Immunology of Human Immunodeficiency Virus Infection and the Acquired Immunodeficiency Syndrome
An Update
- MAXIME SELIGMANN, M.D.;
- ANTHONY J. PINCHING, M.D.;
- FRED S. ROSEN, M.D.;
- JOHN L. FAHEY, M.D.;
- RAKHIM M. KHAITOV, M.D.;
- DAVID KLATZMANN, M.D.;
- SCOTT KOENIG, M.D.;
- NKANDU LUO, M.D.;
- JACOB NGU, M.D.;
- GERT RIETHMÜLLER, M.D.; and
- THOMAS J. SPIRA, M.D.
Abstract
Recent advances in the understanding of the pathogenesis of infection with human immunodeficiency virus (HIV) stems from the demonstration that the membrane glycoprotein, CD4, is the cellular receptor for HIV. This glycoprotein is found mainly on the surface of a major subpopulation of T lymphocytes and also on macrophages, natural killer cells, some B lymphocytes, and neuronal cells. Cells infected with HIV may be destroyed or have their normal function impaired. Host immune responses to HIV are poor and are not sustained. Neutralizing antibody often is not produced, or HIV may escape from normal immunosuppressive mechanisms through the process of rapid antigenic variation. Factors and markers that may be important in the outcome or that may predict progression of HIV infection are genetic (Gc type), environmental (nutritional status or intercurrent sexually transmitted diseases sustained by the host), and immunologic (rate of decline in number and impairment of function of CD4 + lymphocytes and of decline in antibody titers to HIV core protein, p24). A recombinant vaccine will probably be developed for testing in future clinical trials.
- AIDS-related complex
- acquired immunodeficiency syndrome
- Africa
- antiviral agents
- blood transfusion
- cyclosporins
- HTLV-III
- immunity
- cellular
- lymphatic diseases
- neurologic manifestations
- opportunistic infections
- sarcoma
- Kaposi's
- sexually transmitted diseases
- T lymphocytes
- viral vaccines
- virus replication
- B-cell lymphomas
- human immunodeficiency virus
- maternofetal transmission
- target cells
- AIDS-related complex
- acquired immunodeficiency syndrome
- Africa
- antiviral agents
- blood transfusion
- cyclosporins
- HTLV-III
- immunity
- cellular
- lymphatic diseases
- neurologic manifestations
- opportunistic infections
- sarcoma
- Kaposi's
- sexually transmitted diseases
- T lymphocytes
- viral vaccines
- virus replication
- B-cell lymphomas
- human immunodeficiency virus
- maternofetal transmission
- target cells
Article and Author Information
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▸From the Working Group on Immunology of AIDS, World Health Organization and Clinical Immunology Committee of the International Union of Immunologic Societies; Geneva, Switzerland.
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▸Requests for reprints should be addressed to Maxime Seligmann, M.D.; Hôpital Saint-Louis; 75475 PARIS cedex 10, France.
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