MME+ fibro-adipogenic progenitors are the dominant adipogenic population during fatty infiltration in human skeletal muscle

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Gillian Fitzgerald
Guillermo Turiel
Tatiane Gorski
Inés Soro-Arnaiz
Jing Zhang
Nicola C. Casartelli
Evi Masschelein
Nicola A. Maffiuletti
Reto Sutter
Michael Leunig
Jean Farup
Katrien De Bock
机构
[1] Laboratory of Exercise and Health,Human Performance Lab
[2] ETH Zurich,Department of Radiology
[3] Schulthess Clinic,Faculty of Medicine
[4] University Hospital Balgrist,Department of Orthopaedic Surgery
[5] University of Zurich,Department of Biomedicine
[6] Schulthess Clinic,Steno Diabetes Center Aarhus
[7] Aarhus University,undefined
[8] Aarhus University Hospital,undefined
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Fatty infiltration, the ectopic deposition of adipose tissue within skeletal muscle, is mediated via the adipogenic differentiation of fibro-adipogenic progenitors (FAPs). We used single-nuclei and single-cell RNA sequencing to characterize FAP heterogeneity in patients with fatty infiltration. We identified an MME+ FAP subpopulation which, based on ex vivo characterization as well as transplantation experiments, exhibits high adipogenic potential. MME+ FAPs are characterized by low activity of WNT, known to control adipogenic commitment, and are refractory to the inhibitory role of WNT activators. Using preclinical models for muscle damage versus fatty infiltration, we show that many MME+ FAPs undergo apoptosis during muscle regeneration and differentiate into adipocytes under pathological conditions, leading to a reduction in their abundance. Finally, we utilized the varying fat infiltration levels in human hip muscles and found less MME+ FAPs in fatty infiltrated human muscle. Altogether, we have identified the dominant adipogenic FAP subpopulation in skeletal muscle.
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