Clinical relevance of detectable but not quantifiable hepatitis C virus RNA during boceprevir or telaprevir treatment

HarringtonP.R.; ZengW.; NaegerL.K.

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Clinical relevance of detectable but not quantifiable hepatitis C virus RNA during boceprevir or telaprevir treatment

机译：在boceprevir或telaprevir治疗期间可检测到但无法量化的丙型肝炎病毒RNA的临床意义

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Boceprevir- and telaprevir-based treatments for chronic hepatitis C virus (HCV) infection use specific response-guided therapy (RGT) guidelines. Eligibility for shortened treatment duration is based on achieving undetectable HCV RNA early during treatment. It is unclear whether a detected HCV RNA level that is below the assay lower limit of quantitation (detectable/BLOQ) is comparable to an undetectable HCV RNA level for RGT decision making. We analyzed data from boceprevir and telaprevir clinical trials to obtain a comprehensive understanding of the frequency and clinical relevance of detectable/BLOQ HCV RNA measurements. In Phase 3 trials P05216 (boceprevir), C216 (telaprevir), and 108 (telaprevir), detectable/BLOQ levels were reported for approximately 10%-20% of all on-treatment HCV RNA measurements. In P05216 and C216, subjects with detectable/BLOQ HCV RNA, on average, had a reduced sustained virologic response (SVR) rate compared with subjects with undetectable HCV RNA at the same on-treatment timepoint. At key RGT timepoints (week 8 for boceprevir, week 4 for telaprevir), subjects with detectable/BLOQ HCV RNA had an approximately 20% lower SVR rate compared with subjects with undetectable HCV RNA, and this difference widened for later on-treatment timepoints. A similar trend was observed for Study 108, but the differences in SVR rates were modest, potentially explained by a higher frequency of reported detectable/BLOQ results. Analyses of Phase 2 boceprevir and telaprevir trials indicated subjects with detectable/BLOQ HCV RNA at RGT timepoints benefited from extended treatment duration. Conclusion: During boceprevir- and telaprevir-based treatment, subjects with detectable/BLOQ HCV RNA had a reduced virologic response compared with subjects with undetectable HCV RNA. Eligibility for shortened treatment duration should be based on achieving undetectable HCV RNA (i.e., HCV RNA not detected) at RGT decision timepoints.

机译：基于Boceprevir和telaprevir的慢性丙型肝炎病毒（HCV）感染的治疗使用特定的反应指导治疗（RGT）指南。缩短治疗时间的资格基于在治疗过程中尽早获得无法检测到的HCV RNA。尚不清楚检测到的低于测定下限（可检测/ BLOQ）的HCV RNA水平是否可与RGT决策中不可检测的HCV RNA水平相媲美。我们分析了boceprevir和telaprevir临床试验的数据，以全面了解可检测/ BLOQ HCV RNA测量的频率和临床相关性。在3期试验P05216（boceprevir），C216（telaprevir）和108（telaprevir）中，据报告，所有治疗中HCV RNA测量值中约有10％-20％可检测/ BLOQ水平。在P05216和C216中，与在相同治疗时间点未检测到HCV RNA的受试者相比，可检测到/ BLOQ HCV RNA的受试者的平均持续病毒学应答（SVR）率降低。在关键的RGT时间点（boceprevir的第8周，telaprevir的第4周），具有可检测/ BLOQ HCV RNA的受试者的SVR率比未检测到HCV RNA的受试者低约20％，这种差异在以后的治疗时间点上扩大了。研究108观察到类似趋势，但SVR率差异不大，可能是由于报告的可检测/ BLOQ结果频率较高所致。 2期boceprevir和telaprevir试验的分析表明，受益于延长的治疗时间，在RGT时间点可检测到BLOQ HCV RNA的受试者。结论：在基于boceprevir和telaprevir的治疗过程中，具有可检测/ BLOQ HCV RNA的受试者与未检测到HCV RNA的受试者相比，病毒学应答降低。缩短治疗时间的资格应基于在RGT决策时间点获得无法检测到的HCV RNA（即未检测到HCV RNA）。

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《Hepatology: Official Journal of the American Association for the Study of Liver Diseases》 |2012年第4期|共10页
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HarringtonP.R.; ZengW.; NaegerL.K.;
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中图分类消化系及腹部疾病;
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专利

1. Clinical relevance of detectable but not quantifiable hepatitis C virus RNA during boceprevir or telaprevir treatment [J] . HarringtonP.R., ZengW., NaegerL.K. Hepatology: Official Journal of the American Association for the Study of Liver Diseases . 2012,第4期

机译：在boceprevir或telaprevir治疗期间可检测到但无法量化的丙型肝炎病毒RNA的临床意义
2. Lack of Clinically Significant Pharmacokinetic Interaction between the Thrombopoietin Receptor Agonist Eltrombopag and Hepatitis C Virus Protease Inhibitors Boceprevir and Telaprevir (vol 58, pg 6704, 2014) [J] . Wire Mary Beth, Fang Lei, Hussaini Azra, Antimicrobial agents and chemotherapy. . 2015,第5期

机译：血小板生成素受体激动剂Eltrombopag与丙型肝炎病毒蛋白酶抑制剂Boceprevir和Telaprevir之间缺乏临床上重要的药代动力学相互作用（第58卷，第6704页，2014年）
3. Lack of clinically significant pharmacokinetic interaction between the thrombopoietin receptor agonist eltrombopag and hepatitis c virus protease inhibitors boceprevir and telaprevir [J] . WireM.B., FangL., HussainiA., Antimicrobial agents and chemotherapy. . 2014,第11期

机译：血小板生成素受体激动剂Eltrombopag与丙型肝炎病毒蛋白酶抑制剂boceprevir和telaprevir之间缺乏临床上重要的药代动力学相互作用
4. HLA-C gene in Hepatitis C Virus infected Patients in Egypt, to estimate the relation between HLA-C gene and Interferon/Ribavirin as treatment for hepatitis C virus [C] . SHADEN MUAWIA HANAFY, AMAL AHMED ABBAS, SAFY KABEEL ALY MANSOUR International Conference on Cellular and Molecular Biology, Biophysics and Bioengineering . 2015

机译：HLA-C基因在丙型肝炎病毒中感染埃及患者，估计HLA-C基因和干扰素/利巴韦林与丙型肝炎病毒治疗的关系
5. Clinical- & Economic-effectiveness of Treatments for Hepatitis C Virus. [D] . Bichoupan, Kian. 2017

机译：丙型肝炎病毒治疗的临床和经济效果。
6. Erratum for Wire et al. Lack of Clinically Significant Pharmacokinetic Interaction between the Thrombopoietin Receptor Agonist Eltrombopag and Hepatitis C Virus Protease Inhibitors Boceprevir and Telaprevir [O] . Mary Beth Wire, Lei Fang, Azra Hussaini, 2015

机译：Wire等人的勘误血小板生成素受体激动剂Eltrombopag与丙型肝炎病毒蛋白酶抑制剂Boceprevir和Telaprevir之间缺乏临床意义的药代动力学相互作用
7. Clinical relevance of detectable but not quantifiable hepatitis C virus RNA during boceprevir or telaprevir treatment [O] . Patrick R. Harrington, Wen Zeng, Lisa K. Naeger 2012

机译：检测但在Boceprevir或TelaPrevir治疗过程中可检测但不可定量丙型肝炎病毒RNA的临床相关性

Clinical relevance of detectable but not quantifiable hepatitis C virus RNA during boceprevir or telaprevir treatment

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