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线粒体 DNA 测序揭示了变异体和单倍群 M33a2'3 与印度男性低地高原肺水肿易感性的关联。

Mitochondrial DNA sequencing reveals association of variants and haplogroup M33a2'3 with High altitude pulmonary edema susceptibility in Indian male lowlanders.

机构信息

Defence Institute of Physiology and Allied Sciences, Timarpur, Delhi, 110054, India.

NIPER, Hyderabad, Balanagar, Hyderabad, 500037, India.

出版信息

Sci Rep. 2019 Jul 29;9(1):10975. doi: 10.1038/s41598-019-47500-1.

Abstract

High Altitude Pulmonary Edema (HAPE) is a threatening disorder caused due to acute exposure to high altitude above 3000 m. Apart from multiple factors involved, the genetic factors also play an important function in the pathogenesis of HAPE. This study aims to evaluate the role of mtDNA polymorphism and their association with haplogroup in understanding the etiology of HAPE. In this study, all the HAPE susceptible and acclimatized control subjects could be classified into nine haplogroups pertaining mostly to Macrohaplogroup M and U. The frequency of haplogroup M was significantly higher in HAPE susceptibles whereas the haplogroup M33a2'3 was found only in HAPE susceptibles. The variant G4491A and A4944G of MT-ND2, A14002G of MT-ND5, and C8562T of MT-ATP8, were definition site of haplogroup M33a2'3. The frequency of A10398G of MT-ND3, A8701G of MT-ATP6 and C14766T of MT-CYB genes were significantly higher in HAPE susceptibles. mtDNA copy number also plays a significant synergistic role in HAPE susceptibility. Our findings suggests that variants in MT-ND2 and MT-ND5 were predicted to confer decreased protein stability in HAPE susceptibles and in particular, highly conserved variants G4491A, A4944G and A14002G associated with haplogroup M33a2'3 may be the primary cause of susceptibility to HAPE in Indian male lowlanders.

摘要

高原肺水肿(HAPE)是一种由 3000 米以上的急性高原暴露引起的威胁性疾病。除了涉及多种因素外,遗传因素在 HAPE 的发病机制中也起着重要作用。本研究旨在评估 mtDNA 多态性及其与单倍群的关联在了解 HAPE 病因学中的作用。在这项研究中,所有的 HAPE 易感和适应对照组都可以分为主要属于巨单倍群 M 和 U 的九个单倍群。HAPE 易感者中 M 单倍群的频率明显更高,而 HAPE 易感者中只发现了 M33a2'3 单倍群。MT-ND2 的 G4491A 和 A4944G、MT-ND5 的 A14002G 和 MT-ATP8 的 C8562T 是 M33a2'3 单倍群的定义位点。MT-ND3 的 A10398G、MT-ATP6 的 A8701G 和 MT-CYB 基因的 C14766T 在 HAPE 易感者中的频率明显更高。mtDNA 拷贝数在 HAPE 易感性中也起着重要的协同作用。我们的研究结果表明,MT-ND2 和 MT-ND5 中的变异可能导致 HAPE 易感者中蛋白质稳定性降低,特别是与 M33a2'3 单倍群相关的高度保守变异 G4491A、A4944G 和 A14002G 可能是印度低地男性易感 HAPE 的主要原因。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d6a9/6662842/52e4b9bf7d52/41598_2019_47500_Fig1_HTML.jpg

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