Circulating miRNA-150-5p is associated with immune-mediated early β-cell loss in a humanized mouse model.
Details
Serval ID
serval:BIB_8C7F068F778E
Type
Article: article from journal or magazin.
Collection
Publications
Institution
Title
Circulating miRNA-150-5p is associated with immune-mediated early β-cell loss in a humanized mouse model.
Journal
Xenotransplantation
ISSN
1399-3089 (Electronic)
ISSN-L
0908-665X
Publication state
Published
Issued date
03/2019
Peer-reviewed
Oui
Volume
26
Number
2
Pages
e12474
Language
english
Notes
Publication types: Journal Article ; Research Support, Non-U.S. Gov't
Publication Status: ppublish
Publication Status: ppublish
Abstract
Aberrant microRNA (miRNA) expression levels are associated with various graft rejections. We used our humanized mouse model with transplanted human islets to identify miRNAs in islet grafts related to xenograft rejection and circulating miRNAs associated with xenograft rejection-mediated β-cell loss.
Diabetic immunodeficient NOD.scid mice were transplanted with human islets and subsequently achieved stable normoglycemia. Lymphocytes from NOD mice were then adoptively transferred to the humanized mice to induce human β-cell destruction. Islet graft and plasma were collected immediately once blood glucose reached >200 mg/dL. miRNAs in the islet grafts and in the plasma with or without adoptive lymphocyte transfer (ALT) were measured using NanoString nCounter® miRNA Expression Assay and qPCR.
A set of immune-related miRNAs was significantly increased in human islet grafts of ALT-treated mice compared to control mice. Of these miRNAs, miR-150-5p was significantly increased in the circulation of ALT-treated mice at tissue collection and the increase was a result of immune activation rather than simply the presence of lymphocytes in circulation. Furthermore, miR-150-5p was significantly increased in human islet graft and circulation prior to the development of hyperglycemia in the ALT-treated mice.
Our data demonstrated that immune-related miRNAs are associated with human islet xenograft rejection in mice. miR-150-5p is increased in human islet graft and in the circulation during islet xenograft rejection and β-cell destruction prior to hyperglycemia and may be an early biomarker for islet xenograft rejection.
Diabetic immunodeficient NOD.scid mice were transplanted with human islets and subsequently achieved stable normoglycemia. Lymphocytes from NOD mice were then adoptively transferred to the humanized mice to induce human β-cell destruction. Islet graft and plasma were collected immediately once blood glucose reached >200 mg/dL. miRNAs in the islet grafts and in the plasma with or without adoptive lymphocyte transfer (ALT) were measured using NanoString nCounter® miRNA Expression Assay and qPCR.
A set of immune-related miRNAs was significantly increased in human islet grafts of ALT-treated mice compared to control mice. Of these miRNAs, miR-150-5p was significantly increased in the circulation of ALT-treated mice at tissue collection and the increase was a result of immune activation rather than simply the presence of lymphocytes in circulation. Furthermore, miR-150-5p was significantly increased in human islet graft and circulation prior to the development of hyperglycemia in the ALT-treated mice.
Our data demonstrated that immune-related miRNAs are associated with human islet xenograft rejection in mice. miR-150-5p is increased in human islet graft and in the circulation during islet xenograft rejection and β-cell destruction prior to hyperglycemia and may be an early biomarker for islet xenograft rejection.
Keywords
Animals, Disease Models, Animal, Graft Rejection/genetics, Graft Rejection/immunology, Graft Survival/genetics, Graft Survival/immunology, Heterografts/immunology, Humans, Insulin-Secreting Cells/metabolism, Islets of Langerhans Transplantation/immunology, Lymphocytes/immunology, Mice, Mice, Inbred NOD, MicroRNAs/genetics, MicroRNAs/immunology, Transplantation, Heterologous/methods, diabetes, islet, islet transplantation, miRNA, xenograft rejection
Pubmed
Web of science
Create date
26/11/2018 13:14
Last modification date
04/01/2020 6:17