Date published: 2025-9-12

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SCCA2 Activators

The chemical activators of Squamous Cell Carcinoma Antigen 2 (SCCA2) are a collection of compounds that influence SCCA2 expression or activity through various indirect cellular mechanisms. These mechanisms include alterations in gene expression, modulation of signaling pathways, and changes in cellular stress responses. Erlotinib and Acitretin represent a class of compounds that modulate gene expression via receptor signaling pathways. Erlotinib, by inhibiting EGFR, and Acitretin, through its impact on retinoid-responsive genes, demonstrate the influence of cell surface receptor signaling on the transcriptional regulation of SCCA2. Similarly, Calcipotriol and Isoproterenol affect gene expression through Vitamin D receptor signaling and cAMP pathways, respectively. These pathways are crucial in cellular differentiation and response mechanisms, thereby potentially impacting SCCA2 expression in specific cell types.

Further, compounds like Bryostatin 1 and Trichostatin A highlight the role of post-translational modifications in regulating SCCA2. Bryostatin 1's activation of PKC and Trichostatin A's inhibition of histone deacetylases underscore the diverse molecular interactions that can influence SCCA2 expression. BAY 11-7082, Ruxolitinib, and Hydrocortisone demonstrate the impact of inflammatory and immune signaling pathways on SCCA2, reflecting the protein's involvement in response to cellular stress and immune modulation. Additionally, Menadione, Decitabine, and Puromycin present different mechanisms of influencing SCCA2 expression. Menadione induces oxidative stress, potentially affecting signaling pathways that modulate SCCA2 levels. Decitabine alters gene expression patterns through epigenetic modifications, while Puromycin's inhibition of protein synthesis can lead to broader changes in cellular signaling, indirectly impacting SCCA2 activity.

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