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首页> 外文期刊>BMC Infectious Diseases >Prevalent HBV point mutations and mutation combinations at BCP/preC region and their association with liver disease progression
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Prevalent HBV point mutations and mutation combinations at BCP/preC region and their association with liver disease progression

机译:BCP / preC区的流行HBV点突变和突变组合及其与肝病进展的关系

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Background Mutations in the basic core promoter (BCP) and its adjacent precore (preC) region in HBV genome are common in chronic hepatitis B patients. However, the patterns of mutation combinations in these two regions during chronic infection are less understood. This study focused on single base mutations in BCP and preC region and the multi-mutation patterns observed in chronic HBV infection patients. Methods Total 192 blood samples of chronic HBV infection patients were included. Direct PCR sequencing on the target region of HBV genome was successfully conducted in 157 samples. The rest 35 samples were analyzed by clone sequencing. Only the nucleotide substitutions with their frequencies no less than 10% were included in multi-mutation analysis with the exception for the polymorphic sites between genotypes B and C. Results Five high frequency mutations (≥10%) were found in BCP and preC region. Thirteen types of multi-mutations in one fragment were observed, among which 3 types were common combinations (≥5%). The top three multi-mutations were A1762T/G1764A (36%), A1762T/G1764A/G1896A (11%) and T1753(A/C)/A1762T/G1764A/G1896A (8%). Patients with multi-mutations in viral genomes (≥3) were more likely to have liver cirrhosis or hepatocellular carcinoma (OR = 3.1, 95% CI: 1.6-6.0, P = 0.001). G1896A mutation seemed to be involved in liver disease progression independent of the patient age (OR = 3.6, 95% CI: 1.5-8.6; P = 0.004). In addition, patients with more viral mutations detected (≥3) were more likely to be HBeAg negative (OR = 2.7, 95% CI: 1.1-6.4; P = 0.027). Moreover, G1776A mutation was shown to contribute to HBeAg negativity in our study (OR = 8.6, 95% CI: 1.2-44.9; P = 0.01). Conclusions Patients with advanced liver diseases and with HBeAg negativity more likely have multi-mutations in HBV genomes but with different mutation combination patterns. G1896A mutation appears to be independent of infection history.
机译:背景在慢性乙型肝炎患者中,HBV基因组中的基本核心启动子(BCP)及其相邻的前核心(preC)区突变很常见。然而,人们对慢性感染过程中这两个区域的突变组合模式知之甚少。这项研究的重点是BCP和preC区域的单碱基突变以及在慢性HBV感染患者中观察到的多突变模式。方法对192例慢性乙型肝炎病毒感染患者的血液样本进行分析。在157个样品中成功进行了HBV基因组靶区域的直接PCR测序。其余35个样品通过克隆测序进行分析。除基因型B和C之间的多态性位点外,多突变分析仅包括频率不低于10%的核苷酸取代。结果在BCP和preC区发现了5个高频突变(≥10%)。在一个片段中观察到13种类型的多突变,其中3种是常见的组合(≥5%)。前三个多重突变是A1762T / G1764A(36%),A1762T / G1764A / G1896A(11%)和T1753(A / C)/ A1762T / G1764A / G1896A(8%)。病毒基因组中多重突变(≥3)的患者更有可能患有肝硬化或肝细胞癌(OR = 3.1,95%CI:1.6-6.0,P = 0.001)。 G1896A突变似乎与肝癌进展有关,与患者年龄无关(OR = 3.6,95%CI:1.5-8.6; P = 0.004)。此外,检测到更多病毒突变(≥3)的患者更有可能是HBeAg阴性(OR = 2.7,95%CI:1.1-6.4; P = 0.027)。此外,在我们的研究中,G1776A突变可导致HBeAg阴性(OR = 8.6,95%CI:1.2-44.9; P = 0.01)。结论晚期肝病,HBeAg阴性的患者更有可能在HBV基因组中发生多突变,但突变组合方式不同。 G1896A突变似乎与感染史无关。

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