The chemical class known as γ Enolase inhibitors encompasses a diverse range of compounds that either directly or indirectly modulate the activity of γ Enolase. While no direct inhibitors are listed, the indirect inhibitors presented showcase various mechanisms through which γ Enolase can be influenced. Fluoride disrupts glycolysis by inhibiting enolase's metal cofactor, impacting energy production and cellular processes. EGCG, a PI3K inhibitor, modulates the PI3K/AKT pathway, influencing γ Enolase indirectly and suggesting a connection between PI3K signaling and γ Enolase activity. 2-Deoxy-D-Glucose interferes with glycolysis, affecting energy production and cellular processes dependent on enolase function. Neomycin disrupts glycolysis by affecting ion gradients, influencing γ Enolase indirectly. PD98059, a MEK inhibitor, modulates the MAPK/ERK pathway, affecting cellular processes associated with MAPK/ERK activation and γ Enolase function. Auranofin targets redox signaling, impacting cellular processes dependent on redox balance and γ Enolase activity.
ML-9, a calmodulin inhibitor, modulates calcium signaling, influencing γ Enolase indirectly and suggesting a link between calmodulin activation and γ Enolase function. R406, a Syk inhibitor, influences the JAK/STAT pathway, affecting cellular processes associated with JAK/STAT activation and γ Enolase activity. 6-Azauridine interferes with nucleotide metabolism, suggesting a link between RNA synthesis and γ Enolase function. Wortmannin, a PI3K inhibitor, modulates the PI3K/AKT pathway, influencing γ Enolase indirectly. Piceatannol, a Syk inhibitor, influences the JAK/STAT pathway, affecting cellular processes associated with JAK/STAT activation and γ Enolase activity. SB203580, a p38 MAPK inhibitor, disrupts downstream signaling, highlighting a regulatory mechanism for γ Enolase through the p38 MAPK pathway. The diversity of these inhibitors underscores the complexity of γ Enolase regulation, providing insights into strategies targeting this enzyme. Understanding the mechanisms through which these chemicals modulate γ Enolase activity can inform further research into the role of γ Enolase in cellular processes and disease states.
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