Opportunities and Challenges for the Development of MRCK Kinases Inhibitors as Potential Cancer Chemotherapeutics

Cytoskeleton organization and dynamics are rapidly regulated by post-translational modifications of key target proteins. Acting downstream of the Cdc42 GTPase, the myotonic dystrophy-related Cdc42-binding kinases MRCKα, MRCKβ, and MRCKγ have recently emerged as important players in cytoskeleton regu...

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Published inCells (Basel, Switzerland) Vol. 12; no. 4; p. 534
Main Authors Ruscetta, Vanessa M, Seaton, Taj J, Shakeel, Aleen, Vasconcelos, Stanley N S, Viirre, Russell D, Adler, Marc J, Olson, Michael F
Format Journal Article
LanguageEnglish
Published Switzerland MDPI AG 01.02.2023
MDPI
Subjects
Amino acids
Breast cancer
Cancer
Care and treatment
Cdc42 protein
Cell Movement
Chemotherapy
Cytoskeleton
Gene expression
Humans
Invasiveness
Kinases
Metastasis
Methods
Motility
Myosin
Myotonic dystrophy
Myotonin-Protein Kinase - metabolism
Neoplasms - pathology
Ovarian cancer
Phagocytosis
Phosphorylation
Post-translation
Proteins
Review
rho-Associated Kinases - metabolism
Signal Transduction
Canada
cytoskeleton
signal transduction
phosphorylation
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Summary:Cytoskeleton organization and dynamics are rapidly regulated by post-translational modifications of key target proteins. Acting downstream of the Cdc42 GTPase, the myotonic dystrophy-related Cdc42-binding kinases MRCKα, MRCKβ, and MRCKγ have recently emerged as important players in cytoskeleton regulation through the phosphorylation of proteins such as the regulatory myosin light chain proteins. Compared with the closely related Rho-associated coiled-coil kinases 1 and 2 (ROCK1 and ROCK2), the contributions of the MRCK kinases are less well characterized, one reason for this being that the discovery of potent and selective MRCK pharmacological inhibitors occurred many years after the discovery of ROCK inhibitors. The disclosure of inhibitors, such as BDP5290 and BDP9066, that have marked selectivity for MRCK over ROCK, as well as the dual ROCK + MRCK inhibitor DJ4, has expanded the repertoire of chemical biology tools to study MRCK function in normal and pathological conditions. Recent research has used these novel inhibitors to establish the role of MRCK signalling in epithelial polarization, phagocytosis, cytoskeleton organization, cell motility, and cancer cell invasiveness. Furthermore, pharmacological MRCK inhibition has been shown to elicit therapeutically beneficial effects in cell-based and in vivo studies of glioma, skin, and ovarian cancers.
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ISSN:2073-4409
2073-4409
DOI:10.3390/cells12040534