Structure-Activity Relationship Study and Design Strategies of Hydantoin, Thiazolidinedione, and Rhodanine-Based Kinase Inhibitors: A Two-Decade Review.
Muhammad NaufalElvira HermawatiYana Maolana SyahAce Tatang HidayatIka Wiani HidayatJamaludin Al AnshoriPublished in: ACS omega (2024)
Cancer is one of the most prominent causes of the rapidly growing mortality numbers worldwide. Cancer originates from normal cells that have acquired the capability to alter their molecular, biochemical, and cellular traits. The alteration of cell signaling enzymes, such as kinases, can initiate and amplify cancer progression. As a curative method, the targeted therapy utilized small molecules' capability to inhibit kinase's cellular function. This review provides a brief history (1999-2023) of Small Molecule Kinase Inhibitors (SMKIs) discovery with their molecular perspective. Furthermore, this current review also addresses the application and the development of hydantoin, thiazolidinedione, and rhodanine-based derivatives as kinase inhibitors toward several subclasses (EGFR, PI3K, VEGFR, Pim, c-Met, CDK, IGFR, and ERK) accompanied by their structure-activity relationship study and their molecular interactions. The present work summarizes and compiles all the important structural information essential for developing hydantoin, thiazolidinedione, and rhodanine-based kinase inhibitors to improve their potency in the future.
Keyphrases
- small molecule
- structure activity relationship
- papillary thyroid
- squamous cell
- small cell lung cancer
- tyrosine kinase
- induced apoptosis
- healthcare
- signaling pathway
- high throughput
- cardiovascular disease
- mesenchymal stem cells
- gene expression
- type diabetes
- squamous cell carcinoma
- coronary artery disease
- dna methylation
- genome wide
- single molecule
- cell therapy
- cell cycle
- current status
- cardiovascular events
- young adults
- health information
- risk factors
- endothelial cells
- protein kinase