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利什曼原虫属:通过不完全血红素生物合成途径的基因互补实现δ-氨基乙酰丙酸诱导的卟啉病新生。

Leishmania spp.: delta-aminolevulinate-inducible neogenesis of porphyria by genetic complementation of incomplete heme biosynthesis pathway.

作者信息

Dutta Sujoy, Furuyama Kazumichi, Sassa Shigeru, Chang Kwang-Poo

机构信息

Department of Microbiology/Immunology, Chicago Medical School, Rosalind Franklin University, 3333 Green Bay Road, North Chicago, IL 60064, USA.

出版信息

Exp Parasitol. 2008 Apr;118(4):629-36. doi: 10.1016/j.exppara.2007.11.013. Epub 2007 Dec 3.

DOI:10.1016/j.exppara.2007.11.013
PMID:18164705
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2423932/
Abstract

To further develop the Leishmania model for porphyria based on their deficiencies in heme biosynthesis, three Old World species were doubly transfected as before for Leishmania amazonensis with cDNAs, encoding the 2nd and 3rd enzymes in the pathway. Expression of the transgenes was verified immunologically at the protein level and functionally by uroporphyrin neogenesis that occurs only after exposure of the double-transfectants to delta-aminolevulinate. All species examined were equally deficient in heme biosynthesis, as indicated by the accumulation of uroporphyrin as the sole porphyrin and the production of coproporphyrin upon further transfection of one representative species with the downstream gene. The results obtained thus demonstrate that at least the first five enzymes for heme biosynthesis are absent in all species examined, rendering their transfectants inducible with aminolevulinate to accumulate porphyrins and thus useful as cellular models for human porphyrias.

摘要

为了基于利什曼原虫在血红素生物合成方面的缺陷进一步开发用于卟啉症的利什曼原虫模型,如之前对亚马逊利什曼原虫所做的那样,将三种旧世界物种用编码该途径中第二和第三种酶的cDNA进行双重转染。通过免疫方法在蛋白质水平验证转基因的表达,并通过仅在双重转染体暴露于δ-氨基乙酰丙酸后才发生的尿卟啉新生来进行功能验证。所有检测的物种在血红素生物合成方面同样存在缺陷,这表现为尿卟啉作为唯一卟啉的积累,以及在将一个代表性物种进一步用下游基因转染后粪卟啉的产生。因此获得的结果表明,在所检测的所有物种中至少不存在血红素生物合成的前五种酶,使得它们的转染体能被氨基乙酰丙酸诱导积累卟啉,从而可用作人类卟啉症的细胞模型。

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