Interference with tissue factor prolongs intrahepatic islet allograft survival in a nonhuman primate marginal mass model

Dora M. Berman; Over Cabrera; Norman M. Kenyon; Joshua Miller; Susan H. Tam; Vrinda S. Khandekar; Kristen M. Picha; Avery R. Soderman; Robert E. Jordan; Peter J. Bugelski; Denison Horninger; Michael Lark; Janet E. Davis; Rodolfo Alejandro; Per Olof Berggren; Mark Zimmerman; John J. O'Neil; Camillo Ricordi; Norma S. Kenyon

doi:10.1097/01.tp.0000275401.80187.1e

Interference with tissue factor prolongs intrahepatic islet allograft survival in a nonhuman primate marginal mass model

Dora M. Berman^*, Over Cabrera, Norman M. Kenyon, Joshua Miller, Susan H. Tam, Vrinda S. Khandekar, Kristen M. Picha, Avery R. Soderman, Robert E. Jordan, Peter J. Bugelski, Denison Horninger, Michael Lark, Janet E. Davis, Rodolfo Alejandro, Per Olof Berggren, Mark Zimmerman, John J. O'Neil, Camillo Ricordi, Norma S. Kenyon

^*Corresponding author for this work

Surgery, Transplant Surgery Division

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

58 Scopus citations

Abstract

BACKGROUND. Tissue factor (TF) expression on islets can result in an instant blood-mediated inflammatory reaction (IBMIR) that contributes to early islet loss. We tested whether peritransplant protection of islets from IBMIR with a monoclonal anti-TF antibody (CNTO859) would enhance engraftment in our nonhuman primate marginal mass model. METHODS. Each of six pairs of cynomolgus monkeys (CM) with streptozotocin-induced diabetes was closely matched for metabolic control and was transplanted with 5,000 IEQ/kg allogeneic, ABO-compatible islets from the same donor under the cover of steroid-free immunosuppression. For each pair, experimental animals received islets cultured with 20 μg/mL anti-TF and were dosed with 6 mg/kg anti-TF intravenously, 10-25 min before islet infusion; control monkeys received an equal number of islets from the same preparation cultured without anti-TF and no in vivo treatment. RESULTS. Early fasting C-peptide (CP) values were different between (P<0.01), but not within, pairs and correlated with in vitro functional capacity of islets as assessed by perifusion (r=0.60; P=0.022). Compared to their matched controls, experimental animals had decreased posttransplant markers of coagulation, higher fasting CP levels (1 month posttransplant and end of study) and prolonged graft function. CONCLUSIONS. These data suggest that pretreatment of islets and the recipient with anti-TF may limit the effects of IBMIR, thereby enhancing islet engraftment and survival.

Original language	English (US)
Pages (from-to)	308-315
Number of pages	8
Journal	Transplantation
Volume	84
Issue number	3
DOIs	https://doi.org/10.1097/01.tp.0000275401.80187.1e
State	Published - Aug 2007

Keywords

Coagulation
Graft survival
Islet engraftment
Islet transplantation

ASJC Scopus subject areas

Transplantation

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Berman, D. M., Cabrera, O., Kenyon, N. M., Miller, J., Tam, S. H., Khandekar, V. S., Picha, K. M., Soderman, A. R., Jordan, R. E., Bugelski, P. J., Horninger, D., Lark, M., Davis, J. E., Alejandro, R., Berggren, P. O., Zimmerman, M., O'Neil, J. J., Ricordi, C., & Kenyon, N. S. (2007). Interference with tissue factor prolongs intrahepatic islet allograft survival in a nonhuman primate marginal mass model. Transplantation, 84(3), 308-315. https://doi.org/10.1097/01.tp.0000275401.80187.1e

Berman, Dora M. ; Cabrera, Over ; Kenyon, Norman M. ; Miller, Joshua ; Tam, Susan H. ; Khandekar, Vrinda S. ; Picha, Kristen M. ; Soderman, Avery R. ; Jordan, Robert E. ; Bugelski, Peter J. ; Horninger, Denison ; Lark, Michael ; Davis, Janet E. ; Alejandro, Rodolfo ; Berggren, Per Olof ; Zimmerman, Mark ; O'Neil, John J. ; Ricordi, Camillo ; Kenyon, Norma S. / Interference with tissue factor prolongs intrahepatic islet allograft survival in a nonhuman primate marginal mass model. In: Transplantation. 2007 ; Vol. 84, No. 3. pp. 308-315.

@article{5317402390724def9346d7abda0aca27,

title = "Interference with tissue factor prolongs intrahepatic islet allograft survival in a nonhuman primate marginal mass model",

abstract = "BACKGROUND. Tissue factor (TF) expression on islets can result in an instant blood-mediated inflammatory reaction (IBMIR) that contributes to early islet loss. We tested whether peritransplant protection of islets from IBMIR with a monoclonal anti-TF antibody (CNTO859) would enhance engraftment in our nonhuman primate marginal mass model. METHODS. Each of six pairs of cynomolgus monkeys (CM) with streptozotocin-induced diabetes was closely matched for metabolic control and was transplanted with 5,000 IEQ/kg allogeneic, ABO-compatible islets from the same donor under the cover of steroid-free immunosuppression. For each pair, experimental animals received islets cultured with 20 μg/mL anti-TF and were dosed with 6 mg/kg anti-TF intravenously, 10-25 min before islet infusion; control monkeys received an equal number of islets from the same preparation cultured without anti-TF and no in vivo treatment. RESULTS. Early fasting C-peptide (CP) values were different between (P<0.01), but not within, pairs and correlated with in vitro functional capacity of islets as assessed by perifusion (r=0.60; P=0.022). Compared to their matched controls, experimental animals had decreased posttransplant markers of coagulation, higher fasting CP levels (1 month posttransplant and end of study) and prolonged graft function. CONCLUSIONS. These data suggest that pretreatment of islets and the recipient with anti-TF may limit the effects of IBMIR, thereby enhancing islet engraftment and survival.",

keywords = "Coagulation, Graft survival, Islet engraftment, Islet transplantation",

author = "Berman, {Dora M.} and Over Cabrera and Kenyon, {Norman M.} and Joshua Miller and Tam, {Susan H.} and Khandekar, {Vrinda S.} and Picha, {Kristen M.} and Soderman, {Avery R.} and Jordan, {Robert E.} and Bugelski, {Peter J.} and Denison Horninger and Michael Lark and Davis, {Janet E.} and Rodolfo Alejandro and Berggren, {Per Olof} and Mark Zimmerman and O'Neil, {John J.} and Camillo Ricordi and Kenyon, {Norma S.}",

year = "2007",

month = aug,

doi = "10.1097/01.tp.0000275401.80187.1e",

language = "English (US)",

volume = "84",

pages = "308--315",

journal = "Transplantation",

issn = "0041-1337",

publisher = "Lippincott Williams and Wilkins",

number = "3",

}

Berman, DM, Cabrera, O, Kenyon, NM, Miller, J, Tam, SH, Khandekar, VS, Picha, KM, Soderman, AR, Jordan, RE, Bugelski, PJ, Horninger, D, Lark, M, Davis, JE, Alejandro, R, Berggren, PO, Zimmerman, M, O'Neil, JJ, Ricordi, C & Kenyon, NS 2007, 'Interference with tissue factor prolongs intrahepatic islet allograft survival in a nonhuman primate marginal mass model', Transplantation, vol. 84, no. 3, pp. 308-315. https://doi.org/10.1097/01.tp.0000275401.80187.1e

Interference with tissue factor prolongs intrahepatic islet allograft survival in a nonhuman primate marginal mass model. / Berman, Dora M.; Cabrera, Over; Kenyon, Norman M.; Miller, Joshua; Tam, Susan H.; Khandekar, Vrinda S.; Picha, Kristen M.; Soderman, Avery R.; Jordan, Robert E.; Bugelski, Peter J.; Horninger, Denison; Lark, Michael; Davis, Janet E.; Alejandro, Rodolfo; Berggren, Per Olof; Zimmerman, Mark; O'Neil, John J.; Ricordi, Camillo; Kenyon, Norma S.

In: Transplantation, Vol. 84, No. 3, 08.2007, p. 308-315.

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

TY - JOUR

T1 - Interference with tissue factor prolongs intrahepatic islet allograft survival in a nonhuman primate marginal mass model

AU - Berman, Dora M.

AU - Cabrera, Over

AU - Kenyon, Norman M.

AU - Miller, Joshua

AU - Tam, Susan H.

AU - Khandekar, Vrinda S.

AU - Picha, Kristen M.

AU - Soderman, Avery R.

AU - Jordan, Robert E.

AU - Bugelski, Peter J.

AU - Horninger, Denison

AU - Lark, Michael

AU - Davis, Janet E.

AU - Alejandro, Rodolfo

AU - Berggren, Per Olof

AU - Zimmerman, Mark

AU - O'Neil, John J.

AU - Ricordi, Camillo

AU - Kenyon, Norma S.

PY - 2007/8

Y1 - 2007/8

N2 - BACKGROUND. Tissue factor (TF) expression on islets can result in an instant blood-mediated inflammatory reaction (IBMIR) that contributes to early islet loss. We tested whether peritransplant protection of islets from IBMIR with a monoclonal anti-TF antibody (CNTO859) would enhance engraftment in our nonhuman primate marginal mass model. METHODS. Each of six pairs of cynomolgus monkeys (CM) with streptozotocin-induced diabetes was closely matched for metabolic control and was transplanted with 5,000 IEQ/kg allogeneic, ABO-compatible islets from the same donor under the cover of steroid-free immunosuppression. For each pair, experimental animals received islets cultured with 20 μg/mL anti-TF and were dosed with 6 mg/kg anti-TF intravenously, 10-25 min before islet infusion; control monkeys received an equal number of islets from the same preparation cultured without anti-TF and no in vivo treatment. RESULTS. Early fasting C-peptide (CP) values were different between (P<0.01), but not within, pairs and correlated with in vitro functional capacity of islets as assessed by perifusion (r=0.60; P=0.022). Compared to their matched controls, experimental animals had decreased posttransplant markers of coagulation, higher fasting CP levels (1 month posttransplant and end of study) and prolonged graft function. CONCLUSIONS. These data suggest that pretreatment of islets and the recipient with anti-TF may limit the effects of IBMIR, thereby enhancing islet engraftment and survival.

AB - BACKGROUND. Tissue factor (TF) expression on islets can result in an instant blood-mediated inflammatory reaction (IBMIR) that contributes to early islet loss. We tested whether peritransplant protection of islets from IBMIR with a monoclonal anti-TF antibody (CNTO859) would enhance engraftment in our nonhuman primate marginal mass model. METHODS. Each of six pairs of cynomolgus monkeys (CM) with streptozotocin-induced diabetes was closely matched for metabolic control and was transplanted with 5,000 IEQ/kg allogeneic, ABO-compatible islets from the same donor under the cover of steroid-free immunosuppression. For each pair, experimental animals received islets cultured with 20 μg/mL anti-TF and were dosed with 6 mg/kg anti-TF intravenously, 10-25 min before islet infusion; control monkeys received an equal number of islets from the same preparation cultured without anti-TF and no in vivo treatment. RESULTS. Early fasting C-peptide (CP) values were different between (P<0.01), but not within, pairs and correlated with in vitro functional capacity of islets as assessed by perifusion (r=0.60; P=0.022). Compared to their matched controls, experimental animals had decreased posttransplant markers of coagulation, higher fasting CP levels (1 month posttransplant and end of study) and prolonged graft function. CONCLUSIONS. These data suggest that pretreatment of islets and the recipient with anti-TF may limit the effects of IBMIR, thereby enhancing islet engraftment and survival.

KW - Coagulation

KW - Graft survival

KW - Islet engraftment

KW - Islet transplantation

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U2 - 10.1097/01.tp.0000275401.80187.1e

DO - 10.1097/01.tp.0000275401.80187.1e

M3 - Article

C2 - 17700154

AN - SCOPUS:34547860883

VL - 84

SP - 308

EP - 315

JO - Transplantation

JF - Transplantation

SN - 0041-1337

IS - 3

ER -

Interference with tissue factor prolongs intrahepatic islet allograft survival in a nonhuman primate marginal mass model

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Keywords

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