A Phase 1, Dosage-Escalation Study of the Safety and Immunogenicity of a Novel Rabies Vaccine ChAd155-RG vs. the Comparator RABAVERT Vaccine in Healthy Adult Subjects

This is a single-center, observer-blinded, dosage-escalation trial to evaluate the safety, tolerability, reactogenicity, and immunogenicity of ChAd155-RG compared with RABAVERT in rabies virus-naïve healthy male and non-pregnant female adult subjects ages 18-49. There are 4 dose groups: Group A will receive ChAd155-RG at the lower dosage (5x1010vp) on Day 1, then placebo injections on Days 8, 15, and 22; Group B will receive ChAd155-RG at the higher dosage (1x1011vp) on Day 1, then placebo injections on Days 8, 15, and 22; Group C will receive ChAd155-RG at the higher dosage (1x1011vp) on Days 1 and 15, and placebo injections on Days 8 and 22; Group D will receive RABAVERT at the standard dose (1 mL) on Days 1, 8, and 22, and a placebo injection on Day 15. Since this is a dosage-escalation study, sentinel subjects will be used at each dosage level before non-sentinel subjects will be enrolled. The study will be conducted at Emory University Vaccine and Treatment Evaluation Unit (VTEU). This trial is expected to take approximately 48 months to complete. The duration of each subject's participation is approximately 13 months, from recruitment through the last study visit. The primary objectives of this study are: 1) Assessment of the safety, tolerability, and reactogenicity of one dose of ChAd155-RG at 5x1010vp per dose, or one or two doses of ChAd155-RG at 1x1011vp per dose; 2) Comparison of the safety, tolerability, and reactogenicity of one or two doses of ChAd155-RG, with three doses of RABAVERT.

Start Date19 Sep 2019

Sponsor / Collaborator

National Institute of Allergy & Infectious Diseases

100 Clinical Results associated with ChAd155-RG

100 Translational Medicine associated with ChAd155-RG

100 Patents (Medical) associated with ChAd155-RG

Literatures (Medical) associated with ChAd155-RG

01 Dec 2024·Vaccine

Safety and immunogenicity of a ChAd155-vectored rabies vaccine compared with inactivated, purified chick embryo cell rabies vaccine in healthy adults

Article

Author: Scherer, Erin M ; Rouphael, Nadine G. ; Phadke, Varun K. ; Rebolledo, Paulina A ; Girmay, Tigisty ; Gromer, Daniel J ; Vitelli, Alessandra ; Phadke, Varun K ; Rouphael, Nadine G ; Sherman, Amy C. ; Graciaa, Daniel S. ; Neill-Gubitz, Hannah ; Rebolledo, Paulina A. ; Sommella, Andrea ; Sherman, Amy C ; Mulligan, Mark J. ; Mulligan, Mark J ; Graciaa, Daniel S ; Capone, Stefania ; McCullough, Michele P ; Wiley, Zanthia ; Koller, Mark ; McCullough, Michele P. ; Gromer, Daniel J. ; Leary, Maranda ; Min, Ji-Young ; Tsong, Rachel ; Seetahal, Janine ; Scherer, Erin M. ; Retallick, Jamie

BACKGROUNDRabies is a zoonotic viral encephalitis that is endemic in many countries and confers a high mortality. Licensed vaccines require several doses to ensure efficacy. To investigate a logistically favorable approach, we assessed the safety and immunogenicity of ChAd155-RG, a novel investigational rabies vaccine using a replication-defective chimpanzee adenovirus vector.METHODSWe conducted a first-in-human, phase 1, randomized, double-blind, dose-escalation trial comparing ChAd155-RG with a licensed inactivated vaccine (RabAvert) in healthy adults. Participants received either RabAvert at standard dosing or ChAd155-RG at a low dose for one immunization or a high dose for one or two immunizations. To assess safety, we evaluated reactogenicity, unsolicited adverse events, and thrombotic events. To measure immunogenicity, we measured rabies viral neutralizing antibody (VNA) titers and anti-ChAd155 neutralizing antibodies.RESULTSMild to moderate systemic reactogenicity and transient lymphopenia and neutropenia were more common among recipients of ChAd155-RG compared with those who received RabAvert. No thrombotic events or serious adverse events were reported. Only the groups receiving RabAvert or two doses of high-dose ChAd155-RG achieved 100 % seroconversion, and seroprotection was most durable in the RabAvert group. Most participants had preexisting anti-vector antibodies, which were boosted by ChAd155-RG. Baseline and post-vaccination anti-vector antibody titers were negatively associated with post-vaccination rabies VNA titers.CONCLUSIONSIn this phase 1 clinical trial, a novel rabies vaccine using a simian adenovirus vector was safe and tolerable, but generated lower, less durable rabies VNA titers than a standard inactivated rabies virus vaccine, which may be due to preexisting, anti-vector immunity.

PLOS Neglected Tropical DiseasesQ2 · MEDICINE

A next generation vaccine against human rabies based on a single dose of a chimpanzee adenovirus vector serotype C

Q2 · MEDICINE

ArticleOA

Author: Esposito, Marialuisa ; Vitelli, Alessandra ; Capone, Stefania ; Merone, Rossella ; Contino, Alessandra Maria ; Urbanowicz, Richard A ; Folgori, Antonella ; Abbate, Adele ; Wizel, Benjamin ; Horncastle, Emma ; Nicosia, Alfredo ; Sbrocchi, Roberta ; Duncan, Joshua D ; Napolitano, Federico ; Ball, Jonathan K ; Sommella, Andrea ; Hinds, Jospeh ; Ammendola, Virginia ; Colloca, Stefano ; Lahm, Armin ; Lanzaro, Francesca

Rabies, caused by RNA viruses in the Genus Lyssavirus, is the most fatal of all infectious diseases. This neglected zoonosis remains a major public health problem in developing countries, causing the death of an estimated 25,000-159,000 people each year, with more than half of them in children. The high incidence of human rabies in spite of effective vaccines is mainly linked to the lack of compliance with the complicated administration schedule, inadequacies of the community public health system for local administration by the parenteral route and the overall costs of the vaccine. The goal of our work was the development of a simple, affordable and effective vaccine strategy to prevent human rabies virus infection. This next generation vaccine is based on a replication-defective chimpanzee adenovirus vector belonging to group C, ChAd155-RG, which encodes the rabies glycoprotein (G). We demonstrate here that a single dose of this vaccine induces protective efficacy in a murine model of rabies challenge and elicits strong and durable neutralizing antibody responses in vaccinated non-human primates. Importantly, we demonstrate that one dose of a commercial rabies vaccine effectively boosts the neutralizing antibody responses induced by ChAd155-RG in vaccinated monkeys, showing the compatibility of the novel vectored vaccine with the current post-exposure prophylaxis in the event of rabies virus exposure. Finally, we demonstrate that antibodies induced by ChAd155-RG can also neutralize European bat lyssaviruses 1 and 2 (EBLV-1 and EBLV-2) found in bat reservoirs.

100 Deals associated with ChAd155-RG

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Indication	Highest Phase	Country/Location	Organization	Date
Vaccination	Phase 1	US	National Institute of Allergy & Infectious Diseases	19 Sep 2019
Rabies	Phase 1	-	National Institutes of Health	-

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT04019444 (CTgov)	Phase 1	Rabies \| Vaccination	50	ChAd155-RG (Low Dose ChAd155-RG)	gcymfiykfy(sbtdbkuzhs) = bugosrzotk vayspkwsnz (kkrmxrmtde, wayivvvqvc - izgcbywsio) View more	-	10 Apr 2024
				ChAd155-RG (x1) (High Dose ChAd155-RG (x1))	gcymfiykfy(sbtdbkuzhs) = wfdarmeagx vayspkwsnz (kkrmxrmtde, iyhvckmpej - inkjybptbb) View more

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