Breathable blood and viral barrier fabric

Abstract

The nonwoven composite fabric of the invention provides a barrier to blood and viral challenges, and also provides breathability for comfort. The fabric is particularly suited for use as a disposable surgical gown. The fabric comprises a first microporous ply comprising a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently stretched to impart microporosity, and at least one additional ply positioned adjacent the first microporous ply. The nonwoven composite fabric has barrier properties passing the ASTM F1671 viral barrier test, and the MVTR of the composite fabric is at least 300 g/m2/24 hr.

Description

FIELD OF THE INVENTION

[0002] The present invention relates to a nonwoven composite fabric, and more particularly, to a nonwoven composite fabric having blood and viral barrier properties that make the fabric suitable for use as a protective garment in healthcare applications.

BACKGROUND OF THE INVENTION

[0003] In the healthcare field, there is an awareness of the need to provide protection to healthcare workers against the spread of communicable viral or blood-borne diseases, such as AIDS and hepatitis. Protective fabrics for use in surgical gowns, masks, drapes and other protective apparel have been developed for this purpose. Regulations and standards such as the OHSA Universal Precautions act and the current proposed Surgical Gown classification standards under development by the Association for the Advancement of Medical Instrumentation (AAMI) further contribute to the awareness of this need.

[0004] Industry standards for assessing the barrier properties of protective fabrics against penetration by blood and viral agents include ASTM F1670, Standard Test Method for Resistance of Materials Used in Protective Clothing to Penetration by Synthetic Blood, and ASTM F1671, Standard Test Method for Resistance of Materials Used in Protective Clothing to Penetration by Blood-Borne Pathogens Using Phi-x 174 Bacteriophage Penetration as a Test System.

[0005] Protective fabrics are available that meet the above barrier standards (ASTM F1670 and ASTM F1671) at a reasonable cost, but these fabrics are not breathable. These are typically plastic coated fabrics. Their lack of breathability significantly contributes to the discomfort and heat stress of the wearer. One way that gown manufacturers try to improve comfort is by using the coated fabrics only in the frontal and arm areas of the gown. However, this practice compromises protection in other areas of the body.

[0006] A common method used by industry to determine the breathability of a barrier fabric is Moisture Vapor Transfer Rate (MVTR) as determined by ASTM E96, Standard Test Methods for Water Vapor Transmission of Materials. There are breathable barrier fabrics available that provide moisture vapor transfer while passing ASTM F1670 and ASTM F1671. These barrier fabrics are based on perfluoroethylene or copolyester films and membranes. However, because of their expense, they are typically used in protective garments that are reusable, and have limited applicability as disposable garments. Several attempts have been made to reduce the cost of a blood and viral barrier, such as the fabrics described in Langley U.S. Pat. Nos. 5,409,761; 5,560,974 and 5,728,451. Garments in accordance with these patents have been sold by the Kappler Safety Group under the trade name of Pro/Vent®. The product has performed well but must command a premium price as compared to conventional low cost non-barrier gowns manufactured from spunbond-meltblown-spunbond (SMS) composite fabrics or spunlaced pulp/polyester fabrics (e.g. DuPont's Sontara®) that dominate the disposable medical gown market.

[0007] One way of obtaining favorable economics in a breathable composite material utilizes a process wherein a polymer containing a mechanical pore forming agent is extruded in a single pass onto a nonwoven fabric and subsequently incrementally stretched in the cross machine and/or machine direction. The resulting composite material is microporous. It is impervious to the passage of liquids while the presence of micropores provides moisture vapor or air permeability. For example, micropores in the range of about 0.1 micron to about 1 micron can be formed in the composite. Such technologies are described in Wu et al. U.S. Pat. No. 5,865,926 and Brady et al. U.S. Pat. No. 6,258,308, the disclosures of which are incorporated herein by reference. A disadvantage of this type of coating process as compared to a lamination process such as that described in the above-noted U.S. Pat. No. 5,409,761 is that the extrusion coating process has a tendency to form pinholes or discontinuities in the fabric. Such pinholes can cause failure of both ASTM F1670 and ASTM F1671. If the pinholes are sufficiently small, e.g. microscopic, the coating may pass the ASTM F1670 blood penetration test, but would nonetheless fail the more stringent viral penetration test of ASTM F1671.

[0008] The industry accepted requirements for making a claim that a medical fabric passes ASTM F1671 is a pass rate of 29 out of 32 samples tested. This level is also recommended by the Federal Drug Administration (FDA) as the acceptable quality level (AQL) for making a claim to passing ASTM F1671. This quality level is based on an AQL of 4% per the sampling plans described in ANSI/ASQC Z1.4-1993, MIL 105E or ISO 2859-1, Table X-G-2. It can be seen that a frequency of {fraction (29/32)} or 90.625% is the absolute minimum number of passes that must be generated to make the claim that the fabric passes ASTM F1671. Another way of stating the above is that the number of pinholes or imperfections cannot exceed 9.375% as an absolute maximum. In practice a much smaller frequency of pinhole or imperfection occurrence would be desirable.

[0009] An object of the present invention is to provide an economical fabric that will meet the stringent requirements of the ASTM F1671 viral penetration test while maintaining breathability and comfort.

SUMMARY OF THE INVENTION

[0010] The present invention provides a nonwoven composite fabric formed of at least one microporous ply. The present invention achieves a synergistic improvement in performance by combining multiple plies of fabrics that would otherwise fail the industry recognized standard for viral penetration resistance (ASTM F1671) when tested as individual layers.

[0011] More particularly, the present invention utilizes a nonwoven composite formed of at least one microporous ply which is produced from a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently incrementally stretched to impart microporosity.

[0012] According to one aspect of the invention, a nonwoven composite fabric is provided comprising a first microporous ply comprising a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently incrementally stretched to impart microporosity, and at least one additional microporous ply that is positioned adjacent this first microporous ply in opposing surface-to-surface relationship. The nonwoven composite fabric has barrier properties passing the ASTM F1671 viral barrier test. Preferably, the composite fabric has a MVTR at least 300 g/m2/24 hr, and more desirably, the MVTR is at least 600 g/m2/24 hr. The plies of the composite can be separate, yet held in close proximity to each other, or alternatively they may be joined together in any of several ways, such as with a discontinuous adhesive, powder bonding, or by thermal or ultrasonic point bonds.

[0013] In a further more specific embodiment, the nonwoven composite fabric comprises a first microporous ply comprising a nonwoven fabric substrate formed of substantially continuous filaments, an extrusion coating of a filler-containing microporous formable thermoplastic resin adhered to the nonwoven fabric substrate. A multiplicity of micropores formed in the extrusion coating impart microporosity to the ply and a MVTR of at least 300 g/m2/24 hr. A second ply is positioned adjacent to the first microporous ply in opposing surface-to-surface relationship. Both the first and second plies fail the ASTM F1671 viral barrier test when tested as individual layers, but the nonwoven composite fabric passes the ASTM F1671 viral barrier test.

[0014] The composite fabric may include a discrete bond sites interconnecting the first and second plies. Alternatively, the first and second plies are separate from one another over substantially the entire extent of their opposing surfaces, but peripheral portions of the plies are connected to one another to maintain the plies in close proximity to each other. For example, peripheral portions of the plies can be joined by at least one area of thermal or ultrasonic bonds.

[0015] According to a further aspect of the present invention, a medical gown is provided, comprising two separate plies of microporous sheet material positioned in opposing surface-to-surface relationship to form a nonwoven composite. Each ply comprises a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently stretched to impart microporosity. The respective plies are connected together along seam lines. Each ply fails the ASTM F1671 viral barrier test when tested as an individual layer, but the nonwoven composite passes the ASTM F1671 viral barrier test.

[0016] In another embodiment of the invention, a medical gown comprises two individual plies of microporous sheet material positioned in opposing surface-to-surface relationship to form a nonwoven composite, with each ply comprising a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently stretched to impart microporosity. Discrete bond sites interconnect the two plies. Each ply fails the ASTM F1671 viral barrier test when tested as an individual layer, but the nonwoven composite passes the ASTM F1671 viral barrier test.

BRIEF DESCRIPTION OF THE DRAWINGS

[0017] Some of the features and advantages of the invention having been described, others will become apparent from the detailed description which follows, and from the accompanying drawings, which are not necessarily drawn to scale, and wherein:

[0018] FIG. 1 is a perspective view showing a protective medical gown produced from a nonwoven composite fabric in accordance with the present invention.

[0019] FIG. 2 is an exploded perspective view showing a nonwoven composite fabric in accordance with the present invention.

[0020] FIGS. 3, 4, 5 and 6 are enlarged cross-sectional views of nonwoven composite fabrics in accordance with several embodiments of the invention.

[0021] FIG. 7 is a perspective view showing two microporous plies cut out to form the sleeve component for a disposable surgical gown and joined together along their periphery.

DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS

[0022] The present invention now will be described more fully with reference to the accompanying drawings, in which some, but not all embodiments of the invention are shown. Indeed, the present invention may be embodied in many different forms and should not be construed as being limited to the specific illustrative embodiments set forth herein; rather, these embodiments are provided so that this disclosure will satisfy applicable legal requirements. Like numbers refer to like elements throughout.

[0023] Referring to the drawings, there is shown in FIG. 1 a protective medical gown 10 in accordance with the present invention. The medical gown 10 is fabricated from a nonwoven composite fabric that provides a barrier to blood and viral agents, and meets the requirements of ASTM F1670 and ASTM F1671. The nonwoven composite fabric is breathable to provide comfort to the wearer. The barrier fabric has a breathability, expressed in terms of MVTR as measured by ASTM E96 of at least 300 g/m2/24 hr at standard conditions of about 75° F. and a relative humidity of about 65%. Preferably, the fabric has a MVTR of at least 300 g/m2/24 hr.

[0024] FIG. 2 illustrates in greater detail a nonwoven composite fabric 12 in accordance with one embodiment of the present invention. As shown, the composite fabric 12 includes a first microporous ply 14 and a second microporous ply 16 positioned adjacent to the first microporous ply 14 and in opposing surface-to-surface relationship. In the embodiment shown, the first and second plies 14, 16 are joined together by bond sites 18 that bond the first and second plies 14, 16, to one another. It is important that the bond sites do not block the micropores of the plies. Therefore, the bond sites are discrete and spaced apart from one another. The bond sites 18 can be produced by any of a number of available methods. For example, the bond sites can be produced by an adhesive which is preferably applied in the form of a discontinuous adhesive layer. The adhesive layer can be applied by any of several conventional techniques. For example, the adhesive can be printed onto a surface of one or both plies using conventional printing methods and can be applied in various patterns, such as dots as shown in FIG. 2, or lines, stripes, intersecting lines, etc. Alternatively, the discontinuous adhesive layer 18 can comprise a preformed adhesive web that can be brought into contact with the two plies and combined by suitable application of pressure and heat. In yet another approach, the adhesive layer can be formed in situ by spraying or extruding a suitable pressure sensitive adhesive or hot melt adhesive composition. For example, a fine web of discontinuous adhesive can be produced by melt blowing a hot melt adhesive composition using conventional melt blowing technology, as described for example in Butin et al. U.S. Pat. No. 3,849,241. Another approach, known as powder bonding, involves using a finely divided granular or powdered material, such as a thermoplastic polymeric adhesive, which can be activated by heat. In yet another approach, the bond sites 18 can be produced by thermal or ultrasonic bonding.

[0025] In the composite fabric of FIG. 2, at least one of the plies is microporous and includes a nonwoven fabric substrate with a microporous coating of a thermoplastic resin. This microporous ply is preferably formed from a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently stretched to impart microporosity. The nonwoven fibrous substrate can be formed of staple fibers or of continuous filaments. The fibers or filaments of the nonwoven substrate can be natural fibers or can be formed of synthetic polymers such as polyethylene, polypropylene, polyester, nylon, or blends or copolymers thereof. The nonwoven substrate can also be formed of bicomponent fibers or filaments. The nonwoven substrate may be made stable to gamma radiation by appropriate selection of fiber composition. The extrusion coating and stretching can be carried out generally in accordance with the process described in Wu et al. U.S. Pat. No. 5,865,926 or the process described in Brady et al. U.S. Pat. No. 6,258,308. The present invention thus benefits from the economics of these processes. Although the stretching can be carried out by a number of commercially available techniques, such as tentering, a preferred method of stretching is the technique known as incremental stretching or “ring-rolling”, which involves passing the extrusion-coated nonwoven substrate through a pair or pairs of interdigitating rollers. The incremental stretching can be in a single direction (i.e. in the machine direction or in the cross-machine direction) or it can be done in both directions. Fabrics produced in accordance with this process are permeable to moisture vapor, but form a barrier to penetration by liquids such as water. Fabrics produced by this process can consistently pass the blood barrier test of ASTM F1670. However, tests of such fabrics under the more severe viral barrier test of ASTM F1671 were unreliable. It was found that some samples passed the ASTM F1671 test while others taken from the same areas failed to pass the test.

[0026] The present invention overcomes these inconsistencies by producing a lightweight fabric that has been extrusion coated with a microporous formable resin and rendered microporous by stretching generally in accordance with the techniques described above, and combining this fabric with one or more additional plies to form a composite fabric. Although neither ply may consistently pass the ASMT F1671 test when tested as an individual layer, the resulting composite consistently passes ASTM F1671. This is possible since the first ply in contact with the challenge fluid reduces the passage of the bacteriophage challenge by many orders of magnitude. Any passage of bacteriophage coming into contact with the second ply will be of such a weak concentration that the second ply easily blocks the passage. In addition to reduced concentration, any bacteriophage (or virus) that passes through the first ply will be outside of the host liquid and thus must be extremely hardy to pose any significant challenge to the second ply. Table 1 illustrates the application of the ASTM F1671 test to a single ply and to a combined two ply composite of the present invention.

TABLE 1
ASTM F1671
	Challenge	PFU on opposite side
	Single Ply	1 × 108 pfu per ml.	100
	Two Ply	1 × 108 pfu per ml.	0

[0027] In one preferred embodiment of the present invention, the composite fabric is formed of two lightweight microporous plies, each produced in accordance with the teachings of the Wu et al. '926 patent and including a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and incrementally stretched. Each ply of the composite fabric of the present invention preferably has a basis weight of from 20 to 85 gsm (grams per square meter), and more preferably from 25 to 60 gsm. The nonwoven fabric substrate is preferably a spunbond polypropylene nonwoven fabric. The microporous formable resin composition includes a relatively high percentage of a pore-forming filler, as well as conventional additives, stabilizers and processing aids. Typically, the pore-forming filler is an inorganic filler, such as calcium carbonate having a particle-size on the order of about 0.5 to 8 microns. The pore-forming filler is typically present at a concentration of from about 30 to 75% by weight, typically about 40 to 60% by weight.

[0028] In each such ply, the nonwoven fabric substrate 22 predominantly forms one of the exposed surfaces of the ply, and the extrusion coating of microporous formable resin defines a microporous film surface 24 at the opposite surface of the ply. The resin penetrates into the interstices of the nonwoven fabric substrate to form a unitary, integral composite. The microporous formable resin can be any thermoplastic resin that is suitable for processing by melt extrusion, but is preferably an olefin-based polymer, such as polyethylene or polypropylene, or copolymers, terpolymers or blends of olefin-based polymers with other materials such as ethylene vinyl acetate, ethylene methyl acrylate, ethylene acrylic acid, polylactic acid polymers, or blends.

[0029] By utilizing two components of a lightweight coated fabric, the probability of two pinholes or inconsistencies lining up directly upon one another in the laminate is remote. Since lightweight nonwovens are typically used in each ply, the probability of a pinhole due to a strand of nonwoven fiber extending through the coating is much less likely than it would be if a single heavier nonwoven substrate were used as a bilaminate stand-alone fabric. While one might expect that thicker layers of a similar barrier coating or film might also satisfy the viral barrier requirements, increases in coating or film thickness increase cost and decrease overall comfort by resulting in a stiffer, less drapeable, and noisier material. Multiple layers of thinner materials have been found more acceptable when considering these characteristics as compared to a single composite having the equivalent barrier layer thickness. Additionally, it can be seen from Table 2 below that the characteristic MVTR of two plies of the coated fabric components is not significantly lower than the individual components. This is especially significant to maintain comfort.

TABLE 2
MVTR (g/m2/24 hr)
Single Ply 780
Two Ply    630

[0030] Another advantage of laminating two coated webs together is that a pressure sensitive adhesive (PSA) could be utilized without the inherent undesirable tacky feel on the nonwoven side. This is because the tackiness inherent in PSA adhesive is blocked by the existing coating on each component of the laminate.

[0031] FIG. 3 shows the composite of FIG. 2 on an enlarged scale. In this embodiment, the first and second plies 14, 16 are oriented with the film surfaces 24 facing outwardly, and the bond sites 18 thus bond the nonwoven surfaces 22 of the plies to one another.

[0032] However, in an alternate embodiment, shown in FIG. 4, the film surfaces 24 can be oriented inwardly and bonded to one another. In this event, the nonwoven layers 22 are exposed at both surfaces of the composite fabric.

[0033] In yet another embodiment, shown in FIG. 5, the film surface 24 of one ply 16 is bonded to the nonwoven surface 22 of the adjacent ply 14. In this case, one exposed surface of the composite is formed by the film layer, and the opposite exposed surface is defined by the nonwoven layer.

[0034] In a further embodiment of the invention, the two plies can be joined to one another by thermal or ultrasonic spot bonding. This can be carried out generally in accordance with the teachings of Langley U.S. Pat. No. 5,409,761. The thermal or ultrasonic spot bonding can be carried out over the entire extent of the surface of the composite fabric. The plies can be oriented in either a film-to-film orientation, or a nonwoven-to-nonwoven orientation, or a film to nonwoven orientation.

[0035] FIG. 6 illustrates an embodiment of the invention in which a first microporous ply 14, produced as described above and having a film surface 24 on one side and a nonwoven surface 22 on the opposite side, is positioned in opposing face-to-face relationship with a second ply 17 form of a nonwoven web. The nonwoven web can comprise a spunbonded web, a carded thermal bonded web, a spunlaced nonwoven web, or a nonwoven web of other known type. The two plies are separate from one another over substantially the entire extent of their opposing surfaces. They are connected to one another in certain selected areas, such as near the peripheral edge portions of the plies, to maintain the plies in close proximity to each other. The plies can be connected by a line of bonds, such as thermal or ultrasonic bonds, indicated at 19, or by stitching, to form a composite. This composite can be fabricated into medical protective apparel, such as medical gowns, shoe covers, head covers, face masks, sleeve protectors, or into surgical drapes.

[0036] According to another embodiment, a garment, such as a gown, is fabricated using two independent plies 14, 16 of extrusion coated microporous fabric. The plies need not be laminated, but can be joined together when the garment is fabricated and seamed. The two plies 14, 16 can be joined together only along peripheral edge portions of the two plies, with the two plies being otherwise unconnected. Thus for example, in fabricating a gown, two overlying plies can be cut into the shape of components that are to be assembled into a gown, such as a torso portion and a sleeve portion 26 as is shown in FIG. 6. The two plies 14, 16 can be joined only along the peripheral edges of the respective cutout shaped pieces. The joining together of the plies can be achieved by thermal or ultrasonic bonding, or by sewing, as indicated by the reference character 28.

[0037] In an alternative embodiment, the composite fabric of the invention could include one or more additional plies of a material different from that of the first microporous ply and which may or may not be microporous. Since the additional ply or plies will be exposed to a significantly lower challenge than the first ply, the additional ply could be produced according to a process other than that described in the Wu et al. '926 patent, and may be of a material which by itself would not pass ASTM F1670 or 1671. For example, the additional ply could be a microporous film alone, or a laminate of a microporous free film with a nonwoven layer. Alternatively, the additional ply or plies could be another nonwoven fabric, such as, for example, spunbond nonwovens, hydroentangled nonwoven, carded nonwovens, air-laid nonwovens, wet-laid nonwovens, meltblown nonwovens, or composites or laminates of such nonwovens.

[0038] Table 3 includes four basic embodiments and various iterations. Each example was fabricated according to the process of the Wu et al. '926 patent with changes being made to the thickness and color of the incrementally stretched calcium carbonate-filled microporous film, changes in the weight and color of the substrate, that being spunbonded polypropylene. However other substrates could be used, and changes in the percent engagement (i.e., stretching) which produced examples exhibiting varying air flow rates. It should be stated that MVTR was found to be independent of coating thickness, but the same conclusion could not be made relative to the percent engagement. What is evident from Table 3 is that it does not appear that a composite can be produced according to the Wu et al. '926 process that consistently passes the blood penetration test per ASTM F1670. ASTM F1670 is a method in common practice within the medical industry for evaluating the visual penetration of synthetic blood through a protective material. Materials that pass this test are considered blood barriers but can still allow the passage of viruses which is evaluated according to the more stringent viral resistance test as defined by ASTM F1671. Since these tests define a hierarchy of performance, materials failing F1670, will inherently fail F1671. The novelty of the present invention is that a multiple layer approach can be employed to pass the F1671 test with layers that otherwise fail this, and in certain combinations, even the lesser F1670 test.

[0039] The F1670 results presented in Table 3 were generated using an automated multi-celled F1670 device fabricated in-house within Kappler Safety Group (Guntersville, Ala.). This device is designed to allow simultaneous testing of 15 samples per the ASTM F1670 method. The modification for this application is that the 54 minute post pressure exposure time as detailed in ASTM F1670 was not used in an attempt to generate a greater number of tests results. Experience within the industry has demonstrated that fabrics will fail this test during the initial 5 minute 0 pressure hold time, or during the subsequent 1 minute of pressurization at 2 psig, but not during the final 54 minutes which is again at 0 pressure. Example 1, and the associated iterations, which represent a 25 gsm coating weight of an incrementally stretched calcium carbonated filled polyolefin film on a 0.5 oz/yd2 (16.9 gsm) spunbonded polypropylene, show blood penetration failures ranging from a low of 0.8% (i.e., 1 failure in 120 cells tested), to a high of 4.4% (i.e., 16 failures of 360 cells tested). Example 2, and the associated iterations, which represent a 30 gsm coating weight of an incrementally stretched calcium carbonated filled polyolefin film on a 1.0 osy spunbonded polypropylene, show blood penetration failures ranging from a low of 1.7% (i.e., 4 failures in 240 cells tested), to a high of 2.5%, that is 6 failures of 240 cells tested). Example 3, and the associated iterations, which represent a 45 gsm coating weight of an incrementally stretched calcium carbonated filled polyolefin film on a 1.0 osy spunbonded polypropylene, show blood penetration failures ranging from a low of 0% (i.e., 0 failures in 240 cells tested), to a high of 32%, that is 24 failures of 75 cells tested). When comparing the average blood penetration failures per cells tested, no significant difference was noticed between Examples 1 (i.e., average 2.8% failures), Example 2 (i.e., average 2.0% failures), and Example 3 (i.e., average 3.1%), even though the weight of the barrier layer was increased by 80%. Even if Example 3 was found to consistently pass the blood penetration test, at this weight, the fabric would be considered objectionably stiff and noisy which would limit its usefulness in the medical suite.

[0040] Table 4 summarizes results of the more stringent ASTM F1671 viral penetration test. This biological assay test is similar to F1670, however, with the addition of a viral surrogate phiX-174 bacteriophage to the synthetic blood test challenge. The same exposure parameters of 5 minutes at 0 pressure, 1 minute at 2 psig, and 54 minutes at 0 pressure are used. Examples of each embodiment are show in Table 4. Examples 1 and 2 show failures under F1670 and as expected, as well as subsequent failures under F1671. Example 3, which is the heavyweight microporous coating, shows a pass under F1670, and variable results under F1671. Example 4 represents 2 plies of example 1 and passes the F1670 test as well as the F1671 test. Unexpectedly, Example 5 represents a single layer of Example 1 tested in combination with a single layer of Sontara® Medical Grade (DuPont). Sontara® is a hydroentangled nonwoven that has been treated with a liquid repellency. The material exhibits high air permeability and as such, is very comfortable, but by itself offers very little resistance to blood and will fail the F1670 test almost immediately. However, when used in combination with a layer of incrementally stretched calcium carbonated filled polyolefin film, a very comfortable, quiet, blood and viral resistant composite is created. This unexpected result would appear to significantly broaden the types of materials that could be used in a 2-ply configuration to pass the requirements of ASTM F1671.

TABLE 3
BLOOD PENETRATION RESISTANCE
				MVTR	Blood
				(%	Penetration
Example	Weight	Color		open	failures/# cells
No.	coating/substrate	film/substrate	Airflow	cup)	tested)
1	25 gsm/0.5 osy	white/white	86	42	2/120
		white/white	126	50	7/360
		white/blue	82	41	3/120
		white/blue	121	49	9/360
		blue/blue	63	34	1/120
		blue/blue	123	52	8/360
		blue/white	71	41	5/120
		blue/white	118	41	16/360
		blue/white	127	47	10/240
2	30 gsm/1.0 osy	blue/white	123	54	4/240
		blue/white	140	63	4/240
		blue/blue	128	58	5/240
		yellow/yellow	115	41	6/240
3	45 gsm/1.0 osy	blue/white	117	57	0/240
		white/white	78	40	0/120
		white/white	134	55	0/120
		white/white	126	50	0/120
		white/blue	70	35	1/120
		white/blue	134	53	5/360
		white/blue	133	62	2/1-5
		blue/blue	122	51	7/360
		blue/blue	140	65	9/120
		blue/blue	156	70	7/120
		blue/blue	191	70	12/120
		blue/blue	193	78	24/75
		blue/blue	125	55	1/240
4	25 gsm/0.5 osy	blue/white//blue/white	n/t	41	0/120
	(2-ply using
	same fabric)
5	25 gsm/0.5 osy	blue/white//Sontara	n/t	n/t	n/t
	(2-ply using
	Sontara ®
	Medical Grade)

[0041]

TABLE 4
VIRAL RESISTANCE
Example	Coating	Substrate			F1670
No.	Weight	Weight	# of Plies	MVTR	(mod.)	F1671
1	25 gsm	0.5 osy	1	47%	10/240	n/t
2	30 gsm	1.0 osy	1	54%	4/240	Fail
3	45 gsm	1.0 osy	1	57%	0/240	6 Pass
						1 Fail
4	25 gsm	.5 osy	2(w/	41%	0/120	6 Pass
			same)
5	25 gsm	.5 osy	2	n/t	n/t	Pass
			(w/Sontara
			Medical
			Grade)

[0042] Numerous modifications and other embodiments of the inventions set forth herein will come to mind to one skilled in the art to which these inventions pertain having the benefit of the teachings presented in the foregoing descriptions and the associated drawings. Therefore, it is to be understood that the inventions are not to be limited to the specific embodiments disclosed and that modifications and other embodiments are intended to be included within the scope of the appended claims. Although specific terms are employed herein, they are used in a generic and descriptive sense only and not for purposes of limitation.

Claims

1. A nonwoven composite fabric comprising: a first microporous ply comprising a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently incrementally stretched to impart microporosity, and at least one additional ply positioned adjacent said first microporous ply in opposing surface-to-surface relationship, and wherein said nonwoven composite fabric has barrier properties passing the ASTM F1671 viral barrier test.

2. The composite fabric of claim 1, wherein said first and second at least one additional ply fail the ASTM F1671 viral barrier test when tested as individual layers.

3. The composite fabric of claim 1 wherein the MVTR of the composite fabric is at least 300 g/m2/24 hr.

4. The composite fabric of claim 3 where the MVTR is at least 600 g/m2/24 hr.

5. The composite fabric of claim 1 additionally including discrete bond sites connecting said first microporous ply to said at least one additional ply to form the composite fabric.

6. The composite fabric of claim 5, including a discontinuous adhesive forming said bond sites connecting said first microporous ply to said at least one additional ply.

7. The composite fabric of claim 5, including thermal or ultrasonic bonds forming said bond sites connecting said first microporous ply to said at least one additional ply.

8. The composite fabric of claim 1, wherein said microporous ply and said at least one additional ply are separate from one another over substantially the entire extent of their opposing surfaces, and wherein peripheral portions of the plies are connected to one another to maintain the plies in close proximity to each other.

9. The composite fabric of claim 8, wherein the plies are connected to each other along peripheral portions by stitching.

10. The composite fabric of claim 8, wherein the plies are connected to each other along peripheral portions by thermal or ultrasonic bonding.

11. The composite fabric of claim 1, wherein said at least one additional ply comprises a second microporous ply comprising a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently incrementally stretched to impart microporosity.

12. The composite fabric of claim 1, wherein said at least one additional ply comprises an unsupported microporous film.

13. The composite fabric of claim 1, wherein said at least one additional ply comprises a nonwoven fabric.

14. The composite fabric of claim 13, wherein said nonwoven fabric is a fabric selected from the group consisting of spunbond nonwovens, hydroentangled nonwovens, carded nonwovens, air-laid nonwovens, wet-laid nonwovens, meltblown nonwovens, or composites or laminates of such nonwovens.

15. The composite fabric of claim 1, which is formed from gamma radiation stable materials.

16. Medical protective apparel fabricated from the composite fabric of claim 1.

17. Medical protective apparel of claim 16 in the form of medical gowns, foot covers, head covers, face masks, or sleeve protectors.

18. A surgical drape fabricated from the composite fabric of claim 1.

19. A nonwoven composite fabric comprising: a first microporous ply comprising a nonwoven fabric substrate formed of substantially continuous filaments, an extrusion coating of a filler-containing microporous formable thermoplastic resin adhered to said nonwoven fabric substrate, and a multiplicity of micropores formed in said extrusion coating imparting microporosity to the ply and a MVTR of at least 300 g/m2/24 hr., and a second ply positioned adjacent said first microporous ply in opposing surface-to-surface relationship, wherein said first and second plies fail the ASTM F1671 viral barrier test when tested as individual layers, but said nonwoven composite fabric passes the ASTM F1671 viral barrier test.

20. The composite fabric of claim 19, including discrete bond sites interconnecting said first and second microporous plies.

21. The composite fabric of claim 19, wherein said first and second plies are separate from one another over substantially the entire extent of their opposing surfaces, and wherein peripheral portions of the plies are connected to one another to maintain the plies in close proximity to each other.

22. The composite fabric of claim 21, including at least one area of thermal or ultrasonic bonds connecting said first microporous ply to said second microporous ply along said peripheral portions.

23. The composite fabric of claim 19, wherein said microporous formable thermoplastic resin comprises a polyolefin resin containing calcium carbonate filler.

24. The composite fabric of claim 19, wherein said extrusion coating of microporous formable resin defines a film surface on one side of said first microporous ply and the nonwoven fabric substrate defines a nonwoven surface on the opposite side of said ply, and including a layer of discontinuous adhesive bonding said film surface of said first ply to said second microporous ply.

25. The composite fabric of claim 19, wherein said second microporous ply comprises a nonwoven fabric substrate formed of substantially continuous filaments, an extrusion coating of a filler-containing microporous formable thermoplastic resin adhered to said nonwoven fabric substrate, and a multiplicity of micropores formed in said extrusion coating imparting microporosity to the ply and a MVTR of at least 300 g/m2/24 hr.

26. The composite fabric of claim 25, wherein said extrusion coating of microporous formable resin defines a film surface on one side of said first and second microporous plies and the nonwoven fabric substrate defines a nonwoven surface on the opposite side of the respective plies, and including discrete bond sites bonding said first microporous ply to said second microporous ply.

27. The composite fabric of claim 26, wherein the film surface of said first ply is bonded to said film surface of said second ply.

28. The composite fabric of claim 26, wherein the nonwoven surface of said first ply is bonded to said nonwoven surface of said second ply.

29. The composite fabric of claim 26, wherein the film surface of said first ply is bonded to said nonwoven surface of said second ply.

30. The composite fabric of claim 19 wherein said second microporous ply is an unsupported film formed by incrementally stretching an extruded microporous formable precursor.

31. Medical protective apparel comprising two separate plies of microporous sheet material positioned in opposing surface-to-surface relationship to form a nonwoven composite, each ply comprising a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently stretched to impart microporosity, and the respective plies being connected together along seam lines, wherein each ply fails the ASTM F1671 viral barrier test when tested as an individual layer, but said nonwoven composite passes the ASTM F1671 viral barrier test.

32. Medical protective apparel according to claim 31, in the form of a gown having arm and frontal portions fabricated from said two plies of microporous sheet material, and wherein other portions of the gown are formed of a single ply of microporous sheet material.

33. Medical protective apparel according to claim 31, wherein said seam lines comprise lines of sewing.

34. Medical protective apparel according to claim 31, wherein said seam lines comprise lines of thermal or ultrasonic bonding.

35. Medical protective apparel comprising two individual plies of microporous sheet material positioned in opposing surface-to-surface relationship to form a nonwoven composite, each ply comprising a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently stretched to impart microporosity, and including discrete bond sites interconnecting the two plies, wherein each ply fails the ASTM F1671 viral barrier test when tested as an individual layer, but said nonwoven composite passes the ASTM F1671 viral barrier test.

36. Medical protective apparel according to claim 35, wherein the discrete bond sites are formed by a layer of discontinuous adhesive.

37. Medical protective apparel according to claim 35, wherein the discrete bond sites are formed by thermal or ultrasonic bonds.

38. Medical protective apparel comprising first and second individual plies of sheet material positioned in opposing surface-to-surface relationship to form a nonwoven composite, said first ply comprising a microporous formable resin that has been extrusion coated onto a nonwoven fabric substrate and subsequently stretched to impart microporosity, and said second ply comprising a nonwoven fabric, wherein said first and second plies fail the ASTM F1671 viral barrier test when tested as individual layers, but said nonwoven composite passes the ASTM F1671 viral barrier test.

39. A method of making a nonwoven composite fabric that passes the ASTM F1671 viral barrier test comprising: forming a first microporous ply by extrusion coating a microporous formable resin onto a nonwoven fabric substrate and stretching to impart microporosity, and positioning the first microporous ply adjacent at least one additional ply in opposing surface-to-surface relationship forming a nonwoven composite that has barrier properties passing the ASTM F1671 viral barrier test.

40. The method of claim 39, including the step of forming discrete bond sites connecting the respective plies to one another.

41. The method of claim 40, wherein the step of forming discrete bond sites comprises applying a discontinuous adhesive between said first microporous ply and said at least one additional ply and adhesively bonding the respective plies together to form said composite fabric.

42. The method of claim 40, wherein the step of forming discrete bond sites comprises thermally or ultrasonically bonding the first and second plies together to form said composite fabric.

43. The method of claim 39, including the step of sewing said first microporous ply and said at least one additional ply together along peripheral edges to form said composite fabric.

44. The method of claim 39, including forming a second microporous ply by extrusion coating a microporous formable resin onto a nonwoven fabric substrate and stretching to impart microporosity, and wherein said step of positioning the first microporous ply adjacent at least one additional microporous ply comprises positioning the first and second plies in opposing surface-to-surface relationship.

45. The method of claim 39, wherein said step of positioning the first microporous ply adjacent at least one additional microporous ply comprises positioning the first ply in opposing surface-to-surface relationship with a second microporous ply in the form of a microporous free film.

46. A method of making medical protective apparel comprising forming a first microporous ply by extrusion coating a microporous formable resin onto a nonwoven fabric substrate and stretching to impart microporosity, positioning the first microporous ply adjacent at least one additional ply in opposing surface-to-surface relationship forming a nonwoven composite, cutting the respective plies into a component of the medical protective apparel, and forming seam lines in the thus formed apparel component to join the respective plies of the to one another, and assembling the thus formed apparel component with other apparel components to form an article of medical protective apparel.