Cdk5 Regulates STAT3 Activation and Cell Proliferation in Medullary Thyroid Carcinoma Cells

H, Lin; Chen, Mei Chih; Chiu, Chih Yuan; Song, Yuh Min; Lin, Shih Yi

doi:10.1074/jbc.m607234200

Cited by 104 publications

(102 citation statements)

References 42 publications

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“…33 CDK5 was also previously shown to enhance tumor cell proliferation and invasion. [28][29][30]34 CDK5's targets include several important proteins for cell growth and death, such as STAT3, AKT, BCL-2, p53, and RB. 29,[34][35][36][37] By testing multiple CDK5 siRNAs and shRNAs, we confirmed that CDK5 knockdown sensitizes genetically variable myeloma cell lines to bortezomib and other proteasome inhibitors.…”

Section: Discussionmentioning

confidence: 99%

“…[28][29][30]34 CDK5's targets include several important proteins for cell growth and death, such as STAT3, AKT, BCL-2, p53, and RB. 29,[34][35][36][37] By testing multiple CDK5 siRNAs and shRNAs, we confirmed that CDK5 knockdown sensitizes genetically variable myeloma cell lines to bortezomib and other proteasome inhibitors. This finding and its clinical relevance were further explored by the use of CDK5 inhibitors, roscovitine and SCH727965, which were demonstrated to synergize with bortezomib to induce cytotoxicity of both MM cell lines and primary MM samples.…”

Section: Discussionmentioning

confidence: 99%

“…25 Although activity of CDK5 is most evident in neuronal tissues, CDK5 is also active in some non-neuronal tissues 26,27 and survival and metastasis of several tumor cells, including breast, prostate, thyroid, and colon cancer cells. 11,[28][29][30] Upregulation of CDK5 was recently identified as one of genetic changes related to oxaliplatin resistance acquisition in colorectal cancer cells. 31 A recent RNAi screening study demonstrated that silencing CDK5 enhanced the sensitivity to a PARP inhibitor in a breast cancer cell line.…”

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RNAi screen of the druggable genome identifies modulators of proteasome inhibitor sensitivity in myeloma including CDK5

Zhu

Tiedemann

Shi

et al. 2011

Blood

101

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The molecular target(s) cooperating with proteasome inhibition in multiple myeloma (MM) remain unknown. We therefore measured proliferation in MM cells transfected with 13 984 small interfering RNAs in the absence or presence of increasing concentrations of bortezomib. We identified 37 genes, which when silenced, are not directly cytotoxic but do synergistically potentiate the growth inhibitory effects of bortezomib. To focus on bortezomib sensitizers, genes that also sensitized MM to melphalan were excluded. When suppressed, the strongest bortezomib sensitizers were the proteasome subunits PSMA5, PSMB2, PSMB3, and PSMB7 providing internal validation, but others included BAZ1B, CDK5, CDC42SE2, MDM4, NME7, RAB8B, TFE3, TNFAIP3, TNK1, TOP1, VAMP2, and YY1. The strongest hit CDK5 also featured prominently in pathway analysis of primary screen data. Cyclin IntroductionBortezomib is a potent and selective proteasome inhibitor used in the treatment of multiple myeloma (MM) and low-grade lymphoma patients. Bortezomib produces significant clinical responses in both newly diagnosed and advanced MM, but only 40% of patients respond to the single agent, 1,2 and the majority of these patients become resistant over time. The mechanism of antimyeloma activity of bortezomib is therefore a subject of intense study with inhibition of the proteasome, autophagy, and activation of the unfolded protein stress response pathway apparently critical. A downstream consequence of proteasome inhibition relevant to MM is blockade of nuclear factor B (NF-B) activity, which may partly mediate bortezomib activity in MM because activating mutations in the NF-B pathway were identified in at least 17% of MM patients and 41% of human myeloma cell lines and appear to mediate accelerated growth and survival of malignant plasma cells. [3][4][5] However, the 35% to 50% response rate to bortezomib cannot be totally interpreted by NF-B abnormality, suggesting that other specific molecular targets, resistance mechanisms, or perhaps unique pharmacokinetics are inherent in patients. Furthermore, resistance to bortezomib therapy often develops even in initially sensitive patients; and although certain mechanisms such as mutations in proteasome subunits have been postulated, 6 the underlying mechanism defining this nonresponsiveness is largely unknown. Understanding the cooperating mechanisms of sensitivity to proteasome inhibition will not only allow more targeted use of proteasome inhibitors but should also make it possible to rationally design synergistic drug combinations and predict patient response to therapy.To begin to address these issues, a druggable genome RNAi screen was used to identify modifiers of bortezomib sensitivity in human MM cells. Through this high-throughput screen, we identified a panel of genes whose loss of expression enhances bortezomib sensitivity (sensitizer). Using shRNA expression systems and a small-molecule inhibitor, we have further validated one of the most potent bortezomib sensitizer genes as cyclin-dependent kinase 5 (...

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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RNAi screen of the druggable genome identifies modulators of proteasome inhibitor sensitivity in myeloma including CDK5

Zhu

Tiedemann

Shi

et al. 2011

Blood

101

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“…Compared with other CDKs, CDK5 is considered to be an essential regulator of neuronal differentiation, rather than a cell cycle regulator; and controls a wide range of functions, including synapse formation, neuronal migration and axon guidance (7), all of which indicate that CDK5 is important as a 'migration mediator'. Notably, CDK5 had been found to be correlated with increased invasion in prostate carcinoma, glioblastoma multiforme (8,9), pancreatic cancer cells (10,11) and medullary thyroid cancer (12). The inhibition of the activity of CDK5 decreases cancer cell migration and invasion (13), however, the mechanism underlying the involvement of CDK5 in tumorigenesis remains to be fully elucidated.…”

Section: Introductionmentioning

confidence: 99%

Cyclin-dependent kinase 5 regulates the proliferation, motility and invasiveness of lung cancer cells through its effects on cytoskeletal remodeling

Zhou

et al. 2015

Molecular Medicine Reports

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Abstract. Determining the molecular phenotype is a key to understanding and predicting the metastatic potential and the prognosis for patients with lung cancer. Our previous study demonstrated that increased expression of cyclin-dependent kinase 5 (CDK5) in patients with non-small cell lung cancer (NSCLC) is associated with a poorer prognosis. The present study aimed to further investigate the underlying mechanism of CDK5 in vitro and in vivo using the A549 human NSCLC cell line. A 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assay was used to quantify the proliferation of the A549 cells; migration assay and invasiveness assays were performed using Transwell chambers and wound healing assays were used to assess cell motility, which was assessed by measuring the movement of cells. Inhibition of CDK5 by roscovitine and small interfering (si)RNA was used to investigate the mechanism of CDK5 in the process of A549 lung cancer cell proliferation, migration and invasion. The results demonstrated that functional inhibition of CDK5 using roscovitine and siRNA markedly suppressed the proliferation of A549 cells and resulted in a reduced tumor mass in vivo. In addition, the hinhibition of CDK5 reduced the migration and invasiveness of the A549 cells in vitro and in vivo. Notably, CDK5 inhibition also impaired tumor cell cytoskeletal remodeling and led to loss of cell polarity, which may partially explain the reduction of A549 cell mobility and invasiveness.The results of the present study revealed that CDK5 may be important in the regulation of migration and invasiveness in NSCLC through its effects on cytoskeletal remodeling. IntroductionLung cancer has long been the leading cause of cancer-associated mortality worldwide (1). Although numerous therapeutic strategies have improved significantly, the presence of locally advanced or metastatic lung cancer reduces the curability of this life-threatening disease. Several efforts have been made to understand the mechanism and molecular pathogenesis of this disease, with promise in the development of more effective targeted treatment strategies for lung cancer, particularly non-small cell lung cancer (NSCLC). Certain small molecular inhibitors have been developed against certain tyrosine kinases, including epidermal growth factor receptor and vascular endothelial growth factor receptor (2); however, the overall progression free survival rate has not improved satisfactorily (3). The poor survival rate is predominantly attributed to aggressive growth, advanced stage at diagnosis and local recurrence (4). The identification of effectors, which modulate growth, cell migration and invasion will assist in understanding the process of disease progression and enable the development of novel therapeutic targets for patients with NSCLC.Cyclin-dependent kinase 5 (CDK5) has been recognized as a key factor in regulating the migration and plasticity of neuron cells (5,6). Compared with other CDKs, CDK5 is considered to be an essential regulator of neuronal differentiation, ra...

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“…There is presently a substantial amount of data to indicate that CDK5 plays important roles in extraneuronal cells during the process of myogenesis, lens differentiation, spermatogenesis, insulin secretion, apoptosis of ovarian cells and hematopoietic cell differentiation. 3,[5][6][7][8][9][10][11] Furthermore, CDK5 has been suggested to play roles in the regulation of motility of prostate cancer cells, 12 control of glioblastoma cell invasion, 13 modulation of proliferation of medullary thyroid carcinoma cells 14 and apoptotic control of leukemia cells. 15 These potential roles of CDK5 activity in the carcinogenesis of each cell type seem to involve distinct target substrates.…”

Section: Introductionmentioning

confidence: 99%

Single-nucleotide polymorphisms in the promoter of the CDK5 gene and lung cancer risk in a Korean population

et al. 2009

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Cyclin-dependent kinase 5 (CDK5), a proline-directed serine/threonine kinase, which was originally known for its regulatory role in neuronal activities, has recently been suggested to play a role in extraneuronal activities. For example, a recent study detected overexpression of the CDK5 gene in non-small-cell lung cancer. Therefore, in order to explore the association of the CDK5 gene with lung cancer risk in a Korean population, the genotypes of the CDK5 promoter region were determined in 407 lung cancer patients and 402 normal participants. The result showed that the À904 G4A genotype affected susceptibility to lung cancer risk (odd ratios (OR)¼1.53, 95% confidence interval (CI)¼1.02-2.32). Furthermore, subsequent haplotype analysis of three single-nucleotide polymorphism (SNP) regions suggested that the A-G-C haplotype was associated with a higher overall risk of lung cancer (OR¼1.59, 95% CI¼1.16-2.18). These results suggest that CDK5 promoter polymorphisms contribute to the genetic susceptibility to lung cancer in the Korean population.

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Cdk5 Regulates STAT3 Activation and Cell Proliferation in Medullary Thyroid Carcinoma Cells

Cited by 104 publications

References 42 publications

RNAi screen of the druggable genome identifies modulators of proteasome inhibitor sensitivity in myeloma including CDK5

RNAi screen of the druggable genome identifies modulators of proteasome inhibitor sensitivity in myeloma including CDK5

Cyclin-dependent kinase 5 regulates the proliferation, motility and invasiveness of lung cancer cells through its effects on cytoskeletal remodeling

Single-nucleotide polymorphisms in the promoter of the CDK5 gene and lung cancer risk in a Korean population

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