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二甲基亚砜和深度冷冻过程对克氏锥虫感染性、活力及超微结构的影响。

Effects of dimethylsulfoxide and the deep-freezing process on the infectivity, motility, and ultrastructure of Trypanosoma cruzi.

作者信息

Raether W, Michel R, Uphoff M

机构信息

Hoechst Aktiengesellschaft, Frankfurt, Federal Republic of Germany.

出版信息

Parasitol Res. 1988;74(4):307-13. doi: 10.1007/BF00539450.

Abstract

The effects of dimethylsulfoxide (DMSO, final concentration 5%) and the deep-freezing process on the infectivity (ID50), motility, and ultrastructure of nontreated and DMSO-treated Trypanosoma cruzi suspensions (PSG-3 buffer with 10% horse serum) were investigated prior to and after cryopreservation in liquid nitrogen. DMSO equilibration caused distinct suppression of motility and characteristic, fine structural alterations in numerous organelles, such as myelin-like structures in the cytoplasm and/or inside the mitochondrial apparatus, enlargement of the perinuclear space, endoplasmic reticulum, and mitochondrial cristae, as well as condensation of the kinetoplast with loss of its lamellar structure. There was no evidence of loss of infectivity in DMSO-treated parasites. DMSO-treated and deep-frozen organisms showed, however, very similar fine structural alterations, although damage occurring during freezing and thawing was more pronounced. Apart from the frequently enlarged kinetoplast and the loosening of its mitochondrial matrix, numerous trypanosomes revealed total disintegration of the kinetoplast-mitochondrion complex with loss of its whole matrix. Deep-frozen trypanosomes were significantly less infective to mice than nontreated organisms, and their motility was strongly suppressed. These results suggest that cryopreservation and thawing of T. cruzi may lead to severe damage of the mitochondrial apparatus and thus to heavy disorders of metabolic function, exhaustion of the metabolic pool, and finally, to death of such damaged trypanosomes, despite the use of DMSO as a cryoprotective agent.

摘要

在液氮冷冻保存前后,研究了二甲基亚砜(DMSO,终浓度5%)和深度冷冻过程对未处理及经DMSO处理的克氏锥虫悬液(含10%马血清的PSG-3缓冲液)的感染性(半数感染剂量)、活力及超微结构的影响。DMSO平衡导致活力明显抑制,许多细胞器出现特征性的细微结构改变,如细胞质和/或线粒体内出现髓鞘样结构、核周间隙、内质网和线粒体嵴增大,以及动基体浓缩并丧失其板层结构。未发现经DMSO处理的寄生虫感染性丧失。然而,经DMSO处理并深度冷冻的生物体显示出非常相似的细微结构改变,尽管冻融过程中发生的损伤更为明显。除了动基体频繁增大及其线粒体基质疏松外,许多锥虫还显示出动基体-线粒体复合体完全解体并丧失其整个基质。深度冷冻的锥虫对小鼠的感染性明显低于未处理的生物体,其活力也受到强烈抑制。这些结果表明,克氏锥虫的冷冻保存和解冻可能导致线粒体严重损伤,进而导致代谢功能严重紊乱、代谢池耗尽,最终导致这些受损锥虫死亡,尽管使用了DMSO作为冷冻保护剂。

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