Lack of Toxicity and Persistence in the Mouse Associated with Administration of Candidate DNA- and Modified Vaccinia Virus Ankara (MVA)-based HIV Vaccines for Kenya
Overview
Affiliations
Toxicity, biodistribution and persistence of candidate HIV vaccines pTHr.HIVA, a recombinant DNA, and MVA.HIVA, a recombinant modified vaccinia virus Ankara, were determined in the Balb/c mouse. The mice were injected with either two doses of intramuscular pTHr.HIVA DNA (50 microg each, separated by an interval of 14 days), two doses of intradermal MVA.HIVA (10(6) plaque-forming units each, separated by an interval of 14 days), or a combination of the two vaccines, each given in two doses, in a prime-boost regimen. The study showed no significant toxic effects, either local or systemic, under any of these employed dosing regimens. With the exception of the sites of delivery, the vaccine-derived HIVA DNA sequences were undetectable 5 weeks after the last dosing. Thus, both the vaccines alone and in a combination were considered safe and suitable for the use in phase I trials in humans.
Shimada M, Wang H, Ichino M, Ura T, Mizuki N, Okuda K Gene Ther. 2022; 29(10-11):636-642.
PMID: 34987192 DOI: 10.1038/s41434-021-00308-z.
Langenmayer M, Lulf-Averhoff A, Adam-Neumair S, Fux R, Sutter G, Volz A Biologicals. 2018; 54:58-62.
PMID: 29759890 PMC: 7128986. DOI: 10.1016/j.biologicals.2018.05.004.
La Rosa C, Longmate J, Martinez J, Zhou Q, Kaltcheva T, Tsai W Blood. 2016; 129(1):114-125.
PMID: 27760761 PMC: 5216266. DOI: 10.1182/blood-2016-07-729756.
DNA Immunization for HIV Vaccine Development.
Chen Y, Wang S, Lu S Vaccines (Basel). 2015; 2(1):138-59.
PMID: 26344472 PMC: 4494200. DOI: 10.3390/vaccines2010138.
Goossens M, Pauwels K, Willemarck N, Breyer D Curr Gene Ther. 2014; 13(6):413-20.
PMID: 24397528 PMC: 4031919. DOI: 10.2174/156652321306140103221941.