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GALNT2介导的脂肪生成的形态学和分子特征

Morphological and molecular characterization of GALNT2-mediated adipogenesis.

作者信息

Antonucci Alessandra, Marucci Antonella, Scarale Maria Giovanna, De Bonis Concetta, Mangiacotti Davide, Trischitta Vincenzo, Di Paola Rosa

机构信息

Research Unit of Diabetes and Endocrine Diseases, Fondazione IRCCS Casa Sollievo della Sofferenza, San Giovanni Rotondo, FG, Italy.

Department of Experimental Medicine, Sapienza University, Rome, Italy.

出版信息

Int J Obes (Lond). 2021 Jun;45(6):1362-1366. doi: 10.1038/s41366-021-00789-3. Epub 2021 Mar 3.

Abstract

3T3L1 mouse pre-adipocytes develop into adipocytes differently in response to GALNT2 overexpression or to stimulation with rosiglitazone, a reference inducer of adipogenesis. To investigate the biology of alternative pathways of adipogenesis, we studied lipid droplets (LD) morphology, chromatin organization, and gene expression in GALNT2- versus rosiglitazone-induced 3T3L1 adipogenesis. 3T3L1 overexpressing either GALNT2 (GALNT2) or GFP and treated with rosiglitazone (GFPR) were differentiated into adipocytes. LD and nuclei were profiled measuring their morphological features. The expression of adipogenesis-related genes was measured by RT-PCR. As compared to GFPR, GALNT2 showed smaller and more clustered LD, more nuclei with condensed chromatin and several gene expression changes (P < 0.001 for all). As compared to those stimulated by rosiglitazone, GALNT2 overexpressing cells show differences in the most established readouts of adipogenesis. Characterizing alternative pathways of adipogenesis may help tackle those diseases which are secondary to increased dysfunctional mass of adipose tissue.

摘要

3T3L1小鼠前脂肪细胞对GALNT2过表达或罗格列酮(一种脂肪生成的参考诱导剂)刺激的反应不同,会发育成脂肪细胞。为了研究脂肪生成替代途径的生物学特性,我们研究了GALNT2诱导与罗格列酮诱导的3T3L1脂肪生成过程中的脂滴(LD)形态、染色质组织和基因表达。过表达GALNT2(GALNT2)或绿色荧光蛋白(GFP)并用罗格列酮处理(GFPR)的3T3L1细胞被诱导分化为脂肪细胞。对脂滴和细胞核进行分析,测量它们的形态特征。通过逆转录聚合酶链反应(RT-PCR)检测脂肪生成相关基因的表达。与GFPR相比,GALNT2显示出更小且更聚集的脂滴、更多染色质凝聚的细胞核以及一些基因表达变化(所有变化P < 0.001)。与罗格列酮刺激的细胞相比,过表达GALNT2的细胞在最成熟的脂肪生成指标上存在差异。表征脂肪生成的替代途径可能有助于应对那些继发于脂肪组织功能失调性质量增加的疾病。

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