Date published: 2025-9-18

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ZHX3 Inhibitors

Chemical inhibitors of ZHX3 can exert their inhibitory action through various mechanisms, primarily by targeting the cell cycle and transcriptional regulation processes ZHX3 is associated with. Alsterpaullone, Roscovitine, Purvalanol A, Indirubin-3'-monoxime, Flavopiridol, and Olomoucine are all inhibitors of cyclin-dependent kinases (CDKs), a group of proteins critical for the control of cell cycle progression. By inhibiting CDKs, these compounds can disrupt the normal timing and regulation of the cell cycle, which is a process ZHX3 is linked to. For instance, Flavopiridol can impede the transcriptional regulation that relies on cell cycle progression, hence, it can inhibit ZHX3's capability to perform its role in transcriptional events that are cell cycle-dependent.

Further expanding on this theme, PD0332991, Dinaciclib, AZD5438, SU9516, Milciclib, and SNS-032 are also CDK inhibitors but with varying specificities and targets within the CDK family. PD0332991, for example, is specific for CDK4/6 and can inhibit ZHX3 by preventing the cell from advancing through the stages of the cell cycle, which could be vital for ZHX3's function. Meanwhile, Dinaciclib is known for its potent inhibition across a range of CDKs and can hinder the transcriptional machinery that ZHX3 might influence. AZD5438's inhibition of CDKs leads to a disruption in the cell cycle checkpoints, which are critical junctures at which ZHX3 may exert its influence on gene expression. SU9516 modifies the progression through the cell cycle, which can lead to an inhibition of ZHX3's activity in relation to cell division and transcriptional regulation. Milciclib targets multiple CDKs, impacting both the cell cycle and transcriptional mechanisms that ZHX3 is implicated in, thereby inhibiting its function. Lastly, SNS-032 can inhibit the phase transitions of the cell cycle and the regulation of transcription, which can inhibit the functional activity of ZHX3 in these processes.

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