大剂量替诺福韦对肝细胞癌进展患者抑制乙型肝炎病毒复制无效:初步结果

Shin Hwang, G. Song, D. Jung, Y. Yoon, H. Yoo, E. Tak
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引用次数: 1

摘要

背景/目的核苷类似物(NUCs)可以有效抑制乙型肝炎病毒(HBV)的复制,但尽管NUC治疗,肝细胞癌(HCC)复发往往导致HBV复制。本研究的目的是确定大剂量替诺福韦(TNF)治疗是否可以抑制HCC复发相关的HBV复制。方法我们进行了一项单臂前瞻性研究,以评估高剂量TNF (hdTNF)的临床可行性。我们于2015年9月招募10例患者,随访3个月或提前退出。结果10例患者均为晚期肝癌,均为肝癌复发和逐渐进展。患者平均年龄51.2±4.7岁,男性9例。3例患者不能耐受TNF剂量的增加,早期退出治疗。另外7例患者对每天增加TNF - 5片剂的剂量相对耐受。一名患者有轻微的胃肠道症状,另一名患者主诉失眠。尽管hdTNF持续4-8周,但观察到HBV复制增加和HCC进展。随访3个月,7例患者均出现肿瘤进展。在这些患者中,hdTNF前血液HBV DNA为50-200拷贝/ml;在hdTNF治疗4-8周后,血液HBV DNA为50-300拷贝/ml, HBV复制状态未得到改善。在证实这些阴性结果后,该临床研究被提前终止。结论:本研究结果表明,相当一部分患者不能耐受高达推荐剂量5倍的高剂量TNF,并且对抑制HCC进展相关的HBV复制无效。
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High-dose tenofovir is not effective in suppressing hepatitis B virus replication in patients with hepatocellular carcinoma progression: a preliminary result
Backgrounds/Aims Nucleos(t)ide analogues (NUCs) effectively suppress hepatitis B virus (HBV) replication, but hepatocellular carcinoma (HCC) recurrence often leads to HBV replication despite NUC therapy. The aim of this study was to determine whether high-dose tenofovir (TNF) therapy can suppresses HCC recurrence-associated HBV replication. Methods We performed a single-arm prospective study to assess the clinical feasibility of high-dose TNF (hdTNF). We recruited 10 patients during September 2015 and followed up for 3 months or early drop-out. Results All 10 patients had HCC of advanced stages due to HCC recurrence and gradual progression. The average age of patients was 51.2±4.7 years and 9 were male. Three patients did not tolerate the increased TNF dosage and were dropped out early. The other 7 patients were relatively tolerable to the increased dosage of TNF 5 tablets per day. One patient had mild gastrointestinal symptoms and another patient complained of insomnia. Increased HBV replication and HCC progression was observed despite hdTNF for 4-8 weeks. All 7 patients showed tumor progression during the 3 month follow-up. In these patients, blood HBV DNA before hdTNF was 50-200 copies/ml; and 4-8 weeks after hdTNF, the HBV replication status was not improved with blood HBV DNA of 50-300 copies/ml. This clinical study was terminated early after these negative results were confirmed. Conclusions The results of this study indicated that high dose of TNF up to 5-fold the recommended dosage is not tolerated by a considerable proportion of patients and also ineffective in suppressing HCC progression-associated HBV replication.
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