Impaired mRNA splicing and proteostasis in preadipocytes in obesity-related metabolic disease

Preadipocytes are crucial for healthy adipose tissue expansion. Preadipocyte differentiation is altered in obese individuals, which has been proposed to contribute to obesity-associated metabolic disturbances. Here, we aimed at identifying the pathogenic processes underlying impaired adipocyte diffe...

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Veröffentlicht in:eLife 2021-09, Vol.10
Hauptverfasser: Sánchez-Ceinos, Julia, Guzmán-Ruiz, Rocío, Rangel-Zúñiga, Oriol Alberto, López-Alcalá, Jaime, Moreno-Caño, Elena, Del Río-Moreno, Mercedes, Romero-Cabrera, Juan Luis, Pérez-Martínez, Pablo, Maymo-Masip, Elsa, Vendrell, Joan, Fernández-Veledo, Sonia, Fernández-Real, José Manuel, Laurencikiene, Jurga, Rydén, Mikael, Membrives, Antonio, Luque, Raul M, López-Miranda, José, Malagón, María M
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Sprache:eng
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Zusammenfassung:Preadipocytes are crucial for healthy adipose tissue expansion. Preadipocyte differentiation is altered in obese individuals, which has been proposed to contribute to obesity-associated metabolic disturbances. Here, we aimed at identifying the pathogenic processes underlying impaired adipocyte differentiation in obese individuals with insulin resistance (IR)/type 2 diabetes (T2D). We report that down-regulation of a key member of the major spliceosome, PRFP8 /PRP8, as observed in IR/T2D preadipocytes from subcutaneous (SC) fat, prevented adipogenesis by altering both the expression and splicing patterns of adipogenic transcription factors and lipid droplet-related proteins, while adipocyte differentiation was restored upon recovery of PRFP8 /PRP8 normal levels. Adipocyte differentiation was also compromised under conditions of endoplasmic reticulum (ER)-associated protein degradation (ERAD) hyperactivation, as occurs in SC and omental (OM) preadipocytes in IR/T2D obesity. Thus, targeting mRNA splicing and ER proteostasis in preadipocytes could improve adipose tissue function and thus contribute to metabolic health in obese individuals.
ISSN:2050-084X
2050-084X
DOI:10.7554/eLife.65996