BACKGROUND: Human monoclonal antibodies that potently and broadly neutralise HIV-1 are under development to prevent and treat HIV-1 infection. In this phase 1 clinical trial we aimed to determine the safety, tolerability, and pharmacokinetic profile of the broadly neutralising monoclonal antibody VRC07-523LS, an engineered variant of VRC01 that targets the CD4 binding site of the HIV-1 envelope protein. METHODS: This phase 1, open-label, dose-escalation clinical trial was done at the National Institutes of Health Clinical Center in Bethesda, MD, USA. Individuals were recruited from the greater Washington, DC, area by IRB-approved written and electronic media. We enrolled healthy, HIV-1-negative adults aged 18-50 years. Inclusion criteria were good general health, measured through clinical laboratory tests, medical history, and physical examination. Participants self-selected into one of seven open groups during enrolment without randomisation. Four groups received a single intravenous dose of 1, 5, 20, or 40 mg/kg of VRC07-523LS, and one group received a single 5 mg/kg subcutaneous dose. Two groups received three doses of either 20 mg/kg intravenous VRC07-523LS, or 5 mg/kg subcutaneous VRC07-523LS at 12-week intervals. The primary outcome was the safety and tolerability of VRC07-523LS, assessed by dose, route, and number of administrations. This study is registered with ClinicalTrials.gov, NCT03015181. FINDINGS:Between Feb 21, 2017, and September 13, 2017, we enrolled 26 participants, including 11 (42%) men and 15 (58%) women. Two (8%) participants withdrew from the study early: one participant in group 1 enrolled in the study but never received VRC07-523LS, and one participant in group 6 chose to withdraw after a single administration. One (4%) participant in group 7 received only one of the three scheduled administrations. 17 participants received intravenous administrations and 8 participants received subcutaneous administrations. VRC07-523LS was safe and well tolerated, we observed no serious adverse events or dose-limiting toxic effects. All reported local and systemic reactogenicity was mild to moderate in severity. The most commonly reported symptoms following intravenous administration were malaise or myalgia in three (18%) participants and headache or chills in two (12%) participants. The most commonly reported symptoms following subcutaneous administration were pain and tenderness in four participants (50%) and malaise or headache in three (38%) participants. INTERPRETATION:Safe and well tolerated, VRC07-523LS is a strong and practical candidate for inclusion in HIV-1 prevention and therapeutic strategies. The results from this trial also indicate that an HIV-1 broadly neutralising monoclonal antibody engineered for improved pharmacokinetic and neutralisation properties can be safe for clinical use. FUNDING: National Institutes of Health.
RCT Entities:
BACKGROUND:Human monoclonal antibodies that potently and broadly neutralise HIV-1 are under development to prevent and treat HIV-1 infection. In this phase 1 clinical trial we aimed to determine the safety, tolerability, and pharmacokinetic profile of the broadly neutralising monoclonal antibody VRC07-523LS, an engineered variant of VRC01 that targets the CD4 binding site of the HIV-1 envelope protein. METHODS: This phase 1, open-label, dose-escalation clinical trial was done at the National Institutes of Health Clinical Center in Bethesda, MD, USA. Individuals were recruited from the greater Washington, DC, area by IRB-approved written and electronic media. We enrolled healthy, HIV-1-negative adults aged 18-50 years. Inclusion criteria were good general health, measured through clinical laboratory tests, medical history, and physical examination. Participants self-selected into one of seven open groups during enrolment without randomisation. Four groups received a single intravenous dose of 1, 5, 20, or 40 mg/kg of VRC07-523LS, and one group received a single 5 mg/kg subcutaneous dose. Two groups received three doses of either 20 mg/kg intravenous VRC07-523LS, or 5 mg/kg subcutaneous VRC07-523LS at 12-week intervals. The primary outcome was the safety and tolerability of VRC07-523LS, assessed by dose, route, and number of administrations. This study is registered with ClinicalTrials.gov, NCT03015181. FINDINGS: Between Feb 21, 2017, and September 13, 2017, we enrolled 26 participants, including 11 (42%) men and 15 (58%) women. Two (8%) participants withdrew from the study early: one participant in group 1 enrolled in the study but never received VRC07-523LS, and one participant in group 6 chose to withdraw after a single administration. One (4%) participant in group 7 received only one of the three scheduled administrations. 17 participants received intravenous administrations and 8 participants received subcutaneous administrations. VRC07-523LS was safe and well tolerated, we observed no serious adverse events or dose-limiting toxic effects. All reported local and systemic reactogenicity was mild to moderate in severity. The most commonly reported symptoms following intravenous administration were malaise or myalgia in three (18%) participants and headache or chills in two (12%) participants. The most commonly reported symptoms following subcutaneous administration were pain and tenderness in four participants (50%) and malaise or headache in three (38%) participants. INTERPRETATION: Safe and well tolerated, VRC07-523LS is a strong and practical candidate for inclusion in HIV-1 prevention and therapeutic strategies. The results from this trial also indicate that an HIV-1 broadly neutralising monoclonal antibody engineered for improved pharmacokinetic and neutralisation properties can be safe for clinical use. FUNDING: National Institutes of Health.
Authors: Joseph P Casazza; Evan M Cale; Sandeep Narpala; Galina V Yamshchikov; Emily E Coates; Cynthia S Hendel; Laura Novik; LaSonji A Holman; Alicia T Widge; Preeti Apte; Ingelise Gordon; Martin R Gaudinski; Michelle Conan-Cibotti; Bob C Lin; Martha C Nason; Olga Trofymenko; Shinyi Telscher; Sarah H Plummer; Diane Wycuff; William C Adams; Janardan P Pandey; Adrian McDermott; Mario Roederer; Avery N Sukienik; Sijy O'Dell; Jason G Gall; Britta Flach; Travis L Terry; Misook Choe; Wei Shi; Xuejun Chen; Florence Kaltovich; Kevin O Saunders; Judy A Stein; Nicole A Doria-Rose; Richard M Schwartz; Alejandro B Balazs; David Baltimore; Gary J Nabel; Richard A Koup; Barney S Graham; Julie E Ledgerwood; John R Mascola Journal: Nat Med Date: 2022-04-11 Impact factor: 87.241
Authors: Cynthia L Gay; Katherine S James; Marina Tuyishime; Shane D Falcinelli; Sarah B Joseph; Matthew J Moeser; Brigitte Allard; Jennifer L Kirchherr; Matthew Clohosey; Samuel L M Raines; David C Montefiori; Xiaoying Shen; Robert J Gorelick; Lucio Gama; Adrian B McDermott; Richard A Koup; John R Mascola; Michelle Floris-Moore; JoAnn D Kuruc; Guido Ferrari; Joseph J Eron; Nancie M Archin; David M Margolis Journal: J Infect Dis Date: 2022-03-02 Impact factor: 7.759
Authors: Gregory D Sempowski; Kevin O Saunders; Priyamvada Acharya; Kevin J Wiehe; Barton F Haynes Journal: Cell Date: 2020-05-27 Impact factor: 41.582
Authors: Jerry Li; Mina Nikanjam; Coleen K Cunningham; Elizabeth J McFarland; Emily E Coates; Katherine V Houser; Bob C Lin; Adrian B McDermott; Britta Flach; Lucio Gama; Richard A Koup; Barney S Graham; John R Mascola; Julie E Ledgerwood; Edmund V Capparelli Journal: Clin Pharmacol Ther Date: 2020-10-03 Impact factor: 6.875
Authors: Deborah J Anderson; Joseph A Politch; Richard A Cone; Larry Zeitlin; Samuel K Lai; Philip J Santangelo; Thomas R Moench; Kevin J Whaley Journal: Biol Reprod Date: 2020-08-04 Impact factor: 4.161