Disease modifiers and novel markers in hepatitis B virus-related hepatocellular carcinoma.

Journal of liver cancer Pub Date : 2024-09-01 Epub Date: 2024-08-05 DOI:10.17998/jlc.2024.08.03
Lung-Yi Mak
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Abstract

Chronic hepatitis B (CHB) infection is responsible for 40% of the global burden of hepatocellular carcinoma (HCC) with a high case fatality rate. The risk of HCC differs among CHB subjects owing to differences in host and viral factors. Modifiable risk factors include viral load, use of antiviral therapy, co-infection with other hepatotropic viruses, concomitant metabolic dysfunctionassociated steatotic liver disease or diabetes mellitus, environmental exposure, and medication use. Detecting HCC at early stage improves survival, and current practice recommends HCC surveillance among individuals with cirrhosis, family history of HCC, or above an age cut-off. Ultrasonography with or without serum alpha feto-protein (AFP) every 6 months is widely accepted strategy for HCC surveillance. Novel tumor-specific markers, when combined with AFP, improve diagnostic accuracy than AFP alone to detect HCC at an early stage. To predict the risk of HCC, a number of clinical risk scores have been developed but none of them are clinically implemented nor endorsed by clinical practice guidelines. Biomarkers that reflect viral transcriptional activity and degree of liver fibrosis can potentially stratify the risk of HCC, especially among subjects who are already on antiviral therapy. Ongoing exploration of these novel biomarkers is required to confirm their performance characteristics, replicability and practicability.

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与 HBV 相关的 HCC 中的疾病调节因子和新型标记物。
慢性乙型肝炎(CHB)感染占全球肝细胞癌(HCC)发病率的 40%,且病死率很高。由于宿主和病毒因素的不同,慢性乙型肝炎患者患 HCC 的风险也不同。可改变的风险因素包括病毒载量、使用抗病毒治疗、合并感染其他致肝病毒、合并代谢功能障碍相关的脂肪性肝病或糖尿病、环境暴露和药物使用。早期发现 HCC 可提高存活率,目前的做法是建议对肝硬化患者、有 HCC 家族史或年龄超过某一界限的患者进行 HCC 监测。每 6 个月进行一次超声波检查,同时检测或不检测血清甲胎蛋白是广为接受的 HCC 监测策略。新型肿瘤特异性标记物与甲胎蛋白结合后,比单独使用甲胎蛋白能提高诊断准确性,从而在早期发现 HCC。为预测 HCC 风险,已开发出一些临床风险评分,但这些评分均未在临床上实施,也未得到临床实践指南的认可。反映病毒转录活性和肝纤维化程度的生物标志物有可能对HCC风险进行分层,尤其是在已经接受抗病毒治疗的受试者中。需要对这些新型生物标记物进行持续探索,以确认其性能特征、可复制性和实用性。
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