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1 Department of Biomedical
Science,
In canine ileum we
investigated the distribution of pituitary adenylate cyclase-activating
peptide (PACAP), using immunofluorescence and radioimmunoassay and the
binding of 125I-PACAP-27 to
membranes. Nerve profiles immunoreactive to PACAP-27, and often to
vasoactive intestinal polypeptide (VIP) as well, were found in all
plexi, but PACAP was present in ~100-fold lesser amounts than VIP.
High-performance liquid chromatography analysis of deep muscular plexus
(DMP) synaptosomes suggested the presence of PACAP-38, PACAP-27, and a
third unidentified molecular form. High- and low-affinity
125I-PACAP-27 binding sites were
found in DMP synaptosomes and circular smooth muscle (CM) plasma
membranes. In competition studies with DMP membranes, high (H)- and low
(L)-affinity dissociation constants (Kd) and
maximal binding capacities
(Bmax) were as follows:
Kd H = 66.9 pM, Bmax H = 101 fmol/mg;
Kd L = 2.18 nM, Bmax L = 580 fmol/mg
protein. The binding of
125I-PACAP-27 was fast.
Dissociation was slow and incomplete in the presence of unlabeled
PACAP-27 but accelerated by pretreatment with guanosine
5'-O-(3-thiotriphosphate)
(GTP
S). GTP
S or cholera toxin treatment eliminated high-affinity
binding in both membranes. VIP had ~100-fold lower affinity than
PACAP-27 in both membranes. Cross-linking studies identified an
~70-kDa PACAP receptor in each membrane. Thus PACAP coexists with VIP
in ileal enteric nerves and acts on PACAP-preferring, possibly
Gs-coupled, receptors in DMP
synaptosomes and CM membranes.
pituitary adenylate cyclase-activating peptide; PACAP-27; PACAP-38; vasoactive intestinal polypeptide; synaptosome; smooth muscle; intestine
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