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The Journal of Neuroscience, January 7, 2009, 29(1):14-22; doi:10.1523/JNEUROSCI.3569-08.2009
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Neurobiology of Disease
Increased Phospholipase A2 Activity and Inflammatory Response But Decreased Nerve Growth Factor Expression in the Olfactory Bulbectomized Rat Model of Depression: Effects of Chronic Ethyl-Eicosapentaenoate Treatment
Cai Song,1,2 Xiang Yang Zhang,3 andMehar Manku4 1Department of Biomedical Sciences, Atlantic Veterinary College, University of Prince Edward Island, Charlottetown, Prince Edward Island, Canada C1A 4P3, 2National Research Council Institute for Nutrisciences and Health, Charlottetown, Prince Edward Island, Canada C1A 4P3, 3Department of Psychiatry and Behavioral Sciences, Baylor College of Medicine, Houston, Texas 77030, and 4Amarin Neuroscience, Oxford OX4 4GA, United Kingdom
Abstract
Top
Abstract
Introduction
An increased inflammatory response and deficient synthesis of neurotrophic factors (NTFs) may contribute to the etiology of depression. However, the interrelationship between inflammation and NTFs is unknown. Recently, ethyl-eicosapentaenoate (EPA) has been used to treat depression. The mechanism by which EPA benefits depression is also unclear. Using the olfactory bulbectomized (OB) rat model of depression, this study evaluated two pathways from bulbectomy to the induction of depression-like changes (the inflammation–hypothalamic–pituitary–adrenal axis–stress response pathway and inflammation–nerve growth factor–memory pathway) and the effect of EPA on these pathways. When compared with sham-operated rats fed a control diet, significantly increased locomotor and rearing activities in an "open field," impaired memory in the Morris water maze, increased expression of corticotrophin-releasing factor (CRF), and increased secretion of corticosterone were found in OB rats. mRNA expression of nerve growth factor (NGF) was significantly lower in the hippocampus, and phospholipase A2 (PLA2) was higher in the hypothalamus; this change was associated with increased interleukin-1β (IL-1β) and prostaglandin E2 (PGE2) in the serum and brain. EPA treatments normalized these behavioral impairments and reduced CRF expression and corticosterone secretion. EPA also reduced serum concentrations of IL-1β and PGE2, but reversed NGF reduction. Similar to the effects of EPA, the anti-inflammatory drug celecoxib significantly reduced blood PGE2, IL-1β, and corticosterone concentrations and increased NGF expression in OB rats. Furthermore, anti-NGF treatment blocked EPA effects on behavior. These results suggest that an interaction exists between inflammation and NGF in the depression model. EPA may improve depression via its anti-inflammation properties and the upregulation of NGF.
Key words: depression model; behavior; inflammation; EPA; NGF; celecoxib
Introduction
Inflammation may play an important role in major depression for multiple reasons. First, stress, as a trigger for depression, can increase inflammatory responses (Maes et al., 1998; Calcagni and Elenkov, 2006
Increasing evidence suggests that omega (n)-3 fatty acids have antidepressant and neuroprotective effects (Peet and Stokes, 2005
The n-6 fatty acid arachidonic acid is a precursor of eicosanoids, which produce PGE2 and other inflammatory compounds through the action of PLA2. Increased cytosolic PLA2 (cPLA2) activity has been related to the dysfunction of neurotransmitter systems and the HPA axis in depressed patients (Hibbeln et al., 1989
In the present study, olfactory bulbectomized (OB) rats, a valid depression model (Song and Leonard, 2005
Materials and Methods
Experimental design and procedure. There were four independent experiments (Exps.) in this study. In Exp. 1, 40 animals were divided into four groups (n = 10): (1) sham operated + 1% palm oil (control diet), (2) OB + 1% palm oil, (3) sham + 1% EPA, and (4) OB + 1% EPA. Palm oil and EPA were fed to animals for 7 weeks. Six weeks after diet feeding and 4 weeks after bulbectomy, animal behavior was tested in a novel and stressful environment "open field" and Morris water maze task, respectively. After behavioral tests, animals were allowed to rest for 1 d. Then, animals were decapitated, blood samples collected, and brains rapidly removed and dissected on ice. The concentrations of PGE2 and IL-1 were measured in the serum. The mRNA expression and activity of cPLA2 as well as the mRNA expression of NGF were measured in the hippocampus, amygdala, and hypothalamus. In Exp. 2, the groups and treatments were the same as those in Exp. 1. Corticotrophin-releasing factor (CRF) mRNA expression was measured by quantitative PCR in the paraventricular nucleus (PVN) of the hypothalamus by a micropunch technique (Song et al., 2007Animals and diets. Male Sprague Dawley rats (200–220 g and 2 months old at the start of the experiment) were purchased from Charles River. Food and water were available ad libitum. The colony was maintained at 22 ± 1°C with a 12 h light–dark cycle (7:30 A.M. to 7:30 P.M.). Animals were handled daily. The research protocol was approved by the Animal Care Committees of the Universities of British Columbia and Prince Edward Island and conformed to the guidelines of the Canadian Council for Animal Care.
One percent palm oil that contained a negligible amount of n-3 and low n-6 fatty acids was added to rat-chow powder as a control diet to ensure comparable texture and caloric value as the 1% EPA diet. Palm oil (Harlan Teklad Test Diet) was melted in a water bath (<50°C). The rat chow powder was mixed with the palm oil or EPA (Amarin Neuroscience/Laxdale). The food was prepared every 3–4 d and stored at 4°C (Song and Horrobin, 2004
3.6 months old.
Surgery. Bilateral olfactory bulbectomy was performed under ketamine (100 mg/kg, i.p.) and xylazine (20 mg/kg, i.p.) anesthesia. The surgical procedure was the same as that described by van Riezen and Leonard (1990)
In Exp. 3, rats were anesthetized with the same drugs. For intracerebroventricular anti-NGF administration, a 20 gauge guide cannula containing a removable 24 gauge obturator was stereotaxically implanted at the lateral cerebral ventricle as described by Song et al. (2003)
Open field. The wall of the apparatus was made of aluminum and consisted of a white open circular floor. Faint brown grids were marked on the floor of the apparatus to divide it into 60 squares of 10 cm2 for quantifying locomotor activity. A 60 W bulb (white) was positioned 90 cm above the center of the apparatus. Rats were placed singly in the center of the apparatus. The number of squares crossed, rearing times (i.e., when a rat stood completely erect on its hind legs), grooming times (i.e., when a rat scratched its face with its forepaws), defecation, and the number of entries into the central zone of the apparatus were recorded for a period of 3 min (Gray and Lalljee, 1974
Morris water maze. The apparatus and test for spatial learning and memory were the same as described by Song and Horrobin (2004)
Quantitative reverse transcription-PCR. mRNA expressions of NGF, CRF, and cPLA2 were studied in the hippocampus, amygdala, and hypothalamus by quantitative reverse transcription (RT)-PCR. The total RNA was purified from these brain regions using an RNeasy Mini Kit (Qiagen). cDNA was synthesized from 2 µg of total RNA using an Omniscript RT kit (Qiagen). Primer sequences were purchased from Invitrogen: for cPLA2, 5'-TTAACCTGCCGTATCCCTTGA-3' and 5'-AATGGAGGGCTGTCACT-3'; for NGF, 5'-GAAACGGAGACTCCGTTCACC-3' and 5'-GATTGTACCATGGGCCTGGA3'; for CRF, 5'-TGTGTCCCATACCCGCAAG-3' and TCGCCCTTTCGGACATCAT-3'; for β-actin, 5'-TGTGGATTGGTGGCTCTATCC-3' and 5'-CGGACTCATCGTACTCCTGCT-3'. The real-time PCR was performed with a QuantiTect SYBRGreen PCR Kit (Qiagen) at conditions of the initial activation at 95°C for 15 min, denaturation at 94°C for 15 s, annealing at 55°C for 20 s, and extension at 72°C for 15 s with a single fluorescence measurement for up to 45 cycles. Then, a melt step was provided with temperature ramps set from 40 to 95°C. The values were normalized against the endogenous control, β-actin. A sample from the control group was used as an external calibrator across all measurements.
Corticosterone, IL-1, and PGE2 assays. Serum samples from trunk blood of Exp. 2 were used for the corticosterone assay with a commercial radioimmunoassay kit (Immuchem corticosterone RIA kit for rats; catalog no. RCBK9906A; ICN Biochemical). Intra-assay and interassay coefficients of variation were 6.8% and 5.6%, respectively.
The serum concentration of IL-1β was measured by the ELISA method according to the instructions with the kit, and the method was the same as that described by Song et al. (2004)
The concentrations of PGE2 in the serum and hypothalamus (the supernatant of homogenized and sonicated brain tissue) were measured by an enzyme immunoassay (Assay Designs). The assay method was the same as that described previously (Song et al., 1998
Measurement of cPLA2 activities. The hypothalamus was homogenized with a sonicator in ice-cold PBS. The protein concentration was determined in the homogenates with a Coomassie Plus Protein Assay Kit (Pierce) according to the manufacturer's protocol.
The cPLA2 activity was measured with an assay kit (Cayman Chemicals) as described by Bosetti and Weerasinghe (2003)
Statistics. A repeated two-way ANOVA (surgery x diet) was applied to data from the water maze test, whereas a two-way ANOVA was used for analyzing other data from Exps. 1–3. A one-way ANOVA was used for the results from Exp. 4. Differences between groups were assessed by the Newman–Keuls post hoc test (the package was from GB-STAT, Dynamic Microsystems). Significance was set at p < 0.05. Results are expressed as mean ± SEM.
Results
The order in which the results are presented here is the same as the order of the pathway shown in Figure 1.
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Figure 1. The relationship between bulbectomy-induced limbic lesions and depressive symptoms as well as a hypothesis for EPA treatment. Corts, corticosterone; NA, noradrenaline; 5-HT, serotonin.
mRNA expression and activity of cPLA2
The two-way ANOVA indicated that OB surgery significantly changed the mRNA expression (F(1,32) = 18.89, p < 0.001) and activity (F(1,32) = 13.89, p < 0.001) of cPLA2 in the hypothalamus (Fig. 2) but not other brain regions (result not shown). EPA has a significant interaction with OB surgery (mRNA: F(1,32) = 11.23, p < 0.01; concentration: F(1,32) = 12.93, p < 0.01). The Newman–Keuls post hoc test showed that increases in the expression and concentration of PLA2 (expressed as the percentage of control) were found in the OB group fed palm oil (OB-palm) (p < 0.01) when compared with sham-operated rats fed the same diet (Sham-palm). These increases were significantly attenuated by EPA treatment (p < 0.01 for the mRNA and p < 0.05 for the concentration) (Fig. 2A,B).
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Figure 2. Effects of a diet enriched with EPA on OB-induced changes in the expression of mRNA (A) and activity of cPLA2 (B) in the hypothalamus. *p < 0.01 versus sham-operated rats; #p < 0.05, ##p < 0.01 versus OB rats fed palm oil (n = 8–10).
Concentrations of IL-1β and PGE2
The two-way ANOVA indicated a significant effect of OB surgery on serum IL-1β and PGE2 concentrations (IL-1: F(1,32) = 7.96, p < 0.01; PGE2: F(1,32) = 6.88, p < 0.01). The post hoc test showed a significant increase in IL-1β and PGE2 levels in the serum of the OB-palm group compared with the Sham-palm group (p < 0.01). The ANOVA also indicated an interaction between EPA treatment and OB surgery (IL-1: F(1,32) = 6.62, p < 0.05; PGE2: F(1,32) = 8.89, p < 0.01). The Newman–Keuls test revealed that EPA treatment significantly reduced both concentrations of these proinflammatory mediators (p < 0.05 and p < 0.01, respectively) (Fig. 3 A,B).
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Figure 3. Effects of a diet enriched with EPA and the COX2 inhibitor celecoxib on serum concentrations of IL-1 (A, C) and PGE2 (B, D) in OB and sham-operated rats, respectively. *p < 0.01 versus sham-operated rats; #p < 0.05, ##p < 0.01 versus OB rats fed palm oil (n = 8–10).
In Exp. 3, higher levels of serum IL-1β and PGE2 were also found in the OB-palm group than the Sham-palm group (p < 0.05). Celecoxib treatment, similar to the effects of EPA, markedly reduced IL-1 and PGE2 concentrations in the serum of OB rats (IL-1: F(1,32) = 5.93, p < 0.05; PGE2: F(1,32) = 8.48, p < 0.01) (Fig. 3C,D). Similar results were found in the hypothalamus: the PGE2 concentration was higher in OB rats than in sham rats (F(1,32) = 7.24, p < 0.01), and it was attenuated by celecoxib treatment (F(1,32) = 9.43, p < 0.01). Sham: 1435 ± 160; OB: 2376 ± 260; celecoxib: 1026 ± 121; OB with celecoxib: 1572 ± 149 (results are expressed as ng/g brain tissue).CRF mRNA expression and blood corticosterone concentration
The two-way ANOVA showed that OB surgery caused significant differences in CRF mRNA expression in the PVN of the hypothalamus and in serum concentration of corticosterone (CRF: F(1,32) = 7.83, p < 0.01; corticosterone: F(1,32) = 9.62, p < 0.01). The post hoc test revealed that a significant increase in CRF expression and the serum concentration of corticosterone occurred in the OB-palm group (p < 0.01) compared with the Sham-palm group. Additionally, the ANOVA indicated an interaction between diet and OB surgery (CRF: F(1,32) = 6.54, p < 0.05; corticosterone: F(1,32) = 5.83, p < 0.05). The post hoc test between groups confirmed that EPA treatment significantly reduced both CRF expression and corticosterone concentration compared with the OB-palm group (p < 0.05) (Fig. 4 A,B). Celecoxib treatment significantly blocked the elevation of corticosterone levels in OB rats (F(1,32) = 6.82, p < 0.05), which is similar to the effect of EPA (Fig. 4C).
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Figure 4. Effects of a diet enriched with EPA and the COX2 inhibitor celecoxib on the mRNA expression of PVN CRF (A) and serum concentrations of corticosterone (B, C) in OB and sham-operated rats, respectively. *p < 0.05, **p < 0.01 versus sham-operated rats; #p < 0.05 versus OB rats fed palm oil (n = 8–10).
NGF expression in the hippocampus
In Exp. 1, the diet and lesion-induced significant change in NGF mRNA expression was only found in the hippocampus (F(1,24) = 15.84, p < 0.001), not in the hypothalamus or amygdala. The Newman–Keuls post hoc revealed that NGF expression was increased in sham animals fed EPA (Sham-EPA) when compared with the Sham-palm group (p < 0.01) (Fig. 5). However, a significant decrease in NGF expression was found in the OB-palm group when compared with the Sham-palm group (p < 0.01). A two-way ANOVA also indicated a significant interaction between OB and diet (F(1,24) = 6.38, p < 0.05). The post hoc test between groups showed that EPA treatment significantly reversed the reduction of NGF mRNA expression in OB animals (p < 0.05) (Fig. 5A).
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Figure 5. Effects of a diet enriched with EPA (A) and the COX2 inhibitor celecoxib (B) on the mRNA expression of NGF in the hippocampus of OB and sham-operated rats. *p < 0.05, **p < 0.01 versus sham-operated rats; #p < 0.05 versus OB rats fed palm oil (n = 8–10).
Exp. 3 further confirmed the reduction of NGF expression in the hippocampus of OB rats receiving a saline injection (F(1,24) = 10.73, p < 0.01). The reduction was attenuated by chronic celecoxib treatment (F(1,32) = 9.92, p < 0.01) (Fig. 5B).Behavior changes in OB rats and effects of EPA and celecoxib treatments
In the "open field," locomotor activity and rearing scores were significantly increased in the OB-palm group compared with the sham-palm group (locomotor: F(1,32) = 14.73, p < 0.01; rearing: F(1,32) = 8.08, p < 0.01). EPA treatment did not significantly change animal behavior in sham rats. However, OB-induced behavioral changes in the open field were significantly attenuated by EPA treatment (locomotor: F(1,32) = 19.96; p < 0.001; rearing: F(1,32) = 16.98, p < 0.01) (Table 1). Similar hyperactive behaviors were also found in the OB-palm group in the Exp. 3 (locomotor: F(1,32) = 12.75, p < 0.01; rearing: F(1,32) = 7.46, p < 0.05). Similar to EPA, celecoxib significantly attenuated both behavioral changes (locomotor: F(1,32) = 10.83, p < 0.01; rearing: F(1,32) = 9.85; p < 0.01) (Table 1).
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Table 1. The effects of EPA and celecoxib on animal behavior in an ''open field''
In the water maze, there was no significant difference between sham and OB groups on days 1 and 2. On days 3, 4, and 5, members of the OB-palm group took longer to find the platform than sham controls (day 3: F(1,32) = 22.26, p < 0.01; day 4: F(1,32) = 9.43, p < 0.05; day 5: F(1,32) = 13.65, p < 0.01) (Fig. 6A). In the EPA feeding groups, there was no difference in the latency to find the platform between sham and OB animals. However, the ANOVA indicated a significant interaction between OB and EPA treatment on days 3, 4, and 5 (day 3: F(1,32) = 5.06, p < 0.01; day 4: F(1,32) = 3.35, p < 0.05; day 5: F(1,32) = 6.21, p < 0.01). The post hoc analysis revealed a significant difference between the OB-palm and OB-EPA groups (p < 0.05 or 0.01) (Fig. 6A), suggesting that EPA markedly improved spatial memory in OB rats.
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Figure 6. Effects of a diet enriched with EPA (A) and anti-NGF (B) on spatial memory in the Morris water maze in OB and sham-operated rats. *p < 0.05, **p < 0.01 versus sham-operated rats; #p < 0.05 versus OB rats fed palm oil (n = 8–10).
In Exp. 4, the one-way ANOVA indicated that EPA treatment significantly improved OB animal spatial memory in the water maze (F(1,29) = 8.82, p < 0.01). In contrast, chronic anti-NGF administration significantly blocked the effect of EPA (F(1,29) = 6.43, p < 0.05) (Fig. 6B).
Discussion
It has been extensively reported that changes in the behavior, neurotransmission, neuroendocrine, and immune functions of OB rats are similar to those observed in depressed patients (Song and Leonard, 2005As mentioned in the introduction, the newest hypothesis of depression postulates that the deficiency of NTFs is causally related to the etiology of depression. A postmortem study in suicide victims has shown decreased NGF protein levels in the frontal cortex and hippocampus (Dwivedi et al., 2005
Previous studies by others also suggest that inflammation may suppress NTF function. For example, a study from an in vitro model of Alzheimer's disease (AD) induced by aluminum has shown that increased proinflammatory cytokines are correlated with the decrease in NGF and BDNF expression; further, the latter triggers the expression of apoptosis genes (Johnson and Sharma, 2003
B, and CREB signals, which change NGF and BDNF functions (Otten et al., 2000
Another important finding from the present study is the series of mechanisms by which EPA ameliorates depression. n-3 and n-6 fatty acids are important components of the cell membrane. Changing the fatty acid content may influence brain structure and function. Epidemiological investigations have revealed a negative correlation between the intake of n-3 fatty acids and the onset or severity of depression (Cole et al., 2005
Inflammation and NTFs may play opposing roles in the cognitive impairment that often occurs in depressed patients. At physiological levels, IL-1 is an important factor for generating LTP and spatial memory. Suppressed LTP and impaired memory were observed in mice lacking the IL-1R or with IL-1RA overexpression (Avital et al., 2003
An increased inflammatory response may induce an imbalance between astrocyte and microglial activities and trigger the activation of indoleamine 2,3-dioxygenase and its subsequent enzyme kynurenine monooxygenase to cause serotonergic deficiency and glutamatergic overproduction (Müller and Schwarz, 2007
A limitation of this study is a shortage of measurement of the fatty acid profile after EPA treatment. Many studies have demonstrated that n-3 and n-6 diets change the composition of brain lipids, and such changes have been firmly related to their effects on neurotransmission and behavior (Chalon et al., 1998
Footnotes
Received July 29, 2008; revised Oct. 9, 2008; accepted Nov. 13, 2008.This work was supported by Amarin Neuroscience and the Canadian Institutes of Health Research. We thank Xuwen Li, Zhijian Kang, and Yoshie Kadotomi for their technical support.
Correspondence should be addressed to Dr. Cai Song, Department of Biomedical Sciences, University of Prince Edward Island, 550 University Avenue, Charlottetown, Prince Edward Island, Canada C1A 4P3. Email: cai.song{at}nrc.gc.ca
Copyright © 2009 Society for Neuroscience 0270-6474/09/290014-09$15.00/0
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