首页> 外文期刊>The Journal of protozoology research >Chloroquine resistance status a decade after: re-emergence of sensitive Plasmodium falciparum strains in malaria endemic and epidemic areas in Kenya.
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Chloroquine resistance status a decade after: re-emergence of sensitive Plasmodium falciparum strains in malaria endemic and epidemic areas in Kenya.

机译:十年后对氯喹的抗药性:肯尼亚疟疾流行区和流行区再次出现了敏感的恶性疟原虫菌株。

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Development and spread of chloroquine (CQ) resistance led to its withdrawal in most malaria endemic countries. In Kenya, this occurred in 1998 when clinical efficacy dropped below 50%. Less than a decade after CQ was removed from routine use in Malawi, the drug has reversed to activity and is again effective for first-line treatment of uncomplicated malaria. There is a probability of a similar reversed activity in Kenya for more 10 years of its absence in uncomplicated Plasmodium falciparum malaria treatment. The present study was aimed at establishing the CQ resistance status in the country, 10 years after its withdrawal, by looking at high malaria transmission zone, Mbita, a malaria endemic area and some malaria epidemic areas of the Kenyan highlands. The prevalence of T76 and Y86 P. falciparum molecular markers for CQ resistance in Pfcrt and Pfmdr1 genes were investigated by PCR-RFLP and dot blot analysis in 64 samples collected in March to May 2007 in the endemic area and 38 samples collected in April to July the same year in the epidemics. The study shows that 67.3% of field isolates from the endemic site still harbor Y86 mutation in Pfmdr1 while 32.7% have the wild type allele N86 compared to the 94% and 6% prevalence observed in Mwea, an endemic area, in 2004 ( chi 2=10.08, P=0.00015, 95% CI=2.085-27.8). In the epidemics 75% of field isolates from the epidemic sites still harbor Y86 mutation in Pfmdr1 while 25% have the wild type allele N86 compared to the 91.6% and 8.4% prevalence observed in an epidemic area in 1997 ( chi 2=1.585, P=0.208, 95% CI=0.701-19.176). From the study there is a significant change in the proportions of the resistant genotypes in the endemic areas while in the epidemics, there was also a noticeable shift though not significant. This therefore indicates a slow but steady re-emergence of P. falciparum CQ sensitive strains in the country. Though does not warrant the reintroduction of CQ for malaria treatment.
机译:氯喹(CQ)抗药性的发展和扩散导致其在大多数疟疾流行国家被撤消。在肯尼亚,这种情况发生在1998年,当时临床疗效降至50%以下。在马拉维从常规使用中去除CQ不到十年后,该药物已恢复活性,再次有效用于一线治疗简单的疟疾。在没有简单的恶性疟原虫治疗的情况下,如果肯尼亚不存在疟疾,则有十多年的类似逆转活动的可能性。本研究旨在通过观察疟疾高发区,姆比塔,疟疾流行地区和肯尼亚高地的某些疟疾流行地区,来确定该国在退出CQ后的耐药状况。 T76和Y86 P的患病率。通过PCR-RFLP和斑点印迹分析法对2007年3月至2007年5月在中国北京采集的64个样本中的 Pfcrt 和 Pfmdr 1基因中CQ抗药性的恶性疟分子标记进行了研究。流行地区,并于同年4月至7月收集了38个样本。研究表明,来自地方性站点的67.3%的野外分离株在 Pfmdr 1中仍具有Y86突变,而32.7%的野生型等位基因N86与Mwea的94%和6%的流行率相比, 2004年的流行区域(chi 2 = 10.08,P = 0.00015,95%CI = 2.085-27.8)。在流行病中,来自流行病站点的75%的现场分离株在Pfmdr 1中仍具有Y86突变,而25%的野生型等位基因N86与之相比,在该流行病地区的流行率为91.6%和8.4%。 1997(chi 2 = 1.585,P = 0.208,95%CI = 0.701-19.176)。根据研究,在流行地区,耐药基因型的比例发生了显着变化,而在流行病中,尽管不显着,但也有明显的变化。因此,这表明P缓慢而稳定地重新出现。该国的恶性疟原虫CQ敏感菌株。尽管不保证将CQ重新引入疟疾治疗。

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