胰岛素受体基因突变杂合携带者中胰岛素清除受损对骨骼肌体内胰岛素信号传导的部分挽救作用。
Partial rescue of in vivo insulin signalling in skeletal muscle by impaired insulin clearance in heterozygous carriers of a mutation in the insulin receptor gene.
作者信息
Højlund K, Wojtaszewski J F P, Birk J, Hansen B F, Vestergaard H, Beck-Nielsen H
机构信息
Diabetes Research Centre, Department of Endocrinology, Odense University Hospital, Odense, Denmark.
出版信息
Diabetologia. 2006 Aug;49(8):1827-37. doi: 10.1007/s00125-006-0312-6. Epub 2006 Jun 8.
AIMS/HYPOTHESIS: Recently we reported the coexistence of postprandial hypoglycaemia and moderate insulin resistance in heterozygous carriers of the Arg1174Gln mutation in the insulin receptor gene (INSR). Controlled studies of in vivo insulin signalling in humans with mutant INSR are unavailable, and therefore the cellular mechanisms underlying insulin resistance in Arg1174Gln carriers remain to be clarified.
SUBJECTS, MATERIALS AND METHODS: We studied glucose metabolism and insulin signalling in skeletal muscle from six Arg1174Gln carriers and matched control subjects during a euglycaemic-hyperinsulinaemic clamp.
RESULTS
Impaired clearance of exogenous insulin caused four-fold higher clamp insulin levels in Arg1174Gln carriers compared with control subjects (p<0.05). In Arg1174Gln carriers insulin increased glucose disposal and non-oxidative glucose metabolism (p<0.05), but to a lower extent than in controls (p<0.05). Insulin increased Akt phosphorylation at Ser473 and Thr308, inhibited glycogen synthase kinase-3alpha activity, reduced phosphorylation of glycogen synthase at sites 3a+3b, and increased glycogen synthase activity in Arg1174Gln carriers (all p<0.05). In the insulin-stimulated state, Akt phosphorylation at Thr308 and glycogen synthase activity were reduced in Arg1174Gln carriers compared with controls (p<0.05), whereas glycogen synthase kinase-3alpha activity and phosphorylation of glycogen synthase at sites 3a+3b were similar in the two groups.
CONCLUSIONS/INTERPRETATION: In vivo insulin signalling in skeletal muscle of patients harbouring the Arg1174Gln mutation is surprisingly intact, with modest impairments in insulin-stimulated activity of Akt and glycogen synthase explaining the moderate degree of insulin resistance. Our data suggest that impaired insulin clearance in part rescues in vivo insulin signalling in muscle in these carriers of a mutant INSR, probably by increasing insulin action on the non-mutated insulin receptors.
目的/假设:最近我们报道了胰岛素受体基因(INSR)中Arg1174Gln突变的杂合子携带者存在餐后低血糖和中度胰岛素抵抗。目前尚无关于携带突变INSR的人类体内胰岛素信号传导的对照研究,因此,Arg1174Gln携带者胰岛素抵抗的细胞机制仍有待阐明。
对象、材料与方法:我们在正常血糖-高胰岛素钳夹期间研究了6名Arg1174Gln携带者和匹配的对照受试者骨骼肌中的葡萄糖代谢和胰岛素信号传导。
结果
与对照受试者相比,Arg1174Gln携带者中外源胰岛素清除受损导致钳夹胰岛素水平高出四倍(p<0.05)。在Arg1174Gln携带者中,胰岛素增加了葡萄糖处置和非氧化葡萄糖代谢(p<0.05),但程度低于对照组(p<0.05)。胰岛素增加了Arg1174Gln携带者中Ser473和Thr308位点的Akt磷酸化,抑制了糖原合酶激酶-3α活性,降低了糖原合酶3a+3b位点的磷酸化,并增加了糖原合酶活性(均p<0.05)。在胰岛素刺激状态下,与对照组相比,Arg1174Gln携带者中Thr308位点的Akt磷酸化和糖原合酶活性降低(p<0.05),而两组中糖原合酶激酶-3α活性和糖原合酶3a+3b位点的磷酸化相似。
结论/解读:携带Arg1174Gln突变的患者骨骼肌中的体内胰岛素信号传导出人意料地完整,Akt和糖原合酶的胰岛素刺激活性存在适度损害,这解释了中度胰岛素抵抗程度。我们的数据表明,胰岛素清除受损部分挽救了这些突变INSR携带者肌肉中的体内胰岛素信号传导,可能是通过增加胰岛素对未突变胰岛素受体的作用。
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