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Target Concepts:
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Query: EC:6.2.1.1 (
ACS
)
78,556
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Neuromedin U
(
NMU
) and S (NMS) display various physiological activities, including an anorexigenic effect, and share a common C-terminal heptapeptide-amide sequence that is necessary to activate two
NMU
receptors (NMUR1 and NMUR2). On the basis of this knowledge, we recently developed hexapeptide agonists 2 and 3, which are highly selective to human NMUR1 and NMUR2, respectively. However, the agonists are still less potent than the endogenous ligand, hNMU. Therefore, we performed an additional structure-activity relationship study, which led to the identification of the more potent hexapeptide 5d that exhibits similar NMUR1-agonistic activity as compared to hNMU. Additionally, we studied the stability of synthesized agonists, including 5d, in rat serum, and identified two major biodegradation sites: Phe(2)-Arg(3) and Arg(5)-Asn(6). The latter was more predominantly cleaved than the former. Moreover, substitution with 4-fluorophenylalanine, as in 5d, enhanced the metabolic stability at Phe(2)-Arg(3). These results provide important information to guide the development of practical hNMU agonists.
ACS
Med Chem Lett 2015 Mar 12
PMID:Discovery of potent hexapeptide agonists to human neuromedin u receptor 1 and identification of their serum metabolites. 2581 50
Neuromedin U
(
NMU
) is a multifunctional neuropeptide which is characterized by a high conservation through all species. Herein, we describe the synthesis of a novel set of
NMU
-analogs based on the truncated
NMU
-8. Through combination of previously reported modifications, an elaborate structure-activity relationship study was performed aiming for the development of peptides with an increased selectivity toward
NMU
receptor 1 (NMUR1). Compound
7
possessed the highest NMUR1 selectivity (IC
50
= 0.54 nM, selectivity ratio = 5313) together with an increased potency (EC
50
= 3.7 nM), an 18% increase of the maximal effect at NMUR1, and a higher resistance against enzymatic degradation as compared to the native
NMU
-8. The development of a potent NMUR1 agonist with extended half-life could represent an attractive tool to further unveil the role of NMUR1 in
NMU
signaling.
ACS
Med Chem Lett 2018 May 10
PMID:Synthesis and
in Vitro
Evaluation of Stabilized and Selective Neuromedin U-1 Receptor Agonists. 2979 66
