Hepatitis C virus early kinetics and resistance‐associated substitution dynamics during antiviral therapy with direct‐acting antivirals

Perpi?án Elena; Caro‐Pérez Noelia; García‐González Neris; Gregori Josep; González Patricia; Bartres Concepción; Soria Maria Eugenia; Perales Celia; Lens Sabela; Mari?o Zoe; Londo?o María Carlota; Ariza Xavier; Koutsoudakis George; Quer Josep; González‐Candelas Fernando; Forns Xavier; Pérez‐del‐Pulgar Sofía

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Hepatitis C virus early kinetics and resistance‐associated substitution dynamics during antiviral therapy with direct‐acting antivirals

机译：丙型肝炎病毒早期动力学和抗性相关的替代动态在抗病毒治疗期间直接作用抗病毒药

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Summary The emergence of resistance‐associated substitutions (RASs) can compromise the high efficacy of direct‐acting antivirals (DAAs). Little is known about RASs selection at very early time points during DAA treatment. Therefore, we analyzed the potential emergence of RASs immediately after therapy initiation. Samples of 71 patients treated with different DAAs were collected at baseline, during therapy (hours 4 and 8; days 1‐7; weeks 2‐4) or until target not detected. HCV‐RNA levels were determined by qPCR, and RASs were detected by deep sequencing. Sixty‐three (89%) patients achieved a sustained virological response (SVR), 7 (10%) relapsed, and 1 (1%) experienced a breakthrough. Almost all non‐SVR (7/8, 88%) showed RASs either at baseline or relapse. High‐frequency RASs detected at baseline (Y93H and L159F+C316N) remained detectable at early time points during therapy and reappeared as most prevalent substitutions at relapse. Conversely, emergent RASs at relapse (Q80R, D168E/V, R155K and L31V) were not observed during the first hours‐days, before HCV‐RNA became undetectable. HCV‐RNA decay and genetic evolution of the quasispecies followed a similar pattern during the first hours of therapy in SVR and non‐SVR patients. In conclusion, the absence of early RASs selection and the similar dynamics of HCV kinetics and quasispecies in SVR and non‐SVR patients after therapy initiation suggest that RASs selection may occur at later stages in the remaining reservoir, where viral populations persist hidden at very low replication levels. Nevertheless, we cannot completely exclude very early selection, when RASs are present below the sensitivity limit of deep sequencing.

机译：发明内容抵抗相关替代的出现（RASS）可以损害直接作用抗病毒（DAAs）的高效力。在DAA治疗期间，关于RASS选择的令人难以知的是令人讨厌的。因此，我们在治疗启动后立即分析了rass的潜在出现。在基线期间，在治疗期间（小时4和8时1-7天;第2-4周）或直到未检测到的目标未检测到用不同DAA的71名患者的样品。通过QPCR测定HCV-RNA水平，通过深序检测RAS。六十三（89％）患者达到了持续的病毒学反应（SVR），复发7（10％），1（1％）经历了突破。几乎所有非SVR（7/8,88％）在基线或复发时显示了RAS。在基线（Y93H和L159F + C316N）下检测的高频RAS在治疗期间的早期时间点保持可检测，并重新出现作为复发的最普遍的取代。相反，在HCV-RNA变得不可检测之前，在第一小时天期间未观察到复发的紧急RAS（Q80R，D168E / V，R155K和L31V）。 Quasispecies的HCV-RNA衰减和遗传演化在SVR和非SVR患者的第一次治疗过程中遵循类似的模式。总之，治疗开始后，缺乏早期秩序选择和HCV动力学和非SVR患者的类似动态的动态表明，秩序选择可能发生在剩余水库中的后期阶段，病毒群体持续存在于非常低的情况下复制级别。尽管如此，我们不能完全排除非常早期的选择，当时RASS在低于深度测序的灵敏度限制下。

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来源
《Journal of viral hepatitis.》 |2018年第12期|共11页
作者
Perpi?án Elena; Caro‐Pérez Noelia; García‐González Neris; Gregori Josep; González Patricia; Bartres Concepción; Soria Maria Eugenia; Perales Celia; Lens Sabela; Mari?o Zoe; Londo?o María Carlota; Ariza Xavier; Koutsoudakis George; Quer Josep; González‐Candelas Fernando; Forns Xavier; Pérez‐del‐Pulgar Sofía;
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作者单位

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Joint Research Unit Infección y Salud PúblicaFISABIO‐Universitat de València I2SysBio;

Liver Unit Liver Disease Laboratory‐Viral HepatitisVall d'Hebron Institut Recerca (VHIR)‐Hospital;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Liver Unit Liver Disease Laboratory‐Viral HepatitisVall d'Hebron Institut Recerca (VHIR)‐Hospital;

Liver Unit Liver Disease Laboratory‐Viral HepatitisVall d'Hebron Institut Recerca (VHIR)‐Hospital;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Liver Unit Liver Disease Laboratory‐Viral HepatitisVall d'Hebron Institut Recerca (VHIR)‐Hospital;

Joint Research Unit Infección y Salud PúblicaFISABIO‐Universitat de València I2SysBio;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

Liver Unit Hospital ClínicUniversitat de BarcelonaBarcelona Spain;

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原文格式 PDF
正文语种 eng
中图分类传染病;
关键词
direct‐acting antivirals; hepatitis C virus; quasispecies; resistance‐associated substitutions;

机译：直接作用抗病毒;丙型肝炎病毒;Quaspecies;抵抗相关的替代;

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专利

1. Hepatitis C virus early kinetics and resistance‐associated substitution dynamics during antiviral therapy with direct‐acting antivirals [J] . Perpi?án Elena, Caro‐Pérez Noelia, García‐González Neris, Journal of viral hepatitis. . 2018,第S1期

机译：丙型肝炎病毒早期动力学和抗性相关的替代动态在抗病毒治疗期间直接作用抗病毒药
2. Long-Term Follow-Up of Resistance-Associated Substitutions in Hepatitis C Virus in Patients in Which Direct Acting Antiviral-Based Therapy Failed [J] . Kanako Yoshida, Hoang Hai, Akihiro Tamori, International Journal of Molecular Sciences . 2017,第5期

机译：直接作用抗病毒治疗失败的丙型肝炎病毒耐药相关替代基因的长期随访
3. Prevalence of resistance-associated substitutions to direct-acting antiviral agents in hemodialysis and renal transplant patients infected with hepatitis C virus [J] . Infection and Drug Resistance . 2018,第9期

机译：在感染了丙型肝炎病毒的血液透析和肾移植患者中，耐药性替代直接作用抗病毒药的流行
4. MALDI-TOF MS for Monitoring Drug Resistance in Hepatitis B Virus-Infected Patients during Antiviral Therapy [C] . Magda Rybicka, Piotr Stalke, Tomasz Smiatacz, International Mass Spectrometry Conference . 2014

机译：MALDI-TOF MS用于监测抗病毒治疗期间乙型肝炎病毒感染患者耐药性的MS
5. The Distribution of Change over Time in Metabolic, Inflammatory, and Immune Parameters in HCV-monoinfected and HIV/HCV-coinfected Patients Cured of Hepatitis C Virus by Direct-Acting Antiviral Therapy [D] . Emmanuel, Benjamin. 2018

机译：通过直接作用抗病毒治疗，在HCV-单染料和HCV / HCV / HCV-焦收的患者中的代谢，炎症和免疫参数随时间随时间的分布，通过直接作用抗病毒治疗治愈丙型肝炎病毒
6. Long-Term Follow-Up of Resistance-Associated Substitutions in Hepatitis C Virus in Patients in Which Direct Acting Antiviral-Based Therapy Failed [O] . Kanako Yoshida, Hoang Hai, Akihiro Tamori, 2017

机译：直接作用抗病毒疗法无效的患者中丙型肝炎病毒耐药相关替代的长期随访
7. Long-Term Follow-Up of Resistance-Associated Substitutions in Hepatitis C Virus in Patients in Which Direct Acting Antiviral-Based Therapy Failed [O] . Kanako Yoshida, Hoang Hai, Akihiro Tamori, 2017

机译：对直接作用抗病毒药物治疗失败的丙型肝炎病毒耐药相关替代的长期随访

Hepatitis C virus early kinetics and resistance‐associated substitution dynamics during antiviral therapy with direct‐acting antivirals

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