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MCH基因敲除小鼠对与衰老相关的体重增加和胰岛素抵抗具有抗性。

MCH-/- mice are resistant to aging-associated increases in body weight and insulin resistance.

作者信息

Jeon Justin Y, Bradley Richard L, Kokkotou Efi G, Marino Francis E, Wang Xiaomei, Pissios Pavlos, Maratos-Flier Eleftheria

机构信息

Division of Endocrinology, Department of Medicine, Beth Israel Deaconess Medical Center, Boston, MA 02215, USA.

出版信息

Diabetes. 2006 Feb;55(2):428-34. doi: 10.2337/diabetes.55.02.06.db05-0203.

Abstract

Ablation of the hypothalamic peptide, melanin-concentrating hormone (MCH), leads to a lean phenotype and resistance to diet-induced obesity. Observation of MCH(-/-) mice at older ages suggested that these effects persist in mice >1 year old. Leanness secondary to caloric restriction is known to be associated with improved glucose tolerance as well as an overall increase in life span. Because the MCH(-/-) model represents leanness secondary to increased energy expenditure rather than caloric restriction, we were interested in determining whether this model of leanness would be associated with beneficial metabolic effects at older ages. To assess the effects of MCH ablation over a more prolonged period, we monitored male and female MCH(-/-) mice up to 19 months. The lean phenotype of MCH(-/-) mice persisted over the duration of the study. At 19 months, MCH(-/-) male and female mice weighed 23.4 and 30.8% less than their wild-type counterparts, a result of reduced fat mass in MCH(-/-) mice. Aged MCH(-/-) mice exhibited better glucose tolerance and were more insulin sensitive compared with wild-type controls. Aging-associated decreases in locomotor activity were also attenuated in MCH(-/-) mice. We also evaluated two molecules implicated in the pathophysiology of aging, p53 and silent inflammatory regulator 2 (Sir2). We found that expression of the tumor suppressor protein p53 was higher in MCH(-/-) mice at 9 and 19 months of age. In contrast, expression of Sir2 was unchanged. In aggregate, these findings suggest that MCH ablation improves the long-term outcome for several indicators of the aging process.

摘要

切除下丘脑肽——促黑素细胞激素(MCH),会导致小鼠出现瘦型表型,并对饮食诱导的肥胖产生抗性。对老年MCH基因敲除(MCH(-/-))小鼠的观察表明,这些效应在1岁以上的小鼠中依然存在。已知因热量限制导致的消瘦与葡萄糖耐量改善以及寿命总体延长有关。由于MCH(-/-)模型代表的是因能量消耗增加而非热量限制导致的消瘦,我们有兴趣确定这种消瘦模型在老年时是否会伴有有益的代谢效应。为了评估更长时期内MCH切除的影响,我们对雄性和雌性MCH(-/-)小鼠进行了长达19个月的监测。在整个研究期间,MCH(-/-)小鼠的瘦型表型一直持续。19个月时,MCH(-/-)雄性和雌性小鼠的体重分别比野生型对照小鼠轻23.4%和30.8%,这是MCH(-/-)小鼠脂肪量减少的结果。与野生型对照相比,老年MCH(-/-)小鼠表现出更好的葡萄糖耐量,且对胰岛素更敏感。MCH(-/-)小鼠中与衰老相关的运动活动减少也有所减轻。我们还评估了与衰老病理生理学相关的两个分子,即p53和沉默炎症调节因子2(Sir2)。我们发现,在9个月和19个月大时,肿瘤抑制蛋白p53在MCH(-/-)小鼠中的表达较高。相比之下,Sir2的表达没有变化。总的来说,这些发现表明,切除MCH可改善衰老过程中几个指标的长期结果。

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