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首页> 外文期刊>Saudi Pharmaceutical Journal >A study of the role of DIO1 and DIO2 polymorphism in thyroid cancer and drug response to therapy in the Saudi population
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A study of the role of DIO1 and DIO2 polymorphism in thyroid cancer and drug response to therapy in the Saudi population

机译:DIO1和DIO2基因多态性在甲状腺癌中的作用以及沙特人群对治疗的药物反应的研究

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Background Deiodinases comprise a group of selenoproteins that regulate the bioavailability of active thyroid hormones (TH) in a time and tissue specific fashion. They increase the hormonal activity by metabolizing their inactive precursors to active forms or terminate their activity by deactivating active hormones. The role of the deiodinase ( DIO ) gene polymorphisms in thyroid cancer is not fully understood yet. This study evaluated the potential association of the DIO1 and DIO2 genes with differentiated thyroid cancer and differential thyroxine dose requirement in thyroidectomized patients in a Saudi cohort. Methods We selected four variants (one DIO1 and three DIO2 ) for the association studies using Taqman assays in 507 DTC patients undergoing treatment with thyroxin against 560 disease-free individual, all of Saudi Arab origin. Results None of the studied variants was linked to differentiated thyroid cancer. The rs1388378_G??T was initially linked to thyroxine dose requirement (p?=?0.035) when all patients were considered together, but this association was lost when the patients were classified into either near suppressed (0.1?≤?TSH??0.5) or suppressed (TSH??0.1) TSH group. Discussion Although the results suggest only a weak relationship with differentiated thyroid cancer, they strongly indicate that the DIO2 polymorphism influences the hormonal dose requirement in patients undergoing treatment with thyroxine. This probably points to a distinction in the way this gene influences disease as compared to therapy thereof.
机译:背景脱碘酶包括一组硒蛋白,这些硒蛋白以时间和组织特异性方式调节活性甲状腺激素(TH)的生物利用度。它们通过将非活性前体代谢为活性形式来增加激素活性,或者通过使活性激素失活来终止其活性。脱碘酶(DIO)基因多态性在甲状腺癌中的作用尚未完全了解。这项研究评估了沙特队列中经甲状腺切除的患者中DIO1和DIO2基因与分化型甲状腺癌和甲状腺素剂量不同需求之间的潜在联系。方法我们采用Taqman分析法,针对560名接受沙特阿拉伯治疗的DTC患者,针对560名无沙特阿拉伯血统的无病个体选择了四个变体(一个DIO1和三个DIO2)进行关联研究。结果研究的变体均未与分化型甲状腺癌相关。当所有患者一起考虑时,rs1388378_G?>ΔT最初与甲状腺素剂量需求有关(p?=?0.035),但是当患者被分类为接近抑制(0.1?≤?TSH?<?)时,这种联系就消失了。 0.5)或抑制(TSH 0.1)的TSH组。讨论尽管结果表明与分化型甲状腺癌的关系较弱,但它们强烈表明DIO2多态性会影响接受甲状腺素治疗的患者的激素剂量需求。与它的治疗相比,这可能表明该基因影响疾病的方式有所不同。

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