骨唾液蛋白RGD区对小鼠代谢活性的影响

IF 1.5 Q3 DENTISTRY, ORAL SURGERY & MEDICINE Frontiers in dental medicine Pub Date : 2023-03-10 DOI:10.3389/fdmed.2023.1124084
K. Nagasaki, Atsuhiro Nagasaki, J. Taylor, B. Kear, Yinyan Ma, M. Somerman, O. Gavrilova
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引用次数: 1

摘要

骨涎蛋白(BSP)是矿化组织形成的关键调节因子。之前,我们通过将无功能的KAE(赖氨酸-丙氨酸-谷氨酸)序列替换为整合素结合的RGD(精氨酸-甘氨酸-天冬氨酸)序列,生成了BSP-KAE敲入小鼠(KAEKI小鼠),并报道了BSP-RGD基序在调节牙周韧带(PDL)中的重要作用。具体地说,组织学上PDL的无序被注意到,导致PDL的功能减弱,通过动态力学分析测量。有趣的是,KAEKI小鼠的体重也随着年龄的增长而增加。虽然一些与矿化组织相关的蛋白质被报道影响能量代谢,但BSP-RGD区域的代谢作用尚未被阐明。在这里,我们专注于定义BSP-RGD区域在代谢活动中的作用。方法测定野生型(WT)和KAEKI小鼠的体重、体成分和热量摄入。利用能量平衡技术估算能量消耗。收集附睾脂肪、肩胛间脂肪和肝脏进行组织学分析。通过血清分析、胰岛素耐量和葡萄糖耐量试验评估系统代谢表型。结果KAEKI小鼠从出生后13周开始出现轻度肥胖。体重的增加与瘦质量和内脏脂肪的增加相关。组织学检查显示KAEKI与WT小鼠在17 wpn时白色附睾脂肪和肩胛间棕色脂肪的脂肪细胞肥大。代谢分析显示KAEKI小鼠有血脂异常和高瘦素血症,但葡萄糖代谢无明显变化。能量平衡分析显示,KAEKI小鼠的贪食先于体重增加。结论BSP RGD区通过调节食物摄入影响能量代谢,其机制有待进一步研究。
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The RGD region of bone sialoprotein affects metabolic activity in mice
Introduction Bone sialoprotein (BSP) is a key regulator of mineralized tissue formation. Previously, we generated BSP-KAE knock-in mice (KAEKI mice) by substituting a non-function KAE (lysine-alanine-glutamic acid) for the integrin-binding RGD (arginine-glycine-aspartic acid) sequence and reported a vital role of the BSP-RGD motif in modulating the periodontal ligament (PDL). Specifically, histologically a disorganization of the PDL was noted, resulting in a weakened function of the PDL as measured by dynamic mechanical analysis. Intriguingly, also noted was a weight gain as KAEKI mice aged. While several proteins associated with mineralized tissues are reported to affect energy metabolism, the metabolic role of the BSP-RGD region has yet to be elucidated. Here we focus on defining the role of the BSP-RGD region in metabolic activity. Methods Body weight, body composition, and caloric intake were measured in wild type (WT) and KAEKI mice. Energy expenditure was estimated using energy balance technique. Epididymal fat, interscapular fat, and liver were harvested for histological analysis. Systemic metabolic phenotype was assessed by sera analyses, insulin tolerance and glucose tolerance tests. Results The results showed that KAEKI mice developed mild obesity starting from 13 weeks postnatal (wpn). The increase in body weight correlated with an increase in lean mass and visceral adiposity. Histological examination revealed adipocyte hypertrophy in white epididymal fat and interscapular brown fat in KAEKI vs. WT mice at 17 wpn. Metabolic profiling indicated that KAEKI mice had dyslipidemia and hyperleptinemia but no significant changes in glucose metabolism. Energy balance analyses revealed that hyperphagia preceded weight gain in KAEKI mice. Conclusion These data suggest that the RGD region of BSP affects energy metabolism by regulating food intake, with further studies warranted to uncover the underlying mechanisms.
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