首页> 外文期刊>Research communications in molecular pathology and pharmacology >Genetic diversity of drug targets including dihydropteroate synthase, dihydrofolate reductase and cytochrome b, in Pneumocystis carinii f. sp. hominis isolates in Japan.
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Genetic diversity of drug targets including dihydropteroate synthase, dihydrofolate reductase and cytochrome b, in Pneumocystis carinii f. sp. hominis isolates in Japan.

机译:卡氏肺孢子虫中药物靶标的遗传多样性,包括二氢蝶呤合酶,二氢叶酸还原酶和细胞色素b。 sp。日本的人型分离株。

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摘要

This study examined gene polymorphisms in dihydropteroate synthase (DHPS), dihydrofolate reductase (DHFR) and cytochrome b of Pneumocystis carinii isolated from 34 patients with P. carinii pneumonia (PCP) in Japan. Four amino acid substitutions (Thr55Ala, Pro57Ser, His60Gln and Glu169Gly) in DHPS, 2 mutations (Ala67Val and Cys166Tyr) in DHFR and 1 mutation (Leu280Phe) in cytochrome b were found in 9 (26.5%), 2 (5.9%) and 1 (2.9%) patient, respectively. No linkage of mutations in DHPS to those in DHFR or cytochrome b was observed. The patients whose isolates showed mutations in DHPS, DHFR and cytochrome b were not exposed to sulfonamides, DHFR inhibitors and atovaquone before they developed PCP, except for 2 patients. Co-trimoxazole treatment failed more frequently in patients whose isolates had DHPS mutations than in those whose isolates showed wild-type DHPS (n=6 [85.7%] versus n=3 [12.5%]; P=0.001). Our results suggest that DHPS mutations may contribute to failure of co-trimoxazole treatment for PCP.
机译:这项研究检查了从日本34例卡氏肺孢子虫肺炎(PCP)患者中分离出的卡氏肺孢子虫的二氢蝶呤合酶(DHPS),二氢叶酸还原酶(DHFR)和细胞色素b的基因多态性。在9(26.5%),2(5.9%)和1中发现了DHPS中的四个氨基酸取代(Thr55Ala,Pro57Ser,His60Gln和Glu169Gly),DHFR中的2个突变(Ala67Val和Cys166Tyr)和细胞色素b中的1个突变(Leu280Phe)。 (2.9%)患者。没有观察到DHPS突变与DHFR或细胞色素b突变的连锁。分离株显示DHPS,DHFR和细胞色素b突变的患者在发生PCP之前未接触磺酰胺,DHFR抑制剂和阿托伐醌,但2例患者除外。与具有野生型DHPS的分离株相比,co-trimoxazole治疗失败的分离株具有DHPS突变的患者更为频繁(n = 6 [85.7%]对n = 3 [12.5%]; P = 0.001)。我们的结果表明,DHPS突变可能会导致联用三唑治疗PCP失败。

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