Date published: 2025-10-26

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GLT8D1 Inhibitors

GLT8D1 inhibitors are a diverse set of chemical compounds that lead to the functional inhibition of the glycosyltransferase GLT8D1. Cyclopamine acts by suppressing the Hedgehog signaling pathway, which is crucial for various cellular processes, including those associated with glycosylation that GLT8D1 may participate in. Similarly, LY 294002, as a PI3K inhibitor, disrupts the PI3K/AKT pathway, potentially affecting GLT8D1 by altering the availability of glycosylation substrates or overall glycosylation patterns. Compounds like Swainsonine and Kifunensine, which inhibit alpha-mannosidase II and mannosidase I respectively, may lead to the accumulation of misfolded glycoproteins and decrease the glycosylation activity of GLT8D1 by substrate depletion. Likewise, Castanospermine and 2-Deoxy-D-glucose, by interfering with glucosidase and glycolysis respectively, could hinder the proper glycan processing and energy substrates required for GLT8D1's function.

Further influencing the glycosylation landscape that GLT8D1 operates within, Tunicamycin inhibits N-linked glycosylation, potentially causing a backlog of unprocessed glycoproteins and reducing GLT8D1 activity. The compound Brefeldin A disrupts ER to Golgi apparatus transport, which is critical for glycosylation substrate accessibility, thereby potentially reducing GLT8D1's glycosyltransferase function. Miglustat and Deoxynojirimycin, both iminosugars, target enzymes upstream of GLT8D1, such as glucosylceramide synthase and alpha-glucosidase, which could result in misfolded glycoprotein accumulation and interfere with GLT8D1's activity. Similarly, 1-Deoxymannojirimycin, an alpha-mannosidase inhibitor, may disrupt normal glycan maturation, affecting GLT8D1's role in glycan chain elongation. Lastly, PD 98059 targets the MAPK/ERK pathway through MEK inhibition, which can influence signaling pathways that regulate glycosyltransferases like GLT8D1, potentially diminishing its ability to participate in glycan chain elongation. Collectively, these inhibitors disrupt various aspects of the glycosylation pathway, either by directly targeting the glycosylation enzymes or by affecting the availability of substrates and energy, thereby reducing the functional activity of GLT8D1.

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