Date published: 2025-10-31

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C14orf147 Inhibitors

The chemical class of "C14orf147 Inhibitors" comprises a diverse range of compounds that indirectly modulate the activity of the protein encoded by the C14orf147 gene. This class represents a sophisticated approach to influencing protein function, where the focus is on altering various cellular processes and signaling pathways rather than direct interaction with the protein itself. The variety of compounds within this class highlights the intricate nature of protein regulation and the potential for targeting multiple aspects of cellular physiology to achieve desired modulatory effects.

In this class, compounds like Paclitaxel, a microtubule stabilizer, underscore the influence of cytoskeletal dynamics on protein function. By affecting cell division and signaling, Paclitaxel can potentially alter the cellular context in which C14orf147 operates, thereby indirectly influencing its activity. This approach showcases the significance of targeting fundamental cellular structures and processes as a means to modulate protein activity.

Other compounds in the class, such as cisplatin and doxorubicin, which are known for their roles in chemotherapy, demonstrate how DNA interaction and damage can indirectly impact protein activities. Cisplatin, by inducing DNA crosslinking, and doxorubicin, through its effects on DNA replication and repair, exemplify how genotoxic stress can lead to changes in the cellular environment, potentially affecting the function of proteins like C14orf147.

Etoposide and 5-Fluorouracil, affecting topoisomerase activity and pyrimidine synthesis, respectively, further illustrate the complex relationship between DNA processes and protein regulation. By influencing these key aspects of cellular function, these compounds can indirectly modulate the activity of proteins involved in various cellular pathways, including C14orf147.

Additionally, kinase inhibitors such as sunitinib and sorafenib, which affect multiple signaling pathways, reflect the intricate network of intracellular communication and its impact on protein functions. By modulating these signaling networks, kinase inhibitors demonstrate the potential for broad effects on proteins, including those like C14orf147.

Histone deacetylase inhibitors like vorinostat and trichostatin A, along with the proteasome inhibitor bortezomib, represent another facet of this class. These compounds, by altering chromatin structure, gene expression, and protein degradation pathways, respectively, demonstrate the complexity of epigenetic and proteostasis mechanisms in regulating protein activities.

In summary, the "C14orf147 Inhibitors" class represents a comprehensive approach to influencing protein activity, highlighting the potential of leveraging various biochemical pathways and cellular processes. This class not only sheds light on the complex regulation of proteins like C14orf147 but also underscores the broader implications of such modulation in cellular physiology. As research continues to evolve, a deeper understanding of these biochemical interactions is expected to emerge, offering new perspectives on protein regulation. This approach exemplifies the sophistication of current scientific understanding and the ongoing efforts to develop more effective strategies for modulating protein activity in complex biological systems.

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