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ROCK2 and MYLK variants under hypobaric hypoxic environment of high altitude associate with high altitude pulmonary edema and adaptation

机译:高原低压缺氧环境下的ROCK2和MYLK变异与高原肺水肿和适应有关

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Objective: To date, a major class of kinases, serine–threonine kinase, has been scantly investigated in stress-induced rare, fatal (if not treated early), and morbid disorder, high altitude pulmonary edema (HAPE). This study examined three major serine–threonine kinases, ROCK2, MYLK, and JNK1, along with six other genes, tyrosine hydroxylase, G-protein subunits GNA11 and GNB3, and alpha1 adrenergic receptor isoforms 1A, 1B, and 1D as candidate gene markers of HAPE and adaptation.Methods: For this, 57 variants across these nine genes were genotyped in HAPE patients (n=225), HAPE controls (n=210), and highlanders (n=259) by Sequenom MS (TOF)-based MassARRAY? platform using iPLEX? Gold technology. In addition, to study the gene expression, quantitative real-time polymerase chain reaction was performed in human peripheral blood mononuclear cells of the three study groups.Results: A significant association was observed for C allele (ROCK2 single-nucleotide polymorphism, rs10929728) with HAPE (P=0.03) and C, T, and A alleles (MYLK single-nucleotide polymorphisms, rs11717814, rs40305, and rs820336) with both HAPE and adaptation (P=0.001, P=0.006, and P=0.02, respectively). ROCK2 88 kb GGGTTGGT haplotype was associated with lower risk of HAPE (P=0.0009). MYLK 7 kb haplotype CTA, composed of variant alleles, was associated with higher risk of HAPE (P=0.0006) and lower association with adaptation (P=1E–06), whereas haplotype GCG, composed of wild-type alleles, was associated with lower risk of HAPE (P=0.001) and higher association with adaptation (P=1E–06). Haplotype–haplotype and gene–gene interactions demonstrated a correlation in working of ROCK2 and MYLK.Conclusion: The data suggest the association of ROCK2 with HAPE and MYLK with HAPE and adaptation in Indian population. The outcome has provided new insights into the physiology of HAPE and adaptation.
机译:目的:迄今为止,在应激引起的罕见,致命(如果不及早治疗)和病态疾病,高原肺水肿(HAPE)方面,尚未对主要的丝氨酸-苏氨酸激酶进行过研究。这项研究检查了三种主要的丝氨酸-苏氨酸激酶ROCK2,MYLK和JNK1,以及其他六个基因酪氨酸羟化酶,G蛋白亚基GNA11和GNB3以及α1肾上腺素能受体亚型1A,1B和1D作为其候选基因标记方法:为此,通过基于Sequenom MS(TOF)的MassARRAY对HAPE患者(n = 225),HAPE对照(n = 210)和汉兰达(n = 259)的这9个基因中的57个变异体进行了基因分型。 ?平台使用iPLEX?黄金技术。此外,为了研究基因表达,在三个研究组的人外周血单个核细胞中进行了实时定量聚合酶链反应。结果:观察到C等位基因(ROCK2单核苷酸多态性,rs10929728)与具有HAPE和适应性的HAPE(P = 0.03)和C,T和A等位基因(MYLK单核苷酸多态性,rs11717814,rs40305和rs820336)(分别为P = 0.001,P = 0.006和P = 0.02)。 ROCK2 88 kb GGGTTGGT单倍型与较低的HAPE风险相关(P = 0.0009)。由变异等位基因组成的MYLK 7 kb单倍型CTA与HAPE的风险较高(P = 0.0006)和与适应的关联性较低(P = 1E-06),而由野生型等位基因组成的单倍型GCG与HAPE的风险较低(P = 0.001),与适应的相关性较高(P = 1E-06)。单倍型-单倍型和基因-基因的相互作用证明了ROCK2和MYLK在工作中的相关性。结论:数据表明ROCK2与HAPE的关联以及MYLK与HAPE的关联以及印度人群的适应性。结果为HAPE和适应的生理学提供了新的见解。

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