Safety and pharmacokinetics of VRC07-523LS administered via different routes and doses (HVTN 127/HPTN 087): A Phase I randomized clinical trial.

IF 15.8 1区 医学 Q1 Medicine
PLoS Medicine Pub Date : 2024-06-24 eCollection Date: 2024-06-01 DOI:10.1371/journal.pmed.1004329
Stephen R Walsh, Cynthia L Gay, Shelly T Karuna, Ollivier Hyrien, Timothy Skalland, Kenneth H Mayer, Magdalena E Sobieszczyk, Lindsey R Baden, Paul A Goepfert, Carlos Del Rio, Guiseppe Pantaleo, Philip Andrew, Carissa Karg, Zonglin He, Huiyin Lu, Carmen A Paez, Jane A G Baumblatt, Laura L Polakowski, Wairimu Chege, Maija A Anderson, Sophie Janto, Xue Han, Yunda Huang, Julie Dumond, Margaret E Ackerman, Adrian B McDermott, Britta Flach, Estelle Piwowar-Manning, Kelly Seaton, Georgia D Tomaras, David C Montefiori, Lucio Gama, John R Mascola
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A total of 124 participants were randomized to receive 5 VRC07-523LS administrations via IV (T1: 2.5 mg/kg, T2: 5 mg/kg, T3: 20 mg/kg), subcutaneous (SC) (T4: 2.5 mg/kg, T5: 5 mg/kg), or intramuscular (IM) (T6: 2.5 mg/kg or P6: placebo) routes at 4-month intervals. Participants and site staff were blinded to VRC07-523LS versus placebo for the IM group, while all other doses and routes were open-label. Safety data were collected for 144 weeks following the first administration. VRC07-523LS serum concentrations were measured by ELISA through Day 112 in all participants and by binding antibody multiplex assay (BAMA) thereafter in 60 participants (10 per treatment group) through Day 784. Compartmental population pharmacokinetic (PK) analyses were conducted to evaluate the VRC07-523LS serum PK. Neutralization activity was measured in a TZM-bl assay and antidrug antibodies (ADAs) were assayed using a tiered bridging assay testing strategy. 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引用次数: 0

Abstract

Background: Broadly neutralizing antibodies (bnAbs) are a promising approach for HIV-1 prevention. In the Antibody Mediated Prevention (AMP) trials, a CD4-binding site targeting bnAb, VRC01, administered intravenously (IV), demonstrated 75% prevention efficacy against highly neutralization-sensitive viruses but was ineffective against less sensitive viruses. VRC07-523LS is a next-generation bnAb targeting the CD4-binding site and was engineered for increased neutralization breadth and half-life. We conducted a multicenter, randomized, partially blinded Phase I clinical trial to evaluate the safety and serum concentrations of VRC07-523LS, administered in multiple doses and routes to healthy adults without HIV.

Methods and findings: Participants were recruited between 2 February 2018 and 9 October 2018. A total of 124 participants were randomized to receive 5 VRC07-523LS administrations via IV (T1: 2.5 mg/kg, T2: 5 mg/kg, T3: 20 mg/kg), subcutaneous (SC) (T4: 2.5 mg/kg, T5: 5 mg/kg), or intramuscular (IM) (T6: 2.5 mg/kg or P6: placebo) routes at 4-month intervals. Participants and site staff were blinded to VRC07-523LS versus placebo for the IM group, while all other doses and routes were open-label. Safety data were collected for 144 weeks following the first administration. VRC07-523LS serum concentrations were measured by ELISA through Day 112 in all participants and by binding antibody multiplex assay (BAMA) thereafter in 60 participants (10 per treatment group) through Day 784. Compartmental population pharmacokinetic (PK) analyses were conducted to evaluate the VRC07-523LS serum PK. Neutralization activity was measured in a TZM-bl assay and antidrug antibodies (ADAs) were assayed using a tiered bridging assay testing strategy. Injections and infusions were well tolerated, with mild pain or tenderness reported commonly in the SC and IM groups, and mild to moderate erythema or induration reported commonly in the SC groups. Infusion reactions were reported in 3 of 20 participants in the 20 mg/kg IV group. Peak geometric mean (GM) concentrations (95% confidence intervals [95% CIs]) following the first administration were 29.0 μg/mL (25.2, 33.4), 58.5 μg/mL (49.4, 69.3), and 257.2 μg/mL (127.5, 518.9) in T1-T3 with IV dosing; 10.8 μg/mL (8.8, 13.3) and 22.8 μg/mL (20.1, 25.9) in T4-T5 with SC dosing; and 16.4 μg/mL (14.7, 18.2) in T6 with IM dosing. Trough GM (95% CIs) concentrations immediately prior to the second administration were 3.4 μg/mL (2.5, 4.6), 6.5 μg/mL (5.6, 7.5), and 27.2 μg/mL (23.9, 31.0) with IV dosing; 0.97 μg/mL (0.65, 1.4) and 3.1 μg/mL (2.2, 4.3) with SC dosing, and 2.6 μg/mL (2.05, 3.31) with IM dosing. Peak VRC07-523LS serum concentrations increased linearly with the administered dose. At a given dose, peak and trough concentrations, as well as serum neutralization titers, were highest in the IV groups, reflecting the lower bioavailability following SC and IM administration. A single participant was found to have low titer ADA at a lone time point. VRC07-523LS has an estimated mean half-life of 42 days across all doses and routes (95% CI: 40.5, 43.5), over twice as long as VRC01 (15 days).

Conclusions: VRC07-523LS was safe and well tolerated across a range of doses and routes and is a promising long-acting bnAb for inclusion in HIV-1 prevention regimens.

Trial registration: ClinicalTrials.gov/ NCT03387150 (posted on 21 December 2017).

通过不同途径和剂量给药的 VRC07-523LS 的安全性和药代动力学(HVTN 127/HPTN 087):一期随机临床试验。
背景:广谱中和抗体(bnAbs)是一种很有前景的 HIV-1 预防方法。在抗体介导的预防(AMP)试验中,一种以 CD4 结合位点为靶点的 bnAb(VRC01)经静脉注射(IV)后,对中和敏感性高的病毒有 75% 的预防效果,但对敏感性较低的病毒无效。VRC07-523LS 是以 CD4 结合位点为靶点的新一代 bnAb,其设计可提高中和广度和半衰期。我们开展了一项多中心、随机、部分盲法的 I 期临床试验,以评估 VRC07-523LS 的安全性和血清浓度:参与者招募时间为 2018 年 2 月 2 日至 2018 年 10 月 9 日。共有 124 名参与者被随机分配到通过静脉注射(T1:2.5 mg/kg,T2:5 mg/kg,T3:20 mg/kg)、皮下注射(SC)(T4:2.5 mg/kg,T5:5 mg/kg)或肌内注射(IM)(T6:2.5 mg/kg或P6:安慰剂)途径接受 5 次 VRC07-523LS 给药,间隔时间为 4 个月。对于IM组的VRC07-523LS与安慰剂,参与者和研究机构的工作人员均为盲人,而所有其他剂量和途径均为开放标签。在首次给药后的 144 周内收集了安全性数据。所有参与者的 VRC07-523LS 血清浓度在第 112 天之前通过 ELISA 法进行测量,之后在第 784 天之前通过结合抗体多重测定法 (BAMA) 对 60 名参与者(每个治疗组 10 人)进行测量。为评估 VRC07-523LS 血清 PK,进行了区组群体药代动力学 (PK) 分析。中和活性通过 TZM-bl 试验测定,抗药抗体 (ADAs) 通过分层桥接试验策略测定。注射和输液的耐受性良好,SC 组和 IM 组常见轻度疼痛或触痛,SC 组常见轻度至中度红斑或压痕。在 20 毫克/千克静脉注射组的 20 名参与者中,有 3 人出现输液反应。首次给药后的峰值几何平均(GM)浓度(95% 置信区间 [95% CIs])分别为 29.0 μg/mL(25.2, 33.4)、58.5 μg/mL(49.4, 69.3)和 257.T1-T3采用静脉给药,为10.8 μg/mL(8.8,13.3)和22.8 μg/mL(20.1,25.9);T6采用IM给药,为16.4 μg/mL(14.7,18.2)。第二次给药前的最低 GM 浓度(95% CIs)分别为 3.4 μg/mL (2.5, 4.6)、6.5 μg/mL (5.6, 7.5) 和 27.静脉注射时为 0.97 μg/mL (0.65, 1.4) 和 3.1 μg/mL (2.2, 4.3),IM 注射时为 2.6 μg/mL (2.05, 3.31)。VRC07-523LS 的血清浓度峰值随给药剂量呈线性增长。在给定剂量下,静脉注射组的峰值和谷值浓度以及血清中和滴度最高,反映出静脉注射和间歇给药的生物利用度较低。在一个单独的时间点上,发现一名参试者的 ADA 滴度较低。在所有剂量和途径中,VRC07-523LS的平均半衰期估计为42天(95% CI:40.5, 43.5),是VRC01(15天)的两倍多:结论:VRC07-523LS在各种剂量和途径下均安全且耐受性良好,是一种很有希望纳入HIV-1预防方案的长效bnAb:试验注册:ClinicalTrials.gov/ NCT03387150(2017年12月21日发布)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
PLoS Medicine
PLoS Medicine MEDICINE, GENERAL & INTERNAL-
CiteScore
17.60
自引率
0.60%
发文量
227
审稿时长
4-8 weeks
期刊介绍: PLOS Medicine is a prominent platform for discussing and researching global health challenges. The journal covers a wide range of topics, including biomedical, environmental, social, and political factors affecting health. It prioritizes articles that contribute to clinical practice, health policy, or a better understanding of pathophysiology, ultimately aiming to improve health outcomes across different settings. The journal is unwavering in its commitment to uphold the highest ethical standards in medical publishing. This includes actively managing and disclosing any conflicts of interest related to reporting, reviewing, and publishing. PLOS Medicine promotes transparency in the entire review and publication process. The journal also encourages data sharing and encourages the reuse of published work. Additionally, authors retain copyright for their work, and the publication is made accessible through Open Access with no restrictions on availability and dissemination. PLOS Medicine takes measures to avoid conflicts of interest associated with advertising drugs and medical devices or engaging in the exclusive sale of reprints.
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