野生型骨髓细胞重新填充组织巨噬细胞，逆转纯合子CSF1R突变的影响。

IF 4 2区生物学 Q1 GENETICS & HEREDITY

PLoS Genetics Pub Date : 2025-01-27 eCollection Date: 2025-01-01 DOI:10.1371/journal.pgen.1011525

Dylan Carter-Cusack, Stephen Huang, Sahar Keshvari, Omkar Patkar, Anuj Sehgal, Rachel Allavena, Robert A J Byrne, B Paul Morgan, Stephen J Bush, Kim M Summers, Katharine M Irvine, David A Hume

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引用次数: 0

摘要

适应子宫外的生存是哺乳动物生命中的一个关键事件。集落刺激因子1受体（Csf1r）基因（Csf1rko）纯合突变大鼠巨噬细胞缺失严重影响断奶前体细胞生长和器官功能成熟。在断奶时移植野生型骨髓细胞（BMT）可以挽救组织巨噬细胞群，使其正常发育和长期存活。为了解剖巨噬细胞在出生后发育中的表型和功能，我们生成了野生型和Csf1rko大鼠断奶时所有主要器官的转录组学图谱，以及经BMT拯救后的部分器官。转录组学分析揭示了巨噬细胞缺乏对所有主要器官发育的微妙影响。网络分析揭示了csf1r依赖性常驻组织巨噬细胞的共同特征，包括补体C1Q （C1qa/b/c基因）的成分。在Csf1rko大鼠中几乎检测不到循环C1Q，并在BMT后迅速恢复到正常水平。组织特异性巨噬细胞的特征也被确定，特别是包括淋巴结窦巨噬细胞群。CD209B （SIGNR1）的免疫组织化学定位证实了它们在Csf1rko大鼠中的缺失。6-12周时，Csf1rko大鼠出现肺气肿样病理，伴有间质巨噬细胞的选择性丧失和粒细胞增多。这种病理被BMT逆转。随着生理救援，BMT精确地再生了巨噬细胞的丰度和表达谱。唯一的例外是大脑，其中bm衍生的小胶质样细胞与常驻小胶质细胞相比具有不同的表达谱。此外，转移的骨髓不能恢复血单核细胞或csf1r阳性的骨髓祖细胞。这些研究为人类CSF1R突变和先天免疫缺陷与早产相关的病理和治疗提供了一个模型。

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Wild-type bone marrow cells repopulate tissue resident macrophages and reverse the impacts of homozygous CSF1R mutation.

Adaptation to existence outside the womb is a key event in the life of a mammal. The absence of macrophages in rats with a homozygous mutation in the colony-stimulating factor 1 receptor (Csf1r) gene (Csf1rko) severely compromises pre-weaning somatic growth and maturation of organ function. Transfer of wild-type bone marrow cells (BMT) at weaning rescues tissue macrophage populations permitting normal development and long-term survival. To dissect the phenotype and function of macrophages in postnatal development, we generated transcriptomic profiles of all major organs of wild-type and Csf1rko rats at weaning and in selected organs following rescue by BMT. The transcriptomic profiles revealed subtle effects of macrophage deficiency on development of all major organs. Network analysis revealed a common signature of CSF1R-dependent resident tissue macrophages that includes the components of complement C1Q (C1qa/b/c genes). Circulating C1Q was almost undetectable in Csf1rko rats and rapidly restored to normal levels following BMT. Tissue-specific macrophage signatures were also identified, notably including sinus macrophage populations in the lymph nodes. Their loss in Csf1rko rats was confirmed by immunohistochemical localisation of CD209B (SIGNR1). By 6-12 weeks, Csf1rko rats succumb to emphysema-like pathology associated with the selective loss of interstitial macrophages and granulocytosis. This pathology was reversed by BMT. Along with physiological rescue, BMT precisely regenerated the abundance and expression profiles of resident macrophages. The exception was the brain, where BM-derived microglia-like cells had a distinct expression profile compared to resident microglia. In addition, the transferred BM failed to restore blood monocyte or CSF1R-positive bone marrow progenitors. These studies provide a model for the pathology and treatment of CSF1R mutations in humans and the innate immune deficiency associated with prematurity.

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PLoS Genetics GENETICS & HEREDITY-

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期刊介绍： PLOS Genetics is run by an international Editorial Board, headed by the Editors-in-Chief, Greg Barsh (HudsonAlpha Institute of Biotechnology, and Stanford University School of Medicine) and Greg Copenhaver (The University of North Carolina at Chapel Hill). Articles published in PLOS Genetics are archived in PubMed Central and cited in PubMed.