Abstract

A retrovirus HTLV-3 has recently been implicated in the etiology of the Acquired Immunodeficiency Syndrome. This virus is tropic for the T4 subset of lymphocytes, but only in their activated form, and it is cytotoxic for them. Sustained infection of normal peripheral blood lymphocytes by the virus in vitro is, therefore, difficult to achieve. It is the purpose of this research project to test whether sustained infection by HTLV-3 in vivo, and progression from asymptomatic infection to the AIDS related complex or to fully established AIDS, generally requires help, i.e., a cofactor in the form of the presence of a population of B cells infected by the Epstein-Barr virus (EBV). The hypothesis is that with loss of T4 cells by HTLV-3 infection, a temporary immunodeficient state may ensue characterized not only by loss of the population of T cells susceptible to HTLV, but also by unrestrained growth of EBC infected B lymphocytes. The infected B cells would then provide a needed secondary cell population for proliferation of the HTLV-3 virus, as has been described by Montagnier, and also an effective number of EBC-infected B cells for creating newly activated, and thus newly susceptible, T4 cells. Our hypothesis will be tested by 1) evaluating immunocompetence by lymphokine and cytotoxic cell production after EBV infection in vitro; 2) measuring the quantity of the EBV-infected B lymphocytes from the circulation or in biopsy to tissues; 3) searching for dual infection by EBV and HTLV-3 in cloned lymphoblastoid cell lines from the patients; 4) determining whether these conditions occur in reciprocal relation to each other and whether this occurs at times of asymptomatic infection by HTLV-3 or at later prodromal stages of the disease; and 5) assessing in a long term prospectus follow-up whether these measurements predict progression towards end stage disease. These studies will be carried out in a carefully documented university hospital patient population. The specific documentation of these immunologic abnormalities in relation to disease progression will have important implications in developing optimal therapeutic modalities.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
1R01AI022651-01
Application #
3134043
Study Section
Immunobiology Study Section (IMB)
Project Start
1985-09-01
Project End
1988-08-31
Budget Start
1985-09-01
Budget End
1986-08-31
Support Year
1
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
San Diego
State
CA
Country
United States
Zip Code
92037

  Publications

Sesterhenn, Thomas M; Slaven, Bradley E; Smulian, A George et al. (2003) Generation of sequencing libraries for the Pneumocystis Genome project. J Eukaryot Microbiol 50 Suppl:663-5
Bentin, J; Tsoukas, C D; McCutchan, J A et al. (1989) Impairment in T-lymphocyte responses during early infection with the human immunodeficiency virus. J Clin Immunol 9:159-68
Sureau, C; Taylor, J; Chao, M et al. (1989) Cloned hepatitis delta virus cDNA is infectious in the chimpanzee. J Virol 63:4292-7
Kuo, M Y; Chao, M; Taylor, J (1989) Initiation of replication of the human hepatitis delta virus genome from cloned DNA: role of delta antigen. J Virol 63:1945-50
Bentin, J; Vaughan, J H; Tsoukas, C D (1988) T cell proliferation induced by anti-CD3 antibodies: requirement for a T-T cell interaction. Eur J Immunol 18:627-32