If it's the latter, adenovirus containing the DNA sequence for a human antibody. then my understanding of the Oxford Group's vaccine (ChAdOx1 nCoV-19) is incorrect. So are a number of news reports:
Quoted from
Genetic Engineering & Biotechnology News:
AstraZeneca will oversee global development, manufacturing, and distribution of the COVID-19 vaccine candidate that was created by researchers at University of Oxford, and is now being studied in a human clinical trial launched last week.
www.genengnews.com
"ChAdOx1 nCoV-19 uses a viral vector based on a weakened version of the adenovirus containing the genetic material of SARS-CoV-2 spike protein. After vaccination, the surface spike protein is produced, which primes the immune system to attack COVID-19 if it later infects the body. The recombinant adenovirus vector (ChAdOx1) is designed to generate a strong immune response from a single dose and to not replicate, in order to preclude causing an ongoing infection in the vaccinated individual."
Here is another news report from Trial Site News:
University of Oxford investigators have initiated enrollment of healthy participants in a trial testing the COVID-19 vaccine candidate called ChAdOx1 nCoV-19. Originally developed to target MERS, it is based on an adenovirus vaccine vector and the COVID-19 spike protein. It is currently being...
www.trialsitenews.com
"University of Oxford investigators have initiated enrollment of healthy participants in a trial testing the COVID-19 vaccine candidate called ChAdOx1 nCoV-19. Originally developed to target MERS, it is based on an adenovirus vaccine vector and the COVID-19 spike protein."
The
Clinical Trial for this vaccine, NCT04324606, is described at Clinical Trials.gov.
clinicaltrials.gov
The vaccine will be given intramuscularly (IM). If so, the coded sequence will be expressed for a while, but lasting immunity is less likely to happen.
The central issue is whether better results come with antibody-based immunity or with both T cell-based immunity plus antibody-based immunity. If the Oxford vaccine contains DNA code for the SARS-CoV-2 S protein then both types of immunity are possible. But if the Oxford vaccine codes for a neutralizing human antibody directed against the S protein, then no T cell-based immunity is possible. This is widely understood to be much less desirable.
I don't believe the Oxford Group is going about doing this all wrong. But I wonder which is correct, that the Ad-5 vector contains SARS-CoV-2 S protein sequence, or that the vector contains sequence for human antibody directed against S protein.
Do you have a link that directly answers this question? A scientific report or review would be better than a news article.
