UBQLN3 Activators are a collection of chemicals that indirectly bolster the functional activity of UBQLN3 through multiple cellular signaling pathways and stress responses. Forskolin elevates cAMP, which activates PKA, potentially increasing phosphorylation events that modulate UBQLN3's activity in protein quality control. Ionomycin, by raising intracellular calcium levels, may influence UBQLN3's participation in calcium-dependent proteostasis. ALLN and MG132, by inhibiting calpain and the proteasome respectively, could lead to an accumulation of misfolded proteins, subsequently enhancing the role of UBQLN3 in protein triage decisions. Phorbol 12-myristate 13-acetate (PMA) activates PKC, possibly leading to phosphorylation of substrates that affect UBQLN3's function, while chloroquine and bafilomycin A1 disrupt lysosomal function, which may upregulate UBQLN3-mediated pathways as a compensatory mechanism.
Rapamycin and AICAR are known to induce autophagy; this might amplify UBQLN3's involvement in directing autophagic protein degradation. Retinoic acid could enhance UBQLN3 activity by modulating gene expression of proteins involved in UBQLN3-associated pathways. Tunicamycin and thapsigargin create ER stress by inhibiting glycosylation and disrupting calcium stores,respectively, potentially enhancing UBQLN3's response to misfolded proteins in the ER. The chemical influence of these activators demonstrates the multifaceted role of UBQLN3 in maintaining cellular proteostasis through various stress responses and regulatory mechanisms. Together, these compounds provide a diverse set of tools that can indirectly promote the functional activity of UBQLN3, ensuring the proper handling and turnover of proteins within the cell.
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