首页> 美国卫生研究院文献>The Journal of Neurology and Psychopathology >Susceptibility to diabetic neuropathy in patients with insulindependent diabetes mellitus is associated with a polymorphism at the 5end of the aldose reductase gene
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Susceptibility to diabetic neuropathy in patients with insulindependent diabetes mellitus is associated with a polymorphism at the 5end of the aldose reductase gene

机译:胰岛素患者对糖尿病神经病变的敏感性依赖型糖尿病与5端的多态性有关醛糖还原酶基因的末端

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摘要

OBJECTIVES—There is evidence that the polyol pathway is involved in the pathogenesis of diabetic neuropathy. Aldose reductase (ALR2) is the first and rate limiting enzyme of this pathway and recent studies have suggested that polymorphisms in and around the gene are associated with the development of diabetic microvascular disease. The aim was to examine the role of ALR2 in the susceptibility to diabetic neuropathy in patients with insulin dependent diabetes mellitus (IDDM).
METHODS—One hundred and fifty nine British white patients with IDDM and 102 normal healthy controls were studied using the polymerase chain reaction to test for a highly polymorphic microsatellite marker 2.1 kilobase (kb) upstream of the initiation site of the ALR2 gene.
RESULTS—Seven alleles were detected (Z-6, Z-4, Z-2, Z, Z+2, Z+4, and Z+6). There was a highly significant decrease in the frequency of the Z+2 allele in those patients with overt neuropathy compared with those with no neuropathy after 20 years duration of diabetes (14.1% v 38.2%, χ2 =17.3, p<0.00001). A similar difference was also found between the neuropathy group and those patients who have had diabetes for< five years with no overt neuropathy (14.1% v 30.2%, χ2=9.0, p<0.0025). The neuropathy group also had a significant decrease in thefrequency of the Z/Z+2 genotype compared with those patients who haveno neuropathy after 20 years duration of diabetes (14.0% v 44.7%, χ2=13.0, p<0.0005).
CONCLUSION—These results suggest that the aldosereductase gene is intimately involved in the pathogenesis of diabetic neuropathy.

机译:目的—有证据表明多元醇途径与糖尿病性神经病的发病机理有关。醛糖还原酶(ALR2)是该途径的第一个酶和限速酶,最近的研究表明该基因及其周围的多态性与糖尿病微血管疾病的发展有关。目的是研究ALR2在胰岛素依赖型糖尿病(IDDM)患者对糖尿病性神经病的敏感性中的作用。
方法-研究159例英国IDDM白人患者和102位正常健康对照者聚合酶链反应以检测高度多态的微卫星标记,该标记位于ALR2基因起始位点上游2.1 kb。
结果-检测到七个等位基因(Z-6,Z-4,Z-2, Z,Z + 2,Z + 4和Z + 6)。伴有神经病的患者在糖尿病持续20年后,Z + 2等位基因的频率与无神经病的患者相比有显着降低(14.1%v 38.2%,χ 2 = 17.3,p <0.00001)。在神经病变组和患有五年以下糖尿病且无明显神经病变的患者之间也发现了类似的差异(14.1%vs 30.2%,χ 2 = 9.0,p <0.0025)。神经病组也有明显的减少Z / Z + 2基因型的频率与那些糖尿病20年后无神经病变(14.0%v 44.7%,χ 2 = 13.0,p <0.0005)。
结论—这些结果表明醛糖还原酶基因与糖尿病性神经病的发病机制密切相关。

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