A sex-specific reconstitution bias in the competitive CD45.1/CD45.2 congenic bone marrow transplant model

Abstract Allelic variants of the pan-haematopoietic cell marker CD45, identified as CD45.1 and CD45.2, have been established as a marker system to track haematopoietic cells following congenic mouse bone marrow transplants. Despite the frequent use of this model for studying the impact of genetic mo...

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Main Authors: Salema Jafri, Stephen D. Moore, Nicholas W. Morrell, Mark L. Ormiston
Format: Article
Language:English
Published: Nature Publishing Group 2017-06-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-017-03784-9
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spelling doaj-1a9f8a796a894ab1b5b27e661ebbdf592020-12-08T01:09:32ZengNature Publishing GroupScientific Reports2045-23222017-06-01711810.1038/s41598-017-03784-9A sex-specific reconstitution bias in the competitive CD45.1/CD45.2 congenic bone marrow transplant modelSalema Jafri0Stephen D. Moore1Nicholas W. Morrell2Mark L. Ormiston3University of Cambridge, Department of MedicineUniversity of Cambridge, Department of MedicineUniversity of Cambridge, Department of MedicineQueen’s University, Department of Biomedical and Molecular SciencesAbstract Allelic variants of the pan-haematopoietic cell marker CD45, identified as CD45.1 and CD45.2, have been established as a marker system to track haematopoietic cells following congenic mouse bone marrow transplants. Despite the frequent use of this model for studying the impact of genetic modifications on relative differentiation potential, it is now evident that a bias exists in CD45.1 versus CD45.2 cell reconstitution. While this bias has been demonstrated by reduced reconstitution potential in B cells of CD45.1 origin, differences in the development of other lymphocytes, as well as the impact of sex on this bias, remain uncertain. We performed bone marrow transplants with wild-type CD45.1 and CD45.2 donor cells, and characterised haematopoietic cell reconstitution in dual-expressing CD45.1/2 host mice. We report an increase in CD45.2 reconstitution in the bone marrow that persists in the spleen, thymus and blood. Through the use of CD45.1/2 hosts, we demonstrate the intrinsic bias towards CD45.2 reconstitution is independent of an immunogenic response to the CD45.1 epitope. Furthermore, we identify a sex-specific difference in reconstitution efficiencies, with female mice exhibiting a greater bias towards CD45.2 reconstitution than males. This work sheds new light on the limitations of the CD45.1/CD45.2 congenic system for tracking lymphocyte development.https://doi.org/10.1038/s41598-017-03784-9
collection DOAJ
language English
format Article
sources DOAJ
author Salema Jafri
Stephen D. Moore
Nicholas W. Morrell
Mark L. Ormiston
spellingShingle Salema Jafri
Stephen D. Moore
Nicholas W. Morrell
Mark L. Ormiston
A sex-specific reconstitution bias in the competitive CD45.1/CD45.2 congenic bone marrow transplant model
Scientific Reports
author_facet Salema Jafri
Stephen D. Moore
Nicholas W. Morrell
Mark L. Ormiston
author_sort Salema Jafri
title A sex-specific reconstitution bias in the competitive CD45.1/CD45.2 congenic bone marrow transplant model
title_short A sex-specific reconstitution bias in the competitive CD45.1/CD45.2 congenic bone marrow transplant model
title_full A sex-specific reconstitution bias in the competitive CD45.1/CD45.2 congenic bone marrow transplant model
title_fullStr A sex-specific reconstitution bias in the competitive CD45.1/CD45.2 congenic bone marrow transplant model
title_full_unstemmed A sex-specific reconstitution bias in the competitive CD45.1/CD45.2 congenic bone marrow transplant model
title_sort sex-specific reconstitution bias in the competitive cd45.1/cd45.2 congenic bone marrow transplant model
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2017-06-01
description Abstract Allelic variants of the pan-haematopoietic cell marker CD45, identified as CD45.1 and CD45.2, have been established as a marker system to track haematopoietic cells following congenic mouse bone marrow transplants. Despite the frequent use of this model for studying the impact of genetic modifications on relative differentiation potential, it is now evident that a bias exists in CD45.1 versus CD45.2 cell reconstitution. While this bias has been demonstrated by reduced reconstitution potential in B cells of CD45.1 origin, differences in the development of other lymphocytes, as well as the impact of sex on this bias, remain uncertain. We performed bone marrow transplants with wild-type CD45.1 and CD45.2 donor cells, and characterised haematopoietic cell reconstitution in dual-expressing CD45.1/2 host mice. We report an increase in CD45.2 reconstitution in the bone marrow that persists in the spleen, thymus and blood. Through the use of CD45.1/2 hosts, we demonstrate the intrinsic bias towards CD45.2 reconstitution is independent of an immunogenic response to the CD45.1 epitope. Furthermore, we identify a sex-specific difference in reconstitution efficiencies, with female mice exhibiting a greater bias towards CD45.2 reconstitution than males. This work sheds new light on the limitations of the CD45.1/CD45.2 congenic system for tracking lymphocyte development.
url https://doi.org/10.1038/s41598-017-03784-9
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