HIV and HCV:from Co-infection to Epidemiology,Transmission,Pathogenesis,and Treatment

Human immunodeficiency virus (HIV) is the infectious agent causing acquired immu-nodeficiency syndrome (AIDS),a deadliest scourge of human society. Hepatitis C virus (HCV) is a major causative agent of chronic liver disease and infects an estimated 170 million people worldwide,resulting in a serious public health burden. Due to shared routes of transmission,co-infection with HIV and HCV has become common among individuals who had high risks of blood exposures. Among hemophiliacs the co-infection rate accounts for 85%; while among injection drug users (IDU) the rate can be as high as 90%. HIV can accelerate the progression of HCV-related liver disease,particularly when immunodeficiency has developed. Although the effect of HCV on HIV infection is controversial,most studies showed an increase in mortality due to liver disease. HCV may act as a direct cofactor to fasten the progression of AIDS and decrease the tolerance of highly active antiretroviral therapy (HARRT). Conversely,HAART-related hepatotoxicity may enhance the progression of liver fibrosis. Due to above complications,co-infection with HCV and HIV-1 has imposed a critical challenge in the management of these patients. In this review,we focus on the epidemiology and transmission of HIV and HCV,the impact of the two viruses on each other,and their treatment.

Seroprevalence of HBV and HCV among People Living with HIV in Burkina Faso and Diagnostic Performance of HIV/HCV/HBsAg Combined Rapid Test in Comparison with Architect Assays

Background: The diagnosis of human immunodeficiency virus (HIV), hepatitis B virus (HBV), and hepatitis C virus (HCV) remains a constraint for some populations in sub-Saharan Africa. This study aimed to determine the prevalence of HBV and HCV in people living with HIV and to evaluate the performance of a combined rapid test for the simultaneous detection of HIV, HBV, and HCV. Methods: This is a cross-sectional study that took place from February 2017 to November 2018 and included 139 HIV-infected individuals followed up at different medical centers in Ouagadougou, Burkina Faso. HBV and HCV serology tests were performed on-site using finger prick whole blood with HIV/HCV/HBsAg combined rapid test and then serum with two reference tests “Architect HBsAg Qualitative” and “Architect HIV Ag/Ab Combo”. Results: The mean age of the participants was 57 ± 8 years. Of the 139 participants, 10% (14/139) were HIV-1 positive, 71.9% (100/139) were HIV-2 positive, and 18.0% (25/139) were HIV-1/HIV-2 coinfected. The sensitivity and specificity of the HIV/HCV/HBsAg combined rapid test were 33.33% vs 99.11% and 20% vs 99.25% compared to Architect HBsAg Qualitative and Architect HIV Ag/Ab Combo, respectively. The Kappa and Youden Index values were 0.4262 and 0.3244 and 0.2707 and 0.1925, respectively, compared to each of the two reference tests. Conclusion: The results show that the HIV/HCV/HBsAg combined rapid test has poor diagnostic efficiency and should not be recommended for the diagnosis of these viruses.

Progression of Platelet Counts in Treatment Naïve HIV/HCV Co-Infection

Background: Previous research has suggested an association between infection with hepatitis C virus (HCV) or with human immunodeficiency virus (HIV) and low platelet counts. This study estimates platelet count changes over time in HIV/HCV co-infected participants and compares them with the changes in platelet count among HIV mono-infected participants to test if HIV/HCV co-infection is associated with lower platelet counts. Methods: This retrospective cohort study included all HIV treatment naive patients from four sites in the Centers for AIDS Research Network of Integrated Clinical Systems (CNICS) cohort with platelet count measurements between 2002 and 2009. We conducted a mixed effects linear regression modeling the mean change in platelet count per year while adjusting for age, sex, race, baseline CD4 cell count, and site. Index date was the first platelet count after 2002, and participants were censored upon initiation of treatment for HIV or HCV. Results: There were 929 HIV/HCV co-infected and 3558 HIV mono-infected participants with a mean follow-up time of 1.2 years. HIV/HCV co-infected participants had on average a slighter lower platelet count at baseline (234,040 vs. 242,780/μL;p-value = 0.004), and a more rapid mean reduction per year (7230 vs. 3580/μL;p-value 0.001) after adjusting for age, sex, baseline CD4 count. Conclusions: In treatment naive participants, HIV/HCV co-infection is associated with a more rapid decline in platelet count compared with HIV mono-infection.

HIV/HCV Co-Infection—A Dual Neurocognitive Problem

Presence of the hepatitis C virus in HIV infected patients has an additional neurotoxic influence on the Central Nervous System. It has been described that HCV co-infection leads to neuropsychological impairment whose severity is greater than in mono-HIV infected subjects. In the present study we assessed the neuropsychological status of 46 human immunodeficiency virus (HIV)-infected individuals from the Warsaw Hospital for Infectious Diseases. For the purpose of cognitive assessment, neuropsychological tests measuring global cognitive functions, attention and perception, verbal memory, as well as non-verbal aspects of executive functions, e.g. visual monitoring and planning, were assessed. In 60% of the investigated patients, who were co-infected with the hepatitis C virus, the overall cognitive outcome observed was worse than in mono-HIV infected subjects. The following factors were taken into account: ART therapy’s influence on cognitive functions using the CPE rank (CNS Penetration Efficacy, 2010), route of HIV transmission, conditions of human existence and age of investigated patients. The present work should be treated as a preliminary research and interpreted in the context of several limitations described in the text.

Antiretroviral Therapy in HIV/HCV Co-Infection Italian Consensus Workshop

About 50% of people living with the HIV infection in Italy are co-infected with HCV. In this group of patients, the primary cause of mortality is liver disease, which accounts for up to 14% of deaths. HIV/HCV co-infection also exposes patients to a higher risk of progression to AIDS, a faster evolution towards cirrhosis, more frequent drug toxicity, and lower tolerance for antiretroviral therapy. Moreover, HCV infection can play a part in increasing immune system depression;neurological, cognitive and renal damage;and bone fragility. Hence an optimal antiretroviral regimen needs to be chosen for co-administration with anti-HCV therapy and timed appropriately to improve the prognosis of co-infected HIV/HCV patients. Unfortunately, however, data on the safety and efficacy of antiretroviral drugs in these patients is scarce, as are studies of pharmacokinetics in patients with advanced liver impairment. Furthermore, restoring adequate immune constitution seems not to slow the progression of liver disease, and the metabolic and hepatic toxicity of some antiretroviral drugs can even contribute to inflammatory and fibrogenic processes. It is therefore essential that HIV/HCV co-infected patients receive only medications capable of ensuring the best immune recovery but possessing the lowest potential to trigger immune reconstitution syndrome or hepatic and metabolic damage.

The Impact of Human Parvovirus B19 Co-Infection on Liver Function of HCV Infected Patients

Background: Human Parvovirus B19 is most known for causing disease in the pediatric population but can also affect adults. Human co-infection with Parvovirus B19 could deteriorate the prognosis of patient with chronic ill-ness. Objectives: This paper attempts to determine the prevalence of Parvovirus B19 in HCV infected patients and to evaluate the impact of Parvovirus B19 on liver enzymes activity of Hepatitis C patients. Study Design: The study population includes 74 chronic HCV (patient group) and 49 cases without viral hepatitis (control group). Nucleic acid of Parvovirus B19 was detected in Serum samples by nested polymerase chain reaction (nested-PCR) method. Results: Parvovirus B19-DNA infection was detected in 28.0% of chronic HCV patients. Parvovirus B19-HCV co-infection caused increasing in Alanine aminotransferase (ALT) and Aspartate aminotransferase (AST) activity than in B19-negative HCV patients. Conclusion: We conclude that Parvovirus B19 acted synergistically with HCV by increasing the levels alanine ami-notransferase (ALT) and Aspartate aminotransferase (AST).

Clinical, Biological, Immunological and Therapeutic Profile of Patients Co-Infected with HIV-HBV and/or HCV in Kinshasa, in the Democratic Republic of the Congo: Multicenter Cross-Sectional Study

Background and Objective: HIV infection is often associated with HBV and HCV infection, together leading to high morbidity and mortality in developing countries. The objective of this study is to describe the clinical, biological, immunological and therapeutic profile of patients co-infected with HIV-HBV and/or HCV. Methods: A cross-sectional and descriptive study including 180 people living with HIV (PLWHIV) in the city of Kinshasa province was conducted. Socio-demographic, clinical, biological and serological characteristics were analyzed. Results: The frequency of HIV-HBV/HCV co-infection was 23.9%. The distribution of age and sex of patients did not differ significantly according to co-infection status. The notion of pedicure and manicure was significantly more observed in patients free from viral hepatitis (51.1% versus 32.6%, p = 0.034). The median duration of knowledge of the HIV status which was longer in the co-infected (4 years versus 2 years, p = 0.022). A lower median level of GPT was observed in co-infected compared to other patients (14 IU/L versus 20 IU/L, p = 0.041). Serum albumin (3.1 g/L versus 3.3 g/L, p = 0.034) and prothrombin (58.3% versus 65.6%, p = 0.045) were lower in HIV co-infected-VHB and/or VHC. The median INR was higher in co-infected than in other patients (1.6 versus 1.4;p = 0.009). Patients without therapy Antiretroviral (TARV) medication were more numerous in co-infected (20.9% versus 8.0%, p = 0.025). Conclusions: The profile of PLWHIV was dominated by the presence of pedicures and manicures with high transaminases and without anti-viral treatment.

海南省吸毒人员吸毒方式与HIV、HCV、HBV和梅毒感染调查分析

采用血清流行病学方法和行为问卷对 3市县戒毒所5 1 4名吸毒人员进行调查。结果 :单纯口吸者占 6 6 1 5 % ,静脉注射吸毒者占 33 85 % ,共用注射器占静脉吸毒者 2 4 71 % ,检出抗HIV、抗HCV、HBsAg和梅毒阳性率分别为 0 1 95 %、2 9 6 7%、2 2 85 %、7 0 3%。表明 :吸毒者是 4种传染病感染的高危人群 ,静脉 (共用针具 )吸毒方式对HIV、HCV感染较HBV。

2010～2011年广州地区输血传播HBV、HCV、HIV残余风险评估

目的评估广州地区输血传播HBV、HCV、HIV的残余风险,建立适合广州地区献血人群残余风险评估的数学模型。方法收集2010年1月～2011年12月551 047人次广州地区无偿献血者的基本资料及血液ELISA与核酸检测(NAT)的HBV、HCV、HIV数据,利用(WP/I)及WP/LTR模型分别评估重复献血者及初次献血者传播HBV、HCV、HIV的残余风险。结果 2010～2011年广州地区献血者HBV、HCV、HIV经ELISA后的残余风险分别为1/30 147、1/70 591、1/645 099;经NAT检测后的残余风险分别为1/46 643、1/723 526、1/1 254 770。结论广州地区重复献血者传播HBV、HCV、HIV的残余风险低于初次献血者;采用NAT检测后,献血者传播HBV、HCV、HIV的残余风险大大降低。

核酸扩增技术在献血者血液HBV DNA、HCV RNA及HIV-1 RNA筛查中的应用研究

目的探讨在我国无偿献血者的血液筛查中引进核酸扩增技术(NAT)的必要性,了解献血者血清学病毒标志物检测阴性、NAT检测阳性的感染状况。方法应用Roche PCR、PCR-微流芯片、实时荧光PCR方法对深圳市131 174人(次)血清学检测病毒标志物阴性的献血者进行HBV DNA、HCV RNA和HIV-1 RNA检测,对NAT阳性献血者追踪检测并做定量分析。结果HBV DNA阳性22例,阳性率为1/5 962,其中15例为抗-HBc阳性,阳性率为1/8 745;HCV RNA阳性1例,阳性率1/131 174;HIV-1 RNA未检出阳性。对14名HBV DNA阳性者的追踪发现,8人发生了血清转换现象。结论采用高灵敏度的NAT筛查献血者血液中的HBV和HCV,有助于提高输血及血液安全。

无偿献血者ALT报废域值与NAT-HBV/HCV检测结果分析

目的探讨无偿献血者ALT与核酸扩增技术(NAT-HBV/HCV)检测结果的相关性,为优化血液筛查策略提供理论依据。方法回顾性调查本站2006年12月—2007年12月共28 800份无偿献血者样本,用速率法进行ALT检测,ALT单项不合格样本用NAT-HBV/HCV检测;分析ALT值与ELISA-HBV/HCV-OD值的分布规律。结果共筛查出2 516份ALT单项不合格样本;经NAT-HBV/HCV检测出8份阳性,其中HBV-DNA阳性5份,HCV-RNA阳性3份;ALT≤80 U/L的献血者NAT-HBV/HCV阳性率明显低于ALT>80 U/L献血者(P<0.01);经ELISA-HBV/HCV检测OD值,95%ALT单项不合格样本ELSIA-HBV/HCV的OD值<Cut-off值的40%。结论将ALT报废域值设定为ALT≤70 U/L且ELSIA-HBV/HCV检测OD值<其Cut-off值的40%,能够较好地保证血液的安全性,并可减少血液浪费。

血源性艾滋病高发村村民HIV/HBV/HCV混合感染状况调查

目的了解中国中部血源性艾滋病高发村HIV/HBV/HCV混合感染状况。方法以血源性艾滋病高发村2岁以上村民1506人为调查对象,采静脉血检测HIV、HBV、HCV。结果1506人中,1180人进行了所有检测,总调查率78.4%。1180人中,HIV、HBV、HCV感染率分别为15.34%、5.34%、36.44%。HIV/HBV、HIV/HCV、HBV/HCV、HIV/HBV/HCV混合感染率分别为0.25%、12.12%、0.34%、0.34%;有有偿献血史者单项HIV、单项HCV、HIV/HCV感染率高于无有偿献血史者;无有偿献血史者HCV感染者的配偶HCV感染率78.13%(75/96)高于无有偿献血的HCV阴性者的配偶HCV感染率2.91%(19/654)(P<0.0001)。结论由于有偿献血,血源性艾滋病高发村存在较高水平的HIV、HBV或HCV混合感染,主要感染类型为HIV/HCV。

献血者HBV、HCV、HIV的单人份核酸检测

目的应用Procleix ULTRIO Assay和Procleix TIGRIS System进行献血者单人份病毒核酸检测(ID-NAT),以了解ELISA法筛查的HBV、HCV、HIV漏检率,同时对ID-NAT和汇集NAT(MP-NAT)模式进行比较。方法在进行2次ELISA法筛查的同时,应用ULTRIO试剂在TIGRIS系统上行ID-NAT检测,对有活性的标本再分别进行HBV、HCV、HIV的鉴别测定,对ID-NAT阳性标本再进行8个(MP-8-NAT)和16个(MP-16-NAT)样品的模拟混样检测。结果在10064名无偿献血者中,共检出10例ELISA法阴性、ID-NAT阳性标本,ELISA法筛查漏检率为0.99‰,该10例标本经鉴别实验确定为HBV DNA阳性;共检出28例ELISA法阳性、ID-NAT阳性标本,其中HCV6例、HBV22例。将28例ELISA法阳性、ID-NAT阳性及10例ELISA法阴性、ID-NAT阳性标本进行8个、16个样品模拟汇集,结果 MP-8-NAT、MP-16-NAT的阳性检出率分别下降为78.6%、75.0%和30.0%、20.0%。结论 2次ELISA法血清学筛查模式存在较高的HBV漏检;ID-NAT的灵敏度高于MP-NAT,对于ELISA法阴性、ID-NAT阳性标本,MP-NAT存在很高的漏检率。

深圳地区HBV、HCV反应性献血者归队检测结果分析与策略探讨

目的分析深圳地区HBV、HCV反应性无偿献血者随访检测结果数据,探讨献血者归队检测确证方案与归队策略。方法按献血者归队规则程序,适用HBV、HCV酶免(ELISA)与核酸检测(NAT)项目,153例来自2008-2017年初筛为HBsAg+/HBV DNA-、HBsAg-/HBV DNA+、抗-HCV+/HCV RNA-、抗-HCV-/HCV RNA+、且在本血液中心的献血次数达≥10次(≥4000 mL)的无偿献血者进入归队流程,于第3、6个月后进行2次追踪随访检测,采用酶免试验(ELISA)与病毒核酸检测(NAT)方法复检反应性项目,并对2次复检结果统计分析其合格率情况。结果本中心于2008-2017年无偿献血812162献血人次,献血人数429927,占52.93%。在HBsAg、抗-HCV阳性献血者中分别有34.62%(1113/3215)、78.33%(1048/1338)为HBsAg+/HBV DNA-、抗-HCV+/HCV RNA-献血者。153例归队复查献血者,其中67 HBsAg+/HBV DNA-献血者经2次随访检测,有91.04%(61/67)成功归队;39例HBsAg-/HBV DNA+献血者经复查,有79.49%(31/39)成功归队;45例抗-HCV+/HCV RNA-献血者,有73.33%(33/45)成功归队;2例抗-HCV-/HCV RNA+献血者追踪复查确认为抗-HCV-/HCV RNA-。该153例随访复查献血者,总的合格归队率为83.01%(127/153)。其中有2例献血者在第2次随访(6个月后)才出现阳性结果。结论献血者中存在HBV、HCV感染康复期群体,也存在HBsAg、抗-HCV指标检测"假阳性"结果,开展献血者归队策略有利于血筛检测结果确证、减少血源流失、完善献血后续服务;本研究也为反应性献血者复检归队的科学管理程序、复检模式、间隔时间提供了实践与理论支撑数据。

HBV、HCV、HBV和HCV重叠感染与HCC发生关系的研究

目的:探讨HBV、HCV、HBV和HCV重叠感染及复制与广西HCC发生的关系。方法:在肝癌高发区和低发区分别选择符合全国诊断标准的HCC病人78例作为病例A组(肝癌高发区组)、B组(肝癌低发区组),并分别选择相同乡镇、生活习惯、生活水平、年龄士5岁、同性别的原籍健康人群2组分别78人作为对照组C组(肝癌高发区正常人组)和D组(肝癌低发区正常人组),应用PCR法检测研究对象血清中的HBVDNA、HCVRNA,并对阳性率进行比较。结果:HBVDNA、HCVRNA、HBVDNA+HCVRNA阳性率分别为:A组6 9.2%(5 4/7 8)、2 0.5%(1 6/7 8)、1 6.7%(1 3/7 8);B组5 2.6%(4 1/7 8)、6.4%(5/78)、5.1%(4/78);C组18.0%(14/78)、7.7%(6/78)、3.8%(3/78);D组10.3%(8/78)、2.6%(2/78)、1.3%(1/78);其中A组与C组,A组与B组组间的阳性率比较差异均有统计学意义(均P<0.05),B组与D组中HBVDNA阳性率比较差异也有统计学意义(均P<0.01)。结论:HBV、HCV、HBV和HCV的重叠感染及复制与广西肝癌高发区的肝癌发生有密切关系,其中HBV的感染及复制在肝癌的发生中最为重要,高发区中HCV、HBV和HCV的重叠感染的致癌作用也是不容忽视的。

HBV、HCV在原发性肝癌与其他恶性肿瘤患者及健康人群中的感染率调查

为了调查原发性肝癌与其他恶性肿瘤患者及健康人群中HBV、HCV感染率 ,将上述三组人群的HBV、HCV的感染情况进行分析比较。结果显示原发性肝癌组HBV感染率、HBV/HCV混合感染率均明显高于其它恶性肿瘤组和健康对照组 (P <0 0 1) ;其他恶性肿瘤组与健康对照组之间无显著差异 (P >0 0 5 ) ;单纯HCV感染率在三组之间均无显著差异 (P >0 0 5 )。由此可见HBV感染。

广西新发现肝癌高发点HBV、HCV感染与HCC家庭聚集性的研究

目的:探讨广西新发现肝癌高发点乙型肝炎病毒(HBV)、丙型肝炎病毒(HCV)感染在肝癌家族聚集性中的作用。方法:在广西新发现的肝癌高发点选择发生2例以上肝癌病例的高发家族成员作为研究对象,并选择性别和年龄构成相同的无癌家族成员作为对照,应用ELISA法检测HBV和HCV血清学标志物,采用PCR和RT-PCR技术对HBVDNA和HCVRNA进行检测。结果:在肝癌高发家族和无癌家族两组成员中HBsAg、HBsAb、HBeAg、HBVDNA的阳性率分别为24.47%、35.11%、8.51%、14.89%和8.51%、53.19%、4.26%、4.26%,HBsAg、HBsAb和HBVDNA在两组间存在显著性差别,P值分别为0.003、0.012、0.013;而HBeAg在两组间无显著性统计学意义(P>0.05);两组均未发现HCV-Ab和HCVRNA阳性者。结论:广西新肝癌高发点的肝癌家族聚集性的主要危险因素可能是HBV的感染和遗传因素的共同作用;HCV的感染与此高发点的家族聚集性无关。

血液HIV、HBV和HCV筛查策略的探讨

目的比较2种ELISA试剂加1种NAT试剂与1种ELISA试剂加1种NAT试剂筛查血液HBV、HCV、HIV的实验效果。方法以126 457(人)份献血者标本为检测对象,采用A、B 2种国产ELISA试剂平行检测其抗-HIV-1/2和抗-HCV,A、C 2种国产的ELISA试剂平行检测HBs Ag,以1种进口的NAT检测系统及配套试剂检测HBV DNA、HIV RNA和HCV RNA。对ELISA单试剂反应性、NAT阴性的标本做血清学确证试验,阳性者给予追踪随访。结果在本组献血者标本中共检出ELISA单试剂反应性、NAT阴性标本的比例为2.78‰(352/126 457),血清学确证试验阳性率0.13‰(17/126 457),其中抗-HCV:A试剂反应性79例,确证试验(RIBA)阳性1例,随访3个月后仍为阳性;B试剂反应性36例,RIBA阳性4例,随访3个月后,4例中RIBA试验1例转为阴性,1例转为不确定,2例仍为阳性。HBs Ag:A试剂反应性比例为0.88‰(112/126 457),确证试验(中和试验)阳性率0.09‰(11/126 457),有8例实现成功随访,3个月后2例转为阴性,1例转为A和C双试剂反应性,但NAT阴性、中和试验阳性,5例仍为A试剂反应性及中和试验阳性、但4例NAT转为阳性;C试剂反应性比例0.03‰(37/126 457),中和试验阳性率0.01‰(1/126 457),3个月后随访仍为阳性。抗-HIV-1/2:ELISA单试剂反应性、NAT阴性比例为0.69‰(88/126457),确证试验(WB)均为阴性。HBs Ag ELISA A试剂反应性、NAT阳性比例0.04‰(5/126 457);未检出抗-HIV-1/2、抗-HCV ELISA单试剂反应性伴NAT阳性标本。结论 1种ELISA试剂加1种NAT试剂的血液筛查模式,其HCV和HBV的残余风险高于2种ELISA试剂加1种NAT试剂,而2种试剂模式检测HIV的残余风险没有差别。

2010-2013年中国南京地区无偿献血人群HBV、HCV、HIV感染情况分析

本研究在于了解中国南京地区无偿献血者HBV、HCV和HIV感染及分布情况,探讨本地区人群的传染病流行趋势,为献血宣传和招募工作提供指导意见。将2010.6.10-2013.6.9三年间南京地区无偿献血者199777人次的血液标本,采用ELISA法检测HBsAg、抗-HCV和抗-HIV,对三项阴性标本再采用NAT联合检测HBVDNA、HCV-RNA和HIV-RNA,对检测结果进行统计分析,并将抗-HIV初筛反应性标本送南京市疾病预防控制中心确证。结果表明,3年中无偿献血者HBsAg、抗-HCV、抗-HIV感染率分别为0.45%,0.28%,0.11%;NAT呈反应性为0.07%;确证抗-HIV阳性32例,其中男性30例(6例为再次献血者),女性2例;不确定3例,其中男性2例,女性1例。经统计学处理证实,初次献血者与重复献血者HBsAg、抗-HCV、抗-HIV检测不合格率差异有统计学意义。结论:2010.6.10-2013.6.9南京地区无偿献血人群中抗-HCV、抗-HIV阳性率呈逐年下降趋势,HBsAg、NAT检测不合格率随年龄段增加而增加;抗-HCV、抗-HIV检测不合格率随年龄段增加而降低,重复献血者检测不合格率远远低于初次献血者,抗-HIV检测女性酶免检测阳性率高于男性,但确认阳性率男性明显高于女性。因此应提高献血前的征询技巧,重视献血者的招募环节,重点加强初次献血者献血前的征询和评估,加强无偿献血知识的宣传,巩固和发展固定无偿献血者队伍,大力普及NAT检测技术应用于血液筛查,将有效地提高血液安全。

柳州地区HIV感染者合并HBV、HCV及TP感染现状分析

目的分析人类免疫缺陷病毒(HIV)感染者中合并乙型肝炎病毒(HBV)、丙型肝炎病毒(HCV)以及梅毒螺旋体(TP)感染的流行现状及其特点。方法对确诊的184例HIV感染者进行流行病学调查,并采集血标本进行HBV、HCV和梅毒血清学检测。结果HIV感染者感染途径分别为:静脉注射毒品44.0%,性传播20.1%,母婴传播4.3%,输血或血制品3.8%,其他(原因不详)27.7%。184例HIV感染者中,抗-HCV阳性者36人(19.6%),HBsAg阳性者29人(15.8%),梅毒感染者21人(11.4%)。HIV、HBV和HCV三重感染者9人,约占4.9%。结论柳州市HIV感染以静脉注射毒品为主,性传播有所上升,HIV感染正由特殊人群向普通人群蔓延。HIV合并HBV、HCV、TP感染较为常见。建议在性病门诊中常规开展HIV的筛查,对HIV感染者常规进行HBV、HCV的相关检查并积极采取相关的预防治疗措施。