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刚地弓形虫双功能羟甲基二氢蝶呤焦磷酸激酶-二氢蝶酸合酶基因的分离与分子特征分析

Isolation and molecular characterization of the bifunctional hydroxymethyldihydropterin pyrophosphokinase-dihydropteroate synthase gene from Toxoplasma gondii.

作者信息

Pashley T V, Volpe F, Pudney M, Hyde J E, Sims P F, Delves C J

机构信息

Department of Biochemistry and Applied Molecular Biology, UK.

出版信息

Mol Biochem Parasitol. 1997 May;86(1):37-47.

PMID:9178266
Abstract

Toxoplasma gondii is an important cause of AIDS-related opportunistic infection, manifest as toxoplasmic encephalitis. The clinical treatment of choice is the synergistic combination of antifolate agents, pyrimethamine and sulphadiazine, of which the latter targets the parasite's dihydropteroate synthase (DHPS) activity. Here, we describe the isolation of the gene encoding this activity in T. gondii. The nucleotide sequence contains an open reading frame interrupted by five introns, which encodes a protein of 664 amino acids with an M(r) of 72991. Sequence analysis revealed that, in addition to DHPS, the predicted protein contains a second enzyme function, hydroxymethyldihydropterin pyrophosphokinase (PPPK). This enzyme immediately precedes DHPS in the folate biosynthetic pathway. The bifunctional arrangement of the T. gondii pppk-dhps gene is the same as that observed in the related protozoan parasite, Plasmodium falciparum, and confirms previous biochemical data that these activities were inseparable. Recently, specific mutations within conserved motifs of the DHPS gene of P. falciparum have been identified which give rise to sulphonamide drug resistance. Analysis of seven clinical isolates of T. gondii did not reveal any similar mutations in this limited sample of organisms that had been subjected to drug pressure.

摘要

弓形虫是艾滋病相关机会性感染的重要病因,表现为弓形虫脑炎。临床治疗的首选是抗叶酸药物乙胺嘧啶和磺胺嘧啶的协同组合,其中后者作用于寄生虫的二氢蝶酸合酶(DHPS)活性。在此,我们描述了弓形虫中编码该活性的基因的分离。核苷酸序列包含一个被五个内含子打断的开放阅读框,其编码一个由664个氨基酸组成、分子量为72991的蛋白质。序列分析表明,除了DHPS外,预测的蛋白质还包含第二种酶功能,即羟甲基二氢蝶呤焦磷酸激酶(PPPK)。该酶在叶酸生物合成途径中紧接在DHPS之前。弓形虫pppk-dhps基因的双功能排列与在相关原生动物寄生虫恶性疟原虫中观察到的相同,并证实了先前的生化数据,即这些活性是不可分割的。最近,已鉴定出恶性疟原虫DHPS基因保守基序内的特定突变,这些突变导致对磺胺类药物产生耐药性。对七个弓形虫临床分离株的分析并未在这个受到药物压力的有限生物体样本中发现任何类似的突变。

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