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1 ressive decrease in the apparent affinity of oxotremorine-M).
2 entiation of AMPK phosphorylation induced by oxotremorine-M.
3 nhibitor dephostatin prevented inhibition by oxotremorine-M.
4 gnificantly reduced the inhibitory effect of oxotremorine-M.
5 of N-[(3)H]methylscopolamine by the agonist oxotremorine-M.
6 in combination with the M2 receptor agonist oxotremorine-M.
8 efore compared the effects of bradykinin and oxotremorine-M (a muscarinic agonist) on membrane PIP(2)
13 st (quinuclidinyl benzilate) and an agonist (oxotremorine-M) at sites on human m(1)-, m(2)-, m(3)-, a
14 eta-Acetoxynortropane had K(i) values versus oxotremorine-M binding at m(1)-, m(2)-, and m(4)-recepto
15 and oxotremorine, had higher affinity versus oxotremorine-M binding compared to quinuclidinyl benzila
16 loxy(nor)tropanes had higher affinity versus oxotremorine-M binding compared to quinuclidinyl benzila
18 At low concentrations (e.g. 0.1-1 microM oxotremorine-M), 'burst-mode' activity comprised regular
19 arter of the reduction in PIP(2) produced by oxotremorine-M, but equal reduction when PIP(2) synthesi
20 M4 subtype-preferring antagonist himbacine, oxotremorine-M caused a large increase in the sIPSC freq
21 prised to find that in M2/M4 double-KO mice, oxotremorine-M consistently increased the frequency of s
22 In wild-type mice, mAChR activation with oxotremorine-M decreased the amplitude of monosynaptic E
26 4129 did not block the stimulatory effect of oxotremorine-M in the majority of neurons from WT mice.
33 blocked the nonselective muscarinic agonist oxotremorine-M-induced increases in neuronal firing rate
35 mice, but not M(2)- or M(4)-single KO mice, oxotremorine-M inhibited sEPSCs in significantly fewer n
36 ed with anti-CD3/CD28/CD2 in the presence of oxotremorine-M (M1R-M5R agonist), atropine (M1R-M5R anta
37 ent with the nonselective muscarinic agonist oxotremorine-M, M2, and M4 receptors underwent significa
38 , the inhibitory and potentiating effects of oxotremorine-M on EPSCs in M3 single-KO and M1/M3 double
39 moting effect of Muscarinic receptor agonist oxotremorine-M on insulin secretion in cultured mouse is
45 e either attenuated the inhibitory effect of oxotremorine-M or potentiated the stimulatory effect of
47 ensitive to 100 microm Cd(2+) and 2.5 microm oxotremorine M (oxo-M), a muscarinic agonist, and fully
49 r hyperpolarized by the cholinergic agonists oxotremorine-M (Oxo-M) and carbachol (CCh), and that mAC
50 ave demonstrated that the muscarinic agonist oxotremorine-m (oxo-m) blocks the induction of presynapt
51 nts were modulated by the muscarinic agonist oxotremorine-M (oxo-M) in a manner having all of the cha
52 rinic acetylcholine receptor (mAChR) agonist oxotremorine-M (Oxo-M) in dissociated vestibular ganglio
53 bation of cells with the cholinergic agonist oxotremorine-M (Oxo-M) induced an approximately 6-fold i
54 Effects of a muscarinic receptor agonist oxotremorine-M (oxo-M) on bladder afferent nerve (BAN) a
55 Stimulation of M1 receptors by 10 microM oxotremorine-M (Oxo-M) strongly reduced (to 0-10%) curre
56 behavioral responsiveness to challenge with oxotremorine-M (Oxo-M), a nonselective muscarinic acetyl
62 c receptors were stimulated with the agonist oxotremorine-M, several previously described currents we
65 acetylcholine receptors (i.e. application of oxotremorine M to PTX-treated neurons) failed to elicit
66 inositol metabolism, but mutant A212E caused oxotremorine-M to become a weak partial agonist compared
67 y blocked the binding of [(3)H]NMS and [(3)H]oxotremorine-M to M2 receptors with Hill coefficients ne
68 ial Bax accumulation, also was attenuated by oxotremorine-M treatment after treatment with H(2)O(2) o
71 gonists, acetylcholine (ACh), carbachol, and oxotremorine-M, while significantly increasing the maxim