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Vol. 301, Issue 2, 643-650, May 2002
Eli Lilly and Company, Neuroscience Research, Lilly Corporate
Center, Indianapolis, Indiana
Muscarinic receptors play a major role in gallbladder function,
although the muscarinic receptor(s) mediating smooth muscle contractility is unclear. This study compared smooth muscle contractile responses to carbamylcholine (10
7-103 M) in
isolated gallbladder from wild-type and M2, M3,
and M4 receptor knockout mice. Carbamylcholine-induced
contraction in gallbladder was associated with tachyphylaxis and the
release of a cyclooxygenase product because indomethacin
(106 M) inhibited carbamylcholine-induced contraction.
The M3 receptor was the major muscarinic receptor involved
in contraction because carbamylcholine-induced contractility was
inhibited in gallbladder from M3 receptor knockout mice.
Furthermore, the muscarinic receptor antagonists
11-[[[2-diethylamino-O-methyl]-1-piperidinyl]acetyl]-5,11-dihydrol-6H-pyridol[2,3-b][1,4]benzodiazepine-6-one (AF-DX 116) and pirenzepine dextrally shifted contraction to
carbamylcholine in gallbladder from wild-type, M2, and
M4 receptor knockout mice, with affinities consistent with
M3 receptor interaction. In addition, maximal contraction
to carbamylcholine was reduced in gallbladder from M2
receptor knockout mice and affinities for AF-DX 116 and pirenzepine in
gallbladder from M3 receptor knockout mice were consistent
with their affinities at M2 receptors. In M4
receptor knockout mice, contraction to carbamylcholine was dextrally
shifted, although the affinities for AF-DX 116 and pirenzepine in
gallbladder from M2 or M3 knockout mice were
not similar to their affinities at M4 receptors. The
M4 receptor may serve as an accessory protein necessary for
optimal potency of M2 and M3 receptor-mediated
responses. Thus, muscarinic receptor knockout mice provided direct and
unambiguous evidence that M3, and to a lesser extent,
M2 receptors are the predominant muscarinic receptors
mediating gallbladder contractility, and M4 receptors
appear necessary for optimal potency of carbamylcholine in gallbladder contraction.
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