Identifying G protein-coupled receptors involved in adipose tissue function using the innovative RNA-seq database FATTLAS

G protein-coupled receptors (GPCRs) modulate the function of adipose tissue (AT) in general and of adipocytes, specifically. Although it is well-established that GPCRs are widely expressed in AT, their repertoire as well as their regulation and function in (patho)physiological conditions (e.g., obes...

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Veröffentlicht in:iScience 2023-10, Vol.26 (10), p.107841-107841, Article 107841
Hauptverfasser: Kaczmarek, Isabell, Wower, Isabel, Ettig, Katja, Kuhn, Christina Katharina, Kraft, Robert, Landgraf, Kathrin, Körner, Antje, Schöneberg, Torsten, Horn, Susanne, Thor, Doreen
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Sprache:eng
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Zusammenfassung:G protein-coupled receptors (GPCRs) modulate the function of adipose tissue (AT) in general and of adipocytes, specifically. Although it is well-established that GPCRs are widely expressed in AT, their repertoire as well as their regulation and function in (patho)physiological conditions (e.g., obesity) is not fully resolved. Here, we established FATTLAS, an interactive public database, for improved access and analysis of RNA-seq data of mouse and human AT. After extracting the GPCRome of non-obese and obese individuals, highly expressed and differentially regulated GPCRs were identified. Exemplarily, we describe four receptors (GPR146, MRGPRF, FZD5, PTGER2) and analyzed their functions in a (pre)adipocyte cell model. Besides all receptors being involved in adipogenesis, MRGPRF is essential for adipocyte viability and regulates cAMP levels, while GPR146 modulates adipocyte lipolysis via constitutive activation of Gi proteins. Taken together, by implementing and using FATTLAS we describe four hitherto unrecognized GPCRs associated with AT function and adipogenesis. [Display omitted] •Implementing the innovative and freely accessible RNA-seq database FATTLAS•Describing the GPCRome of adipose tissue in non-obese and obese conditions•Identification of four GPCRs that have not been linked to adipocyte function•Functional characterization of the identified GPCRs (FZD5, MRGPRF, PTGER2, GPR146)
ISSN:2589-0042
2589-0042
DOI:10.1016/j.isci.2023.107841