首页> 美国卫生研究院文献>Journal of Translational Medicine >Future detection and monitoring of diabetes may entail analysis of both β-cell function and volume: How markers of β-cell loss may assist
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Future detection and monitoring of diabetes may entail analysis of both β-cell function and volume: How markers of β-cell loss may assist

机译:未来对糖尿病的检测和监测可能需要对β细胞功能和体积进行分析:β细胞丢失的标志物如何帮助

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摘要

Disease heterogeneity is as major issue in Type II Diabetes Mellitus (T2DM), and this patient inter-variability might not be sufficiently reflected by measurements of glycated haemoglobin (HbA1c).Β-cell dysfunction and β-cell death are initiating factors in development of T2DM. In fact, β-cells are known vanish prior to the development of T2DM, and autopsy of overt T2DM patients have shown a 60% reduction in β-cell mass.As the decline in β-cell function and mass have been proven to be pathological traits in T2DM, methods for evaluating β-cell loss is becoming of more interest. However, evaluation of β-cell death or loss is currently invasive and unattainable for the vast majority of diabetes patients. Serological markers, reflecting β-cell loss would be advantageous to detect and monitor progression of T2DM. Biomarkers with such capacities could be neo-epitopes of proteins with high β-cell specificity containing post translational modifications. Such tools may segregate T2DM patients into more appropriate treatment groups, based on their β-cell status, which is currently not possible. Presently individuals presenting with adequately elevated levels of both insulin and glucose are classified as T2DM patients, while an important subdivision of those is pending, namely those patients with sufficient β-cell capacity and those without. This may warrant two very different treatment options and patient care paths.Serological biomarkers reflecting β-cell health status may also assist development of new drugs for T2DM and aid physicians in better characterization of individual patients and tailor individual treatments and patient care protocols.
机译:疾病异质性是II型糖尿病(T2DM)的主要问题,该患者之间的变异性可能无法通过糖化血红蛋白(HbA1c)的测量得到充分反映。Β细胞功能障碍和β细胞死亡是糖尿病发展的起始因素。 T2DM。实际上,已知β细胞在T2DM发生之前就已经消失了,而且明显的T2DM患者的尸检显示β细胞质量减少了60%,因为β细胞功能和质量的下降已被证明是病理性的在T2DM的性状中,用于评估β细胞损失的方法变得越来越受关注。但是,目前对于大多数糖尿病患者而言,β细胞死亡或丢失的评估是侵入性的,无法实现。反映β细胞丢失的血清学标志物将有利于检测和监测T2DM的进展。具有这种能力的生物标记物可以是具有高β-细胞特异性的蛋白质的新表位,其包含翻译后修饰。此类工具可以根据T2DM患者的β细胞状态将其分为更合适的治疗组,目前尚无法实现。目前,胰岛素和葡萄糖水平都充分升高的患者被归类为T2DM患者,而这些患者的重要细分仍在等待中,即具有足够的β细胞功能的患者和没有β细胞功能的患者。这可能需要两种截然不同的治疗选择和患者护理途径。反映β细胞健康状况的血清生物标志物也可能有助于开发用于T2DM的新药,并帮助医生更好地表征个体患者并制定个体化治疗方法和患者护理方案。

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