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怀孕会引发分子变化,这反映出胰岛素对葡萄糖氧化途径的控制受损,而这种情况仅在有2型糖尿病家族史的女性中会在孕期结束后持续存在。

Pregnancy induces molecular alterations reflecting impaired insulin control over glucose oxidative pathways that only in women with a family history of Type 2 diabetes last beyond pregnancy.

作者信息

Piccinini M, Mostert M, Seardo M A, Bussolino S, Alberto G, Lupino E, Ramondetti C, Buccinnà B, Rinaudo M T

机构信息

Department of Medicine and Experimental Oncology-Section of Biochemistry, University of Turin, 10126 Turin, Italy.

出版信息

J Endocrinol Invest. 2009 Jan;32(1):6-12. doi: 10.1007/BF03345670.

Abstract

In circulating lymphomonocytes (CLM) of patients with Type 2 diabetes (DM2) pyruvate dehydrogenase (PDH), the major determinant of glucose oxidative breakdown, is affected by a cohort of alterations reflecting impaired insulin stimulated glucose utilization. The cohort is also expressed, although incompletely, in 40% of healthy young subjects with a DM2-family history (FH). Pregnancy restrains glucose utilization in maternal peripheral tissues to satisfy fetal requirements. Here we explore whether pregnant women develop the PDH alterations and, if so, whether there are differences between women with and without FH (FH+, FH-). Ten FH+ and 10 FH- were evaluated during pregnancy (12-14, 24-26, and 37-39 weeks) and 1 yr after (follow-up) for fasting plasma glucose and insulin as well as body mass index (BMI), and for the PDH alterations. Twenty FH- and 20 FH+ non-pregnant women served as controls. All FH+ and FH- controls exhibited normal clinical parameters and 8 FH+ had an incomplete cohort of PDH alterations. In FH- and FH+ pregnant women at 12-14 weeks clinical parameters were normal; from 24-26 weeks, with unvaried glucose, insulin and BMI rose more in FH- and only in the latter recovered the 12-14 weeks values at follow-up. In all FH-, the cohort of PDH alterations was incomplete at 24-26 weeks, complete at 37-39 weeks, and absent at follow-up but complete from 12-14 weeks including follow-up in all FH+. In FH-, the cohort is an acquired trait restricted to pregnancy signaling transiently reduced insulin-stimulated glucose utilization; in FH+, instead, it unveils the existence of an inherited DM2-related background these women all have, that is awakened by pregnancy and as such lastingly impairs insulin-stimulated glucose utilization.

摘要

在2型糖尿病(DM2)患者的循环淋巴细胞(CLM)中,丙酮酸脱氢酶(PDH)作为葡萄糖氧化分解的主要决定因素,受到一系列反映胰岛素刺激葡萄糖利用受损的改变的影响。在40%有DM2家族史(FH)的健康年轻受试者中,这一系列改变也有表达,尽管并不完全。妊娠会抑制母体外周组织中的葡萄糖利用,以满足胎儿的需求。在此,我们探究孕妇是否会出现PDH改变,如果出现,有FH(FH+)和无FH(FH-)的女性之间是否存在差异。对10名FH+和10名FH-孕妇在孕期(12 - 14周、24 - 26周和37 - 39周)及产后1年(随访)进行评估,检测空腹血糖、胰岛素以及体重指数(BMI),并检测PDH改变情况。20名FH-和20名FH+非孕妇作为对照。所有FH+和FH-对照的临床参数均正常,8名FH+有不完全的PDH改变系列。在12 - 14周时,FH-和FH+孕妇的临床参数正常;从24 - 26周起,血糖不变,但胰岛素和BMI在FH-中升高更多,且仅在后者中随访时恢复到12 - 14周时的值。在所有FH-中,PDH改变系列在24 - 26周时不完全,在37 - 39周时完全,随访时不存在,但在所有FH+中从12 - 14周包括随访时都是完全的。在FH-中,该系列是一种仅限于妊娠的后天获得性特征,表明胰岛素刺激的葡萄糖利用暂时减少;而在FH+中,它揭示了这些女性都具有的与DM2相关的遗传背景的存在,这种背景被妊娠唤醒,从而持续损害胰岛素刺激的葡萄糖利用。

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