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Human Pancreatic Islet Preparations Release HMGB1 : (Ir)Relevance for Graft Engraftment

Authors :
Nano, Rita
Racanicchi, Leda
Melzi, Raffaella
Mercalli, Alessia
Maffi, Paola
Sordi, Valeria
Ling, Zhidong
Scavini, Marina
Korsgren, Olle
Celona, Barbara
Secchi, Antonio
Piemonti, Lorenzo
Nano, Rita
Racanicchi, Leda
Melzi, Raffaella
Mercalli, Alessia
Maffi, Paola
Sordi, Valeria
Ling, Zhidong
Scavini, Marina
Korsgren, Olle
Celona, Barbara
Secchi, Antonio
Piemonti, Lorenzo
Publication Year :
2013

Abstract

High levels of donor-derived high-mobility group box 1 (HMGB1) protein have been associated with poor islet graft outcome in mouse models. The aim of our work was to determine whether HMGB1 released by human islets had independent proinflammatory effects that influence engraftment in humans. Human islet preparations contained and released HMGB1 in different amounts, as determined by Western blot and ELISA (median 17 pg/ml/IEQ/24 h; min-max 0-211, n=74). HMGB1 release directly correlated with brain death, donor hyper-amilasemia, and factors related to the pancreas digestion procedure (collagenase and digestion time). HMGB1 release was significantly positively associated with the release of other cytokines/chemokines, particularly with the highly released "proinflammatory" CXCL8/IL-8, CXCL1/GRO-alpha, and the IFN-gamma-inducible chemokines CXCL10/IP-10 and CXCL9/MIG. HMGB1 release was not modulated by Toll-like receptor 2,3,4,5, and 9 agonists or by exposure to IL-1 beta. When evaluated after islet transplantation, pretransplant HMGB1 release was weakly associated with the activation of the coagulation cascade (evaluated as serum cross-linked fibrin products), but not with the immediate posttransplant inflammatory response. Concordantly, HMGB1 did not affect short-term human islet function. Our data show that human islet HMGB1 release is a sign of "damaged" islets, although without any independent direct role in graft failure.

Details

Database :
OAIster
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1235057336
Document Type :
Electronic Resource
Full Text :
https://doi.org/10.3727.096368912X657783