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Oxymatrine inhibits hepatitis B infection with an advantage of overcoming drug-resistance.

机译:氧化苦参碱具有克服耐药性的优势,可抑制乙型肝炎感染。

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Oxymatrine (OMTR) is an anti-hepatitis drug used in China. Its mechanism of action is unknown. Recently, we found that OMTR inhibits hepatitis B virus (HBV) via down-regulating the expression of heat-stress cognate 70 (Hsc70), a host protein required for HBV DNA replication. Goal of this study was to assess the effect of OMTR on clinical HBV drug-resistance. OMTR monotherapy (oral, 12 months) reduced blood HBV DNA by 96% and HBeAg by 70% in the chronic hepatitis B (CHB) patients resistant to lamivudine (n = 17), equal to its efficacy in the naive CHB cohort (n = 20). Liver biopsy study showed that OMTR treatment caused a decrease of Hcs70 mRNA in liver cells, parallel with a reduction of intracellular HBV DNA. Combination of lamivudine with OMTR (n = 15) (oral, 12 months) showed an enhanced anti-HBV effect as compared to lamivudine monotherapy (n = 25). The incidence of drug resistance against lamivudine in the combination group was significantly lower than that in the lamivudine group (1/15 vs 7/25; p<0.01). The results were further confirmed in vitro. Treatment of HBV(+) HepH2215 cells with sub-optimal dose of OMTR for 8 months suppressed HBV replication without inducing drug resistance, whereas lamivudine monotherapy caused drug-resistant mutation in 3 months. Combination of OMTR with lamivudine prevented HBV from developing drug resistance.
机译:氧化苦参碱(OMTR)是在中国使用的抗肝炎药物。其作用机理未知。最近,我们发现OMTR通过下调热应激关联蛋白70(Hsc70)(一种HBV DNA复制所需的宿主蛋白)的表达来抑制乙型肝炎病毒(HBV)。这项研究的目的是评估OMTR对临床HBV耐药性的影响。在对拉米夫定耐药的慢性乙型肝炎(CHB)患者中,OMTR单一疗法(口服,12个月)可将血液HBV DNA降低96%,HBeAg降低70%(n = 17),相当于其在单纯CHB队列中的疗效(n = 20)。肝活检研究表明,OMTR治疗导致肝细胞中Hcs70 mRNA的下降,同时细胞内HBV DNA下降。与拉米夫定单一疗法(n = 25)相比,拉米夫定联合OMTR(n = 15)(口服,12个月)显示出增强的抗HBV效果。联合组对拉米夫定的耐药率显着低于拉米夫定组(1/15 vs 7/25; p <0.01)。在体外进一步证实了该结果。用亚最佳剂量的OMTR治疗HBV(+)HepH2215细胞8个月可抑制HBV复制而不会引起耐药性,而拉米夫定单一疗法则在3个月内引起耐药性突变。 OMTR与拉米夫定的组合可防止HBV产生耐药性。

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