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Vaccine platforms employed for available and candidate COVID-19 vaccines

Vaccine platforms employed for available and candidate COVID-19 vaccines
Platform type Description COVID-19 vaccine examples* Other vaccine examples Comments
Whole virus vaccines
Inactivated vaccines
  • Produced by growing SARS-CoV-2 in cell culture then chemically inactivating the virus.
  • Often combined with an adjuvant to stimulate immune response.
  • CoronaVac (Sinovac)
  • BBIBP-CorV/HB02 (Covilo, Sinopharm [Beijing])
  • Covaxin (Bharat Biotech)
  • Hepatitis A vaccine
  • Inactivated poliovirus vaccine
  • Immune response targets multiple viral antigens.
Live attenuated vaccines
  • Produced by developing weakened versions of wild-type SARS-CoV-2 through genetic modification or growth in adverse conditions.
  • COVI-VAC (Codagenix/Serum Institute of India) – in early trials
  • Measles, mumps, rubella vaccine
  • Varicella vaccine
  • Immune response targets multiple viral antigens.
  • Can be administered intranasally and thus might induce mucosal immune response at the site of viral entry.
  • Theoretic concern about reversion to or recombination with wild-type virus.
  • Not appropriate for immunocompromised individuals.
Viral component vaccines
mRNA vaccines
  • Consist of mRNA encoding target gene.
  • Once administered, mRNA is translated into target protein, which elicits immune response.
  • BNT162b2 (Pfizer-BioNTech vaccine)
  • mRNA-1273 (Moderna vaccine)
 
  • mRNA remains in cell cytoplasm, does not enter nucleus, and does not interact with or integrate into recipient DNA.
  • May require low temperature storage.
Vector virus vaccines (both replication incompetent and competent)
  • Uses a different virus (not SARS-CoV-2) as a vector or carrier that expresses the viral protein that is the intended target.
   
  • Pre-existing immunity to the vector can attenuate vaccine immunogenicity (thus, viral vectors that are uncommon in humans, animal virus vectors, or vectors that do not induce self-immunity are preferred).
  • Replication-incompetent vector vaccines
  • Viral vector has been engineered not to replicate.
  • Ad26.COV2.S (Janssen/Johnson & Johnson)
  • ChAdOx1 nCoV-19/AZD1222 (AstraZeneca)
  • Gam-COVID-Vac Sputnik V (Gamaleya Institute)
  • Ad5-nCoV (CanSino)
  • Ad26.ZEBOV/MVA-BN-Filo (an Ebola virus vaccine)
  • Failure of the vector to reproduce could theoretically reduce potential adverse events that could occur with replicating vectors.
  • Example vectors include adenovirus, modified vaccinia Ankara (MVA), human parainfluenza virus, influenza virus, adeno-associated virus (AAV), and Sendai virus.
  • Replication-competent vector vaccines
  • Viral vector is derived from attenuated or vaccine strains of viruses.
  • DelNS1-2019-nCoV-RBD-OPT1, an intranasal flu-based RBD vaccine (University of Hong Kong) – in trials
  • rVSV-ZEBOV (an Ebola virus vaccine)
  • Often result in more robust immune response compared with replication-incompetent vectors (stimulate innate immune response).
  • Can be administered intranasally and thus might induce mucosal immune response at the site of viral entry.
  • Example vectors include measles vaccine strains, influenza virus, vesicular stomatitis virus (VSV), and Newcastle disease virus (NDV).
Recombinant protein vaccines
  • Composed of purified viral proteins that have been expressed in one of various systems (eg, insect and mammalian cells, yeast cells, plants).
  • NVX-CoV2373 (Novavax)
  • Human papillomavirus vaccines
  • Hepatitis B vaccines
  • Stimulates immunity to the purified viral protein.
DNA vaccines
  • Consist of plasmid DNA that contain mammalian expression promotors and the target gene, so that the target protein is expressed in the recipient.
  • ZyCoV-D (Zydus Cadila)
 
  • Are often of low immunogenicity.
  • Need special delivery devices (eg, electroporators).
* This is not an exhaustive list of example COVID-19 vaccines and vaccine candidates for each vaccine platform. The World Health Organization maintains an updated list of vaccines in development.
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