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首页> 外文期刊>The FASEB Journal >RGD peptides induce relaxation of pulmonary arteries and airways via β3-integrins
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RGD peptides induce relaxation of pulmonary arteries and airways via β3-integrins

机译:RGD肽通过β3--1整联蛋白诱导肺动脉和气道的弛豫

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Novel relaxants of pulmonary arteries and airways are of special interest to obtain insights into pulmonary signaling pathways and to develop treatment strategies for lung diseases. Herein, we demonstrate that Arg-Gly-Asp (RGD) peptides induce a dose-dependent relaxation of pulmonary arteries and airways in mouse. The relaxing effect was specific because it was strongly reduced using the control peptides RGE or RAD (P<0.001). Longer peptide sequences containing RGD and its flanking amino acids found in fibronectin showed a similar effect even at a 10-fold lower concentration. The relevance of RGD-induced pulmonary vasorelaxation was demonstrated in isometric force measurements, lung slices, and the isolated perfused lung model under normoxia and hypoxia and in vivo. As cell surface receptor we identified β3- but not β1-integrin subunits. Moreover, vasorelaxation by RGD peptides was strongly diminished after removal of the endothelium in endothelial nitric oxide synthase-deficient (eNOS?/? mice; P<0.01) and after pharmacological inhibition of the NO/sGC pathway (P<0.05). Additionally, several potassium channels like Kv, Kir, and KATP played a role. In airways the response was mediated by Kv and KCa channels. Thus, RGD peptides are relaxants of pulmonary arteries and airways. These findings may help to establish novel therapeutic approaches for pulmonary hypertension and obstructive lung disease.—Welschoff, J., Matthey, M., Wenzel, D. RGD peptides induce relaxation of pulmonary arteries and airways via β3-integrins.
机译:新颖的肺动脉和呼吸道的松弛剂是特别兴趣的,以获得对肺信号传导途径的见解,并为肺病产生治疗策略。在此,我们证明了Arg-Gly-Asp(RGD)肽诱导小鼠肺动脉和气道的剂量依赖性松弛。放松效果是特异性的,因为使用对照肽RGE或RAD强烈地减少(P <0.001)。含有RGD的较长的肽序列及其在纤连蛋白中发现的侧翼氨基酸表现出类似的效果,即使浓度为10倍。在常氧和缺氧和体内,在等轴力测量,肺切片和分离的灌注肺模型中证明了RGD诱导的肺血管扩展的相关性。作为细胞表面受体,我们鉴定了β3-但不是β1-整合蛋白亚基。此外,在除去内皮型一氧化氮合酶(Enos?/ eice; P <0.01)中的内皮内切除后,通过RGD肽的血管插入强烈地降低,并且在NO / SGC途径的药理抑制后(P <0.05)。此外,几种像KV,KIR和KATP这样的钾通道发挥了作用。在呼吸道中,响应由KV和KCA通道介导。因此,RGD肽是肺动脉和气道的弛豫剂。这些发现可能有助于为肺动脉高压和阻塞性肺病建立新的治疗方法.-威尔彻夫,J.,Matthey,M.,Wenzel,D。RGD肽通过β3--1-1-1-1-1-1-1-1-1-1-1-1-1-1-1-1-1-1-1-1-1-1种诱导肺动脉和气道的弛豫。

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