Date published: 2025-12-20

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TMEM200C Activators

TMEM200C, predicted to be an integral component of the cell membrane, holds significance in cellular processes yet to be fully elucidated. The integral nature of this transmembrane protein suggests its involvement in membrane-related functions, potentially contributing to cellular structure, signaling, or transport processes. Despite limited knowledge of its precise function, exploring potential activators may provide insights into the regulation of TMEM200C. The activation of TMEM200C involves a diverse array of chemical modulators that influence specific pathways. Direct activators, such as Retinoic Acid and TPA, directly enhance TMEM200C expression through retinoic acid signaling and the PKC/AP-1 pathway, respectively. Indirect activators, exemplified by Forskolin and Dibutyryl cAMP, modulate the cAMP/PKA/CREB pathway, highlighting the intricacy of signaling cascades regulating TMEM200C. Histone deacetylase inhibitors like Sodium Butyrate and Trichostatin A create a permissive chromatin environment, indirectly promoting TMEM200C transcription. The specific influences of these chemicals on cellular pathways provide a nuanced understanding of TMEM200C activation.

In summary, TMEM200C, as a transmembrane protein, remains an enigmatic player in cellular processes associated with the cell membrane. The activation of TMEM200C is intricately regulated by a variety of chemical modulators, each influencing specific pathways and contributing to the intricate network governing TMEM200C expression. While further research is required to unveil the precise functions and implications of TMEM200C activation, this exploration sheds light on potential avenues for unraveling its role in cellular membrane dynamics.

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