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Implementation of a Congenital Hypothyroidism Newborn Screening Procedure with Mutation Detection on Genomic DNA Extracted from Blood Spots: The Experience of the Italian Northeastern Reference Center

机译:先天性甲状腺功能减退症新生儿筛查程序的实施与突变检测从血斑中提取的基因组DNA:意大利东北参考中心的经验。

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After a couple of decades from the institution of nationwide congenital hypothyroidism (CH) newborn screening program, the first generation properly treated is now displaying normal reproductive rate and the causative molecular defects are spreading from one generation to the next. In the present study we propose a method of detection of mutations in the thyrotropin receptor (TSHR) and in the paired box 8 (PAX8) genes that have been proved to be responsible for some forms of CH. The method, carried out by means of denaturing high-performance liquid chromatography (DHPLC) followed by direct sequencing, takes advantage of the CH newborn screening procedure, because genomic DNA for the analysis is extracted from the same blood spot collected for recall confirmation. Among 16 hypothyroid newborns with thyroid hypoplasia born between January 1999 and April 2005 in northeastern Italy, three heterozygous causative mutations in the TSHR gene were evidenced, whereas the analysis of the PAX8 gene revealed an unknown heterozygous substitution that could interfere with the start of transcription.
机译:在全国范围的先天性甲状腺功能减退症(CH)新生儿筛查计划实施后的几十年中,经过适当治疗的第一代患者现在显示出正常的生殖率,并且致病性分子缺陷正从另一代人蔓延到下一代。在本研究中,我们提出了一种检测促甲状腺激素受体(TSHR)和成对框8(PAX8)基因突变的方法,这些基因已被证明可导致某些形式的CH。通过变性高效液相色谱(DHPLC)然后直接测序进行的方法利用了CH新生儿筛查程序的优势,因为用于分析的基因组DNA是从收集的相同血斑中提取的,以进行召回确认。在意大利东北部于1999年1月至2005年4月之间出生的16例甲状腺功能低下的甲状腺发育不足的新生儿中,TSHR基因中出现了3个杂合性致病突变,而对PAX8基因的分析表明存在未知的杂合替代,可能会干扰转录的开始。

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