Date published: 2025-9-13

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HARS2 Activators

HARS2, a mitochondrial histidyl-tRNA synthetase, plays an essential role in the translation of mitochondrial proteins by charging histidine to its cognate tRNA. Specific chemical compounds can enhance the activity of HARS2 through various biochemical mechanisms. For instance, certain molecules that stimulate adenylate cyclase to increase intracellular cAMP levels lead to the activation of protein kinase A, which can phosphorylate transcription factors that boost the expression of mitochondrial proteins, including HARS2. Similarly, polyphenolic compounds known to activate sirtuins, particularly SIRT1, can modulate the acetylation status of transcription factors and coactivators, fostering mitochondrial biogenesis and potentially augmenting the levels and activity of HARS2. Additionally, PPAR-gamma agonists can alter the transcriptional landscape by upregulating genes linked to glucose and lipid metabolism, thereby potentially increasing the expression of genes encoding mitochondrial enzymes and proteins such as HARS2 to meet heightened metabolic requirements.

Further biochemical mechanisms involve compounds that activate AMP-activated protein kinase, which in turn stimulates transcription of genes associated with energy metabolism, possibly promoting the expression of HARS2. Inhibition of GSK-3 by certain ions leads to the activation of transcription factors critical for mitochondrial biogenesis, enhancing the expression of mitochondrial proteins, including HARS2. Moreover, autophagy inducers can precipitate the renewal of mitochondria, consequently elevating the levels of mitochondrial components like HARS2. Activation of retinoid receptors by specific metabolites of vitamin A also influences the transcription of genes implicated in mitochondrial function, potentially leading to an increased presence of HARS2 in mitochondrial matrices. Other mechanisms include the use of AMPK activators that can upregulate genes vital for mitochondrial replication and function, suggesting a rise in HARS2 expression as a response to an increased demand for mitochondrial maintenance and energy production. Lastly, the activation of sirtuins by certain compounds further supports mitochondrial function by deacetylating and activating transcription factors involved in mitochondrial biogenesis, which could result in an upsurge of HARS2 expression, thus enhancing its function within the mitochondria.

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