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疟原虫在其宿主红细胞膜上诱导产生的新渗透途径:将药物靶向输送到受感染细胞的潜在途径。

New permeability pathways induced by the malarial parasite in the membrane of its host erythrocyte: potential routes for targeting of drugs into infected cells.

作者信息

Ginsburg H, Stein W D

机构信息

Department of Biological Chemistry, Hebrew University of Jerusalem, Israel.

出版信息

Biosci Rep. 1987 Jun;7(6):455-63. doi: 10.1007/BF01116501.

Abstract

Malarial parasites propagate asexually inside the erythrocytes of their vertebrate host. Six hours after invasion, the permeability of the host cell membrane to anions and small nonelectrolytes starts to increase and reaches its peak as the parasite matures. This increased permeability differs from the native transport systems of the normal erythrocyte in its solute selectivity pattern, its enthalpy of activation and its susceptibility to inhibitors, suggesting the appearance of new transport pathways. A biophysical analysis of the permeability data indicates that the selectivity barrier discriminates between permeants according to their hydrogen bonding capacity and has solubilization properties compared to those of iso-butanol. The new permeability pathways could result from structural defects caused in the host cell membrane by the insertion of parasite-derived polypeptides. It is suggested that the unique transport properties of the new pathways be used to target drugs into infected cells, to affect the parasite either directly or through the modulation of the intraerythrocytic environment. The feasibility of drug targeting is demonstrated in in vitro cultures of the human malarial parasite Plasmodium falciparum.

摘要

疟原虫在其脊椎动物宿主的红细胞内进行无性繁殖。入侵六小时后,宿主细胞膜对阴离子和小分子非电解质的通透性开始增加,并在寄生虫成熟时达到峰值。这种增加的通透性在溶质选择性模式、活化焓及其对抑制剂的敏感性方面不同于正常红细胞的天然转运系统,表明出现了新的转运途径。对通透性数据的生物物理分析表明,选择性屏障根据渗透物的氢键能力区分渗透物,并且与异丁醇相比具有增溶特性。新的通透性途径可能是由寄生虫衍生多肽插入宿主细胞膜导致的结构缺陷引起的。有人提出,利用新途径独特的转运特性将药物靶向感染细胞,直接或通过调节红细胞内环境来影响寄生虫。在人类疟原虫恶性疟原虫的体外培养中证明了药物靶向的可行性。

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