Asai Akira, Nagao Mototsugu, Hayakawa Koji, Miyazawa Teruo, Sugihara Hitoshi, Oikawa Shinichi
Department of Endocrinology, Diabetes and Metabolism, Graduate School of Medicine, Nippon Medical School, Tokyo, Japan.
Food and Health Science Research Unit, Graduate School of Agricultural Science, Tohoku University, 468-1 Aramaki Aza Aoba, Aoba-ku, Sendai, 980-8572, Japan.
Diabetologia. 2020 Sep;63(9):1836-1846. doi: 10.1007/s00125-020-05191-8. Epub 2020 Jun 19.
AIMS/HYPOTHESIS: Obesity caused by overeating plays a pivotal role in the development of type 2 diabetes. However, it remains poorly understood how individual meal size differences are determined before the development of obesity. Here, we investigated the underlying mechanisms in determining spontaneous food intake in newly established Oikawa-Nagao Diabetes-Prone (ON-DP) and Diabetes-Resistant (ON-DR) mice.
Food intake and metabolic phenotypes of ON-DP and ON-DR mice under high-fat-diet feeding were compared from 5 weeks to 10 weeks of age. Differences in leptin status at 5 weeks of age were assessed between the two mouse lines. Adipose tissue explant culture was also performed to evaluate leptin production capacity in vitro.
ON-DP mice showed spontaneous overfeeding compared with ON-DR mice. Excessive body weight gain and fat accumulation in ON-DP mice were completely suppressed to the levels seen in ON-DR mice by pair-feeding with ON-DR mice. Deterioration of glucose tolerance in ON-DP mice was also ameliorated under the pair-feeding conditions. While no differences were seen in body weight and adipose tissue mass when comparing the two mouse lines at 5 weeks of age, the ON-DP mice had lower plasma leptin concentrations and adipose tissue leptin gene expression levels. In accordance with peripheral leptin status, ON-DP mice displayed lower anorexigenic leptin signalling in the hypothalamic arcuate nucleus when compared with ON-DR mice without apparent leptin resistance. Explant culture studies revealed that ON-DP mice had lower leptin production capacity in adipose tissue. ON-DP mice also displayed higher DNA methylation levels in the leptin gene promoter region of adipocytes when compared with ON-DR mice.
CONCLUSIONS/INTERPRETATION: The results suggest that heritable lower leptin production capacity plays a critical role in overfeeding-induced obesity and subsequent deterioration of glucose tolerance in ON-DP mice. Leptin production capacity in adipocytes, especially before the development of obesity, may have diagnostic potential for predicting individual risk of obesity caused by overeating and future onset of type 2 diabetes. Graphical abstract.
目的/假设:暴饮暴食导致的肥胖在2型糖尿病的发生发展中起关键作用。然而,在肥胖发生之前个体进食量差异是如何确定的,目前仍知之甚少。在此,我们研究了新建立的及川-长野糖尿病易感性(ON-DP)和糖尿病抗性(ON-DR)小鼠自发食物摄入量的潜在决定机制。
比较5至10周龄的高脂饮食喂养下ON-DP和ON-DR小鼠的食物摄入量和代谢表型。评估两个品系小鼠在5周龄时瘦素状态的差异。还进行了脂肪组织外植体培养以体外评估瘦素产生能力。
与ON-DR小鼠相比,ON-DP小鼠表现出自发过度进食。通过与ON-DR小鼠配对喂养,ON-DP小鼠过度的体重增加和脂肪堆积被完全抑制到ON-DR小鼠的水平。在配对喂养条件下,ON-DP小鼠葡萄糖耐量的恶化也得到改善。虽然在5周龄时比较两个品系小鼠的体重和脂肪组织质量没有差异,但ON-DP小鼠的血浆瘦素浓度和脂肪组织瘦素基因表达水平较低。与外周瘦素状态一致,与没有明显瘦素抵抗的ON-DR小鼠相比,ON-DP小鼠在下丘脑弓状核中显示出较低的厌食性瘦素信号传导。外植体培养研究表明,ON-DP小鼠脂肪组织中瘦素产生能力较低。与ON-DR小鼠相比,ON-DP小鼠脂肪细胞中瘦素基因启动子区域的DNA甲基化水平也更高。
结论/解读:结果表明,遗传性较低的瘦素产生能力在ON-DP小鼠的过度进食诱导的肥胖及随后的葡萄糖耐量恶化中起关键作用。脂肪细胞中的瘦素产生能力,尤其是在肥胖发生之前,可能具有预测暴饮暴食导致肥胖的个体风险和未来2型糖尿病发病的诊断潜力。图形摘要。
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