抗原加工基因1密码子333和密码子637多态性相关的转运体与原发性开角型青光眼相关。

Molecular diagnosis : a journal devoted to the understanding of human disease through the clinical application of molecular biology Pub Date : 2004-01-01 DOI:10.1007/BF03260069

Hui-Ju Lin, Chang Hai Tsai, Fuu-Jen Tsai, Wen-Chi Chen, Huey-Yi Chen, Seng-Sheen Fan

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引用次数: 9

摘要

免疫系统中的遗传因素被广泛怀疑在青光眼的病因中起作用。在这项研究中，我们评估了原发性开角型青光眼(POAG)与抗原加工相关转运体(TAP)基因多态性之间的关系。我们评估的TAP基因多态性为TAP1-1密码子333 A/G (Ile-Val)、TAP1-2密码子637 (Asp-Gly)、TAP2-1密码子379 (Val-Ile)、TAP2-2密码子665 (Thr-Ala)和密码子687 (Stop-Gln)以及TAP2-3密码子565 (Ala-Tht)。由于青光眼缺乏预测指标，许多青光眼患者只有在其视力和视野出现不可逆转的恶化时才被诊断出来。我们的目的是确认TAP1和TAP2基因是否可以用来识别青光眼的易感性。方法:选取66例POAG患者和105名健康志愿者进行病例对照研究。我们通过pcr分析确定了TAP1和TAP2基因的多态性。结果:POAG患者与健康对照组TAP1-1密码子333和TAP1-2密码子637基因多态性分布差异有统计学意义(p分别为0.0375和0.01)。而TAP2-1密码子370、TAP2-2密码子665和TAP2-3密码子565在两组间差异无统计学意义(p分别为0.273、0.19和0.131)。在TAP1-1密码子333中，“GG”纯合子与“GA”杂合子差异显著(OR为4.32;95% ci 1.336, 13.969)。在TAP1-2密码子637中，“GG”纯合子与“GA”杂合子存在显著差异(OR 15;95% ci 1.733, 129.860)。“GG”纯合子与“AA”纯合子的比值也有显著差异(OR 10.8;95% ci 1.286, 91.880)。因此，TAP1-1密码子333和TAP1-2密码子637基因多态性是POAG有用的遗传标记。在POAG患者和健康对照组之间，TAP1-2“GG”纯合子的患病率存在显著差异，尽管在TAP基因的等位基因上，两组之间没有显著差异。结论:免疫系统扮演仲裁者的角色，帮助决定神经细胞在压力下是存活下来，还是因损伤而牺牲自己。TAP1-1和TAP1-2在免疫系统中发挥重要作用。TAP1-1和TAP1-2基因多态性可能通过转录后改变和基因表达调控的改变，参与免疫系统参与POAG的发生。

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Transporter associated with antigen processing gene 1 codon 333 and codon 637 polymorphisms are associated with primary open-angle glaucoma.

Introduction: Genetic factors in the immune system are widely suspected to have a role in the etiology of glaucoma. In this study, we evaluated the association between primary open-angle glaucoma (POAG) and the transporter associated with antigen processing (TAP) gene polymorphisms. The TAP gene polymorphisms we evaluated were TAP1-1 codon 333 A/G (Ile-Val), TAP1-2 codon 637 (Asp-Gly), TAP2-1 codon 379 (Val-Ile), TAP2-2 codon 665 (Thr-Ala) and codon 687 (Stop-Gln), and TAP2-3 codon 565 (Ala-Tht). Due to the lack of predictive markers for glaucoma, many glaucoma patients are only diagnosed when their visual acuity and visual field has irreversibly deteriorated. Our aim was to confirm whether or not the TAP1 and TAP2 genes can be used to identify suspectability to glaucoma.

Methods: Sixty-six patients with POAG and 105 healthy volunteers were enrolled in this case-control study. We resolved the TAP1 and TAP2 gene polymorphisms by PCR-based analysis.

Results: There was a significant difference in the distribution of TAP1-1 codon 333 and TAP1-2 codon 637 gene polymorphisms (p = 0.0375 and 0.01, respectively) between POAG patients and healthy controls. However, there was no significant difference between the two groups in TAP2-1 codon 370, TAP2-2 codon 665, and TAP2-3 codon 565 (p = 0.273, 0.19, and 0.131, respectively). In TAP1-1 codon 333, there was a significant difference between the "GG" homozygote and "GA" heterozygote (OR 4.32; 95% CI 1.336, 13.969). In TAP1-2 codon 637, there was a significant difference between the "GG" homozygote and "GA" heterozygote (OR 15; 95% CI 1.733, 129.860). There was also a significant difference between "GG" homozygote and "AA" homozygote (OR 10.8; 95% CI 1.286, 91.880). Therefore, TAP1-1 codon 333 and TAP1-2 codon 637 gene polymorphisms were useful genetic markers of POAG. The prevalence of the TAP1-2 "GG" homozygote differs significantly between POAG patients and healthy controls, although in the alleles of the both TAP genes, there were no significant differences between the two groups.

Conclusion: The immune system acts as an arbiter to help determine whether under stress a neuronal cell will survive or sacrifice itself to injuries. TAP1-1 and TAP1-2 play an important role in the immune system. TAP1-1 and TAP1-2 gene polymorphisms may, by way of post-transcriptional changes and altered regulation of gene expression, be involve the immune system in the development of POAG.

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Molecular diagnosis : a journal devoted to the understanding of human disease through the clinical application of molecular biology

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