Abstract

We have been studying means of active immunization against the human cytomegalovirus (CMV). A live attenuated vaccine, called Towne, was developed in this laboratory. Vaccination studies have been carried out in normal subjects and in renal transplant patients showing that Towne is well-tolerated, does not induce latency, and provides protection approximately equal to that of natural immunity. One objective is to find a means to prevent intrauterine CMV infection. We now propose to study vaccine efficacy in a population of normal women at high risk of infection, in order to determine whether vaccine can prevent infection by natural contact with CMV infected secretions. Since children in day care centers are frequently infected with CMV, their mothers and day care personnel are at risk of inopportune infection. We will give vaccine or placebo to seronegative female day care center personnel who are practicing contraception, comparing the two groups for CMV infection rates. We will subsequently vaccinate seronegative mothers who are on contraception, in order to compare them with placebo vaccinated mothers with respect to infection by CMV as a result of exposure to their day care center children. Infection will be determined by virus isolation from urine and the appearance of IgM antibodies. In order to develop new improved vaccines, we will study isolated CMV proteins. We have previously found that viral envelope can elicit neutralizing antibodies and CMV-specific lymphocyte proliferation in guinea pigs and in humans. gA, a particular glycoprotein complex contained in the envelope, can elicit the same responses in guinea pigs. Purified native gA will be used for immunization of humans, with determination of both humoral and cellular responses by a variety of methods. Immune responses to whole virus, early antigens and late antigens will be studied by radioimmunoprecipitation, immunoblot and lymphocyte proliferation in individual recipients of live vaccine, wild virus, and subunit vaccine to determine whether response to specific proteins correlate with neutralizing antibodies and with protection against infection or disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD018957-10
Application #
3316100
Study Section
Experimental Virology Study Section (EVR)
Project Start
1978-05-01
Project End
1991-11-30
Budget Start
1987-12-01
Budget End
1988-11-30
Support Year
10
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Children's Hospital of Philadelphia
Department
Type
DUNS #
073757627
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Berencsi, K; Gonczol, E; Endresz, V et al. (1996) The N-terminal 303 amino acids of the human cytomegalovirus envelope glycoprotein B (UL55) and the exon 4 region of the major immediate early protein 1 (UL123) induce a cytotoxic T-cell response. Vaccine 14:369-74
Berencsi, K; Uri, A; Valyi-Nagy, T et al. (1994) Early region 3-replacement adenovirus recombinants are less pathogenic in cotton rats and mice than early region 3-deleted viruses. Lab Invest 71:350-8
Berencsi, K; Rando, R F; deTaisne, C et al. (1993) Murine cytotoxic T cell response specific for human cytomegalovirus glycoprotein B (gB) induced by adenovirus and vaccinia virus recombinants expressing gB. J Gen Virol 74 ( Pt 11):2507-12
Starr, S E (1992) Cytomegalovirus vaccines: current status. Infect Agents Dis 1:146-8
Plotkin, S A (1991) Cytomegalovirus vaccine development--past and present. Transplant Proc 23:85-9
Gonczol, E; deTaisne, C; Hirka, G et al. (1991) High expression of human cytomegalovirus (HCMV)-gB protein in cells infected with a vaccinia-gB recombinant: the importance of the gB protein in HCMV immunity. Vaccine 9:631-7
Plotkin, S A; Starr, S E; Friedman, H M et al. (1990) Vaccines for the prevention of human cytomegalovirus infection. Rev Infect Dis 12 Suppl 7:S827-38
Gonczol, E; Ianacone, J; Ho, W Z et al. (1990) Isolated gA/gB glycoprotein complex of human cytomegalovirus envelope induces humoral and cellular immune-responses in human volunteers. Vaccine 8:130-6
Marshall, G S; Ricciardi, R P; Rando, R F et al. (1990) An adenovirus recombinant that expresses the human cytomegalovirus major envelope glycoprotein and induces neutralizing antibodies. J Infect Dis 162:1177-81
Gonczol, E; Plotkin, S (1990) Progress in vaccine development for prevention of human cytomegalovirus infection. Curr Top Microbiol Immunol 154:255-74

Showing the most recent 10 out of 23 publications