A longitudinal extending body with oriented fibers comprised of an organic compound, preferably cellulose fibers, with a hydrophilic and hydrophobic polymer having absorbable and non res sorbable qualities in the body, with an internal construction to promote cell growth. The longitudinal body has at least one wall having oriented fiber to include cellulose fiber extending the length of said body. This extending body has a surface that is smooth to the touch for additional processing methods such as machining, compression molding and 3 D printing.

A medical textile product includes a textile substrate having opposed first and second surfaces with the textile substrate including a textile construction of one or more yarns. The second surface includes a coating of a substantially water-insoluble, non-porous elastomeric sealant. The one or more yarns at the first surface are pre-treated with a removable composition, such that the water-insoluble elastomeric sealant encapsulates a portion of fibers of the one or more yarns at the second surface of the textile substrate. The textile substrate is substantially impermeable to fluid. The first surface is substantially free of the substantially water-insoluble elastomeric sealant. The textile substrate may be a non-tubular substrate, such as a planar sheet, a shaped sheet, and a tape, or a tubular substrate, such as a cylindrical conduit, a tubular conduit, a Y-shaped, a T-shaped conduit, a multi-channel conduit, and a bulbous shaped conduit.

The present invention discloses a degradable foldable biological amniotic membrane composite repair stent, comprising a tubular body with an axially extending through hole, the front end of the tubular body is provided with an elastic balloon, and the end of the tubular body is connected to a one-way valve which seals the through hole here, the outer face of the elastic balloon is coated with a foldable reticulated polylactic acid stent, the outer surface of the foldable reticulated polylactic acid stent is coated with a biological amniotic membrane, and there are a plurality of micropores on meshes of the foldable reticulated polylactic acid stent, the plurality of micropores are filled with biological amniotic membrane powder; in the initial state, the elastic balloon, the foldable reticulated polylactic acid stent, and the biological amniotic membrane are compressed into a tight state; in the use state, after being implanted in the body and expanded under pressure, it can conform to the lacrimal duct/uterine cavity to form a tubular or drop-like shape or other spatial shape that adapts to the body cavity.

The present invention discloses a degradable foldable biological amniotic membrane composite repair stent, comprising a tubular body with an axially extending through hole, the front end of the tubular body is provided with an elastic balloon, and the end of the tubular body is connected to a one-way valve which seals the through hole here, the outer face of the elastic balloon is coated with a foldable reticulated polylactic acid stent, the outer surface of the foldable reticulated polylactic acid stent is coated with a biological amniotic membrane, and there are a plurality of micropores on meshes of the foldable reticulated polylactic acid stent, the plurality of micropores are filled with biological amniotic membrane powder; in the initial state, the elastic balloon, the foldable reticulated polylactic acid stent, and the biological amniotic membrane are compressed into a tight state; in the use state, after being implanted in the body and expanded under pressure, it can conform to the lacrimal duct/uterine cavity to form a tubular or drop-like shape or other spatial shape that adapts to the body cavity.

Combination cellulose materials and methods of making and using these materials. The combination material includes a first cellulosic material and a second cellulosic material.

Combination cellulose materials and methods of making and using these materials. The combination material includes a first cellulosic material and a second cellulosic material.

Polymeric composite stents reinforced with fibers for implantation into a bodily lumen are disclosed.

Disclosed are hydrogels polymerized with or around a solid biofunctional moiety, biodegradable or permanent, designed to be implantable in a mammalian body, intended to block or mitigate the formation of tissue adhesions, and intended to aid in functional healing. The hydrogels of the present invention are characterized by comprising multiphasic structural elements: a) at least one gel phase, b) at least one solid phase, c) optional polymeric chains connecting gel and solid phases, d) optional shape designs that provide for an interpenetrating geometry between gels and solids, e) optional shape designs that enhance a tissue-hydrogel interface, and f) optional shape designs that provide a biofunctional aspect. The hydrophobicity of the various phases is chosen to reduce tissue adhesion and enhance tissue healing. The morphology of the polymers comprising the gel phase is typically of high molecular weight and has morphology that encourages entanglement. Useful polymeric structures include branching chains, comb or brush, and dendritic morphologies.

Stents fabricated from polymer composites toughened by a dispersed phase are disclosed.

The invention provides a patch and a patch preparation having an adhesive layer with a high adhesive force, wherein the hydrophobic adhesive layer does not bloom even when an organic fluid component having high polarity is contained therein. The patch contains a support and an adhesive layer on at least one surface of the support, wherein the adhesive layer contains a synthetic rubber having a viscosity average molecular weight of 500,000-1,600,000, an organic fluid component having high polarity, a tackifier, and magnesium aluminometasilicate. In the patch preparation, the above-mentioned adhesive layer further contains a drug.