HBV相关慢加急性肝衰竭恢复期患者肝组织HBV cccDNA水平及其临床意义

目的观察HBV cccDNA在HBV相关慢加急性肝衰竭(HBV-ACLF)恢复期患者肝组织中的表达水平,并探讨其与HBV标志物、肝组织病理改变的关系。方法选取2015年1月—2023年10月在南昌市第九医院住院的HBV-ACLF恢复期患者30例为肝衰竭组,另选取同期9例性别及年龄匹配的慢性乙型肝炎患者(CHB)作为对照组,检测肝组织HBV cccDNA水平,并分析其与临床资料、实验室检查指标的关联性。计量资料两组间比较采用成组t检验或Mann-Whitney U检验;多组间比较采用单因素方差分析或Kruskal-Wallis H检验。计数资料组间比较采用Fisher精确检验。相关性分析采用Spearman相关分析。结果肝衰竭组肝组织HBV cccDNA水平显著低于对照组[(−0.92±0.70)log10 copies/cell vs(−0.13±0.91)log10 copies/cell,t=2.761,P=0.009]。肝衰竭组中,血清HBeAg阳性与阴性患者肝组织HBV cccDNA水平比较,差异无统计学意义(P>0.05);肝组织炎症活动度G0~G2级、G3级、G4级患者的肝组织HBV cccDNA水平比较,差异无统计学意义(P>0.05);肝组织纤维化程度S0~S2期、S3期、S4期患者的肝组织HBV cccDNA水平比较,差异无统计学意义(P>0.05);血清HBV DNA阴性与血清HBV DNA阳性患者肝组织HBV cccDNA水平比较,差异无统计学意义(P>0.05)。肝衰竭组肝组织HBV cccDNA水平与肝组织HBV DNA水平呈正相关(r=0.426,P=0.043),与血清HBV DNA水平无明显相关性(P>0.05)。结论肝组织HBV cccDNA水平在HBV-ACLF恢复期明显降低,肝组织HBV cccDNA持续稳定存在,较血清及肝组织HBV DNA更能反映HBV的持续感染与复制。

低病毒载量HBeAg阴性不确定期慢性HBV感染者肝组织病理分析

目的分析低病毒载量HBeAg阴性不确定期慢性HBV感染者肝组织病理特征。方法选取2013年9月—2021年6月于延安大学附属医院感染病科行肝组织活检的271例低病毒载量HBeAg阴性慢性HBV感染者作为研究对象,比较不同年龄、性别、乙型肝炎家族史、HBsAg及ALT水平患者的肝组织损伤程度。计数资料两组间比较采用χ2检验。结果271例HBeAg阴性慢性HBV感染者中86例(31.73%)肝组织炎症活动度≥A2、72例(26.57%)肝纤维化分期≥F2,112例(41.33%)患者存在中、重度肝组织损伤。ALT>20 U/L患者中肝组织炎症活动度≥A2比例高于ALT≤20 U/L患者,差异有统计学意义(χ2=3.938,P=0.047)。不同年龄、性别、乙型肝炎家族史、HBsAg水平患者的肝组织炎症活动度≥A2比例差异均无统计学意义(P值均>0.05);不同年龄、性别、乙型肝炎家族史、HBsAg水平、ALT水平患者的肝纤维化分期≥F2比例差异均无统计学意义(P值均>0.05);进一步对年龄≤30岁和无乙型肝炎家族史患者进行分层分析,结果显示肝组织炎症活动度≥A2比例和肝纤维化分期≥F2比例的组间差异亦无统计学意义(P值均>0.05)。不同年龄、性别、乙型肝炎家族史、HBsAg水平、ALT水平等临床特征患者的肝组织损伤程度差异均无统计学意义(P值均>0.05)。结论超过40%的低病毒载量HBeAg阴性慢性HBV感染者肝组织存在显著损伤,不同年龄、性别、乙型肝炎家族史、HBsAg及ALT水平患者的肝组织损伤程度未见明显差异,即使年龄<30岁否认乙型肝炎家族史,患者仍有相当比例的肝组织存在损伤,需要引起临床医师的重视。

鱼腥草素钠抗HBV作用及分子机制初步研究

目的 探究鱼腥草素钠抗乙型肝炎病毒(HBV)活性,并对其潜在的相关分子机制进行初步探讨。方法MTT法检测鱼腥草素钠对HepG2.2.15细胞的毒性;ELISA法及免疫细胞化学(ICC)检测细胞内外HBsAg及HBeAg的水平;qPCR检测细胞上清中HBV DNA含量,细胞内HBV DNA、pgRNA、HBV cccDNA及抗病毒基因的表达;Western blot检测细胞内OAS1基因的表达。结果 鱼腥草素钠质量浓度在5~20μg/mL范围内对HepG2.2.15细胞无细胞毒性,ELISA及ICC结果显示鱼腥草素钠可显著降低细胞上清中HBsAg、HBeAg的水平,抑制胞内HBsAg、HBeAg的表达;qPCR结果显示鱼腥草素钠可下调细胞内HBV DNA、pgRNA及HBV cccDNA的表达,上调抗病毒相关基因PKR、STAT2及IRF9的表达,并上调OAS1基因及蛋白的表达。结论 鱼腥草素钠可降低HepG2.2.15细胞中HBsAg等病毒抗原的水平,抑制HBV复制相关基因的表达;其抗HBV作用机制可能与激活JAK-STAT信号通路、升高抗病毒蛋白表达量有关。

Current status of drug therapy for chronic hepatitis B

In this editorial,we comment on the article by Meng et al.Chronic hepatitis B(CHB)is a significant global health problem,particularly in developing countries.Hepatitis B virus(HBV)infection is one of the most important risk factors for cirrhosis and hepatocellular carcinoma.Prevention and treatment of HBV are key measures to reduce complications.At present,drug therapy can effectively control virus replication and slow disease progression,but completely eliminating the virus remains a challenge.Anti-HBV treatment is a long-term process,and there are many kinds of antiviral drugs with different mechanisms of action,it is essential to evaluate the safety and efficacy of these drugs to reduce side effects and improve patients’compliance.We will summarize the current status of CHB drug treatment,hoping to provide a reference for the selection of clinical antiviral drugs.

Antiviral therapy for hepatitis B virus infection is beneficial for the prognosis hepatocellular carcinoma

In this editorial,we comment on the article by Mu et al,published in the recent issue of the World Journal of Gastrointestinal Oncology.We pay special attention to the immune tolerance mechanism caused by hepatitis B virus(HBV)infection,the pathogenesis of hepatocellular carcinoma(HCC),and the role of antiviral therapy in treating HCC related to HBV infection.HBV infection leads to systemic innate immune tolerance by directly inhibiting pattern recognition receptor recognition and antiviral signaling pathways,as well as by inhibiting the immune functions of macrophages,natural killer cells and dendritic cells.In addition,HBV leads to an immunosuppressive cascade by expressing inhibitory molecules to induce exhaustion of HBV-specific cluster of differentiation 8+T cells,ultimately leading to long-term viral infection.The loss of immune cell function caused by HBV infection ultimately leads to HCC.Long-term antiviral therapy can improve the prognosis of patients with HCC and prevent tumor recurrence and metastasis.

Gut microbiota shifts in hepatitis B-related portal hypertension after transjugular intrahepatic portosystemic shunt:Mechanistic and clinical implications

In this article,we provide commentary on the recent article by Zhao et al.We focus on the shifts in the gut microbiota of patients with hepatitis B virus(HBV)-associated cirrhosis/portal hypertension(PH)following transjugular intrahepatic portosystemic shunt(TIPS)and the implications for understanding the mechanisms,diagnosis,and treatment.By comparing the gut microbiota composition and dynamic changes before and after TIPS in patients with and without hepatic encephalopathy,the authors found an increase in non-probiotic bacteria in those who developed hepatic encephalopathy post-TIPS,with Morganella species present only in the hepatic encephalopathy group.The gut microbiota changes post-TIPS among patients without the occurrence of hepatic encephalopathy suggest potential therapeutic benefits through prophylactic microbiome therapies.Furthermore,the specific gut microbiota alterations may hold promise to predict the risk of hepatic encephalopathy in individuals undergoing TIPS for HBVrelated PH.Despite these promising findings,future studies are needed to address limitations,including a small sample size,a relatively short evaluation period for gut microbiota alterations,the absence of data on dynamic alterations in gut microbiota post-TIPS and their correlation with blood ammonia levels,and the lack of validation in animal models.In conclusion,Zhao et al's study has shed new light on the link of gut microbiota with post-TIPS hepatic encephalopathy,potentially through the intricate gut-liver axis,and has important clinical implications for improving the management of patients with HBV-related PH.

芍药苷对HBV感染引起小鼠肝组织损伤的保护作用及机制探讨

目的探讨芍药苷(PF)对乙型肝炎病毒(HBV)感染引起的肝组织损伤的作用及机制。方法2022年6月至2023年1月,将40只C57BL/6小鼠按随机数字表法分为假手术(Sham)组、HBV组、5 mg/kg PF组和10 mg/kg PF组,每组10只。除对照组外,其余各组小鼠通过尾静脉注射重组腺病毒载体构建AAV8-1.3HBV感染模型。于造模前24 h至造模后5周,每日为小鼠灌胃给予不同剂量的PF溶液或等体积溶剂。随后,采用生化分析法检测小鼠血清天冬氨酸转氨酶(AST)和丙氨酸转氨酶(ALT)水平;酶联免疫吸附测定(ELISA)检测小鼠血清乙型肝炎e抗原(HBeAg)和乙型肝炎表面抗原(HbsAg)水平;苏木精-伊红(HE)染色检测小鼠肝组织病理变化;Masson染色检测肝组织纤维化情况;ELISA检测小鼠肝组织乳酸脱氢酶(LDH)、白细胞介素-1β(IL-1β)和白细胞介素-18(IL-18)水平;原位末端转移酶标记法(TUNEL)检测小鼠肝组织细胞凋亡情况;蛋白质印迹法检测小鼠肝组织焦亡相关蛋白核因子-κB(NF-κB)、Nod样受体蛋白3(NLRP3)及焦孔素D(GSDMD)的表达。结果Sham组血清AST(44.89±7.82)U/L、ALT为(43.13±5.72)U/L,HBeAg和HbsAg无表达,HBV组AST、ALT、HBeAg和HbsAg分别为(98.76±12.21)U/L、(75.38±1.23)U/L、(52.22±7.15)U/L、(67.33±9.25)U/L,HBV组小鼠各指标显著升高(P<0.05);与Sham组比较,HBV组肝组织内细胞形态发生明显改变,炎性细胞浸润明显,出现大量肝纤维化;HBV组肝组织LDH、IL-1β、IL-18显著高于Sham组(P<0.05),HBV组细胞凋亡明显增加,HBV组NF-κB、NLRP3、GSDMD表达,显著高于Sham组(P<0.05)。与HBV组比较,5 mg/kg PF组和10 mg/kg PF组小鼠血清AST、ALT、HBeAg和HbsAg水平显著降低(P<0.05);肝组织病理损伤明显减轻,肝纤维化程度改善;肝组织LDH、IL-1β及IL-18水平显著降低,细胞凋亡明显降低,NF-κB、NLRP3及GSDMD蛋白表达显著下调(均P<0.05),5 mg/kg PF组和10 mg/kg PF组之间差异有统计学意义(P<0.05)。结论PF可通过调控NLRP3介导的细胞焦亡减轻HBV感染引起的肝组织损伤,PF对HBV感染引起小鼠肝组织损伤有保护作用。

Exploring the performance of large language models on hepatitis B infection-related questions:A comparative study

BACKGROUND Patients with hepatitis B virus(HBV)infection require chronic and personalized care to improve outcomes.Large language models(LLMs)can potentially provide medical information for patients.AIM To examine the performance of three LLMs,ChatGPT-3.5,ChatGPT-4.0,and Google Gemini,in answering HBV-related questions.METHODS LLMs’responses to HBV-related questions were independently graded by two medical professionals using a four-point accuracy scale,and disagreements were resolved by a third reviewer.Each question was run three times using three LLMs.Readability was assessed via the Gunning Fog index and Flesch-Kincaid grade level.RESULTS Overall,all three LLM chatbots achieved high average accuracy scores for subjective questions(ChatGPT-3.5:3.50;ChatGPT-4.0:3.69;Google Gemini:3.53,out of a maximum score of 4).With respect to objective questions,ChatGPT-4.0 achieved an 80.8%accuracy rate,compared with 62.9%for ChatGPT-3.5 and 73.1%for Google Gemini.Across the six domains,ChatGPT-4.0 performed better in terms of diagnosis,whereas Google Gemini demonstrated excellent clinical manifestations.Notably,in the readability analysis,the mean Gunning Fog index and Flesch-Kincaid grade level scores of the three LLM chatbots were significantly higher than the standard level eight,far exceeding the reading level of the normal population.CONCLUSION Our results highlight the potential of LLMs,especially ChatGPT-4.0,for delivering responses to HBV-related questions.LLMs may be an adjunctive informational tool for patients and physicians to improve outcomes.Nevertheless,current LLMs should not replace personalized treatment recommendations from physicians in the management of HBV infection.

乙型肝炎患者血清lncRNA XIST表达与HBV-DNA载量、肝纤维化的关系

目的 探讨乙型肝炎患者血清长链非编码RNA X染色体失活特异转录本(lncRNA XIST)表达与乙肝病毒脱氧核糖核酸(HBV-DNA)载量、肝纤维化的关系。方法 选取2020年6月—2022年6月黄冈市中心医院收治的87例乙型肝炎患者作为乙肝组,另取同期该院健康体检者71例作为对照组。所有纳入对象均检测血清lncRNA XIST表达与HBV-DNA载量及肝纤维化指标[透明质酸(HA)、层粘连蛋白(LN)、Ⅳ型胶原(Ⅳ-C)、Ⅲ型前胶原(PC-Ⅲ)]。采用Pearson相关分析探讨血清lncRNA XIST与HBV DNA载量、肝纤维化指标的关系,采用受试者工作特征(ROC)曲线分析血清lncRNA XIST对乙型肝炎的诊断价值。结果 乙肝组血清TBil、ALT、AST、lncRNA XIST、HA、LN、Ⅳ-C、PC-Ⅲ水平均高于对照组(P <0.05)。高载量组乙型肝炎患者血清lncRNA XIST及HA、LN、Ⅳ-C、PC-Ⅲ水平均高于中、低载量组(P <0.05);中载量组乙型肝炎患者血清lncRNA XIST及HA、LN、Ⅳ-C、PC-Ⅲ水平均高于低载量组(P <0.05)。Pearson相关分析结果显示,乙型肝炎患者血清lncRNA XIST相对表达量与HBV-DNA载量、HA、LN、Ⅳ-C、PC-Ⅲ均呈正相关(r=0.445、0.420、0.369、0.330和0.419,均P=0.000)。ROC曲线结果显示,血清lncRNA XIST诊断乙型肝炎的敏感性为80.65%(95%CI:0.801,0.811),特异性为88.74%(95%CI:0.866,0.908)。结论 乙型肝炎患者血清lncRNA XIST表达升高,且随着HBV-DNA载量增加而逐渐上升,同时与肝纤维化密切相关,有望作为临床诊断乙型肝炎的有效指标。

C-X-C chemokine receptor type 5+CD8+T cells as immune regulators in hepatitis Be antigen-positive chronic hepatitis B under interferonalpha treatment

BACKGROUND C-X-C chemokine receptor type 5(CXCR5)^(+)CD8^(+)T cells represent a unique immune subset with dual roles,functioning as cytotoxic cells in persistent viral infections while promoting B cell responses.Despite their importance,the specific role of CXCR5^(+)CD8^(+)T cells in chronic hepatitis B(CHB),particularly during interferon-alpha(IFN-α)treatment,is not fully understood.This study aims to elucidate the relationship between CXCR5^(+)CD8^(+)T cells and sustained serologic response(SR)in patients undergoing 48 weeks of pegylated IFN-α(peg-IFN-α)treatment for CHB.AIM To elucidate the relationship between CXCR5^(+)CD8^(+)T cells and sustained SR in patients undergoing 48 weeks of peg-IFN-αtreatment for CHB.METHODS This study enrolled 60 patients with hepatitis Be antigen(HBeAg)-positive CHB undergoing 48 weeks of peg-IFN-αtreatment.Participants were assessed for eligibility based on criteria such as persistent HBsAg-positive status for at least six months,HBeAb-negative,hepatitis B virus DNA levels exceeding 2×10^(4) copies/mL,and alanine aminotransferase(ALT)levels between 2 and 10 times the upper limit of normal.Blood samples were collected at baseline and at weeks 12,24,48,and a 24-week treatment-free follow-up(week 72)to measure serum interleukin(IL)-21 concentration via ELISA and to analyze CXCR5 and programmed death-ligand 1(PD-L1)expression on CD8^(+)T cells by flow cytometry,CXCR5 is a chemokine receptor that directs immune cells to specific tissues,while PD-L1 is a protein that regulates immune responses by inhibiting T cell activity.RESULTS Patients with CHB exhibited significantly lower levels of circulating CXCR5^(+)CD8^(+)T cells compared to healthy controls(P<0.01).Notably,CXCR5^(+)CD8^(+)T cells were prominently expressed in patients who achieved sustained SR compared to non-SR(NSR).A significant correlation was observed between CXCR5 and PD-L1 expression(r=-0.189,P=0.002).However,there was no significant correlation between serum IL-21 levels and CXCR5+CD8+lymphocytes(r=-0.03,P=0.625)or serum ALT levels(r=0.026,P=0.678).CONCLUSION The enhanced expression of CXCR5^(+)CD8^(+)T cells in patients achieving HBeAg seroconversion during IFN-αtreatment suggests that these cells play a crucial role in antiviral immune responses against hepatitis B.This study highlights the potential of CXCR5^(+)CD8^(+)T cells as immune regulators in CHB,which may inform future therapeutic strategies to optimize antiviral treatments.

Trends of alkaline phosphatase to prealbumin ratio in patients with hepatitis B linked to hepatocellular carcinoma development

BACKGROUND Chronic hepatitis B often progresses silently toward hepatocellular carcinoma(HCC),a leading cause of mortality worldwide.Early detection of HCC is crucial,yet challenging.AIM To investigate the role of dynamic changes in alkaline phosphatase to prealbumin ratio(APR)in hepatitis B progression to HCC.METHODS Data from 4843 patients with hepatitis B(January 2015 to January 2024)were analyzed.HCC incidence rates in males and females were compared using the log-rank test.Data were evaluated using Kaplan–Meier analysis.The Linear Mixed-Effects Model was applied to track the fluctuation of APR levels over time.Furthermore,Joint Modeling of Longitudinal and Survival data was employed to investigate the temporal relationship between APR and HCC risk.RESULTS The incidence of HCC was higher in males.To ensure the model’s normality assumption,this study applied a logarithmic transformation to APR,yielding ratio.Ratio levels were higher in females(t=5.26,P<0.01).A 1-unit increase in ratio correlated with a 2.005-fold higher risk of HCC in males(95%CI:1.653-2.431)and a 2.273-fold higher risk in females(95%CI:1.620-3.190).CONCLUSION Males are more prone to HCC,while females have higher APR levels.Despite no baseline APR link,rising APR indicates a higher HCC risk.

ALT正常的慢性HBV感染患者口服核苷(酸)类似物病毒学应答的预测模型建立

目的:探讨口服核苷(酸)类似物的丙氨酸转移酶(ALT)正常的慢性乙型肝炎病毒(HBV)感染患者的病毒学应答的预测因素,及其列线图预测模型的建立。方法:选取2020年2月至2024年2月沧州市中心医院收治的ALT正常的慢性HBV感染患者200例,根据血清HBV脱氧核糖核酸(DNA)含量将病毒学应答模式分为完全病毒学应答组(n=124)和部分病毒学应答组(n=76),收集人口学特征参数、基本临床情况及各实验室指标,采用Logistic回归模型分析部分病毒学应答的危险因素,构建部分病毒学应答列线图风险预测模型并验证其效能。结果:相较于完全病毒学应答组,部分病毒学应答组患者乙型肝炎e抗原(HBeAg)阳性占比、服药依从性“差”占比,HBV DNA、乙型肝炎表面抗原(HBsAg)水平显著升高,白蛋白水平显著降低,差异均有统计学意义(P<0.05);但两组患者在体重指数、年龄、性别、乙型病毒性肝炎家族史、高血压史、糖尿病史、抗病毒药物类型、吸烟史和饮酒史,乙型肝炎核心抗体、血尿素氮、血肌酐、血尿酸、总胆红素、碱性磷酸酶、三酰甘油、总胆固醇、空腹血糖、白细胞计数、中性粒细胞计数、血小板计数和肝硬度值方面的差异均无统计学意义(P>0.05)。Logistic回归分析显示,HBV DNA水平高、HBsAg水平高、HBeAg阳性、白蛋白水平低和服药依从性“差”是部分病毒学应答的危险因素(P<0.05)。基于上述危险因素(服药依从性、HBeAg状态,HBV DNA、HBsAg和白蛋白水平)构建部分病毒学应答的列线图风险模型,模型C指数为0.796(95%CI=0.713~0.860),ROC曲线下面积为0.857(95%CI=0.802~0.911),特异度为85.30%,灵敏度为74.40%。结论:服药依从性“差”、HBeAg阳性、HBV DNA水平升高、HBsAg水平升高和白蛋白水平降低是ALT正常的慢性HBV感染患者部分病毒学应答的独立预测因子,基于此构建的列线图预测模型有着较高的预测效能。

Hepatitis B core-related antigen as a promising serological marker for monitoring hepatitis B virus cure

Hepatitis B virus(HBV)infection is a global health concern.The current sequen-tial endpoints for the treatment of HBV infection include viral suppression,hepatitis B e antigen(HBeAg)seroconversion,functional cure,and covalently closed circular DNA(cccDNA)clearance.Serum hepatitis B core-related antigen(HBcrAg)is an emerging HBV marker comprising three components:HBeAg,hepatitis B core antigen,and p22cr.It responds well to the transcriptional activity of cccDNA in the patient's liver and is a promising alternative marker for serolo-gical testing.There is a strong correlation,and a decrease in its level corresponds to sustained viral suppression.In patients with chronic hepatitis B(CHB),serum HBcrAg levels are good predictors of HBeAg seroconversion(both spontaneous and after antiviral therapy),particularly in HBeAg-positive patients.Both low baseline HBcrAg levels and decreasing levels early in antiviral therapy favored HBsAg seroconversion,which may serve as a good surrogate option for treatment endpoints.In this review,we summarize the role of serum HBcrAg in the treat-ment of CHB.Therefore,long-term continuous monitoring of serum HBcrAg levels contributes to the clinical management of patients with CHB and optimizes the choice of treatment regimen,making it a promising marker for monitoring HBV cure.

Timing of post-vaccination tests in infants born to mothers with chronic hepatitis B virus infection

Immunoprophylaxis is routinely recommended for infants born to mothers with hepatitis B virus(HBV)infection within the first 12-24 hours.Detection of he-patitis B surface antibody(HBsAb)resulting from hepatitis B immunoglobulin administered at birth may be perceived as a real vaccine response.This makes it difficult to detect HBV infection.For this reason,it is recommended that infants born to hepatitis B surface antigen positive mothers and who received immunop-rophylaxis at birth should have HBsAb testing when they are 9-15 months old.

Clinical features of abnormalα-fetoprotein in 15 patients with chronic viral hepatitis B after treatment with antiviral drugs

BACKGROUND Liver function of chronic hepatitis B(CHB)patients is essentially normal after treatment with antiviral drugs.In rare cases,persistently abnormally elevatedα-fetoprotein(AFP)is seen in CHB patients following long-term antiviral treatment.However,in the absence of imaging evidence of liver cancer,a reasonable expla-nation for this phenomenon is still lacking.AIM To explore the causes of abnormal AFP in patients with CHB who were not diag-nosed with liver cancer.METHODS From November 2019 to May 2023,15 patients with CHB after antiviral treatment and elevated AFP were selected.Clinical data and quality indicators related to laboratory testing,imaging data,and pathological data were obtained through inpatient medical records.RESULTS All patients had increased AFP and significantly elevated IgG.Cancer was excluded by imaging examination.Only four patients had elevated alanine ami-notransferase,10 had elevated aspartate aminotransferase,nine had elevated total bilirubin,and two had antinuclear antibodies.The liver biopsy and histopatho-logical examination indicated that 14 patients had rosette,moderate,or higher interfacial inflammation,lymphocyte infiltration,and severe hepatic fibers(11 cases),which was consistent with the pathological features of autoimmune hepa-titis(AIH).After 8-12 week of hormone therapy,the levels of AFP and IgG,and liver function returned to normal(P<0.05).CONCLUSION For patients with CHB and elevated AFP after antiviral treatment,autoimmune hepatitis should be considered.CHB with AIH is clinically insidious and difficult to detect,and prone to progression to cirrhosis.Liver puncture pathological examination should be performed when necessary to confirm diagnosis.

Hepatitis B virus infection and its treatment in Eastern Ethiopia

Hepatitis B virus(HBV)infection causes acute and chronic hepatitis,compensated and decompensated cirrhosis,and hepatocellular carcinoma worldwide.The actual status of HBV infection and its treatment in certain regions of Asian and African countries,including Ethiopia,has not been well-documented thus far.Antiviral therapy for HBV infection can prevent the progression of HBV-related liver diseases and decrease the HBV-related symptoms,such as abdominal symp-toms,fatigue,systemic symptoms and others.In Eastern Ethiopia,HBV-infected patients with cirrhosis were found to be positive for the HBV e antigen and to have a higher viral load than those without cirrhosis.Notably,54.4%of patients practiced khat chewing and 18.1%consumed excessive amounts of alcohol.Teno-fovir disoproxil fumarate effectively suppressed HBV DNA in those infected with HBV.It is important to elucidate the actual status of HBV infection in Eastern Ethiopia to eliminate HBV infection worldwide by 2030.HBV vaccination and the educational programs for Health Science students that provide practical strategies could help to reduce HBV infection in Eastern Ethiopia.

Prevalence of cardiometabolic co-morbidities in patients with vs persons without chronic hepatitis B: The FitLiver cohort study

BACKGROUND Chronic hepatitis B(CHB)affects>300 million people worldwide.The combi-nation of CHB and cardiometabolic co-morbidities increases the risk of liver-related morbidity and mortality.However,international guidelines for CHB treatment do not provide recommendations for follow-up examinations or treatment of patients with CHB and cardiometabolic comorbidities.In studies investigating cardiometabolic co-morbidity in patients with CHB,inconsistent findings have been observed,and both lower and higher prevalence of car-diometabolic co-morbidities compared to the general population have been re-ported.It is unclear whether patients with CHB living in Denmark have an increased prevalence of cardiometabolic co-morbidities.We examined patients with CHB and age-,sex-,body mass index(BMI)-,and country-of-birth matched comparison group.Defining cardiometabolic co-morbidity:Obesity(BMI>25 kg/m2/abnormal waist-to-hip ratio),metabolic dysfunction-associated steatotic liver disease(MASLD),hypercholesterolemia(total-cholesterol>5 mmol/L/statin use),hypertension(systolic≥135 mmHg/diastolic≥85 mmHg/antihypertensive medication)and type 2 diabetes(T2D)(2-hour oral glucose tolerance test glucose>11.1 mmol/L/HbA1c>48 mmol/mol/antidiabetic medication).Physical activity was evaluated using maximal oxygen consumption(VO2max),activity monitors,and a questionnaire.RESULTS We included 98 patients with CHB and 49 persons in the comparison group.The two groups were well-matched,showing no significant differences in age,sex,BMI,country-of-birth,education,or employment.Among patients with CHB,the following prevalence of cardiometabolic co-morbidity was found:77%were obese,45%had MASLD,38%had hypercholesterolemia,26%had hypertension,and 7%had T2D,which did not differ significantly from the comparison group,apart from lower prevalence of hemoglobin A1c(HbA1c)≥48 mmol/L or known T2D.Both groups had low VO2max of 27 mL/kg/minute in the patients with CHB and 30 mL/kg/minute in the comparison group,and the patients with CHB had a shorter self-assessed sitting time.CONCLUSION The patients with CHB and the comparison group were well-matched and had a similar prevalence of car-diometabolic comorbidities.Furthermore,both groups had low levels of physical fitness.

Evaluating the scope of human leukocyte antigen polymorphisms influencing hepatitis B virus-related liver cancer and cirrhosis through multi-clustering analysis

Hepatitis B virus remains a major cause of cirrhosis and hepatocellular carcinoma,with genetic polymorphisms and mutations influencing immune responses and disease progression.Nguyen et al present novel findings on specific human leukocyte antigen(HLA)alleles,including rs2856718 of HLA-DQ and rs3077 and rs9277535 of HLA-DP,which may predispose individuals to cirrhosis and liver cancer,based on multi-clustering analysis.Here,we discuss the feasibility of this approach and identify key areas for further investigation,aiming to offer insights for advancing clinical practice and research in liver disease and related cancers.

慢性乙型肝炎患者抗病毒治疗中血清HBV RNA水平变化与HBeAg阳性及肝硬化的关系

目的探讨慢性乙型肝炎(CHB)患者抗病毒治疗中血清乙型肝炎病毒(HBV)RNA水平变化与乙型肝炎病毒e抗原(HBeAg)及肝硬化的关系。方法选择核苷(酸)类似物抗病毒治疗中的CHB患者491例,其中HBeAg阳性206例、阴性285例,有肝硬化117例、无肝硬化374例。用全自动荧光定量PCR分析仪检测血清HBV DNA,用全自动核酸检测分析系统检测血清HBV RNA。二分类多因素非条件Logistic回归分析HBV RNA阳性对CHB患者抗病毒治疗中HBeAg阳性、肝硬化的影响,用Pearson相关法分析血清HBV RNA水平与HBV DNA水平的相关性。结果HBeAg阳性患者年龄小于HBeAg阴性患者(P<0.05),HBV RNA阳性率、HBV DNA阳性率及HBV RNA、HBV DNA水平高于HBeAg阴性患者(P均<0.05)。肝硬化患者年龄大于无肝硬化患者(P<0.05),HBV DNA阳性率、HBV DNA水平低于无肝硬化患者(P均<0.05)。肝硬化患者与无肝硬化患者性别、HBV RNA阳性率、HBV RNA水平比较差异无统计学意义(P均>0.05)。年龄小、HBV DNA阳性、HBV RNA阳性是CHB患者抗病毒治疗中HBeAg阳性的危险因素(P均<0.05)。男性、年龄大、HBV DNA阳性、HBV RNA阳性是CHB患者抗病毒治疗中肝硬化的危险因素(P均<0.05)。CHB患者血清HBV RNA水平与HBV DNA水平呈正相关(P均<0.05)。结论HBV RNA阳性是CHB患者抗病毒治疗中HBeAg阳性、肝硬化的危险因素,HBV RNA检测可作为HBV DNA评估病毒复制活性的有效补充。

Hepatitis B virus infection and metabolic dysfunction associated steatotic liver disease:Rising pandemic with complex interaction

Due to sedentary lifestyle and rising prevalence of obesity,patients with general population and those who are infected with chronic hepatitis B are found to have metabolic dysfunction associated steatotic liver disease(MASLD).Both chronic hepatitis B virus(HBV)infection and MASLD can damage hepatocytes in their own way,but concomitant HBV-MASLD has its own clinical implications.Cherry on top is the presence of diabetes mellitus,hypertension or obesity which added more chances of unfavorable outcomes in these patients.In this article,we co-mment on the article by Wang et al published in the recent issue.This article provides a comprehensive overview of the complex interaction between HBV-MASLD,HBV alone and MASLD alone patients.We discuss key findings from recent studies,including the promising outcomes observed in patients with concurrent HBV and MASLD,warrants further research.The insights presented here offer renewed understanding of this complex interaction.