Whether to target single or multiple CDKs for therapy? That is the question

Węsierska‐Gądek, Józefa; Maurer, Margarita; Zulehner, Nora; Komina, Oxana

doi:10.1002/jcp.22426

Cited by 50 publications

(32 citation statements)

References 121 publications

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“…In addition, selective inhibitors are in need for targeting tumors where a single kinase is aberrantly regulated. 88,89 Currently, a few ATP-competitive CDK4/6 dual inhibitors, i.e., Palbociclib (PD0332991), Ribociclib (LEE011) and Abemaciclib (LY2835219) are undergoing clinical trials. Mechanistically, these drug candidates inhibit CDK4/6, halt Rb phosphorylation and arrest G1 cell cycle progression of cancer cells.…”

Section: Structural Features and Regulationmentioning

confidence: 99%

Targeting CDK6 in cancer: State of the art and new insights

et al. 2015

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Cyclin-dependent kinase 6 (CDK6) plays a vital role in regulating the progression of the cell cycle. More recently, CDK6 has also been shown to have a transcriptional role in tumor angiogenesis. Up-regulated CDK6 activity is associated with the development of several types of cancers. While CDK6 is over-expressed in cancer cells, it has a low detectable level in non-cancerous cells and CDK6-null mice develop normally, suggesting a specific oncogenic role of CDK6, and that its inhibition may represent an ideal mechanism-based and low toxic therapeutic strategy in cancer treatment. Identification of selective small molecule inhibitors of CDK6 is thus needed for drug development. Herein, we review the latest understandings of the biological regulation and oncogenic roles of CDK6. The potential clinical relevance of CDK6 inhibition, the progress in the development of small-molecule CDK6 inhibitors and the rational design of potential selective CDK6 inhibitors are also discussed.

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Section: Structural Features and Regulationmentioning

confidence: 99%

Targeting CDK6 in cancer: State of the art and new insights

et al. 2015

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“…application of antibiotics, corticosteroids, purine analogs and monoclonal antibodies. [7][8][9][10][11] The combined therapy of purine analogs with alkylator significantly increased patients' response to administered therapy. 8,10,11 There are a large number of new anticancer compounds currently undergoing preclinical or clinical tests.…”

Section: Introductionmentioning

confidence: 99%

“…12 Some of them reflect their action toward uncycling and cycling cell populations. 6,7,12 Despite the increasing number of clinical diagnostic parameters and overall improvement of patients' response to therapy, there are still patients who display a poor reaction to administered drugs. 13,14 The results revealed that in the group of CLL patients treated previously with chlorambucil or fludarabine, an reveal their predictive value for clinical response for CLL patients much earlier, after ex vivo testing of their PBMC sensitivity to planned treatment options.…”

Section: Introductionmentioning

confidence: 99%

Toward personalized therapy for chronic lymphocytic leukemia

Rogalińska

Franiak-Pietryga

Błoński

et al. 2013

Cancer Biology & Therapy

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“…It is in this deeper mechanistic understanding of the executive 'enzymatic engines' of the mammalian cell division cycle (Schwartz and Shah, 2005;Marretta and Ales, 2010), that the drug targets of a more effectual apothecary for both vascular proliferative disorders (Charron et al, 2006) and otherwise intractable cancers can be found (Johnson and Shapiro, 2010;Krystof and Uldrijan, 2010). Located at the headwaters of oncogenesis, where growth-promoting proto-oncogenes meet and physically inactivate the predominant endogenous tumor suppressor proteins (Sherr and McCormick, 2002), a class of inducible regulatory proteins called "Cyclins" residealong with their Cyclin-dependent, proline-directed protein kinase (CDK) partners (Hall and Vulliet, 1991;Pines, 1995) and their respective polypeptide CDK inhibitors, which themselves represent a potent form of physiological growth inhibition/tumor suppression (Viallard, et al, 2001;Wesierska-Gadek et al, 2011). In the course of the mammalian cell division cycle, the Cyclins appear in a sequential manner, in accordance with the progressive stages of the cell cycle [note, the alphabetical designation Cyclins A through G denotes the order of scientific discovery/cloning, rather than the temporal induction of the gene product per se], participating directly in the enzymatic activation of one or more cognate CDKs (Gerard and Goldbetter, 2009) while physically guiding the activated protein kinase complexes to specific substrates (first demonstrated by Peeper et al, 1993) and subcellular locations (Morgan, 1997).…”

Section: Setting the Stage -Targeting Metastasis One Of The Gravest mentioning

confidence: 99%