Microencapsulated islet allografts in diabetic NOD mice and nonhuman primates

S. A. Safley; N. S. Kenyon; D. M. Berman; G. F. Barber; H. Cui; S. Duncanson; T. De Toni; M. Willman; P. De Vos; A. A. Tomei; A. Sambanis; N. M. Kenyon; C. Ricordi; C. J. Weber

doi:10.26355/eurrev_202008_22651

Microencapsulated islet allografts in diabetic NOD mice and nonhuman primates

S. A. Safley
, N. S. Kenyon
, D. M. Berman
, G. F. Barber
, H. Cui
, S. Duncanson
, T. De Toni
, M. Willman
, P. De Vos
, A. A. Tomei
, A. Sambanis
, N. M. Kenyon
, C. Ricordi
, C. J. Weber

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

OBJECTIVE: Our goal was to assess the efficacy of encapsulated allogenelc Islets transplanted in diabetic NOD mice and streptozotocin (STZ)-diabetic nonhuman primates (NHPs).MATERIALS AND METHODS: Murine or NHP islets were microencapsulated and transplanted in non-immunosuppressed mice or NHPs given clinically-acceptable immunosuppressive regimens, respectively. Two NHPs were treated with autologous mesenchymal stem cells (MSCs) and peri-transplant oxygen therapy. Different transplant sites (intraperitoneal [i.p.], omental pouch, omental surface, and bursa omentalis) were tested in separate NHPs. Graft function was monitored by exogenous insulin requirements. fasting blood glucose levels, glucose tolerance tests, percent hemoglobin A1c (%HbA1c), and C-peptide levels. In vitro assessment of grafts included histology, immunohistochemistry. and viability staining; host immune responses were characterized by flow cytometry and cytokine/chemokine multiplex ELISAS.RESULTS: Microencapsulated islet allografts functioned long-term i.p. in diabetic NOD mice without immunosuppression, but for a relatively short time in immunosuppressed NHPs. In the NHPs, encapsulated allo-islets initially reduced hyperglycemia. decreased exogenous insulin requirements, elevated C-peptide levels, and lowered % HbA1c in plasma, but graft function diminished with time, regardless of transplant site. At necropsy. microcapsules were intact and non-fibrotic, but many islets exhibited volume loss, central necrosis and endogenous markers of hypoxia. Animals receiving supplemental oxy- gen and autologous MSCs showed improved graft function for a longer post-transplant period. In diabetic NHPs and mice, cell-free microcapsules did not elicit a fibrotic response.CONCLUSIONS: The evidence suggested that hypoxia was a major factor for damage to encapsulated islets in vivo. To achieve long-term function, new approaches must be developed to increase the oxygen supply to microencapsulated islets and/or identify donor insulin-secreting cells which can tolerate hypoxia.

Original language	English
Pages (from-to)	8551-8565
Number of pages	15
Journal	European Review for Medical and Pharmacological Sciences
Volume	24
Issue number	16
DOIs	https://doi.org/10.26355/eurrev_202008_22651
Publication status	Published - 2020

Keywords

Diabetes
Hypoxia
Islet transplantation
Microencapsulation
Nonhuman primates

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10.26355/eurrev_202008_22651

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Safley, S. A., Kenyon, N. S., Berman, D. M., Barber, G. F., Cui, H., Duncanson, S., De Toni, T., Willman, M., De Vos, P., Tomei, A. A., Sambanis, A., Kenyon, N. M., Ricordi, C., & Weber, C. J. (2020). Microencapsulated islet allografts in diabetic NOD mice and nonhuman primates. European Review for Medical and Pharmacological Sciences, 24(16), 8551-8565. https://doi.org/10.26355/eurrev_202008_22651

@article{a5c025ac4cd34cec9321c1079d167291,

title = "Microencapsulated islet allografts in diabetic NOD mice and nonhuman primates",

abstract = "OBJECTIVE: Our goal was to assess the efficacy of encapsulated allogenelc Islets transplanted in diabetic NOD mice and streptozotocin (STZ)-diabetic nonhuman primates (NHPs).MATERIALS AND METHODS: Murine or NHP islets were microencapsulated and transplanted in non-immunosuppressed mice or NHPs given clinically-acceptable immunosuppressive regimens, respectively. Two NHPs were treated with autologous mesenchymal stem cells (MSCs) and peri-transplant oxygen therapy. Different transplant sites (intraperitoneal [i.p.], omental pouch, omental surface, and bursa omentalis) were tested in separate NHPs. Graft function was monitored by exogenous insulin requirements. fasting blood glucose levels, glucose tolerance tests, percent hemoglobin A1c (\%HbA1c), and C-peptide levels. In vitro assessment of grafts included histology, immunohistochemistry. and viability staining; host immune responses were characterized by flow cytometry and cytokine/chemokine multiplex ELISAS.RESULTS: Microencapsulated islet allografts functioned long-term i.p. in diabetic NOD mice without immunosuppression, but for a relatively short time in immunosuppressed NHPs. In the NHPs, encapsulated allo-islets initially reduced hyperglycemia. decreased exogenous insulin requirements, elevated C-peptide levels, and lowered \% HbA1c in plasma, but graft function diminished with time, regardless of transplant site. At necropsy. microcapsules were intact and non-fibrotic, but many islets exhibited volume loss, central necrosis and endogenous markers of hypoxia. Animals receiving supplemental oxy- gen and autologous MSCs showed improved graft function for a longer post-transplant period. In diabetic NHPs and mice, cell-free microcapsules did not elicit a fibrotic response.CONCLUSIONS: The evidence suggested that hypoxia was a major factor for damage to encapsulated islets in vivo. To achieve long-term function, new approaches must be developed to increase the oxygen supply to microencapsulated islets and/or identify donor insulin-secreting cells which can tolerate hypoxia.",

keywords = "Diabetes, Hypoxia, Islet transplantation, Microencapsulation, Nonhuman primates",

author = "Safley, \{S. A.\} and Kenyon, \{N. S.\} and Berman, \{D. M.\} and Barber, \{G. F.\} and H. Cui and S. Duncanson and \{De Toni\}, T. and M. Willman and \{De Vos\}, P. and Tomei, \{A. A.\} and A. Sambanis and Kenyon, \{N. M.\} and C. Ricordi and Weber, \{C. J.\}",

year = "2020",

doi = "10.26355/eurrev\_202008\_22651",

language = "English",

volume = "24",

pages = "8551--8565",

journal = "European Review for Medical and Pharmacological Sciences",

issn = "1128-3602",

publisher = "Verduci Editore s.r.l",

number = "16",

}

Safley, SA, Kenyon, NS, Berman, DM, Barber, GF, Cui, H, Duncanson, S, De Toni, T, Willman, M, De Vos, P, Tomei, AA, Sambanis, A, Kenyon, NM, Ricordi, C & Weber, CJ 2020, 'Microencapsulated islet allografts in diabetic NOD mice and nonhuman primates', European Review for Medical and Pharmacological Sciences, vol. 24, no. 16, pp. 8551-8565. https://doi.org/10.26355/eurrev_202008_22651

TY - JOUR

T1 - Microencapsulated islet allografts in diabetic NOD mice and nonhuman primates

AU - Safley, S. A.

AU - Kenyon, N. S.

AU - Berman, D. M.

AU - Barber, G. F.

AU - Cui, H.

AU - Duncanson, S.

AU - De Toni, T.

AU - Willman, M.

AU - De Vos, P.

AU - Tomei, A. A.

AU - Sambanis, A.

AU - Kenyon, N. M.

AU - Ricordi, C.

AU - Weber, C. J.

PY - 2020

Y1 - 2020

N2 - OBJECTIVE: Our goal was to assess the efficacy of encapsulated allogenelc Islets transplanted in diabetic NOD mice and streptozotocin (STZ)-diabetic nonhuman primates (NHPs).MATERIALS AND METHODS: Murine or NHP islets were microencapsulated and transplanted in non-immunosuppressed mice or NHPs given clinically-acceptable immunosuppressive regimens, respectively. Two NHPs were treated with autologous mesenchymal stem cells (MSCs) and peri-transplant oxygen therapy. Different transplant sites (intraperitoneal [i.p.], omental pouch, omental surface, and bursa omentalis) were tested in separate NHPs. Graft function was monitored by exogenous insulin requirements. fasting blood glucose levels, glucose tolerance tests, percent hemoglobin A1c (%HbA1c), and C-peptide levels. In vitro assessment of grafts included histology, immunohistochemistry. and viability staining; host immune responses were characterized by flow cytometry and cytokine/chemokine multiplex ELISAS.RESULTS: Microencapsulated islet allografts functioned long-term i.p. in diabetic NOD mice without immunosuppression, but for a relatively short time in immunosuppressed NHPs. In the NHPs, encapsulated allo-islets initially reduced hyperglycemia. decreased exogenous insulin requirements, elevated C-peptide levels, and lowered % HbA1c in plasma, but graft function diminished with time, regardless of transplant site. At necropsy. microcapsules were intact and non-fibrotic, but many islets exhibited volume loss, central necrosis and endogenous markers of hypoxia. Animals receiving supplemental oxy- gen and autologous MSCs showed improved graft function for a longer post-transplant period. In diabetic NHPs and mice, cell-free microcapsules did not elicit a fibrotic response.CONCLUSIONS: The evidence suggested that hypoxia was a major factor for damage to encapsulated islets in vivo. To achieve long-term function, new approaches must be developed to increase the oxygen supply to microencapsulated islets and/or identify donor insulin-secreting cells which can tolerate hypoxia.

AB - OBJECTIVE: Our goal was to assess the efficacy of encapsulated allogenelc Islets transplanted in diabetic NOD mice and streptozotocin (STZ)-diabetic nonhuman primates (NHPs).MATERIALS AND METHODS: Murine or NHP islets were microencapsulated and transplanted in non-immunosuppressed mice or NHPs given clinically-acceptable immunosuppressive regimens, respectively. Two NHPs were treated with autologous mesenchymal stem cells (MSCs) and peri-transplant oxygen therapy. Different transplant sites (intraperitoneal [i.p.], omental pouch, omental surface, and bursa omentalis) were tested in separate NHPs. Graft function was monitored by exogenous insulin requirements. fasting blood glucose levels, glucose tolerance tests, percent hemoglobin A1c (%HbA1c), and C-peptide levels. In vitro assessment of grafts included histology, immunohistochemistry. and viability staining; host immune responses were characterized by flow cytometry and cytokine/chemokine multiplex ELISAS.RESULTS: Microencapsulated islet allografts functioned long-term i.p. in diabetic NOD mice without immunosuppression, but for a relatively short time in immunosuppressed NHPs. In the NHPs, encapsulated allo-islets initially reduced hyperglycemia. decreased exogenous insulin requirements, elevated C-peptide levels, and lowered % HbA1c in plasma, but graft function diminished with time, regardless of transplant site. At necropsy. microcapsules were intact and non-fibrotic, but many islets exhibited volume loss, central necrosis and endogenous markers of hypoxia. Animals receiving supplemental oxy- gen and autologous MSCs showed improved graft function for a longer post-transplant period. In diabetic NHPs and mice, cell-free microcapsules did not elicit a fibrotic response.CONCLUSIONS: The evidence suggested that hypoxia was a major factor for damage to encapsulated islets in vivo. To achieve long-term function, new approaches must be developed to increase the oxygen supply to microencapsulated islets and/or identify donor insulin-secreting cells which can tolerate hypoxia.

KW - Diabetes

KW - Hypoxia

KW - Islet transplantation

KW - Microencapsulation

KW - Nonhuman primates

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U2 - 10.26355/eurrev_202008_22651

DO - 10.26355/eurrev_202008_22651

M3 - Article

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SN - 1128-3602

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EP - 8565

JO - European Review for Medical and Pharmacological Sciences

JF - European Review for Medical and Pharmacological Sciences

IS - 16

ER -

Microencapsulated islet allografts in diabetic NOD mice and nonhuman primates

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Keywords

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