Date published: 2025-9-13

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Prickle2 Activators

Prickle2, a pivotal protein in the planar cell polarity (PCP) signaling pathway, plays an instrumental role in the orchestration of cellular alignment across the tissue plane, a process crucial for numerous developmental and physiological processes. It is a part of the non-canonical Wnt signaling pathway, which diverges from the canonical pathway by not relying on beta-catenin mediated transcription. Instead, it influences the orientation and movement of cells and their appendages. The expression of Prickle2, like many genes, is subject to complex control by a network of signaling pathways and transcription factors. The precise tuning of Prickle2 expression is essential for its role in PCP and, therefore, in the proper formation of the body plan and the function of various tissues. Prickle2's significance extends beyond development into adult physiology, with research indicating its involvement in neural networking and potentially in cognitive functions.

The expression of Prickle2 can be potentially induced by a diverse array of chemical activators that interact with various molecular pathways. Compounds such as Valproic acid, an HDAC inhibitor, might induce Prickle2 expression by loosening the compact chromatin structure, thereby exposing the gene to transcriptional machinery. Forskolin, through the elevation of cAMP, could potentially stimulate Prickle2 expression via cAMP response element-binding protein, a transcription factor that binds to DNA sequences near the gene, promoting its transcription. Phytochemicals like Epigallocatechin gallate (EGCG) and Curcumin are other examples of compounds that could induce Prickle2 expression. EGCG may upregulate gene expression by inhibiting detrimental enzymatic activity that normally suppresses transcription, while Curcumin might exert its effect by obstructing pathways that repress Prickle2 transcription. Environmental chemicals like Bisphenol A and dietary supplements such as Vitamin D3 also represent classes of compounds that could play a role in the regulation of Prickle2. Bisphenol A might inadvertently induce the expression of Prickle2 by interfering with hormonal signaling pathways, whereas Vitamin D3, after conversion to its active form, could potentially stimulate Prickle2 expression by interacting with vitamin D response elements in the genome. It is important to note that while these compounds have been associated with gene expression modulation, their specific effects on Prickle2 require experimental validation, and their use is purely speculative in this context.

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