激素敏感性脂肪酶基因突变与 2 型糖尿病风险
Null mutation in hormone-sensitive lipase gene and risk of type 2 diabetes.
机构信息
Program for Personalized and Genomic Medicine and Department of Medicine, University of Maryland School of Medicine (J.S.A., L.M.Y.-A., R.B.H., T.I.P., U.T.S., S.C., S.S., J.R.O., D.-W.G., J.C.M., A.R.S., C.S., C.M.D.), and the Geriatrics Research and Education Clinical Center (D.-W.G., A.S.R., A.R.S., C.S.), Department of Radiology and Nuclear Medicine (R.J.B.), and the Veterans Affairs (VA) Research Service, Department of Medicine, Division of Gerontology and Geriatric Medicine (A.S.R.), Baltimore VA Medical Center - all in Baltimore; and the Department of Medicine, Columbia University, New York (W.S.B.).
出版信息
N Engl J Med. 2014 Jun 12;370(24):2307-2315. doi: 10.1056/NEJMoa1315496. Epub 2014 May 21.
BACKGROUND
Lipolysis regulates energy homeostasis through the hydrolysis of intracellular triglycerides and the release of fatty acids for use as energy substrates or lipid mediators in cellular processes. Genes encoding proteins that regulate energy homeostasis through lipolysis are thus likely to play an important role in determining susceptibility to metabolic disorders.
METHODS
We sequenced 12 lipolytic-pathway genes in Old Order Amish participants whose fasting serum triglyceride levels were at the extremes of the distribution and identified a novel 19-bp frameshift deletion in exon 9 of LIPE, encoding hormone-sensitive lipase (HSL), a key enzyme for lipolysis. We genotyped the deletion in DNA from 2738 Amish participants and performed association analyses to determine the effects of the deletion on metabolic traits. We also obtained biopsy specimens of abdominal subcutaneous adipose tissue from 2 study participants who were homozygous for the deletion (DD genotype), 10 who were heterozygous (ID genotype), and 7 who were noncarriers (II genotype) for assessment of adipose histologic characteristics, lipolysis, enzyme activity, cytokine release, and messenger RNA (mRNA) and protein levels.
RESULTS
Carriers of the mutation had dyslipidemia, hepatic steatosis, systemic insulin resistance, and diabetes. In adipose tissue from study participants with the DD genotype, the mutation resulted in the absence of HSL protein, small adipocytes, impaired lipolysis, insulin resistance, and inflammation. Transcription factors responsive to peroxisome-proliferator-activated receptor γ (PPAR-γ) and downstream target genes were down-regulated in adipose tissue from participants with the DD genotype, altering the regulation of pathways influencing adipogenesis, insulin sensitivity, and lipid metabolism.
CONCLUSIONS
These findings indicate the physiological significance of HSL in adipocyte function and the regulation of systemic lipid and glucose homeostasis and underscore the severe metabolic consequences of impaired lipolysis. (Funded by the National Institutes of Health and others).
背景
脂肪分解通过水解细胞内甘油三酯并释放脂肪酸,将能量代谢平衡作为能量底物或脂质代谢介质,从而调节能量代谢平衡。因此,编码通过脂肪分解调节能量代谢平衡的蛋白质的基因很可能在决定代谢紊乱易感性方面发挥重要作用。
方法
我们对 Old Order Amish 参与者的 12 个脂肪分解途径基因进行了测序,这些参与者的空腹血清甘油三酯水平处于分布的极值,并在编码激素敏感脂肪酶(HSL)的 LIPE 外显子 9 中发现了一个新的 19 个碱基对的移码缺失,HSL 是脂肪分解的关键酶。我们对 2738 名 Amish 参与者的 DNA 进行了缺失基因分型,并进行了关联分析,以确定缺失对代谢特征的影响。我们还从 2 名携带缺失突变的纯合子(DD 基因型)、10 名杂合子(ID 基因型)和 7 名非携带者(II 基因型)的研究参与者中获得了腹部皮下脂肪组织活检标本,用于评估脂肪组织学特征、脂肪分解、酶活性、细胞因子释放以及信使 RNA(mRNA)和蛋白质水平。
结果
突变携带者有血脂异常、肝脂肪变性、全身胰岛素抵抗和糖尿病。在携带 DD 基因型的研究参与者的脂肪组织中,该突变导致 HSL 蛋白缺失、小脂肪细胞、脂肪分解受损、胰岛素抵抗和炎症。对过氧化物酶体增殖物激活受体 γ(PPAR-γ)反应的转录因子和下游靶基因在携带 DD 基因型的参与者的脂肪组织中下调,改变了影响脂肪生成、胰岛素敏感性和脂质代谢途径的调节。
结论
这些发现表明 HSL 在脂肪细胞功能和全身脂质及葡萄糖代谢平衡调节中的生理意义,并强调了脂肪分解受损的严重代谢后果。(由美国国立卫生研究院和其他机构资助)。
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