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Oligomerization of recombinant and endogenously expressed human histamine H4 receptors.

机译:重组和内源表达的人类组胺H4受体的寡聚化。

摘要

In this study, we report the homo- and hetero-oligomerization of the human histamine H4R by both biochemical (Western blot and immobilized metal affinity chromatography) and biophysical [bioluminescence resonance energy transfer and time-resolved fluorescence resonance energy transfer (tr-FRET)] techniques. The H4R receptor is the most recently discovered member of the histamine family of G-protein-coupled receptors. Using specific polyclonal antibodies raised against the C-terminal tail of the H4R, we demonstrate the presence of H4R oligomers in human embryonic kidney 293 and COS-7 cells heterologously overexpressing H4Rs and putative native H4R oligomers in human phytohaemagglutinin blasts endogenously expressing H4Rs. Moreover, we show that H4R homo-oligomers are formed constitutively, are formed at low receptor densities (300 fmol/mg of protein), and are present at the cell surface, as detected by tr-FRET. The formation of these oligomers is independent of N-glycosylation and is not modulated by H4R ligands, covering the full spectrum of agonists, neutral antagonists, and inverse agonists. Although we show H4R homo-oligomer formation at physiological expression levels, the detection of H1R-H4R hetero-oligomers was achieved only at higher H1R expression levels and are most likely not physiologically relevant.
机译:在这项研究中,我们通过生化(Western印迹和固定化金属亲和色谱)和生物物理[生物发光共振能量转移和时间分辨荧光共振能量转移(tr-FRET))报告了人类组胺H4R的均聚和杂聚]技术。 H4R受体是G蛋白偶联受体的组胺家族中最新发现的成员。使用针对H4R C末端尾巴的特异性多克隆抗体,我们证明了人类胚胎肾293和COS-7细胞中H4R寡聚体的存在异源过表达H4Rs,而在人类植物血凝素胚芽细胞中内源表达H4Rs的推定天然H4R寡聚体。此外,我们显示,通过tr-FRET检测,H4R均聚物是组成性形成的,以低受体密度(300 fmol / mg蛋白质)形成,并存在于细胞表面。这些低聚物的形成与N-糖基化无关,并且不受H4R配体的调节,涵盖了激动剂,中性拮抗剂和反向激动剂的全部范围。尽管我们在生理表达水平上显示了H4R同源寡聚体的形成,但仅在更高的H1R表达水平下才实现了对H1R-H4R异源寡聚体的检测,并且很可能与生理学无关。

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