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首页> 外文期刊>Memórias do Instituto Oswaldo Cruz >Population genetic structure of the major malaria vector Anopheles darlingi (Diptera: Culicidae) from the Brazilian Amazon, using microsatellite markers
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Population genetic structure of the major malaria vector Anopheles darlingi (Diptera: Culicidae) from the Brazilian Amazon, using microsatellite markers

机译:使用微卫星标记的来自巴西亚马逊河的主要疟疾媒介按蚊(Diptera:Culicidae)的种群遗传结构

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The population genetic structure of Anopheles darlingi, the major human malaria vector in the Neotropics, was examined using seven microsatellite loci from nine localities in central and western Amazonian Brazil. High levels of genetic variability were detected (5-25 alleles per locus; H E = 0.519-0.949). There was deviation from Hardy-Weinberg Equilibrium for 59.79% of the tests due to heterozygote deficits, while the analysis of linkage disequilibrium was significant for only two of 189 (1.05%) tests, most likely caused by null alleles. Genetic differentiation (F ST = 0.001-0.095; Nm = 4.7-363.8) indicates that gene flow is extensive among locations < 152 km apart (with two exceptions) and reduced, but not absent, at a larger geographic scale. Genetic and geographic distances were significantly correlated (R2 = 0.893, P < 0.0002), supporting the isolation by distance (IBD) model. The overall estimate of Ne was 202.4 individuals under the linkage disequilibrium model, and 8 under the heterozygote excess model. Analysis of molecular variance showed that nearly all variation (~ 94%) was within sample locations. The UPGMA phenogram clustered the samples geographically, with one branch including 5/6 of the state of Amazonas localities and the other branch the Acre, Rond?nia, and remaining Amazonas localities. Taken together, these data suggest little genetic structure for An. darlingi from central and western Amazonian Brazil. These findings also imply that the IBD model explains nearly all of the differentiation detected. In practical terms, populations of An. darlingi at distances < 152 km should respond similarly to vector control measures, because of high gene flow.
机译:使用来自巴西中部和西部巴西九个地区的七个微卫星基因座,对新热带地区主要的人类疟疾传播媒介按蚊的种群遗传结构进行了研究。检测到高水平的遗传变异性(每个基因座5-25个等位基因; H E = 0.519-0.949)。由于杂合子缺陷,有59.79%的测试偏离了Hardy-Weinberg平衡,而只有189个测试(1.05%)中有两个测试对连锁不平衡的分析很显着,最有可能是由无效等位基因引起的。遗传分化(F ST = 0.001-0.095; Nm = 4.7-363.8)表明,基因流在相距小于152 km的位置之间广泛分布(两个例外),并且在较大的地理范围内有所减少,但并不缺乏。遗传距离和地理距离显着相关(R2 = 0.893,P <0.0002),支持按距离隔离(IBD)模型。在连锁不平衡模型下,Ne的总体估计为202.4个人,在杂合子过量模型下,Ne的总体估计为8。分子变异分析表明,几乎所有变异(〜94%)都在样品位置内。 UPGMA象形图按地理位置对样本进行聚类,其中一个分支包括Amazonas州的州的5/6,另一分支包括Acre,Rond?nia和其余Amazonas州。综上所述,这些数据表明An的遗传结构很少。来自亚马逊中部和西部巴西的达令吉。这些发现还暗示,IBD模型几乎可以解释所检测到的所有差异。实际上,An的人口。由于基因流量高,在距离<152 km的达令吉,对媒介控制措施的响应应类似。

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