CSF1R-dependent macrophages control postnatal somatic growth and organ maturation

Homozygous mutation of the Csf1r locus (Csf1rko) in mice, rats and humans leads to multiple postnatal developmental abnormalities. To enable analysis of the mechanisms underlying the phenotypic impacts of Csf1r mutation, we bred a rat Csf1rko allele to the inbred dark agouti (DA) genetic background...

Descripción completa

Detalles Bibliográficos
Autores principales: Keshvari, Sahar, Caruso, Melanie, Teakle, Ngari, Batoon, Lena, Sehgal, Anuj, Patkar, Omkar L., Ferrari-Cestari, Michelle, Snell, Cameron E., Chen, Chen, Stevenson, Alex, Davis, Felicity M., Bush, Stephen J., Pridans, Clare, Summers, Kim M., Pettit, Allison R., Irvine, Katharine M., Hume, David A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8205168/
https://www.ncbi.nlm.nih.gov/pubmed/34081701
http://dx.doi.org/10.1371/journal.pgen.1009605
_version_ 1783708456543322112
author Keshvari, Sahar
Caruso, Melanie
Teakle, Ngari
Batoon, Lena
Sehgal, Anuj
Patkar, Omkar L.
Ferrari-Cestari, Michelle
Snell, Cameron E.
Chen, Chen
Stevenson, Alex
Davis, Felicity M.
Bush, Stephen J.
Pridans, Clare
Summers, Kim M.
Pettit, Allison R.
Irvine, Katharine M.
Hume, David A.
author_facet Keshvari, Sahar
Caruso, Melanie
Teakle, Ngari
Batoon, Lena
Sehgal, Anuj
Patkar, Omkar L.
Ferrari-Cestari, Michelle
Snell, Cameron E.
Chen, Chen
Stevenson, Alex
Davis, Felicity M.
Bush, Stephen J.
Pridans, Clare
Summers, Kim M.
Pettit, Allison R.
Irvine, Katharine M.
Hume, David A.
author_sort Keshvari, Sahar
collection PubMed
description Homozygous mutation of the Csf1r locus (Csf1rko) in mice, rats and humans leads to multiple postnatal developmental abnormalities. To enable analysis of the mechanisms underlying the phenotypic impacts of Csf1r mutation, we bred a rat Csf1rko allele to the inbred dark agouti (DA) genetic background and to a Csf1r-mApple reporter transgene. The Csf1rko led to almost complete loss of embryonic macrophages and ablation of most adult tissue macrophage populations. We extended previous analysis of the Csf1rko phenotype to early postnatal development to reveal impacts on musculoskeletal development and proliferation and morphogenesis in multiple organs. Expression profiling of 3-week old wild-type (WT) and Csf1rko livers identified 2760 differentially expressed genes associated with the loss of macrophages, severe hypoplasia, delayed hepatocyte maturation, disrupted lipid metabolism and the IGF1/IGF binding protein system. Older Csf1rko rats developed severe hepatic steatosis. Consistent with the developmental delay in the liver Csf1rko rats had greatly-reduced circulating IGF1. Transfer of WT bone marrow (BM) cells at weaning without conditioning repopulated resident macrophages in all organs, including microglia in the brain, and reversed the mutant phenotypes enabling long term survival and fertility. WT BM transfer restored osteoclasts, eliminated osteopetrosis, restored bone marrow cellularity and architecture and reversed granulocytosis and B cell deficiency. Csf1rko rats had an elevated circulating CSF1 concentration which was rapidly reduced to WT levels following BM transfer. However, CD43(hi) non-classical monocytes, absent in the Csf1rko, were not rescued and bone marrow progenitors remained unresponsive to CSF1. The results demonstrate that the Csf1rko phenotype is autonomous to BM-derived cells and indicate that BM contains a progenitor of tissue macrophages distinct from hematopoietic stem cells. The model provides a unique system in which to define the pathways of development of resident tissue macrophages and their local and systemic roles in growth and organ maturation.
format Online
Article
Text
id pubmed-8205168
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-82051682021-06-29 CSF1R-dependent macrophages control postnatal somatic growth and organ maturation Keshvari, Sahar Caruso, Melanie Teakle, Ngari Batoon, Lena Sehgal, Anuj Patkar, Omkar L. Ferrari-Cestari, Michelle Snell, Cameron E. Chen, Chen Stevenson, Alex Davis, Felicity M. Bush, Stephen J. Pridans, Clare Summers, Kim M. Pettit, Allison R. Irvine, Katharine M. Hume, David A. PLoS Genet Research Article Homozygous mutation of the Csf1r locus (Csf1rko) in mice, rats and humans leads to multiple postnatal developmental abnormalities. To enable analysis of the mechanisms underlying the phenotypic impacts of Csf1r mutation, we bred a rat Csf1rko allele to the inbred dark agouti (DA) genetic background and to a Csf1r-mApple reporter transgene. The Csf1rko led to almost complete loss of embryonic macrophages and ablation of most adult tissue macrophage populations. We extended previous analysis of the Csf1rko phenotype to early postnatal development to reveal impacts on musculoskeletal development and proliferation and morphogenesis in multiple organs. Expression profiling of 3-week old wild-type (WT) and Csf1rko livers identified 2760 differentially expressed genes associated with the loss of macrophages, severe hypoplasia, delayed hepatocyte maturation, disrupted lipid metabolism and the IGF1/IGF binding protein system. Older Csf1rko rats developed severe hepatic steatosis. Consistent with the developmental delay in the liver Csf1rko rats had greatly-reduced circulating IGF1. Transfer of WT bone marrow (BM) cells at weaning without conditioning repopulated resident macrophages in all organs, including microglia in the brain, and reversed the mutant phenotypes enabling long term survival and fertility. WT BM transfer restored osteoclasts, eliminated osteopetrosis, restored bone marrow cellularity and architecture and reversed granulocytosis and B cell deficiency. Csf1rko rats had an elevated circulating CSF1 concentration which was rapidly reduced to WT levels following BM transfer. However, CD43(hi) non-classical monocytes, absent in the Csf1rko, were not rescued and bone marrow progenitors remained unresponsive to CSF1. The results demonstrate that the Csf1rko phenotype is autonomous to BM-derived cells and indicate that BM contains a progenitor of tissue macrophages distinct from hematopoietic stem cells. The model provides a unique system in which to define the pathways of development of resident tissue macrophages and their local and systemic roles in growth and organ maturation. Public Library of Science 2021-06-03 /pmc/articles/PMC8205168/ /pubmed/34081701 http://dx.doi.org/10.1371/journal.pgen.1009605 Text en © 2021 Keshvari et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Keshvari, Sahar
Caruso, Melanie
Teakle, Ngari
Batoon, Lena
Sehgal, Anuj
Patkar, Omkar L.
Ferrari-Cestari, Michelle
Snell, Cameron E.
Chen, Chen
Stevenson, Alex
Davis, Felicity M.
Bush, Stephen J.
Pridans, Clare
Summers, Kim M.
Pettit, Allison R.
Irvine, Katharine M.
Hume, David A.
CSF1R-dependent macrophages control postnatal somatic growth and organ maturation
title CSF1R-dependent macrophages control postnatal somatic growth and organ maturation
title_full CSF1R-dependent macrophages control postnatal somatic growth and organ maturation
title_fullStr CSF1R-dependent macrophages control postnatal somatic growth and organ maturation
title_full_unstemmed CSF1R-dependent macrophages control postnatal somatic growth and organ maturation
title_short CSF1R-dependent macrophages control postnatal somatic growth and organ maturation
title_sort csf1r-dependent macrophages control postnatal somatic growth and organ maturation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8205168/
https://www.ncbi.nlm.nih.gov/pubmed/34081701
http://dx.doi.org/10.1371/journal.pgen.1009605
work_keys_str_mv AT keshvarisahar csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT carusomelanie csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT teaklengari csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT batoonlena csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT sehgalanuj csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT patkaromkarl csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT ferraricestarimichelle csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT snellcamerone csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT chenchen csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT stevensonalex csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT davisfelicitym csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT bushstephenj csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT pridansclare csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT summerskimm csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT pettitallisonr csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT irvinekatharinem csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation
AT humedavida csf1rdependentmacrophagescontrolpostnatalsomaticgrowthandorganmaturation

Ejemplares similares