Zhou Hongyi, Xu Cheng, Lee Hakjoo, Yoon Yisang, Chen Weiqin
Department of Physiology, Medical College of Georgia at Augusta University, Augusta, GA 30912, USA.
Department of Physiology, Medical College of Georgia at Augusta University, Augusta, GA 30912, USA.
Mol Metab. 2020 Jun;36:100971. doi: 10.1016/j.molmet.2020.02.014. Epub 2020 Mar 4.
Understanding the mechanisms that control brown adipose tissue (BAT) mass and functionality is crucial for our understanding of how the disruption of energy homeostasis leads to obesity. Bernerdinali Seip Congenital Lipodystrophy (BSCL) type 2 (BSCL2, a.k.a. SEIPIN), a lipodystrophy-associated protein, has been shown to not be required for brown adipogenesis, but it has been shown to be essential for perinatal BAT development. However, its role in mature BAT maintenance and thermogenic programing remains poorly understood.
We subjected Bscl2 and Bscl2 (BKO) mice with a brown adipose-specific loss of BSCL2 through UCP1 promoter-driven Cre to environmental, pharmacological and diet interventions to challenge BAT functionality and reprogramming. We carried out physiological, molecular and transcriptomic analyses of BAT.
The deletion of BSCL2 in mature brown adipocytes increased sympathetic nervous system-independent cAMP/protein kinase A (PKA) signaling in BAT. Such activation reduced BAT triglyceride content and mass and was sufficient to reduce plasma triglyceride, but not enough to combat thermoneutral and high fat diet-induced obesity. Surprisingly, BKO mice displayed an impaired response to acute and chronic cold challenges despite cAMP/PKA activation. When subjected to chronic cold exposure or the administration of a β3-adrenergic agonist, CL 316,243, BKO mice failed to induce BAT recruitment and underwent dramatic brown adipocyte loss. Transcriptomic analysis revealed pathological BAT remodeling with inflammation and fibrosis, which was further exacerbated by a chronic thermogenic challenge in BKO mice. Mechanistically, we found abnormal mitochondrial shapes and function in BAT of BKO mice housed at 21 °C; as well as mitochondrial DNA depletion and necroptotic-mediated brown adipocyte death after chronic thermogenic insult.
BSCL2-mediated lipid catabolism within BAT is crucial for mature brown adipocyte function and survival both during times of activation and quiescence. BSCL2 is an important regulator of mature brown adipocyte mitochondrial metabolism, necroptosis and thus adaptive thermogenesis.
了解控制棕色脂肪组织(BAT)质量和功能的机制,对于我们理解能量稳态的破坏如何导致肥胖至关重要。2型贝纳迪纳利·塞普先天性脂肪营养不良(BSCL)(BSCL2,又称SEIPIN),一种与脂肪营养不良相关的蛋白质,已被证明对于棕色脂肪生成并非必需,但已被证明对于围产期BAT发育至关重要。然而,其在成熟BAT维持和产热编程中的作用仍知之甚少。
我们通过UCP1启动子驱动的Cre使Bscl2和Bscl2(BKO)小鼠棕色脂肪特异性缺失BSCL2,使其接受环境、药理学和饮食干预,以挑战BAT功能和重编程。我们对BAT进行了生理、分子和转录组分析。
成熟棕色脂肪细胞中BSCL2的缺失增加了BAT中不依赖交感神经系统的cAMP/蛋白激酶A(PKA)信号传导。这种激活降低了BAT甘油三酯含量和质量,足以降低血浆甘油三酯,但不足以对抗热中性和高脂肪饮食诱导的肥胖。令人惊讶的是,尽管cAMP/PKA被激活,但BKO小鼠对急性和慢性寒冷挑战的反应受损。当接受慢性寒冷暴露或给予β3-肾上腺素能激动剂CL 316,243时,BKO小鼠未能诱导BAT募集并经历显著的棕色脂肪细胞丢失。转录组分析揭示了伴有炎症和纤维化的病理性BAT重塑,在BKO小鼠中,慢性产热挑战进一步加剧了这种重塑。从机制上讲,我们发现在21°C饲养的BKO小鼠的BAT中,线粒体形状和功能异常;以及慢性产热损伤后线粒体DNA耗竭和坏死性凋亡介导的棕色脂肪细胞死亡。
BAT内BSCL2介导的脂质分解代谢对于成熟棕色脂肪细胞在激活和静止期间的功能和存活至关重要。BSCL2是成熟棕色脂肪细胞线粒体代谢、坏死性凋亡以及适应性产热的重要调节因子。
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