4.8 Article

Distinct properties of adipose stem cell subpopulations determine fat depot-specific characteristics

期刊

CELL METABOLISM
卷 34, 期 3, 页码 458-472

出版社

CELL PRESS
DOI: 10.1016/j.cmet.2021.11.014

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资金

  1. Korean government (Ministry of Science and ICT) [2017M3A9B6073099, 2020R1A2C400163011, NRF-2018R1A5A1024340, NRF-2020R1A3B2078617]
  2. BK21 Plus program
  3. National Research Foundation
  4. National Research Foundation of Korea [2017M3A9B6073099] Funding Source: Korea Institute of Science & Technology Information (KISTI), National Science & Technology Information Service (NTIS)

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This study characterized adipose stem cells (ASCs) in two different types of white adipose tissues (EAT and IAT) and investigated the effects of intrinsic and tissue micro-environmental factors on ASC features. The results showed that ASC subpopulations in EAT and IAT exhibited different molecular features and adipogenic potential. Furthermore, ASCs in these two depots responded differently to obesogenic stimuli, influencing the characteristics of the adipose tissues.
In mammals, white adipose tissues are largely divided into visceral epididymal adipose tissue (EAT) and subcutaneous inguinal adipose tissue (IAT) with distinct metabolic properties. Although emerging evidence suggests that subpopulations of adipose stem cells (ASCs) would be important to explain fat depot differences, ASCs of two fat depots have not been comparatively investigated. Here, we characterized heterogeneous ASCs and examined the effects of intrinsic and tissue micro-environmental factors on distinct ASC features. We demonstrated that ASC subpopulations in EAT and IAT exhibited different molecular features with three adipogenic stages. ASC transplantation experiments revealed that intrinsic ASC features primarily determined their adipogenic potential. Upon obesogenic stimuli, EAT-specific SDC1(+) ASCs promoted fibrotic remodeling, whereas IAT-specific CXCL14(+) ASCs suppressed macrophage infiltration. Moreover, IAT-specific BST2(high) ASCs exhibited a high potential to become beige adipocytes. Collectively, our data broaden the understanding of ASCs with new insights into the origin of white fat depot differences.

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