Serotonergic Neurotransmission System Modulator, Vortioxetine, and Dopaminergic D2/D3 Receptor Agonist, Ropinirole, Attenuate Fibromyalgia-Like Symptoms in Mice

Sałat, Kinga; Furgała-Wojas, Anna

doi:10.3390/molecules26082398

Cited by 12 publications

(13 citation statements)

References 99 publications

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“…Recent researches revealed that VRT is also involved in the modulation of the glutamatergic and gammaaminobutyric acid (GABA)ergic neurotransmission in the specific brain regions [38]. Moreover, animal studies demonstrated the antinociceptive effects of VRT in sciatic nerve constriction [39] and oxaliplatin-induced neuropathy [40] or reserpine-induced fibromyalgia in mice [41]. Some researches proved the antinociceptive effects of carrageenan-induced paw inflammation in mice [42], but others noted the lack of influence of this antidepressant in the inflammatory neuropathic pain [39].…”

Section: Resultsmentioning

confidence: 99%

The Analgezic Effect of Vortioxetine on somatic and visceral Pain using the mouse models

2022

pnr

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Experimental investigation of the vortioxetine effects on somatic and visceral nociception in mice. Material and method: We used healthy, non-genetically modified white Swiss mice (20-25 g), randomly assigned in 3 groups of 6 animals each, treated orally 14 consecutive days, as follows: Group I (DW): distilled water 0,1 ml/10 g body weight, Group 2 (VRT): 20 mg/kbw vortioxetine. In the 14 th day of the experiment the Group 3 (KET) received the positive control drug ketoprofen (15 mg/kbw), 15 minutes before the performing the tests. The somatic pain testing was performed using hot plate assay. The writhing test based on chemical peritoneal irritation induced by diluted acetic acid (0,6%) was used as standardized visceral pain model. The data were statistically analyzed using SPSS variant 17.0 for Windows and ANOVA one-way method. The research protocol was approved by the Grigore T. Popa University`s Committee for Research and Ethical Issues. Results: Ketoprofen showed a substantial and progressive prolongation in reaction time in hot plate test, respectively a decrease in the behavioral manifestations in writhing test. The administration of vortioxetine resulted in a considerable increase in the time response to thermal noxious paws stimulation in hot plate test, and a diminution in the number of writhes in writhing test. Conclusion:Using the mouse models of acute pain hot plate analgesia meter and acid acetic writhing test, we revealed that the oral administration of vortioxetine during 14 days resulted in significant somatic and visceral analgesic effects, but less intense than of ketoprofen.

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Section: Resultsmentioning

confidence: 99%

The Analgezic Effect of Vortioxetine on somatic and visceral Pain using the mouse models

2022

pnr

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“…Учитывая способность АДР снижать неприятные ощущения в ногах при СБН, а также их антидепрессивный эффект, возник интерес к применению данной группы препаратов у пациентов с таким тяжелым аффективноболевым расстройством, как фибромиалгия. Она является заболеванием с низким порогом восприятия боли, аффективными расстройствами и мышечной слабостью [21]. В основе его лежит сложная дисфункция нервной системы без пускового фактора, что представляет серьезную проблему для диагностики, лечения и профилактики данного заболевания.…”

Section: терапия фибромиалгииunclassified

“…Исследование на мышах с химически индуцированными фибромиалгическими симптомами, вызванными подкожным введением резерпина, позволило оценить эффективность препаратов СИОЗС вортиоксетина и АДР ропинирола на болевой порог, выраженность депрессии и тревоги, а также двигательные нарушения. Внутрибрюшинное введение вортиоксетина и ропинирола в дозе 10 мг/кг купировало тактильную аллодинию, при этом ропинирол проявлял свойства, подобные антидепрессантам, а вортиоксетинподобные анксиолитикам, что можно учитывать при определении ведущих симптомов болезни [21,22]. Интересен тот факт, что в другом исследовании у пациентов с ИКР часто в анамнезе был диагноз фибромиалгии, что вновь возвращает к мысли о возможной генетической предрасположенности к развитию такого симптомокомплекса на фоне врожденных особенностей нейромедиаторной передачи [23].…”

Section: терапия фибромиалгииunclassified

Dopamine receptor agonists: standard and non-standard applications in medicine

2022

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Dopamine receptor agonists (DRA) are a class of therapeutic drugs able to directly stimulate dopaminergic receptors facilitating a stronger effect of the endogenous dopamine, which is widely used in treatment of diseases that are accompanied with dopaminergic neurotransmission deficiency. A classical hypodopaminergic condition is Parkinson’s disease and DRA are traditionally associated with it. However, even the first DRA, Bromocriptine, widely adopted in PD treatment, was initially registered as a medication for treatment of prolactinaemia and associated pituitary adenomas and is still widely used in gynecology and endocrinology. In several countries DRA are used in treatment of diabetes, eating disorders, and addictions. Dopamine is the cardinal neurotransmitter of the emotional control and the main neurotransmitter of the reward system, and that defines the interest for researching the dopaminergic agents in treatment of primarily mental illnesses, as well as correction of secondary affective disorders. The experimental effectiveness of ADR in slowing down the rate of progression of the neurodegenerative process in severe incurable diseases, as well as potential neuroprotection in cerebrovascular insufficiency, will allow in the future to determine the criteria for the use of ADR in these non-standard situations, which may even lead to a change in clinical recommendations for the treatment of individual nosologies. Presented in this article are both traditional uses of DRA and an overview of non-standard applications of this class of medications with a discussion of recent studies. In the future, the likelihood of a rethinking of ADRs as a class of only antiparkinsonian drugs, with the expansion of their therapeutic indications.

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“…Two main models of fibromyalgia-like conditions have been described to mimic altered, long-lasting, reflexive and nonreflexive pain-related behaviors [ 7 ]. In an experimental model of reserpine-induced myalgia (RIM3) with three injections of reserpine, the effect of various drugs has been tested in mice, including TRPV1 receptor antagonists [ 8 ], serotonin transporters inhibitors [ 9 ], bradykinin receptor antagonists [ 10 ], ligands of the nociceptin/orphanin FQ receptor [ 11 ], dopaminergic receptor agonists [ 12 ], toxins [ 13 , 14 , 15 ], gabapentinoids [ 14 ], resolvins [ 16 ], and plant-based polyphenol products [ 17 , 18 , 19 ]. In mice subjected to intramuscular injection of acidified saline solution (ASI), the effect of gabapentinoids [ 7 ] and plant-based polyphenol products [ 20 ] has also been tested.…”

Section: Introductionmentioning

confidence: 99%

Long-Lasting Nociplastic Pain Modulation by Repeated Administration of Sigma-1 Receptor Antagonist BD1063 in Fibromyalgia-like Mouse Models

Bagó-Mas

Deulofeu

Vela³

et al. 2022

IJMS

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Sigma-1 receptor (s1R) ligands have been shown to be effective at relieving neuropathic and inflammatory pain, but have not yet been tested in experimental models of fibromyalgia. The objective of this study was to evaluate the effect of a s1R antagonist (BD1063) compared to pregabalin. ICR-CD1 female mice were subjected to either six repeated injections of reserpine, to cause reserpine-induced myalgia (RIM6), or acidified saline intramuscular injections (ASI). In these two models, we evaluated the effect of BD1063 and pregabalin on thermal hypersensitivity, anxiety-like and depression-like behaviors, and on spinal cord gliosis. BD1063 exerted an antinociceptive effect on both reflexive (thermal hyperalgesia) and nonreflexive (anxiety- and depression-like) pain behaviors, and reduced spinal astroglial and microglial reactivity, following repeated treatment for 2 weeks. Interestingly, the effects of BD1063 were long-term, lasting several weeks after treatment discontinuation in both fibromyalgia-like models. Similar results were obtained with pregabalin, but the effects on pain behaviors lasted for a shorter length of time, and pregabalin did not significantly modulate spinal glial reactivity. The inhibitory and long-lasting effect of pharmacological blockade of s1Rs on both sensory and affective dimensions of nociplastic-like pain and spinal cord gliosis in two experimental models of fibromyalgia support the application of this therapeutic strategy to treat fibromyalgia.

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Serotonergic Neurotransmission System Modulator, Vortioxetine, and Dopaminergic D2/D3 Receptor Agonist, Ropinirole, Attenuate Fibromyalgia-Like Symptoms in Mice

Cited by 12 publications

References 99 publications

The Analgezic Effect of Vortioxetine on somatic and visceral Pain using the mouse models

The Analgezic Effect of Vortioxetine on somatic and visceral Pain using the mouse models

Dopamine receptor agonists: standard and non-standard applications in medicine

Long-Lasting Nociplastic Pain Modulation by Repeated Administration of Sigma-1 Receptor Antagonist BD1063 in Fibromyalgia-like Mouse Models

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