HIV-1-Tat Protein Inhibits SC35-mediated Tau Exon 10 Inclusion through Up-regulation of DYRK1A Kinase

Authors

Ferdous Kadri, From the Department of Medicine, Stanley S. Scott Cancer Center, and Department of Microbiology, Immunology and Parasitology, Louisiana State University Health Sciences Center, New Orleans, Louisiana 70112 and.
Marco Pacifici, From the Department of Medicine, Stanley S. Scott Cancer Center, and.
Anna Wilk, From the Department of Medicine, Stanley S. Scott Cancer Center, and.
Amanda Parker-Struckhoff, From the Department of Medicine, Stanley S. Scott Cancer Center, and.
Luis Del Valle, From the Department of Medicine, Stanley S. Scott Cancer Center, and.
Kurt F. Hauser, the Departments of Pharmacology and Toxicology and.
Pamela E. Knapp, Anatomy and Neurobiology, Virginia Commonwealth University, Richmond, Virginia 23284.
Christopher Parsons, From the Department of Medicine, Stanley S. Scott Cancer Center, and.
Duane Jeansonne, From the Department of Medicine, Stanley S. Scott Cancer Center, and.
Adam Lassak, From the Department of Medicine, Stanley S. Scott Cancer Center, and.
Francesca Peruzzi, From the Department of Medicine, Stanley S. Scott Cancer Center, and fperuz@lsuhsc.edu.

Document Type

Article

Publication Date

12-25-2015

Abstract

The HIV-1 transactivator protein Tat is implicated in the neuronal damage that contributes to neurocognitive impairment affecting people living with HIV/AIDS. Aberrant splicing of TAU exon 10 results in tauopathies characterized by alterations in the proportion of TAU isoforms containing three (3R) or four (4R) microtubule-binding repeats. The splicing factor SC35/SRSF2 binds to nuclear RNA and facilitates the incorporation of exon 10 in the TAU molecule. Here, we utilized clinical samples, an animal model, and neuronal cell cultures and found that Tat promotes TAU 3R up-regulation through increased levels of phosphorylated SC35, which is retained in nuclear speckles. This mechanism involved Tat-mediated increased expression of DYRK1A and was prevented by DYRK1A silencing. In addition, we found that Tat associates with TAU RNA, further demonstrating that Tat interferes with host RNA metabolism in the absence of viral infection. Altogether, our data unravel a novel mechanism of Tat-mediated neuronal toxicity through dysregulation of the SC35-dependent alternative splicing of TAU exon 10. Furthermore, the increased immunostaining of DYRK1A in HIV+ brains without pathology points at dysregulation of DYRK1A as an early event in the neuronal complications of HIV infection.

Publication Source (Journal or Book title)

The Journal of biological chemistry

First Page

30931

Last Page

46

Recommended Citation

Kadri, F., Pacifici, M., Wilk, A., Parker-Struckhoff, A., Del Valle, L., Hauser, K. F., Knapp, P. E., Parsons, C., Jeansonne, D., Lassak, A., & Peruzzi, F. (2015). HIV-1-Tat Protein Inhibits SC35-mediated Tau Exon 10 Inclusion through Up-regulation of DYRK1A Kinase. The Journal of biological chemistry, 290 (52), 30931-46. https://doi.org/10.1074/jbc.M115.675751