Research output: Contribution to journal › Review article › peer-review
Genes that control vaccinia virus immunogenicity. / Shchelkunov, S. N.; Shchelkunova, G. A.
In: Acta Naturae, Vol. 12, No. 1, 01.01.2020, p. 33-41.Research output: Contribution to journal › Review article › peer-review
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TY - JOUR
T1 - Genes that control vaccinia virus immunogenicity
AU - Shchelkunov, S. N.
AU - Shchelkunova, G. A.
N1 - Щелкунов С.Н., Щелкунова Г.А. Гены, влияющие на иммуногенность вируса осповакцины // Acta Naturae. - 2020. - Т. 12. - № 1. - C. 33-41
PY - 2020/1/1
Y1 - 2020/1/1
N2 - The live smallpox vaccine was a historical first and highly effective vaccine. However, along with high immunogenicity, the vaccinia virus (VACV) caused serious side effects in vaccinees, sometimes with lethal outcomes. Therefore, after global eradication of smallpox, VACV vaccination was stopped. For this reason, most of the human population worldwide lacks specific immunity against not only smallpox, but also other zoonotic orthopoxviruses. Outbreaks of diseases caused by these viruses have increasingly occurred in humans on different continents. However, use of the classical live VACV vaccine for prevention against these diseases is unacceptable because of potential serious side effects, especially in individuals with suppressed immunity or immunodeficiency (e.g., HIV-infected patients). Therefore, highly attenuated VACV variants that preserve their immunogenicity are needed. This review discusses current ideas about the development of a humoral and cellular immune response to orthopoxvirus infection/vaccination and describes genetic engineering approaches that could be utilized to generate safe and highly immunogenic live VACV vaccines.
AB - The live smallpox vaccine was a historical first and highly effective vaccine. However, along with high immunogenicity, the vaccinia virus (VACV) caused serious side effects in vaccinees, sometimes with lethal outcomes. Therefore, after global eradication of smallpox, VACV vaccination was stopped. For this reason, most of the human population worldwide lacks specific immunity against not only smallpox, but also other zoonotic orthopoxviruses. Outbreaks of diseases caused by these viruses have increasingly occurred in humans on different continents. However, use of the classical live VACV vaccine for prevention against these diseases is unacceptable because of potential serious side effects, especially in individuals with suppressed immunity or immunodeficiency (e.g., HIV-infected patients). Therefore, highly attenuated VACV variants that preserve their immunogenicity are needed. This review discusses current ideas about the development of a humoral and cellular immune response to orthopoxvirus infection/vaccination and describes genetic engineering approaches that could be utilized to generate safe and highly immunogenic live VACV vaccines.
KW - Immune modulating proteins
KW - Immunogenicity
KW - Protectiveness
KW - Smallpox
KW - Vaccination
KW - IMMUNE-RESPONSE
KW - immune modulating proteins
KW - PROTECTION
KW - smallpox
KW - VIRULENCE
KW - immunogenicity
KW - protectiveness
KW - DELETION
KW - ATTENUATION
KW - COWPOX
KW - SMALLPOX VACCINE
KW - POXVIRUS INFECTION
KW - ANTIBODY-RESPONSES
KW - HORSEPOX
KW - vaccination
UR - http://www.scopus.com/inward/record.url?scp=85086405929&partnerID=8YFLogxK
U2 - 10.32607/actanaturae.10935
DO - 10.32607/actanaturae.10935
M3 - Review article
C2 - 32477596
AN - SCOPUS:85086405929
VL - 12
SP - 33
EP - 41
JO - Acta Naturae
JF - Acta Naturae
SN - 2075-8251
IS - 1
ER -
ID: 24515711