1998
DOI: 10.1128/mcb.18.6.3620
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Human T-Cell Leukemia Virus Type 1 Tax and Cell Cycle Progression: Role of Cyclin D-cdk and p110Rb

Abstract: Human T-cell leukemia virus type 1 is etiologically linked to the development of adult T-cell leukemia and various human neuropathies. The Tax protein of human T-cell leukemia virus type I has been implicated in cellular transformation. Like other oncoproteins, such as Myc, Jun, and Fos, Tax is a transcriptional activator. How it mechanistically dysregulates the cell cycle is unclear. Previously, it was suggested that Tax affects cell-phase transition by forming a direct protein-protein complex with p16INK4a ,… Show more

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Cited by 182 publications
(156 citation statements)
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“…Under our in vitro assay conditions, p34 SEI-1 acts as both an activator and inhibitor of CDK4, which distinguishes p34 SEI-1 from other CDK4-binding proteins. INK4 (5)(6)(7)(8)(9)(10)(11) and KIP proteins (12)(13)(14) only inhibit CDK4; gankyrin functions as a competitor to antagonize INK4 proteins (17), while Tax is competent in activating CDK4 (15,16), quenching p16 (32,33), and affecting cyclin Ds (34). It is important to point out that most of these studies were performed by in vitro or cell-based studies, and their biological relevance remains to be established.…”
Section: Dissecting the Structural Elements For The Different Functiomentioning
confidence: 99%
“…Under our in vitro assay conditions, p34 SEI-1 acts as both an activator and inhibitor of CDK4, which distinguishes p34 SEI-1 from other CDK4-binding proteins. INK4 (5)(6)(7)(8)(9)(10)(11) and KIP proteins (12)(13)(14) only inhibit CDK4; gankyrin functions as a competitor to antagonize INK4 proteins (17), while Tax is competent in activating CDK4 (15,16), quenching p16 (32,33), and affecting cyclin Ds (34). It is important to point out that most of these studies were performed by in vitro or cell-based studies, and their biological relevance remains to be established.…”
Section: Dissecting the Structural Elements For The Different Functiomentioning
confidence: 99%
“…In HTLV-I-infected cells, Tax inhibits cellular proteins that regulate cell cycle checkpoints, such as p16 ink4A , p21 waf1/cip1 , p53, and MAD-1 (Suzuki et al, 1996;Cereseto et al, 1996;Akagi et al, 1997;PiseMasison et al, 1998;Mulloy et al, 1998;Jin et al, 1998). Furthermore, Tax induces cyclin D2 upregulation and the consequent hyper-phosphorylation of the retinoblastoma (Rb) protein and constitutive cyclin E-CDK2 activity (Neuveut et al, 1998;Cereseto et al, 1999). Thus, it is tempting to speculate that, in HTLV-I-infected T-cells, Tax may override the physiological role of c-Myb in cell cycle progression.…”
Section: C-myb Promoter Transrepression By Tax Is Independent Of Its mentioning
confidence: 99%
“…Indeed, Tax protein induces the expression of numerous genes involved in the differentiation and the proliferation of T cells. 59,60 Through the functional inactivation of P16 INKA4 , 61 and the activation of cyclin D2 62 and cyclin D3, 63 Tax intervenes directly in the pathway controlling T cell proliferation. Furthermore, the N terminus of Tax has recently been found to directly and specifically interact with CDK4, resulting in a Tax/CDK holoenzyme complex that capably phosphorylates the Rb protein.…”
Section: Tax Triggers T Cell Proliferation and Genetic Instabilitymentioning
confidence: 99%