Socio-Demographic and Occupational Aspects of HIV-HBV Co-Infection in Bangui, Central African Republic (CAR): Hospital-Based Cross-Sectional Study

Objective: HIV-HBV co-infection is a major public health problem that has not been sufficiently explored in the Central African workplace. The aim of this study was to assess the frequency of HIV-HBV co-infection among people who living with HIV (PLHIV) in the infectious and tropical diseases department of the Centre Hospitalier Universitaire de lAmiti Sino-Centrafricaine in Bangui. Methods: A retrospective study was carried out from January 1, 2010 to December 31, 2021 in the Infectious and Tropical Diseases Department at the Amiti Sino-Centrafricaine University Hospital. It included the files of all PLHIV, which included the results of HBV serology. A standardized form was used to collect socio-demographic and professional data by documentary review. Data was analysed using Epi-Info 7 software. Means, proportions were calculated as well as Chi square witch was significant if p-value was below 0.05. Results: The study included 265 patients, 188 were women (70.1%) and 77 men (29.1%), giving a sex ratio of 0.45. Mean age was 35.8 years, higher in men (40 years) than in women (35.8 years) (p 0.0001). The age groups 25 to 34 (37.7%) and 35 to 44 (33.6%) were in the majority (71.3%). The majority of PLHIV were unemployed (57.1%), including housewives (43.0%). HBV prevalence was 14.3%, including 7.2% among the unemployed, who account for half of all co-infections. The search for associations between HIV-HBV co-infection and all socio-demographic characteristics (age, sex, marital status) and socio-professional categories showed no significant difference (p 0.05). Conclusion: PLHIV were predominantly young adults, female, and unemployed;no occupation was significantly associated with co-infection. The vast majority of co-infected people were not covered by the occupational health system (unemployed or informal sector). Urgent action is needed to improve workers access to occupational medicine in CAR.

Seroprevalence of HCV and its co-infection with HBV and HIV among liver disease patients of South Tamil Nadu

AIM:To determine the seroprevalence of hepatitis C virus(HCV) and its co-infection with hepatitis B virus(HBV),hepatitis delta agent(HDV) and human immunodeficiency virus(HIV) among liver disease patients of south Tamil Nadu. METHODS:A total of 1012 samples comprising 512 clinically diagnosed cases of liver disease patients and 500 apparently healthy age and sex matched individuals were screened for Hepatitis C virus(anti HCV and HCV RNA) ,Hepatitis B virus(HBsAg),Hepatitis delta agent(anti HDV) and Human immuno virus(antibodies to HIV-1 and HIV-2) using commercially available enzyme linked immunosorbent assay kits.HCV RNA wasdetected by RT-PCR.Liver function tests like ALT,AST,GGT,ALP,bilirubin and albumin were also studied. RESULTS:The seroprevalence of HCV was found to be 5.6%among liver disease patients by ELISA.27/512,49/512 and 12/512 patients were positive for HIV,HBV &HDV respectively.Co-infection of HCV&HBV was found in 8 patients,with 6 for HCV&HIV and 4 for HCV,HBV&HIV co-infections.Sex-wise analysis showed that HIV,HCV&HBV and HCV&HIV co-infection was high among females whereas for HBV it was high in males. The mean ALT and AST in HCV positive cases were 42.1±8.3 and 49±10.1.In people co-infected with HCV&HBV or HCV&HIV or HCV,HBV&HIV the mean ALT of 58.0±03.16,56.78±4.401 and 64.37±4.01 respectively. CONCLUSION:We strongly recommend routine test of the blood for HCV in addition to HBV and HIV.We also recommend individualized counseling to identify those at risk and testing for those who want it.Improved surveillance and periodic epidemiological studies will have to be undertaken to monitor and prevent these blood-borne viruses.

Prevalence of Pulmonary Tuberculosis and HIV Co-Infection among Women in Bogodogo, Burkina Faso

Introduction: The tuberculosis (TB) and HIV co-infection is a deadly combination, each accelerating the progression of the other. TB, caused by Mycobacterium tuberculosis (M. tuberculosis), is the leading cause of deaths among people living with HIV, accounting for around 40% of all HIV-positive deaths. The aim of this study was to estimate the prevalence of the tuberculosis-HIV co-infection in women. Material and Methods: The study population consisted of all suspected patients visiting the laboratory of the Bogodogo University Hospital, from May 2023 to January 2024, to be screened for M. tuberculosis. This was a descriptive cross-sectional study. Socio-demographic data were collected during individual interviews with consenting patients. M. tuberculosis was identified using the GeneXpert device, and HIV was diagnosed using the Abbott Determine diagnostic test. Results: Our study population was aged, on average, 37 ± 17.5 years. The overall tuberculosis infection rate was 65%, and 35% were married. Housewives were the most infected with 22.5%. The most infected age group was the ]20 - 40], with 32.5%. Some 37.5% of the women were anorexic and 45% had asthenia. Of the suspected cases, 47.5% were people who had contact with infected persons. TB/HIV co-infection was 5%. Conclusion: Tuberculosis is still rife in many parts of the world. It infects both men and women very quickly. HIV-tuberculosis co-infection is a reality, with HIV accelerating the progression of tuberculosis and vice versa. Raising awareness of HIV and tuberculosis should be done in tandem, as their co-infection leads to a poor vital prognosis.

HIV,HCV,and HBV Co-Infections in a Rural Area of Shanxi Province with a History of Commercial Blood Donation

Background： Unhygienic blood collection in the early 1990s led to blood-borne infections in Central China. This study aimed to estimate human immunodeficiency virus （HIV） co-infection with hepatitis C and B viruses （HCV and HBV） and their risk factors in a rural area of Shanxi Province with a history of commercial blood donation. Methods： A cross-sectional study was conducted in 2004. All adult residents in the target area were invited to participate in the study. Face-to-face interviews were completed and blood specimens were tested for HIV, HCV, and HBV surface antigen （HBsAg）. Results： Prevalence rates of HIV, HCV, and HBsAg were 1.3% （40/3 062）, 12.7% （389/3 062）, and 3.5% （103/2982）, respectively. Of the 40 HIV-positive specimens, 85% were HCV positive and 2.5% were HBsAg positive. The history of commercial blood donation was positively associated with HIV, HCV, and HIV/HCV co-infections, but was negatively associated with HBsAg seropositivity. Migration for employment in the last 5 years was positively related to HIV, HBsAg, and HIV/HCV co-infections. Univariate logistic analysis showed that illegal drug use, number of sex partners, extramarital sex behavior, commercial sex behavior, and condom use rate were not related to anti-HIV, anti-HCV, HBsAg seropositivity or their co-infections. Conclusion： The history of commercial blood donation was the main risk factor for HIV, HCV, and HIV/HCV co-infections in this former commercial blood donation area. HIV and HCV prevention and treatment interventions are important in this area.

Insights from respiratory virus co-infections

Respiratory viral co-infections present significant challenges in clinical settings due to their impact on disease severity and patient outcomes.Current diagnostic methods often miss these co-infections,complicating the epidemiology and management of these cases.Research,primarily conducted in vitro and in vivo,suggests that co-infections can lead to more severe illnesses,increased hospitalization rates,and greater healthcare utilization,especially in high-risk groups such as children,the elderly,and immunocompromised individuals.Common coinfection patterns,risk factors,and their impact on disease dynamics highlight the need for advanced diagnostic techniques and tailored therapeutic strategies.Understanding the virological interactions and immune response modulation during co-infections is crucial for developing effective public health interventions and improving patient outcomes.Future research should focus on the molecular mechanisms of co-infection and the development of specific therapies to mitigate the adverse effects of these complex infections.

Mathematical Modeling of the Co-Infection Dynamics of HIV and Tuberculosis Incorporating Inconsistency in HIV Treatment

A non-linear HIV-TB co-infection has been formulated and analyzed. The positivity and invariant region has been established. The disease free equilibrium and its stability has been determined. The local stability was determined and found to be stable under given conditions. The basic reproduction number was obtained and according to findings, co-infection diminishes when this number is less than unity, and persists when the number is greater than unity. The global stability of the endemic equilibrium was calculated. The impact of HIV on TB was established as well as the impact of TB on HIV. Numerical solution was also done and the findings indicate that when the rate of HIV treatment increases the latent TB increases while the co-infected population decreases. When the rate of HIV treatment decreases the latent TB population decreases and the co-infected population increases. Encouraging communities to prioritize the consistent treatment of HIV infected individuals must be emphasized in order to reduce the scourge of HIV-TB co-infection.

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。

Identification and Pathogen Characteristics Analysis of a Co-infection with CSFV,PRRSV and PCV2

[Objective] The aim of this study was to identify swine diseases caused by CSFV,PRRSV and PCV2 and thus to analyze its pathogeny chracteristics.[Method] The tissues and viscera of the diseased swine were collected from Xiangtan of Hunan(Code of HN/XT)to extract DNA and RNA for PCR amplification and sequencing.Meanwhile,the virulent strains were isolated and identified by cell separation technology.[Result] The sequencing analysis results showed that the amino acid homology between CSFV,PRRSV,PCV2 and sequen...

2016—2022年我国17家血液中心献血者HBV感染相关标记物检测情况分析

目的探讨我国17家省会城市血液中心(简称血液中心)献血者HBV的感染情况,为安全献血者管理提供参考。方法选取17家血液中心,收集2016—2022年献血者HBsAg和乙型肝炎病毒核酸(HBV DNA)检测结果,比较初次献血者和重复献血者HBsAg不合格率及年度变化趋势、初次献血者和重复献血者HBsAg不合格率差异、HBsAg合格献血者HBV DNA单独不合格(HBsAg-/HBV DNA+)情况和献血者总体HBV不合格率,比较不同地区血液中心献血者总体HBV不合格率。结果2016—2022年17家血液中心初次献血者HBsAg不合格率为59.60‱(1.60‱~142.85‱),重复献血者HBsAg不合格率为16.67‱(0.60‱~48.68‱),HBsAg合格献血者中HBV DNA单独不合格率为6.69‱(1.30‱~17.57‱),献血者总体HBV不合格率为47.06‱(3.46‱~103.78‱),上述4项不合格率的比较,差异均有统计学意义(P<0.05)。东部地区献血者HBV总体不合格率(34.04‱)低于中部地区(50.42‱)和西部地区(52.07‱),3个地区献血者间差异均有统计学意义(P<0.05)。结论17个省会城市初次献血者和重复献血者的HBsAg不合格率随时间整体呈下降趋势,重复献血者是相对安全的献血人群,HBV DNA检测可进一步降低HBV经血传播的风险。献血人群HBV感染分布具有地域性,东部地区献血者HBV不合格率明显低于中西部地区,与一般人群HBV流行分布情况一致。

HBsAg ELISA+/HBV DNA NAT-献血者血清学与分子生物学特征分析

目的 了解西安地区无偿献血人群HBsAg ELISA检测结果与HBV DNA检测结果不一致的标本相关血清学标志物的分布情况。方法 收集2022年11月1日—2023年4月30日陕西省血液中心HBsAg ELISA+/HBV DNA NAT-(ELISA+/NAT-)标本共计71份,对其采用电化学发光法检测乙肝血清学标志物,同时复检巢式PCR扩增HBV S区和C区基因片段。结果 双ELISA+/NAT-标本(n=30)巢式PCR检测阳性率远高于单ELISA+/NAT-标本(n=41)(60%vs 24.40%,P<0.05)。前者献血者100%为初次献血者,血清抗-HBc阳性率100%,血清学模式以1、4、5此3项阳性(80%)为主;后者献血者中31.7%为重复献血者,血清抗-HBc阳性率仅为19.51%,血清学模式以单2项阳性(43.90%)和全阴(36.58%)为主。结论 单ELISA+结果存在较多假阳性,导致不必要的血液报废;而NAT-标本可能存在低水平的HBV DNA,产生漏检风险。建议针对单HBsAg ELISA+/NAT-献血者,采用多套系统多种方法追溯检测,提高献血者HBV筛查的准确度,减少不必要的血液浪费。

献血者HBVs基因变异的生物信息学分析

目的分析HBV DNA+/HBsAg-献血者的传染性指标、S区基因序列突变情况及生物信息学特征变化。方法通过PCR方法筛查出1份HBV DNA+/HBsAg-的标本,应用酶联免疫和化学发光方法检测该标本乙肝病毒5项指标,对该标本HBVs区基因片段测序并分析变异情况,应用分析软件对所测序列进行生物信息学分析。结果该标本HBV DNA+、HBsAg-、HBsAb+、HBeAg+、HBeAb-、HBcAb+;HBVs区基因序列内发生氨基酸单位点突变(P151L),空间结构发生改变。结论HBVs区基因序列空间结构改变,可能是导致检测结果出现血清学HBsAg-/HBsAb+/HBV DNA+的原因。

HBV C基因型有关的HBsAg阴性HBV DNA阳性患者S区突变对HBsAg的影响

目的通过构建HBV C基因型突变质粒研究HBsAg阴性HBV DNA阳性患者HBV S区突变对HBsAg水平的影响。方法收集2022年8月至2023年4月首都医科大学附属北京佑安医院107例HBsAg-/HBV DNA+患者血液样本,对成功提取扩增的HBV DNA S区进行测序,通过构建HBV C基因型突变质粒对HBV S区突变位点进行细胞功能验证,探讨OBI可能发生的分子机制。结果对成功提取扩增的68例患者进行测序,发现HBV S区存在大量突变,包括免疫逃逸突变(如sG145R、sK122R、sS114T、sT131P等)和跨膜结构域(transmembrane domain,TMD)突变(如sT5A、sG10D、sF20S等)。通过构建HBV C基因型突变质粒,进行细胞转染和细胞免疫荧光实验发现sG145R突变会明显降低HBsAg的表达,但是sK122R、sI26N、sQ29N、sR169H、sS114T、sT131P这6个突变位点并未影响细胞内外HBsAg的表达。结论通过测序发现HBsAg-/HBV DNA+患者HBV S区存在大量突变位点,通过构建sG145R、sK122R、sI26N、sQ29N、sS114T和ST131P等突变质粒发现sG145R突变会明显降低细胞内外HBsAg的表达,但是sK122R、sI26N、sQ29N、sR169H、sS114T、sT131P并未明显降低细胞内外HBsAg的表达。

IL-18评价人工肝治疗HBV相关慢加急性肝衰竭有效性及短期预后效果的研究

目的探讨血清白细胞介素-18(IL-18)评价人工肝治疗乙型肝炎病毒(HBV)相关慢加急性肝衰竭(HBV-ACLF)的有效性及短期预后效果。方法选取2022年1月—11月于我院接受治疗的HBV-ACLF患者151例,所有患者均成功接受人工肝治疗,根据患者90 d内结局分为死亡组(n=63)和生存组(n=88),另选择73例健康受试者作为对照(健康组)。检测患者入院时、治疗后及健康受试者血清IL-18水平,分析IL-18水平对患者预后的评估价值。结果HBV-ACLF患者入院时及治疗后血清IL-18均显著高于健康组,死亡组患者入院时及治疗后血清IL-18均显著高于生存组(P<0.05)。Spearman相关性分析显示IL-18与终末期肝病模型(MELD)呈正相关。多因素Cox回归分析显示,血清IL-18水平是HBV-ACLF患者人工肝治疗后死亡的独立危险因素(P<0.05)。受试者工作曲线(ROC)显示患者入院时、治疗后血清IL-18水平诊断HBV-ACLF患者人工肝治疗后90 d死亡率的曲线下面积分别为0.760、0.739。Kaplan-Meier曲线显示,低IL-18水平患者的生存率高于高IL-18水平患者(P<0.05)。结论血清IL-18可辅助评价HBV-ACLF患者人工肝治疗效果及治疗后短期预后。

HBV pgRNA联合HBcrAg对慢性乙型肝炎患者停药后复发的预测价值

目的分析乙型肝炎病毒(hepatitis B virus,HBV)前基因组RNA(pregenomic RNA,pgRNA)水平联合HBV核心相关抗原(hepatitis B virus core-related antigen,HBcrAg)定量对慢性乙型肝炎(chronic viral hepatitis B,CHB)患者停药后复发风险的预测价值。方法选取中国人民解放军联勤保障部队第926医院2020年6月至2021年6月收治的113例CHB患者为研究对象,所有患者均已给予足疗程的正规抗病毒治疗,停药前均检测批pgRNA与HBcrAg。根据患者停药1年内复发情况分为复发组(38例)和未复发组(70例),比较两组患者的一般资料、肝功能、肾功能、甲胎蛋白(alphafetoprotein,AFP)、pgRNA及HBcAg水平等指标。应用多因素Logistic回归分析CHB患者停药后复发的影响因素。应用受试者工作特征(receiver operator characteristic,ROC)曲线分析pgRNA联合HBcrAg对CHB患者停药后复发风险的预测价值。结果复发组患者饮酒史比例[47.37%(18/38)比22.86%(16/70)]、AFP[(29.64±7.18)μg/L比(20.38±6.46)μg/L]、pgRNA[(7.97±1.99)lg拷贝/ml比(4.97±1.24)lg拷贝/ml]和HBcrAg[(7.04±1.76)lg IU/ml比(5.11±1.28)lg IU/ml]水平均显著高于未复发组(P均<0.05)。多因素Logistic回归分析表明,饮酒史(OR=5.354,95%CI:1.055~68.858,P=0.046)、AFP(OR=1.189,95%CI:1.036~1.468,P=0.015)、pgRNA(OR=1.047,95%CI:1.117~8.109,P=0.007)和HBcrAg(OR=2.152,95%CI:1.154~4.308,P=0.021)是CHB患者停药后复发的独立危险因素。pgRNA与HBcrAg联合预测CHB患者停药后复发的ROC曲线下面积为0.954,最佳截点为>0.128,此时敏感度为98.9%,特异度为97.1%。结论pgRNA和HBcrAg与CHB患者停药后复发风险密切相关,早期监测两者水平有助于发现停药后复发高风险的患者,早期调整治疗方案。

妊娠合并慢性乙型肝炎血清HBV pgRNA、PreS1抗原表达与肝内胆汁淤积症的相关性分析

目的 探究妊娠合并慢性乙型肝炎病人血清乙型肝炎病毒(HBV)前基因组RNA(HBV pgRNA)、前S1抗原(PreS1Ag)水平变化及与妊娠期肝内胆汁淤积症(ICP)发生的相关性。方法 选取2017年6月至2020年6月在雅安市人民医院进行孕期检查的慢性乙型肝炎孕妇279例作为研究对象,根据入组病人是否患有ICP分为合并ICP组43例、未合并ICP组236例。比较两组病人血清中HBV pgRNA、PreS1 Ag水平,并分析两组血清HBV pgRNA、PreS1 Ag表达与HBV DNA表达水平相关性;比较两组病人妊娠结局,并分析合并ICP组病人血清HBV pgRNA表达水平及PreS1 Ag阳性表达率与妊娠结局的关系。受试者操作特征(ROC)曲线分析血清HBV pgRNA、PreS1 Ag光密度[D(λ)]值诊断慢性乙型肝炎孕妇合并ICP的效能。结果 合并ICP组慢性乙型肝炎病人血清HBV表面抗原(HbsAg)水平[(3.71±0.92)log IU/mL]、HBV e抗原(HbeAg)阳性率[65.12%(28/43)]、HBV DNA含量[(8.03±1.69)log copies/mL]、天冬氨酸转氨酶(AST)[(79.68±15.73)U/L]、丙氨酸转氨酶(ALT)[(72.08±16.95)U/L]、PreS1 Ag阳性表达率[88.37%(38/43)]、PreS1 Ag D(λ)值水平(1.24±0.25)及HBV pgRNA表达水平[(5.17±1.25)log copies/mL]明显高于未合并ICP组[(2.26±0.74)log IU/mL、24.15%(57/236)、(5.19±1.07)logcopies/mL、(23.01±12.47)U/L、(21.76±10.51)U/L、67.80%(160/236)、(0.92±0.23)、(3.02±0.98)logcopies/mL](P<0.05)。血清HBV pgRNA诊断慢性乙型肝炎孕妇合并ICP的曲线下面积(AUC)为0.89,灵敏度为81.40%,特异度为80.50%。PreS1 Ag D(λ)值诊断慢性乙型肝炎孕妇合并ICP的AUC为0.83,灵敏度为76.70%,特异度为79.20%。二者联合诊断的AUC为0.91,灵敏度为93.00%,特异度为78.40%。合并ICP组、未合并ICP组血清PreS1 Ag阳性的慢性乙型肝炎病人血清HBV DNA、HBV pgRNA表达水平均明显高于PreS1 Ag阴性表达病人(P<0.05)。合并ICP组、未合并ICP组血清HBV pgRNA、PreS1 Ag D(λ)值均与HBV DNA表达水平呈正相关(P<0.05)。合并ICP组产后出血、早产的发生率明显高于未合并ICP组(P<0.05)。发生不良妊娠结局的慢性乙型肝炎合并ICP病人血清PreS1 Ag阳性表达率、PreS1 Ag D(λ)值、HBV pgRNA表达水平均明显高于未发生不良妊娠结局病人(P<0.05)。结论 合并ICP的慢性乙型肝炎病人血清HBV pgRNA表达水平、PreS1 Ag阳性表达率及D(λ)值水平均明显升高,对ICP有一定诊断价值,且两者水平变化均与HBV DNA含量有关,并可能预示病人不良妊娠结局的发生。

化学发光微粒子免疫法检测HBV相关性肝硬化失代偿期患者血清HBcAb含量的临床意义

目的探讨化学发光微粒子免疫法检测HBV相关性肝硬化失代偿期患者血清HBcAb含量的临床应用价值。方法选择2017年1月—2019年3月本院确诊的HBsAg阳性的肝硬化失代偿期患者30例作为研究对象,根据患者血清HBV DNA含量分为:<500 IU/ml组(16例)和≥500 IU/ml组(14例)两组。化学发光微粒子免疫法检测肝硬化失代偿期患者血清HBcAb含量,并比较分析两组患者HBcAb含量差异。在<500 IU/ml组肝硬化失代偿期患者中,分析患者血清HBcAb含量与其它病毒学指标HBsAg、HBeAg相关性;同时在≥500 IU/ml组肝硬化失代偿期患者中,分析患者血清HBcAb含量与其它病毒学指标HBV DNA、HBsAg、HBeAg相关性。结果肝硬化失代偿期患者血清HBV DNA高低对HBcAb含量无明显影响。在<500 IU/ml组中,患者血清HBcAb含量与HBsAg呈正相关(r=0.450,P=0.042),而与HBeAg状态无明显相关性;在≥500 IU/ml组中,患者血清HBcAb含量却与HBV DNA呈负相关(r=-0.381,P=0.046),并且与HBsAg也呈显著负相关(r=-0.582,P=0.029),但HBeAg-患者和HBeAg+患者HBcAb含量差异无统计学意义(P=0.154)。结论化学发光微粒子免疫法检测HBV≥500 IU/ml的HBV相关性肝硬化失代偿期患者血清HBcAb含量高低与HBV复制水平、HBsAg分泌密切相关。

92031例癌症患者HBV血清标志物特征分析

目的了解癌症患者乙型肝炎病毒(hepatitis B virus,HBV)的感染状态和感染特点。方法回顾性分析2017年7月26日至2023年9月18日于广西医科大学附属肿瘤医院确诊的92031例癌症患者的HBV血清标志物检测结果,以肝癌、非肝癌进行分组,比较未感染(全阴或Anti-HBs阳性)、感染(除外Anti-HBs任何一项阳性)、隐性感染(occult hepatitis B virus infection,OBI;HBsAg阴性、血清或肝组织HBV DNA阳性)的占比。结果92031例癌症患者的HBV总感染率为73.75%(67876/92031),其中肝癌患者的HBV总感染率为97.65%(8922/9137),非肝癌患者的HBV总感染率为71.12%(58954/82894),肝癌组的普通感染率和OBI率均显著高于非肝癌组(均P<0.001)。肝癌组HBV血清标志物中HBsAg、HBeAg、Anti-HBe、Anti-HBc的阳性率明显高于非肝癌组(均P<0.001),但Anti-HBs的阳性率低于非肝癌组(P<0.001)。肝癌组和非肝癌组分别有20种和27种血清标志物组合模式,其中14种模式构成比在两组间差异有统计学意义(均P<0.001);两组均有7种OBI血清组合模式,其中5种模式构成比在两组间的差异有统计学意义(均P<0.05)。结论癌症患者HBV感染状态和血清学组合模式复杂,区分肝癌与非肝癌进行HBV感染统计更利于癌症患者的HBV感染评估。

基于HBV感染的确认探讨核酸检测反应性献血者的归队策略

目的基于血液筛查核酸检测反应性献血者的HBV感染的确认,探讨核酸检测反应性献血者的归队策略。方法联合应用自建的高灵敏度核酸检测体系、血液核酸筛查等多种核酸检测(NAT)方法,并结合血清学检测、献血者随访,对核酸检测反应性(NAT-yield)献血者中的HBV感染进行确认和感染状态识别。依据确认的HBV感染血浆样本,比较不同确认方法、确认指标或指标组合对HBV感染确认的效果。结果2010年11月—2021年2月,在血液筛查检出的876位NAT-yield献血者中共确认HBV感染者511人(OBI 451人,急性早期HBV感染者27人,不能确认感染者33人,无感染者30人,不能确认HBV感染者335人)。采用单检系统对混检系统检出的HBV感染血浆进行复测的检出率为96.6%,明显高于混检系统对单检系统检出的HBV DNA反应性(HBV DNA R)组和鉴别试验无反应性(NDR)组的复测检出率(76.4%和55.7%)(P<0.05)。NDR样本在模式2(ID×5+鉴别×2)下复测检出率(65.2%)高于模式1(ID×2+鉴别×1)(39.2%)(P<0.05);2种单检复测模式下的HBV DNA R样本复测检出率无明显差异(P>0.05),但均明显高于NDR样本(P<0.05)。回溯OBI献血者既往NAT数据,有46%经历多次NAT检测而未能检出。有59.1%OBI献血者随访检不出HBV DNA。OBI献血者中抗-HBc+占比为90.2%,单独抗-HBc+为49.2%,远高于不能确认感染组(P<0.05);HBeAg、抗-HBe和抗-HBc IgM在OBI和不能确认感染组中的比例极低且无差异(P>0.05)。结论近60%的NAT-yield献血者可以确认HBV感染。为保证献血者归队的安全性,需要更高灵敏度的HBV DNA确证技术提高HBV感染的确认率。抗-HBc是NAT-yield献血者OBI风险排查和归队评估最重要的血清学指标。

癌胚性TUFT1异常表达与HBV相关肝细胞癌的研究进展

肝细胞癌(hepatocellular carcinoma,HCC)的预防、早期诊断及精准治疗仍是亟需攻克的难题。肝炎病毒(HBV or HCV)慢性持续性感染、化学致癌物摄入和非酒精性脂肪性肝病(non-alcoholic fatty liver disease,NAFLD)等与HCC进展密切相关。最新发现,在牙釉质发育和矿化中起重要作用的釉丛蛋白(Tuftelin,TUFT1)异常转录,在人体组织中广泛分布。TUFT1作为酸性、磷酸化糖蛋白可促进肿瘤进展与转移。然而,TUFT1表达与HCC的研究报道尚不多见。本文综述了TUFT1基因结构、组织分布与肿瘤的关系,重点分析其在HBV-HCC进展中作用及其应用前景。

一例HBV再激活后血清HBsAg阴性HBeAg阳性的病例分析

回顾性分析一例HBV再激活后血清HBsAg阴性HBeAg阳性的病例。通过分析其诊断过程,以加强检验对HBV再激活的认识。为HBV再激活的发生机制和诊治的探讨提供一定依据。