Date published: 2025-9-11

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ISCA1 Inhibitors

ISCA1 inhibitors are chemical compounds designed to specifically inhibit the activity of the Iron-Sulfur Cluster Assembly 1 (ISCA1) protein. ISCA1 is involved in the assembly of iron-sulfur (Fe-S) clusters, which are essential cofactors in numerous cellular processes, including electron transport, enzyme catalysis, and the regulation of gene expression. These inhibitors target the ISCA1 protein's ability to facilitate the maturation and incorporation of iron-sulfur clusters into specific apoproteins. Structurally, ISCA1 inhibitors are often small molecules that interact with the protein's binding sites, either by blocking access to its ligands or by inducing conformational changes that impair its activity. Inhibition of ISCA1 leads to disruptions in Fe-S cluster biogenesis, which can affect several key biological pathways, given the critical role of Fe-S clusters in cellular metabolism and redox homeostasis.

The chemical structure of ISCA1 inhibitors typically includes moieties that enable them to chelate metal ions or interfere with the protein's iron-binding sites, a critical feature given ISCA1's role in managing iron incorporation into Fe-S clusters. These inhibitors may also contain hydrophobic or hydrophilic domains to optimize their interaction with cellular membranes and proteins. Variability in these structural features allows for a range of compounds with different binding affinities and specificities for ISCA1. The study of ISCA1 inhibitors is valuable for understanding the broader roles of Fe-S cluster assembly in cellular physiology and in delineating how the perturbation of these pathways can lead to changes in cellular behavior and metabolic flux.

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