Date published: 2025-9-10

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KIF4B Activators

Kinesin family member 4B (KIF4B) is a protein encoded by the KIF4B gene in humans, functioning as a microtubule-associated motor protein. It plays a pivotal role in the intricate ballet of chromosome segregation and is intimately involved in the mechanisms of anaphase spindle dynamics and cytokinesis. The precise regulation of KIF4B is crucial for the maintenance of genomic stability and the orderly progression of cell division. As a member of the kinesin-4 protein family, KIF4B is speculated to engage in the transport of chromosome arm-associated proteins during mitosis, and its activity is tightly integrated with the function of the mitotic spindle, the cellular structure that separates chromosomes during cell division.

The expression of KIF4B, like many genes involved in cell cycle progression, may be susceptible to induction by a variety of biochemical compounds that are involved in modulating microtubule dynamics, cell cycle checkpoints, and gene expression pathways. Compounds such as paclitaxel and epothilone B, which stabilize microtubules, could potentially induce the expression of KIF4B by necessitating increased support from motor proteins during microtubule stabilization. Conversely, agents like vinblastine and nocodazole that disrupt microtubules might stimulate a compensatory cellular response to produce more KIF4B to bolster microtubule dynamics. Additionally, compounds that interact with cellular signaling pathways and affect gene expression, such as forskolin, retinoic acid, and lithium chloride, might also play a role in the upregulation of KIF4B expression. Forskolin, through elevation of cAMP, and retinoic acid, by engaging nuclear receptors, could promote transcriptional activity leading to increased KIF4B levels. Lithium chloride, through its inhibition of GSK-3 and consequent activation of Wnt signaling, may also stimulate the transcription of genes necessary for cell division, including KIF4B. It's important to highlight that while these compounds have been shown to influence cellular processes, their specific effects on the expression of KIF4B require targeted research to elucidate the exact molecular mechanisms involved.

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