Prospects for the Personalized Multimodal Therapy Approach to Pain Management via Action on NO and NOS

Shnayder, Natalia A.; Петрова, М. М.; Попова, Т. Е.; Davidova, T.; Боброва, О. П.; Trefilova, Vera V.; Goncharova, P. S.; Balberova, Olga V; Petrov, K. V.; Gavrilyuk, Oksana A.; Соловьева, И. А.; Medvedev, German V.; Насырова, Р. Ф.

doi:10.3390/molecules26092431

Cited by 14 publications

(8 citation statements)

References 117 publications

(153 reference statements)

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“…In literature, there are poor knowledge about the relationship between orofacial nociception and NO [35,40]. Nevertheless, it has been demonstrated that nNOS [17] and iNOS [41,42] might play a critical role in central mechanisms of the development and/or maintenance of inflammatory pain, supporting our results. Other studies demonstrated the nNOS expression at trigeminal level not only in mammals [43][44][45][46] but also in birds and in reptiles [47].…”

Section: Discussionsupporting

confidence: 87%

Peripheral Purinergic Modulation in Pediatric Orofacial Inflammatory Pain Affects Brainstem Nitroxidergic System: A Translational Research

Borsani

Ballini

Buffoli

et al. 2022

BioMed Research International

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Physiology of orofacial pain pathways embraces primary afferent neurons, pathologic changes in the trigeminal ganglion, brainstem nociceptive neurons, and higher brain function regulating orofacial nociception. The goal of this study was to investigate the nitroxidergic system alteration at brainstem level (spinal trigeminal nucleus), and the role of peripheral P2 purinergic receptors in an experimental mouse model of pediatric inflammatory orofacial pain, to increase knowledge and supply information concerning orofacial pain in children and adolescents, like pediatric dentists and pathologists, as well as oro-maxillo-facial surgeons, may be asked to participate in the treatment of these patients. The experimental animals were treated subcutaneously in the perioral region with pyridoxalphosphate-6-azophenyl-2 ′ ,4 ′ -disulphonic acid (PPADS), a P2 receptor antagonist, 30 minutes before formalin injection. The pain-related behavior and the nitroxidergic system alterations in the spinal trigeminal nucleus using immunohistochemistry and western blotting analysis have been evaluated. The local administration of PPADS decreased the face-rubbing activity and the expression of both neuronal and inducible nitric oxide (NO) synthase isoforms in the spinal trigeminal nucleus. These results underline a relationship between orofacial inflammatory pain and nitroxidergic system in the spinal trigeminal nucleus and suggest a role of peripheral P2 receptors in trigeminal pain transmission influencing NO production at central level. In this way, orofacial pain physiology should be elucidated and applied to clinical practice in the future.

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Section: Discussionsupporting

confidence: 87%

Peripheral Purinergic Modulation in Pediatric Orofacial Inflammatory Pain Affects Brainstem Nitroxidergic System: A Translational Research

Borsani

Ballini

Buffoli

et al. 2022

BioMed Research International

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“…In contrast, the amounts of GPCR Prkar1b ( Marbach et al, 2021 ), P2ry12 ( Defaye et al, 2021 ), and Htr2c ( Brasch-Andersen et al, 2011 ) in the TG were dramatically decreased after CFA injection. For the ion channels, we observed that the noticeably elevated expression of Rapgef3 ( Liu et al, 2021 ), Nos1 ( Shnayder et al, 2021 ), TRPM8 ( Weyer and Lehto, 2017 ), and CXCL12 ( Luo et al, 2016 ) in the TG were remarkably increased after CFA injection. On the contrary, the levels of ion channel transcripts for Sgk3 ( Liu et al, 2015 ) was significantly reduced in the TG after CFA injection.…”

Section: Resultsmentioning

confidence: 94%

RNA sequencing profiling of mRNAs, long noncoding RNAs, and circular RNAs in Trigeminal Ganglion following Temporomandibular Joint inflammation

Liu

Zhao

Han

et al. 2022

Front. Cell Dev. Biol.

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Patients with temporomandibular joint disorders (TMD) have high levels of inflammatory pain-related disability, which seriously affects their physical and mental health. However, an effective treatment is yet to be developed. Both circular RNAs (circRNAs) and long noncoding RNAs (lncRNAs) contribute to regulating pain conduction. In our current study, we report the expression profiles of circRNAs, lncRNAs, and mRNAs in the trigeminal ganglion (TG) associated with complete Freund’s adjuvant (CFA)-induced TMD inflammation pain. The collected TGs from the experimental (CFA) and control (saline) groups were processed for deep RNA sequencing. Overall, 1078,909,068 clean reads were obtained. A total of 15,657 novel lncRNAs were identified, where 281 lncRNAs were differentially expressed on CFA3D and 350 lncRNAs were differentially expressed on CFA6D. In addition, a total of 55,441 mRNAs and 27,805 circRNAs were identified, where 3,914 mRNAs and 91 circRNAs were found differentially expressed, between the CFA3D and saline groups, while 4,232 mRNAs and 98 DE circRNAs were differentially expressed between the CFA6D and saline groups. Based on functional analyses, we found that the most significant enriched biological processes of the upregulated mRNAs were involved in the immunity, neuron projection, inflammatory response, MAPK signaling pathway, Ras signaling pathway, chemokine signaling pathway, and inflammatory response in TG. Further analyses of Gene Ontology and the Kyoto Encyclopedia of Genes and Genomes pathway suggest the involvement of dysregulated genes in the pain occurrence mechanism. Our findings provide a resource for expression patterns of gene transcripts in regions related to pain. These results suggest that apoptosis and neuroinflammation are important pathogenic mechanisms underlying TMD pain. Some of the reported differentially expressed genes might be considered promising therapeutic targets. The current research study revealed the expression profiles of circRNAs, lncRNAs, and mRNAs during TMD inflammation pain and sheds light on the roles of circRNAs and lncRNAs underlying the pain pathway in the trigeminal system of TMD inflammation pain.

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“…As reviewed by Shnayder N.A. et al, in patients with peripheral chronical pain syndromes, an association can be found between single-nucleotide variants of NOS1 , NOS2 , and NOS3 genes encoding nNOS, iNOS, and eNOS and acute and chronic peripheral pain [ 12 ]. Therefore, the administration of the appropriate NOS inhibitor could be considered as a new personalized pharmacotherapy strategy.…”

Section: Special Issue Overviewmentioning

confidence: 99%

Preface to Nitric Oxide Modulators in Health and Disease I

Maccallini

Amoroso

2022

Molecules

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Prospects for the Personalized Multimodal Therapy Approach to Pain Management via Action on NO and NOS

Cited by 14 publications

References 117 publications

Peripheral Purinergic Modulation in Pediatric Orofacial Inflammatory Pain Affects Brainstem Nitroxidergic System: A Translational Research

Peripheral Purinergic Modulation in Pediatric Orofacial Inflammatory Pain Affects Brainstem Nitroxidergic System: A Translational Research

RNA sequencing profiling of mRNAs, long noncoding RNAs, and circular RNAs in Trigeminal Ganglion following Temporomandibular Joint inflammation

Preface to Nitric Oxide Modulators in Health and Disease I

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