Date published: 2025-9-13

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ACAT-2 Activators

ACAT-2 Activators encompass a diverse set of chemical compounds that serve to augment the functional activity of ACAT-2 through various biochemical mechanisms. For instance, Forskolin and 8-Bromo-cAMP boost intracellular cAMP, which activates protein kinase A (PKA) and can lead to the phosphorylation of proteins that interact with ACAT-2, thus enhancing its enzymatic role in cholesterol esterification. Similarly, Oleic Acid and Squalene provide a substrate for ACAT-2, which facilitates its activity in esterifying cholesterol, while 5-Aminolevulinic acid could increase cholesterol demand in mitochondria, indirectly promoting ACAT-2 action. Pregnenolone and Geranylgeranyl pyrophosphate, by their roles in steroidogenesis and protein prenylation, respectively, may upregulate ACAT-2 activity to meet the cellular needs for cholesterol-derived molecules. Additionally, modulators of cholesterol homeostasis, such as Cholic Acid, may enhance ACAT-2 activity by stimulating cholesterol turnover for bile acid synthesis.

Furthermore, compounds like LXR agonists GW3965 and T0901317 indirectly augment ACAT-2 function by upregulating genes in cholesterol metabolism, which could lead to increased cholesterol transport and efflux, enhancing the esterification function of ACAT-2. Pioglitazone, through PPAR-gamma agonism, alters lipid metabolism pathways which can incidentally upregulate ACAT-2 activity. Lastly, Retinoic Acidcould stimulates ACAT-2 activity by increasing the demand for cholesterol in the membranes during cell differentiation. Collectively, these activators work through distinct yet complementary mechanisms to enhance the functional activity of ACAT-2 without directly upregulating its expression or activating the protein in a direct fashion. Instead, they modulate the biochemical landscape in which ACAT-2 operates, ensuring that the protein's enzymatic activity related to cholesterol esterification is heightened in response to the cellular metabolic requirements.

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