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首页> 外文期刊>Scientific reports. >Targeting erythrocyte carbonic anhydrase and 18O-isotope of breath CO2 for sorting out type 1 and type 2 diabetes
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Targeting erythrocyte carbonic anhydrase and 18O-isotope of breath CO2 for sorting out type 1 and type 2 diabetes

机译:针对红细胞碳酸酐酶和18O-同位素的呼吸二氧化碳,用于分类1型和2型糖尿病

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The inability to envisage the acute onset and progression of type 1 diabetes (T1D) has been a major clinical stumbling block and an important area of biomedical research over the last few decades. Therefore there is a pressing need to develop a new and an effective strategy for early detection of T1D and to precisely distinguish T1D from type 2 diabetes (T2D). Here we describe the precise role of the enzymatic activity of carbonic anhydrase (CA) in erythrocytes in the pathogenesis of T1D and T2D. We show that CA activities are markedly altered during metabolism of T1D and T2D and this facilitates to the oxygen-18 ((18)O) isotopic fractionations of breath CO2. In our observations, T1D exhibited considerable depletions of (18)O-isotopes of CO2, whereas T2D manifested isotopic enrichments of (18)O in breath CO2, thus unveiling a missing link of breath(18)O-isotopic fractionations in T1D and T2D. Our findings suggest that the alterations in erythrocytes CA activities may be the initial step of altered metabolism of T1D and T2D, and breath (18)O-isotope regulated by the CA activity is a potential diagnostic biomarker that can selectively and precisely distinguish T1D from T2D and thus may open a potential unifying strategy for treating these diseases.
机译:无法设想1型糖尿病(T1D)的急性发作和进展是在过去几十年中的主要临床绊脚石和生物医学研究的重要领域。因此,需要一种需要开发一种新的和有效的早期检测T1D的有效策略,并精确地区分T1D型糖尿病(T2D)。在这里,我们描述了碳酸酐酶(CA)在T1D和T2D发病机制中红细胞酶活性的精确作用。我们表明,在T1D和T2D的新陈代谢期间,CA活性明显改变,这有利于氧气-18((18)o)呼吸二氧化碳的同位素分级。在我们的观察中,T1D表现出相当大的耗尽二氧化碳的(18)O-同位素,而T2D表现出(18)o在呼吸二氧化碳中的同位素富集,从而揭示T1D和T2D中的缺失的呼吸链路(18)o-同位素分级。我们的研究结果表明,红细胞Ca活性的改变可能是改变T1D和T2D的代谢改变的初始步骤,并且通过CA活性调节的呼气(18)O-同位素是潜在的诊断生物标志物,可以选择性,精确地区分T2D的潜在诊断生物标志物因此,可以开辟治疗这些疾病的潜在统一策略。

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