Date published: 2025-10-14

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INCA1 Activators

INCA1, short for Inhibitor of CDK, Cyclin A1 interacting protein, is a distinctive entity within the cellular machinery, encoded by the INCA1 gene in humans. This protein garners special attention due to its integral role in cell cycle regulation, primarily through its interactions with cyclin A1 and the inhibition of cyclin-dependent kinase 2 (CDK2). CDK2 is a pivotal enzyme that propels cell cycle progression, and thus, INCA1 serves as a crucial checkpoint in maintaining the precision of cell division. The expression of INCA1 is not static and can be influenced by numerous intracellular and extracellular stimuli. Understanding the factors that can induce INCA1 expression is an area of significant interest, as it sheds light on the complex regulatory networks that govern cell proliferation and the maintenance of genomic stability.

Chemical compounds, through diverse mechanisms, have the potential to act as activators, leading to the upregulation of INCA1 expression. For instance, certain compounds may upregulate INCA1 by initiating a cellular stress response, a common reaction to external stimuli, which necessitates a rapid cellular adaptation to maintain homeostasis. Others could stimulate INCA1 synthesis by interacting with specific transcription factors or by altering the epigenetic landscape, thereby enhancing the transcription of the INCA1 gene. Some chemicals might induce the expression of INCA1 as part of a defense mechanism against oxidative damage or in response to DNA damage that activates cell cycle checkpoints. Moreover, environmental factors, such as exposure to heavy metals or endocrine-disrupting compounds, could also lead to an increase in INCA1 expression as the cell mobilizes its protective measures. The intricate interplay between these activators and the INCA1 gene exemplifies the dynamic nature of gene regulation in response to environmental and chemical signals, highlighting the adaptability of cellular systems to maintain equilibrium and safeguard their genomic integrity.

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