Protective role for lipid modifications of Src-family kinases against chromosome missegregation

Honda, Takeshi; Soeda, Shuhei; Tsuda, Kunihiko; Yamaguchi, Chihiro; Aoyama, Kazumasa; Morinaga, Takao; Yuki, Ryuzaburo; Nakayama, Yuji; Yamaguchi, Noritaka; Yamaguchi, Naoto

doi:10.1038/srep38751

Cited by 23 publications

(26 citation statements)

References 58 publications

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“…Cells exhibit chromosome instability through abnormal chromosome segregation in the next cell cycle of tetraploid cells. v-Src-induced chromosome bridge formation also contributes to the chromosome instability (7,25,44). The chromosome instability generates genetic diversity, and cells capable of adapting to growth-suppressive conditions by anti-cancer drugs or cells gaining metastatic ability can be selected (7).…”

Section: V-src Induces Mitotic Slippage Through Cdk1 Phosphorylationmentioning

confidence: 99%

The tyrosine kinase v-Src causes mitotic slippage by phosphorylating an inhibitory tyrosine residue of Cdk1

Horiuchi

Kuga

Saito

et al. 2018

Journal of Biological Chemistry

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The nonreceptor tyrosine kinase v-Src is an oncogene first identified in Rous sarcoma virus. The oncogenic effects of v-Src have been intensively studied; however, its effects on chromosomal integrity are not fully understood. Here, using HeLa S3/v-Src cells having inducible v-Src expression, we found that v-Src causes mitotic slippage in addition to cytokinesis failure, even when the spindle assembly checkpoint is not satisfied because of the presence of microtubule-targeting agents. v-Src's effect on mitotic slippage was also observed in cells after a knockdown of C-terminal Src kinase (Csk), a protein-tyrosine kinase that inhibits Src-family kinases and was partially inhibited by PP2, an Src-family kinase inhibitor. Proteomic analysis and kinase assay revealed that v-Src phosphorylates cyclin-dependent kinase 1 (Cdk1) at Tyr-15. This phosphorylation attenuated Cdk1 kinase activity, resulting in a decrease in the phosphorylation of Cdk1 substrates. Furthermore, v-Src-induced mitotic slippage reduced the sensitivity of the cells to microtubule-targeting agents, and cells that survived the microtubule-targeting agents exhibited polyploidy. These results suggest that v-Src causes mitotic slippage by attenuating Cdk1 kinase activity via direct phosphorylation of Cdk1 at Tyr-15. On the basis of these findings, we propose a model for v-Src-induced oncogenesis, in which v-Src-promoted mitotic slippage due to Cdk1 phosphorylation generates genetic diversity via abnormal cell division of polyploid cells and also increases the tolerance of cancer cells to microtubule-targeting agents.

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Section: V-src Induces Mitotic Slippage Through Cdk1 Phosphorylationmentioning

confidence: 99%

The tyrosine kinase v-Src causes mitotic slippage by phosphorylating an inhibitory tyrosine residue of Cdk1

Horiuchi

Kuga

Saito

et al. 2018

Journal of Biological Chemistry

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“…To synchronize cells at the G 1 /S boundary, a double thymidine block was performed as described 20 , 38 , 39 . In brief, cells treated with 4 mM thymidine for 16 h were incubated in thymidine-free complete medium for 9 h, and the cells were further treated with 4 mM thymidine for 16 h.…”

Section: Methodsmentioning

confidence: 99%

“…Cell lysates were prepared in SDS-sample buffer were separated by SDS-PAGE and electrotransferred onto polyvinylidene difluoride membranes (PVDF, Millipore). Immunodetection was performed as reported previously 20 , 34 , 36 , 43 . Sequential reprobing of membranes with a variety of antibodies was performed after the complete removal of primary and secondary antibodies from membranes in stripping buffer or inactivation of horseradish peroxidase by 0.1% NaN 3 , according to the manufacturer’s instructions.…”

Section: Methodsmentioning

confidence: 99%

v-Src-driven transformation is due to chromosome abnormalities but not Src-mediated growth signaling

Honda

Morii

Nakayama

et al. 2018

Sci Rep

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v-Src is the first identified oncogene product and has a strong tyrosine kinase activity. Much of the literature indicates that v-Src expression induces anchorage-independent and infinite cell proliferation through continuous stimulation of growth signaling by v-Src activity. Although all of v-Src-expressing cells are supposed to form transformed colonies, low frequencies of v-Src-induced colony formation have been observed so far. Using cells that exhibit high expression efficiencies of inducible v-Src, we show that v-Src expression causes cell-cycle arrest through p21 up-regulation despite ERK activation. v-Src expression also induces chromosome abnormalities and unexpected suppression of v-Src expression, leading to p21 down-regulation and ERK inactivation. Importantly, among v-Src-suppressed cells, only a limited number of cells gain the ability to re-proliferate and form transformed colonies. Our findings provide the first evidence that v-Src-driven transformation is attributed to chromosome abnormalities, but not continuous stimulation of growth signaling, possibly through stochastic genetic alterations.

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“…The authors found that, upon palmitoylation, Rif1 reduced the silencing of chromatin by competing with Silent Information Regulator/Repressor Activator Protein 1 (SIR/RAP1) complex for telomeric DNA binding. Thereby, Rif1palmitoylation may influence telomere anchoring, nuclear organization, and heterochromatin silencing [91]. Collectively, experimental evidence indicates that protein palmitoylation can be modulated by metabolic signals and may represent a novel mechanism regulating chromatin structure and gene expression.…”

Section: Palmitoylation Of Chromatin Remodelers and Histone Proteinsmentioning

confidence: 99%

Nutrient-Dependent Changes of Protein Palmitoylation: Impact on Nuclear Enzymes and Regulation of Gene Expression

Spinelli

Fusco

Grassi

2018

IJMS

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Diet is the main environmental stimulus chronically impinging on the organism throughout the entire life. Nutrients impact cells via a plethora of mechanisms including the regulation of both protein post-translational modifications and gene expression. Palmitoylation is the most-studied protein lipidation, which consists of the attachment of a molecule of palmitic acid to residues of proteins. S-palmitoylation is a reversible cysteine modification finely regulated by palmitoyl-transferases and acyl-thioesterases that is involved in the regulation of protein trafficking and activity. Recently, several studies have demonstrated that diet-dependent molecules such as insulin and fatty acids may affect protein palmitoylation. Here, we examine the role of protein palmitoylation on the regulation of gene expression focusing on the impact of this modification on the activity of chromatin remodeler enzymes, transcription factors, and nuclear proteins. We also discuss how this physiological phenomenon may represent a pivotal mechanism underlying the impact of diet and nutrient-dependent signals on human diseases.

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Protective role for lipid modifications of Src-family kinases against chromosome missegregation

Cited by 23 publications

References 58 publications

The tyrosine kinase v-Src causes mitotic slippage by phosphorylating an inhibitory tyrosine residue of Cdk1

The tyrosine kinase v-Src causes mitotic slippage by phosphorylating an inhibitory tyrosine residue of Cdk1

v-Src-driven transformation is due to chromosome abnormalities but not Src-mediated growth signaling

Nutrient-Dependent Changes of Protein Palmitoylation: Impact on Nuclear Enzymes and Regulation of Gene Expression

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