Department of Biophysics, Universidade Federal de São Paulo, Escola Paulista de Medicina, São Paulo 04023-062, Brazil.
Biol Chem. 2009 Dec;390(12):1265-70. doi: 10.1515/BC.2009.143.
Binding of angiotensin II (DRVYIHPF, AngII) to its AT(1) receptor can trigger a process known as tachyphylaxis (loss of receptor response owing to repeated agonist stimulation). We propose a two-state binding model for tachyphylaxis where the N-terminal Asp(1) and Arg(2) residues of the peptide are supposed to initially bind to the N-terminal segment (Arg(23)) and to the EC-3 loop (Asp(281)) of an AT(1) molecule, respectively (state 1). Sequentially, a disruption of the salt bond between the AngII Asp(1) beta-carboxyl function and the receptor Arg(23) can occur with release of the peptide N-terminal segment, favoring the binding of the Arg(2) residue to the EC-3 loop (Asp(178,281), state 2). In the present study, we expanded this investigation by assaying pharmacological properties of different AngII analogs in guinea-pig ileum bearing modifications at positions 1 and 2. Most of these peptides were weak agonists but many of them had the ability to induce tachyphylaxis. These findings support the two-state model for tachyphylaxis, but alternative mechanisms were revealed where state 1 was no longer needed, depending on the chemical structure of AngII residue 1. Otherwise, any modification of the wild type AngII Arg(2) residue was deleterious for the tachyphylaxis mechanism.
血管紧张素 II(DRVYIHPF,AngII)与 AT(1)受体的结合可触发一种称为脱敏(由于重复激动剂刺激导致受体反应丧失)的过程。我们提出了一种脱敏的两态结合模型,其中肽的 N 端 Asp(1)和 Arg(2)残基分别假定最初与 AT(1)分子的 N 端片段(Arg(23))和 EC-3 环(Asp(281))结合(状态 1)。随后,AngII Asp(1)β-羧基功能和受体 Arg(23)之间的盐键可能会中断,导致肽 N 端片段释放,有利于 Arg(2)残基与 EC-3 环(Asp(178,281))结合(状态 2)。在本研究中,我们通过检测在位置 1 和 2 上进行修饰的豚鼠回肠中不同 AngII 类似物的药理特性,扩展了这一研究。这些肽大多是弱激动剂,但其中许多具有诱导脱敏的能力。这些发现支持了脱敏的两态模型,但也揭示了替代机制,其中不需要状态 1,这取决于 AngII 残基 1 的化学结构。否则,野生型 AngII Arg(2)残基的任何修饰都会对脱敏机制造成损害。
