Retrovirology (Feb 2005)

HIV-1 Tat protein enhances Microtubule polymerization

  • Prevot Charles,
  • Watkins Jennifer D,
  • Esquieu Didier,
  • Opi Sandrine,
  • Lancelot Sophie,
  • Campbell Grant R,
  • Barbier Pascale,
  • Carre Manon,
  • de Mareuil Jean,
  • Braguer Diane,
  • Peyrot Vincent,
  • Loret Erwann P

DOI
https://doi.org/10.1186/1742-4690-2-5
Journal volume & issue
Vol. 2, no. 1
p. 5

Abstract

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Abstract Background HIV infection and progression to AIDS is characterized by the depletion of T cells, which could be due, in part, to apoptosis mediated by the extra-cellular HIV-encoded Tat protein as a consequence of Tat binding to tubulin. Microtubules are tubulin polymers that are essential for cell structure and division. Molecules that target microtubules induce apoptosis and are potent anti-cancer drugs. We studied the effect on tubulin polymerization of three Tat variants: Tat HxB2 and Tat Eli from patients who are rapid progressors (RP) and Tat Oyi from highly exposed but persistently seronegative (HEPS) patients. We compared the effect on tubulin polymerization of these Tat variants and peptides corresponding to different parts of the Tat sequence, with paclitaxel, an anti-cancer drug that targets microtubules. Results We show that Tat, and specifically, residues 38–72, directly enhance tubulin polymerization. We demonstrate that Tat could also directly trigger the mitochondrial pathway to induce T cell apoptosis, as shown in vitro by the release of cytochrome c from isolated mitochondria. Conclusions These results show that Tat directly acts on microtubule polymerization and provide insights into the mechanism of T cell apoptosis mediated by extra-cellular Tat.