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荧光素酶与N端信号肽融合后,可从转染的恶性疟原虫中分泌出来,并转运至被感染红细胞的细胞质中。

Luciferase, when fused to an N-terminal signal peptide, is secreted from transfected Plasmodium falciparum and transported to the cytosol of infected erythrocytes.

作者信息

Burghaus P A, Lingelbach K

机构信息

Philipps-Universität Marburg, FB Biologie/Zoologie, Abt. Parasitologie, D-35032 Marburg, Germany.

出版信息

J Biol Chem. 2001 Jul 20;276(29):26838-45. doi: 10.1074/jbc.M100111200. Epub 2001 May 25.

Abstract

Plasmodium falciparum, a unicellular parasite that causes human malaria, infects erythrocytes where it develops within a vacuole. The vacuolar membrane separates the parasite from the erythrocyte cytosol. Some secreted parasite proteins remain inside the vacuole, and others are transported across the vacuolar membrane. To identify the protein sequences responsible for this distribution we investigated the suitability of the green fluorescent protein and luciferase as reporters in transiently transfected parasites. Because of the higher sensitivity of the enzymatic assay, luciferase was quantified 3 days after transfection, whereas reliable detection of green fluorescent protein required prolonged drug selection. Luciferase was confined to the parasite cytosol in subcellular fractions of infected erythrocytes. When parasites were transfected with a hybrid gene coding for the cleavable N-terminal signal peptide of a secreted parasite protein fused to luciferase, the reporter protein was secreted. It was recovered with the vacuolar content and the erythrocyte cytosol. The results suggest that no specific protein sequences are required for translocation across the vacuolar membrane. The high local concentration of luciferase within the vacuole argues against free diffusion, and thus transport into the erythrocyte cytosol must involve a rate-limiting step.

摘要

恶性疟原虫是一种导致人类疟疾的单细胞寄生虫,它感染红细胞并在液泡内发育。液泡膜将寄生虫与红细胞胞质溶胶分隔开来。一些分泌的寄生虫蛋白留在液泡内,而其他蛋白则穿过液泡膜进行转运。为了确定负责这种分布的蛋白质序列,我们研究了绿色荧光蛋白和荧光素酶作为瞬时转染寄生虫报告基因的适用性。由于酶促测定的灵敏度更高,转染3天后对荧光素酶进行了定量,而可靠检测绿色荧光蛋白则需要延长药物筛选时间。在感染红细胞的亚细胞组分中,荧光素酶局限于寄生虫胞质溶胶中。当用编码与荧光素酶融合的分泌型寄生虫蛋白的可裂解N端信号肽的杂交基因转染寄生虫时,报告蛋白被分泌出来。它与液泡内容物和红细胞胞质溶胶一起被回收。结果表明,穿过液泡膜的转运不需要特定的蛋白质序列。液泡内荧光素酶的高局部浓度排除了自由扩散的可能性,因此转运到红细胞胞质溶胶中必然涉及一个限速步骤。

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