155871-1017

pubmed-article:10639311, pubmed-article:12049628, pubmed-article:12114499, pubmed-article:15050687, pubmed-article:16289656, pubmed-article:17083724, pubmed-article:17631934, pubmed-article:17661632, pubmed-article:18455747, pubmed-article:19603446, pubmed-article:19732026, pubmed-article:20956357, pubmed-article:21651489, pubmed-article:7716549, pubmed-article:9223324, pubmed-article:9311822, pubmed-article:9525916

Amino acid residues serine 16 and 46 of HIV-1 Tat are phosphorylated by CDK2; mutation of these two residues reduces HIV-1 transcription in cells, Cdk2 activity is enhanced by HIV-1 Tat expression in Jurkat T cells and is associated with Tat-induced apoptosis, Cdk2 phosphorylates HIV-1 Tat, Cdk2/cyclin E stimulates Tat-dependent HIV-1 transcription, HIV-1 Tat 41/44 peptide TAALS from the core domain of Tat inhibits Tat-mediated HIV-1 gene expression and replication by binding the Cdk2/Cyclin E complex and inhibiting the phosphorylation of serine 5 of RNAPII, HIV-1 Tat induces Cdk2 to phosphorylate the RNA Polymerase C-terminal domain, HIV-1 Tat induces Cyclin E-associated cdk activity in lymphocytes, indicating Tat drives cells to the late G1 phase of the cell cycle, HIV-1 Tat induces a G1 arrest in cells of glial origin, leading to a downregulation of cyclin E-Cdk2 kinase activity and phosphorylation of Rb, Iron chelators 311 and ICL670 decrease cellular activity of CDK2 and reduce HIV-1 Tat phosphorylation by CDK2, Tat-mediated phosphorylation of RNA Polymerase C-terminal domain involves dynamic interactions of Cdk2 with Tat amino acids 15-24 and 36-49 and requires cysteine 22 in the activation domain of Tat and amino acids 42-72 of Tat, When expressed in astrocytes, neurons, and non-glial 293T cells, HIV-1 Tat interacts with a number of cell cycle-related proteins including cyclin A, cyclin B, cyclin D3, Cdk2, Cdk4, Cdk1/Cdc2, cdc6, p27, p53, p63, hdlg, and PCNA