Date published: 2025-11-3

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YLAT1 Activators

Chemical activators of YLAT1 can play a significant role in the functional activation of this amino acid transport protein. The activation process of YLAT1 involves various amino acid substrates that bind to the protein and induce conformational changes that enhance its transport capacity. L-Arginine, for example, is not only a substrate for YLAT1 but also serves as a precursor for the production of nitric oxide. The nitric oxide produced can increase the fluidity of the cell membrane, which in turn facilitates the uptake of substrates by YLAT1. Similarly, L-Leucine, as a substrate, activates YLAT1 by increasing the concentration gradient, thereby promoting the uptake process intrinsic to the protein's function. L-Lysine and L-Histidine can allosterically bind to YLAT1, inducing conformational changes that activate the protein. This substrate-induced activation mechanism may increase the affinity of YLAT1 for its substrates, thus enhancing its transport activity.

Further, aromatic amino acids like L-Phenylalanine, L-Tryptophan, and L-Tyrosine can activate YLAT1 by binding to it, which possibly triggers a conformational shift, thereby increasing the transport activity of YLAT1. L-Glutamine might activate the protein by acting as a competitive substrate, stimulating the transport system to increase substrate uptake. In a similar way, L-Aspartic acid, by serving as a substrate, can activate the transport activity of YLAT1 through substrate-specific activation. L-Serine and L-Threonine, by contributing to the substrate pool, can activate YLAT1 by promoting the transport function of the protein through increased substrate availability. Lastly, L-Isoleucine can activate YLAT1 by binding to the transport protein, which may lead to a conformational change that enhances the transport activity of the protein, ensuring efficient transport of the amino acid substrates across the cell membrane.

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