PLK1, A Potential Target for Cancer Therapy

Liu, Zhixian; Sun, Qiangming; Wang, Xiaosheng

doi:10.1016/j.tranon.2016.10.003

Cited by 318 publications

(264 citation statements)

References 136 publications

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“…To more specifically test for the response to mitotic checkpoints, we inhibited AurBK or PLK1 by use of chemical inhibitors. These molecules are currently being tested as anticancer targets for their critical role in mitosis and involvement in the mitosis checkpoints . As shown in Figure and Supporting Information Figure S4, inhibition of these molecules induced a cell accumulation in mitosis and a great increase of cell size (phase contrast and light scattering), terminal differentiation (by means of involucrin expression) and polyploidy in cells from trachea, oral mucosa, and pharynx.…”

Section: Resultsmentioning

confidence: 99%

Response of head and neck epithelial cells to a DNA damage‐differentiation checkpoint involving polyploidization

et al. 2018

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Background Squamous epithelia of the head and neck undergo continuous cell renewal and are continuously exposed to mutagenic hazard, the main cause of cancer. How they maintain homeostasis upon cell cycle deregulation is unclear. Methods To elucidate how head and neck epithelia respond to cell cycle stress, we studied human keratinocytes from various locations (oral mucosa, tonsil, pharynx, larynx, and trachea). We made use of genotoxic or mitotic drugs (doxorubicin [DOXO], paclitaxel, and nocodazole), or chemical inhibitors of the mitotic checkpoint kinases, Aurora B and polo‐like‐1. We further tested the response to inactivation of p53, ectopic cyclin E, or to the chemical carcinogen 7,12‐dimethylbenz[a]anthracene (DMBA). Results All treatments provoked DNA damage or mitosis impairment and strikingly triggered squamous differentiation and polyploidization, resulting in irreversible loss of clonogenic capacity. Conclusion Keratinocytes from head and neck epithelia share a cell‐autonomous squamous DNA damage‐differentiation response that is common to the epidermis and might continuously protect them from cancer.

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Section: Resultsmentioning

confidence: 99%

Response of head and neck epithelial cells to a DNA damage‐differentiation checkpoint involving polyploidization

et al. 2018

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“…Group A was characterized by IGF1R, and ER‐alpha pathways' activation and PLK1 downregulation ( P < 5.0 × 10 −4 ). PLK1 (polo like kinase 1), a key regulator of mitosis, cooperates with ER‐dependent gene transcription, and its overexpression in cancer cells is associated with poor prognosis . PLK1 downregulation enriched in group A seems to be associated with good‐prognosis, high proportion of stromal cells and low chromosome instability ( P = 7.513 × 10 −5 , t test; FC = 2.88; Figure ) …”

Section: Resultsmentioning

confidence: 99%

Integrative molecular profiling identifies a novel cluster of estrogen receptor‐positive breast cancer in very young women

et al. 2019

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Very young breast cancer patients are more common in Asian countries than Western countries and are thought to have worse prognosis than older patients. The aim of the current study was to identify molecular characteristics of young patients with estrogen receptor ( ER )‐positive breast cancer by analyzing mutations and copy number variants ( CNV ), and by applying expression profiling. The whole exome and transcriptome of 47 Korean young breast cancer ( KYBR ) patients (age <35) were analyzed. Genomic profiles were constructed using mutations, CNV and differential gene expression from sequencing data. Pathway analyses were also performed using gene sets to identify biological processes. Our data were compared with young ER + breast cancer patients in The Cancer Genome Atlas ( TCGA ) dataset. TP 53 , PIK 3 CA and GATA 3 were highly recurrent somatic mutation genes. APOBEC ‐associated mutation signature was more frequent in KYBR compared with young TCGA patients. Integrative profiling was used to classify our patients into 3 subgroups based on molecular characteristics. Group A showed luminal A‐like subtype and IGF 1R signal dysregulation. Luminal B patients were classified into groups B and C, which showed chromosomal instability and enrichment for APOBEC 3A/B deletions, respectively. Group B was characterized by 11q13 ( CCND 1) amplification and activation of the ubiquitin‐mediated proteolysis pathway. Group C showed 17q12 ( ERBB 2) amplification and lower ER and progesterone receptor expression. Group C was also distinguished by immune activation and lower epithelial‐mesenchyme transition ( EMT ) degree compared with group B. This study showed that integrative genomic profiling could classify very young patients with breast cancer into molecular subgroups that are potentially linked to different clinical characteristics.

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“…Non‐microtubule components of mitosis, including polo‐like kinase 1 (PLK1), are required for complete cell division and have emerged as promising targets for cancer therapy. Human PLK1 is highly expressed in malignant lymphomas and acute myeloid leukaemia (AML), and elevated PLK1 is associated with poor prognosis in several cancer types (Liu et al , ).…”

Section: Dlts In Cycle 1 and Determination Of Maximum Tolerated Dosementioning

confidence: 99%

Phase I dose‐escalation trial investigating volasertib as monotherapy or in combination with cytarabine in patients with relapsed/refractory acute myeloid leukaemia

et al. 2018

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PLK1, A Potential Target for Cancer Therapy

Cited by 318 publications

References 136 publications

Response of head and neck epithelial cells to a DNA damage‐differentiation checkpoint involving polyploidization

Response of head and neck epithelial cells to a DNA damage‐differentiation checkpoint involving polyploidization

Integrative molecular profiling identifies a novel cluster of estrogen receptor‐positive breast cancer in very young women

Phase I dose‐escalation trial investigating volasertib as monotherapy or in combination with cytarabine in patients with relapsed/refractory acute myeloid leukaemia

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