The chemical class known as LONP1 Inhibitors comprises various compounds that indirectly suppress the activity of LONP1, a key mitochondrial protease. These inhibitors primarily exert their effects by disrupting mitochondrial function and proteostasis, thereby influencing LONP1's role in mitochondrial quality control. Proteasome inhibitors like Bortezomib and MG132 exemplify this mechanism by leading to the accumulation of proteins within the cell, which can overwhelm LONP1's proteolytic capacity and indirectly inhibit its function.
Compounds that impair mitochondrial ATP production, such as Oligomycin, Antimycin A, and Rotenone, are also significant members of this class. By inhibiting various components of the electron transport chain, these compounds reduce ATP synthesis, crucial for LONP1's activity. This reduction in ATP levels indirectly inhibits LONP1, demonstrating the dependency of LONP1's function on adequate cellular energy levels. Additionally, inhibitors of glycolysis like 2-Deoxy-D-glucose contribute to this class by reducing the overall ATP pool available to the cell, further impacting LONP1 activity. Auranofin, through its inhibition of thioredoxin reductase, affects the redox balance within mitochondria, which can indirectly inhibit LONP1 by altering the mitochondrial environment in which it operates. Compounds such as Cadmium Chloride and Mito-TEMPO highlight the role of mitochondrial health and dynamics in LONP1 activity.
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| Product Name | CAS # | Catalog # | QUANTITY | Price | Citations | RATING |
|---|---|---|---|---|---|---|
Actinonin | 13434-13-4 | sc-201289 sc-201289B | 5 mg 10 mg | $170.00 $385.00 | 3 | |
A peptide deformylase inhibitor that can affect mitochondrial protein maturation, potentially inhibiting LONP1 by altering the pool of proteins needing degradation. | ||||||
Doxycycline Hyclate | 24390-14-5 | sc-204734B sc-204734 sc-204734A sc-204734C | 100 mg 1 g 5 g 25 g | $27.00 $50.00 $105.00 $194.00 | 25 | |
An antibiotic known to inhibit mitochondrial biogenesis, potentially inhibiting LONP1 by affecting overall mitochondrial health and protein turnover. | ||||||