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US20180325830A1 - Coated biological composition - Google Patents

Coated biological composition
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Publication number
US20180325830A1
US20180325830A1US15/898,558US201815898558AUS2018325830A1US 20180325830 A1US20180325830 A1US 20180325830A1US 201815898558 AUS201815898558 AUS 201815898558AUS 2018325830 A1US2018325830 A1US 2018325830A1
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US
United States
Prior art keywords
biological composition
coated
coated biological
mixture
protectant
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Pending
Application number
US15/898,558
Inventor
Timothy Ganey
Tracy Scott Anderson
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Vivex Biologics Group Inc
Original Assignee
Vivex Biomedical Inc
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
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Priority claimed from US15/590,444external-prioritypatent/US20170247659A1/en
Priority claimed from US15/837,694external-prioritypatent/US11160904B2/en
Application filed by Vivex Biomedical IncfiledCriticalVivex Biomedical Inc
Priority to US15/898,558priorityCriticalpatent/US20180325830A1/en
Publication of US20180325830A1publicationCriticalpatent/US20180325830A1/en
Assigned to HERITAGE BANK OF COMMERCEreassignmentHERITAGE BANK OF COMMERCESECURITY INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: ADVANCED NUMED TECHNOLOGIES, LTD., UMTB BIOMEDICAL, INC., VIVEX BIOMEDICAL INTERNATIONAL, INC., VIVEX BIOMEDICAL, INC.
Assigned to VIVEX BIOLOGICS, INC.reassignmentVIVEX BIOLOGICS, INC.CHANGE OF NAME (SEE DOCUMENT FOR DETAILS).Assignors: VIVEX BIOMEDICAL, INC.
Assigned to VIVEX BIOLOGICS GROUP, INC.reassignmentVIVEX BIOLOGICS GROUP, INC.CHANGE OF NAME (SEE DOCUMENT FOR DETAILS).Assignors: VIVEX BIOLOGICS, INC.
Assigned to VIVEX BIOMEDICAL, INC.reassignmentVIVEX BIOMEDICAL, INC.ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: ANDERSON, Tracy Scott, GANEY, TIMOTHY
Assigned to BANKUNITED, N.A.reassignmentBANKUNITED, N.A.NOTICE OF GRANT OF SECURITY INTEREST IN PATENTSAssignors: VIVEX BIOLOGICS GROUP, INC.
Assigned to VIVEX BIOMEDICAL, INC., ADVANCED NUMED TECHNOLOGIES, LTD., VIVEX BIOMEDICAL INTERNATIONAL, INC., UMTB BIOMEDICAL, INCreassignmentVIVEX BIOMEDICAL, INC.RELEASE BY SECURED PARTY (SEE DOCUMENT FOR DETAILS).Assignors: HERITAGE BANK OF COMMERCE
Priority to US17/072,625prioritypatent/US12226532B2/en
Assigned to HERITAGE BANK OF COMMERCEreassignmentHERITAGE BANK OF COMMERCESECURITY INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: VIVEX BIOLOGICS GROUP, INC.
Assigned to VIVEX BIOLOGICS GROUP, INC.reassignmentVIVEX BIOLOGICS GROUP, INC.RELEASE BY SECURED PARTY (SEE DOCUMENT FOR DETAILS).Assignors: BANKUNITED, N.A.
Pendinglegal-statusCriticalCurrent

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Abstract

A coated biological composition has a mixture of biologic material and a volume of a liquid protectant. The mixture of biologic material has non-whole cellular components or whole cells or combinations of the non-whole cellular components and whole cells, wherein the mixture is compatible with biologic function. The volume of a liquid protectant is intermixed with the mixture of biologic material, wherein the liquid protectant forms a coating externally enveloping each of the non-whole cellular components, if any, and each of the whole cells, if any, of the mixture of biologic material, to form the coated biological composition. The coated biological composition is frozen and thereafter thawed and then frozen a second time for storage or frozen at least once and thawed and stored under refrigeration above freezing, or frozen and thawed and then concentrated by drying, or while frozen without thawing lyophilized for ambient or room temperature storage.

Description

Claims (65)

What is claimed is:
1. A coated biological composition comprising:
a mixture of biologic material having non-whole cellular components including vesicular components and active and inactive components of biological activity, cell fragments, cellular excretions, cellular derivatives, and extracellular components, or whole cells or combinations of the non-whole cellular components and whole cells, wherein the mixture is compatible with biologic function;
a volume of a liquid protectant intermixed with the mixture of biologic material; and
wherein the liquid protectant forms a coating externally enveloping each of the non-whole cellular components, if any, and each of the whole cells, if any, of the mixture of biologic material, to form the coated biological composition and wherein the coated biological composition is frozen and thereafter thawed and then frozen a second time for storage or frozen at least once and thawed and stored under refrigeration above freezing, or frozen and thawed and then concentrated by drying, or while frozen without thawing lyophilized for ambient or room temperature storage.
2. The coated biological composition ofclaim 1 wherein the thawed coated biological composition re-frozen for storage prior to use.
3. The coated biological composition ofclaim 1 wherein the thawed coated biological composition is refrigerated above freezing for storage prior to use.
4. The coated biological composition ofclaim 1 wherein the thawed coated composition is processed to be stored at room temperature for storage.
5. The coated biological composition ofclaim 1 wherein the thawed coated biological composition is concentrated by drying prior to being stored at room temperature to form a dried coated biological composition.
6. The coated biological composition ofclaim 5 wherein the coated biological composition is freeze dried or hypothermic dehydrated.
7. The coated biological composition ofclaim 6 wherein the dried coated biological composition is micronized into particles of 1000 microns or less.
8. The coated biological composition ofclaim 6 wherein the dried coated biological composition is micronized into particles of 400 microns or less.
9. The coated biological composition ofclaim 1 wherein the liquid protectant is a polyampholyte protectant or polyampholyte cryoprotectant.
10. The coated biological composition ofclaim 1 wherein the liquid protectant is a polyampholyte protectant or polyampholyte cryoprotectant, or a glycerol-based protectant, or dimethyl sulfoxide (DMSO) or glycols or trehalose or other molecular hydrogel preservatives or sucrose or dextrose based protectant.
11. The coated biological composition ofclaim 1 wherein the liquid protectant is dimethyl sulfoxide (DMSO).
12. The coated biological composition ofclaim 5 wherein the dried coated biological composition has a moisture content of 5% or less.
13. The coated biological composition ofclaim 12 wherein an initial volume of the liquid protectant when reduced to a solid for drying or freeze-drying yields 5% or less of the initial volume.
14. The coated biological composition ofclaim 13 wherein the dried coated biological composition when reconstituted in a liquid is suitable for direct implantation.
15. The coated biological composition ofclaim 1 further comprises a volume of cartilage particles, the particles intermixed with the biological material and coated with the liquid protectant.
16. The coated biological composition ofclaim 1 further comprises a volume of nucleus pulposus particles.
17. The coated biological composition ofclaim 1 wherein the coating deters attachment to other cells for a predetermine time.
18. The coated biological composition ofclaim 1 wherein the coating buffers inflammation.
19. The coated biological composition ofclaim 1 wherein the liquid protectant is a polyampholyte protectant of a polyamine polymer compound.
20. The coated biological composition ofclaim 1 wherein the coating retards or reduces premature differentiation of the whole cells of the mixture.
21. The coated biological composition ofclaim 1 wherein the coating sustains regenerative potential and biologic function of the mixture during preservation and implantation.
22. The coated biological composition ofclaim 1 wherein the coating is configured to be metabolized after implantation after a predetermined time.
23. The coated biological composition ofclaim 22 wherein the predetermined time is three or more days.
24. The coated biological composition ofclaim 23 wherein the predetermined time is up to six days.
25. The coated biological composition ofclaim 1 wherein the coating forms a spherical shell about each whole cell.
26. The coated biological composition ofclaim 19 wherein the polyampholyte protectant is a cryoprotectant.
27. The coated biological composition ofclaim 26 wherein the polyampholyte protectant forms a strong hydrophilic characteristic of the coating to protect the cell membrane external of the whole cells.
28. The coated biological composition ofclaim 27 wherein the protectant when frozen as a cryoprotectant interrupts crack propagation externally protecting the cell membrane.
29. The coated biological composition ofclaim 1 wherein the mixture is mechanically selected allogeneic biologic material derived from bone marrow.
30. The coated biological composition ofclaim 1 further comprises bone particles, the bone particles being added to the mixture and coated with liquid protectant.
31. The coated biological composition ofclaim 30 wherein the bone particles include a mixture of cortical bone particles and cancellous bone particles.
32. The coated biological composition ofclaim 29 wherein the mixture of mechanically selected material derived from bone marrow further includes a select number of non-whole cell fractions including one or more of exosomes, transcriptosomes, proteasomes, membrane rafts, lipid rafts.
33. The coated biological composition ofclaim 32 wherein the combination of non-whole cell components with a select number of the non-whole cell fractions sustains pluripotency in both graft or host cells or combinations thereof.
34. The coated biological composition ofclaim 33 wherein the select number of the non-whole cell fractions sustains pluripotency in graft or host cells or combinations thereof includes differentiated committed cells and non-differentiated and non-committed cells.
35. The coated biological composition ofclaim 29 wherein the biological composition is predisposed to demonstrate or support elaboration of active volume or spatial geometry consistent in morphology with that of endogenous bone.
36. The coated biological composition ofclaim 1 wherein the biological composition extends regenerative resonance that compliments or mimics tissue complexity.
37. The coated biological composition ofclaim 1 wherein the mixture is treated in the protectant prior to preservation or cryopreservation or freeze drying.
38. The coated biological composition ofclaim 37 wherein the protectant creates a physical or electrical or chemical gradient or combination thereof for tissue regeneration.
39. The coated biological composition ofclaim 38 wherein the gradient has a physical characteristic of modulus or topography such as charge density, field shape or cryo- or chemo-taxic tendencies.
40. The coated biological composition ofclaim 38 wherein the gradient has a chemical characteristic of spatially changing compositions of density or species of functional molecules, wherein the molecules can offer a fixed catalytic function as a co-factor.
41. The coated biological composition ofclaim 38 wherein the gradient has an electrical characteristic of charge based or pH based or electron affinities that confer metastability in biologic potential.
42. The coated biological composition ofclaim 29 wherein the bone marrow which is derived from a cadaver has separation-enhanced non-whole cell fractions vitality including one or more of the following: separating the fractions from cells heightens their vitality, reversing “arrest” of donors, accentuating responsive molecular coupling, matrix guarding in neutralizing inflammation or providing a basis for metabolic satience by balancing stimulus for repair.
43. The coated biological composition ofclaim 1 wherein the liquid protectant is a cryoprotectant polyampholyte of carboxylated polylysine.
44. The coated biological composition ofclaim 36 wherein the regenerative resonance occurs in the presence or absence of a refractory response.
45. The coated biological composition ofclaim 43 wherein the cryopreservation occurs at a temperature that is sub-freezing.
46. The coated biological composition ofclaim 45 wherein the cryopreservation temperature is from 0 degrees C. to −200 degrees C.
47. The coated biological composition ofclaim 1 wherein the mixture creates a physical or electrical or chemical gradient or combination thereof for tissue regeneration.
48. The coated biological composition ofclaim 47 wherein the gradient has a physical characteristic such as modulus or topography.
49. The coated biological composition ofclaim 47 wherein the gradient has a chemical characteristic such as spatially changing compositions of density or species of functional molecules.
50. The coated biological composition ofclaim 47 wherein the gradient has an electrical characteristic such as charge based or pH based.
51. The coated biological composition ofclaim 1 can be organelle fragments.
52. The coated biological composition ofclaim 1 wherein active and inactive components of biological activity can be extants of the human metabolome.
53. The coated biological composition ofclaim 43 wherein the composition is maintained at ambient temperature prior to freeze drying.
54. The coated biological composition ofclaim 1 wherein the mixture of biological material is intermixed with a liquid protectant of a polyampholyte protectant for direct implantation wherein said protectant is a 1-50 w/w % aqueous solution of at least one polyamine polymer compound comprised of at least one polymer of units having side-chain amino groups, said at least one polymer of units being selected from a group consisting of ε-poly-L-lysine, α-poly-L-lysine, poly-arginine, allylamine polymer and partially methoxy-carbonylated allylamine polymer; and 50-99 mol % of amino groups, other than those forming amino-acid-to-amino-acid linkages, of said at least one polymer compound is blocked with carboxylic anhydride to form pendant moieties, each of which is linked to main chain of the polymer via an amide linkage and essentially has a not-blocked carboxylic group.
55. The coated biological composition according toclaim 54, wherein said liquid protectant is obtained by dissolving the at least one polyamine polymer compound in a physiological solution.
56. The coated biological composition according toclaim 55, wherein the physiological solution is a saline, Dulbecco-modified eagle MEM culture medium (DMEM), or a culture medium for cells or tissues.
57. The coated biological composition according toclaim 54, wherein said at least one polymer compound is ε-poly-L-lysine having number-average molecular weight in a range of 1000-20,000.
58. The coated biological composition according toclaim 54, wherein remaining side-chain amino groups or remaining side-chain and terminal amino groups of the at least one polymer compound are not blocked by covalent bonding.
59. A method of making a coated biological composition comprises the steps of:
collecting, recovering and processing bone marrow from a cadaver donor;
mechanically separating cellular and non-cellular components of bone marrow from cadaverous bone;
concentrating by centrifugation and filtering;
separation by density gradient centrifugation;
collecting non-cellular fractions or non-cellular components or combinations thereof of predetermined density;
washing the non-cellular fractions or non-cellular components or combinations thereof to create a mixture;
quantifying non-whole cell fraction concentration exceeds zero;
suspending to a predetermined concentration in a liquid protectant;
freezing the mixture at a predetermined controlled rate; and
thereafter thawing and then freezing a second time for storage or frozen at least once thawed and stored under refrigeration above freezing, or frozen and thawed and then concentrated by drying, or while frozen without thawing lyophilized for ambient or room temperature storage.
60. A method of preparing the mixture for use made according to the method ofclaim 59 wherein the liquid protectant is a polyampholyte protectant or polyampholyte cryoprotectant, or a glycerol-based protectant, or dimethyl sulfoxide (DMSO) or glycols or trehalose or other molecular hydrogel preservatives or sucrose or dextrose based protectant.
61. The method of preparing the mixture for use made according to the method ofclaim 59 further comprises the step of adding a volume of cartilage particles, the particles intermixed with the biological material and coated with the liquid protectant.
62. The method of preparing the mixture for use made according to the method ofclaim 59 further comprises the step of adding a volume of nucleus pulposus particles, the particles intermixed with the biological material and coated with the liquid protectant.
63. The method of preparing the mixture for use made according to the method ofclaim 59 further comprises the step of adding a volume of bone particles, the particles intermixed with the biological material and coated with the liquid protectant.
64. The method of preparing the mixture for use made according to the method ofclaim 59 by the steps of:
diluting the mixture in saline without spinning; and
implanting the diluted mixture by packing, injection or any other suitable means into a patient.
65. The method of preparing the mixture for use made according to the method ofclaim 64 wherein the step of diluting the mixture includes warming the mixture at a temperature of 37 degrees C. for 2 to 3 minutes in a warm water bath.
US15/898,5582015-03-062018-02-17Coated biological compositionPendingUS20180325830A1 (en)

Priority Applications (2)

Application NumberPriority DateFiling DateTitle
US15/898,558US20180325830A1 (en)2017-05-092018-02-17Coated biological composition
US17/072,625US12226532B2 (en)2015-03-062020-10-16Coated biological composition

Applications Claiming Priority (5)

Application NumberPriority DateFiling DateTitle
US15/590,444US20170247659A1 (en)2015-03-062017-05-09Acellular biologic composition and method of manufacture
US15/590,475US10760058B2 (en)2015-03-062017-05-09Acellular biologic composition and method of manufacture
US15/591,513US10513690B2 (en)2015-03-062017-05-10Biologic composition and method of manufacture
US15/837,694US11160904B2 (en)2017-05-092017-12-11Biological composition in a protectant shroud and methods
US15/898,558US20180325830A1 (en)2017-05-092018-02-17Coated biological composition

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US15/590,475Continuation-In-PartUS10760058B2 (en)2015-03-062017-05-09Acellular biologic composition and method of manufacture
US15/590,444Continuation-In-PartUS20170247659A1 (en)2015-03-062017-05-09Acellular biologic composition and method of manufacture
US15/591,513Continuation-In-PartUS10513690B2 (en)2015-03-062017-05-10Biologic composition and method of manufacture
US15/837,694Continuation-In-PartUS11160904B2 (en)2015-03-062017-12-11Biological composition in a protectant shroud and methods

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US11779610B2 (en)2013-07-302023-10-10Musculoskeletal Transplant FoundationAcellular soft tissue-derived matrices and methods for using same
US11191788B2 (en)2013-07-302021-12-07Musculoskeletal Transplant FoundationAcellular soft tissue-derived matrices and methods for preparing same
US11524093B2 (en)2015-07-242022-12-13Musculoskeletal Transplant FoundationAcellular soft tissue-derived matrices and methods for preparing same
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KR20210026990A (en)*2019-08-292021-03-10충남대학교산학협력단Composition for cryopreservation of Canidae sperm comprising exosomes derived from conditioned media of mesenchymal stem cell as effective component
KR102235332B1 (en)*2019-08-292021-04-02충남대학교 산학협력단Composition for cryopreservation of Canidae sperm comprising exosomes derived from conditioned media of mesenchymal stem cell as effective component
US20230021326A1 (en)*2019-10-312023-01-26Uniwersytet JagiellonskiThe use of polyelectrolytes as cryoprotectants and a method of cryopreservation with their use
WO2021086211A1 (en)*2019-10-312021-05-06Uniwersytet JagiellońskiThe use of polyelectrolytes as cryoprotectants and a method of cryopreservation with their use
US20220080082A1 (en)*2020-09-112022-03-17Vivex Biologics Group, Inc.Infused cartilage particles
US20220080081A1 (en)*2020-09-112022-03-17Vivex Biologics Group, Inc.Infused cartilage fibers
US11738118B2 (en)*2020-09-112023-08-29Vivex Biologies Group, Inc.Infused cartilage particles
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