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胰岛淀粉样多肽(IAPP)和爪蟾抗菌肽B在支持脂质膜上形成脂质/肽管。

Formation of lipid/peptide tubules by IAPP and temporin B on supported lipid membranes.

作者信息

Kinnunen Paavo K J, Domanov Yegor A, Mattila Juha-Pekka, Varis Teemu

机构信息

Helsinki Biophysics & Biomembrane Group, Medical Biochemistry/Institute of Biomedicine, University of Helsinki, P.O. Box 63 (Haartmaninkatu 8), FIN-00014, Finland.

出版信息

Soft Matter. 2015 Dec 21;11(47):9188-200. doi: 10.1039/b925228b.

Abstract

The conversion of various and to is accelerated by , which are also postulated to represent targets mediating the cytotoxicity of protofibrils. Yet, our understanding of the molecular details governing -catalyzed fibrillogenesis of precursors remains limited. To obtain insight into the intricate interplay of and biophysics we have recently introduced supported bilayers (SLBs) with fluorescent analogs as model biomembranes, observed by time-lapse . Here we demonstrate that human islet () induces within minutes of its application on bilayers the expulsion of numerous flexible tubules from the . Intriguingly, these flexible tubules gradually evolve into a network of straight tubes locally attached to the substrate. Two-color imaging of the and the fluorescently labeled revealed to be distributed along the . Similar linear tubules were observed with the antimicrobial temporin B and the non-amyloidogenic rat , revealing that the above mesoscopic perturbations are not related to formation by the human . Micromanipulation experiments revealed that the linearity of the tubules was caused by tension, stretching the tubules between their points of attachment to the substrate. After longer incubation times, for SLBs containing the oxidatively modified 1-palmitoyl-2-azelaoyl-sn-glycero-3-phosphocholine (, bearing a terminal carboxyl at the end of the chain) and human (but not the other ) some of the straight transformed into highly regular helices. This is likely to reflect tension originating from an efficient aggregation of the into parallelly aligned bundles, associated with tubes containing the oxidized , possibly together with a concomitant flow of along the tubules to the immobile aggregates attaching the tubules to the substrate, these two processes cause, upon shortening of the linear scaffold, the attached excess tubule to adopt a helical morphology, coiling around the core. The above studies are in line with the multiphasic kinetics of fibrillation in the presence of oxidized containing liposomes, assessed by fluorescence enhancement. In addition to demonstrating the feasibility of SLBs as biomimetic model system for studying -assisted fibrillation, our results accentuate the role of chemical composition in modulation of different stages of this process and the associated transformation of architecture. Accordingly, changes in the chemical nature of cellular arising from pathophysiological processes such as oxidative stress may participate in the triggering amyloidogenesis as well as amplification of its detrimental effects in vivo.

摘要

各种物质向“to”的转化会被某些物质加速,这些物质也被假定为介导原纤维细胞毒性的靶点。然而,我们对控制前体“-催化”纤维形成的分子细节的理解仍然有限。为了深入了解“和生物物理学”之间复杂的相互作用,我们最近引入了带有荧光类似物的支持双层膜(SLBs)作为模型生物膜,并通过延时观察。在这里,我们证明人类胰岛()在应用于双层膜后几分钟内,会诱导从膜中排出大量柔性小管。有趣的是,这些柔性小管逐渐演变成局部附着在底物上的直管网络。对“和荧光标记物”的双色成像显示,“沿着”分布。用抗菌肽temporin B和非淀粉样生成的大鼠“也观察到了类似的线性小管”,这表明上述介观扰动与人类“的形成无关”。微操作实验表明,小管的线性是由张力引起的,在小管附着到底物的点之间拉伸小管。经过更长的孵育时间后,对于含有氧化修饰的1-棕榈酰-2-壬二酰-sn-甘油-3-磷酸胆碱(,链末端带有一个羧基)和人类“(但不是其他的)的SLBs”,一些直管转变成了高度规则的螺旋结构。这可能反映了由于“有效聚集形成平行排列的束”而产生的张力,这与含有氧化“的管相关”,可能还伴随着“沿着小管流向将小管附着到底物的固定聚集体”,这两个过程在缩短线性支架时,会使附着的多余小管呈现螺旋形态,围绕核心盘绕。上述研究与在含有氧化脂质体存在下纤维形成的多相动力学一致,通过荧光增强进行评估。除了证明SLBs作为研究“辅助纤维形成”的仿生模型系统的可行性外,我们的结果还强调了化学成分在调节该过程不同阶段以及相关结构转变中的作用。因此,病理生理过程如氧化应激引起的细胞膜化学性质变化可能参与触发淀粉样蛋白生成以及其在体内有害作用的放大。

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