Date published: 2025-9-10

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CCDC138 Activators

Epidermal Growth Factor (EGF) and Retinoic Acid orchestrate cellular signaling and gene expression regulation, impacting cytoskeletal organization and ciliogenesis, processes that could engage CCDC138's functional role in the cell. Microtubule dynamics, critical for cellular structure and division, are influenced by Taxol and Nocodazole; these alterations can extend to the operational purview of CCDC138, particularly if it is involved in chromosomal segregation or ciliary maintenance. Compounds like Lithium Chloride and Forskolin act on the Wnt signaling and cAMP pathways, respectively. These signaling cascades are essential for a plethora of cellular functions, including those governing the structure and function of cilia, where CCDC138 might be implicated. Additionally, chemical agents such as 5-Azacytidine, which modulates DNA methylation, and MG132, a proteasome inhibitor, can impact gene expression and protein stability, potentially affecting the turnover and function of CCDC138 within the cellular milieu.

The chemical interplay extends with Y-27632, a ROCK inhibitor that influences cytoskeletal dynamics, and Chloroquine, which alters autophagic and endosomal trafficking processes. These compounds could have a bearing on CCDC138 activity by modifying the structural framework of the cell, which is indispensable for the proper localization and function of ciliary proteins. Rapamycin, known for its role in autophagy and ciliogenesis, and ZM-447439, an Aurora kinase inhibitor, further contribute to the intricate regulatory environment that could dictate CCDC138's activity by affecting cell division and possibly ciliary disassembly.

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