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首页> 外文期刊>BMC Microbiology >Detection of mixed populations of wild-type and YMDD hepatitis B variants by pyrosequencing in acutely and chronically infected patients
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Detection of mixed populations of wild-type and YMDD hepatitis B variants by pyrosequencing in acutely and chronically infected patients

机译:焦磷酸测序法检测急慢性感染患者中野生型和YMDD乙型肝炎变异株的混合种群

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Background Lamivudine (LAM) is associated with the highest known rate of resistance mutations among nucleotide analogs used to treat chronic hepatitis B virus (HBV) infection. Despite this, LAM continues in widespread use, especially in combination therapies. The primary LAM resistance mutation (rtM204V/I) occurs in the YMDD motif of HBV polymerase. The aim of this study was to characterize Brazilian HBV isolates from acute and chronic cases by direct sequencing, and to identify HBV quasispecies in the YMDD motif using a pyrosequencing method capable of detecting single-nucleotide polymorphisms. HBV DNA from serum samples of 20 individuals with acute HBV infection and 44 with chronic infection undergoing antiviral therapies containing LAM were analyzed by direct sequencing and pyrosequencing methods. Results Phylogenic analyses of direct-sequenced isolates showed the expected genotypes (A, D and F) for the Brazilian population in both acute and chronic infections. However, within genotype A isolates, subgenotype A2 was more frequently detected in acute cases than in chronic cases (P?=?0.012). As expected, none of the individuals with acute hepatitis B had LAM-resistant isolates as a dominant virus population, whether detected by direct sequencing or pyrosequencing. However, pyrosequencing analyses showed that 45% of isolates (9/20) had minor subpopulations (4-17%) of LAM-resistant isolates. Among chronic patients undergoing LAM treatment, YMDD mutants were frequently found as a dominant virus population. In cases where wild-type virus was the dominant population, subpopulations of YMDD variants were usually found, demonstrating the complexity of HBV quasispecies. Conclusions YMDD variants were frequently detected as a minor population in acute HBV infection. The occurrence of pre-existing variants may lead to a high frequency of resistant mutants during antiviral therapy in the chronic phase. In chronic infection, detection of YMDD variants before virological or biochemical breakthrough might contribute to making better therapy choices and thus improving treatment outcome.
机译:背景拉米夫定(LAM)与用于治疗慢性乙型肝炎病毒(HBV)感染的核苷酸类似物中已知的耐药突变率最高。尽管如此,LAM仍在继续广泛使用,尤其是在联合疗法中。主要的LAM抗性突变(rtM204V / I)发生在HBV聚合酶的YMDD基序中。这项研究的目的是通过直接测序来鉴定急性和慢性病例中的巴西HBV分离株,并使用能够检测单核苷酸多态性的焦磷酸测序方法在YMDD基序中鉴定HBV准种。通过直接测序和焦磷酸测序方法分析了20例急性HBV感染者和44例慢性感染者的血清样品中的HBV DNA,这些患者接受了含LAM的抗病毒治疗。结果对直接测序菌株的系统进化分析显示,巴西人群在急性和慢性感染中均具有预期的基因型(A,D和F)。但是,在基因型A分离株中,与慢性病例相比,急性病例中A2亚型的检出率更高(P = 0.012)。不出所料,无论是通过直接测序还是焦磷酸测序检测,急性乙型肝炎患者都没有作为主要病毒种群的LAM抗性分离株。但是,焦磷酸测序分析表明,有45%的分离株(9/20)的LAM抗性分离株具有较小的亚群(4-17%)。在接受LAM治疗的慢性患者中,经常发现YMDD突变体为优势病毒种群。在以野生型病毒为主要种群的情况下,通常会发现YMDD变体的亚群,这说明了HBV准种的复杂性。结论YMDD变异在急性HBV感染中经常被发现为少数人群。在慢性期进行抗病毒治疗期间,先前存在的变体的出现可能导致耐药突变体的出现频率很高。在慢性感染中,在病毒学或生化突破之前检测YMDD变异可能有助于做出更好的治疗选择,从而改善治疗效果。

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