伊马替尼对早期体重增加过程中血管胰岛素敏感性和游离脂肪酸转运的影响。
Effects of imatinib on vascular insulin sensitivity and free fatty acid transport in early weight gain.
作者信息
Box Camiel V J, Sandhu Amandeep K, Turaihi Alexander H, Xiaoké Pan, Dallinga-Thie Geesje, Aman Jurjan, Eringa Etto C
机构信息
Department of Physiology, Amsterdam Cardiovascular Sciences (ACS), Amsterdam University Medical Center, Amsterdam, The Netherlands.
Department of Pulmonary Medicine, Amsterdam University Medical Center, Amsterdam, The Netherlands.
出版信息
PLoS One. 2021 Jul 2;16(7):e0250442. doi: 10.1371/journal.pone.0250442. eCollection 2021.
BACKGROUND
Vascular endothelial dysfunction is an essential part of the pathophysiology of type 2 diabetes and its complications. In type 2 diabetes, endothelial dysfunction is characterized by reduced insulin signaling and increased transendothelial transport of fatty acids (FA). As the Abl kinase inhibitor imatinib was previously shown to reverse type 2 diabetes and to inhibit VEGF signaling via Abl kinases, we studied the effect of imatinib on vascular insulin sensitivity and fatty acid transport in vivo and in vitro.
METHODS
C57/BL6J mice were fed a chow diet or Western diet (WD), and received daily imatinib injections for two weeks. Insulin-mediated vasoreactivity of resistance arteries was studied using intravital microscopy, and metabolic insulin sensitivity using the hyperinsulinemic-euglycemic clamp. The effect of imatinib on triglyceride content in skeletal muscle and heart in vivo was also determined. In vitro, the effect of imatinib on fatty acid transport was studied in human umbilical vein endothelial cells (HUVECs) by evaluating the effect of imatinib on fluorescently labeled FA uptake both under basal and VEGF-B-stimulated conditions.
RESULTS
Imatinib prevented the WD-induced weight gain in mice, independently from food intake. In line with this, imatinib enhanced insulin-mediated vasoreactivity of resistance arteries in the WD-fed mice. However, imatinib did not affect triglyceride content in muscle. In cultured endothelial cells, VEGF-B stimulation resulted in a time-dependent uptake of fatty acids in parallel with increased phosphorylation of the Abl kinase substrate Crk-like protein (CrkL) at Tyr207. Although imatinib effectively prevented VEGF-B-mediated Abl kinase activation, it had no effect on VEGF-B mediated endothelial FA uptake.
CONCLUSION
Imatinib prevents weight gain and preserves insulin-mediated vasodilation in WD-fed mice, but does not affect endothelial FA transport despite inhibiting VEGF-B signaling. The beneficial effect of imatinib on insulin-mediated vasodilation may contribute to the anti-diabetic effects of imatinib.
背景
血管内皮功能障碍是2型糖尿病及其并发症病理生理学的重要组成部分。在2型糖尿病中,内皮功能障碍的特征是胰岛素信号传导减少以及脂肪酸(FA)跨内皮转运增加。由于Abl激酶抑制剂伊马替尼先前已被证明可逆转2型糖尿病并通过Abl激酶抑制VEGF信号传导,因此我们研究了伊马替尼在体内和体外对血管胰岛素敏感性和脂肪酸转运的影响。
方法
给C57/BL6J小鼠喂食普通饮食或西式饮食(WD),并每天注射伊马替尼,持续两周。使用活体显微镜研究胰岛素介导的阻力动脉血管反应性,并使用高胰岛素-正常血糖钳夹技术研究代谢胰岛素敏感性。还测定了伊马替尼对体内骨骼肌和心脏中甘油三酯含量的影响。在体外,通过评估伊马替尼在基础和VEGF-B刺激条件下对荧光标记的FA摄取的影响,研究伊马替尼对人脐静脉内皮细胞(HUVEC)中脂肪酸转运的影响。
结果
伊马替尼可防止WD诱导的小鼠体重增加,且与食物摄入量无关。与此一致的是,伊马替尼增强了WD喂养小鼠中胰岛素介导的阻力动脉血管反应性。然而,伊马替尼不影响肌肉中的甘油三酯含量。在培养的内皮细胞中,VEGF-B刺激导致脂肪酸的时间依赖性摄取,同时Abl激酶底物Crk样蛋白(CrkL)在Tyr207处的磷酸化增加。尽管伊马替尼有效地阻止了VEGF-B介导的Abl激酶激活,但它对VEGF-B介导的内皮FA摄取没有影响。
结论
伊马替尼可防止WD喂养小鼠体重增加并保留胰岛素介导的血管舒张,但尽管抑制VEGF-B信号传导,却不影响内皮FA转运。伊马替尼对胰岛素介导的血管舒张的有益作用可能有助于其抗糖尿病作用。
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