Structure-Activity Relationships of Rat Neuromedin U for Smooth Muscle Contraction
Rat neuromedin U (r-NMU) and its fragment peptide amides were synthesized by solid-phase methodology. Using a chicken crop smooth muscle contraction assay, the potency of r-NMU and its fragments relative to porcine neuromedin U-8 (p-NMU-8) was r-NMU : 10.25±2.88, r-NMU (6-23) : 8.01±1.04, r-NMU (10-...
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Veröffentlicht in: | Chemical & pharmaceutical bulletin 1991/08/25, Vol.39(8), pp.2016-2020 |
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Zusammenfassung: | Rat neuromedin U (r-NMU) and its fragment peptide amides were synthesized by solid-phase methodology. Using a chicken crop smooth muscle contraction assay, the potency of r-NMU and its fragments relative to porcine neuromedin U-8 (p-NMU-8) was r-NMU : 10.25±2.88, r-NMU (6-23) : 8.01±1.04, r-NMU (10-23) : 2.76±0.46, r-NMU (13-23) : 2.81±0.52, and r-NMU (16-23) : 0.88±0.19, respectively. Two heptapeptides, r-NMU (17-23) and r-NMU (16-22), had a relative potency of 0.61 and 0.03 respectively, and elicited maximal contraction at a dose of 10 μM to a similar degree to p-NMU-8. The other shorter C-terminal fragments did not elicit the maximal contraction or any activity. In a rat uterus contraction assay, r-NMU (13-23), but not r-NMU (16-23), at a dose of 4 nM retained as high a stimulatory activity as r-NMU itself. r-NMU (17-22) was the smallest peptide fragment to elicit the maximal sustained contraction at 10 μM. These results indicate that the amino acid sequence Phe-Leu-Phe-Arg-Pro-Arg, corresponding to positions 17 to 22 of r-NMU, may be essential for contractile activity. N-terminal peptide segments Try-Gln-Gly-Pro corresponding to positions 6 to 9, and Ser-Gly-Gly corresponding to positions 13 to 15, appear to be of special importance for potent activity. |
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ISSN: | 0009-2363 1347-5223 |
DOI: | 10.1248/cpb.39.2016 |