Date published: 2025-9-15

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TRIM43C Activators

Chloroquine, by inhibiting lysosomal degradation, may cause an accumulation of cellular proteins that interact with Tripartite motif-containing 43C, enhancing its activity. NAD+ enhances sirtuin activity, which modulates DNA repair and transcription processes that Tripartite motif-containing 43C is involved with, leading to an active protein environment. Ionomycin raises intracellular calcium levels, activating signaling pathways that may include Tripartite motif-containing 43C, subsequently enhancing its activity.

Trichostatin A increases histone acetylation, making DNA more accessible to Tripartite motif-containing 43C, thus facilitating its functional activity. 5-Azacytidine, by inhibiting DNA methylation, alters gene expression, which could enhance the activity of Tripartite motif-containing 43C by changing its chromatin context. PDTC, through its modulation of redox-sensitive pathways, likely enhances Tripartite motif-containing 43C activity due to its potential sensitivity to redox changes. Thapsigargin, by increasing cytosolic calcium, activates calcium-dependent pathways that potentially boost Tripartite motif-containing 43C function. Lastly, sodium orthovanadate, by inhibiting phosphatases, may lead to an increase in the phosphorylation state of proteins that regulate or interact with Tripartite motif-containing 43C, thereby enhancing its activity.

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