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在胆汁模型和人体胆汁中对超分子聚集体进行成像。

Imaging supramolecular aggregates in bile models and human bile.

作者信息

Kaplun A, Konikoff F M, Eitan A, Rubin M, Vilan A, Lichtenberg D, Gilat T, Talmon Y

机构信息

Department of Chemical Engineering, Technion, Haifa, Israel.

出版信息

Microsc Res Tech. 1997 Oct 1;39(1):85-96. doi: 10.1002/(SICI)1097-0029(19971001)39:1<85::AID-JEMT7>3.0.CO;2-Z.

Abstract

Investigation of cholesterol crystallization is essential for the understanding of gallstone formation. Previous work has revealed a variety of aggregates of different sizes and shapes prior to the appearance of "classical" plate-like cholesterol monohydrate crystals both in native biles and model systems. In this article, we review existing data based on various microscopic techniques and present data on microstructural pathways leading to cholesterol crystal formation in two different bile models and in native bile. In continuation of our recent investigation of microstructures in nucleating human bile, we now present data suggesting that polymorphism is not limited to complex native bile, but also appears in two, simplified model systems. These studies employed cryo-transmission electron microscopy (cryo-TEM) and video-enhanced light microscopy, using Nomarski optics (VELM). Only the combined use of these two complementary, non-perturbing direct methods can cover the whole range of microstructures ranging from a few nanometers to several microns. Concentrated isotropic solutions of bile models, composed of cholesterol, lecithin and taurocholate, were diluted to induce cholesterol supersaturation and start an evolution of microstructures, leading to cholesterol crystallization. Initially, small spheroidal micelles were observed by cryo-TEM. Subsequently, uni-, oligo- and multilamellar vesicles, compatible with structures seen at the same time by VELM, appeared in coexistence with micelles. Thereafter, during a dynamic phase of cholesterol crystallization, filaments, tubular and helical microstructures, as well as classical plate-like cholesterol monohydrate crystals were noted by light microscopy. Eventually, large plate-like crystals were observed by VELM, while cryo-TEM revealed only small spheroidal micelles. The crystallization process in native human bile during ex vivo incubation was found to bear close resemblance to the findings in the model systems, further supporting the applicability of these systems to the exploration of microstructural aspects of nucleating human bile.

摘要

对胆固醇结晶的研究对于理解胆结石形成至关重要。先前的研究表明,在天然胆汁和模型系统中,在出现“经典”板状胆固醇一水合物晶体之前,会形成各种不同大小和形状的聚集体。在本文中,我们回顾了基于各种显微镜技术的现有数据,并展示了在两种不同胆汁模型和天然胆汁中导致胆固醇晶体形成的微观结构途径的数据。延续我们最近对成核人胆汁微观结构的研究,我们现在展示的数据表明,多态性不仅限于复杂的天然胆汁,在两种简化的模型系统中也会出现。这些研究采用了低温透射电子显微镜(cryo-TEM)和使用诺马斯基光学(VELM)的视频增强光学显微镜。只有结合使用这两种互补的、非侵入性的直接方法,才能涵盖从几纳米到几微米的整个微观结构范围。由胆固醇、卵磷脂和牛磺胆酸盐组成的胆汁模型的浓缩各向同性溶液被稀释以诱导胆固醇过饱和,并引发微观结构的演变,导致胆固醇结晶。最初,通过低温透射电子显微镜观察到小的球形胶束。随后,与同时通过VELM看到的结构兼容的单、寡和多层囊泡与胶束共存出现。此后,在胆固醇结晶的动态阶段,通过光学显微镜观察到丝状、管状和螺旋状微观结构以及经典的板状胆固醇一水合物晶体。最终,通过VELM观察到大型板状晶体,而低温透射电子显微镜仅显示小的球形胶束。发现离体孵育过程中天然人胆汁中的结晶过程与模型系统中的发现非常相似,进一步支持了这些系统在探索成核人胆汁微观结构方面的适用性。

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