[Analysis of the incidence of low viral load/low-level viremia and its associated factors in patients with HBV-related primary liver cancer].

Q3 Medicine
K Y Hao, Y Dong, Y Fan, X Jiang, X Xiong, L Gao, Z H Wang, P Li, Y C Yu
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引用次数: 0

Abstract

Objective: To retrospectively analyze the viral levels and associated factors in patients with hepatitis B virus (HBV)-related primary liver cancer (PHC) in real-world settings and further explore the correlation between low viral load (LVL) and/or low-level viremia (LLV) and PHC. Methods: Five hundred twenty-four cases with HBV-related PHC with complete pathologically confirmed data from 2013 to 2020 were included. Percentages (%) were used to express their viral load, antiviral (oral) status, patient compliance, presence or absence of cirrhosis, family history of liver cancer, and others. LVL definition: After excluding detection errors by PCR method, serum HBV DNA <50-2 000 IU/ml, and those who had received antiviral drug treatment were called LLV. Antiviral treatment (AVT) rate definition: As of the confirmed diagnosis of PHC, those who had been regularly treated using oral antiviral drugs for six months or more (≥6 months). Results: General situation: The ratio of male to female enrolled patients was 15.90:1 (493/31). Patients aged >40 years accounted for 91.98% (482 cases). Hepatitis B surface antigen (HBsAg) positivity condition: The ratio of HBsAg-positive to HBsAg-negative/anti-HBc-positive (HBsAg-/anti-HBc+) PHC patients was 5.89:1 (448/76). Among the 76 HBsAg-/anti-HBc+patients, the ratio of HBsAg-/anti-HBs+/anti-HBc+ to HBsAg-/anti-HBs-/anti-HBc+ patients was 0.95:1 (37/39). Hepatitis B e antigen (HBeA) positivity condition: The ratio of HBeAg-negative to HBeAg-positive cases was 3.23:1 (400/124). HBV DNA level condition: The medical history records of 75.00% of patients (393/524) had traceable HBV DNA test reports. Out of 393 patients, 45.04% (177/393) accounted for undetectable HBV DNA, 13.49% (53/393) accounted for LVL, 41.48% (163/393) accounted for HBV DNA exceeding the upper limit of LVL, and 4.07% (16/393) accounted for LLV. Among HBsAg-positive and HBsAg-/anti-HBc+ patients, the HBV DNA positivity rates were 59.12% (214/362) and 6.45% (2/31), respectively. Antiviral treatment condition: Among the 448 HBsAg-positive PHC patients, the total AVT rate was 18.08% (81/448), of which seven patients did not have their HBV DNA results traced back. Among them, the AVT rate of 148 patients with HBV DNA lower than the lowest detection value was 41.22% (61/148); the AVT rate of 53 patients with LVL was 18.87% (10/53); and the AVT rate of 163 patients with HBV DNA≥LVL upper limit was 1.84% (3/163). Liver cirrhosis and family history condition: 348 patients (66.41%) had liver cirrhosis. 67 patients (12.79%) had a distinct family history of HBV-related liver cirrhosis and liver cancer. Alpha-fetoprotein (AFP) condition: 514 patients underwent AFP testing, with 30.93% of the patients had normal AFP levels, and 69.07% had AFP levels exceeding the upper limit of normal values (355/514). Among them, 10 μg/L400 μg/L accounted for 34.44% (177/514) and 34.63% (178/514), respectively. Tissue typing condition: 99.05% (519/524) were hepatocellular carcinoma, and well-differentiated and moderately differentiated cases accounted for only 8.59%. Conclusions: In the real world, comprehensive, timely screening, standardized, and effective antiviral treatment have not yet been achieved for patients with chronic hepatitis B, resulting in the persistence of HBsAg and/or HBV DNA positivity (especially LVL and/or LLV). Although LVL does not account for a high proportion among all HBV-related PHC populations, the vast majority of LVL populations have not received any antiviral treatment. In addition, some PHC populations with HBV DNA>2 000 IU/ml have not received standard antiviral treatment before the onset of the disease, which should be paid attention to. At the same time, HBsAg-/anti-HBc+ populations may have latent HBV infection and may even progress to PHC. Notably, PHC may still occur after HBeAg seronegative conversion.

[分析 HBV 相关原发性肝癌患者低病毒载量/低水平病毒血症的发生率及其相关因素]。
目的回顾性分析现实世界中与乙型肝炎病毒(HBV)相关的原发性肝癌(PHC)患者的病毒水平和相关因素,进一步探讨低病毒载量(LVL)和/或低水平病毒血症(LLV)与原发性肝癌之间的相关性。研究方法纳入 2013 年至 2020 年期间病理证实数据完整的 524 例 HBV 相关 PHC 病例。用百分比(%)表示其病毒载量、抗病毒(口服)情况、患者依从性、有无肝硬化、肝癌家族史等。LVL 定义:排除 PCR 方法的检测误差后,血清 HBV DNA 结果:总体情况:男女患者比例为 15.90:1(493/31)。年龄大于 40 岁的患者占 91.98%(482 例)。乙型肝炎表面抗原(HBsAg)阳性情况:HBsAg 阳性与 HBsAg 阴性/抗-HBc 阳性(HBsAg-/抗-HBc+)的初级保健患者比例为 5.89:1(448/76)。在 76 名 HBsAg-/anti-HBc+ 患者中,HBsAg-/anti-HBs+/anti-HBc+ 与 HBsAg-/anti-HBs-/anti-HBc+ 的比例为 0.95:1(37/39)。乙型肝炎 e 抗原(HBeA)阳性情况:HBeAg 阴性与 HBeAg 阳性病例的比例为 3.23:1(400/124)。HBV DNA 水平情况:75.00%的患者(393/524)的病史记录中有可追溯的 HBV DNA 检测报告。在 393 名患者中,45.04%(177/393)的患者检测不到 HBV DNA,13.49%(53/393)的患者检测到 LVL,41.48%(163/393)的患者检测到 HBV DNA 超过 LVL 上限,4.07%(16/393)的患者检测到 LLV。在 HBsAg 阳性和 HBsAg-/anti-HBc+ 患者中,HBV DNA 阳性率分别为 59.12%(214/362)和 6.45%(2/31)。抗病毒治疗情况:在 448 名 HBsAg 阳性的 PHC 患者中,总的 AVT 率为 18.08%(81/448),其中 7 名患者的 HBV DNA 结果未被追溯。其中,148 例 HBV DNA 低于最低检测值患者的 AVT 率为 41.22%(61/148);53 例 LVL 患者的 AVT 率为 18.87%(10/53);163 例 HBV DNA≥LVL 上限患者的 AVT 率为 1.84%(3/163)。肝硬化和家族史情况:348名患者(66.41%)患有肝硬化。67名患者(12.79%)有明显的 HBV 相关肝硬化和肝癌家族史。甲胎蛋白(AFP)情况:514名患者接受了甲胎蛋白检测,30.93%的患者甲胎蛋白水平正常,69.07%的患者甲胎蛋白水平超过正常值上限(355/514)。其中,10 μg/L400 μg/L 分别占 34.44%(177/514)和 34.63%(178/514)。组织分型情况:99.05%(519/524)为肝细胞癌,分化良好和中度分化的病例仅占 8.59%。结论在现实世界中,慢性乙型肝炎患者尚未得到全面、及时的筛查、规范和有效的抗病毒治疗,导致 HBsAg 和/或 HBV DNA 阳性(尤其是 LVL 和/或 LLV)持续存在。尽管在所有与 HBV 相关的 PHC 群体中,LVL 所占比例并不高,但绝大多数 LVL 群体都没有接受过任何抗病毒治疗。此外,一些 HBV DNA>2 000 IU/ml 的 PHC 群体在发病前并未接受过标准的抗病毒治疗,这一点应引起重视。同时,HBsAg-/抗-HBc+人群可能存在潜伏的 HBV 感染,甚至可能发展为 PHC。值得注意的是,HBeAg 血清阴性转阴后仍可能发生 PHC。
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来源期刊
中华肝脏病杂志
中华肝脏病杂志 Medicine-Medicine (all)
CiteScore
1.20
自引率
0.00%
发文量
7574
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