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糖尿病、高血压与衰老:衰老及心血管代谢疾病的离子假说

Diabetes mellitus, hypertension and ageing: the ionic hypothesis of ageing and cardiovascular-metabolic diseases.

作者信息

Barbagallo M, Resnick L M, Dominguez L J, Licata G

机构信息

Chair of Geriatrics, University of Palermo, Italy.

出版信息

Diabetes Metab. 1997 Sep;23(4):281-94.

PMID:9342541
Abstract

Ageing in industrialised societies is associated with an increasing prevalence of hypertension, atherosclerotic vascular diseases, reduced insulin sensitivity and non-insulin-dependent diabetes mellitus (NIDDM). It has been suggested that hyperinsulinaemia/insulin resistance and/or hyperglycaemia could play a role in determining and/or exacerbating the hypertension and vascular disease associated with diabetes mellitus and ageing. Insulin-resistant states, such as essential hypertension and NIDDM, as well as "normal" ageing, are characterised by similar intracellular ionic defects, i.e. accumulation of cytosolic free calcium and depletion of free magnesium. The importance of calcium and magnesium ions in regulating cell functions is well-known. A rise in cellular free calcium and a depletion in cellular magnesium may induce cellular insulin resistance and vasoconstriction. Ionic levels quantitatively predict the extent of elevated blood pressure, fasting blood glucose, HBA1c and hyperinsulinaemic response to oral glucose challenge. We suggest that ionic disturbance might be the missing link responsible for the frequent clinical coexistence of hypertension, atherosclerosis and metabolic disorders. Ageing cells may become more vulnerable to ion disturbances, leading to possible elevation of intracellular free calcium and concurrent magnesium depletion. The "ionic hypothesis" of ageing supposes that an alteration in the cellular mechanisms which maintain the homeostasis of cytosolic calcium concentrations may play a key role in the ageing process, and that a sustained accumulation of cellular calcium and/or the depletion of cellular magnesium may also provide the final common pathway for many ageing-associated diseases, including hypertension and NIDDM.

摘要

在工业化社会中,衰老与高血压、动脉粥样硬化性血管疾病的患病率上升、胰岛素敏感性降低以及非胰岛素依赖型糖尿病(NIDDM)有关。有人提出,高胰岛素血症/胰岛素抵抗和/或高血糖可能在决定和/或加剧与糖尿病和衰老相关的高血压和血管疾病中起作用。胰岛素抵抗状态,如原发性高血压和NIDDM,以及“正常”衰老,都具有相似的细胞内离子缺陷,即胞质游离钙积累和游离镁耗竭。钙和镁离子在调节细胞功能中的重要性是众所周知的。细胞游离钙升高和细胞镁耗竭可能会诱导细胞胰岛素抵抗和血管收缩。离子水平可以定量预测血压升高、空腹血糖、糖化血红蛋白(HBA1c)以及口服葡萄糖激发试验后的高胰岛素血症反应程度。我们认为离子紊乱可能是导致高血压、动脉粥样硬化和代谢紊乱在临床上频繁共存的缺失环节。衰老细胞可能更容易受到离子紊乱的影响,导致细胞内游离钙可能升高以及同时出现镁耗竭。衰老的“离子假说”认为,维持胞质钙浓度稳态的细胞机制发生改变可能在衰老过程中起关键作用,并且细胞钙的持续积累和/或细胞镁的耗竭也可能为许多与衰老相关的疾病,包括高血压和NIDDM,提供最终的共同途径。

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