Biorhythmic and receptor mediated interplay between melatonin and insulin: its consequences on diabetic erythrocytes

Adrita Banerjee, A. Chattopadhyay, D. Bandyopadhyay
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引用次数: 1

Abstract

Diabetes mellitus, one of the crucial epidemics of this country has snatched the sleep of mankind with a steep slope of 108 million in 1980 to more than 460 million in today’s world. The global statistics based on numerological information from World Health Organization (WHO) proposed alarmingly about 642 million affected individuals by 2040. Type 1 diabetes is due to damaged pancreatic β-cells while type 2 diabetes is a result of insulin insensitivity associated with hyperglycaemia. Hyperglycaemia is a principal symptom of diabetes. As a result, the circulatory erythrocytes [red blood cells (RBCs)] become the first and most vulnerable victims to confront such a stressful environment. The RBCs possess many components including haemoglobin, membrane proteins and lipids. They prefer to interact with glucose and form glycated haemoglobin and membrane phospholipid asymmetry which alters RBC adherence. These alterations trigger intracellular reactive oxygen species (ROS) formation and oxidative damage in diabetic erythrocytes. Melatonin, an indoleamine, ameliorates oxidative stress in various tissues and has the capacity of shielding erythrocytes from deleterious stress. A crucial relationship between melatonin and insulin indicates their interplay in occurrence of diabetes. Biorhythm entrained and receptor mediated action of melatonin on pancreatic β-cells in the context of hyperglycaemia are discussed for the first time in the review. Since melatonin protects against erythrocytes, as well as beneficial to diabetes, it is worthy to address proficiency of this indoleamine to the diabetic erythrocytes. In summary, this review has discussed the fostering role of melatonin in hyperglycaemia and encouraged further investigation related to the molecular pathways of melatonin on glucose metabolism. 
褪黑素和胰岛素之间的生物节律和受体介导的相互作用:其对糖尿病红细胞的影响
糖尿病,这个国家的主要流行病之一,夺走了人类的睡眠,从1980年的1.08亿急剧上升到今天的4.6亿多。基于世界卫生组织(世卫组织)数字学信息的全球统计表明,到2040年,受影响的人数将达到令人震惊的6.42亿人。1型糖尿病是由于胰腺β细胞受损,而2型糖尿病是胰岛素不敏感与高血糖相关的结果。高血糖是糖尿病的主要症状。因此,循环红细胞[红细胞(rbc)]成为面对这种压力环境的第一个也是最脆弱的受害者。红细胞含有许多成分,包括血红蛋白、膜蛋白和脂质。它们倾向于与葡萄糖相互作用,形成糖化血红蛋白和膜磷脂不对称,从而改变红细胞粘附性。这些改变触发细胞内活性氧(ROS)的形成和糖尿病红细胞的氧化损伤。褪黑素是一种吲哚胺,可以改善各种组织中的氧化应激,并具有保护红细胞免受有害应激的能力。褪黑激素和胰岛素之间的重要关系表明它们在糖尿病发生中的相互作用。本文首次讨论了在高血糖情况下褪黑素对胰腺β细胞的生物节律调控和受体介导作用。由于褪黑素对红细胞有保护作用,并且对糖尿病有益,因此值得解决这种吲哚胺对糖尿病红细胞的熟练程度。综上所述,本文讨论了褪黑素在高血糖中的促进作用,并鼓励进一步研究褪黑素对葡萄糖代谢的分子途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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