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Rat Atrial Natriuretic Polypeptide Increases Net Water, Sodium and Chloride Absorption Across Rat Small Intestine In Vivo
Japan. J . Pharmacol. 4 5 , 7 - 1 3 ( 1 9 8 7 )
7
Rat Atrial Natriuretic Polypeptide Increases Net Water, Sodium and Chloride Absorption Across Rat Small Intestine In Vivo Yasushi K A N A I , Norio 0 H N U M A and Hisayuki
MATSUO*
Suntory Institute for Biomedical Research, S h i m a m o t o , M i s h i m a , Osaka 618, Japan ' D e p a r t m e n t of Biochemistry, Miyazaki Medical College, Kiyotake, Miyazaki 8 8 9 - 1 6 , Japan Accepted May 13, 1987
A b s t r a c t — L o c a l i z a t i o n o f b i n d i n g sites f o r s y n t h e t i c rat atrial n a t r i u r e t i c (a-rANP) vivo
perfused
demonstrated base
of
polypeptide
and t h e effect of the peptide on net w a t e r and electrolyte m o v e m e n t small
intestine
that specific
epithelia
and
of
the
binding
lamina
rat
were
sites w e r e
propria
of the
studied.
Autoradiographic
localized small
on
a space
intestine.
between
Alpha-rANP
/ ¿ g / m i n ) i n f u s e d i n t o t h e s u p e r i o r m e s e n t e r i c artery of rats increased net of w a t e r (70%
( 4 6 % i n c r e a s e in c o m p a r i s o n w i t h c o n t r o l s ) ,
increase)
These
across the small
increases
employed.
were
also
T h u s it w o u l d
intestinal tract
observed
when
circulating
glucose-free
water-electrolyte
Ringer's
Ringer's
Na-glucose
and
through
solution
cotransport
regulating
not
CI
solution. was
system
These observations suggest that
balance
the (0.25
absorption
( 8 4 % increase)
perfused w i t h
be c o n c l u d e d t h a t t h e
is n o t i n v o l v e d i n t h e a c t i o n o f a - r A N P . controls
Na
in
study
a-rANP
only
renal
f u n c t i o n b u t a l s o i n t e s t i n a l w a t e r , N a a n d CI a b s o r p t i o n .
Atrial seses
natriuretic
potent
polypeptide
diuretic
and
(ANP)
pos-
Dawley
natriuretic
acti-
[
vities ( 1 - 3 ) . Koseki et al. ( 4 , 5) h a v e that in
specific the
lecting
as
the
small
on
of
inner
and
Furthermore,
localized
the
sites
glomerulus, tubule
kidneys. were
binding
ANP
extra-renal
intestine,
heart, liver a n d brain In
this
study,
localization [
1 2 5
of
l]a-rANP
we
have
in t h e
39
at 4
min
following
col-
tion.
For
whole
rat
cording
ug
to
of
a-rANP
and
intravenous
body
50
jum
lung,
Japan)
eye,
effects
investigated
binding
f o r 4 w e e k s at 4 ° C . For
autoradiography,
10
jum
semi-micro
frozen
sites
perfused
the
room
for
apposed
temperature.
the
microscopic
rat
These
sections
tighly to the X-ray
the
films.
autoradiography,
the
the
To
complete
dissected
organs
the
a-rANP
lactoperoxidase
was
sists a-rANP:
radioiodinated
method
as
by
described
previously ( 4 ) . The specific activity of
[
1 2 5
l]-
studies:
9
mM
91
mM
picric 16
Na HP0 2
mM 4
( p H 7.2)
20
NaH P0 2
12H 0.
sections were washed saline
acid,
2
in
Ten
4
were
solution fixation
were
kept
which
con-
mg/l
para-
2H 0 2
um
Male
Sprague-
and
frozen
phosphate-buffered
and dipped into the
nuclear
track emulsion ( N T B - 2 , Kodack, U.S.A.)
a - r A N P w a s 0.65 mCi//¿g. Autoradiographic
of
formaldehyde,
light
rats
the
f o r 2 4 hr in Z a m b o n i ' s s o l u t i o n Methods
were
For
1 0 0 ml of Z a m b o n i ' s
aorta.
process,
monoiodinated
sections
w e r e m o u n t e d o n t o glass slides a n d d r i e d at
small intestine.
Synthetic
ac-
freeze-dried
s e c t i o n s w e r e p r e p a r e d a n d p l a c e d in c o n t a c t
perfused w i t h
of
sacrificed administra-
autoradiography,
(7),
of
w i t h X - r a y f i l m s ( N o . 1 5 0 , Fuji F i l m C o . , L t d . ,
via
Materials and
ng
sites
movement
Preparation
39
combination
such
clarified.
in v i v o
given
organs
small intestine and
applying
cold
Ullberg
effect of a - r A N P on net w a t e r and electrolyte by
were
binding
adrenal,
specific
g)
either a l o n e or in
with
of
(6), while A N P
in t h e s e o r g a n s are n o t y e t
(350
were
medullary recta
rats
l]a-rANP
shown
a-rANP
vasa
1 2 5
and
exposed for 2 weeks. After the sections were
Copyright 1987. Production and Hosting by Elseiver B.V. On behalf of Japanese Pharmacological Society. This is an open access article under the CC BY-NC-ND License (http://creativecommons.org/licenses/by-nc-nd/ ).
8
Y. Kanai, Ν. Ohnuma & Η. Matsuo
developed and fixed, they were stained haematoxylin-eosin and Small
intestine
performed small
the
Seeber
of et
Dawley
with
al.(9).
rats
weighing i.p.)
performed. After and
distal
small
end
intestine
of
a
ileum.
perfused
peristatic
pump
for
10
min
solution
contained
K C l , 1.4
mM
ml,
specific
solution
activity
was of
3.4
MgCI ,
5
2
mM mM
(10,000 d p m /
at
the
peristatic Sweden). at
was
37°C.
measured (Model
LS-7500,
and
Beckman,
U.S.A.).
Na
concentrations were determined flame
photometer
Japan).
CI
was
titration
(Model
750,
measured
by
/¿moles/min/m intestine.
using
of
Positive
absorption
and
secretion. All mean±S.E.
a
Hitachi, Potentio
chloridimeter
Hiranuma, Japan). the
expressed length
of
numbers negative
results w e r e Statistical
Κ
b y use of a
Water
as ß\ the
represent
net
numbers, expressed
analysis
or
small net
as
the
was
per-
f o r m e d by S t u d e n t ' s r-test.
mCi/mmol, the
osmotic
Localization [
1 2 5
of
l]a-rANP:
specific
When
binding
rats w e r e
sites
given
39
for ng
of [
( M o d e l 3 W 2 , A d v a n c e d Instruments, U.S.A.).
at 4
The
localized on the kidney and the lung (Fig. 1 ) .
mesenteric
nulated from the femoral
275
Results
Ringer's
replacing
mosmol/l
superior
was
col
a
by a liquid scintillation spectrometer
and electrolyte flux w a s
D-mannitol. The
perfusate
samples
ml/min,
11.4 by
in t h e
(Chloride counter,
Ringer's
infused
maintained
metrie
P-1,
was
Pharmacia,
was
washed
Glucose-free
prepared
P-3,
temperature
circulation
/¿g/min w i t h
warmed
NaCI,
C-inulin
England).
glucose w i t h 5 m M pressure
1 4
a-rANP
/¿I/0.25
Radioactivity
the this
The
The
mM
2
(Model
in
confirmed. Through
with
effluent w a s
mM
C a C I , 0.1
g l u c o s e a n d 6 0 juM Amersham,
137
or
Body
tubes
(Model
periods.
saline
pump
duodenum
at t h e rate of 0.5
Pharmacia, S w e d e n ) . The lected
the
tube,
the
was
blood
intestine w a s
and were
of bile d u c t ,
normal
small
25
pentobarbital
both
the
was
Ringer's solution by using
into
g
operation,
rate of
rat
Sprague-
tracheotomy
ligation
cannulated
male
200-300 a
of
et al. ( 8 )
sodium and
We
of
modification
Fasting
with
mg/kg,
were
a
studies:
experiment
Dharmsathphorn
anesthetized (50
perfusion
perfusion
intestine
methods
with
photographed.
artery
was
artery w i t h
tubes (Clay Adams, U.S.A).
can PE-10
Completing
this
Lu^,
ZMk'!
On
1 2 5
l]a-rANP
min, the
shown
high
other in t h e
intravenously and density organs,
small
sacrificed
radioactivities radioactivities
intestine,
liver,
were were
adrenal,
A k
J?
Fig. 1 . Whole body autoradiography of the rat given 39 ng of [ l ] a - r A N P intravenously. The animal was sacrificed at 4 min after injection. Ey, eye; Lu, l u n g ; En, endocardium; Li, liver; S, small intestine; A , adrenal; K, kidney. 1 2 5
Effect of A N P in Small Intestine
9
Fig. 2. Semi-micro autoradiography of the small intestine f r o m rat given 39 ng of [ l ] a - r A N P either alone (A) or in combination w i t h 39 /¿g of cold or-rANP ( B ) . The animal was sacrificed at 4 min after injection. Microautoradiogram superimposed on a histological image of the small intestine from a rat given 39 ng [ l ] a - r A N P ( C ) . 1 2 5
1 2 5
e n d o c a r d i u m and eye ball.
and D ) .
To determine whether the small 39
intestine
ng
of
[
was
specific
l]a-rANP
1 2 5
binding or
was
in
the
nonspecific,
injected
either
a l o n e ( F i g . 2 , A a n d C ) or in c o m b i n a t i o n 39
/ig
of
cold
grains w e r e 2A)
a-rANP
observed
and were
along
displaced
a-rANP
(Fig.
obtained
autoradiogram
histological were
(Fig.
2B).
image
distributed
the
with
Figure
of
on
2B). villus
an
of
electrolyte
2C
shows
superimposed
the
the
villus. The
space
a-rANP
on
movement:
i n t e s t i n e o f rats w a s
(Fig.
excess on
net
When
and
the
small Ringer's
s o l u t i o n in v i v o , t h e r e w a s n e t w a t e r a b s o r p tion
across
absorption
the was
small nearly
intestine constant
and
from
solution,
(126±7
of
(60-180
min
W h e n the
small
perfused
with
rats w e r e a-rANP
(0.25
/¿g/min)
with in
to
a
statistical
comparison 183±8
significance
with
the
//l/min/m).
controls
Significant
increases w e r e also o b s e r v e d
in n e t
absorp-
tion
70%
increase,
of
Na and
CI
(84% and
respectively). The net m o v e m e n t of Κ across the intestinal tract c h a n g e d f r o m secretion to a b s o r p t i o n ; h o w e v e r , t h e d i f f e r e n c e in n e t Κ flux
was
only
1/40-1/44
of that
observed
in N a a n d C I .
this
When
to
modified
60
state
c a u s e d a 4 6 % i n c r e a s e in t h e m e a n n e t w a t e r (P<0.01)
propria.
perfused w i t h
tracts
Ringer's
absorption
a
steady
(Table 1).
intestinal
an
the
water
at t h e
of the perfusion)
of
grains
between
base of t h e epithelia a n d t h e lamina Effects
with Dense
M e a n n e t f l u x e s o f w a t e r , N a a n d CI w e r e calculated
the
intestine
was
perfused
R i n g e r ' s s o l u t i o n , in w h i c h
with
a
glucose
1 8 0 m i n a f t e r t h e s t a r t o f p e r f u s i o n in c o n t r o l
was
animals that
w a t e r absorption w a s l o w e r e d to 5 3 % of that
received
saline
(Fig. 3A,
open
c i r c l e ) . I n c r e a s e in n e t w a t e r f l u x a c r o s s intestinal tract w a s d e m o n s t r a t e d w h e n /¿g/min
of
a-rANP
superior
mesenteric
the
from
displaced the
with
original
D-mannitol,
Ringer's
change was
also n o t e d
the
under these
conditions, w h e n
was
infused
into
artery
during
perfusion
( F i g . 3 A , c l o s e d c i r c l e ) . I n c r e a s e s in t h e
net
infused, significant
compared
5 7 % increase, respectively).
When with
the
modified
glucose
was
small
controls
( F i g . 3,
intestine
Ringer's displaced
was
solution with
B-D).
net
Similar
CI.
Even
α-rANP
was
observed
i n t h e n e t a b s o r p t i o n o f w a t e r , N a a n d CI as compared
the
Na and
increases w e r e
f l u x e s o f N a , Κ a n d CI w e r e a l s o o b s e r v e d as with
solution.
0.25
in
basal
to
the
controls
(47%,
85%
and
perfused in
Discussion
which
D-mannitol,
after 6 0 m i n , α - r A N P t e n d e d t o increase n e t f l u x e s o f w a t e r , N a a n d CI ( F i g . 4 , A ,
the Β
It h a s b e e n d e m o n s t r a t e d t h a t
autoradio
graphy provides a useful tool to identify distribution
of A N P
receptors
in t h e
the
kidney
10
Y. Kanai, Ν. Ohnuma & H. Matsuo 220·
24-
ç165E ö χ 3 Li ra ζ
LU
<
12·
I
=> 110-
55"
6-
LJ Ζ
Ζ 60
120
0-
180
0
PERFUSION TIME (min)
1
1
60
120
—ι 180
PERFUSION TIME (min]
0.4-
30-
1 I
ε 1 20Ε
0.2¬
1
χ
χ 3
10-
ZD •-0.2-
r ~T— 120
-1— 60
—1 180
-r— 60
PERFUSION TIME (min)
120
180
PERFUSION TIME (min)
Fig. 3. Time course of net water ( A ) , Na ( Β ) . Κ (C) and CI ( D ) flux across the w a l l of rat intestinal tracts perfused w i t h Ringer's solution. A l p h a - r A N P ( # ) or saline ( O ) (0.25 ¿¿g/25 μ Ι / m i n ) was infused into the superior mesenteric artery during the perfusion of the small intestine. Each point represents the mean±S.E. of 6 determinations. (4-6,
1 0 ) , brain
other organs
( 1 1 , 1 2 ) , eye
( 6 ) . It h a s b e e n
(6, 11) also
t h a t t h e r e c e p t o r s f o r A N P e x i s t in t h e lateral
membranes
cortex
(13)
and
isolated
vascular
Our autoradiographic between
the
base
from
rat
systems
and
reported basokidney
(14-16).
study w a s of the
of
the
epithelia
area
and
the
o b s e r v e d specific b i n d i n g has n o t been characterized, receptors
are
they
suggest
that
present
in t h e
small
a n d m a y p l a y a role in w a t e r a n d
intestine electrolyte
h a n d l i n g in t h e s m a l l i n t e s t i n e . In
the
α-rANP
present
study,
0.25
/¿g/min
infused into the superior
lamina propria (Figs. 1 and 2 ) . H o w e v e r , the
artery increased net absorption of w a t e r , and
resolution for determining sites
for
α-rANP
membrane laries
in
of
the
exist
the lamina
had
insufficient
if s p e c i f i c in
epithelia propria.
the or
binding
CI
with
across
Ringer's
the
small
solution
intestine
in v i v o . T h e
mecha
nisms by w h i c h α - r A N P increased w a t e r
the
solute
Although
the
absorption
in t h e
small
intestine
u n k n o w n at p r e s e n t . H o w e v e r , t h e
Na
perfused
basolateral capil
of
mesenteric
obtained
autoradiogram
well
a-rANP
and are
following
11
Effect of A N P in Small Intestine 22024 165-
18-
Q 12 Ε
110'
=5
Ft
55 •
6
τ
0—J— 60
I 120
- 1 — —Γ 120 60 PERFUSION TIME (min) -
180
PERFUSION TIME (min)
180
30-
0.4 π
0.2·
20-
o 10-
χ
¥
LU
2
- ι — 120
~"r~~ 60
o -
180
"Ί 180
120
60
PERFUSION TIME (min)
PERFUSION TIME (min)
Fig. 4. Time course of net water ( A ) , Na ( Β ) , Κ (C) and CI (D) flux across the w a l l of rat intestinal tracts perfused w i t h glucose-free Ringer's solution. A l p h a - r A N P ( • ) or saline ( • ) (0.25 /¿g/25 /¿l/min) w a s infused into the superior mesenteric artery during perfusion of the small intestine. Each point represents the mean±S.E. of 6 determinations.
three possibilities deserve t o be c o n s i d e r e d : 1 )
fluid
α-rANP,
capillaries,
p r e s e n c e or a b s e n c e
acting
on
might increase w a t e r , by
decreasing
pressure
which
submucosal Na and
Ci
intracapillary regulates
paracellular
fluid
through
the
shunt
α-rANP
m i g h t stimulate active Na
on
Na-K-ATPase
activity
observed
in e i t h e r
of glucose to the
the
same
absorption
e x t e n t , it is l i k e l y t h a t t h e N a - g l u c o s e p o r t s y s t e m is n o t i n v o l v e d i n t h e
absorption
o f f l u i d a b s o r p t i o n b y α - r A N P . In v i e w o f t h e
pathway.
3)
2)
transport. because
has n o
(17).
was
hydrostatic
H o w e v e r , t h i s p o s s i b i l i t y is u n l i k e l y it h a s b e e n r e p o r t e d t h a t A N P
absorption
effect
a-rANP
cotrans-
stimulation
general effect of A N P o n the vascular system (14-16), Our effect
the
first
finding expected
possibility
is s e e m i n g l y from
of A N P . Recently,
the
is m o s t contrary
natriuretic
Seeber et al. ( 9 )
likely. to
the
action reported
m i g h t i n c r e a s e t h e e n t r y o f N a a n d CI a c r o s s
t h a t rat atrial e x t r a c t s u p r e s s e d t h e N a - g l u c o s e
the brushborder
c o t r a n s p o r t across t h e rat
membrane. Since
enhanced
intestine
perfused
12
Y. Kanai, N. Ohnuma & H. Matsuo Table 1 .
Effect of α - r A N P on net fluxes of water, Na, Κ and CI across the rat small intestine Water (μΙ/min/m)
Na (¿¿nnoles/min/m)
(/¿moles/min/m)
(//moles/min/m)
126±7
11.0±1.7
-0.029±0.043
14.7±1.8
183±8**
20.2±1.8**
CI
Ringer's solution control (n = 6) α-rANP (n = 6)
0.259±0.077**
24.9*1.7"
Glucose free Ringer's solution control (n=6) a-rANP (n=6)
6.4±1.2
-0.009±0.038
9.7±1.2
11.9±1.5*
-0.024±0.087
15.2±1.1**
66±7 97±3**
A l p h a - r A N P (0.25 /¿g/25 μΙ/rnin) or saline was infused through the superior mesenteric artery. Glucosefree Ringer's solution contains D-mannitol instead of glucose. Net absorption of water, Na, Κ and CI was calculated from the data (from 60 min to 180 min) in Figs. 3 and 4. Each value represents the mean±S.E. Significant difference from the controls, P < 0 . 0 5 ( * ) , P < 0 . 0 1 ( * * ) .
in
vivo.
However,
this
work
evaluate for the f o l l o w i n g used
crude
extract
is
difficult
reasons:
instead
of
1)
to
They
synthetic
a-
r A N P , w h i c h h a s b e e n i d e n t i f i e d as t h e n a t i v e circulating
ANP
in rats
( 1 8 ) . 2)
In v i e w
of
t h e e x t r e m e l y s h o r t b i o l o g i c a l half life o f A N P in t h e rat ( t
1 / 2
= 26.5 sec)
(19), the
duration
of c o l l e c t i o n period seems to be t o o
long to
detect the acute effect of A N P . O'Grady peptin
et al.
III
(20)
inhibited
reported
Na-K-2CI
that
cotransport
in s h o r t c i r c u l a t e d t e l e o s t i n t e s t i n e . it
is q u e s t i o n a b l e
plicable
to
whether
mammals.
It
this
has
atrio-
However,
is a l s o
been
ap
reported
i n r a b b i t s t h a t A N P d i d n o t a f f e c t CI t r a n s p o r t across the thick loop,
where
ascending
Na-K-2CI
limb
of
Henle's
cotransport
is
also
operating (21 ). Since
we
administered
α-rANP
directly
i n t o t h e m e s e n t e r i c a r t e r y , it is p o s s i b l e
that
the
this
vascular
maneuver.
effect
is
Although
exaggerated our
by
autoradiographic
study s h o w e d that the specific binding for
α-rANP
between lamina
were
the
base
localized of
propria, w e
the
on
the
epithelia
sites space
and
the
can not exclude a possi
bility that A N P directly acts, on the epithelia, leading
to
a
different
the experimental Our
observations
that A N P intestine
result
depending
reported
here
suggest
has a d i s t i n c t t a r g e t o n t h e and
on
conditions.
may
modulate
fluid
balance, although the underlying
and
small salt
mechanisms
which
a c c o u n t for the action of α - r A N P
on
the small intestine remain t o be e l u c i d a t e d . A c k n o w l e d g m e n t s : We are grateful to Y. Minami¬ take and Y. Hayashi (Suntory Institute for B i o medical Research) for providing synthetic a - r A N P and [ l ] a - r A N P . We also thank Dr. M . Imai of the National Cardiovascular Center Research Institute for reviewing this article. 1 2 5
References 1 Kangawa, K. and Matsuo, H.: Purification and complete amino acid sequence of α - h u m a n atrial natriuretic polypeptide (a-hANP). Biochem. Biophys. Res. C o m m u n . 1 1 8 , 1 3 1 - 1 3 9 (1984) 2 Yukimura, T., Ito, K., Takenaga, T., Yamamoto, K., Kangawa, K. and Matsuo, H.: Renal effects of a synthetic α - h u m a n atrial natriuretic poly peptide ( a - h A N P ) in anesthetized dogs. Eur. J . Pharmacol. 103, 3 6 3 - 3 6 6 ( 1 9 8 4 ) 3 Ishihara, T., Aisaka, K., Hattori, Y., Hamasaki, S., Morita, M., N o g u c h i , T., Kangawa, K. and Matsuo, H.: Vasodilatory and diuretic actions of α-human atrial natriuretic polypeptide (ah A N P ) . Life Sei. 36, 1 2 0 5 - 1 21 5 (1 985) 4 Koseki, C , Hayashi, Y., Torikai, S., Furuya, M., O h n u m a , N. and Imai, M.: Localization of binding sites for α-rat atrial natriuretic polypeptide in rat kidney. A m . J . Physiol. 2 5 0 , F 2 1 0 - F 2 1 6 (1986) 5 Koseki, C , Kanai, Y., Hayashi, Y., O h n u m a , N. and Imai, M.: Intrarenal localization for α-rat atrial natriuretic polypeptide: A n autoradio graphic study w i t h [ 1 ] - labeled ligand injected in vivo into the rat aorta. Japan. J . Pharmacol. 42, 2 7 - 3 3 (1986) 1 2 5
Effect of A N P in Small Intestine 6 Bianchi, C , G u t k o w s k a , J . , Thibault, G., Garcia, R., Genest, J . and Cantin, M.: Radioautographic localization of [ i] - atria I natriuretic factor ( A N F ) in rat tissues. Histochemistry 8 2 , 4 4 1 - 4 5 2 (1985) 1 2 5
7 Uliberg, S.: The technique of w h o l e body auto radiography. Cryosectioning of large specimens. Sei. Tools (special issue on w h o l e body auto radiography), 2 - 2 8 (1977) 8 Dharmsathaphorn, K., Sherwin, R.S. and Dobbins, J.W.: Somatostatin inhibits fluid secretion in the rat j e j u n u m . Gastroenterology 78, 1 5 5 4 - 1 5 5 8 ( 1 9 8 0 ) 9 Seeber, M., Vidal, N.A., Carchio, S . M . and Karara, A.L.: Inhibition of water-sodium absorption by an atrial extract. Can. J . Physiol. Pharmacol. 64, 2 4 4 - 2 4 7 ( 1 9 8 6 ) 10 M u r p h y , K.M.M., M c L a u g h l i n , L.L., Michener, M.L. and Needlemann, P.: Autoradiographic localization of atriopeptin III receptors in rat kidney. Eur. J . Pharmacol. 1 1 1 , 2 9 1 - 2 9 2 ( 1 9 8 4 ) 11 Quirion, R., Dalpe, M., De Lean, Α., G u t k o w s k a , J . , Cantin, M . and Genest, J . : Atrial natriuretic factor ( A N F ) binding sites in brain and related structures. Peptides 5, 1 1 6 7 - 1 1 7 2 ( 1 9 8 4 ) 12 Quirion, R., Dalpe, M. and D a w , T.V.: Character ization and distribution of receptor for the atrial natriuretic peptides in mammalian brain. Proc. Natl. A c a d . Sei. U.S.A. 8 3 , 1 7 4 - 1 7 8 (1986) 13 Hori, R., Inui, K., Saito, H., M a t s u k a w a , Y., Okumura, K., Nakao, K., M o r i i , N. and Imura, H.: Specific receptors for atrial natriuretic poly peptide on basolateral membranes isolated from rat renal cortex. Biochem. Biophys. Res. C o m m u n . 129, 7 7 3 - 7 7 9 ( 1 9 8 5 ) 14 Napier, M.A., Vandlen, R.L., Schonberg, G.A., Nutt, R.F., Brady, S., Lyte, T., Winquist, R., Faison, E.P., Heinel, L.A. and Blaine, E.H.:
Ί3
Specific membrane receptors for atrial natriuretic factor in renal and vascular tissues. Proc. Natl. A c a d . Sei. U.S.A. 8 1 , 5 9 4 6 - 5 9 5 0 ( 1 9 8 4 ) 15 Shenk, D.B., J o h n s o n , L.K., Schwartz, K., Sista, H., Scarborough, R.M. and Lewichi, J.Α.: Distinct atrial natriuretic factor sites on cultured bovine aortic smooth muscle and endothelial cells. Biochem. Biophys. Res. C o m m u n . 127, 4 3 3 - 4 4 2 (1985) 1 6 Hirata, Y., Tomita, M., Yoshimi, H. and Ikeda, M.: Specific receptors for atrial natriuretic factor ( A N F ) in cultured vascular smooth muscle cells of rat aorta. Biochem. Biophys. Res. C o m m u n . 125, 5 6 2 - 5 6 8 ( 1 9 8 4 ) 17 Thibault, G., Garcia, R., Cantin, M . and Genest, J . : Atrial natriuretic factor characterization and partial purification. Hypertension 5, Supp I, I7 5 - I - 8 0 (1983) 18 Miyata, Α., Kangawa, K., Toshimori, T., Hattoh, T. and Matsuo, H.: Molecular forms of atrial natriuretic polypeptides in mammalian tissues and plasma. Biochem. Biophys. Res. C o m m u n . 129, 2 4 8 - 2 5 5 (1985) 19 Friedrich, C.L., Rudorf, E.L., George, R.A., Heikki, R., Miklos* T., Detlev, G.R., Bernd, S. and Thomas, U.: Atriopeptin III kinetics and pharmacodynamics in normal and anephric rats. J . Pharmacol. Exp. Ther. 2 3 6 , 41 6 - 4 1 8 (1 985) 20 O'Grady, S.M., Field, M., Nash, N.T. and Rao, M.C.: Atrial natriuretic factor inhibits Na-K-Cl cotransport in teleost intestine. A m . J . Physiol. 2 4 9 , C 5 3 1 - C 5 3 4 (1985) 21 Kondo, Y., Imai, M., Kangawa, K. and Matsuo, H.: Lack of direct action of α - h u m a n atrial natriure tic polypeptide on the in vitro perfused segments of Henle's loop isolated from rabbit kidney. Pflugers A r c h . 4 0 6 , 2 7 3 - 2 7 8 ( 1 9 8 6 )
7
Rat Atrial Natriuretic Polypeptide Increases Net Water, Sodium and Chloride Absorption Across Rat Small Intestine In Vivo Yasushi K A N A I , Norio 0 H N U M A and Hisayuki
MATSUO*
Suntory Institute for Biomedical Research, S h i m a m o t o , M i s h i m a , Osaka 618, Japan ' D e p a r t m e n t of Biochemistry, Miyazaki Medical College, Kiyotake, Miyazaki 8 8 9 - 1 6 , Japan Accepted May 13, 1987
A b s t r a c t — L o c a l i z a t i o n o f b i n d i n g sites f o r s y n t h e t i c rat atrial n a t r i u r e t i c (a-rANP) vivo
perfused
demonstrated base
of
polypeptide
and t h e effect of the peptide on net w a t e r and electrolyte m o v e m e n t small
intestine
that specific
epithelia
and
of
the
binding
lamina
rat
were
sites w e r e
propria
of the
studied.
Autoradiographic
localized small
on
a space
intestine.
between
Alpha-rANP
/ ¿ g / m i n ) i n f u s e d i n t o t h e s u p e r i o r m e s e n t e r i c artery of rats increased net of w a t e r (70%
( 4 6 % i n c r e a s e in c o m p a r i s o n w i t h c o n t r o l s ) ,
increase)
These
across the small
increases
employed.
were
also
T h u s it w o u l d
intestinal tract
observed
when
circulating
glucose-free
water-electrolyte
Ringer's
Ringer's
Na-glucose
and
through
solution
cotransport
regulating
not
CI
solution. was
system
These observations suggest that
balance
the (0.25
absorption
( 8 4 % increase)
perfused w i t h
be c o n c l u d e d t h a t t h e
is n o t i n v o l v e d i n t h e a c t i o n o f a - r A N P . controls
Na
in
study
a-rANP
only
renal
f u n c t i o n b u t a l s o i n t e s t i n a l w a t e r , N a a n d CI a b s o r p t i o n .
Atrial seses
natriuretic
potent
polypeptide
diuretic
and
(ANP)
pos-
Dawley
natriuretic
acti-
[
vities ( 1 - 3 ) . Koseki et al. ( 4 , 5) h a v e that in
specific the
lecting
as
the
small
on
of
inner
and
Furthermore,
localized
the
sites
glomerulus, tubule
kidneys. were
binding
ANP
extra-renal
intestine,
heart, liver a n d brain In
this
study,
localization [
1 2 5
of
l]a-rANP
we
have
in t h e
39
at 4
min
following
col-
tion.
For
whole
rat
cording
ug
to
of
a-rANP
and
intravenous
body
50
jum
lung,
Japan)
eye,
effects
investigated
binding
f o r 4 w e e k s at 4 ° C . For
autoradiography,
10
jum
semi-micro
frozen
sites
perfused
the
room
for
apposed
temperature.
the
microscopic
rat
These
sections
tighly to the X-ray
the
films.
autoradiography,
the
the
To
complete
dissected
organs
the
a-rANP
lactoperoxidase
was
sists a-rANP:
radioiodinated
method
as
by
described
previously ( 4 ) . The specific activity of
[
1 2 5
l]-
studies:
9
mM
91
mM
picric 16
Na HP0 2
mM 4
( p H 7.2)
20
NaH P0 2
12H 0.
sections were washed saline
acid,
2
in
Ten
4
were
solution fixation
were
kept
which
con-
mg/l
para-
2H 0 2
um
Male
Sprague-
and
frozen
phosphate-buffered
and dipped into the
nuclear
track emulsion ( N T B - 2 , Kodack, U.S.A.)
a - r A N P w a s 0.65 mCi//¿g. Autoradiographic
of
formaldehyde,
light
rats
the
f o r 2 4 hr in Z a m b o n i ' s s o l u t i o n Methods
were
For
1 0 0 ml of Z a m b o n i ' s
aorta.
process,
monoiodinated
sections
w e r e m o u n t e d o n t o glass slides a n d d r i e d at
small intestine.
Synthetic
ac-
freeze-dried
s e c t i o n s w e r e p r e p a r e d a n d p l a c e d in c o n t a c t
perfused w i t h
of
sacrificed administra-
autoradiography,
(7),
of
w i t h X - r a y f i l m s ( N o . 1 5 0 , Fuji F i l m C o . , L t d . ,
via
Materials and
ng
sites
movement
Preparation
39
combination
such
clarified.
in v i v o
given
organs
small intestine and
applying
cold
Ullberg
effect of a - r A N P on net w a t e r and electrolyte by
were
binding
adrenal,
specific
g)
either a l o n e or in
with
of
(6), while A N P
in t h e s e o r g a n s are n o t y e t
(350
were
medullary recta
rats
l]a-rANP
shown
a-rANP
vasa
1 2 5
and
exposed for 2 weeks. After the sections were
Copyright 1987. Production and Hosting by Elseiver B.V. On behalf of Japanese Pharmacological Society. This is an open access article under the CC BY-NC-ND License (http://creativecommons.org/licenses/by-nc-nd/ ).
8
Y. Kanai, Ν. Ohnuma & Η. Matsuo
developed and fixed, they were stained haematoxylin-eosin and Small
intestine
performed small
the
Seeber
of et
Dawley
with
al.(9).
rats
weighing i.p.)
performed. After and
distal
small
end
intestine
of
a
ileum.
perfused
peristatic
pump
for
10
min
solution
contained
K C l , 1.4
mM
ml,
specific
solution
activity
was of
3.4
MgCI ,
5
2
mM mM
(10,000 d p m /
at
the
peristatic Sweden). at
was
37°C.
measured (Model
LS-7500,
and
Beckman,
U.S.A.).
Na
concentrations were determined flame
photometer
Japan).
CI
was
titration
(Model
750,
measured
by
/¿moles/min/m intestine.
using
of
Positive
absorption
and
secretion. All mean±S.E.
a
Hitachi, Potentio
chloridimeter
Hiranuma, Japan). the
expressed length
of
numbers negative
results w e r e Statistical
Κ
b y use of a
Water
as ß\ the
represent
net
numbers, expressed
analysis
or
small net
as
the
was
per-
f o r m e d by S t u d e n t ' s r-test.
mCi/mmol, the
osmotic
Localization [
1 2 5
of
l]a-rANP:
specific
When
binding
rats w e r e
sites
given
39
for ng
of [
( M o d e l 3 W 2 , A d v a n c e d Instruments, U.S.A.).
at 4
The
localized on the kidney and the lung (Fig. 1 ) .
mesenteric
nulated from the femoral
275
Results
Ringer's
replacing
mosmol/l
superior
was
col
a
by a liquid scintillation spectrometer
and electrolyte flux w a s
D-mannitol. The
perfusate
samples
ml/min,
11.4 by
in t h e
(Chloride counter,
Ringer's
infused
maintained
metrie
P-1,
was
Pharmacia,
was
washed
Glucose-free
prepared
P-3,
temperature
circulation
/¿g/min w i t h
warmed
NaCI,
C-inulin
England).
glucose w i t h 5 m M pressure
1 4
a-rANP
/¿I/0.25
Radioactivity
the this
The
The
mM
2
(Model
in
confirmed. Through
with
effluent w a s
mM
C a C I , 0.1
g l u c o s e a n d 6 0 juM Amersham,
137
or
Body
tubes
(Model
periods.
saline
pump
duodenum
at t h e rate of 0.5
Pharmacia, S w e d e n ) . The lected
the
tube,
the
was
blood
intestine w a s
and were
of bile d u c t ,
normal
small
25
pentobarbital
both
the
was
Ringer's solution by using
into
g
operation,
rate of
rat
Sprague-
tracheotomy
ligation
cannulated
male
200-300 a
of
et al. ( 8 )
sodium and
We
of
modification
Fasting
with
mg/kg,
were
a
studies:
experiment
Dharmsathphorn
anesthetized (50
perfusion
perfusion
intestine
methods
with
photographed.
artery
was
artery w i t h
tubes (Clay Adams, U.S.A).
can PE-10
Completing
this
Lu^,
ZMk'!
On
1 2 5
l]a-rANP
min, the
shown
high
other in t h e
intravenously and density organs,
small
sacrificed
radioactivities radioactivities
intestine,
liver,
were were
adrenal,
A k
J?
Fig. 1 . Whole body autoradiography of the rat given 39 ng of [ l ] a - r A N P intravenously. The animal was sacrificed at 4 min after injection. Ey, eye; Lu, l u n g ; En, endocardium; Li, liver; S, small intestine; A , adrenal; K, kidney. 1 2 5
Effect of A N P in Small Intestine
9
Fig. 2. Semi-micro autoradiography of the small intestine f r o m rat given 39 ng of [ l ] a - r A N P either alone (A) or in combination w i t h 39 /¿g of cold or-rANP ( B ) . The animal was sacrificed at 4 min after injection. Microautoradiogram superimposed on a histological image of the small intestine from a rat given 39 ng [ l ] a - r A N P ( C ) . 1 2 5
1 2 5
e n d o c a r d i u m and eye ball.
and D ) .
To determine whether the small 39
intestine
ng
of
[
was
specific
l]a-rANP
1 2 5
binding or
was
in
the
nonspecific,
injected
either
a l o n e ( F i g . 2 , A a n d C ) or in c o m b i n a t i o n 39
/ig
of
cold
grains w e r e 2A)
a-rANP
observed
and were
along
displaced
a-rANP
(Fig.
obtained
autoradiogram
histological were
(Fig.
2B).
image
distributed
the
with
Figure
of
on
2B). villus
an
of
electrolyte
2C
shows
superimposed
the
the
villus. The
space
a-rANP
on
movement:
i n t e s t i n e o f rats w a s
(Fig.
excess on
net
When
and
the
small Ringer's
s o l u t i o n in v i v o , t h e r e w a s n e t w a t e r a b s o r p tion
across
absorption
the was
small nearly
intestine constant
and
from
solution,
(126±7
of
(60-180
min
W h e n the
small
perfused
with
rats w e r e a-rANP
(0.25
/¿g/min)
with in
to
a
statistical
comparison 183±8
significance
with
the
//l/min/m).
controls
Significant
increases w e r e also o b s e r v e d
in n e t
absorp-
tion
70%
increase,
of
Na and
CI
(84% and
respectively). The net m o v e m e n t of Κ across the intestinal tract c h a n g e d f r o m secretion to a b s o r p t i o n ; h o w e v e r , t h e d i f f e r e n c e in n e t Κ flux
was
only
1/40-1/44
of that
observed
in N a a n d C I .
this
When
to
modified
60
state
c a u s e d a 4 6 % i n c r e a s e in t h e m e a n n e t w a t e r (P<0.01)
propria.
perfused w i t h
tracts
Ringer's
absorption
a
steady
(Table 1).
intestinal
an
the
water
at t h e
of the perfusion)
of
grains
between
base of t h e epithelia a n d t h e lamina Effects
with Dense
M e a n n e t f l u x e s o f w a t e r , N a a n d CI w e r e calculated
the
intestine
was
perfused
R i n g e r ' s s o l u t i o n , in w h i c h
with
a
glucose
1 8 0 m i n a f t e r t h e s t a r t o f p e r f u s i o n in c o n t r o l
was
animals that
w a t e r absorption w a s l o w e r e d to 5 3 % of that
received
saline
(Fig. 3A,
open
c i r c l e ) . I n c r e a s e in n e t w a t e r f l u x a c r o s s intestinal tract w a s d e m o n s t r a t e d w h e n /¿g/min
of
a-rANP
superior
mesenteric
the
from
displaced the
with
original
D-mannitol,
Ringer's
change was
also n o t e d
the
under these
conditions, w h e n
was
infused
into
artery
during
perfusion
( F i g . 3 A , c l o s e d c i r c l e ) . I n c r e a s e s in t h e
net
infused, significant
compared
5 7 % increase, respectively).
When with
the
modified
glucose
was
small
controls
( F i g . 3,
intestine
Ringer's displaced
was
solution with
B-D).
net
Similar
CI.
Even
α-rANP
was
observed
i n t h e n e t a b s o r p t i o n o f w a t e r , N a a n d CI as compared
the
Na and
increases w e r e
f l u x e s o f N a , Κ a n d CI w e r e a l s o o b s e r v e d as with
solution.
0.25
in
basal
to
the
controls
(47%,
85%
and
perfused in
Discussion
which
D-mannitol,
after 6 0 m i n , α - r A N P t e n d e d t o increase n e t f l u x e s o f w a t e r , N a a n d CI ( F i g . 4 , A ,
the Β
It h a s b e e n d e m o n s t r a t e d t h a t
autoradio
graphy provides a useful tool to identify distribution
of A N P
receptors
in t h e
the
kidney
10
Y. Kanai, Ν. Ohnuma & H. Matsuo 220·
24-
ç165E ö χ 3 Li ra ζ
LU
<
12·
I
=> 110-
55"
6-
LJ Ζ
Ζ 60
120
0-
180
0
PERFUSION TIME (min)
1
1
60
120
—ι 180
PERFUSION TIME (min]
0.4-
30-
1 I
ε 1 20Ε
0.2¬
1
χ
χ 3
10-
ZD •-0.2-
r ~T— 120
-1— 60
—1 180
-r— 60
PERFUSION TIME (min)
120
180
PERFUSION TIME (min)
Fig. 3. Time course of net water ( A ) , Na ( Β ) . Κ (C) and CI ( D ) flux across the w a l l of rat intestinal tracts perfused w i t h Ringer's solution. A l p h a - r A N P ( # ) or saline ( O ) (0.25 ¿¿g/25 μ Ι / m i n ) was infused into the superior mesenteric artery during the perfusion of the small intestine. Each point represents the mean±S.E. of 6 determinations. (4-6,
1 0 ) , brain
other organs
( 1 1 , 1 2 ) , eye
( 6 ) . It h a s b e e n
(6, 11) also
t h a t t h e r e c e p t o r s f o r A N P e x i s t in t h e lateral
membranes
cortex
(13)
and
isolated
vascular
Our autoradiographic between
the
base
from
rat
systems
and
reported basokidney
(14-16).
study w a s of the
of
the
epithelia
area
and
the
o b s e r v e d specific b i n d i n g has n o t been characterized, receptors
are
they
suggest
that
present
in t h e
small
a n d m a y p l a y a role in w a t e r a n d
intestine electrolyte
h a n d l i n g in t h e s m a l l i n t e s t i n e . In
the
α-rANP
present
study,
0.25
/¿g/min
infused into the superior
lamina propria (Figs. 1 and 2 ) . H o w e v e r , the
artery increased net absorption of w a t e r , and
resolution for determining sites
for
α-rANP
membrane laries
in
of
the
exist
the lamina
had
insufficient
if s p e c i f i c in
epithelia propria.
the or
binding
CI
with
across
Ringer's
the
small
solution
intestine
in v i v o . T h e
mecha
nisms by w h i c h α - r A N P increased w a t e r
the
solute
Although
the
absorption
in t h e
small
intestine
u n k n o w n at p r e s e n t . H o w e v e r , t h e
Na
perfused
basolateral capil
of
mesenteric
obtained
autoradiogram
well
a-rANP
and are
following
11
Effect of A N P in Small Intestine 22024 165-
18-
Q 12 Ε
110'
=5
Ft
55 •
6
τ
0—J— 60
I 120
- 1 — —Γ 120 60 PERFUSION TIME (min) -
180
PERFUSION TIME (min)
180
30-
0.4 π
0.2·
20-
o 10-
χ
¥
LU
2
- ι — 120
~"r~~ 60
o -
180
"Ί 180
120
60
PERFUSION TIME (min)
PERFUSION TIME (min)
Fig. 4. Time course of net water ( A ) , Na ( Β ) , Κ (C) and CI (D) flux across the w a l l of rat intestinal tracts perfused w i t h glucose-free Ringer's solution. A l p h a - r A N P ( • ) or saline ( • ) (0.25 /¿g/25 /¿l/min) w a s infused into the superior mesenteric artery during perfusion of the small intestine. Each point represents the mean±S.E. of 6 determinations.
three possibilities deserve t o be c o n s i d e r e d : 1 )
fluid
α-rANP,
capillaries,
p r e s e n c e or a b s e n c e
acting
on
might increase w a t e r , by
decreasing
pressure
which
submucosal Na and
Ci
intracapillary regulates
paracellular
fluid
through
the
shunt
α-rANP
m i g h t stimulate active Na
on
Na-K-ATPase
activity
observed
in e i t h e r
of glucose to the
the
same
absorption
e x t e n t , it is l i k e l y t h a t t h e N a - g l u c o s e p o r t s y s t e m is n o t i n v o l v e d i n t h e
absorption
o f f l u i d a b s o r p t i o n b y α - r A N P . In v i e w o f t h e
pathway.
3)
2)
transport. because
has n o
(17).
was
hydrostatic
H o w e v e r , t h i s p o s s i b i l i t y is u n l i k e l y it h a s b e e n r e p o r t e d t h a t A N P
absorption
effect
a-rANP
cotrans-
stimulation
general effect of A N P o n the vascular system (14-16), Our effect
the
first
finding expected
possibility
is s e e m i n g l y from
of A N P . Recently,
the
is m o s t contrary
natriuretic
Seeber et al. ( 9 )
likely. to
the
action reported
m i g h t i n c r e a s e t h e e n t r y o f N a a n d CI a c r o s s
t h a t rat atrial e x t r a c t s u p r e s s e d t h e N a - g l u c o s e
the brushborder
c o t r a n s p o r t across t h e rat
membrane. Since
enhanced
intestine
perfused
12
Y. Kanai, N. Ohnuma & H. Matsuo Table 1 .
Effect of α - r A N P on net fluxes of water, Na, Κ and CI across the rat small intestine Water (μΙ/min/m)
Na (¿¿nnoles/min/m)
(/¿moles/min/m)
(//moles/min/m)
126±7
11.0±1.7
-0.029±0.043
14.7±1.8
183±8**
20.2±1.8**
CI
Ringer's solution control (n = 6) α-rANP (n = 6)
0.259±0.077**
24.9*1.7"
Glucose free Ringer's solution control (n=6) a-rANP (n=6)
6.4±1.2
-0.009±0.038
9.7±1.2
11.9±1.5*
-0.024±0.087
15.2±1.1**
66±7 97±3**
A l p h a - r A N P (0.25 /¿g/25 μΙ/rnin) or saline was infused through the superior mesenteric artery. Glucosefree Ringer's solution contains D-mannitol instead of glucose. Net absorption of water, Na, Κ and CI was calculated from the data (from 60 min to 180 min) in Figs. 3 and 4. Each value represents the mean±S.E. Significant difference from the controls, P < 0 . 0 5 ( * ) , P < 0 . 0 1 ( * * ) .
in
vivo.
However,
this
work
evaluate for the f o l l o w i n g used
crude
extract
is
difficult
reasons:
instead
of
1)
to
They
synthetic
a-
r A N P , w h i c h h a s b e e n i d e n t i f i e d as t h e n a t i v e circulating
ANP
in rats
( 1 8 ) . 2)
In v i e w
of
t h e e x t r e m e l y s h o r t b i o l o g i c a l half life o f A N P in t h e rat ( t
1 / 2
= 26.5 sec)
(19), the
duration
of c o l l e c t i o n period seems to be t o o
long to
detect the acute effect of A N P . O'Grady peptin
et al.
III
(20)
inhibited
reported
Na-K-2CI
that
cotransport
in s h o r t c i r c u l a t e d t e l e o s t i n t e s t i n e . it
is q u e s t i o n a b l e
plicable
to
whether
mammals.
It
this
has
atrio-
However,
is a l s o
been
ap
reported
i n r a b b i t s t h a t A N P d i d n o t a f f e c t CI t r a n s p o r t across the thick loop,
where
ascending
Na-K-2CI
limb
of
Henle's
cotransport
is
also
operating (21 ). Since
we
administered
α-rANP
directly
i n t o t h e m e s e n t e r i c a r t e r y , it is p o s s i b l e
that
the
this
vascular
maneuver.
effect
is
Although
exaggerated our
by
autoradiographic
study s h o w e d that the specific binding for
α-rANP
between lamina
were
the
base
localized of
propria, w e
the
on
the
epithelia
sites space
and
the
can not exclude a possi
bility that A N P directly acts, on the epithelia, leading
to
a
different
the experimental Our
observations
that A N P intestine
result
depending
reported
here
suggest
has a d i s t i n c t t a r g e t o n t h e and
on
conditions.
may
modulate
fluid
balance, although the underlying
and
small salt
mechanisms
which
a c c o u n t for the action of α - r A N P
on
the small intestine remain t o be e l u c i d a t e d . A c k n o w l e d g m e n t s : We are grateful to Y. Minami¬ take and Y. Hayashi (Suntory Institute for B i o medical Research) for providing synthetic a - r A N P and [ l ] a - r A N P . We also thank Dr. M . Imai of the National Cardiovascular Center Research Institute for reviewing this article. 1 2 5
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Ί3
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