长期联合抗逆转录病毒治疗的 HIV 单感染患者通过瞬时弹性成像预测肝纤维化和脂肪变性的相关因素。
Predictive factors associated with liver fibrosis and steatosis by transient elastography in patients with HIV mono-infection under long-term combined antiretroviral therapy.
机构信息
Laboratory of Clinical Research in STI/AIDS (LAPCLIN-AIDS), National Institute of Infectious Diseases Evandro Chagas-Oswaldo Cruz Foundation (INI/FIOCRUZ), Rio de Janeiro, Brazil.
Plataform of Clinical Research, National Institute of Infectious Diseases Evandro Chagas-Oswaldo Cruz Foundation (INI/FIOCRUZ), Rio de Janeiro, Brazil.
出版信息
J Int AIDS Soc. 2018 Nov;21(11):e25201. doi: 10.1002/jia2.25201.
INTRODUCTION
Non-alcoholic fatty liver disease is characterized by the presence of hepatic steatosis and can be associated with fibrosis progression, development of cirrhosis and liver-related complications. Data on the prevalence of liver fibrosis and steatosis in HIV patients remain contradictory in resource-limited settings. We aimed to describe the prevalence and factors associated with liver fibrosis and steatosis in patients with HIV mono-infection under long-term antiretroviral therapy (ART) in Rio de Janeiro, Brazil.
METHODS
Clinical assessment, fasting blood collection and liver stiffness measurement (LSM)/controlled attenuation parameter (CAP) by transient elastography were performed on the same day for this cross-sectional study (PROSPEC-HIV study; NCT02542020). Patients with viral hepatitis co-infection, ART-naïve or missing data were excluded. Liver fibrosis and steatosis were defined by LSM ≥ 8.0 kPa and CAP ≥ 248 dB/m respectively. HIV history, cumulative and current ART regimens were evaluated. Multivariate logistic regression models adjusted for age and gender were performed.
RESULTS
In total, 395 patients (60% female; median age of 45 (IQR, 35 to 52) years, body mass index = 25.7 (23.2 to 29.4) kg/m , alanine aminotransferase = 30 (23 to 42) IU/L, duration of ART for 7 (4 to 14) years) were included. LSM and CAP were reliable in 93% (n = 367) and 87% (n = 344) respectively. The prevalence of fibrosis and steatosis were 9% (95% confidence interval (CI), 7 to 13) and 35% (95% CI, 30 to 40) respectively. The following factors were associated with fibrosis (odds ratio (OR) (95% CI)): older age (per 10 years; 1.80 (1.27 to 2.55); p = 0.001) and CD4+ count <200 cells/mm (7.80 (2.09 to 29.09), p = 0.002). Type 2 diabetes had a trend towards the presence of liver fibrosis (2.67 (0.96 to 7.46), p = 0.061). Central obesity (10.74 (4.40 to 26.20), p < 0.001), type 2 diabetes (9.74 (3.15 to 30.10), p < 0.001), dyslipidaemia (2.61 (1.35 to 5.05), p = 0.003) and metabolic syndrome (4.28 (2.45 to 7.46), p < 0.001) were associated with steatosis. A dominant backbone ART regimen of zidovudine (AZT), d4T, ddI or ddC was associated with steatosis (1.90 (1.07 to 3.38), p = 0.028) independently of metabolic features.
CONCLUSION
Integrated strategies for preventing non-communicable diseases in people with HIV mono-infection are necessary to decrease the burden of liver diseases. Clinical Trial Number: NCT02542020.
简介
非酒精性脂肪性肝病的特征是存在肝脂肪变性,并且可能与纤维化进展、肝硬化发展和肝脏相关并发症有关。在资源有限的环境中,关于 HIV 患者肝纤维化和脂肪变性的流行率的数据仍然存在矛盾。我们旨在描述巴西里约热内卢接受长期抗逆转录病毒治疗(ART)的 HIV 单感染患者的肝纤维化和脂肪变性的流行率和相关因素。
方法
这项横断面研究(PROSPEC-HIV 研究;NCT02542020)同日进行临床评估、空腹采血和通过瞬态弹性成像进行肝硬度测量(LSM)/受控衰减参数(CAP)。排除了病毒性肝炎合并感染、ART 初治或数据缺失的患者。LSM≥8.0kPa 和 CAP≥248dB/m 分别定义为肝纤维化和脂肪变性。评估了 HIV 病史、累积和当前的 ART 方案。进行了调整年龄和性别多变量逻辑回归模型。
结果
共纳入 395 名患者(60%为女性;中位年龄 45(IQR,35 至 52)岁,体重指数 25.7(23.2 至 29.4)kg/m ,丙氨酸氨基转移酶 30(23 至 42)IU/L,ART 持续时间为 7(4 至 14)年)。LSM 和 CAP 的可靠性分别为 93%(n=367)和 87%(n=344)。纤维化和脂肪变性的患病率分别为 9%(95%置信区间(CI),7 至 13)和 35%(95%CI,30 至 40)。以下因素与纤维化相关(比值比(OR)(95%CI)):年龄较大(每 10 岁;1.80(1.27 至 2.55);p=0.001)和 CD4+计数<200 个细胞/mm(7.80(2.09 至 29.09),p=0.002)。2 型糖尿病与肝纤维化的存在呈趋势(2.67(0.96 至 7.46),p=0.061)。中心性肥胖(10.74(4.40 至 26.20),p<0.001)、2 型糖尿病(9.74(3.15 至 30.10),p<0.001)、血脂异常(2.61(1.35 至 5.05),p=0.003)和代谢综合征(4.28(2.45 至 7.46),p<0.001)与脂肪变性相关。以齐多夫定(AZT)、d4T、ddI 或 ddC 为骨干的整合型抗逆转录病毒治疗方案与脂肪变性相关(1.90(1.07 至 3.38),p=0.028),独立于代谢特征。
结论
需要采取综合策略预防 HIV 单感染患者的非传染性疾病,以降低肝脏疾病的负担。临床试验编号:NCT02542020。
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