Exogenous Interleukin-2 Administration Corrects the Cell Cycle Perturbation of Lymphocytes from Human Immunodeficiency Virus-Infected Individuals

Author:

Paiardini Mirko12,Galati Domenico3,Cervasi Barbara12,Cannavo Giuseppe3,Galluzzi Luca2,Montroni Maria4,Guetard Denise5,Magnani Mauro2,Piedimonte Giuseppe3,Silvestri Guido1

Affiliation:

1. Vaccine Research Center and Division of Infectious Diseases, Department of Medicine, Emory University, Atlanta, Georgia1;

2. Istituto di Chimica Biologica “G. Fornaini,” Universitá di Urbino, Urbino,2

3. Dipartimento di Patologia Generale, Malattie Infettive ed Ispezione degli Alimenti, Facoltádi Medicina Veterinaria, and Dipartimento di Igiene, Medicia Preventiva e Sanitá Pubblica, Facoltá di Medicina e Chirurgia, Universitá degli Studi di Messina, Messina,3 and

4. Servizio di Immunologia Clinica, Facoltá di Medicina e Chirurgia, Universitá di Ancona, Ancona,4 Italy; and

5. Unite de Oncologie Virale and Département SIDA et Retrovirus, Institut Pasteur, Paris, France5

Abstract

ABSTRACT Human immunodeficiency virus (HIV)-induced immunodeficiency is characterized by progressive loss of CD4 + T cells associated with functional abnormalities of the surviving lymphocytes. Increased susceptibility to apoptosis and loss of proper cell cycle control can be observed in lymphocytes from HIV-infected individuals and may contribute to the lymphocyte dysfunction of AIDS patients. To better understand the relation between T-cell activation, apoptosis, and cell cycle perturbation, we studied the effect of exogenous interleukin-2 (IL-2) administration on the intracellular turnover of phase-dependent proteins. Circulating T cells from HIV-infected patients display a marked discrepancy between a metabolic profile typical of G 0 and a pattern of expression of phase-dependent proteins that indicates a more-advanced position within the cell cycle. This discrepancy is enhanced by in vitro activation with ConA and ultimately results in a marked increase of apoptotic events. Conversely, treatment of lymphocytes with IL-2 alone restores the phase-specific pattern of expression of cell cycle-dependent proteins and is associated with low levels of apoptosis. Interestingly, exogenous IL-2 administration normalizes the overall intracellular protein turnover, as measured by protein synthesis, half-life of newly synthesised proteins, and total protein ubiquitination, thus providing a possible explanation for the effect of IL-2 on the intracellular kinetics of cell cycle-dependent proteins. The beneficial effect of IL-2 administration is consistent with the possibility of defective IL-2 function in vivo, which is confirmed by the observation that lymphocytes from HIV-infected patients show abnormal endogenous IL-2 paracrine/autocrine function upon in vitro mitogen stimulation. Overall these results confirm that perturbation of cell cycle control contributes to HIV-related lymphocyte dysfunction and, by showing that IL-2 administration can revert this perturbation, suggest a new mechanism of action of IL-2 therapy in HIV-infected patients.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

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