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首页> 美国卫生研究院文献>Frontiers in Synaptic Neuroscience >Brain-derived neurotrophic factor in VMH as the causal factor for and therapeutic tool to treat visceral adiposity and hyperleptinemia in type 2 diabetic Goto–Kakizaki rats
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Brain-derived neurotrophic factor in VMH as the causal factor for and therapeutic tool to treat visceral adiposity and hyperleptinemia in type 2 diabetic Goto–Kakizaki rats

机译:VMH的脑源性神经营养因子是2型糖尿病Goto-Kakizaki大鼠内脏肥胖和高脂血症的病因和治疗工具

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We previously reported that the type 2 diabetic Goto–Kakizaki (GK) rats at young adult ages (6–12 weeks) exhibited increased visceral fat mass and hyperleptinemia, due to hyperphagia caused primarily by neuropeptide Y (NPY) overexpression in the hypothalamic arcuate nucleus. Later, we found that GK rats continued to exhibit mesenteric fat accumulation and hyperleptinemia at least until 26 weeks of age, while hyperphagia and NPY overexpression ceased at 15 weeks of age. Therefore, we hypothesized that the long-lasting fat accumulation and hyperleptinemia are due to unidentified brain dysfunction other than NPY overexpression. In GK rats aged 26 weeks, glucose transporter-2 (GLUT2) mRNA expression in ventromedial hypothalamus (VMH) was markedly reduced in parallel with significant decreases in brain-derived neurotrophic factor (BDNF) mRNA level and BDNF-expressing cell numbers in the VMH. Pharmacologic inhibition of glucose utilization reduced BDNF mRNA expression in VMH in vivo and in vitro. The results suggested that impaired glucose utilization caused the reduction of BDNF. On the other hand, intracerebroventricular injection of BDNF for 6 days ameliorated hyperleptinemia in a long-lasting manner concurrently with feeding suppression in GK rats. Restricted feeding paired to BDNF-treated rats reduced plasma leptin level only transiently. BDNF treatment also reduced mesenteric fat mass in GK rats. These results reveal a novel action mode of BDNF to long-lastingly counteract visceral adiposity and hyperleptinemia in addition to and independently of its anorexigenic action. These results suggest that visceral fat accumulation and hyperleptinemia are at least partly due to the reduction of BDNF in VMH primarily caused by impaired glucose utilization in GK rats. The BDNF supplementation could provide an effective treatment of visceral obesity, hyperleptinemia and leptin resistance in type 2 diabetes.
机译:我们先前曾报道,成年幼龄(6至12周)的2型糖尿病Goto–Kakizaki(GK)大鼠表现出内脏脂肪量增加和高脂血症,这主要是由于下丘脑弓状核中神经肽Y(NPY)过度表达引起的食欲亢进。后来,我们发现GK大鼠至少在26周龄之前仍表现出肠系膜脂肪蓄积和高瘦素血症,而食欲亢进和NPY高表达在15周龄时停止。因此,我们假设持久的脂肪积累和高瘦素血症是由于除NPY过表达以外的未知的脑功能障碍所致。在26周龄的GK大鼠中,下丘脑下丘脑(VMH)中的葡萄糖转运蛋白2(GLUT2)mRNA表达显着降低,同时脑源性神经营养因子(BDNF)mRNA水平和BDNF表达细胞数量显着降低。体内和体外对葡萄糖利用的药理抑制作用降低了VMH中BDNF mRNA的表达。结果表明,葡萄糖利用受损导致BDNF降低。另一方面,脑室内注射BDNF持续6天可长期改善高脂血症,同时抑制GK大鼠的进食。限制喂养与BDNF处理的大鼠配对只能暂时降低血浆瘦素水平。 BDNF治疗还减少了GK大鼠的肠系膜脂肪量。这些结果揭示了BDNF除了其厌食作用外,还可以持久地抵消内脏脂肪和高瘦素血症的新型作用方式。这些结果表明,内脏脂肪蓄积和高瘦素血症至少部分归因于VMH中BDNF的降低,这主要是由于GK大鼠葡萄糖利用受损所致。 BDNF补充剂可以有效治疗2型糖尿病的内脏肥胖,高瘦素血症和瘦素抵抗。

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