Allosteric Modulators of Dopamine D2 Receptors for Fine-Tuning of Dopaminergic Neurotransmission in CNS Diseases: Overview, Pharmacology, Structural Aspects and Synthesis

Kaczor, Agnieszka A.; Wróbel, Tomasz M.; Bartuzi, Damian

doi:10.3390/molecules28010178

Cited by 10 publications

(5 citation statements)

References 120 publications

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“…In this regard, the primary reinforcing effects of abuse substances have been linked to the elevation of dopamine in the nucleus accumbens by either stimulating the dopamine neurons in the VTA or inhibiting the reuptake of the dopamine in the NAc [ 3 ]. Dopamine-receptors (DA-receptors) are widely distributed in the brain (mainly in the central nervous system and peripheral nervous system), play a key role in reward-related phenomena (in the ventral tegmental area), and are divided into two pharmacological families: D1-like receptors (D1R subtype—with effects on memory, attention, locomotion, impulse control, and regulation of renal function, and D5R subtype—with effects on decision making, cognition, attention, and renin secretion) and D2-like receptors (D2R subtype—with effects on locomotion, learning, attention, memory, sleep, D3R subtype—with effects on cognition, sleep, impulse control, attention, and DRD4 subtype—with effects on cognition, sleep, attention, and impulse control) [ 13 , 14 , 15 , 16 ]. The distribution and function of peripheral dopamine receptors have been described by Missale et al in 1988 and outlined effects such as inhibition of norepinephrine release (D2-like) and vasodilation (D1-like) on blood vessels, inhibition of aldosterone secretion (D2-like), stimulation of epinephrine/norepinephrine release (D1-like) and inhibition of epinephrine/norepinephrine release (D2-like) on the adrenal gland, increase of filtration rate (D1-like), stimulation of renin secretion (D1-like), inhibition of Na+ reabsorption (D1-like), inhibition of vasopressin action (d2-like), and inhibition of norepinephrine release (D2-like) on kidneys [ 14 ].…”

Section: Resultsmentioning

confidence: 99%

Understanding the Mechanisms of Action and Effects of Drugs of Abuse

et al. 2023

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Aim. Drug abuse and addiction are major public health concerns, with millions of people worldwide affected by the negative consequences of drug use. To better understand this complex issue, a review was conducted to examine the mechanisms of action and effects of drugs of abuse, including their acute and chronic effects, the symptoms of abstinence syndrome, as well as their cardiovascular impacts. Methods. The analyzed data were obtained after surveying an electronic database, namely PubMed, with no time limit, grey literature sources, and reference lists of relevant articles. Results. The review highlights the different categories of drugs of abuse, such as opioids, stimulants, depressants, hallucinogens, and cannabis, and discusses the specific ways that each drug affects the brain and body. Additionally, the review explores the short-term and long-term effects of drug abuse on the body and mind, including changes in brain structure and function, physical health problems, and mental health issues, such as depression and anxiety. In addition, the review explores the effects of drug abuse on cardiovascular health, focusing on electrocardiogram changes. Moreover, the analysis of relevant literature also highlighted possible genetic susceptibility in various addictions. Furthermore, the review delves into the withdrawal symptoms that occur when someone stops using drugs of abuse after a period of chronic use. Conclusion. Overall, this review provides a comprehensive overview of the current state of knowledge on drug abuse and addiction. The findings of this review can inform the development of evidence-based prevention and intervention strategies to address this critical public health issue.

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Section: Resultsmentioning

confidence: 99%

Understanding the Mechanisms of Action and Effects of Drugs of Abuse

et al. 2023

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“…Another approach is to develop D2 receptor allosteric modulators, which bind to a distinct site from the orthosteric site and enhance or inhibit the binding and efficacy of the endogenous ligand or other drugs. For instance, PAOPA is a positive allosteric modulator of D2 receptors, which increases the affinity and potency of dopamine and D2 receptor agonists, and reverses the motor and cognitive impairments induced by D2 receptor antagonists [228,229]. In addition, a novel modulator of dopamine D2 receptors for the treatment of drug dependence exerts its therapeutic effect by suppressing the interaction between D2L receptors and FABP3 [127].…”

Section: Dopamine D2-like Receptors As Therapeutic Targetsmentioning

confidence: 99%

Dopamine D1–D5 Receptors in Brain Nuclei: Implications for Health and Disease

Kawahata,

Finkelstein,

Fukunaga

2024

Receptors

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Understanding the intricate role of dopamine D1–D5 receptors is pivotal in addressing the challenges posed by the aging global population, as well as by social stress and advancing therapeutic interventions. Central to diverse brain functions such as movement, cognition, motivation, and reward, dopamine receptors are ubiquitously distributed across various brain nuclei. This comprehensive review explores the nuanced functions of each dopamine receptor, D1, D2, D3, D4, and D5, in distinct brain regions, elucidating the alterations witnessed in several neurological and psychiatric disorders. From the substantia nigra and ventral tegmental area, crucial for motor control and reward processing, to the limbic system influencing emotional responses, motivation, and cognitive functions, each brain nucleus reveals a specific involvement of dopamine receptors. In addition, genetic variations in dopamine receptors affect the risk of developing schizophrenia and parkinsonism. The review further investigates the physiological significance and pathogenic impacts of dopamine receptors in critical areas like the prefrontal cortex, hypothalamus, and striatum. By unraveling the complexities of dopamine receptor biology, especially those focused on different brain nuclei, this review provides a foundation for understanding their varied roles in health and disease, which is essential for the development of targeted therapeutic strategies aimed at mitigating the impact of aging and mental health on neurological well-being.

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“…The choice of these receptors is due to rather extensive information about their allosteric sites and the diversity of their endogenous and synthetic allosteric regulators, including autoantibodies and synthetic pepducins. At the same time, for a number of other GPCRs, there is also a lot of data on allosteric regulation and their analysis is presented in a number of recent comprehensive reviews and analytical articles: for muscarinic acetylcholine receptors [ 171 , 172 , 173 , 174 ], for metabotropic glutamate receptors [ 171 , 175 , 176 ], for 5-hydroxytryptamine (serotonin) receptors [ 177 , 178 ], for dopamine receptors [ 177 , 179 ], for opioid receptors [ 178 , 180 , 181 ], for cannabinoid receptors [ 176 , 182 , 183 , 184 ], for adenosine receptors [ 185 ], for neuropeptide Y receptors [ 186 ], for melanocortin receptors [ 186 ], for angiotensin receptors [ 187 ], for glucagon-like peptide-1 receptors [ 176 , 188 ], and for free fatty acid receptors [ 58 ].…”

Section: Allosteric Sites In Different Families Of Gpcrsmentioning

confidence: 99%

Allosteric Regulation of G-Protein-Coupled Receptors: From Diversity of Molecular Mechanisms to Multiple Allosteric Sites and Their Ligands

2023

IJMS

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Allosteric regulation is critical for the functioning of G protein-coupled receptors (GPCRs) and their signaling pathways. Endogenous allosteric regulators of GPCRs are simple ions, various biomolecules, and protein components of GPCR signaling (G proteins and β-arrestins). The stability and functional activity of GPCR complexes is also due to multicenter allosteric interactions between protomers. The complexity of allosteric effects caused by numerous regulators differing in structure, availability, and mechanisms of action predetermines the multiplicity and different topology of allosteric sites in GPCRs. These sites can be localized in extracellular loops; inside the transmembrane tunnel and in its upper and lower vestibules; in cytoplasmic loops; and on the outer, membrane-contacting surface of the transmembrane domain. They are involved in the regulation of basal and orthosteric agonist-stimulated receptor activity, biased agonism, GPCR-complex formation, and endocytosis. They are targets for a large number of synthetic allosteric regulators and modulators, including those constructed using molecular docking. The review is devoted to the principles and mechanisms of GPCRs allosteric regulation, the multiplicity of allosteric sites and their topology, and the endogenous and synthetic allosteric regulators, including autoantibodies and pepducins. The allosteric regulation of chemokine receptors, proteinase-activated receptors, thyroid-stimulating and luteinizing hormone receptors, and beta-adrenergic receptors are described in more detail.

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Allosteric Modulators of Dopamine D2 Receptors for Fine-Tuning of Dopaminergic Neurotransmission in CNS Diseases: Overview, Pharmacology, Structural Aspects and Synthesis

Cited by 10 publications

References 120 publications

Understanding the Mechanisms of Action and Effects of Drugs of Abuse

Understanding the Mechanisms of Action and Effects of Drugs of Abuse

Dopamine D1–D5 Receptors in Brain Nuclei: Implications for Health and Disease

Allosteric Regulation of G-Protein-Coupled Receptors: From Diversity of Molecular Mechanisms to Multiple Allosteric Sites and Their Ligands

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