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Functional Analysis of Thyroid Peroxidase Gene Mutations Detected in Patients with Thyroid Dyshormonogenesis

机译:甲状腺失育血管发生患者检测到甲状腺过氧化物酶基因突变的功能分析

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摘要

Thyroid peroxidase (TPO) is the key enzyme in the biosynthesis of thyroid hormones. We aimed to identify the spectrum of mutations in the TPO gene leading to hypothyroidism in the population of West Bengal to establish the genetic etiology of the disease. 200 hypothyroid patients (case) and their corresponding sex and age matched 200 normal individuals (control) were screened depending on their clinical manifestations. Genomic DNA was isolated from peripheral blood samples and TPO gene (Exon 7 to Exon 14) was amplified by PCR. The PCR products were subjected to sequencing to identify mutations. Single nucleotide changes such as Glu 641 Lys, Asp 668 Asn, Thr 725 Pro, Asp 620 Asn, Ser 398 Thr, and Ala 373 Ser were found. Changes in the TPO were assayed in vitro to compare mutant and wild-type activities. Five mutants were enzymatically inactive in the guaiacol and iodide assays. This is a strong indication that the mutations are present at crucial positions of the TPO gene, resulting in inactivated TPO. The results of this study may help to develop a genetic screening protocol for goiter and hypothyroidism in the population of West Bengal.
机译:甲状腺过氧化物酶(TPO)是甲状腺激素生物合成中的关键酶。我们旨在鉴定TPO基因中突变的谱,导致西孟加拉邦群中的甲状腺功能亢进,建立疾病的遗传病因。 200甲状腺功能率患者(病例)及其相应的性别和年龄匹配的200个正常个体(对照)根据其临床表现筛选。从外周血样品中分离基因组DNA,通过PCR扩增TPO基因(外显子7到外显子14)。对PCR产物进行测序以鉴定突变。发现单核苷酸诸如Glu 641 Lys,ASP 668Asn,Thr 725 Pro,ASP 620ASN,SER 398 THR和ALA 373 Ser。在体外测定TPO的变化以比较突变体和野生型活动。在GuaiaIacol和碘化物测定中酶促酶活性酶活性。这是强烈的指示,突变存在于TPO基因的关键位置,导致灭活的TPO。该研究的结果可能有助于为西孟加拉科人群进行甲状腺肿和甲状腺功能亢进的遗传筛查方案。

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