首页> 美国卫生研究院文献>Journal of Clinical Microbiology >High Prevalence of M184 Mutation among Patients with Viroimmunologic Discordant Responses to Highly Active Antiretroviral Therapy and Outcomes after Change of Therapy Guided by Genotypic Analysis
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High Prevalence of M184 Mutation among Patients with Viroimmunologic Discordant Responses to Highly Active Antiretroviral Therapy and Outcomes after Change of Therapy Guided by Genotypic Analysis

机译:对高活性抗逆转录病毒疗法进行病毒免疫学不一致反应的患者中M184突变的高发生率以及在基因型分析指导下改变疗法后的结果

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摘要

Whether highly active antiretroviral therapy (HAART) should be modified in patients with persistent increases in CD4+ T cells despite detectable viral loads is an unresolved question. Forty-three heavily pretreated human immunodeficiency virus (HIV)-infected patients with virologic failure during HAART were studied before a change of therapy guided by genotypic analysis and during follow-up. Patients with an increase in CD4+ cell count (>100 cells/ml) over pre-HAART values were considered to be discordant patients (20 individuals), whereas patients with a lower increase or no increase in CD4+ cell count were considered failing patients (23 individuals). Based on univariate analysis, a high CD4+ cell count before antiretroviral treatment, homosexual behavior as a risk factor for HIV infection, reduced drug exposure to nonnucleoside reverse transcriptase inhibitors, low replicative capacity of HIV isolates, and more frequent detection of HIV isolates with a non-B subtype, an R5 biological phenotype, and M184V and T215Y/F mutations were factors associated with a discordant response to HAART. Based on multivariate analysis, only the M184V mutation remained significantly associated with a viroimmunologic discordant response (odds ratio, 25.48; 95% confidence interval, 1.43 to 453.93). No difference in lamivudine exposure was found between discordant (95%) and failing (91%) patients. Twelve months after the genotypic analysis-guided change of therapy, 3 discordant (15%) and 6 failing patients (26%) achieved undetectable viral loads (<50 copies/ml), whereas in patients with HIV RNA loads of >500 copies/ml, discordant responses were observed in 5 out of 15 discordant patients and in 4 out of 16 failing patients. A relationship between the M184V mutation and a viroimmunologic discordant response to HAART was found. After the genotypic analysis-driven change of therapy, similar rates of virologic suppression were detected in the two groups.
机译:CD4 + T细胞持续增加,尽管病毒载量可检测,是否应修改高活性抗逆转录病毒疗法(HAART),这仍是一个尚未解决的问题。在由基因型分析指导的治疗改变之前和随访期间,研究了43例经过严重预处理的人类免疫缺陷病毒(HIV)感染严重的病毒性肝炎患者。 CD4 + 细胞计数增加(> 100细胞/ ml)超过HAART前值的患者被认为是不一致的患者(20人),而CD4升高较低或没有升高的患者 + 细胞计数被认为是衰竭患者(23人)。根据单因素分析,抗逆转录病毒治疗前CD4 + 细胞计数高,同性恋行为是HIV感染的危险因素,药物暴露于非核苷逆转录酶抑制剂的减少,HIV分离株的复制能力低等等频繁检测到具有非B亚型,R5生物表型以及M184V和T215Y / F突变的HIV分离株是与HAART反应不一致相关的因素。基于多变量分析,仅M184V突变仍与病毒免疫不一致反应显着相关(比值比为25.48; 95%置信区间为1.43至453.93)。在不一致的患者(95%)和失败的患者(91%)之间未发现拉米夫定暴露的差异。在基因型分析指导的治疗改变后十二个月,3名不和谐(15%)和6名衰竭患者(26%)达到了不可检测的病毒载量(<50拷贝/ ml),而HIV RNA载量> 500拷贝/毫升,不和谐的反应观察到15名不和谐患者中的5名和16名衰竭患者中的​​4名。发现M184V突变与对HAART的病毒免疫学不一致反应之间的关系。在基因型分析驱动的治疗方法改变后,两组的病毒学抑制率相似。

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