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

被引:10
作者
Perpinan, Elena [1 ]
Caro-Perez, Noelia [1 ]
Garcia-Gonzalez, Neris [5 ]
Gregori, Josep [2 ,3 ]
Gonzalez, Patricia [1 ]
Bartres, Concepcion [1 ]
Eugenia Soria, Maria [2 ]
Perales, Celia [2 ]
Lens, Sabela [1 ]
Marino, Zoe [1 ]
Carlota Londono, Maria [1 ]
Ariza, Xavier [1 ]
Koutsoudakis, George [1 ]
Quer, Josep [2 ,4 ]
Gonzalez-Candelas, Fernando [5 ]
Forns, Xavier [1 ]
Perez-del-Pulgar, Sofia [1 ]
机构
[1] Univ Barcelona, CIBEREHD, IDIBAPS, Liver Unit,Hosp Clin, Barcelona, Spain
[2] HUVH, VHIR, Dept Internal Med, Liver Unit,Liver Dis Lab Viral Hepatitis, Barcelona, Spain
[3] Roche Diagnost SL, Barcelona, Spain
[4] Univ Autonoma Barcelona, Barcelona, Spain
[5] Univ Valencia, FISABIO, Joint Res Unit Infecc & Salud Publ, I2SysBio,CIBERESP, Valencia, Spain
关键词
direct-acting antivirals; hepatitis C virus; quasispecies; resistance-associated substitutions; SIMEPREVIR PLUS SOFOSBUVIR; GENOTYPE 1-INFECTED PATIENTS; TREATMENT HCV RNA; DECREASED SENSITIVITY; NAIVE PATIENTS; INFECTION; BASE-LINE; VARIANTS; DACLATASVIR; INHIBITORS;
D O I
10.1111/jvh.12986
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
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.
引用
收藏
页码:1515 / 1525
页数:11
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