نبذة مختصرة : Background: Age and obesity are dominant risk factors for several common cardiometabolic disorders, and both are known to impair adipose tissue function. However, the underlying cellular and genetic factors linking aging and obesity on adipose tissue function have remained elusive. Adipose stem and precursor cells (ASPCs) are an understudied, yet crucial adipose cell type due to their deterministic adipocyte differentiation potential, which impacts the capacity to store fat in a metabolically healthy manner. Methods: We integrated subcutaneous adipose tissue (SAT) bulk (n=435) and large single-nucleus RNA sequencing (n=105) data with the UK Biobank (UKB) (n=391,701) data to study age-obesity interactions originating from ASPCs by performing cell-type decomposition, differential expression testing, cell-cell communication analyses, and construction of polygenic risk scores for body mass index (BMI). Results: We found that the SAT ASPC proportions significantly decrease with age in an obesity-dependent way consistently in two independent cohorts, both showing that the age dependency of ASPC proportions is abolished by obesity. We further identified 76 genes (72 SAT ASPC marker genes and 4 transcription factors regulating ASPC marker genes) that are differentially expressed by age in SAT and functionally enriched for developmental processes and adipocyte differentiation (i.e., adipogenesis). The 76 age-perturbed ASPC genes include multiple negative regulators of adipogenesis, such as RORA, SMAD3, TWIST2, and ZNF521, form tight clusters of longitudinally co-expressed genes during human adipogenesis, and show age-based differences in cellular interactions between ASPCs and adipose cell types. Finally, our genetic data demonstrate that cis-regional variants of these genes interact with age as predictors of BMI in an obesity-dependent way in the large UKB, while no such gene-age interaction on BMI is observed with non-age-dependent ASPC marker genes, thus independently confirming our cellular ASPC results at the ...
Relation: This work was supported by NIH grants R01HG010505, R01DK132775, R01HL170604, and R01DK093757. The twin and CRYO studies were supported by Academy of Finland (Grant Nos 335443, 314383, 272376, and 266286), Sigrid Jusélius Foundation, Finnish Medical Foundation, Finnish Diabetes Research Foundation, Novo Nordisk Foundation (#NNF20OC0060547, NNF17OC0027232, NNF10OC1013354) and Government Research Funds to Helsinki University Hospital (K.H.P.), as well as Orion Research foundation (S.H), Maud Kuistila foundation (S.H.), Finnish Medical Foundation (S.H.), and University of Helsinki (S.H.).; Kar , A , Alvarez , M , Garske , K M , Huang , H , Lee , S H T , Deal , M , Das , S S , Koka , A , Jamal , Z , Mohlke , K L , Laakso , M , Heinonen , S , Pietiläinen , K H & Pajukanta , P 2024 , ' Age-dependent genes in adipose stem and precursor cells affect regulation of fat cell differentiation and link aging to obesity via cellular and genetic interactions ' , Genome Medicine , vol. 16 , no. 1 , 19 . https://doi.org/10.1186/s13073-024-01291-x; http://hdl.handle.net/10138/572918; e08ad8cf-0752-43ab-8201-455e64bfcce9; 85183921852; 001154325900002
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