Retreatment with sofosbuvir/ledipasvir with or without lead-in interferon- injections in patients infected with genotype 1b hepatitis C virus after unsuccessful daclatasvir/asunaprevir therapy

被引:5
|
作者
Uemura, Hayato [1 ]
Uchida, Yoshihito [1 ]
Kouyama, Jun-ichi [1 ]
Naiki, Kayoko [1 ]
Yamaba, Shinpei [1 ]
Fuchigami, Akira [1 ]
Saito, Yoichi [1 ]
Shiokawa, Keisuke [1 ]
Fujii, Yohei [1 ]
Uchiya, Hiroshi [1 ]
Nakazawa, Manabu [1 ]
Ando, Satsuki [1 ]
Nakao, Masamitsu [1 ]
Motoya, Daisuke [1 ]
Sugawara, Kayoko [1 ]
Inao, Mie [1 ]
Imai, Yukinori [1 ]
Nakayama, Nobuaki [1 ]
Tomiya, Tomoaki [1 ]
Mochida, Satoshi [1 ]
机构
[1] Saitama Med Univ, Dept Gastroenterol & Hepatol, Fac Med, 38 Morohongo, Moroyama, Saitama 3500495, Japan
关键词
asunaprevir; daclatasvir; interferon-; ledipasvir; NS5A-RAS; sofosbuvir; RESISTANCE-ASSOCIATED VARIANTS; JAPANESE PATIENTS; ANTIVIRAL ACTIVITY; NS5A INHIBITORS; RIBAVIRIN; SOFOSBUVIR; BETA; DACLATASVIR; LEDIPASVIR; INDUCTION;
D O I
10.1111/hepr.12980
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
AimTo improve the therapeutic efficacy of sofosbuvir/ledipasvir (SOF/LDV) for the retreatment of patients after daclatasvir/asunaprevir (DCV/ASV), a customized therapy with or without lead-in interferon (IFN)- injections was formulated according to the types of resistance-associated substitutions (RAS) in the non-structural protein (NS)5A region of genotype 1b hepatitis C virus (HCV). MethodsThirty-three patients failing prior DCV/ASV received SOF/LDV for 12weeks. Patients with HCV carrying unfavorable NS5A-RAS and/or those previously treated with simeprevir were given lead-in IFN- injections twice a day for 2weeks; sequential changes in the NS5A-RAS during the injection period were evaluated using deep sequencing. ResultsLead-in injections were not undertaken in 27 patients; a sustained viral response (SVR) was achieved in 26 patients, while viral relapse occurred in 1 patient with HCV carrying NS5A-L28M/R30H/Y93H mutations. Among the 6 patients receiving lead-in injections, viral relapse occurred in 2 patients who had an unfavorable IFN-3-related gene single nucleotide polymorphism allele; both patients had been previously treated with simeprevir, and HCV carrying NS5A-L31V/Y93H mutations had emerged after DCV/ASV. Deep sequencing revealed no changes in the NS5A-RAS profiles during the lead-in injection period in either patient. In contrast, in a patient with a favorable allele who was infected with similar unfavorable HCV strains, NS5A-L31/Y93 wild-type strains appeared during the injection period, enabling an SVR. ConclusionUsing customized therapies based on the NS5A-RAS profiles, a high SVR rate was obtained after SOF/LDV in patients failing prior DCV/ASV. Lead-in IFN- injections did not improve the efficacy in patients with HCV carrying unfavorable NS5A-RAS except in those with a favorable IFN-3-related gene allele.
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收藏
页码:233 / 243
页数:11
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