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住院患者服用比克替拉韦/恩曲他滨/替诺福韦艾拉酚胺后病毒载量增加:病例报告及文献复习。

Increased viral load in a hospitalized patient on treatment with crushed bictegravir/emtricitabine/tenofovir alafenamide: A case report and review of the literature.

机构信息

Medical University of South Carolina College of Pharmacy, Charleston, SC, USA.

University of South Carolina College of Pharmacy, Columbia, SC, USA.

出版信息

Am J Health Syst Pharm. 2022 Aug 5;79(16):1330-1336. doi: 10.1093/ajhp/zxac120.

Abstract

PURPOSE

To describe a case of increased viral load in a patient with HIV-1 infection receiving treatment with crushed bictegravir/emtricitabine/tenofovir alafenamide (B/FTC/TAF).

SUMMARY

A 43-year-old man, newly diagnosed with HIV, was hospitalized due to failure to thrive, neurological changes, and hypotension. Before treatment, the HIV viral load (VL) was 769,704 copies/mL and the CD4+ T-cell count was 36 cells/μL. On hospital day (HD) 8, B/FTC/TAF by mouth daily was initiated. During the hospitalization, the patient's course was complicated by opportunistic infections, bilateral pneumothorax, seizure activity, and acute respiratory distress, requiring multiple intubations and extended time in the intensive care unit. A repeat VL measurement on HD 28 was 5,887 copies/mL after the patient had received 14 of 20 scheduled B/FTC/TAF doses. Because of a failed swallow study and continued nutritional deficits, a percutaneous endoscopic gastrostomy (PEG) tube was placed on HD 38 and continuous tube feeds via the PEG tube were initiated. Subsequently, the B/FTC/TAF order was modified to be crushed, mixed in 30 mL water, and administered daily via the PEG tube. A repeat VL measurement on HD 65 showed an increase to 8,047 copies/mL, despite receipt of 37 consecutive doses of B/FTC/TAF. B/FTC/TAF was discontinued and dolutegravir 50 mg twice daily, darunavir 800 mg plus ritonavir 100 mg (DRV/r), and tenofovir disoproxil fumarate/FTC 300 mg/200 mg were started due to virological increase, need for a viable option compatible with PEG tube delivery, and potential for integrase inhibitor resistance. At the time of regimen change (HD 67), a resistance panel showed minor mutations, E157Q and V118I. The regimen was streamlined with discontinuation of DRV/r on HD 92. The patient was discharged on HD 161. The PEG tube was removed 2 months after discharge, oral B/FTC/TAF was reinitiated, and the patient was virologically suppressed at 1 year after discharge.

CONCLUSION

Controlled studies are needed to verify acceptable pharmacokinetic and pharmacodynamic metrics for crushed B/FTC/TAF given via tube, with and without tube feeds, before use in this manner.

摘要

目的

描述 1 例接受比克替拉韦/恩曲他滨/丙酚替诺福韦(B/FTC/TAF)治疗的 HIV-1 感染者病毒载量(VL)增加的病例。

摘要

一位 43 岁男性,新诊断为 HIV 感染,因生长不良、神经改变和低血压住院。治疗前,HIV VL 为 769704 拷贝/mL,CD4+T 细胞计数为 36 个/μL。入院第 8 天,开始口服 B/FTC/TAF 每日 1 次。住院期间,患者并发机会性感染、双侧气胸、癫痫发作和急性呼吸窘迫,需要多次插管和长时间入住重症监护病房。在接受了 20 次 B/FTC/TAF 计划剂量中的 14 次后,入院第 28 天重复测量 VL 为 5887 拷贝/mL。由于吞咽研究失败和持续的营养不足,入院第 38 天放置了经皮内镜胃造口术(PEG)管,并开始通过 PEG 管进行连续管饲。随后,将 B/FTC/TAF 方案修改为粉碎,混合在 30 mL 水中,每日通过 PEG 管给药。入院第 65 天重复测量 VL 显示,尽管连续接受了 37 次 B/FTC/TAF 治疗,但 VL 增至 8047 拷贝/mL。由于病毒学增加、需要与 PEG 管输送兼容的可行选择以及整合酶抑制剂耐药的潜在可能性,停止使用 B/FTC/TAF,并开始使用多替拉韦 50 mg 每日 2 次、达芦那韦 800 mg 加利托那韦 100 mg(DRV/r)和富马酸替诺福韦二吡呋酯/FTC 300 mg/200 mg。在改变治疗方案时(入院第 67 天),耐药性分析显示存在次要突变 E157Q 和 V118I。入院第 92 天停止使用 DRV/r。入院第 161 天患者出院。出院后 2 个月取出 PEG 管,口服 B/FTC/TAF 重新开始,出院后 1 年病毒学抑制。

结论

在以这种方式使用之前,需要进行对照研究来验证通过管饲给予粉碎的 B/FTC/TAF 的可接受的药代动力学和药效学指标,包括有和无管饲的情况。

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