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FAM13A affects body fat distribution and adipocyte function.
Citation | “Fam13A Affects Body Fat Distribution And Adipocyte Function.”. Nature Communications, p. 1465. . |
Center | Stanford University |
Author | Mohsen Fathzadeh, Jiehan Li, Abhiram Rao, Naomi Cook, Indumathi Chennamsetty, Marcus Seldin, Xiang Zhou, Panjamaporn Sangwung, Michael J Gloudemans, Mark Keller, Allan Attie, Jing Yang, Martin Wabitsch, Ivan Carcamo-Orive, Yuko Tada, Aldons J Lusis, Myung Kyun Shin, Cliona M Molony, Tracey McLaughlin, Gerald Reaven, Stephen B Montgomery, Dermot Reilly, Thomas Quertermous, Erik Ingelsson, Joshua W Knowles |
Abstract |
Genetic variation in the FAM13A (Family with Sequence Similarity 13 Member A) locus has been associated with several glycemic and metabolic traits in genome-wide association studies (GWAS). Here, we demonstrate that in humans, FAM13A alleles are associated with increased FAM13A expression in subcutaneous adipose tissue (SAT) and an insulin resistance-related phenotype (e.g. higher waist-to-hip ratio and fasting insulin levels, but lower body fat). In human adipocyte models, knockdown of FAM13A in preadipocytes accelerates adipocyte differentiation. In mice, Fam13a knockout (KO) have a lower visceral to subcutaneous fat (VAT/SAT) ratio after high-fat diet challenge, in comparison to their wild-type counterparts. Subcutaneous adipocytes in KO mice show a size distribution shift toward an increased number of smaller adipocytes, along with an improved adipogenic potential. Our results indicate that GWAS-associated variants within the FAM13A locus alter adipose FAM13A expression, which in turn, regulates adipocyte differentiation and contribute to changes in body fat distribution. |
Year of Publication |
2020
|
Journal |
Nature communications
|
Volume |
11
|
Issue |
1
|
Number of Pages |
1465
|
Date Published |
03/2020
|
ISSN Number |
2041-1723
|
DOI |
10.1038/s41467-020-15291-z
|
Alternate Journal |
Nat Commun
|
PMID |
32193374
|
PMCID |
PMC7081215
|
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