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Publication | Open Access

DPPIV+ fibro-adipogenic progenitors form the niche of adult skeletal muscle self-renewing resident macrophages

22

Citations

46

References

2023

Year

Abstract

Adult tissue-resident macrophages (RMs) are either maintained by blood monocytes or through self-renewal. While the presence of a nurturing niche is likely crucial to support the survival and function of self-renewing RMs, evidence regarding its nature is limited. Here, we identify fibro-adipogenic progenitors (FAPs) as the main source of colony-stimulating factor 1 (CSF1) in resting skeletal muscle. Using parabiosis in combination with FAP-deficient transgenic mice (Pdgfrα<sup>CreERT2</sup> × DTA) or mice lacking FAP-derived CSF1 (Pdgfrα<sup>CreERT2</sup> × Csf1<sup>flox/null</sup>), we show that local CSF1 from FAPs is required for the survival of both TIM4<sup>-</sup> monocyte-derived and TIM4<sup>+</sup> self-renewing RMs in adult skeletal muscle. The spatial distribution and number of TIM4<sup>+</sup> RMs coincide with those of dipeptidyl peptidase IV (DPPIV)<sup>+</sup> FAPs, suggesting their role as CSF1-producing niche cells for self-renewing RMs. This finding identifies opportunities to precisely manipulate the function of self-renewing RMs in situ to further unravel their role in health and disease.

References

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