Co-expression of urotensin II and its receptor (GPR14) in human cardiovascular and renal tissues

尾加压素Ⅱ 内科学 自分泌信号 内分泌学 肾功能 受体 旁分泌信号 医学 肌酐 泌尿系统 尿 生物
作者
Mika Matsushita,Masayoshi Shichiri,Taihei Imai,Masatora Iwashina,Hiroyuki Tanaka,Nobuyuki Takasu,Yukio Hirata
出处
期刊:Journal of Hypertension [Ovid Technologies (Wolters Kluwer)]
卷期号:19 (12): 2185-2190 被引量:239
标识
DOI:10.1097/00004872-200112000-00011
摘要

Background Urotensin-II (UII), a cyclic dodecapeptide originally isolated from fish urophysis that has potent cardiovascular effects, has recently been identified as an endogenous ligand for the orphan G protein-coupled receptor, GPR14. The physiological roles of endogenous UII and its receptor in humans remain unknown. Objective To investigate the presence of human (h) UII-like immunoreactivity (hUII-LI) in human biological fluids, and the expression of hUII and GPR14 genes in human tissues. Methods We have established a specific radioimmunoassay for hUII and the real-time quantitative reverse transcriptase polymerase chain reaction method using LightCycler for the quantification of hUII and GPR14 mRNAs. Results Gel filtration and reverse-phase high performance liquid chromatography of human urine extracts revealed a single major peak of hUII-LI co-eluting with known hUII. The concentrations of hUII-LI in urine from normal individuals were 7.4 ± 0.9 μg/g creatinine, whereas its plasma concentration was undetectable (< 50 pg/ml). Urinary hUII concentrations from patients with essential hypertension and those with renal tubular abnormality, but not with glomerular diseases, were significantly greater than those from normal individuals. The resulting fractional excretion of hUII, exceeding the glomerular filtration rate, suggests a renal origin of urinary UII-LI. hUII mRNAs were abundantly expressed in the kidney and the right atrium, but far less so in the vasculature, whereas GPR14 mRNAs were equally and abundantly expressed in both cardiovascular and renal tissues. Conclusions These data suggest that urinary hUII is derived mainly from a renal source, and that hUII functions as an autocrine/paracrine vasoactive factor not only in the cardiovascular system, but also in the kidney, with an as yet unspecified function.

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