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US20070009606A1 - Manufacturing process, such as three dimensional printing, including binding of water-soluble material followed by softening and flowing and forming films of organic-solvent-soluble material - Google Patents

Manufacturing process, such as three dimensional printing, including binding of water-soluble material followed by softening and flowing and forming films of organic-solvent-soluble material
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US20070009606A1
US20070009606A1US11/127,298US12729805AUS2007009606A1US 20070009606 A1US20070009606 A1US 20070009606A1US 12729805 AUS12729805 AUS 12729805AUS 2007009606 A1US2007009606 A1US 2007009606A1
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solvent
organic
soluble
soluble material
particles
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US11/127,298
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James Serdy
Emanuel Sachs
Thomas West
Sunil Saini
Jie Cai
Andrea Caruso
John Sharobiem
Peter Materna
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Massachusetts Institute of Technology
Theken Spine LLC
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Individual
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Assigned to THERICS, LLCreassignmentTHERICS, LLCASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: AFBS. INC.
Assigned to THERICS, LLCreassignmentTHERICS, LLCASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: WEST, THOMAS GEORGE, CARUSO, ANDREA B., MATERNA, PETER A., SAINI, SUNIL, CAI, JIE, SHAROBIEM, JOHN
Assigned to MASSACHUSETTS INSTITUTE OF TECHNOLOGYreassignmentMASSACHUSETTS INSTITUTE OF TECHNOLOGYASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: SERDY, JAMES G.
Publication of US20070009606A1publicationCriticalpatent/US20070009606A1/en
Assigned to MASSACHUSETTS INSTITUTE OF TECHNOLOGYreassignmentMASSACHUSETTS INSTITUTE OF TECHNOLOGYASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: SACHS, EMANUEL M.
Assigned to THEKEN SPINE, LLCreassignmentTHEKEN SPINE, LLCMERGER (SEE DOCUMENT FOR DETAILS).Assignors: THEKEN DISC, LLC, THERICS, LLC
Abandonedlegal-statusCriticalCurrent

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Abstract

The invention includes biostructures which may be characterized as having substantially all of the organic-solvent-soluble material in the form of a network of irregularly shaped perforated films. The biostructure may further include particles of a substantially-insoluble material, which may be a member of the calcium phosphate family. The biostructure may be osteoconductive. The biostructure may further contain an Active Pharmaceutical Ingredient or other bioactive substance. The API may be a substance which stimulates the production of bone morphogenetic protein, such as Lovastatin or related substances, thereby making the biostructure effectively osteoinductive. One or more of the polymers may have a resorption rate in the human body such as to control the release of the API. Methods of manufacture are also disclosed.

Description

Claims (37)

8. The biostructure ofclaim 1, wherein the organic-solvent-soluble material comprises at least one substance selected from the group consisting of polylactones; polyamines; polymers and copolymers of trimethylene carbonate with any other monomer; vinyl polymers; acrylic acid copolymers; polyethylene glycols; polyethylenes; Polylactides; Polyglycolides; Epsilon-caprolactone; Polylacatones; Polydioxanones; other Poly(alpha-hydroxy acids); Polyhydroxyalkonates; Polyhydroxybutyrates; Polyhydroxyvalerates; Polycarbonates; Polyacetals; Polyorthoesters; Polyamino acids and their esters; Polyphosphoesters; Polyesteramides; Polyfumerates; Polyanhydrides; Polycyanoacrylates; Poloxamers; Polysaccharides; Polyurethanes; Polyesters; Polyphosphazenes; Polyacetals; Polyalkanoates; Polyurethanes; Poly(lactic acid) (PLA); Poly(L-lactic acid) (PLLA); Poly (DL-lactic acid); Poly-DL-lactide-co-glycolide (PDLGA); Poly(L-lactide-co-glycolide) (PLLGA); Polycaprolactone (PCL); Poly-epsilon-caprolactone; Polycarbonates; Polyglyconates; Polyanhydrides; PLLA-co-GA; PLLA-co-GA 82:18; Poly-DL-lactic acid (PDLLA); PLLA-co-DLLA; PLLA-co-DLLA 50:50; PGA-co-TMC (Maxon B); Polyglycolic acid (PGA); Poly-p-dioxanone (PDS); PDLLA-co-GA; PDLLA-co-GA (85:15); aliphatic polyester elastomeric copolymer; epsilon-caprolactone and glycolide in a mole ratio of from about 35:65 to about 65:35; epsilon-caprolactone and glycolide in a mole ratio of from about 45:55 to about 35:65; epsilon-caprolactone and lactide selected from the group consisting of L-lactide, D-lactide and lactic acid copolymers in a mole ratio of epsilon-caprolactone to lactide of from about 35:65 to about 65:35; Poly(L-lactide and caprolactone in a ratio of about 70:30); poly (DL-lactide and caprolactone in a ratio of about 85:15); poly(DL-lactide and caprolactone and glycolic acid in a ratio of about 80:10:10); poly(DL-lacticde and caprolactone in a ratio of about 75:25); poly(L-lactide and glycolic acid in a ratio of about 85:15); poly(L-lactide and trimethylene carbonate in a ratio of about 70:30); poly(L-lactide and glycolic acid in a ratio of about 75:25); Gelatin; Collagen; Elastin; Alginate; Chitin; Hyaluronic acid; Aliphatic polyesters; Poly(amino acids); Copoly(ether-esters); Polyalkylene oxalates; Polyamides; Poly(iminocarbonates); Polyoxaesters; Polyamidoesters; Polyoxaesters containing amine groups; Poly(anhydrides); and mixtures, copolymers, and terpolymers thereof.
21. A method of manufacturing a biostructure, the method comprising:
forming at least one powder mixture by mixing particles of an organic-solvent-soluble material and particles of a water-soluble material;
manufacturing a preform by causing particles of the water-soluble material in the powder mixture to join or adhere to other particles of the water-soluble material to form a water-soluble structure which also contains or holds particles of the organic-solvent-soluble material;
forming a film of the organic-solvent-soluble material by causing particles of the organic-solvent-soluble material to soften and at least partially flow to conform to surfaces of the water-soluble structure; and
causing or allowing the organic-solvent-soluble material to harden, wherein forming the film of the organic-solvent-soluble material comprises exposing the preform to a fluid in a supercritical or critical state or at a pressure greater than half the critical pressure of the fluid, under suitable conditions and for a suitable time duration to cause organic-solvent-soluble material in the preform to soften and at least partially flow.
24. A method of manufacturing a biostructure, the method comprising:
forming at least one powder mixture by mixing particles of an organic-solvent-soluble material and particles of a water-soluble material;
manufacturing a preform by causing particles of the water-soluble material in the powder mixture to join or adhere to other particles of the water-soluble material to form a water-soluble structure which also contains or holds particles of the organic-solvent-soluble material;
forming a film of the organic-solvent-soluble material by exposing the preform to a vapor of an organic solvent in which the organic-solvent-soluble material is soluble, under suitable conditions and for a suitable time duration to cause organic-solvent-soluble material in the preform to soften and at least partially flow to conform to surfaces of the water-soluble structure;
causing or allowing enough of the organic solvent to escape from the preform so that the organic-solvent-soluble material hardens; and
exposing the preform to a clean-up solvent suitable to remove residual organic solvent,
wherein the clean-up solvent comprises carbon dioxide in a pressurized liquid, pressurized gas, critical or supercritical state.
25. A method of manufacturing a biostructure, the method comprising:
forming at least one powder mixture by mixing particles of an organic-solvent-soluble material and particles of a water-soluble material;
manufacturing a preform by causing particles of the water-soluble material in the powder mixture to join or adhere to other particles of the water-soluble material to form a water-soluble structure which also contains or holds particles of the organic-solvent-soluble material;
forming a film of the organic-solvent-soluble material by causing particles of the organic-solvent-soluble material to soften and at least partially flow to conform to surfaces of the water-soluble structure; and
causing or allowing the organic-solvent-soluble material to harden, wherein the organic-solvent-soluble material comprises an Active Pharamaceutical Ingredient.
US11/127,2982004-05-122005-05-12Manufacturing process, such as three dimensional printing, including binding of water-soluble material followed by softening and flowing and forming films of organic-solvent-soluble materialAbandonedUS20070009606A1 (en)

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US57041204P2004-05-122004-05-12
US11/127,298US20070009606A1 (en)2004-05-122005-05-12Manufacturing process, such as three dimensional printing, including binding of water-soluble material followed by softening and flowing and forming films of organic-solvent-soluble material

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US11/127,298AbandonedUS20070009606A1 (en)2004-05-122005-05-12Manufacturing process, such as three dimensional printing, including binding of water-soluble material followed by softening and flowing and forming films of organic-solvent-soluble material
US11/579,783Expired - Fee RelatedUS7815826B2 (en)2004-05-122005-05-12Manufacturing process, such as three-dimensional printing, including solvent vapor filming and the like
US12/899,033AbandonedUS20110076762A1 (en)2004-05-122010-10-06Articles formed by manufacturing processes, such as three-dimensional printing, including solvent vapor filming and the like

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US12/899,033AbandonedUS20110076762A1 (en)2004-05-122010-10-06Articles formed by manufacturing processes, such as three-dimensional printing, including solvent vapor filming and the like

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EP (1)EP1763703A4 (en)
JP (1)JP2007537007A (en)
CA (1)CA2564605A1 (en)
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US7815826B2 (en)2010-10-19
WO2005114322A2 (en)2005-12-01
EP1763703A4 (en)2010-12-08
US20080032083A1 (en)2008-02-07
US20110076762A1 (en)2011-03-31
WO2005114322A3 (en)2007-03-22
CA2564605A1 (en)2005-12-01
EP1763703A2 (en)2007-03-21
JP2007537007A (en)2007-12-20
WO2005114323A2 (en)2005-12-01
WO2005114323A3 (en)2006-12-21

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