2019
DOI: 10.1038/s41386-019-0371-2
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Selective D2 and D3 receptor antagonists oppositely modulate cocaine responses in mice via distinct postsynaptic mechanisms in nucleus accumbens

Abstract: The dopamine D 3 receptor (D 3 R) has emerged as a promising pharmacotherapeutic target for the treatment of several diseases including schizophrenia, Parkinson's disease, and substance use disorders. However, studies investigating the D 3 R's precise role in dopamine neurotransmission or how it may be exploited to modulate responses to drugs of abuse have produced contrasting results, in part because most D 3 R-targeted compounds often also interact with D 2 receptors (D 2 R). To resolve this issue, we set ou… Show more

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Cited by 28 publications
(22 citation statements)
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“…One key question remaining is how pretreatment with PG01037 attenuates opioidinduced hyperactivity (present results) but potentiates cocaine-induced hyperactivity (Manvich et al, 2019). The enhancement of cocaine-induced locomotion by D3R antagonism occurs coincidentally with an increase in DA-induced excitability and activity of DA D1 receptorexpressing MSNs within the NAc (Manvich et al, 2019). However, it is unknown whether this or other modulations of MSN activity within the NAc underlie the inhibitory influence of D3R antagonism on opioid-induced hyperlocomotion.…”
Section: Pg01037 and Modulation Of Locomotor Activity: Potential Mechmentioning
confidence: 69%
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“…One key question remaining is how pretreatment with PG01037 attenuates opioidinduced hyperactivity (present results) but potentiates cocaine-induced hyperactivity (Manvich et al, 2019). The enhancement of cocaine-induced locomotion by D3R antagonism occurs coincidentally with an increase in DA-induced excitability and activity of DA D1 receptorexpressing MSNs within the NAc (Manvich et al, 2019). However, it is unknown whether this or other modulations of MSN activity within the NAc underlie the inhibitory influence of D3R antagonism on opioid-induced hyperlocomotion.…”
Section: Pg01037 and Modulation Of Locomotor Activity: Potential Mechmentioning
confidence: 69%
“…It is possible that PG01037 potentiates drug-induced hyperactivity that is DA-dependent but attenuates drug-induced hyperactivity that is DAindependent. This hypothesis is further supported by findings that intra-NAc administration of a selective D3R antagonist potentiates the locomotor-activating effects of cocaine (Manvich et al, 2019) but attenuates the locomotor-activating effects of morphine (Liang et al, 2011).…”
Section: Pg01037 and Modulation Of Locomotor Activity: Potential Mechmentioning
confidence: 70%
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“…25 Furthermore, the selective antagonism of D3DR has been shown to enhance the stimulant behavior effects of cocaine in mice, which is opposite to the effect produced by selective antagonism of D2DR or nonselective D 2 -like receptor antagonists. 26 Also, selective antagonist binding at the D 3 receptor has been shown to display promising results in reducing cocaine, and opioid reward and are highly effective in mitigating relapse to drug-seeking behavior in preclinical models. [27][28][29] Extensive medicinal chemistry research efforts had led to the development of D 3 dopamine receptor selective partial agonists and antagonists such as BP 897, NGB 2904, SB 277011A, and GSK598809.…”
mentioning
confidence: 99%