The size of human subcutaneous adipocytes, but not adiposity, is associated with inflammation, endoplasmic reticulum stress, and insulin resistance markers

Abstract: Background The fat storage capacity of the adipose tissue prevents ectopic lipid deposition, which is one of the risk factors for metabolic abnormalities in obesity. This capacity depends upon the adipogenic gene expression and blood supply provision for tissue expansion through angiogenesis. Here, we studied hyperplasia/hypertrophy of subcutaneous white adipose tissue (scWAT) concerning adipogenic gene expression, angiogenic status, and metabolic parameters in non-obese and different classes of … Show more

“…It has been well documented that hypertrophic adipocytes are prone to developing organelle dysfunction, such as ER stress, mitochondrial dysfunction, and activation of the NLRP3 inflammasome pathway [ 42 , 43 ], suggesting that hypertrophically stressed adipocytes undergo pyroptotic cell death and initiate an inflammatory response. Given that BAC in Nfe2l1 (f)-KO mice exhibit noticeable hypertrophy, we reason that the BAT inflammation is the secondary consequence of hypertrophic stress.…”

Single-nucleus RNA-sequencing reveals NRF1/NFE2L1 as a key factor determining the thermogenesis and cellular heterogeneity and dynamics of brown adipose tissues in mice

“…It has been well documented that hypertrophic adipocytes are prone to developing organelle dysfunction, such as ER stress, mitochondrial dysfunction, and activation of the NLRP3 inflammasome pathway [ 42 , 43 ], suggesting that hypertrophically stressed adipocytes undergo pyroptotic cell death and initiate an inflammatory response. Given that BAC in Nfe2l1 (f)-KO mice exhibit noticeable hypertrophy, we reason that the BAT inflammation is the secondary consequence of hypertrophic stress.…”

Single-nucleus RNA-sequencing reveals NRF1/NFE2L1 as a key factor determining the thermogenesis and cellular heterogeneity and dynamics of brown adipose tissues in mice