ATAD1 Activators play a pivotal role in enhancing the functional activity of ATAD1, primarily through pathways that bolster mitochondrial health and function. Resveratrol, by activating SIRT1, promotes deacetylation of proteins crucial for mitochondrial integrity, indirectly supporting ATAD1's role in mitochondrial maintenance. Similarly, the AMPK activator AICAR, and Metformin, both enhance mitochondrial biogenesis, thereby indirectly enhancing ATAD1's activity. Nicotinamide Mononucleotide (NMN), as a precursor to NAD+, elevates SIRT1 function, crucial for mitochondrial health, thereby supporting ATAD1 indirectly. Rapamycin's role in inhibiting mTOR leads to augmented mitophagy, a process essential for removing damaged mitochondria, thus indirectly maintaining the mitochondrial environment where ATAD1 operates. Bezafibrate, by activating PPARs and thus increasing mitochondrial fatty acid oxidation, supports ATAD1's function in maintaining mitochondrial energy metabolism.
The influence of other compounds on mitochondrial function and integrity further delineates the indirect activation pathways for ATAD1. SRT1720, as a SIRT1 activator, enhances mitochondrial function through the deacetylation of mitochondrial proteins, indirectly supporting ATAD1's role. Urolithin A, which induces mitophagy, and Elamipretide, known for stabilizing cardiolipin in mitochondrial membranes, both contribute to an environment conducive to ATAD1's optimal functioning. Pioglitazone, a PPAR-gamma agonist, enhances mitochondrial biogenesis, indirectly supporting ATAD1. Furthermore, Quercetin and Berberine, through their roles in enhancing mitochondrial biogenesis and function, possibly by activating AMPK and SIRT1 pathways, indirectly augment the functional capacity of ATAD1. Collectively, these chemical compounds, by influencing various pathways that converge on mitochondrial health and function, indirectly enhance the activity of ATAD1, underscoring its pivotal role in maintaining mitochondrial integrity.
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