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Novel venom-derived inhibitors of the human EAG channel, a putative antiepileptic drug target.

Biochem Pharmacol. 2018; 
Ma L, Chin YKY, Dekan Z, Herzig V, Chow CY, Heighway J, Lam SW, Guillemin GJ, Alewood PF, King GF.
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Peptide Synthesis Human atrial natriuretic peptide (1 M; GenScript, Piscataway, NJ, USA) and the analgesic drug Prialt (i. Get A Quote

摘要

Recently, we and other groups revealed that gain-of-function mutations in the human ether à go-go voltage-gated potassium channel hEAG1 (Kv10.1) lead to developmental disorders with associated infantile-onset epilepsy. However, the physiological role of hEAG1 in the central nervous system remains elusive. Potent and selective antagonists of hEAG1 are therefore much sought after, both as pharmacological tools for studying the (patho)physiological functions of this enigmatic channel and as potential leads for development of anti-epileptic drugs. Since animal venoms are a rich source of potent ion channel modifiers that have been finely tuned by millions of year of evolution, we screened 108 arachnid venoms for h... More

关键词

Epilepsy; Ion channel; Kv10.1; hEAG1; hERG