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母体端粒酶逆转录酶变体与早产和早产胎膜早破有关。

Maternal human telomerase reverse transcriptase variants are associated with preterm labor and preterm premature rupture of membranes.

机构信息

The University of Texas Medical Branch, Division of Maternal-Fetal Medicine, Galveston TX, United States of America.

Geisel School of Medicine, Dartmouth College, Hanover NH, United States of America.

出版信息

PLoS One. 2018 May 17;13(5):e0195963. doi: 10.1371/journal.pone.0195963. eCollection 2018.

DOI:10.1371/journal.pone.0195963
PMID:29771920
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5957404/
Abstract

OBJECTIVE

Premature aging and short telomere lengths of fetal tissues are associated with spontaneous preterm labor (PTL) and preterm premature rupture of membranes (pPROM). Maintenance of telomere length is performed by the enzyme telomerase. Human telomerase reverse transcriptase (hTERT) is a subunit of telomerase, and its dysfunction affects telomere shortening. This study assessed whether maternal or fetal genetic variations in the hTERT gene are associated with PTL or pPROM.

METHODS

A case (PTL or pPROM) control (term birth) genetic association study was conducted in 654 non-Hispanic white mothers (438 term, 162 PTL, 54 pPROM) and 502 non-Hispanic white newborns (346 term, 116 PTB, 40 pPROM). Maternal and fetal DNA samples were genotyped for 23 single nucleotide polymorphisms (SNPs) within the hTERT gene. Allele frequencies were compared between cases and controls, stratified by PTL and pPROM. Maternal and fetal data were analyzed separately.

RESULTS

Allelic differences in one SNP of hTERT (rs2853690) were significantly associated with both PTL (adjusted OR 2.24, 95%CI 1.64-3.06, p = 2.32e-05) and with pPROM (adjusted OR 7.54, 95%CI 3.96-14.33, p = 2.39e-07) in maternal DNA. There was no significant association between the hTERT SNPs analyzed and PTL or pPROM in the fetal samples.

CONCLUSION

hTERT polymorphisms in fetal DNA do not associate with PTL or pPROM risk; however, maternal genetic variations in hTERT may play a contributory role in risk of PTL and PPROM.

摘要

目的

胎儿组织的过早衰老和端粒长度缩短与自发性早产(PTL)和早产胎膜早破(pPROM)有关。端粒长度的维持是通过端粒酶完成的。人端粒酶逆转录酶(hTERT)是端粒酶的一个亚单位,其功能障碍会影响端粒缩短。本研究评估 hTERT 基因的母体或胎儿遗传变异是否与 PTL 或 pPROM 相关。

方法

对 654 名非西班牙裔白人母亲(438 名足月,162 名 PTL,54 名 pPROM)和 502 名非西班牙裔白人新生儿(346 名足月,116 名 PTB,40 名 pPROM)进行了病例对照(足月分娩)遗传关联研究。对 hTERT 基因内的 23 个单核苷酸多态性(SNP)进行了母体和胎儿 DNA 分型。在 PTL 和 pPROM 分层的情况下,比较病例和对照组之间的等位基因频率。分别分析母体和胎儿数据。

结果

hTERT 基因中的一个 SNP(rs2853690)的等位基因差异与 PTL(调整后的 OR 2.24,95%CI 1.64-3.06,p = 2.32e-05)和 pPROM(调整后的 OR 7.54,95%CI 3.96-14.33,p = 2.39e-07)均显著相关。在胎儿样本中,分析的 hTERT SNPs 与 PTL 或 pPROM 之间没有显著关联。

结论

胎儿 DNA 中的 hTERT 多态性与 PTL 或 pPROM 风险无关;然而,hTERT 的母体遗传变异可能在 PTL 和 pPROM 风险中起作用。

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