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磷脂基质作为硫芥(HD)的作用靶点:模型膜系统中的核磁共振研究

Phospholipid matrix as a target for sulfur mustard (HD): NMR study in model membrane systems.

作者信息

Debouzy J C, Aous S, Dabouis V, Neveux Y, Gentilhomme E

机构信息

CRSSA, Unité de Biophysique, La Tronche cedex, France.

出版信息

Cell Biol Toxicol. 2002;18(6):397-408. doi: 10.1023/a:1020815723009.

Abstract

Although the interactions of sulfur mustard (HD) with nucleic acids and proteins have been well studied, the toxic interactions with the membrane matrix and specially the phospholipid bilayer have so far been poorly investigated. We have used several NMR techniques to study these interactions: 1H NMR to observe the localization of HD in membranes of small unilamellar vesicles (SUV) of lecithin; 31P NMR to verify the hypothesis of pore formation in membranes of large unilamellar vesicles (LUV); and pseudo solid state 31P and 2H NMR to analyze the dynamic consequences of the presence of HD in multilayer dispersions of dimyristoylphosphatidylcholine (DMPC). Immediate and late modifications of the DMPC-HD complexes have been observed at the macroscopic and microscopic levels. After intoxication, HD is spontaneously incorporated into the membrane and locates at the level of the chain methylene groups. This incorporation occurs without formation of pores in the membrane. The presence of HD in the phospholipid dispersion differentially increases the membrane fluidity depending upon the level involved. Weak at the superficial level (phosphate group), this increase is dose-dependent on progression into the membrane. This increase is related to a lowering of transition temperature when measured at the chain level. Macroscopically, HD induces dose- and time-dependent modifications of the DMPC-HD complexes, leading to the formation of an optically transparent gel. This gel formation is confirmed at a microscopic level, where all structures disappear after intoxication.

摘要

尽管芥子气(HD)与核酸和蛋白质的相互作用已得到充分研究,但迄今为止,其与膜基质特别是磷脂双层的毒性相互作用研究甚少。我们使用了多种核磁共振技术来研究这些相互作用:利用氢核磁共振(1H NMR)观察HD在卵磷脂小单层囊泡(SUV)膜中的定位;利用磷核磁共振(31P NMR)验证大单层囊泡(LUV)膜中形成孔的假设;利用准固态磷核磁共振(31P NMR)和氘核磁共振(2H NMR)分析HD存在于二肉豆蔻酰磷脂酰胆碱(DMPC)多层分散体中的动态影响。已在宏观和微观层面观察到DMPC-HD复合物的即时和后期变化。中毒后,HD自发掺入膜中并定位在链亚甲基水平。这种掺入不会在膜中形成孔。磷脂分散体中HD的存在根据所涉及的水平不同程度地增加膜流动性。在表面水平(磷酸基团)较弱,这种增加在向膜内深入时呈剂量依赖性。当在链水平测量时,这种增加与转变温度的降低有关。宏观上,HD诱导DMPC-HD复合物发生剂量和时间依赖性变化,导致形成光学透明凝胶。在微观层面证实了这种凝胶形成,中毒后所有结构均消失。

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