mixtures thereof.
Polymers in preferred embodiments of the present invention comprise a water-soluble or water-swellable polysaccharide, preferably selected from the group consisting of methylcellulose, hydroxyalkyl cellulose, cellulose sulfate, water-soluble chitosan, salts of carboxymethyl cellulose, carboxymethyl cellulose (CMC), carboxyethyl cellulose, chitin, carboxymethyl chitin, hyaluronic acid, salts of hyaluronic acid, alginate, alginic acid, propylene glycol alginate, glycogen, dextran, dextran sulfate, curdlan, pectin, pullulan, xanthan, chondroitin, chondroitin sulfates, carboxymethyl dextran, carboxymethyl chitosan, heparin, heparin sulfate, heparan, heparan sulfate, dermatan sulfate, keratan sulfate, carrageenans, chitosan, starch, amylose, amylopectin and polyuronic acids including polymannuronic acid, polyglucuronic acid and polyguluronic acid. Most preferred is sodium carboxymethyl cellulose.
The composite hemostat of the present invention remains very flexible, conforms to a bleeding site, and retains good tensile and compressive strength to withstand handling during application. The hemostat can be cut into different sizes and shapes to fit the surgical needs. It can be rolled up or packed into irregular anatomic areas. The fabric in a preferred embodiment is a knitted oxidized regenerated cellulose (ORC), such as Surgicel Nu-Knit®, available from Ethicon, Inc., Somerville, N.J.
As noted above, the wound dressing of the present invention must comprise a porous polymeric matrix dispersed at least partially there through in order to provide and maintain hemostasis in cases of severe bleeding. A preferred method of making the porous polymeric matrix is to contact the fabric with the appropriate amount of polymer solution, thereby dispersing the dissolved polymer through the fabric, flash-freeze the polymer and fabric, and then remove the solvent from the frozen structure under vacuum, i.e. lyophilization. Through this preferred lyophilization method, a fabric comprising a matrix of the water-soluble or water-swellable polymer and having microporous or nanoporous structure is obtained. The lyophilization condition is important to the novel porous structure in order to create a large surface area in the hemostat with which body fluids can interact.
The features of such microporous structure can be controlled to suit a desired application by choosing the conditions to form the composite hemostat during lyophilization. To maximize the surface area of the porous matrix of the present invention, a preferred method is to quickly freeze the fabric/polymer construct at lower than 0° C., preferably at about −50° C., and to remove the solvent under high vacuum. The porous matrix produced thereby provides a large fluid absorbing capacity to the hemostatic wound dressing. When the hemostatic wound dressing comes into contact with body fluid, a very large surface area of polymer is exposed to the fluid instantly. The hydration force of the hemostat and subsequent formation of a tacky gelatinous layer helps to create an adhesive interaction between the hemostat and the bleeding site. The microporous structure of the polymeric matrix also allows blood to quickly pass through the fabric surface before the hydration takes place. The formation of a gelatinous sheet on oxidized cellulose upon blood contact will enhance the sealing property of the water-soluble gelatinous layer, which is critical to fast hemostasis for moderate to severe bleeding.
The fabric comprises polymer in an amount effective to provide and maintain hemostasis in cases of severe bleeding. If the ratio of polymer to fabric is too low, the polymer does not provide an effective seal to physically block the bleeding. If the ratio is too high, the composite hemostat wound dressing will be too stiff or too brittle to conform to wound tissue in surgical applications. Such an excessive ratio will also prevent the blood from quickly passing through the fabric surface to form the gelatinous layer on oxidized cellulose that is critical for enhancing the sealing property. A preferred weight ratio of polymer to fabric is from about 1:99 to about 15:85. A more preferred weight ratio of polymer to fabric is from about 3:97 to about 10:90.
In certain embodiments of the present invention, the porous polymeric matrix is dispersed substantially homogeneously on at least the wound-contacting surface of the fabric and through the fabric. In such cases, the fabric may be immersed in the polymer solution to provide homogeneous distribution throughout the fabric prior to lyophilization. In other embodiments, it is preferred that only the wound-contact surface of the hemostat sticks well to wet surfaces, while the physician handling side, or top surface of the fabric, does not. In such cases, the fabric may be partially immersed in the polymer solution so as to provide polymer at least on the wound-contact surface of the fabric. In this way, a gradient of polymer in the fabric is provided, whereby the fabric will comprise an effective amount of the lyophilized polymer adjacent the wound-contacting area, while the top surface of the fabric comprises little or no dispersed polymer and maintains ease of handling for the physician.
The present invention is best exemplified in the figures prepared by scanning electron microscope. The samples were prepared by cutting 1 cm2 sections by using a razor. Micrographs of both top surface and wound-contacting surfaces and cross-sections were prepared and mounted on carbon stubs using carbon paint. The samples were gold-sputtered and examined by scanning electron microscopy (SEM) under high vacuum at 4 KV.
In comparing the surface morphologies of wound-contact surface 22 and top surface 24 of fabric 20, it is apparent that wound-contact surface 22 contained significantly less Na-CMC. The coating was significantly thinner on the fibers than the coating on the top surface. While some Na-CMC was observed to span across some fibers, the coating was incomplete or had perforations present. The coating layer thickness, where present, did not exceed about 2 microns.
It is clear from
Hemostatic fabrics according to the present invention are set forth in
As shown in
It is clear from
It also is clear from
In certain embodiments of the invention, a drug or a combination of pharmaceutical agents can be incorporated into the hemostat. To fabricate such a hemostat, a drug or agent is first dissolved with a polymer in a solvent. The fabric is then coated with the polymer/drug solution, and the solvent is removed through lyophilization. Preferred drugs and agent include analgesics, anti-infective agents, antibiotics, adhesion preventive agents, procoagulants and wound healing growth factors.
While the following examples demonstrate certain embodiments of the invention, they are not to be interpreted as limiting the scope of the invention, but rather as contributing to a complete description of the invention.
ORC/HEC Porous Patch Preparation:
One gram of hydroxyethyl cellulose (HEC, from Aldrich) was dissolved in 99 grams of deionized water. After complete dissolution of the polymer, 10 grams of the HEC solution was transferred into a crystallization dish with a diameter of 10 cm. A piece of Surgicel Nu-Knit® absorbable hemostat, based on oxidized regenerated cellulose (ORC), having a diameter of 9.8 cm (about 1.3 gram) was placed on the HEC solution in the crystallization dish. After soaking the fabric in the solution for 3 minutes, the wet fabric in the dish was then lyophilized overnight. A very flexible patch was formed. The patch was further dried at room temperature under vacuum.
ORC/CS Porous Patch Preparation
One gram of cellulose sulfate (CS, from ACROS Organics) was dissolved in 99 grams of deionized water. After complete dissolution of the polymer, 10 grams of the CS solution was transferred into a crystallization dish with a diameter of 10 cm. A piece of Surgicel Nu-Knit® fabric with a diameter of 9.8 cm (about 1.3 gram) was placed on the CS solution in the crystallization dish. After soaking the fabric for 3 minutes, the wet fabric was then lyophilized overnight. A very flexible patch was formed. The patch was further dried at room temperature under vacuum.
ORC/MC Porous Patch Preparation
One gram of methyl cellulose (MC, from Aldrich) was dissolved in 99 grams of deionized water. After complete dissolution of the polymer, 10 grams of the MC solution was transferred into a crystallization dish with a diameter of 10 cm. A piece of Surgicel Nu-Knit® fabric with a diameter of 9.8 cm (about 1.3 gram) was placed on the MC solution in the crystallization dish. After soaking the fabric for 3 minutes, the wet fabric in the dish was then lyophilized overnight. A very flexible patch was formed. The patch was further dried at room temperature under vacuum.
ORC/Water-Soluble Chitosan (WS-CH) Porous Patch Preparation
One gram of WS-CH was dissolved in 99 grams of deionized water. After complete dissolution of the polymer, 10 grams of the WS-CH solution was transferred into a crystallization dish with a diameter of 10 cm. A piece of Surgicel Nu-Knit® fabric with a diameter of 9.8 cm (about 1.3 gram) was placed on WS-CH solution in the crystallization dish. After soaking the fabric for 3 minutes, the wet fabric in the dish was then lyophilized overnight. A very flexible patch was formed. The patch was further dried at room temperature under vacuum.
ORC/Na-CMC Porous Patch Preparation
One gram of sodium salt of CMC (Na-CMC, from Aqualon) was dissolved in 99 grams of deionized water. After complete dissolution of the polymer, 10 grams of the Na-CMC solution was transferred into a crystallization dish with a diameter of 10 cm. A piece of Surgicel Nu-Knit® fabric with a diameter of 9.8 cm (about 1.3 gram) was placed on the CMC solution in the crystallization dish. After soaking the fabric for 3 minutes, the wet fabric in the dish was then lyophilized overnight. A very flexible patch was formed. The patch was further dried at room temperature under vacuum.
ORC/Na-CMC Film Preparation
One gram of sodium salt of CMC (Na-CMC, from Aqualon) was dissolved in 99 grams of deionized water. After complete dissolution of the polymer, 10 grams of the Na-CMC solution was transferred into a crystallization dish with a diameter of 10 cm. A piece of Surgicel Nu-Knit® fabric with a diameter of 9.8 cm (about 1.3 gram) was placed on the Na-CMC solution in the crystallization dish. The wet fabric in the dish was then air-dried overnight. A rigid and brittle patch was formed. The ORC/Na-CMC film was further dried at room temperature under vacuum. The film was not effective as a hemostat because it was too stiff and did not conform to the bleeding site well.
Na-CMC Porous Patch Preparation
One gram of sodium salt of CMC (Na-CMC, medium viscosity grade from Sigma) was dissolved in 99 grams of deionized water. After complete dissolution of the polymer, 60 grams of the Na-CMC solution was transferred into a crystallization dish with a diameter of 10 cm. The solution in the dish was then lyophilized overnight. A porous sponge was formed. The patch was further dried at room temperature under vacuum.
Hemostatic Performance of Different Materials in Porcine Splenic Incision Model
A porcine spleen incision model was used for hemostasis evaluation of different materials. The materials were cut into 2.5 cm×1.5 cm rectangles. A linear incision of 1.5 cm with a depth of 0.3 cm was made with a surgical blade on a porcine spleen. After application of the test article, digital tamponade was applied to the incision for 2 minutes. The hemostasis was then evaluated. Additional applications of digital tamponade for 30 seconds each time were used until complete hemostasis was achieved. Fabrics failing to provide hemostasis within 12 minutes were considered to be failures. Table 1 lists the results of the evaluation.
As indicated from the results, wound dressings prepared using lyophilization as the means for removing solvent improved hemostatic property of hemostatic fabrics, while the air-dried process failed to enhance the hemostatic property of hemostatic fabrics. Additionally, lyophilized Na-CMC sponge alone failed to achieve hemostasis.
Hemostatic Performance of Example 5 (ORC/Na-CMC) in a Porcine Splenic Arterial Needle Puncture Model
A puncture defect was made on a porcine splenic artery with an 18-gauge needle. After the needle was removed, severe bleeding was observed. A test article (2.5 cm×2.5 cm) was applied over the puncture site. Digital pressure was applied over the test article for 2 minutes. The hemostatic performance was evaluated. The observations are listed in Table 2.
Hemostatic Performance of Different Materials in a Porcine Splenic Incision Model with Tamponade for 30 Seconds
A porcine spleen incision model was used for hemostasis evaluation of different materials. The materials were cut into 2.5 cm×1.5 cm rectangles. A linear incision of 1.5 cm with a depth of 0.3 cm was made with a surgical blade on porcine spleen. After application of the test article, digital tamponade was applied to the incision for 30 seconds. The hemostasis evaluation was then performed. Additional applications of digital tamponade for 30 seconds each time were used until complete hemostasis was achieved. Table 3 lists the results of the evaluation.
Hemostatic Performance of Different Materials in a Porcine Splenic Cross-Hatch Model
A porcine spleen cross-hatch model was used for hemostasis evaluation of different materials. The materials were cut into 3 cm×3 cm squares. A surgical defect (2 cm×2 cm, 0.2 cm deep) was made with a surgical blade on the porcine spleen. Additional bleeding was induced by making three additional equally spaced, side-to-side horizontal incisions and three additional equally spaced, side-to-side vertical incisions within the defect. After application of the test article, digital tamponade was applied to the incision for 2 minutes. The hemostasis evaluation was then performed. Additional applications of digital pressure for 30 second each time were used until complete hemostasis was achieved. Table 4 lists the results of the evaluation.
Number | Name | Date | Kind |
---|---|---|---|
2517772 | Doub et al. | Aug 1950 | A |
2773000 | Masci et al. | Dec 1956 | A |
2914444 | Smith | Nov 1959 | A |
3328259 | Anderson | Jun 1967 | A |
3328529 | Anderson | Jun 1967 | A |
3364200 | Aston et al. | Jan 1968 | A |
3868955 | Siragusa et al. | Mar 1975 | A |
4289824 | Smith | Sep 1981 | A |
4407787 | Stemberger | Oct 1983 | A |
4600574 | Lindner et al. | Jul 1986 | A |
4626253 | Broadnax, Jr. | Dec 1986 | A |
4752466 | Saferstein et al. | Jun 1988 | A |
4840626 | Linsky et al. | Jun 1989 | A |
5134229 | Saferstein et al. | Jul 1992 | A |
5180398 | Boardman et al. | Jan 1993 | A |
5409703 | McAnalley et al. | Apr 1995 | A |
5643596 | Pruss et al. | Jul 1997 | A |
5645849 | Pruss et al. | Jul 1997 | A |
5821343 | Keogh | Oct 1998 | A |
5866165 | Liu et al. | Feb 1999 | A |
5914118 | Yamamura et al. | Jun 1999 | A |
5925552 | Keogh et al. | Jul 1999 | A |
5945319 | Keogh | Aug 1999 | A |
6017741 | Keogh | Jan 2000 | A |
6214808 | Soe et al. | Apr 2001 | B1 |
6261679 | Chen et al. | Jul 2001 | B1 |
6306424 | Vyakarnam et al. | Oct 2001 | B1 |
6333029 | Vyakarnam et al. | Dec 2001 | B1 |
6365149 | Vyakarnam et al. | Apr 2002 | B2 |
6500777 | Wiseman et al. | Dec 2002 | B1 |
20010025154 | Rapp | Sep 2001 | A1 |
20020012693 | Cohen et al. | Jan 2002 | A1 |
20020120348 | Melican et al. | Aug 2002 | A1 |
20030073663 | Wiseman et al. | Apr 2003 | A1 |
20040005350 | Looney et al. | Jan 2004 | A1 |
Number | Date | Country |
---|---|---|
217243 | Dec 1982 | CS |
235108 | May 1985 | CS |
238016 | Nov 1985 | CS |
0 177 064 | Apr 1986 | EP |
0 216 378 | Apr 1987 | EP |
0 372 969 | Jun 1990 | EP |
0468114 | Jan 1992 | EP |
0 636 378 | Feb 1995 | EP |
0 815 879 | Jun 1997 | EP |
1172115 | Jan 2002 | EP |
1 378 255 | Jan 2004 | EP |
942 305 | Nov 1963 | GB |
983 073 | Feb 1965 | GB |
2 314 840 | Aug 1996 | GB |
2 314 842 | Jan 1998 | GB |
2 344 519 | Jun 2000 | GB |
159332 | May 1987 | IN |
60-87225 | May 1985 | JP |
2146264 | Mar 2000 | RU |
WO 96016643 | Jun 1996 | WO |
WO 96040033 | Dec 1996 | WO |
WO 9800180 | Jan 1998 | WO |
WO 98000446 | Jan 1998 | WO |
WO 98033479 | Aug 1998 | WO |
WO 9901168 | Jan 1999 | WO |
WO 0123653 | Apr 2001 | WO |
WO 0202155 | Jan 2002 | WO |
WO 0122059 | Mar 2002 | WO |
WO 02022059 | Mar 2002 | WO |
WO 02058750 | Aug 2002 | WO |
WO 03020191 | Mar 2003 | WO |
Number | Date | Country | |
---|---|---|---|
20040001879 A1 | Jan 2004 | US |