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UniversitΣt Tⁿbingen - Lehrstuhl Tierphysiologie |
-Publikationen-
Annette Schmid,
Michael Koch
, Hans-Ulrich Schnitzler:
Conditioned pleasure attenuates the startle
response in rats
in: Neurobiol. Learning Memory, (1995) 64:1-3
Abstract:
The acoustic startle response of rats was found to be attenuated
if elicited in the presence of a conditioned stimulus predicting
reward. During conditioning, animals received a total of twenty
one pairings of light with palatable food and sucrose solution,
whereas controls received food and sucrose in the absence of
light. The amplitude of the acoustic startle response was
significantly reduced in the presence of light in conditioned
animals, but not in controls. It is assumed that a conditioned
response to light is the activation of a central state of
pleasure. We therefore suggest that 'pleasure-attenuated startle'
reflects a mechanism by which a defensive or aversive response is
attenuated during a pleasant, hedonic state.
Neural mechanismsof pleasure-attenuated startle
Michael Koch, Annette Schmid
Hans-Ulrich Schnitzler:
Pleasure-attenuation of startle is disrupted by
lesions of the nucleus accumbens
in: Neuroreport (1996) 7:1442-1446
Abstract:
The nucleus accumbens (NAC) and the amygdala have been implicated
in processes by which reinforcers control instrumental behavior.
Since reinforcement has both motivational and motor components,
it is necessary to differentiate between these two aspects of
reinforcement. The acoustic startle response (ASR) is attenuated
in the presence of a secondary reinforcer. In contrast to other
paradigms used for investigating mechanisms of reward, the
"pleasure-attenuated-startle" (PAS) paradigm indicates
the rewarding properties of a treatment by an attenuation rather
than by reinforcement of a response, thus allowing to determine
the motivational impact of a treatment independent from its motor
stimulating effects. Here, we report that the ASR was attenuated
in the presence of a reinforcer in conditioned sham-operated
animals and in rats with lesions of the amygdala, but not in
animals bearing 6-hydroxydopamine lesions of the NAC. These
findings suggest that the catecholaminergic innervation of the
NAC is important for the behavioral control by conditioned reward
Noise facilitation, startle and amygdala
Annette Schanbacher
,
Michael Koch, Hans-Ulrich Schnitzler:
Lesions of the amygdala do not affect the
enhancement of the acoustic startle response by background noise
in: Physiol. Behav.(1996) 60:1341-1346
Abstract:
The acoustic startle response (ASR) is enhanced in the presence
of loud background noise. We examined whether or not this
increase of response strength is mediated by the amygdala, which
is known to be involved in various phenomena of enhancement of
the ASR. To achieve this aim, we tested whether or not amygdaloid
lesions with the excitotoxin N-methyl-D-aspartate (NMDA) would
abolish the enhancement of the ASR by background noise in 13
Wistar rats. Loss of foot shock sensitization in these rats, as
well as histological evaluation, proved the successful
destruction of the amygdala. However, the enhancement by
background noise of the ASR, which was observed in sham-operated
controls, was not affected in amygdala-lesioned rats. Therefore,
we conclude that the background noise facilitation does not
involve emotional components that are mediated by the amygdala.
On the basis of these findings, we differentiate between the
startle-enhancing effect of background noise and the
amygdala-mediated effect of foot shocks on the ASR.
Somatostatin modulates fear-potentiated startle
Markus Fendt
, Michael
Koch, Hans-Ulrich Schnitzler:
Somatostatin in the pontine reticular formation
modulates fear-potentiation of the acoustic startle response: An
anatomical, electrophysiological and behavioral study
in: J. Neurosci. (1996) 16:3097-3103
Abstract:
The amplitude of the acoustic startle response (ASR) in rats is
increased in the presence of a cue which has previously been
paired with an aversive stimulus such as a footshock. This
phenomenon is called fear-potentiated startle and is a model to
study the neuronal and neurochemical mechanisms of the
acquisition and expression of fear.
The present study investigated the role in fear-potentiated startle of somatostatin (SOM) in the caudal pontine reticular nucleus (PnC) by a combination of anatomical, electrophysiological and behavioral methods. The PnC is an essential part of the primary startle circuit and is also the recipient of modulatory influences. First, we showed that the central gray (CG), which is involved in fear conditioning, is the main source of SOM-somatostatinergic input to the PnC. In the second experiment, we iontophoretically applied the SOM-somatostatin receptor agonist sandostatin on PnC neurons and extracellularly recorded the activity of PnC neurons. Sandostatin had no effect on tone-tone-evoked or spontaneous activity, but markedly attenuated the increase of neuronal activity seen after the administration of glutamate. In our third experiment, we injected different doses of sandostatin into the PnC of awake rats. Sandostatin dose-dependently blocked the fear-potentiation of the ASR, but had no effect on the baseline ASR amplitude.
The present study indicates that the SOM-somatostatinergic projection from the CG to the PnC is important for the modulation of fear-potentiated startle. We present a possible neural circuitry for the expression of fear-potentiated startle based on these data and previous findings.
Superior colliculus and sensorimotor gating
Markus Fendt
Michael Koch, Hans-Ulrich Schnitzler:
Sensorimotor gating deficit after lesions of the
superior colliculus
in: NeuroReport (1994) 5:1725-1728
Abstract:
The superior colliculus (SC) is important for the processing of
sensory information of different modalities and for the mediation
of adequate motor responses in mammals. The present study
investigated the effects of excitotoxic lesions of the SC on two
different modulations of the acoustic startle response (ASR) in
rats. Modulations of the ASR (i. e. increase or decrease of the
response strength) represent useful models for the study of
sensorimotor integration phenomena. Lesions of the SC decreased
the prepulse inhibition of the ASR without affecting the baseline
startle amplitude or the enhancement of the ASR by
footshock-sensitization. These results suggest a crucial role of
the SC in the prepulse inhibition of the ASR, a model of
sensorimotor gating.
Central gray and sensitization
Markus Fendt,
Michael
Koch, Hans-Ulrich Schnitzler:
Lesions of the central gray block conditioned fear
as measured with the potentiated startle paradigm
in: Brain Res. (1994) 661:163-173
Abstract: The amplitude of the acoustic startle response (ASR) in rats is increased in the presence of a cue which has previously been paired with an electric footshock. This phenomenon is termed fear-potentiated startle and is a useful model to investigate the neural systems underlying fear and anxiety. A series of studies have shown, that the amygdaloid complex is necessary for the acquisition and the expression of conditioned fear. Further experiments have delineated an efferent amygdalofugal pathway to the primary startle circuit, at the level of the caudal pontine reticular formation, which mediates the expression of conditioned fear [10]. Yet it was unclear, whether this amygdaloreticular pathway directly transfers the effects of conditioned fear from the amygdala to the primary startle circuit, or whether there exist one or more relay nuclei within this pathway or even additional parallel circuits. Based on our previous finding that the midbrain central gray (CG) is involved in the mediation of the facilitatory effects on the ASR of unconditioned aversive events, the present study tested the hypothesis that the CG is important for the potentiation of the ASR by conditioned fear. Therefore, we lesioned the CG before and after fear-conditioning and examined the effects of these lesions on fear-potentiated startle. Pre- and post-training lesions of the CG totally blocked the potentiation of the ASR amplitude by conditioned fear, which was seen in sham-lesioned rats, indicating that CG lesions affected the expression of conditioned fear. The baseline ASR amplitude was not influenced by CG lesions. We discuss possible pathways and mechanisms underlying the expression of conditioned and unconditioned fear in rats.
CRF modulates fear-potentiated startle
Markus Fendt
, Michael
Koch, Hans-Ulrich Schnitzler:
Corticotropin-releasing factor in the caudal
pontine reticular nucleus regulates the expression of
fear-potentiated startle
in: Eu. J. Neurosci. (1997) 9:299-305
Abstract:
The neuronal basis of the expression of states of fear is still
not completely understood. The fear-potentiated startle paradigm
is a valuable model to investigate the neuronal basis of fear.
Previous studies have demonstrated that the neuropeptide
corticotropin-releasing factor (CRF) plays an important role in
fear-related processes, notably in the potentiation of the
acoustic startle response. The present study investigated the
role in fear-potentiated startle of CRF in the caudal pontine
reticular nucleus, a brain nucleus that mediates the acoustic
startle response. A combination of anatomical,
electrophysiological and behavioural methods was applied. First,
we could show that the central nucleus of the amygdala gives rise
to a CRF-ergic projection to the caudal pontine reticular
nucleus. In the second experiment, we iontophoretically applied
CRF on caudal pontine reticular nucleus neurones and
extracellularly recorded the activity of these neurones. CRF had
a mainly excitatory effect on the tone-evoked activity of caudal
pontine reticular nucleus neurones. In our third experiment, we
injected the CRF antagonist
a
-helical
CRF into the caudal pontine reticular nucleus of awake rats.
Here,
a
-helical CRF dose-dependently
blocked fear-potentiated startle, but had no effect on the
baseline startle amplitude. The present results further
characterise the hypothetical neuronal circuitry underlying the
expression of fear-potentiated startle
Central gray and fear-potentiated startle
Markus Fendt
, Michael
Koch, Hans-Ulrich Schnitzler:
Lesions of the central gray block the
sensitization of the acoustic startle response in rats
in: Behav. Brain Res. (1996) 74:127-134
Abstract:
The amplitude of the acoustic startle response (ASR) in rats is
increased after administration of footshocks, a phenomenon termed
sensitization. The neural circuitry underlying this kind of
modulation of the ASR is only partly understood. It has been
shown that the central nucleus of the amygdala (cA) and its
efferent pathway to the caudal pontine reticular nucleus (PnC),
an essential part of the primary startle circuit, is important
for the sensitization of the ASR [23]. It was unclear, however,
whether the amygdaloreticular pathway directly transfers the
effects of footshocks onto the PnC, or whether there exists a
relay nucleus within this pathway. The present study tested the
hypothesis that the midbrain central gray (CG) is important for
the sensitization of the ASR. Neuroanatomical tracing experiments
indicate that a descending projection from the medial part of the
cA might form synapses in the region of the midbrain CG, where a
descending projection to the PnC takes its origin. We lesioned
the dorsal and lateral part of the CG with the neurotoxin
quinolinic acid and measured the effects of this lesion on the
sensitization of the ASR by footshocks. Lesions confined to the
dorsal and lateral parts of the CG totally blocked the
sensitization of the ASR, without affecting the ASR amplitude in
the absence of sensitizing stimuli. These findings suggest a
crucial role of the CG for the sensitization of the ASR. The
present data are reconciled with other findings from our
laboratory and from the literature and we discuss possible
mechanisms underlying the mediation of the sensitization of the
ASR in rats
Markus Fendt
, Martin
Kungel, Michael Koch, Hans-Ulrich Schnitzler:
Cholecystokinin enhances the acoustic startle
response in rats
in: NeuroReport (1995) 6:2081-2084
Abstract:
The present study examined the effects of the neuropeptide
cholecystokinin (CCK) on neurons of the caudal pontine reticular
nucleus (PnC), which mediates the acoustic startle response (ASR)
in rats. Electrophysiological experiments revealed an excitatory
effect of CCK on acoustically responsive neurons in the PnC. On
the behavioral level, CCK also enhanced the ASR. Since the PnC is
not only an obligatory relay station of the brain circuit
mediating the ASR, but also receives modulatory input from brain
areas involved in the expression of fear and anxiety, the
enhancement of the ASR by CCK could be interpreted as an
anxiogenic-like effect of this peptide.
Amygdala, Noradrenaline and Startle
Markus Fendt, Michael Koch
Hans-Ulrich Schnitzler:
Amygdaloid noradrenaline is involved in the
sensitization of the acoustic startle response in rats
in: Pharmacol. Biochem. Behav. (1993) 48:307-314
Abstract:
The present study examined the role of noradrenaline (NA) in the
central nucleus of the amygdala (cA) in the sensitization of the
acoustic startle response (ASR) in rats. In the first experiment
local microinjections of 0, 0.5, 1, 2 nmol of the
a
2-adrenergic antagonist yohimbine into the
cA increased the magnitude of the ASR in a dose-dependent way. In
the second experiment footshocks were applied in order to
increase the ASR amplitude (sensitization). Local microinjections
of 0, 4, 8, 16 nmol of the
a
2-adrenergic agonist ST-91 into the cA dose-dependently decreased
the sensitizing effects of footshocks on the amplitude of the
ASR. It is conjectured that yohimbine increases, and ST-91
decreases local NA-release by acting at presynaptic
autoreceptors. The present data suggest that the release of NA in
the cA is involved in the mediation of the sensitizing effects of
footshocks on the ASR.
Glutamat and fear-potentiated startle
Markus Fendt
, Michael
Koch, Hans-Ulrich Schnitzler:
NMDA receptors in the pontine brainstem are
necessary for fear-potentiation of the startle response
in: Eu. J. Pharmacol. (1996) 318:1-6
Abstract:
The fear-potentiated startle paradigm in rats is a valuable
animal model for the investigation of the neural and
neurochemical basis of fear. In this model, rats are trained to
associate a neutral stimulus with an aversive stimulus, so that
after conditioning the CS alone elicits a state of fear leading
to an exaggerated acoustic startle response (ASR). The
fear-potentiated startle paradigm does not require instrumental
responding for the indication of states of fear. The ASR is
mediated by a simple brainstem circuit, with the caudal pontine
reticular nucleus (PnC) as an interface that receives input from
startle-enhancing circuits. In the present study, we tested the
hypothesis that NMDA receptors on PnC neurones are involved in
the mediation of fear-potentiated startle. After
fear-conditioning, we injected the NMDA receptor antagonist
DL-2-amino-5-phosponopentanoic acid (AP-5) into the PnC of awake
rats and tested the effect on the expression of fear-potentiated
startle. Injections of AP-5 (0.125 - 0.5 nmol) into the PnC
dose-dependently attenuated fear-potentiated startle without
affecting the baseline ASR amplitude. The results suggests that,
at the level of the PnC, glutamate may mediate fear-potentiated
startle via NMDA receptors.
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