Besides their role in hemostasis, platelets are involved in inflammatory and immunological processes, and we hypothezise that platelet activation may play an immunopathogenetic role in HIV-1 infection. Blood was drawn from 15 controls and 20 HIV-1-infected patients with normal platelet counts, classified into groups of non-AIDS and AIDS. Platelet activation was detected using flow cytometry with mAbs against the release markers P-selectin and CD63, mAb against GPIb, and the probe annexin V detecting surface exposure of aminophospholipids. The amount of microvesicles was measured using mAb against GPIIIa. Compared to controls, blood samples from HIV-l-infected patients showed significantly enhanced levels of microvesicles and activated platelets as detected by their exposure of P-selectin, CD63, and aminophospholipids, as well as reduction in GPIb expression. Increased expression of P-selectin and amounts of microvesicles were most pronounced in advanced clinical and immunological disease. When studying the effect of HIV- 1 protease inhibitor therapy (indinavir) on platelet activation, we found that concomitant with a profound decrease in plasma vital load, there was a near normalization of several of the parameters reflecting enhanced plato let activation. Finally, we demonstrated that platelets may be an important source of the chemokine RANTES in HIV-l-infected patients. Although both unstimulated and SFLLRN-stimulated platelets from asymptomatic patients had enhanced release of RANTES, platelets from AIDS patients were characterized by markedly enhanced spontaneous, but decreased SFLLRN-stimulated release of this chemokine. Taken together, these results, which demonstrate for the first time increased platelet activation in HIV-1-infected patients with normal platelet counts, may represent a previously unrecognized immunopathogenic factor in HIV-1 infection.
CITATION STYLE
Holme, P. A., Müller, F., Solum, N. O., Brosstad, F., Frøland, S. S., & Aukrust, P. (1998). Enhanced activation of platelets with abnormal release of RANTES in human immunodeficiency virus type 1 infection. The FASEB Journal, 12(1), 79–89. https://doi.org/10.1096/fsb2fasebj.12.1.79
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