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US20030082155A1 - Stem cells of the islets of langerhans and their use in treating diabetes mellitus - Google Patents

Stem cells of the islets of langerhans and their use in treating diabetes mellitus
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US20030082155A1
US20030082155A1US10/120,687US12068702AUS2003082155A1US 20030082155 A1US20030082155 A1US 20030082155A1US 12068702 AUS12068702 AUS 12068702AUS 2003082155 A1US2003082155 A1US 2003082155A1
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Prior art keywords
stem cell
cell
nestin
positive
cells
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Abandoned
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US10/120,687
Inventor
Joel Habener
Henryk Zulewski
Melissa Thomas
Elizabeth Abraham
Mario Vallejo
Colin Leech
Anna Nolan
Andreas Lechner
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General Hospital Corp
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Corning Optical Communications LLC
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Priority claimed from US09/731,261external-prioritypatent/US20010046489A1/en
Priority claimed from US09/963,875external-prioritypatent/US20020164307A1/en
Application filed by Corning Optical Communications LLCfiledCriticalCorning Optical Communications LLC
Priority to US10/120,687priorityCriticalpatent/US20030082155A1/en
Priority to PCT/US2002/030700prioritypatent/WO2003026584A2/en
Priority to AU2002331910Aprioritypatent/AU2002331910B2/en
Priority to CA002461861Aprioritypatent/CA2461861A1/en
Priority to IL16111902Aprioritypatent/IL161119A0/en
Priority to AT02768905Tprioritypatent/ATE489475T1/en
Priority to JP2003530223Aprioritypatent/JP2005533746A/en
Priority to CNA028231929Aprioritypatent/CN1589330A/en
Priority to DE60238431Tprioritypatent/DE60238431D1/en
Priority to EP02768905Aprioritypatent/EP1438418B1/en
Publication of US20030082155A1publicationCriticalpatent/US20030082155A1/en
Assigned to THE GENERAL HOSPITAL CORPORATIONreassignmentTHE GENERAL HOSPITAL CORPORATIONASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: ABRAHAM, ELIZABETH J., HABENER, JOEL F., THOMAS, MELISSA K., ZULEWSKI, HENRYK, LECHNER, ANDREAS, LEECH, COLIN A., NOLAN, ANNA LOUISE, VALLEJO, MARIO
Assigned to CORNING CABLE SYSTEMS LLCreassignmentCORNING CABLE SYSTEMS LLCCORRECTIVE ASSIGNMENT TO CORRECT THE SPELLING OF THE THIRD ASSIGNOR PREVIOUSLY RECORDED ON REEL 013993 FRAME 0921.Assignors: CLAPP, DONNIE R. JR., SMITH, KELLY J., STRAUSE, KEVIN L.
Priority to HK05100504.4Aprioritypatent/HK1067155A1/en
Priority to US11/438,790prioritypatent/US8110399B2/en
Abandonedlegal-statusCriticalCurrent

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Abstract

Methods and compositions are described for the treatment of type I insulin-dependent diabetes mellitus and other conditions using newly identified stem cells that are capable of differentiation into a variety of pancreatic islet cells, including insulin-producing beta cells, as well as hepatocytes. Nestin and ABCG2 have been identified as molecular markers for pancreatic stem cells, while cytokeratin-19 serves as a marker for a distinct class of islet ductal cells. Methods are described whereby nestin and/or ABCG2-positive stem cells can be isolated from pancreatic islets and cultured to obtain further stem cells or pseudo-islet like structures. Methods for ex vivo differentiation of the pancreatic stem cells are disclosed. Methods are described whereby pancreatic stem cells can be isolated, expanded, and transplanted into a patient in need thereof, either allogeneically, isogeneically or xenogenically, to provide replacement for lost or damaged insulin-secreting cells or other cells.

Description

Claims (88)

We claim:
1. A method of treating a patient with diabetes mellitus, comprising the steps of:
(a) isolating a nestin-positive pancreatic stem cell from a pancreatic islet of a donor; and
(b) transferring the stem cell into the patient, wherein the stem cell differentiates into an insulin-producing cell.
2. The method ofclaim 1, wherein said nestin-positive pancreatic stem cell is also ABCG2-positive.
3. The method ofclaim 1, wherein said nestin-positive pancreatic stem cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
4. The method ofclaim 1, wherein said nestin-positive pancreatic stem cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
5. A method of treating a patient with diabetes mellitus, comprising the steps of:
(a) isolating an ABCG2-positive pancreatic stem cell from a pancreatic islet of a donor; and
(b) transferring the stem cell into the patient, wherein the stem cell differentiates into an insulin-producing cell.
6. The method ofclaim 1 or5, wherein the patient serves as the donor for said stem cells of step a.
7. The method ofclaim 1 or5, wherein, prior to the step of transferring, the stem cell is treated ex vivo with an agent selected from the group consisting of EGF, bFGF-2, high glucose, KGF, HGF/SF, GLP-1, exendin-4, IDX-1, a nucleic acid molecule encoding IDX-1, betacellulin, activin A, TGF-β, and combinations thereof.
8. The method ofclaim 1 or5, wherein the step of transferring is performed via endoscopic retrograde injection.
9. The method ofclaim 1 or5, additionally comprising the step of:
(c) treating the patient with an immunosuppressive agent.
10. The method ofclaim 9, wherein the immunosuppressive agent is selected from the group consisting of FK-506, cyclosporin, and GAD65 antibodies.
11. A method of treating a patient with diabetes mellitus, comprising the steps of:
(a) isolating a nestin-positive pancreatic stem cell from a pancreatic islet of a donor;
(b) expanding the stem cell ex vivo to produce a progenitor cell; and
(c) transferring the progenitor cell into the patient, wherein the progenitor cell differentiates into an insulin-producing beta cell.
12. The method ofclaim 11, wherein said nestin-positive pancreatic stem cell is also ABCG2-positive.
13. The method ofclaim 11, wherein said nestin-positive pancreatic stem cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
14. The method ofclaim 11, wherein said nestin-positive pancreatic stem cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
15. A method of treating a patient with diabetes mellitus, comprising the steps of:
(a) isolating an ABCG2-positive pancreatic stem cell from a pancreatic islet of a donor;
(b) expanding the stem cell ex vivo to produce a progenitor cell; and
(c) transferring the progenitor cell into the patient, wherein the progenitor cell differentiates into an insulin-producing beta cell.
16. The method ofclaim 11 or15, wherein the patient serves as the donor for said stem cells of step a.
17. The method ofclaim 11 or15, wherein the step of expanding is performed in the presence of an agent selected from the group consisting of EGF, bFGF-2, high glucose, KGF, HGF/SF, GLP-1, exendin-4, IDX-1, a nucleic acid molecule encoding IDX-1, betacellulin, activin A, TGF-β, and combinations thereof.
18. The method ofclaim 11 or15, wherein the step of transferring is performed via endoscopic retrograde injection.
19. The method ofclaim 11 or15 additionally comprising the step of:
(d) treating the patient with an immunosuppressive agent.
20. The method ofclaim 19, wherein the immunosuppressive agent is selected from the group consisting of FK-506, cyclosporin, and GAD65 antibodies.
21. A method of treating a patient with diabetes mellitus, comprising the steps of:
(a) isolating a nestin-positive pancreatic stem cell from a pancreatic islet of a donor;
(b) expanding the stem cell to produce a progenitor cell;
(c) differentiating the progenitor cell in culture to form pseudo-islet like aggregates; and
(d) transferring the pseudo-islet like aggregates into the patient.
22. The method ofclaim 21, wherein said nestin-positive pancreatic stem cell is also ABCG2-positive.
23. The method ofclaim 21, wherein said nestin-positive pancreatic stem cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
24. The method ofclaim 21, wherein said nestin-positive pancreatic stem cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
25. A method of treating a patient with diabetes mellitus, comprising the steps of:
(a) isolating an ABCG2-positive pancreatic stem cell from a pancreatic islet of a donor;
(b) expanding the stem cell to produce a progenitor cell;
(c) differentiating the progenitor cell in culture to form pseudo-islet like aggregates; and
(d) transferring the pseudo-islet like aggregates into the patient.
26. The method ofclaim 21 or25, wherein the patient serves as the donor for said stem cells of step a.
27. The method ofclaim 21 or25, wherein the step of expanding is performed in the presence of an agent selected from the group consisting of EGF, bFGF-2, high glucose, KGF, HGF/SF, GLP-1, exendin-4, IDX-1, a nucleic acid molecule encoding IDX-1, betacellulin, activin A, TGF-β, and combinations thereof.
28. The method ofclaim 21 or25, wherein the step of transferring is performed via endoscopic retrograde injection.
29. The method ofclaim 21 or25 additionally comprising the step of:
(e) treating the patient with an immunosuppressive agent.
30. The method ofclaim 29, wherein the immunosuppressive agent is selected from the group consisting of FK-506, cyclosporin, and GAD65 antibodies.
31. A method of isolating a stem cell from a pancreatic islet of Langerhans, comprising the steps of:
(a) removing a pancreatic islet from a donor;
(b) culturing cells from the pancreatic islet; and
(c) selecting a nestin-positive clone from the culture.
32. The method ofclaim 31, wherein said nestin-positive clone is also an ABCG2-positive clone.
33. The method ofclaim 31, wherein said nestin-positive clone is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
34. The method ofclaim 31, wherein said nestin-positive clone does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
35. A method of isolating a stem cell from a pancreatic islet of Langerhans, comprising the steps of:
(a) removing a pancreatic islet from a donor;
(b) culturing cells from the pancreatic islet; and
(c) selecting an ABCG2-positive clone from the culture.
36. The method ofclaim 31 or35, wherein the culturing is first performed in a vessel coated with concanavalin A and then again performed in a vessel not coated with concanavalin A.
37. The method ofclaim 31 or35, comprising the additional step of:
(d) expanding the nestin-positive clone by treatment with an agent selected from the group consisting of EGF, bFGF-2, high glucose, KGF, HGF/SF, GLP-1, exendin-4, IDX1, a nucleic acid molecule encoding IDX-1, betacellulin, activin A, TGF-β, and combinations thereof.
38. The method ofclaim 35 comprising the additional step of:
(d) expanding the ABCG2-positive clone by treatment with an agent selected from the group consisting of EGF, bFGF-2, high glucose, KGF, HGF/SF, GLP-1, exendin-4, IDX-1, a nucleic acid molecule encoding IDX-1, betacellulin, activin A, TGF-β, and combinations thereof.
39. A method of inducing the differentiation of a nestin-positive pancreatic stem cell into a pancreatic progenitor cell, comprising the step of:
treating a nestin-positive pancreatic stem cell with an agent selected from the group consisting of EGF, bFGF-2, high glucose, KGF, HGF/SF, IDX-1, a nucleic acid molecule encoding IDX-1, GLP-1, exendin-4, betacellulin, activin A, TGF-β, and combinations thereof, whereby the stem cell subsequently differentiates into a pancreatic progenitor cell.
40. The method ofclaim 39, wherein said nestin-positive pancreatic stem cell is also an ABCG2-positive clone.
41. The method ofclaim 39, wherein said nestin-positive pancreatic stem cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
42. The method ofclaim 39, wherein said nestin-positive pancreatic stem cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
43. A method of inducing the differentiation of an ABCG2-positive pancreatic stem cell into a pancreatic progenitor cell, comprising the step of:
treating an ABCG2-positive pancreatic stem cell with an agent selected from the group consisting of EGF, bFGF-2, high glucose, KGF, HGF/SF, IDX-1, a nucleic acid molecule encoding IDX-1, GLP-1, exendin-4, betacellulin, activin A, TGF-β, and combinations thereof, whereby the stem cell subsequently differentiates into a pancreatic progenitor cell.
44. The method ofclaim 39 or43, wherein the pancreatic progenitor cell subsequently forms pseudo-islet like aggregates.
45. An isolated, nestin-positive human pancreatic or liver stem cell that is not a neural stem cell.
46. The isolated stem cell ofclaim 45, wherein said cell is also ABCG2-positive.
47. The isolated stem cell ofclaim 45, wherein said cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
48. The isolated stem cell ofclaim 45, wherein said cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
49. An isolated, ABCG2-positive human pancreatic or liver stem cell that is not a neural stem cell.
50. The isolated cell ofclaim 49, wherein said cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
51. The isolated cell ofclaim 49, wherein said cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
52. The isolated stem cell ofclaim 49, wherein said cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
53. The isolated stem cell ofclaim 45 or49, that differentiates to form insulin-producing beta cells.
54. The isolated stem cell ofclaim 45 or49, that differentiates to form glucagon-producing alpha cells.
55. The isolated stem cell ofclaim 45 or49, that differentiates to form pseudo-islet like aggregates.
56. The isolated stem cell ofclaim 45 or49, that differentiates to form hepatocytes.
57. A method of identifying a pancreatic cell as a stem cell, comprising the step of:
contacting a cell with a labeled nestin-specific antibody, whereby if the cell becomes labeled with the antibody the cell is identified as a stem cell.
58. The method ofclaim 57, further comprising the step of contacting a cell with a labeled antibody that binds to a marker selected from the group consisting of ABCG2, Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2, whereby if the cell becomes labeled with the antibody the cell is identified as a stem cell.
59. The method ofclaim 30 further comprising the step of:
contacting the cell with a labeled cytokeratin-19 specific antibody, whereby if the cell does not become labeled with the antibody the cell is identified as a stem cell.
60. The method ofclaim 57 further comprising the step of:
contacting the cell with a labeled collagen IV specific antibody, whereby if the cell does not become labeled with the antibody the cell is identified as a stem cell.
61. The method ofclaim 57, further comprising the step of contacting the cell with a labeled antibody that binds to a marker selected from the group consisting of of CD34, CD45, CD133, MHC class I and MHC class II, whereby if the cell does not become labeled with the antibody the cell is identified as a stem cell.
62. A method of inducing a nestin-positive pancreatic stem cell to differentiate into hepatocytes, comprising the step of:
treating the nestin-positive pancreatic stem cell with an effective amount of an agent that induces the stem cell to differentiate into hepatocytes or into progenitor cells that differentiate into hepatocytes.
63. The method ofclaim 62, wherein said nestin-positive pancreatic stem cell is also ABCG2-positive.
64. The method ofclaim 62, wherein said nestin-positive pancreatic stem cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
65. The method ofclaim 62, wherein said nestin positive pancreatic stem cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
66. A method of inducing an ABCG2-positive pancreatic stem cell to differentiate into hepatocytes, comprising the step of:
treating the ABCG2-positive pancreatic stem cell with an effective amount of an agent that induces the stem cell to differentiate into hepatocytes or into progenitor cells that differentiate into hepatocytes.
67. The method ofclaim 62 or66, wherein the agent is cyclopamine.
68. A method of treating a patient with liver disease, comprising the steps of:
(a) isolating a nestin-positive pancreatic stem cell from a pancreatic islet of a donor; and
(b) transferring the stem cell into the patient, wherein the stem cell differentiates into a hepatocyte.
69. The method ofclaim 68, wherein said nestin-positive pancreatic stem cell is also ABCG2-positive.
70. The method ofclaim 68, wherein said nestin-positive pancreatic stem cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
71. The method ofclaim 68, wherein said nestin positive pancreatic stem cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
72. A method of treating a patient with liver disease, comprising the steps of:
(a) isolating an ABCG2-positive pancreatic stem cell from a pancreatic islet of a donor; and
(b) transferring the stem cell into the patient, wherein the stem cell differentiates into a hepatocyte.
73. The method ofclaim 68 or72, wherein the patient serves as the donor for said stem cells of step a.
74. A method of treating a patient with liver disease, comprising the steps of:
(a) isolating a nestin-positive pancreatic stem cell from a pancreatic islet of a donor;
(b) expanding the stem cell ex vivo to produce a progenitor cell; and
(c) transferring the progenitor cell into the patient, wherein the progenitor cell differentiates into a hepatocyte.
75. The method ofclaim 74, wherein said nestin-positive pancreatic stem cell is also ABCG2-positive.
76. The method ofclaim 74, wherein said nestin-positive pancreatic stem cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
77. The method ofclaim 74, wherein said nestin positive pancreatic stem cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
78. A method of treating a patient with liver disease, comprising the steps of:
(a) isolating an ABCG2-positive pancreatic stem cell from a pancreatic islet of a donor;
(b) expanding the stem cell ex vivo to produce a progenitor cell; and
(c) transferring the progenitor cell into the patient, wherein the progenitor cell differentiates into a hepatocyte.
79. The method ofclaim 74 or78, wherein the patient serves as the donor for said stem cells of step a.
80. A method of treating a patient with liver disease, comprising the steps of:
(a) isolating a nestin-positive pancreatic stem cell from a pancreatic islet of a donor;
(b) differentiating the stem cell ex vivo to produce a hepatocyte; and
(c) transferring the hepatocyte into the patient.
81. The method ofclaim 80, wherein said nestin-positive pancreatic stem cell is also ABCG2-positive.
82. The method ofclaim 80, wherein said nestin-positive pancreatic stem cell is also positive for at least one of the markers selected from the group consisting of Oct3/4, GLP-1 receptor, latrophilin (type 2), Hes-1, Nestin, Integrin subunits α6 and β1, C-kit, MDR-1, SUR-1, or Kir 6.2.
83. The method ofclaim 80, wherein said nestin positive pancreatic stem cell does not express at least one of the markers selected from the group consisting of CD34, CD45, CD133, MHC class I and MHC class II.
84. A method of treating a patient with liver disease, comprising the steps of:
(a) isolating an ABCG2-positive pancreatic stem cell from a pancreatic islet of a donor;
(b) differentiating the stem cell ex vivo to produce a hepatocyte; and
(c) transferring the hepatocyte into the patient.
85. The method ofclaim 80 or84, wherein the patient serves as the donor for said stem cells of step a.
86. A pharmaceutical composition comprising the isolated stem cell ofclaim 45 admixed with a physiologically compatible carrier.
87. A pharmaceutical composition comprising the isolated stem cell ofclaim 46 admixed with a physiologically compatible carrier.
88. A pharmaceutical composition comprising the isolated stem cell ofclaim 49 admixed with a physiologically compatible carrier.
US10/120,6871999-12-062002-04-11Stem cells of the islets of langerhans and their use in treating diabetes mellitusAbandonedUS20030082155A1 (en)

Priority Applications (12)

Application NumberPriority DateFiling DateTitle
US10/120,687US20030082155A1 (en)1999-12-062002-04-11Stem cells of the islets of langerhans and their use in treating diabetes mellitus
DE60238431TDE60238431D1 (en)2001-09-262002-09-26 STRAIN CELLS OF LANGERHANS ISLANDS AND THEIR USE IN THE TREATMENT OF DIABETES MELLITUS
AU2002331910AAU2002331910B2 (en)2001-09-262002-09-26Stem cells of the islets of langerhans and their use in treating diabetes mellitus
AT02768905TATE489475T1 (en)2001-09-262002-09-26 ISLANDS OF LANGERHANS STEM CELLS AND THEIR USE IN THE TREATMENT OF DIABETES MELLITUS
EP02768905AEP1438418B1 (en)2001-09-262002-09-26Stem cells of the islets of langerhans and their use in treating diabetes mellitus
CA002461861ACA2461861A1 (en)2001-09-262002-09-26Stem cells of the islets of langerhans and their use in treating diabetes mellitus
IL16111902AIL161119A0 (en)2001-09-262002-09-26Stem cells of the islets of langerhans and their use in treating diabetes mellitus
PCT/US2002/030700WO2003026584A2 (en)2001-09-262002-09-26Stem cells of the islets of langerhans and their use in treating diabetes mellitus
JP2003530223AJP2005533746A (en)2001-09-262002-09-26 Islets of Langerhans and their use in the treatment of diabetes mellitus
CNA028231929ACN1589330A (en)2001-09-262002-09-26Stem cells of the islets of langerhans and their use in treating diabetes
HK05100504.4AHK1067155A1 (en)2001-09-262005-01-19Stem cells of the islets of langerhans and their use in treating diabetes mellitus
US11/438,790US8110399B2 (en)2000-10-062006-05-22Stem cells of the islets of langerhans and their use in treating diabetes mellitus

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US16908299P1999-12-061999-12-06
US09/731,261US20010046489A1 (en)1999-12-062000-12-06Stem cells of the islets of langerhans and their use in treating diabetes mellitus
US09/963,875US20020164307A1 (en)1999-12-062001-09-26Stem cells of the islets of langerhans and their use in treating diabetes mellitus
US10/120,687US20030082155A1 (en)1999-12-062002-04-11Stem cells of the islets of langerhans and their use in treating diabetes mellitus
US10/136,891US6923959B2 (en)1999-12-062002-05-02Method of pre-inducing a state of immune tolerance before organ transplantation

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US09/731,261Continuation-In-PartUS20010046489A1 (en)1999-12-062000-12-06Stem cells of the islets of langerhans and their use in treating diabetes mellitus
US09/963,875Continuation-In-PartUS20020164307A1 (en)1999-12-062001-09-26Stem cells of the islets of langerhans and their use in treating diabetes mellitus
US09/963,845Continuation-In-PartUS6655752B2 (en)1999-04-302001-09-26Device for activating trailer electric wheel brakes

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CN (1)CN1589330A (en)
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AU (1)AU2002331910B2 (en)
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EP1438418A4 (en)2005-12-21
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US20070128176A1 (en)2007-06-07
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EP1438418B1 (en)2010-11-24

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