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Plasma Proteomic Study in Pulmonary Arterial Hypertension Associated with Congenital Heart Diseases

机译:与先天性心脏病相关的肺动脉高血压血浆蛋白质组学研究

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Pulmonary arterial hypertension associated with congenital heart disease (CHD-PAH) has serious consequence and plasma protein profiles in CHD-PAH are unknown. We aimed to reveal the differential plasma proteins in 272 CHD patients with or without PAH. Various types of CHD-PAH were studied. Differential plasma proteins were first detected by iTRAQ proteomic technology and those with significant clinical relevance were selected for further ELISA validation in new cohort of patients. Among the 190 differential plasma proteins detected by iTRAQ, carbamoyl-phosphate synthetase I (CPSI, related to urea cycle and endogenous nitric oxide production) and complement factor H-related protein 2 (CFHR2, related to complement system and coagulant mechanism) were selected for further ELISA validation in new cohort of 152 patients. Both CPSI and CFHR2 were down-regulated with decreased plasma levels (p??0.01). Thus, we for the first time in CHD-PAH patients identified a large number of differential plasma proteins. The decreased CPSI expression in CHD-PAH patients may reveal a mechanism related to endogenous nitric oxide and the decrease of CFHR2 protein may demonstrate the deficiency of the immune system and coagulation mechanism. The findings may open a new direction for translational medicine in CHD-PAH with regard to the diagnosis and progress of the disease.
机译:与先天性心脏病(CHD-PAH)相关的肺动脉高血压在CHD-PAH中具有严重的后果和血浆蛋白质谱是未知的。我们的目标是揭示272例CHD患者的血管血浆蛋白,患者有或没有PAH。研究了各种类型的CHD-PAH。 ITRAQ蛋白质组学技术首先检测差分血浆蛋白,并选择具有显着性临床相关性的人进行患者新队列的ELISA验证。选择于ITRAQ检测到的190个差分血浆蛋白质中,选择了氨基甲酰基磷酸盐合成酶I(CPSI,与尿素循环和内源性一氧化氮产生相关)和补体因子H相关蛋白2(CFHR2,与补体系统和凝结剂机制相关)进一步的ELISA验证了152名患者的新队列。 CPSI和CFHR2都以降低的血浆水平降低(P?<?0.01)。因此,我们在CHD-PAH患者中首次鉴定了大量差异血浆蛋白。 CHD-PAH患者中的CPSI表达降低可能揭示与内源性一氧化氮有关的机制,CFHR2蛋白的降低可以证明免疫系统的缺乏和凝固机制。在疾病的诊断和进展方面,该研究结果可能在CHD-PAH中开辟了翻译医学的新方向。

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