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First published online November 30, 2007
Journal of Experimental Biology 210, 4411-4417 (2007)
Published by The Company of Biologists 2007
doi: 10.1242/jeb.010488
Octopamine partially restores walking in hypokinetic cockroaches stung by the parasitoid wasp Ampulex compressa
Department of Life Sciences and Zlotowski Center for Neuroscience, Ben-Gurion University of the Negev, Beer Sheva, Israel
* Author for correspondence (e-mail: libersat{at}bgu.ac.il)
Accepted 15 October 2007
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Key words: Periplaneta americana, parasitoid wasp, brain, subesophageal ganglion, walking, octopamine
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Introduction |
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). The parasitoid wasp Ampulex compressa hijacks the
nervous system of its host, the cockroach Periplaneta americana, and
thus controls its motivation to generate specific behaviors
(Libersat, 2003). It was shown
previously that the wasp injects venom directly into the head ganglia
(Haspel et al., 2003). As a
result, the cockroach first grooms for 30 min and then enters a hypokinetic
state that lasts for 2–5 weeks
(Libersat, 2003).
Venom-induced hypokinesia is characterized by little, if any, spontaneous
walking (Libersat, 2003). One
of the neuronal signatures of this hypokinetic state is a change in the
activity of neurons secreting octopamine (OA), a monoamine specific to
invertebrates. In stung animals the spontaneous firing rate of thoracic
octopaminergic neurons is dramatically decreased and the neurons respond more
weakly to both sensory stimuli and direct injection of current
(Rosenberg et al., 2006). It
seems likely that the observed alteration in the activity of octopaminergic
neurons is part of the mechanism by which the wasp induces a change in the
behavioral state of its prey. In the present study, we explore the possibility
that the wasp venom modifies OA levels, which eventually affects spontaneous
walking in the cockroach.
OA in invertebrates, like noradrenaline in vertebrates, has been associated
with the preparation for and execution of demanding motor behaviors
(Evans, 1985;
Roeder, 1999;
Libersat and Pflüger,
2004; Pflüger and
Stevenson, 2005). More specifically, OA is known to generate and
enhance motor output patterns in the central nervous system. In C.
elegans and in earthworms, it causes hyperactivity and stimulates
locomotion (Mizutani et al.,
2002; Komuniecki et al.,
2004). OA applied directly to the thoracic ganglia in a variety of
insect species initiates and sensitizes specific neuronal components
(Sombati and Hoyle, 1984;
Claassen and Kammer, 1986;
Stevenson and Kutsch, 1987;
Orchard et al., 1993;
Weisel-Eichler and Libersat,
1996). OA-null mutant flies display reduced walking, once more
suggesting a central role of OA in the initiation and/or modulation of
locomotion (Saraswati et al.,
2004). Moreover, the walking phenotype can be partially rescued by
feeding the mutants with OA (Saraswati et
al., 2004). In addition, insect adipokinetic hormone I (AKH-I), a
peptide that regulates energy homeostasis, enhances the activity of specific
OA neurons that bear AKH receptors and consequently stimulates walking in
cockroaches (Wicher et al.,
2006). Also in cockroaches, OA changes the gain of specific
synapses for escape (Goldstein and Camhi,
1991; Casagrand and Ritzmann,
1992) and modulates the activity of OA neurons
(Achenbach et al., 1997).
Cockroach octopaminergic cells have been mapped in each ganglion of the nerve
cord (Eckert et al., 1992;
Sinakevitch et al., 2005).
Not only OA, but also dopamine (DA), has been shown to be involved in the
regulation of walking in insects. For example, light induced activation of DA
neurons in Drosophila elevates walking
(Lima and Miesenbock, 2005).
Mutations with reduced levels of dopamine, as well as pharmacological
interventions altering dopamine levels, are consistently associated with
alterations in walking, although the direction of the effect is variable
(Jordan et al., 2006).
In this work, we perform a series of pharmacological experiments involving an agonist and an antagonist of OA receptors to test their effects on the locomotor behavior of stung and control cockroaches. We show that experimental elevation of OA, but not of DA levels, restores walking in stung cockroaches. Moreover, we show that walking can be restored by direct injection of OA into the brain, but not into the subesophageal ganglion (SEG), of stung cockroaches.
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Behavioral testing
A few hours prior to pharmacological experiments, cockroaches were
presented to a wasp for venom injection. Only stung cockroaches that showed
the characteristic venom-induced hypokinesia were used for experiments. As
described elsewhere (Fouad et al.,
1994), hypokinetic cockroaches usually show no spontaneous walking
and respond to a touch or wind stimulus with a short startle or a step forward
followed by a step backwards. Control cockroaches were screened to ensure
normal escape behavior. To test locomotor activity, cockroaches were placed
into a round observation arena (diameter 80 cm) and given at least 5 min to
adapt to the new environment. Spontaneous walking behavior was monitored by
measuring the amount of time spent by the cockroaches walking during 10 min
before and after injection.
Statistical analyses of data were performed using Sigmastat© (one-way ANOVA with the Bonferroni t-test for multiple comparisons and t-test or paired t-test; Jandel Scientific, Corte Madre, CA, USA). When data did not pass tests of normality and heterogeneity of variance a parallel non-parametric test was performed.
Drugs
Where not mentioned otherwise, drugs were purchased from Sigma-Aldrich
(Rehovot, Israel). Drugs were administered either via the hemolymph
or directly into a specific head ganglion. Hemolymph injections were performed
using a Hamilton microsyringe. 10 µl of solution was injected between the
third and fourth sternite into the abdominal hemocoel. Epinastine-HCl (50 mmol
l–1; Haorui Pharma-Chem Inc., Edison, NJ, USA),
cis(z)flupenthixol dihydrochloride (100 mmol l–1), quinpirole
(5 mmol l–1), SKF 82958
(6-chloro-1-phenyl-3-prop-2-enyl-1,2,4,5-tetrahydro-3-benzazepine-7,8-diol; 9
mmol l–1) and chlordimeform-HCl (CDM; 50 mmol
l–1) were dissolved directly in cockroach saline [in mmol
l–1: NaCl 214, KCl 3.1, CaCl2 9.0, TES-buffer 10;
pH 7.2 (Hancox and Pitman,
1995)].
For injection into the head ganglia, CDM and epinastine were used at a concentration of 2 mmol l–1 in cockroach saline, together with an inert tracer (Janus Green B, Sigma). To inject into the SEG, cockroaches were immobilized using modeling clay ventral side up. A slit was made in the ventral cuticle between the neck and the head and 14 nl of solution was injected into the ventral medial area of the SEG using a nano-volumetric injector (Medical Systems, NY, USA). To inject into the brain, cockroaches were immobilized dorsal side up. To prevent hemolymph loss after the cut, the neck was clamped down tightly using a minuten pin bent to form a metal bracket. A window was opened in the cuticle between the ocelli and 54 nl of solution was injected into the medial area of the brain. The injection volume for the SEG and brain was chosen according to the respective ganglion size. After the behavioral test, to verify the success and exact position of the injection site, we exposed the brain and SEG and visualized the localization of injections.
A stock solution of AKH-I (locust;
Glp-Leu-Asn-Phe-Thr-Pro-Ans-Trp-Gly-Thr-NH2, American Peptide
Company, Inc., Sunnyvale, CA, USA) was prepared in distilled water. The final
concentration was 2 µmol l–1
(Wicher et al., 2006).
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) with low
affinity for other amine receptors, and has been used as an octopamine agonist
in many studies (Stevenson et al.,
2005). Cockroaches were divided into three treatment groups: (1)
controls injected with saline (control/saline), (2) stung cockroaches injected
with saline (stung/saline) and (3) stung individuals injected with CDM
(stung/CDM). Spontaneous walking differed among the three treatment groups
(Fig. 1; P<0.001;
one-way ANOVA). Pairwise comparisons of saline-injected individuals showed
that stung cockroaches walked significantly less than controls [stung/saline,
0±0% (mean% ± s.d.), N=7; control/saline,
16.31±9.12%, N=6; P<0.05; Bonferroni
t-test]. Injection of CDM significantly increased spontaneous walking
in stung cockroaches compared to both saline-injected stung and control
cockroaches (stung/CDM, 33.74±15.07%, N=7; P<0.001
and P<0.05, respectively; Bonferroni t-test). The effect
of CDM on spontaneous walking of stung cockroaches followed a clear time
course (Fig. 2). Maximal effect
was observed 2 h after injection, while after 4.5 and 24 h spontaneous walking
did not differ from pre-injection values
(Fig. 2; stung/CDM: 2 h,
33.74±15.07%; 24 h, 4.05±6.52%; P<0.001 and
P=1, respectively; one-way ANOVA, Bonferroni t-test).
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Effect of systemic injection of AKH-I on spontaneous walking
We demonstrated that an OA receptor agonist injected into the hemolymph of
stung cockroaches induces walking to a level comparable to controls. AKH-I
modulates the activity of octopaminergic neurons and is known to stimulate
locomotor activity in cockroaches (Baumann
and Penzlin, 1984; Wicher et
al., 2006). Here we investigated whether or not the presumed
reduced levels of OA in stung animals are related to a reduction in AKH-I
levels. AKH-I (2 µmol l–1) injected into the hemolymph had
a pronounced effect on spontaneous walking of controls
(Fig. 4; control/AKH-I –
before treatment, 10.7±9.9%; after treatment, 29.0±12.1%,
N=11; P<0.001; paired t-test, Wilcoxon signed
rank test). In contrast, no significant effect on spontaneous walking was
observed in stung cockroaches (stung/AKH-I – before and after:
0±0%, N=10). Increasing the concentration did not initiate
walking in stung individuals (data not shown). Stung cockroaches injected with
CDM and control cockroaches injected with AKH-I did not differ in the
percentage time spent walking (stung/CDM, 33.74±15.07%; control/AKH-I,
29.0±12.1%; t-test; P=0.22).
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To test whether AKH-I elevates spontaneous walking in controls via the octopaminergic system, we injected control individuals with a mixture of AKH-I and the OA receptor antagonist epinastine. Epinastine blocked the effect of AKH-I on spontaneous walking (Fig. 5; control/AKH-I, 29.0%±12.1, N=11; control/epinastine/AKH-I, 8.9%±11.1, N=7; P<0.01; one-way ANOVA, Bonferroni t-test). Epinastine (no AKH-I)-injected controls walked significantly less than AKH-I injected controls (control/epinastine, 9.1±7.0%, N=10; P<0.001; Bonferroni t-test). The two experimental groups, epinastine with AKH-I and epinastine alone, were not significantly different from each other (P=1; Bonferroni t-test). When comparing spontaneous walking before and after treatment, epinastine significantly reduced the percentage time that control cockroaches spent walking (control/epinastine – before treatment, 18.0%±6.9; after treatment, 9.1%±7.0, N=10; P<0.05; paired t-test). In contrast, epinastine injected together with AKH-I did not affect the percentage time controls spent walking (control/epinastine/AKH-I – before, 15.0±11.4%; after, 8.9±11.1%, N=7; P=0.36; paired t-test).
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Effect of direct injection of OA into the head ganglia
In the cockroach central nervous system octopaminergic neurons provide
dense innervation to the central complex of the brain and to specific regions
of the SEG (Sinakevitch et al.,
2005). These regions of octopaminergic innervation coincide well
with the areas where the wasp injects its venom
(Haspel et al., 2003). With
this in mind, we injected the OA receptor agonist CDM directly into the head
ganglia of stung and control cockroaches with behavioral observations
following after 5 min. Stung cockroaches injected with CDM into the medial
protocerebrum of the brain walked significantly longer than stung cockroaches
injected with saline in the same area (Fig.
7A; stung/CDM/brain, 36.73±25.68%, N=10;
stung/saline/brain, 0±0%, N=10; P<0.001;
Kruskal–Wallis one-way ANOVA). Control cockroaches injected with CDM
into the brain did not walk significantly more than those injected with saline
(Fig. 7A; control/saline/brain,
22.92±17.71%, N=14; control/CDM/brain, 53.31±35.84%,
N=14; P>0.05; Dunn's post hoc test). This was
almost certainly due to the variability in walking duration of CDM injected
controls, since walking behavior was significantly elevated when comparing
walking before and after the injection (control/CDM/brain – before
treatment, 11.83±11.85%, N=14; after treatment:
53.31±35.84%; P<0.001; paired t-test). Walking was
not significantly different when comparing before and after saline injection
in the brain. Stung cockroaches injected with CDM into the SEG did not differ
from stung cockroaches injected with saline
(Fig. 7B; stung/CDM/SEG,
0±0%, N=14; stung/saline/SEG, 0±0%, N=10;
P>0.05; Dunn's post hoc test). Furthermore, unlike
control cockroaches injected with CDM into the brain, injection of CDM into
the SEG did not increase walking in control cockroaches
(Fig. 7B; control/saline/SEG,
10.41±8.12%, N=12; control/CDM/SEG – before treatment,
13.99±5.29%, N=13; after treatment, 10.22±7.67%;
P=0.18; paired t-test). In good agreement with the CDM
results in stung individuals, the OA receptor antagonist epinastine injected
into the brain of control individuals reduced spontaneous walking
[control/epinastine/brain – before treatment, 16.20±9.29%,
N=10; after treatment (Fig.
7A), 0.47±1.49%; P<0.001; paired
t-test].
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). In
control cockroaches, the OA receptor antagonist epinastine significantly
reduced the amount of spontaneous walking. It was shown previously that in
headless cockroaches and decapitated flies injection of OA increases
coordinated walking (Yellman et al.,
1997; Ridgel and Ritzmann,
2005). In crickets, hemolymph injection of CDM induces a state of
hyperactivity (Stevenson et al.,
2005). In locusts, OA injected into the metathoracic ganglion
produces walking movements (Sombati and
Hoyle, 1984). Moreover, flies with a deficit in neural OA show
reduced walking activity (Saraswati et
al., 2004; Roeder,
2005; Fox et al.,
2006). Therefore, together with the present results there is
strong evidence that OA initiates walking behavior by activating command-like
circuits in the central brain. Furthermore, it was shown that OA evokes
walking movements in insects when applied onto the thoracic nerve cord. It
therefore appears likely that OA acts on several levels within the distributed
neuronal network for walking and thus acts as a true neuromodulator as
proposed by Libersat and Pflüger
(Libersat and Pflüger,
2004). The increase in walking duration observed in OA-injected
stung cockroaches suggests that OA might be either depleted or not secreted
after a sting. In support of this hypothesis, we showed previously that the
activity level of octopaminergic neurons in the thoracic ganglia is strongly
depressed in stung cockroaches (Rosenberg
et al., 2006). The question as to whether or not this also occurs
in octopaminergic neurons in the head ganglia remains to be investigated by
direct intracellular recording.
It was demonstrated that Drosophila mutants with an impaired
central complex show locomotor deficits
(Strauss and Heisenberg,
1993). In the present study, we show that in stung cockroaches
focal injection of a potent OA receptor agonist around the central complex
area restores walking. Conversely, in controls, focal injection of a selective
OA receptor antagonist into the same area reduces walking. However, it appears
that the relevant neurons that modulate walking reside in the SEG and send
axons to innervate the motor centers, such as the central complex. In locusts
and cockroaches a specific group of octopaminergic neurons in the SEG sends
(i) ascending axons towards the brain, innervating all its major neuropiles
(Bräunig, 1991;
Sinakevitch et al., 2005), or
(ii) descending axons that form extensive ramifications in the neuropiles of
the thoracic and abdominal ganglia
(Bräunig and Burrows,
2004; Sinakevitch et al.,
2005). Within the group of octopaminergic ascending SEG neurons,
at least three provide dense innervation in the protocerebral bridge and
ellipsoid body of the central complex
(Sinakevitch et al., 2005), a
region implicated in control of walking
(Strausfeld, 1999;
Strauss, 2002) and the
location of venom injection (Haspel et
al., 2003). The wasp injects venom into both the SEG and into the
brain (Haspel et al., 2003).
Thus, the SEG sting might be affecting the activity of SEG OA ascending
neurons to cause reduced OA levels in the walking centers of the brain.
Alternatively, reduced OA levels in these brain areas might be the consequence
of the sting directly into the central brain. This issue should be resolved by
direct measurements of OA levels in central areas of the brains of stung and
control cockroaches. Our study provides additional evidence for the role of OA
in the control of walking mediated via the central complex.
We demonstrated previously that removing the brain in cockroaches
significantly enhances walking behavior, suggesting that the brain has an
overall inhibitory effect on walking
(Libersat et al., 1999;
Gal and Libersat, 2006).
However, the present data show that injection of OA towards or into the
central complex initiates and maintains walking. Thus, we can think of two
possible alternative explanations to account for this. The first is that the
brain may have both, inhibitory and excitatory components that are responsible
for initiation and maintenance of walking – with the inhibitory
component, however, being more dominant. The second is that OA may drive
neurons that in turn release the inhibition that the brain normally exerts
onto the thoracic locomotory circuits for walking maintenance.
DA receptor agonists had no measurable effects on spontaneous walking of
stung cockroaches. In flies DA induces grooming and walking behavior
(Yellman et al., 1997). The
rate-limiting enzyme required for catecholamine biosynthesis is tyrosine
hydroxylase. Pharmacological inhibition of this enzyme with
-methyl-P-tyrosine results in a dose-related inhibition of
walking activity in adult flies (Pendleton
et al., 2002). Similar results were found with reserpine, an
inhibitor of catecholamine uptake into vesicles, in both flies
(Pendleton et al., 2002) and
cockroaches (Weisel-Eichler and Libersat,
2002). Conversely, light induced activation of DA neurons in
Drosophila elevates locomotor activity
(Lima and Miesenbock, 2005).
However, the effect of DA appears to be receptor specific. SKF 82958, a D1 DA
receptor agonist, had no effect on walking, whereas quinpirole, a D2 DA
receptor agonist, enhanced locomotion
(Yellman et al., 1997). In the
present study quinpirole did not restore walking in stung cockroaches, which
could have one of several possible explanations. It might be that DA receptor
agonists are not permeable to the neuroepithelium. This seems unlikely though,
since we found that even direct injection of DA receptor agonists into the
brain or SEG of stung cockroaches does not elevate walking, although it
enhances grooming (F.L., unpublished observations)
(Weisel-Eichler et al., 1999).
It thus seems that these DA receptor agonists are ineffective in activating
walking in stung cockroaches, possibly because DA receptors are impaired in
stung individuals (Weisel-Eichler and
Libersat, 2002). Weisel-Eichler and Libersat showed that injecting
a DA receptor agonist into a stung cockroach failed to elicit a grooming
response. It is also possible, however, that cockroach walking is simply not
affected or regulated by DA receptor agonists. Importantly, we show that DA
receptor agonists do not restore walking in stung cockroaches, indicating that
the venom does not affect walking via interfering with the
dopaminergic system.
OA receptor agonists stimulate and maintain walking behavior in stung
cockroaches. A similar effect was observed in control individuals injected
with AKH-I and, moreover, the effect of AKH-I on walking was blocked by an OA
receptor antagonist. This suggests that AKH-I activates OA neurons to increase
walking. AKH also stimulates walking in Drosophila and is thought to
be the starvation signal bringing about food foraging
(Lee and Park, 2004). We
expected that AKH-I would stimulate walking in stung cockroaches by elevating
OA levels. The lack of effect suggests that AKH-I is not sufficient to
activate OA neurons in stung cockroaches to a level that can trigger walking.
The fact that OA itself does activate walking in stung individuals indicates
that the walking central pattern generator is not impaired; however, it might
have an elevated threshold for activation. There are additional modulators
that could neutralize the effect of AKH-I on OA neurons in stung cockroaches,
and these include 
-aminobutyric acid (GABA), as well taurine and β
alanine. GABA has been found to be present in the venom in large quantities
(Moore et al., 2006) and is
known to have an inhibitory effect on OA neurons
(Washio, 1994). AKH is known
to affect the activity of octopaminergic neurons via calcium
channels, whereas GABA inhibits the activity of octopaminergic neurons
via activating chloride channels
(Washio, 1994;
Wicher, 2001). This GABAergic
inhibitory pathway could be the cause of reduced activity in octopaminergic
neurons found in stung cockroaches and, consequently, the inability of AKH to
activate walking in stung individuals.
To conclude, we have shown in the present study that changes in levels of OA are likely to account for the modulation of spontaneous walking of cockroaches stung by the wasp A. compressa. To our knowledge, this is the first direct evidence that OA agonist injected into the insect brain activates walking. The present results imply that OA has a more prevalent role than DA in the regulation of spontaneous walking in the cockroach. We further show that AKH-I evokes walking via the octopaminergic system. However, AKH-I is most probably not the main modulatory substance affecting the activity of octopaminergic neurons in stung cockroaches. We propose that venom injection into the head ganglia selectively depresses the initiation and maintenance of walking by modifying the release of OA as a neuromodulator in restricted regions of the cockroach brain. This seems likely considering that specific octopaminergic neurons provide extensive innervation of neuropiles that are targeted by the wasp venom injection, and are involved in the control of initiation of walking.
List of abbreviations
-aminobutyric acid
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Acknowledgments |
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  K. Phillips ZOMBIE'ROACHES J. Exp. Biol., December 15, 2007; 210(24): iii - iii. [Full Text] [PDF]
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