Dynactin p135, also known by its alternate name p150^Glued, is a core component of the dynactin complex, playing a pivotal role in the process of dynein-mediated transport within cells. It is integral to the function of the motor protein dynein, thereby facilitating the intracellular movement of vesicles, organelles, and during the cell cycle, the segregation of chromosomes. Dynactin p135 is not just a passive scaffold but actively participates in the regulation of dynein's attachment to its cargo and the microtubule track along which it moves. The protein's structure allows it to interact with various other proteins and signaling molecules, which can influence its expression and function. Understanding the regulation of Dynactin p135's expression is crucial, as it is implicated in a variety of fundamental cellular activities.
The expression of Dynactin p135 can be influenced by a host of chemical activators, each operating through distinct cellular pathways and mechanisms. Compounds like retinoic acid, for instance, can initiate a transcriptional cascade by interacting with nuclear receptors, potentially leading to an upsurge in Dynactin p135 transcription. Similarly, agents such as 5-Azacytidine and Trichostatin A, which modulate the epigenetic landscape, could de-repress genes and enhance transcription, thereby stimulating an increase in Dynactin p135 levels. On the other hand, Forskolin, known to elevate cAMP levels, might activate a protein kinase A-dependent pathway, resulting in the stimulation of Dynactin p135 expression. Lithium Chloride, often associated with Wnt signaling, might also promote the expression of Dynactin p135 through stabilization of the transcriptional coactivator β-catenin. Additionally, histone deacetylase inhibitors like Sodium Butyrate can create a chromatin environment that is permissive for transcription, possibly inducing the expression of Dynactin p135. It is important to note that while these chemicals have the potential to influence Dynactin p135 expression, the specific pathways and the extent of their effects on Dynactin p135 would require comprehensive research to elucidate.
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