Shin-Woo Kim, Hyun Wook Jang, Hyun-Ha Chang, Yoonjung Kim, Sohyun Bae
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The secondary endpoints were safety and tolerability assessments.</p><p><strong>Results: </strong>Our retrospective analysis involved 40 patients. The leading reasons for switching to DTG+DRV/c were treatment failure in 17 patients (42.5%), simplification after multiple previous regimens in 15 (37.5%), and adverse drug reactions in 8 (20.0%). Among the 17 patients in the treatment failure group, we observed enhanced viral suppression and improved CD4+ T-cell counts after initiating the dual regimen. In the non-treatment failure group (23 patients), viral suppression and CD4+ T-cell levels were consistently maintained. No significant alterations in renal function, liver function, glucose levels, or lipid profiles were observed post-switch. High tolerability was observed, with 34/40 patients (85.0%) responding well to the regimen. However, six patients discontinued treatment before reaching the 144-week mark.</p><p><strong>Conclusion: </strong>Our findings confirm that DTG+DRV/c is an effective and well-tolerated switch therapy regimen for treatment-experienced patients with HIV, with sustained benefits observed for up to 144 weeks of follow-up. 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引用次数: 0
摘要
背景:对于对核苷类逆转录酶抑制剂耐药或不耐受的人类免疫缺陷病毒(HIV)患者,尤其是那些有治疗失败史的患者来说,多鲁曲韦加科比司他增效达鲁那韦(DTG+DRV/c)双方案是一种很有前景的替代方案:我们纳入了一家三级大学医院所有改用 DTG+DRV/c 方案的有治疗经验的 HIV 患者。我们通过系列实验室数据和临床结果评估了该方案的有效性、安全性和耐受性。主要终点是血浆 HIV-RNA 水平的患者比例:我们的回顾性分析涉及 40 名患者。转用 DTG+DRV/c 的主要原因是:17 名患者(42.5%)治疗失败;15 名患者(37.5%)在使用过多种治疗方案后进行了简化;8 名患者(20.0%)出现药物不良反应。在治疗失败组的 17 名患者中,我们观察到,在开始使用双重疗法后,病毒抑制率有所提高,CD4+ T 细胞计数也有所改善。在非治疗失败组(23 名患者)中,病毒抑制和 CD4+ T 细胞水平始终保持不变。切换后,肾功能、肝功能、血糖水平或血脂概况均未出现明显变化。耐受性较高,34/40 的患者(85.0%)对治疗方案反应良好。然而,有6名患者在治疗144周之前中断了治疗:我们的研究结果证实,DTG+DRV/c 对有治疗经验的艾滋病患者来说是一种有效且耐受性良好的转换治疗方案,可在长达 144 周的随访中持续获益。该方案显示出对不同患者群体的适应性,并显示出病毒学和免疫学方面的改善,尤其是对有治疗失败史的患者。
Effectiveness and Tolerability of Dual Therapy with Dolutegravir Plus Darunavir/cobicistat in Treatment-Experienced Patients with HIV: A 144-Week Follow-Up.
Background: A dual regimen with dolutegravir plus cobicistat-boosted darunavir (DTG+DRV/c) is a promising alternative for patients with human immunodeficiency virus (HIV) with resistance or intolerance to nucleoside reverse transcriptase inhibitors, especially those with a history of treatment failure.
Materials and methods: We included all treatment-experienced patients with HIV who switched to the DTG+DRV/c regimen at a tertiary university hospital. We assessed the regimen's effectiveness, safety, and tolerability through serial laboratory data and clinical findings. The primary endpoint was the proportion of patients with plasma HIV-RNA levels <50 copies/mL at week 144 post-switch. The secondary endpoints were safety and tolerability assessments.
Results: Our retrospective analysis involved 40 patients. The leading reasons for switching to DTG+DRV/c were treatment failure in 17 patients (42.5%), simplification after multiple previous regimens in 15 (37.5%), and adverse drug reactions in 8 (20.0%). Among the 17 patients in the treatment failure group, we observed enhanced viral suppression and improved CD4+ T-cell counts after initiating the dual regimen. In the non-treatment failure group (23 patients), viral suppression and CD4+ T-cell levels were consistently maintained. No significant alterations in renal function, liver function, glucose levels, or lipid profiles were observed post-switch. High tolerability was observed, with 34/40 patients (85.0%) responding well to the regimen. However, six patients discontinued treatment before reaching the 144-week mark.
Conclusion: Our findings confirm that DTG+DRV/c is an effective and well-tolerated switch therapy regimen for treatment-experienced patients with HIV, with sustained benefits observed for up to 144 weeks of follow-up. This regimen showed adaptability across different patient groups and demonstrated virological and immunological improvements, particularly in patients with a history of treatment failure.
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