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利用小角中子散射研究血管紧张素 II 与模型膜的相互作用。

Use of small angle neutron scattering to study the interaction of angiotensin II with model membranes.

机构信息

Niels Bohr Institute, Copenhagen, Denmark.

出版信息

Eur Biophys J. 2011 May;40(5):687-98. doi: 10.1007/s00249-011-0675-6. Epub 2011 Feb 3.

Abstract

Understanding biological processes assumes a detailed understanding of the interaction of all involved molecules. Here the effect of the peptide hormone angiotensin II (Ang II), an agonist of the angiotensin receptors, on the structure of unilamellar and multilamellar dimyristoyl phosphatidylcholine vesicles was studied by small angle neutron scattering, dynamic light scattering and differential scanning calorimetry. The calorimetry data indicate a weak interaction of Ang II with the surface of the membrane bilayer, as the pretransition persists during all experiments, and the main transition is only slightly shifted towards higher temperatures. From the SANS data we were able to confirm the calorimetric data and verify the interaction of the hormone with the membrane surface. At low temperatures, when the lipid molecules are in the gel phase, more precisely in the ripple phase, the peptide penetrates in the head group core, but due to the close packing of the acyl chains, the hydrophobic region is not affected. In a temperature region below but close to the region of the phase transition, the hydrophibic core starts to be affected by the peptide, and the same is true for the fluid phase. Upon binding of the peptide, the thickness of the head group increases, and the scattering length density of the head group starts to rise with increasing peptide concentrations. This interaction and binding to the membrane surface may be relevant for the relocation, binding and reconstitution of the angiotensin receptors into the membrane. Second, the peptide adsorption to the membrane surface may contribute to the binding of Ang II in the active site of the receptor.

摘要

理解生物过程需要详细了解所有相关分子的相互作用。在这里,通过小角中子散射、动态光散射和差示扫描量热法研究了肽激素血管紧张素 II(Ang II),即血管紧张素受体激动剂,对单分子层和多分子层二肉豆蔻酰磷脂酰胆碱囊泡结构的影响。量热数据表明,Ang II 与膜双层表面的相互作用较弱,因为在所有实验中,预转变都持续存在,而主转变仅略微向更高温度移动。从 SANS 数据中,我们能够证实量热数据,并验证激素与膜表面的相互作用。在低温下,当脂质分子处于凝胶相时,更准确地说是在纹波相时,肽渗透到头基团核心,但由于酰链的紧密堆积,疏水区不受影响。在低于但接近相变区域的温度区域内,疏水区核心开始受到肽的影响,而在流动相也是如此。在肽结合后,头基团的厚度增加,并且随着肽浓度的增加,头基团的散射长度密度开始上升。这种与膜表面的相互作用和结合可能与血管紧张素受体在膜中的重新定位、结合和再构成有关。其次,肽对膜表面的吸附可能有助于 Ang II 在受体的活性部位结合。

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