Pancreatic Islet Basement Membrane Loss and Remodeling After Mouse Islet Isolation and Transplantation: Impact for Allograft Rejection

dc.contributor.authorIrving-Rodgers, H. F
dc.contributor.authorChoong, F. J
dc.contributor.authorHummitzsch, K
dc.contributor.authorParish, Christopher
dc.contributor.authorRodgers, R. J.
dc.contributor.authorSimeonovic, Charmaine
dc.date.accessioned2016-04-11T04:37:50Z
dc.date.available2016-04-11T04:37:50Z
dc.date.issued2014
dc.date.updated2016-06-14T08:36:36Z
dc.description.abstractThe isolation of islets by collagenase digestion can cause damage and impact the efficiency of islet engraftment and function. In this study, we assessed the basement membranes (BMs) of mouse pancreatic islets as a molecular biomarker for islet integrity, damage after isolation, and islet repair in vitro as well as in the absence or presence of an immune response after transplantation. Immunofluorescence staining of BM matrix proteins and the endothelial cell marker platelet endothelial cell adhesion molecule-1 (PECAM-1) was performed on pancreatic islets in situ, isolated islets, islets cultured for 4 days, and islet grafts at 3-10 days posttransplantation. Flow cytometry was used to investigate the expression of BM matrix proteins in isolated islet β-cells. The islet BM, consisting of collagen type IV and components of Engelbreth-Holm-Swarm (EHS) tumor laminin 111, laminin α2, nidogen-2, and perlecan in pancreatic islets in situ, was completely lost during islet isolation. It was not reestablished during culture for 4 days. Peri- and intraislet BM restoration was identified after islet isotransplantation and coincided with the migration pattern of PECAM-1(+) vascular endothelial cells (VECs). After islet allotransplantation, the restoration of VEC-derived peri-islet BMs was initiated but did not lead to the formation of the intraislet vasculature. Instead, an abnormally enlarged peri-islet vasculature developed, coinciding with islet allograft rejection. The islet BM is a sensitive biomarker of islet damage resulting from enzymatic isolation and of islet repair after transplantation. After transplantation, remodeling of both peri- and intraislet BMs restores β-cell-matrix attachment, a recognized requirement for β-cell survival, for isografts but not for allografts. Preventing isolation-induced islet BM damage would be expected to preserve the intrinsic barrier function of islet BMs, thereby influencing both the effector mechanisms required for allograft rejection and the antirejection strategies needed for allograft survival.
dc.description.sponsorshipThis work was supported by a National Health and Medical Research Council of Australia (NH&MRC)/JDRF Special Program Grant in Type 1 Diabetes (#418138), the Diabetes Australia Research Trust Apex Award 2010, a NHMRC Program Grant (#455395), and a research grant from the Roche Organ Transplantation Research Foundation (ROTRF)/JDRF (#477554991). The authors declare no conflict of interest.en_AU
dc.identifier.issn0963-6897en_AU
dc.identifier.urihttp://hdl.handle.net/1885/100998
dc.publisherCognizant Communication Corporation
dc.relationhttp://purl.org/au-research/grants/nhmrc/418138
dc.relationhttp://purl.org/au-research/grants/nhmrc/455395
dc.rightsCopyright © 2014 Cognizant Comm. Corp. http://www.sherpa.ac.uk/romeo/issn/0963-6897/..."Publisher's version/PDF must be used. On a non-profit server" from SHERPA/RoMEO site (as at 11/04/16).
dc.sourceCell Transplantation
dc.subjectallografts
dc.subjectanimals
dc.subjectbasement membrane
dc.subjectcarcinoma, embryonal
dc.subjectcell line, tumor
dc.subjectdisease models, animal
dc.subjectendothelial cells
dc.subjectgraft rejection
dc.subjectislets of langerhans
dc.subjectislets of langerhans transplantation
dc.subjectmale
dc.subjectmice
dc.subjectmice, inbred c57bl
dc.subjectmice, inbred cba
dc.subjecttransplantation tolerance
dc.titlePancreatic Islet Basement Membrane Loss and Remodeling After Mouse Islet Isolation and Transplantation: Impact for Allograft Rejection
dc.typeJournal article
dcterms.accessRightsOpen Accessen_AU
local.bibliographicCitation.issue1en_AU
local.bibliographicCitation.lastpage72en_AU
local.bibliographicCitation.startpage59en_AU
local.contributor.affiliationIrving-Rodgers, H.F., Queensland University of Technology, Australiaen_AU
local.contributor.affiliationChoong, Fui Jiun, College of Medicine, Biology and Environment, CMBE John Curtin School of Medical Research, Immunology and Infectious Disease, The Australian National Universityen_AU
local.contributor.affiliationHummitzsch, K., The University of Adelaide, Australiaen_AU
local.contributor.affiliationParish, Christopher, College of Medicine, Biology and Environment, CMBE John Curtin School of Medical Research, Immunology and Infectious Disease, The Australian National Universityen_AU
local.contributor.affiliationRodgers, Ray, University of Adelaide, Australiaen_AU
local.contributor.affiliationSimeonovic, Charmaine, College of Medicine, Biology and Environment, CMBE John Curtin School of Medical Research, Immunology and Infectious Disease, The Australian National Universityen_AU
local.contributor.authoremailchristopher.parish@anu.edu.auen_AU
local.contributor.authoruidu4532610en_AU
local.description.notesImported from ARIESen_AU
local.identifier.absfor110704en_AU
local.identifier.ariespublicationf5625xPUB6275en_AU
local.identifier.citationvolume23en_AU
local.identifier.doi10.3727/096368912X659880en_AU
local.identifier.essn1555-3892en_AU
local.identifier.scopusID2-s2.0-84892563727
local.identifier.thomsonID000330604300006
local.identifier.uidSubmittedByu3488905en_AU
local.publisher.urlhttps://www.cognizantcommunication.com/en_AU
local.type.statusPublished Versionen_AU

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