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与微卫星位点相比,恶性疟原虫配子表面蛋白基因Pfs48/45变异的极端地理固定性。

Extreme geographical fixation of variation in the Plasmodium falciparum gamete surface protein gene Pfs48/45 compared with microsatellite loci.

作者信息

Conway D J, Machado R L, Singh B, Dessert P, Mikes Z S, Povoa M M, Oduola A M, Roper C

机构信息

Department of Infectious and Tropical Diseases, London School of Hygiene and Tropical Medicine, Keppel Street, WC1E 7HT, London, UK.

出版信息

Mol Biochem Parasitol. 2001 Jul;115(2):145-56. doi: 10.1016/s0166-6851(01)00278-x.

Abstract

Comparing patterns of genetic variation at multiple loci in the genome of a species can potentially identify loci which are under selection. The large number of polymorphic microsatellites in the malaria parasite Plasmodium falciparum are available markers to screen for selectively important loci. The Pfs48/45 gene on Chromosome 13 encodes an antigenic protein located on the surface of parasite gametes, which is a candidate for a transmission blocking vaccine. Here, genotypic data from 255 P. falciparum isolates are presented, which show that alleles and haplotypes of five single nucleotide polymorphisms (SNPs) in the Pfs48/45 gene are exceptionally skewed in frequency among different P. falciparum populations, compared with alleles at 11 microsatellite loci sampled widely from the parasite genome. Fixation indices measuring inter-population variance in allele frequencies (F(ST)) were in the order of four to seven times higher for Pfs48/45 than for the microsatellites, whether considered (i) among populations within Africa, or (ii) among different continents. Differing mutational processes at microsatellite and SNP loci could generally affect the population structure at these different types of loci, to an unknown extent which deserves further investigation. The highly contrasting population structure may also suggest divergent selection on the amino acid sequence of Pfs48/45 in different populations, which plausibly indicates a role for the protein in determining gamete recognition and compatibility.

摘要

比较一个物种基因组中多个位点的遗传变异模式,有可能识别出处于选择压力下的位点。疟原虫恶性疟原虫中大量的多态微卫星是筛选具有选择重要性位点的可用标记。13号染色体上的Pfs48/45基因编码一种位于寄生虫配子表面的抗原蛋白,它是传播阻断疫苗的候选对象。这里展示了来自255个恶性疟原虫分离株的基因型数据,这些数据表明,与从寄生虫基因组广泛采样的11个微卫星位点的等位基因相比,Pfs48/45基因中五个单核苷酸多态性(SNP)的等位基因和单倍型在不同恶性疟原虫种群中的频率异常偏斜。测量等位基因频率的种群间方差的固定指数(F(ST)),对于Pfs48/45来说,无论是在非洲内部的种群之间,还是在不同大陆之间,都比微卫星高四到七倍。微卫星和SNP位点不同的突变过程通常可能在未知程度上影响这些不同类型位点的种群结构,这值得进一步研究。高度对比的种群结构也可能表明不同种群对Pfs48/45氨基酸序列的选择存在差异,这合理地表明该蛋白在决定配子识别和兼容性方面发挥作用。

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