CMTM2a, an integral player in transcription corepressor activity, orchestrates cellular processes in the cytoplasm and nucleus. Actinomycin D, a potent RNA polymerase inhibitor, directly targets CMTM2a, disrupting its involvement in negative regulation of transcription and testosterone biosynthetic processes. Trichostatin A and SAHA modulate CMTM2a's transcription corepressor activity, influencing cellular dynamics in critical cellular compartments.
Etoposide and Camptothecin, inhibitors of topoisomerases, directly impact CMTM2a, disrupting its role in transcription corepressor activity and influencing processes related to testosterone biosynthesis. Flavopiridol and Vorinostat provide insights into CMTM2a's modulation through cyclin-dependent kinase and histone deacetylase inhibition, respectively. The DNA intercalators Doxorubicin and Ellipticine, along with the crosslinking agent Cisplatin, target CMTM2a, influencing its transcription corepressor activity and the regulation of testosterone biosynthesis. Azacitidine and 5-Aza-2'-deoxycytidine, DNA methyltransferase inhibitors, serve as direct CMTM2a inhibitors, providing a comprehensive understanding of the regulatory mechanisms involved in transcription and testosterone biosynthesis.
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