 |
|||||
|
|||||
|
|||||
|
|||||
|
|||||
Previous Article | Next Article
The Journal of Neuroscience, April 15, 2003, 23(8):3483
A Critical Role for Nucleus Accumbens Dopamine in Partner-Preference Formation in Male Prairie Voles
Brandon J. Aragona, Yan Liu, J. Thomas Curtis, Friedrich K. Stephan, and Zuoxin Wang Department of Psychology and Program in Neuroscience, Florida State University, Tallahassee, Florida 32306-1270
ABSTRACT
TOP
ABSTRACT
Introduction
Although the role of nucleus accumbens (NAcc) dopamine (DA) in reward learning has been extensively studied, few investigations have addressed its involvement in learning socially relevant information. Here, we have examined the involvement of NAcc DA in social attachment of the "monogamous" prairie vole (Microtus orchrogaster). We first demonstrated that DA is necessary for the formation of social attachment in male prairie voles, because administration of haloperidol blocked, whereas apomorphine induced, partner-preference formation. We then provided the first descriptions of DA neuroanatomy and tissue content in vole NAcc, and mating appeared to induce a 33% increase in DA turnover. We also showed that administration of haloperidol directly into the NAcc blocked partner preferences induced by mating and apomorphine. In addition, administration of apomorphine into the NAcc but not the caudate putamen induced partner preferences in the absence of mating. Together, our data support the hypothesis that NAcc DA is critical for pair-bond formation in male prairie voles.
Key words: dopamine; nucleus accumbens; pair bonding; apomorphine; haloperidol; tyrosine hydroxylase; dopamine transporter; mating
Introduction
Perhaps the most important form of associative learning to humans is the formation of social attachments. Although considerable work has been done on dopamine (DA) involvement in associative learning, few studies have examined the formation of socially relevant associations. This is a concern because DA systems have been implicated in disorders associated with the inability to form social attachments (Mikkelsen et al., 1981
; Schneier et al., 2000
Prairie voles display a suite of behaviors characteristic of monogamy: preferential mating with one partner, remaining together during gestation, and biparental care throughout lactation (McGuire and Novak, 1984
Mating-induced partner preferences likely involve reinforcing properties associated with mating along with approach behavior oriented toward the partner. Therefore, partner-preference formation can be viewed as a natural example of reward learning, a process that has significant DA involvement (Robbins and Everitt, 1996
Materials and Methods
Subjects. Subjects were sexually naive male prairie voles from a laboratory breeding colony. At ~21 d of age, subjects were weaned and housed in same-sex sibling pairs in plastic cages (20 × 50 × 40 cm). Water and food were provided ad libitum, a 14/10 hr light/dark cycle was maintained, and the temperature was ~20°C. All subjects were between 80-120 d of age when tested and weighed between 40-50 gm. Ovariectomized (OVX) females served as stimulus animals. For manipulations that required mating (24 hr pairings), females were estrogen primed with subcutaneous estrodial benzoate (EB) pellets implanted 4 d before pairing (Smith et al., 2001
Partner preference test. The testing apparatus consisted of a central cage (20 × 25 × 45 cm) joined by hollow tubes (7.5 × 16 cm) with two parallel identical cages, each housing a stimulus animal (Curtis et al., 2001
Perfusion and immunocytochemistry. Animals were anesthetized with sodium pentobarbital (1 mg per 10 gm body weight) and perfused transcardially with 0.9% saline followed by 4% paraformaldehyde in 0.1 M PBS, pH 7.6, at 4°C. Brains were postfixed for 30 min in the same fixative and then immersed in 30% sucrose in PBS. For immunocytochemistry, a set of 30 µm coronal sections that spanned the NAcc at 90 µm intervals was rinsed in 0.1 M PBS, pH 7.4, treated with 0.3% hydrogen peroxide in PBS, incubated in a blocking solution [PBS with 0.3% Triton X-100 (PBT), 10% normal goat serum (NGS), and 2% bovine albumin (BSA)] for 1 hr, and then incubated in 1:30,000 rabbit anti-dopamine transporter (anti-DAT) polyclonal antibody (a gift from Dr. Michael Kuhar, Emory University, Atlanta, GA) in PBT with 2% NGS and 2% BSA at 4°C for 48 hr. After incubation with 1:300 biotinylated goat anti-rabbit antibody (Vector Laboratories, Burlingame, CA) in PBT with 2% NGS and 2% BSA at room temperature for 2 hr, sections were rinsed, incubated with ABC complex (Vector Laboratories) for 1.5 hr, and then stained using 3-3'-diaminobenzidine (DAB kit; Vector Laboratories). A similar staining method was used on an alternate set of brain sections for tyrosine hydroxylase (TH) immunocytochemistry with rabbit anti-tyrosine hydroxylase polyclonal antibody as a primary antibody (1:8000; Chemicon, Temecula, CA).
Tissue microdissection. Subjects were killed via rapid decapitation, and brains were immediately extracted and frozen. Coronal sections (300 µm) were cut on a cryostat and frost mounted onto microscope slides. Bilateral tissue punches with a 1 mm diameter were taken from the NAcc, caudate putamen (CP), and paraventricular nucleus of the hypothalamus (PVN) (areas that showed high-density TH staining) and stored at
80°C until analyzed. Neurochemical extraction was performed as described previously (Aragona et al., 2002
HPLC with electrochemical detection. Peak separation was achieved using a microdialysis MD-150 analytical column (ESA, Chelmsford, MA). The mobile phase consisted of 75 mM sodium dihydrogen phosphate monohydrate (Electron Microscopy Sciences, Fort Washington, PA), 1.7 mM 1-octanesulfonic acid sodium salt, 0.01% triethylamine (Aldrich, Milwaukee, WI), 25 µM EDTA (Fisher Scientific), and 10% acetonitrile ( Electron Microscopy Sciences), and the pH was adjusted to 3.85 with 85% phosphoric acid (Fisher Scientific). Samples were first oxidized at 250 mV and then reduced at
Stereotaxic cannulation and injection. Subjects were anesthetized with sodium pentobarbital (2.5 mg per 40 gm body weight), and 26 gauge bilateral guide cannulas (Plastics One, Roanoke, VA) aimed at the NAcc were implanted stereotaxically (nose bar,
Results
Experiment 1a: does peripheral administration of the dopamine antagonist haloperidol block mating-induced partner preferences?
Sexually naive males were randomly assigned into one of three groups that received intraperitoneal injections of either 200 µl of saline (n = 8) or saline containing 0.4 µg (n = 10) or 4 µg (n = 8) of the nonselective DA antagonist haloperidol. Subjects were then immediately paired with EB-primed OVX females and allowed to mate ad libitum for 24 hr. Behavior was videotaped, and the effect of haloperidol on mating was assessed. Males that did not mate within the first 6 hr were excluded from the experiment. After 24 hr of mating, subjects were tested for partner preferences.
As expected, saline-injected control subjects formed partner preferences with their respective mates after 24 hr of mating (p = 0.05) (Fig. 1A). However, both doses of haloperidol blocked mating-induced partner preferences (0.4 µg, p = 0.33; 4.0 µg, p = 0.78) (Fig. 1A). Although haloperidol blocked partner preferences, it did not affect the number of mating bouts during the initial cohabitation period (control, 6.9 ± 1.5; 0.4 µg of Halo, 7.2 ± 3.0; 4 µg of Halo, 6.4 ± 2.7) or locomotor activity measured by cage entries during the partner-preference test (control, 105.7 ± 17.5; 0.4 µg of Halo, 67.5 ± 14.1; 4 µg of Halo, 97.64 ± 10.4). Therefore, haloperidol blockade of DA receptors prevented the formation of a partner preference without disruption of mating.
View larger version (10K):[in this window]
[in a new window]
Figure 1. Peripheral administration of dopamine drugs influenced partner preferences in male prairie voles. A, Males injected intraperitoneally with saline and mated with a partner for 24 hr had more side-by-side contact with the partner versus a conspecific stranger. This partner preference was not seen in males receiving saline injections containing the dopamine antagonist Halo. B, Males injected with saline and paired with a partner for 6 hr in the absence of mating showed nonselective side-by-side contact during the partner-preference test. However, males receiving the low (0.5 µg) but not the high (5 and 50 µg) dose of the dopamine agonist Apo had more contact with the partner versus a stranger. *p < 0.05; paired samples t test. Error bars indicate SEM.
Experiment 1b: does peripheral administration of the dopamine agonist apomorphine induce partner preferences in the absence of mating?
Sexually naive males were divided into four groups that received intraperitoneal injections of either 200 µl of saline (n = 8) or saline containing 0.5 µg (n = 9), 5 µg (n = 10), or 50 µg (n = 8) of apomorphine. Immediately after injection, subjects were paired with OVX females that were not treated with estradiol for 6 hr of cohabitation in the absence of mating. Thereafter, subjects were tested for partner preferences. All behavior was videotaped and reviewed, and the absence of mating was confirmed.
Subjects that received saline injections before 6 hr of cohabitation showed nonselective side-by-side contact during the partner-preference test (p = 0.96) (Fig. 1B). However, those that received low-dose intraperitoneal administration of apomorphine (0.5 µg) showed partner preferences (p < 0.05) (Fig. 1B). Subjects given higher doses of apomorphine (5 and 50 µg) did not show partner-preference formation (p = 0.35 and 0.39, respectively). Locomotor activity during the partner-preference test was not different between the four groups (control, 82.1 ± 11.5; 0.5 µg of Apo, 101.8 ± 39.4; 5 µg of Apo, 118.2 ± 20.6; 50 µg of Apo, 117.8 ± 31.5.)
Experiment 2: what is the dopamine innervation in nucleus accumbens of male prairie voles?
Experiment 1 showed that DA is involved in partner-preference formation in male prairie voles. Previous experiments with females have also shown that DA, and specifically NAcc DA, is important for partner-preference formation (Gingrich et al., 2000
Figure 2 shows matched sections of TH and DAT labeling in the NAcc and several other brain areas of male prairie voles. Light microscopic analysis revealed similar patterns of staining for both TH and DAT in the NAcc, CP, and olfactory tubercle (OT). The massive TH and DAT staining in these areas indicates dense DA-terminal innervation. For TH, staining appears extremely dense in the NAcc, CP, and OT. DAT is most densely stained in the CP and OT, with lighter staining in the medial portion of the NAcc, especially in the more caudal sections. Inspection of subcommissural regions of the ventral forebrain reveals that the ventral pallidum (VP) has only moderate labeling (Fig. 2C,D); however, fibers are clearly visible at higher magnification.
View larger version (189K):[in this window]
[in a new window]
Figure 2. A-D, Photomicrographs displaying immunoreactive staining for TH (left) and DAT (right) at rostral (A, B) and caudal (C, D) levels of NAcc from representative brain sections of male prairie voles. ac, Anterior commissure. Scale bar, 500 µm.
Experiment 3: does mating increase dopamine turnover in nucleus accumbens of male prairie voles?
Sexually naive males were paired either with a male sibling (control, n = 8), an EB-primed OVX female with which the subject chose not to mate (nonmated, n = 8), or an EB-primed OVX female with which the subject mated (mated, n = 12). Subjects in the mated group were killed 30 min after mating onset and averaged 40 min total time together. Therefore, control and nonmated groups were paired for 40 min and then killed. Bilateral tissue punches were taken from the NAcc, CP, and PVN (Fig. 3A), and tissue samples were assayed for several neurochemicals.
View larger version (36K):[in this window]
[in a new window]
Figure 3. Effect of mating on dopamine turnover and neurochemical content in the male prairie vole brain. A, Schematic illustration of tissue-punch location for NAcc and CP. The illustration is from the atlas of Paxinos and Watson (1986)
In the NAcc, mated males had 33% higher mean values of DA turnover compared with control and nonmated subjects, but this increase was not statistically significant (p = 0.17) (Fig. 3B). A similar trend was also found in the CP but not in the PVN (Fig. 3B). Figure 3C shows that under baseline conditions, DA turnover in the NAcc was approximately two times greater than in the CP, whereas the CP had approximately three times the amount of DA compared with the NAcc. The PVN contained much less DA compared with the NAcc and CP. The PVN was primarily noradrenergic and also had approximately two times the 5-HT compared with the NAcc and CP. Mating and social experience had no significant effects on any of the other neurochemicals measured.
Experiment 4a: does site-specific administration of the dopamine antagonist haloperidol into nucleus accumbens block mating-induced partner preferences?
Sexually naive males were implanted with guide cannulas bilaterally aimed at the NAcc. After 3-5 d of recovery, subjects were divided into one of two groups that received microinjections of 200 nl of CSF alone per side (n = 5) or CSF with 4 ng of haloperidol (n = 7). Subjects were then paired with an EB-primed OVX female for 24 hr of mating and then tested for partner preferences. All behavior was videotaped and analyzed as in experiment 1a.
As expected, the control group displayed significant partner-preference formation (p < 0.05), and haloperidol treatment completely blocked mating-induced partner preferences (p = 1) (Fig. 4A). This effect was not caused by disruption of mating during the first 6 hr of the cohabitation period. Rather, haloperidoltreated subjects showed a trend for more mating bouts compared with control animals (control, 5.4 ± 1; 4 ng of Halo, 8.1 ± 1.4; p = 0.1). Haloperidol-treated animals did not differ from controls in locomotor activity during the first 6 hr of the cohabitation period (as measured by the number of times the subject crossed the center of the cage) or during the partner-preference test.
View larger version (11K):[in this window]
[in a new window]
Figure 4. NAcc dopamine is involved in partner-preference formation of male prairie voles. A, Males microinjected with artificial CSF into the NAcc and mated with a partner for 24 hr had more side-by-side contact with the partner versus a conspecific stranger. This mating-induced partner preference was blocked by NAcc administration of CSF containing Halo. B, Males microinjected with CSF and paired with a partner for 6 hr in the absence of mating showed nonselective side-by-side contact with the partner or stranger. However, males receiving the low (0.04 ng) but not the high (4 ng) dose of the dopamine agonist Apo displayed partner preferences. This apomorphine-induced (0.04 ng) partner preference was blocked by coadministration of haloperidol (0.4 ng). In addition, apomorphine (0.04 ng) failed to induce partner preferences when administered into the CP. *p < 0.05 and **p < 0.005; paired samples t test. Error bars indicate SEM.
Experiment 4b: does site-specific administration of the dopamine agonist apomorphine into nucleus accumbens induce partner preferences in the absence of mating?
Sexually naive males were cannulated, as described in experiment 4a, and divided into one of four groups that received microinjections of either CSF alone (200 nl per side; n = 7), CSF containing 0.04 ng (n = 8) or 4 ng (n = 7) of apomorphine, or CSF containing 0.04 ng of apomorphine with 0.4 ng of haloperidol (n = 8). To assess site specificity, a final group of subjects (n = 6) was implanted with guide cannulas aimed at the CP (2 mm dorsal to NAcc) and received injections of CSF containing 0.04 ng of apomorphine. All subjects were paired with OVX females that were not treated with estradiol for 6 hr of cohabitation in the absence of mating and then immediately tested for partner preferences. Behavior was videotaped and analyzed as in experiment 1b.
Control subjects that received CSF injections into the NAcc before 6 hr of cohabitation showed nonselective side-by-side contact during the partner-preference test (p = 0.7) (Fig. 4B). However, similar to intraperitoneal administration, subjects that received administration of apomorphine at a low dose (0.04 ng) but not a high dose (4 ng) showed partner preferences (p < 0.01) (Fig. 4B). This apomorphine-induced partner preference was blocked by coadministration of 0.4 ng of haloperidol (p = 0.74). In addition, apomorphine failed to induce partner preferences when injected into the CP (p = 0.93), suggesting that DA acts in a site-specific manner to influence partner preferences (Fig. 4B). Drug treatment did not affect locomotor activity during the partner-preference test; however, subjects receiving NAcc apomorphine showed decreased locomotor activity during the 6 hr of cohabitation (as measured by the number of times the subject crossed the center of the cage) (control, 297.8 ± 79.5; 0.04 ng of Apo, 135.1 ± 14.7, 4 ng of Apo, 151.7 ± 24.2; p = 0.04). Importantly, there were no differences in locomotor activity between the two apomorphine groups. Injection sites for apomorphine in the NAcc and CP are illustrated in Figure 5. All NAcc injections were located in the more rostral portions of the NAcc, where TH/DAT is most abundant.
View larger version (57K):[in this window]
[in a new window]
Figure 5. A schematic illustration (left) showing locations of microinjections of apomorphine into the NAcc or CP, and a representative photomicrograph of vole brain section (right) displaying the site of microinjection into the NAcc.
Discussion
This study shows, for the first time, that DA is critically involved in social attachment in male prairie voles. Administration of the DA antagonist haloperidol blocked mating-induced partner preferences, whereas the DA agonist apomorphine induced this behavior in the absence of mating. This is also the first study to describe DA neuroanatomy, tissue content, and turnover in the vole NAcc. Although not statistically significant, mating appears to increase DA turnover in the NAcc by 33%, suggesting that DA may be released during mating. The involvement of the NAcc in pair bonding was demonstrated by site-specific administration of haloperidol or apomorphine into the NAcc. Haloperidol blocked partner preferences induced either by mating or by apomorphine. Similar to intraperitoneal administration, apomorphine in the NAcc induced partner-preference formation in the absence of mating at low but not high doses. Together, these data suggest that mating induces DA release in NAcc, and that released DA is necessary for pair-bond formation of male prairie voles.
DA is involved in partner-preference formation
DA receptor antagonism by peripheral haloperidol administration blocked mating-induced partner preferences. Importantly, haloperidol did not disrupt mating or locomotor activity, and therefore, its effect on partner-preference formation was not secondary to effects on mating or locomotion. These data suggest that haloperidol affected a social consequence of mating and demonstrate that access to DA receptors is necessary for partner-preference formation in male prairie voles.
Peripheral administration of apomorphine at a low dose induced partner-preference formation in the absence of mating, providing additional evidence that DA is involved in pair-bond formation in male prairie voles. However, in a previous study, administration of apomorphine at a high dose (e.g., 50 µg) induced partner preferences in females (Wang et al., 1999
Neuroanatomical and neurochemical description of vole NAcc
The NAcc and VP have been implicated in social attachment (Gingrich et al., 2000
The DOPAC/DA ratio is commonly used as an index of DA turnover (Blackburn et al., 1989
NAcc is important for DA regulation of partner-preference formation
As with peripheral administration, haloperidol administered into the NAcc blocked mating-induced partner preferences without disrupting mating. In fact, subjects that received haloperidol directly into the NAcc showed a trend for increased mating behavior. This increase in mating is analogous to increases in free food consumption after haloperidol injection into the NAcc of rats (Salamone et al., 1991
Similar to peripheral administration, apomorphine injected directly into the NAcc induced partner preferences in the absence of mating at a low but not a high dose. A possible explanation for the apomorphine dose-response follows from the fact that apomorphine is a general DA agonist and has approximately three orders of magnitude greater binding affinity for D2-type compared with D1-type receptors (Missale et al., 1998
Administration of low-dose apomorphine has also been reported to reduce locomotor activity (Van Ree and Wolterink, 1981
Finally, these behavioral effects of apomorphine appear to be site-specific, because partner-preference formation occurred after injections into the NAcc but not the CP. These data, together with the data from female prairie voles (Gingrich et al., 2000
Conclusion
This study provides ample evidence that NAcc DA is involved in social attachment. NAcc DA has been implicated in many, although perhaps not all, aspects of reward learning (Berridge and Robinson, 1998
FOOTNOTES Received Oct. 11, 2002; revised Jan. 22, 2003; accepted Jan. 29, 2003.
This work was supported by National Institutes of Health Grants MH-67396 to B.J.A., HD-40722 to J.T.C., and MH-58616 and MH-66734 to Z.X.W. We thank Christie D. Fowler and Jennifer R. Stowe for critical reading of this manuscript and Y. Joy Yu for technical assistance. We also thank Dr. Michael Kuhar of Emory University for providing the DAT antibody.
Correspondence should be addressed to Brandon J. Aragona, Department of Psychology, Florida State University, Tallahassee, FL 32306-1270. E-mail: aragona{at}psy.fsu.edu.
References
- Aragona BJ, Curtis JT, Davidson AJ, Wang ZX, Stephan FK (2002) Behavioral and neurochemical investigation of circadian time-place learning in the rat. J Biol Rhythms 17:330-344
[Abstract/Free Full Text] .- Berridge KC, Robinson TE (1998) What is the role of dopamine in reward: hedonic impact, reward learning, or incentive salience? Brain Res Brain Res Rev 28:309-369[Medline].
- Blackburn JR, Phillips AG, Jakubovic A, Fibiger HC (1989) Dopamine and preparatory behavior. II. A neurochemical analysis. Behav Neurosci 103:15-23[Web of Science][Medline].
- Carter CS, Getz LL (1993) Monogamy and the prairie vole. Sci Am 268:100-106[Web of Science][Medline].
- Cho MM, DeVries AC, Williams JR, Carter CS (1999) The effects of oxytocin and vasopressin on partner preferences in male and female prairie voles (Microtus ochrogaster). Behav Neurosci 113:1071-1079[Web of Science][Medline].
- Ciliax BJ, Heilman C, Demchyshyn LL, Pristupa ZB, Ince E, Hersch SM, Niznik HB, Levey AI (1995) The dopamine transporter: immunochemical characterization and localization in brain. J Neurosci 15:1714-1723[Abstract].
- Curtis JT, Liu Y, Wang ZX (2001) Lesions of the vomeronasal organ disrupt mating-induced pair bonding in female prairie voles (Microtus ochrogaster). Brain Res 901:167-174[Web of Science][Medline].
- Curtis JT, Stowe JR, Wang ZX (2003) Differential effects of intraspecific interactions on the striatal dopamine system in social and non-social voles. Neuroscience, in press.
- DeVries AC, DeVries MB, Taymans S, Carter CS (1995) Modulation of pair bonding in female prairie voles (Microtus ochrogaster) by corticosterone. Proc Natl Acad Sci USA 92:7744-7748
[Abstract/Free Full Text] .- DeVries AC, DeVries MB, Taymans SE, Carter CS (1996) The effects of stress on social preferences are sexually dimorphic in prairie voles. Proc Natl Acad Sci USA 93:11980-11984
[Abstract/Free Full Text] .- Dewsbury DA (1987) The comparative psychology of monogamy. Nebr Symp Motiv 35:1-50.
- Di Chiara G (1995) The role of dopamine in drug abuse viewed from the perspective of its role in motivation. Drug Alcohol Depend 38:95-137[Web of Science][Medline].
- Di Chiara G (1999) Drug addiction as dopamine-dependent associative learning disorder. Eur J Pharmacol 375:13-30[Web of Science][Medline].
- Freed C, Revay R, Vaughan RA, Kriek E, Grant S, Uhl GR, Kuhar MJ (1995) Dopamine transporter immunoreactivity in rat brain. J Comp Neurol 359:340-349[Web of Science][Medline].
- Getz LL, Carter CS (1996) Prairie-vole partnerships. Am Sci 84:56-62.
- Getz LL, Hofmann JE (1986) Social organization in free-living prairie voles, Microtus ochrogaster. Behav Ecol Sociobiol 18:275-282[Web of Science].
- Gingrich B, Liu Y, Cascio C, Wang ZX, Insel TR (2000) Dopamine D2 receptors in the nucleus accumbens are important for social attachment in female prairie voles (Microtus ochrogaster). Behav Neurosci 114:173-183[Web of Science][Medline].
- Hokfelt T, Martensson R, Bjorklund A, Kleinau S, Goldstein M (1984) Distributional maps of tyrosine-hydroxylase-immunoreactive neurons in the rat brain. In: Handbook of chemical neuroanatomy (Bjorklund A, Hokfelt T, eds), pp 277-379. Amsterdam: Elsevier.
- Hull EM, Eaton RC, Markowski VP, Moses J, Lumley LA, Loucks JA (1992) Opposite influence of medial preoptic D1 and D2 receptors on genital reflexes: implications for copulation. Life Sci 51:1705-1713[Web of Science][Medline].
- Ikemoto S, Panksepp J (1999) The role of nucleus accumbens dopamine in motivated behavior: a unifying interpretation with special reference to reward-seeking. Brain Res Brain Res Rev 31:6-41[Medline].
- Insel TR, Hulihan TJ (1995) A gender-specific mechanism for pair bonding: oxytocin and partner-preference formation in monogamous voles. Behav Neurosci 109:782-789[Web of Science][Medline].
- Insel TR, Shapiro LE (1992) Oxytocin receptor distribution reflects social organization in monogamous and polygamous voles. Proc Natl Acad Sci USA 89:5981-5985
[Abstract/Free Full Text] .- Insel TR, Young LJ (2001) The neurobiology of attachment. Nat Rev Neurosci 2:129-136[Web of Science][Medline].
- Insel TR, Wang ZX, Ferris CF (1994) Patterns of brain vasopressin receptor distribution associated with social organization in microtine rodents. J Neurosci 14:5381-5392[Abstract].
- Insel TR, Preston S, Winslow JT (1995) Mating in the monogamous male: behavioral consequences. Physiol Behav 57:615-627[Medline].
- Jansson A, Goldstein M, Tinner B, Zoli M, Meador-Woodruff JH, Lew JY, Levey AI, Watson S, Agnati LF, Fuxe K (1999) On the distribution patterns of D1, D2, tyrosine hydroxylase and dopamine transporter immunoreactivities in the ventral striatum of the rat. Neuroscience 89:473-489[Web of Science][Medline].
- Kelley AE, Berridge KC (2002) The neuroscience of natural rewards: relevance to addictive drugs. J Neurosci 22:3306-3311
[Free Full Text] .- Lim MM, Young LJ (2002) Blockade of vasopressin V1a receptors in the ventral pallidum prevents partner-preference formation in monogamous male prairie voles. Soc Neurosci Abstr 28:89.2.
- Liu Y, Wang ZX (2002) Both dopamine and oxytocin receptors are required for partner-preference formation in female prairie voles. Soc Neurosci Abstr 28:90.2.
- Liu Y, Curtis JT, Wang ZX (2001) Vasopressin in the lateral septum regulates pair bond formation in male prairie voles (Microtus ochrogaster). Behav Neurosci 115:910-919[Web of Science][Medline].
- Mas M, Fumero B, Gonzalez-Mora JL (1995) Voltammetric and microdialysis monitoring of brain monoamine neurotransmitter release during sociosexual interactions. Behav Brain Res 71:69-79[Web of Science][Medline].
- McGuire B, Novak M (1984) A comparison of maternal behaviour in the meadow vole (Microtus pennsylvanicus), prairie vole (M. ochrogaster) and pine vole (M. pinetorum). Anim Behav 32:1132-1141.
- Mikkelsen EJ, Detlor J, Cohen DJ (1981) School avoidance and social phobia triggered by haloperidol in patients with Tourette's disorder. Am J Psychiatry 138:1572-1576
[Abstract/Free Full Text] .- Missale C, Nash SR, Robinson SW, Jaber M, Caron MG (1998) Dopamine receptors: from structure to function. Physiol Rev 78:189-225
[Abstract/Free Full Text] .- Nesse RM, Berridge KC (1997) Psychoactive drug use in evolutionary perspective. Science 278:63-66
[Abstract/Free Full Text] .- Nirenberg MJ, Chan J, Pohorille A, Vaughan RA, Uhl GR, Kuhar MJ, Pickel VM (1997) The dopamine transporter: comparative ultrastructure of dopaminergic axons in limbic and motor compartments of the nucleus accumbens. J Neurosci 17:6899-6907
[Abstract/Free Full Text] .- Nobrega JN, Gernert M, Loscher W, Raymond R, Belej T, Richter A (1999) Tyrosine hydroxylase immunoreactivity and [3H]WIN 35,428 binding to the dopamine transporter in a hamster model of idiopathic paroxysmal dystonia. Neuroscience 92:211-217[Web of Science][Medline].
- Oliveras D, Novak M (1986) A comparison of paternal behaviour in the meadow vole Microtus pennsylvanicus, the pine vole M. pinetorum and the prairie vole M. ochrogaster. Anim Behav 34:519-526[Web of Science].
- Paxinos G, Watson C (1986) In: The rat brain in stereotaxic coordinates, Ed 2. San Diego: Academic.
- Pfaus JG, Damsma G, Nomikos GG, Wenkstern DG, Blaha CD, Phillips AG, Fibiger HC (1990) Sexual behavior enhances central dopamine transmission in the male rat. Brain Res 530:345-348[Web of Science][Medline].
- Pitkow LJ, Sharer CA, Ren X, Insel TR, Terwilliger EF, Young LJ (2001) Facilitation of affiliation and pair-bond formation by vasopressin receptor gene transfer into the ventral forebrain of a monogamous vole. J Neurosci 21:7392-7396
[Abstract/Free Full Text] .- Radhakishun FS, Van Ree JM (1987) The hypomotility elicited by small doses of apomorphine seems exclusively mediated by dopaminergic systems in the nucleus accumbens. Eur J Pharmacol 137:41-47[Web of Science][Medline].
- Robbins TW, Everitt BJ (1996) Neurobehavioural mechanisms of reward and motivation. Curr Opin Neurobiol 6:228-236[Web of Science][Medline].
- Salamone JD, Steinpreis RE, McCullough LD, Smith P, Grebel D, Mahan K (1991) Haloperidol and nucleus accumbens dopamine depletion suppress lever pressing for food but increase free food consumption in a novel food choice procedure. Psychopharmacology 104:515-521[Medline].
- Schneier FR, Liebowitz MR, Abi-Dargham A, Zea-Ponce Y, Lin SH, Laruelle M (2000) Low dopamine D(2) receptor binding potential in social phobia. Am J Psychiatry 157:457-459
[Abstract/Free Full Text] .- Self DW, Barnhart WJ, Lehman DA, Nestler EJ (1996) Opposite modulation of cocaine-seeking behavior by D1- and D2-like dopamine receptor agonists. Science 271:1586-1589[Abstract].
- Self DW, Genova LM, Hope BT, Barnhart WJ, Spencer JJ, Nestler EJ (1998) Involvement of cAMP-dependent protein kinase in the nucleus accumbens in cocaine self-administration and relapse of cocaine-seeking behavior. J Neurosci 18:1848-1859
[Abstract/Free Full Text] .- Shippenberg TS, Bals-Kubik R, Herz A (1993) Examination of the neurochemical substrates mediating the motivational effects of opioids: role of the mesolimbic dopamine system and D-1 vs. D-2 dopamine receptors. J Pharmacol Exp Ther 265:53-59
[Abstract/Free Full Text] .- Smith MT, Pencea V, Wang ZX, Luskin MB, Insel TR (2001) Increased number of BrdU-labeled neurons in the rostral migratory stream of the estrous prairie vole. Horm Behav 39:11-21[Medline].
- Van Ree JM, Wolterink G (1981) Injection of low doses of apomorphine into the nucleus accumbens of rats reduces locomotor activity. Eur J Pharmacol 72:107-111[Web of Science][Medline].
- Volkmar FR (2001) Pharmacological interventions in autism: theoretical and practical issues. J Clin Child Psychol 30:80-87[Web of Science][Medline].
- Voorn P, Jorritsma-Byham B, Van Dijk C, Buijs RM (1986) The dopaminergic innervation of the ventral striatum in the rat: a light- and electron-microscopical study with antibodies against dopamine. J Comp Neurol 251:84-99[Web of Science][Medline].
- Wang Y, Lavond DG, Chambers KC (1997) The effects of cooling the area postrema of male rats on conditioned taste aversions induced by LiC1 and apomorphine. Behav Brain Res 82:149-158[Web of Science][Medline].
- Wang ZX, Yu G, Cascio C, Liu Y, Gingrich B, Insel TR (1999) Dopamine D2 receptor-mediated regulation of partner preferences in female prairie voles (Microtus ochrogaster): a mechanism for pair bonding? Behav Neurosci 113:602-611[Web of Science][Medline].
- Williams JR, Catania KC, Carter CS (1992) Development of partner preferences in female prairie voles (Microtus ochrogaster): the role of social and sexual experience. Horm Behav 26:339-349[Medline].
- Williams JR, Insel TR, Harbaugh CR, Carter CS (1994) Oxytocin administered centrally facilitates formation of a partner preference in female prairie voles (Microtus ochrogaster). J Neuroendocrinol 6:247-250[Web of Science][Medline].
- Winslow JT, Hastings N, Carter CS, Harbaugh CR, Insel TR (1993) A role for central vasopressin in pair bonding in monogamous prairie voles. Nature 365:545-548[Medline].
- Wise RA (1996) Neurobiology of addiction. Curr Opin Neurobiol 6:243-251[Web of Science][Medline].
- Young LJ, Wang ZX, Insel TR (1998) Neuroendocrine bases of monogamy. Trends Neurosci 21:71-75[Web of Science][Medline].
- Young LJ, Lim MM, Gingrich B, Insel TR (2001) Cellular mechanisms of social attachment. Horm Behav 40:133-138[Medline].
- Zahm DS (2000) An integrative neuroanatomical perspective on some subcortical substrates of adaptive responding with emphasis on the nucleus accumbens. Neurosci Biobehav Rev 24:85-105[Web of Science][Medline].
Copyright © 2003 Society for Neuroscience 0270-6474/03/2383483-08$05.00/0
This article has been cited by other articles:
B. J. Aragona and Z. Wang
Opposing Regulation of Pair Bond Formation by cAMP Signaling within the Nucleus Accumbens Shell
J. Neurosci., November 28, 2007; 27(48): 13352 - 13356.
[Abstract] [Full Text] [PDF]
D. Meyer
Selective Serotonin Reuptake Inhibitors and Their Effects on Relationship Satisfaction
The Family Journal, October 1, 2007; 15(4): 392 - 397.
[Abstract] [PDF]
E. A.D Hammock and L. J Young
Oxytocin, vasopressin and pair bonding: implications for autism
Phil Trans R Soc B, December 29, 2006; 361(1476): 2187 - 2198.
[Abstract] [Full Text] [PDF]
H. P. Nair and L. J. Young
Vasopressin and Pair-Bond Formation: Genes to Brain to Behavior
Physiology, April 1, 2006; 21(2): 146 - 152.
[Abstract] [Full Text] [PDF]
L. Huang, H. Maaswinkel, and L. Li
Olfactoretinal centrifugal input modulates zebrafish retinal ganglion cell activity: a possible role for dopamine-mediated Ca2+ signalling pathways
J. Physiol., December 15, 2005; 569(3): 939 - 948.
[Abstract] [Full Text] [PDF]
A. Nicot, T. Otto, P. Brabet, and E. M. DiCicco-Bloom
Altered Social Behavior in Pituitary Adenylate Cyclase-Activating Polypeptide Type I Receptor-Deficient Mice
J. Neurosci., October 6, 2004; 24(40): 8786 - 8795.
[Abstract] [Full Text] [PDF]
This Article Abstract 
Full Text (PDF) Submit an eLetter Alert me when this article is cited Alert me when eLetters are posted Alert me if a correction is posted Citation Map Services Email this article to a friend Similar articles in this journal Similar articles in Web of Science Similar articles in PubMed Alert me to new issues of the journal Download to citation manager 
Citing Articles Citing Articles via HighWire Citing Articles via Web of Science (58) Citing Articles via Google Scholar Google Scholar Articles by Aragona, B. J. Articles by Wang, Z. Search for Related Content PubMed PubMed Citation Articles by Aragona, B. J. Articles by Wang, Z. Pubmed/NCBI databases
Compound via MeSH
Hazardous Substances DB
|
|
|
|
 |
|