Identification of a Major Susceptibility Locus for Lethal Graft-versus-host Disease in MHC-matched Mice

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 2009 Jun 16

PMID 19525392

Citations 2

Authors

Thai M Cao

Laura C Lazzeroni

Schickwann Tsai

Wendy W Pang

Amy Kao

Nicola J Camp

Alun Thomas

Judith A Shizuru

Affiliations

Soon will be listed here.

Abstract

Graft-vs-host disease (GVHD) is the major cause of morbidity and mortality after allogeneic hemopoietic cell transplantation. From a genetic perspective, GVHD is a complex phenotypic trait. Although it is understood that susceptibility results from interacting polymorphisms of genes encoding histocompatibility Ags and immune regulatory molecules, a detailed and integrative understanding of the genetic background underlying GVHD remains lacking. To gain insight regarding these issues, we performed a forward genetic study. A MHC-matched mouse model was used in which irradiated recipient BALB.K and B10.BR mice demonstrate differential susceptibility to lethal GHVD when transplanted using AKR/J donors. Assessment of GVHD in (B10.BR x BALB.K)F(1) mice revealed that susceptibility is a dominant trait and conferred by deleterious alleles from the BALB.K strain. To identify the alleles responsible for GVHD susceptibility, a genome-scanning approach was taken using (B10.BR x BALB.K)F(1) x B10.BR backcross mice as recipients. A major susceptibility locus, termed the Gvh1 locus, was identified on chromosome 16 using linkage analysis (logarithm of the odds, 9.1). A second locus was found on chromosome 13, named Gvh2, which had additive but protective effects. Further identification of Gvh genes by positional cloning may yield new insight into genetic control mechanisms regulating GVHD and potentially reveal novel approaches for effective GVHD therapy.

Citing Articles

Fine mapping of the Bmgr5 quantitative trait locus for allogeneic bone marrow engraftment in mice.

Wang Y, Chen X, Tsai S, Thomas A, Shizuru J, Cao T Immunogenetics. 2013; 65(8):585-96.

PMID: 23666360 PMC: 3713196. DOI: 10.1007/s00251-013-0709-6.

Alloimmune response results in expansion of autoreactive donor CD4+ T cells in transplants that can mediate chronic graft-versus-host disease.

Zhao D, Young J, Chen Y, Shen E, Yi T, Todorov I J Immunol. 2010; 186(2):856-68.

PMID: 21149609 PMC: 3891909. DOI: 10.4049/jimmunol.1002195.

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