The Renaissance of CDK Inhibition in Cancer Therapy
A special issue of Cancers (ISSN 2072-6694). This special issue belongs to the section "Cancer Therapy".
Deadline for manuscript submissions: closed (30 September 2021) | Viewed by 39509
Special Issue Editors
Interests: cell cycle; mesothelioma; DNA damage; tumor suppressor genes; RB family; p53; oncolytic viruses; cell death; CDK inhibitors; p27
Special Issues, Collections and Topics in MDPI journals
2. Department of Medical Biotechnologies, University of Siena, Siena, Italy
Interests: cell cycle; tumor suppressor genes; RB family; CDK inhibitors; environment and cancer
Special Issues, Collections and Topics in MDPI journals
Interests: cell cycle; targeted therapy; RB family; tumor suppressors; SRC family kinases; WEE1 kinase; mesothelioma
Special Issues, Collections and Topics in MDPI journals
Special Issue Information
Dear Colleagues,
Progression through the cell cycle largely relies on protein phosphorylation events, which are mainly driven by the sequential activation of cyclin-dependent kinases (CDKs). Cell cycle deregulation, owing to aberrant CDK expression and other mechanisms affecting the cell cycle’s core machinery, is one of the main, well-established, features of cancer. Not surprisingly, the pharmacological inhibition of CDKs was devised early on as a strategy to halt tumorigenesis. The application of such a straightforward strategy, however, proved to be challenging and many hurdles have been encountered on the long road to the successful application of CDK inhibitors for cancer treatment. First, more than twenty CDKs have been identified in mammalian cells; all of these interact with different classes of cyclins and are involved in multiple functions beyond cell cycle regulation, including transcription, DNA replication, and DNA repair. Because of such complexity, the first generations of ‘pan-CDK’ inhibitors, which non-specifically targeted multiple kinases, failed in the clinical setting. The lack of a thorough understanding of the mechanism of action impaired the identification of biomarkers for patient selection and the design of possible effective combination strategies.
The recent development of selective CDK4/6 inhibitors has revolutionized the field, leading to the rapid approval by both the Food and Drug Administration and European Medical Agency of their clinical use for the treatment of advanced or metastatic . In just a few years, the number of new selective CDK inhibitors and their potential application in a variety of cancer types—as either single agents or in combination strategies—has increased impressively (with hundreds of currently ongoing trials registered on clinicaltrials.gov).
This Special Issue aims to present a collection of studies, both at the preclinical and clinical level, on the use of CDK inhibitors as an antitumoral strategy for different cancers, which will provide insights into the molecular mechanisms driving their action and possible resistance. This Special Issue also aims to learn how to make the most of this new powerful tool in the anticancer drug arsenal, how to combine it with other anticancer strategies, and how to identify those patients who can benefit from such new approaches for an immediate improvement.
Dr. Francesca Pentimalli
Dr. Paola Indovina
Prof. Dr. Antonio Giordano
Guest Editors
Manuscript Submission Information
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Keywords
- cyclin dependent kinases (CDKs)
- CDK inhibitors
- cancer
- cell cycle
- cancer therapy
- predictive biomarkers
- acquired resistance
- drug combination strategies
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