Date published: 2025-10-29

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TAF II p135 Inhibitors

TAF II p135 inhibitors, as listed, primarily focus on compounds that influence transcriptional regulation either by targeting components of the transcription machinery or by affecting processes upstream or downstream of transcription initiation. The TAF II p135 subunit of TFIID plays a crucial role in the formation of the preinitiation complex, and its proper function is essential for the transcription of most RNA polymerase II-transcribed genes. The inhibitors identified here do not target TAF II p135 directly, but their modes of action are likely to impact its activity. Compounds like Triptolide and DRB inhibit general transcription machinery, potentially affecting TAF II p135 activity by altering the overall transcriptional landscape. Flavopiridol and α-Amanitin target specific stages of transcription (elongation and initiation, respectively), and their indirect effects could extend to TAF II p135. Actinomycin D and Cordycepin disrupt RNA synthesis, which would invariably influence transcription initiation processes involving TAF II p135.

The complexity of transcriptional regulation means that these inhibitors could have broad and sometimes unpredictable effects. For example, Trichostatin A and Bortezomib affect chromatin structure and protein degradation, respectively, both of which are crucial for the regulation of transcription initiation. Rocaglamide and Anisomycin, by inhibiting translation, could alter the availability of transcription factors and co-activators, indirectly affecting TAF II p135's role in transcription. JQ1, a well-known inhibitor of BET bromodomains, represents an interesting case where the alteration of chromatin reader interactions could potentially impact TAF II p135 function. These inhibitors offer a diverse toolkit for exploring the regulation of transcription and the role of TAF II p135 within this process. It is important to note that due to the essential nature of transcription, the use of these inhibitors requires careful consideration, particularly in in vivo systems, due to the potential for broad effects on cellular function. The study of these inhibitors provides valuable insights into the complex mechanisms of transcriptional regulation and the pivotal role played by TAF II p135 within this framework.

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