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在中性条件下,研究了胰高血糖素纤维形成过程中含胰高血糖素的磷脂双层的形态变化的 P 和 C 固态 NMR 分析。

P and C solid-state NMR analysis of morphological changes of phospholipid bilayers containing glucagon during fibril formation of glucagon under neutral condition.

机构信息

Graduate School of Engineering, Yokohama National University, 79-5 Tokiwadai, Hodogaya-ku, Yokohama 240-8501, Japan.

Graduate School of Engineering, Yokohama National University, 79-5 Tokiwadai, Hodogaya-ku, Yokohama 240-8501, Japan.

出版信息

Biochim Biophys Acta Biomembr. 2020 Jul 1;1862(7):183290. doi: 10.1016/j.bbamem.2020.183290. Epub 2020 Mar 25.

Abstract

Glucagon is a 29 amino acid peptide hormone secreted by pancreatic α-cells that interacts with specific receptors located in various organs. Glucagon tends to form gel-like fibrillar aggregates that are cytotoxic due to their activation of apoptotic signaling pathways. To understand the glucagon-membrane interactions, morphological changes in dimyristoylphosphatidylcholine (DMPC) bilayers containing glucagon in neutral solution were investigated by observing P NMR spectra. First, lipid bilayers with a DMPC/glucagon molar ratio of 50/1 were observed. One day after preparing the DMPC/glucagon lipid bilayer sample, lipid bilayers were disrupted below the phase transition temperature (Tc). Membrane disruption was reduced 2 days after preparation due to the reduction of glucagon-DMPC interaction, and subsequently increased by 4 days and was reduced again by 7 days. TEM measurements showed that small ellipsoidal intermediates of glucagon were observed inside the small size of lipid bilayer after 4 days, while fibrils grew inside lipid bilayer after 19 days. These results indicate that morphological changes in DMPC/glucagon lipid bilayers are correlated with the evolution of glucagon aggregate state. Particularly, fibril intermediate shows a strong glucagon lipid bilayer interaction. We further investigated the structure and kinetics of glucagon fibril formation inside the DMPC lipid bilayer in a neutral solution using C solid-state NMR spectroscopy. α-Helical structures were observed around Gly4 and Ala19 in the monomeric form, which changed to β-sheet structures in the fibril form. The fibrillation process can be explained by a two-step autocatalytic reaction mechanism in which the first step is a homogeneous nuclear formation (k), and the second step is an autocatalytic heterogeneous fibrillation process (k).

摘要

胰高血糖素是一种由胰腺α细胞分泌的 29 个氨基酸肽激素,与位于各种器官中的特定受体相互作用。胰高血糖素往往会形成凝胶状的纤维状聚集物,由于它们激活凋亡信号通路,因此具有细胞毒性。为了了解胰高血糖素与膜的相互作用,通过观察 P NMR 谱研究了中性溶液中含有胰高血糖素的二肉豆蔻酰磷脂酰胆碱(DMPC)双层的形态变化。首先,观察了 DMPC/胰高血糖素摩尔比为 50/1 的脂质双层。在制备 DMPC/胰高血糖素脂质双层样品的一天后,低于相变温度(Tc)时破坏了脂质双层。由于胰高血糖素-DMPC 相互作用的减少,在制备后两天内,膜破坏减少,随后在第四天增加,并在第七天再次减少。TEM 测量表明,在第四天后,在小脂质双层的小尺寸内观察到小椭圆体中间产物,而在第十九天后,纤维在脂质双层内生长。这些结果表明,DMPC/胰高血糖素脂质双层的形态变化与胰高血糖素聚集态的演变有关。特别是,纤维中间物显示出与 DMPC 脂质双层的强烈相互作用。我们使用 C 固体核磁共振光谱法进一步研究了中性溶液中 DMPC 脂质双层内胰高血糖素纤维形成的结构和动力学。在单体形式中观察到围绕 Gly4 和 Ala19 的α-螺旋结构,在纤维形式中变为β-折叠结构。纤化过程可以通过两步自催化反应机制来解释,其中第一步是均匀核形成(k),第二步是自催化异质纤化过程(k)。

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