评价感染 HIV-1 CRF01_AE 和 B 亚型的初治患者在起始一线治疗时的免疫应答和临床恶化情况。
Evaluating immunologic response and clinical deterioration in treatment-naive patients initiating first-line therapies infected with HIV-1 CRF01_AE and subtype B.
机构信息
Faculty of Medicine, The Kirby Institute, UNSW, Sydney, Australia.
出版信息
J Acquir Immune Defic Syndr. 2013 Mar 1;62(3):293-300. doi: 10.1097/QAI.0b013e31827a2e8f.
BACKGROUND
HIV-1 group M viruses diverge 25%-35% in envelope, important for viral attachment during infection, and 10%-15% in the pol region, under selection pressure from common antiretrovirals. In Asia, subtypes B and CRF01_AE are common genotypes. Our objectives were to determine whether clinical, immunological, or virological treatment responses differed by genotype in treatment-naive patients initiating first-line therapy.
METHODS
Prospectively collected longitudinal data from patients in Thailand, Hong Kong, Malaysia, Japan, Taiwan, and South Korea were provided for analysis. Covariates included demographics, hepatitis B and C coinfections, baseline CD4 T lymphocyte count, and plasma HIV-1 RNA levels. Clinical deterioration (a new diagnosis of Centers for Disease Control and Prevention category B/AIDS-defining illness or death) was assessed by proportional hazards models. Surrogate endpoints were 12-month change in CD4 cell count and virologic suppression post therapy, evaluated by linear and logistic regression, respectively.
RESULTS
Of 1105 patients, 1036 (93.8%) infected with CRF01_AE or subtype B were eligible for inclusion in clinical deterioration analyses and contributed 1546.7 person-years of follow-up (median: 413 days, interquartile range: 169-672 days). Patients >40 years demonstrated smaller immunological increases (P = 0.002) and higher risk of clinical deterioration (hazard ratio = 2.17; P = 0.008). Patients with baseline CD4 cell counts >200 cells per microliter had lower risk of clinical deterioration (hazard ratio = 0.373; P = 0.003). A total of 532 patients (48.1% of eligible) had CD4 counts available at baseline and 12 months post therapy for inclusion in immunolgic analyses. Patients infected with subtype B had larger increases in CD4 counts at 12 months (P = 0.024). A total of 530 patients (48.0% of eligible) were included in virological analyses with no differences in response found between genotypes.
CONCLUSIONS
Results suggest that patients infected with CRF01_AE have reduced immunologic response to therapy at 12 months, compared with subtype B-infected counterparts. Clinical deterioration was associated with low baseline CD4 counts and older age. The lack of differences in virologic outcomes suggests that all patients have opportunities for virological suppression.
背景
HIV-1 组 M 病毒在包膜中发生 25%-35%的变异,这对病毒感染时的附着很重要,在多靶点抗逆转录病毒药物的选择压力下,pol 区发生 10%-15%的变异。在亚洲,亚型 B 和 CRF01_AE 是常见的基因型。我们的目的是确定初治患者开始一线治疗时,不同基因型之间的临床、免疫或病毒学治疗反应是否存在差异。
方法
对来自泰国、中国香港、马来西亚、日本、中国台湾和韩国的患者前瞻性收集的纵向数据进行分析。协变量包括人口统计学特征、乙型肝炎和丙型肝炎合并感染、基线 CD4 淋巴细胞计数和血浆 HIV-1 RNA 水平。临床恶化(新诊断的美国疾病控制与预防中心(CDC)B 类/艾滋病定义性疾病或死亡)通过比例风险模型评估。替代终点是治疗后 12 个月的 CD4 细胞计数变化和病毒学抑制,分别通过线性和逻辑回归评估。
结果
在 1105 名患者中,有 1036 名(93.8%)感染了 CRF01_AE 或亚型 B,有资格进行临床恶化分析,并提供了 1546.7 人年的随访(中位数:413 天,四分位距:169-672 天)。年龄>40 岁的患者免疫反应增加较小(P=0.002),临床恶化风险较高(风险比=2.17;P=0.008)。基线 CD4 细胞计数>200 个/微升的患者临床恶化风险较低(风险比=0.373;P=0.003)。共有 532 名患者(符合条件的患者的 48.1%)在基线和治疗后 12 个月有 CD4 计数,可纳入免疫分析。感染亚型 B 的患者在 12 个月时 CD4 计数增加更大(P=0.024)。共有 530 名患者(符合条件的患者的 48.0%)纳入病毒学分析,未发现基因型之间的反应存在差异。
结论
结果表明,与感染亚型 B 的患者相比,感染 CRF01_AE 的患者在 12 个月时的治疗免疫反应降低。临床恶化与低基线 CD4 计数和年龄较大有关。病毒学结果无差异表明所有患者都有机会实现病毒学抑制。
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