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Cortical and subcortical gray matter structural alterations in normoglycemic obese and type 2 diabetes patients: relationship with adiposity, glucose, and insulin

机译:常规血糖肥胖和2型糖尿病患者的皮质和皮质灰质结构改变:与肥胖,葡萄糖和胰岛素的关系

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Type 2 diabetes (T2DM) is associated with structural cortical and subcortical alterations, although it is insufficiently clear if these alterations are driven by obesity or by diabetes and its associated complications. We used FreeSurfer5.3 and FSL-FIRST to determine cortical thickness, volume and surface area, and subcortical gray matter volume in a group of 16 normoglycemic obese subjects and 28 obese T2DM patients without clinically manifest micro- and marcoangiopathy, and compared them to 31 lean normoglycemic controls. Forward regression analysis was used to determine demographic and clinical correlates of altered (sub)cortical structure. Exploratively, vertex-wise correlations between cortical structure and fasting glucose and insulin were calculated. Compared with controls, obese T2DM patients showed lower right insula thickness and lower left lateral occipital surface area (P (FWE) 0.05). Normoglycemic obese versus controls had lower thickness (P (FWE) 0.05) in the right insula and inferior frontal gyrus, and higher amygdala and thalamus volume. Thalamus volume and left paracentral surface area were also higher in this group compared with obese T2DM patients. Age, sex, BMI, fasting glucose, and cholesterol were related to these (sub)cortical alterations in the whole group (all P 0.05). Insulin were related to temporal and frontal structural deficits (all P (FWE) 0.05). Parietal/occipital structural deficits may constitute early T2DM-related cerebral alterations, whereas in normoglycemic obese subjects, regions involved in emotion, appetite, satiety regulation, and inhibition were affected. Central adiposity and elevated fasting glucose may constitute risk factors.
机译:2型糖尿病(T2DM)与结构皮质和皮比奇改变相关,尽管如果这些改变由肥胖或糖尿病及其相关的并发症驱动,则不充分清晰。我们使用FreSurfer5.3和FSL-First来确定皮质厚度,体积和表面积,以及一组16个常规血糖肥胖受试者和28名肥胖T2DM患者的皮质灰质体积,没有临床上显现的微观和Marcoang病变,并将其与31次进行比较瘦季度血糖控制。前转回归分析用于确定改变(子)皮质结构的人口统计和临床关联。探索地,计算皮质结构和空腹葡萄糖与胰岛素之间的顶点相关性。与对照相比,肥胖的T2DM患者显示出较低的右侧肠厚度和左下侧枕表面区域(P(FWE)<0.05)。右侧血糖和较低额相回到的常见膜与控制的较低厚度(p(fwe)<0.05),较高的杏仁芽孢杆菌和丘脑体积。与肥胖的T2DM患者相比,该组的丘脑体积和左侧高级表面积也更高。年龄,性别,BMI,空腹葡萄糖和胆固醇与整个组中的这些(亚)皮质改变有关(所有P <0.05)。胰岛素与时间和前结构缺陷有关(所有P(FWE)<0.05)。顶点/枕骨结构赤字可能构成早期的T2DM相关的脑改变,而在常规血糖肥胖受试者中,涉及情绪,食欲,饱腹感和抑制的地区受到影响。中央肥胖和升高的空腹葡萄糖可能构成风险因素。

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