Hatem-Vaquero Marco, Griera Mercedes, Garcia-Ayuso Diego, Campillo Sofia, Bohorquez Lourdes, Calleros Laura, Rodriguez-Puyol Diego, Rodriguez-Puyol Manuel, de Frutos Sergio
Department of Systems Biology, Physiology Unit, from Universidad de Alcalá, Alcalá de Henares, Madrid, Spain.
Instituto Ramón y Cajal de Investigación Sanitária (IRYCIS), Fundación Renal Iñigo Álvarez de Toledo (FRIAT) and REDinREN from Instituto de Salud Carlos III, Madrid, Spain.
Cell Physiol Biochem. 2020 Jan 24;54(1):71-87. doi: 10.33594/000000206.
BACKGROUND/AIMS: Diabetes type 2, metabolic syndrome or non-alcoholic fatty liver disease are insulin resistance-related metabolic disorders, which lack a better prognosis before their full establishment. We studied the importance of the intracellular scaffold protein integrin linked kinaes (ILK) as a key modulator in the initial pathogenesis and the early progression of those insulin resistance- related disorders.
Adult mice with a global transgenic downregulation of ILK expression (cKD-ILK) and littermates without that depletion (CT) were fed with either standard (STD) or high fat (HFD) diets during 2 and 6 weeks. Weights, blood glucose and other systemic biochemical parameters were determined in animals under fasting conditions and after glucose or pyruvate intraperitoneal injections to test their tolerance. In RNA or proteins extracted from insulin-sensitive tissues, we determined by reverse transcription-quantitative PCR and western blot the expression of ILK, metabolites transporters and other metabolism and inflammatory markers. Glucose uptake capacity was studied in freshly isolated tissues.
HFD feeding was able to early and progressively increase glycaemia, insulinemia, circulating glycerol, body weight gain, liver-mediated gluconeogenesis along this time lapse, but cKD-ILK have all these systemic misbalances exacerbated compared to CT in the same HFD time lapse. Interestingly, the tisular expression of ILK in HFD-fed CT was dramatically downregulated in white adipose tissue (WAT), skeletal muscle and liver at the same extent of the original ILK downregulation of cKD-ILK. We previously published that basal STD-fed cKD-ILK compared to basal STD-CT have different expression of glucose transporters GLUT4 in WAT and skeletal muscle. In the same STD-fed cKD-ILK, we observed here the increased expressions of hepatic GLUT2 and WAT pro-inflammatory cytokines TNF-α and MCP-1. The administration of HFD exacerbated the expression changes in cKD-ILK of these and other markers related to the imbalanced metabolism observed, such as WAT lipolysis (HSL), hepatic gluconeogenesis (PCK-1) and glycerol transport (AQP9).
ILK expression may be taken as a predictive determinant of metabolic disorders establishment, because its downregulation seems to correlate with the early imbalance of glucose and glycerol transport and the subsequent loss of systemic homeostasis of these metabolites.
背景/目的:2型糖尿病、代谢综合征或非酒精性脂肪性肝病是与胰岛素抵抗相关的代谢紊乱疾病,在其完全形成之前缺乏较好的预后。我们研究了细胞内支架蛋白整合素连接激酶(ILK)作为这些与胰岛素抵抗相关疾病初始发病机制和早期进展的关键调节因子的重要性。
对ILK表达进行整体转基因下调的成年小鼠(cKD-ILK)及其未进行该基因敲除的同窝小鼠(CT),在2周和6周内分别给予标准(STD)或高脂(HFD)饮食。在禁食条件下以及腹腔注射葡萄糖或丙酮酸后,测定动物的体重、血糖和其他全身生化参数,以测试其耐受性。从胰岛素敏感组织中提取RNA或蛋白质,通过逆转录定量PCR和蛋白质印迹法测定ILK、代谢物转运蛋白以及其他代谢和炎症标志物的表达。在新鲜分离的组织中研究葡萄糖摄取能力。
在这段时间内,高脂饮食能够早期并逐渐增加血糖、胰岛素血症、循环甘油水平、体重增加以及肝脏介导的糖异生,但与相同高脂饮食时间的CT相比,cKD-ILK的所有这些全身失衡情况都更加严重。有趣的是,在高脂饮食喂养的CT中,白色脂肪组织(WAT)、骨骼肌和肝脏中ILK的组织表达下调程度与cKD-ILK最初的ILK下调程度相同。我们之前发表过,与基础STD-CT相比,基础STD喂养的cKD-ILK在WAT和骨骼肌中葡萄糖转运蛋白GLUT4的表达不同。在相同的STD喂养的cKD-ILK中,我们在此观察到肝脏GLUT2以及WAT促炎细胞因子TNF-α和MCP-1的表达增加。高脂饮食的给予加剧了cKD-ILK中这些以及其他与观察到的代谢失衡相关标志物的表达变化,如WAT脂解(HSL)、肝脏糖异生(PCK-1)和甘油转运(AQP9)。
ILK表达可被视为代谢紊乱发生的预测决定因素,因为其下调似乎与葡萄糖和甘油转运的早期失衡以及这些代谢物随后的全身稳态丧失相关。
