Your search keyword '"Erika Pintér"' showing total 194 results

1. Topiramate inhibits adjuvant-induced chronic orofacial inflammatory allodynia in the rat

Author

Violetta Mohos, Máté Harmat, Jozsef Kun, Tímea Aczél, Balázs Zoltán Zsidó, Tamás Kitka, Sándor Farkas, Erika Pintér, and Zsuzsanna Helyes

Subjects

topiramate, sumatriptan, orofacial pain, trigeminal activation, inflammatory pain, animal model, Therapeutics. Pharmacology, RM1-950

Abstract

Chronic orofacial pain disorders are common debilitating conditions, affecting the trigeminal system. Its underlying pathophysiological mechanisms are still unclear and the therapy is often unsatisfactory, therefore, preclinical models are crucial to identify the key mediators and novel treatment options. Complete Freund’s adjuvant (CFA)-induced orofacial inflammatory allodynia/hyperalgesia is commonly used in rodents, but it has not been validated with currently used drugs. Here we tested the effects of the adjuvant analgesic/antiepileptic voltage-gated Na+ channel blocker complex mechanism of action topiramate in comparison with the gold standard antimigraine serotonin 5-HT1B/D receptor agonist sumatriptan in this model. CFA was injected subcutaneously into the right whisker pad of male Sprague-Dawley rats (250–300 g), then mechanonociceptive threshold values were investigated with von Frey filaments (3, 5, and 7 days after CFA injection). Effects of topiramate (30 mg/kg per os) and sumatriptan (1 mg/kg subcutaneous) on the adjuvant-induced chronic inflammatory orofacial allodynia were investigated 60, 120, and 180 min after the treatments each day. To determine the optimal concentration for drug effect analysis, we tested the effects of two different CFA-concentrations (1 and 0.5 mg/mL) on mechanonociceptive thresholds. Both concentrations of CFA induced a chronic orofacial allodynia in 60% of all rats. Although, higher CFA concentration induced greater allodynia, much more stable threshold reduction was observed with the lower CFA concentration: on day 3 the thresholds decreased from 18.30 g to approximately 11 g (low) and 5 g (high), respectively, however a slight increase was observed in the case of higher CFA concentration (on days 5, 7, and 11). In all investigation days, topiramate showed significant anti-allodynic effect comparing the pre and post drug dose and comparing the vehicle treated to the drug treated groups. Sumatriptan also caused a significant threshold increase compared to pre dose thresholds (day 3) and also showed a slight anti-allodynic effect compared to the vehicle-treated group (day 3 and 5). In the present study CFA-induced chronic orofacial allodynia was reversed by topiramate in rats validating the model with the adjuvant analgesic. Other than establishing a validated orofacial pain-related syndrome model in rats, new ways are opened for the repurposing of topiramate.

Published

2024

2. The anti-inflammatory effect of dimethyl trisulfide in experimental acute pancreatitis

Author

Erik Márk Orján, Eszter Sára Kormányos, Gabriella Mihalekné Fűr, Ágnes Dombi, Emese Réka Bálint, Zsolt Balla, Beáta Adél Balog, Ágnes Dágó, Ahmad Totonji, Zoárd István Bátai, Eszter Petra Jurányi, Tamás Ditrói, Ammar Al-Omari, Gábor Pozsgai, Viktória Kormos, Péter Nagy, Erika Pintér, Zoltán Rakonczay, and Lóránd Kiss

Subjects

Medicine, Science

Abstract

Abstract Various organosulfur compounds, such as dimethyl trisulfide (DMTS), display anti-inflammatory properties. We aimed to examine the effects of DMTS on acute pancreatitis (AP) and its mechanism of action in both in vivo and in vitro studies. AP was induced in FVB/n mice or Wistar rats by caerulein, ethanol-palmitoleic acid, or L-ornithine-HCl. DMTS treatments were administered subcutaneously. AP severity was assessed by pancreatic histological scoring, pancreatic water content, and myeloperoxidase activity measurements. The behaviour of animals was followed. Pancreatic heat shock protein 72 (HSP72) expression, sulfide, and protein persulfidation were measured. In vitro acinar viability, intracellular Ca2+ concentration, and reactive oxygen species production were determined. DMTS dose-dependently decreased the severity of AP. It declined the pancreatic infiltration of leukocytes and cellular damage in mice. DMTS upregulated the HSP72 expression during AP and elevated serum sulfide and low molecular weight persulfide levels. DMTS exhibited cytoprotection against hydrogen peroxide and AP-inducing agents. It has antioxidant properties and modulates physiological but not pathophysiological Ca2+ signalling. Generally, DMTS ameliorated AP severity and protected pancreatic acinar cells. Our findings indicate that DMTS is a sulfur donor with anti-inflammatory and antioxidant effects, and organosulfur compounds require further investigation into this potentially lethal disease.

Published

2023

3. TRPA1 Covalent Ligand JT010 Modifies T Lymphocyte Activation

Author

Katalin Szabó, Géza Makkai, János Konkoly, Viktória Kormos, Balázs Gaszner, Tímea Berki, and Erika Pintér

Subjects

TRPA1, lymphocytes, monocytes, CD4+ cells, CD14+ cells, B cells, Microbiology, QR1-502

Abstract

Transient Receptor Potential Ankyrin 1 (TRPA1) is a non-selective cation channel involved in sensitivity to a plethora of irritating agents and endogenous mediators of oxidative stress. TRPA1 influences neuroinflammation and macrophage and lymphocyte functions, but its role is controversial in immune cells. We reported earlier a detectable, but orders-of-magnitude-lower level of Trpa1 mRNA in monocytes and lymphocytes than in sensory neurons by qRT-PCR analyses of cells from lymphoid organs of mice. Our present goals were to (a) further elucidate the expression of Trpa1 mRNA in immune cells by RNAscope in situ hybridization (ISH) and (b) test the role of TRPA1 in lymphocyte activation. RNAscope ISH confirmed that Trpa1 transcripts were detectable in CD14+ and CD4+ cells from the peritoneal cavity of mice. A selective TRPA1 agonist JT010 elevated Ca2+ levels in these cells only at high concentrations. However, a concentration-dependent inhibitory effect of JT010 was observed on T-cell receptor (TcR)-induced Ca2+ signals in CD4+ T lymphocytes, while JT010 neither modified B cell activation nor ionomycin-stimulated Ca2+ level. Based on our present and past findings, TRPA1 activation negatively modulates T lymphocyte activation, but it does not appear to be a key regulator of TcR-stimulated calcium signaling.

Published

2024

4. Elucidation of the binding mode of organic polysulfides on the human TRPA1 receptor

Author

Balázs Nemes, Szabolcs László, Balázs Zoltán Zsidó, Csaba Hetényi, Adam Feher, Ferenc Papp, Zoltan Varga, Éva Szőke, Zoltán Sándor, and Erika Pintér

Subjects

human TRPA1, site-directed mutagenesis, DMTS, DATS, DADS, binding site, Physiology, QP1-981

Abstract

Introduction: Previous studies have established that endogenous inorganic polysulfides have significant biological actions activating the Transient Receptor Potential Ankyrin 1 (TRPA1) receptor. Organic polysulfides exert similar effects, but they are much more stable molecules, therefore these compounds are more suitable as drugs. In this study, we aimed to better understand the mechanism of action of organic polysulfides by identification of their binding site on the TRPA1 receptor.Methods: Polysulfides can readily interact with the thiol side chain of the cysteine residues of the protein. To investigate their role in the TRPA1 activation, we replaced several cysteine residues by alanine via site-directed mutagenesis. We searched for TRPA1 mutant variants with decreased or lost activating effect of the polysulfides, but with other functions remaining intact (such as the effects of non-electrophilic agonists and antagonists). The binding properties of the mutant receptors were analyzed by in silico molecular docking. Functional changes were tested by in vitro methods: calcium sensitive fluorescent flow cytometry, whole-cell patch-clamp and radioactive calcium-45 liquid scintillation counting.Results: The cysteines forming the conventional binding site of electrophilic agonists, namely C621, C641 and C665 also bind the organic polysulfides, with the key role of C621. However, only their combined mutation abolished completely the organic polysulfide-induced activation of the receptor.Discussion: Since previous papers provided evidence that organic polysulfides exert analgesic and anti-inflammatory actions in different in vivo animal models, we anticipate that the development of TRPA1-targeted, organic polysulfide-based drugs will be promoted by this identification of the binding site.

Published

2023

5. Functionally active TRPA1 ion channel is downregulated in peptidergic neurons of the Edinger-Westphal nucleus upon acute alcohol exposure

Author

Ammar Al-Omari, Miklós Kecskés, Balázs Gaszner, Tünde Biró-Sütő, Balázs Fazekas, Gergely Berta, Mónika Kuzma, Erika Pintér, and Viktória Kormos

Subjects

alcohol, centrally projecting Edinger-Westphal nucleus, transient receptor potential ankyrin 1, urocortin 1, cocaine-and amphetamine-regulated transcript, JT010, Biology (General), QH301-705.5

Abstract

Introduction: The centrally projecting Edinger-Westphal nucleus (EWcp) contributes to the control of alcohol consumption by its urocortin 1 (UCN1) and cocaine- and amphetamine-regulated transcript (CART) co-expressing peptidergic neurons. Our group recently showed that the urocortinergic centrally projecting EWcp is the primary seat of central nervous system transient receptor potential ankyrin 1 (TRPA1) cation channel mRNA expression. Here, we hypothesized that alcohol and its metabolites, that pass through the blood-brain barrier, may influence the function of urocortinergic cells in centrally projecting EWcp by activating TRPA1 ion channels. We aimed to examine the functional activity of TRPA1 in centrally projecting EWcp and its possible role in a mouse model of acute alcohol exposure.Methods: Electrophysiological measurements were performed on acute brain slices of C57BL/6J male mice containing the centrally projecting EWcp to prove the functional activity of TRPA1 using a selective, potent, covalent agonist JT010. Male TRPA1 knockout (KO) and wildtype (WT) mice were compared with each other in the morphological studies upon acute alcohol treatment. In both genotypes, half of the animals was treated intraperitoneally with 1 g/kg 6% ethanol vs. physiological saline-injected controls. Transcardial perfusion was performed 2 h after the treatment. In the centrally projecting EWcp area, FOS immunohistochemistry was performed to assess neuronal activation. TRPA1, CART, and urocortin 1 mRNA expression as well as urocortin 1 and CART peptide content was semi-quantified by RNAscope in situ hybridization combined with immunofluorescence.Results: JT010 activated TRPA1 channels of the urocortinergic cells in acute brain slices. Alcohol treatment resulted in a significant FOS activation in both genotypes. Alcohol decreased the Trpa1 mRNA expression in WT mice. The assessment of urocortin 1 peptide immunoreactivity revealed lower basal urocortin 1 in KO mice compared to WTs. The urocortin 1 peptide content was affected genotype-dependently by alcohol: the peptide content decreased in WTs while it increased in KO mice. Alcohol exposure influenced neither CART and urocortin 1 mRNA expression nor the centrally projecting EWcp/CART peptide content.Conclusion: We proved the presence of functional TRPA1 receptors on urocortin 1 neurons of the centrally projecting EWcp. Decreased Trpa1 mRNA expression upon acute alcohol treatment, associated with reduced neuronal urocortin 1 peptide content suggesting that this cation channel may contribute to the regulation of the urocortin 1 release.

Published

2023

6. Transient receptor potential ankyrin 1 ion channel expressed by the Edinger-Westphal nucleus contributes to stress adaptation in murine model of posttraumatic stress disorder

Author

János Konkoly, Viktória Kormos, Balázs Gaszner, Pedro Correia, Gergely Berta, Tünde Biró-Sütő, Dóra Zelena, and Erika Pintér

Subjects

TRPA1, PTSD, Edinger-Westphal nucleus, single prolonged stress, urocortin 1, stress adaptation, Biology (General), QH301-705.5

Abstract

The centrally projecting Edinger-Westphal nucleus (EWcp) is involved in stress adaptation. Transient receptor potential ankyrin 1 (TRPA1) mRNA was previously shown to be expressed abundantly in mouse and human EWcp urocortin 1 (UCN1) positive neurons and reacted to chronic stress. Since UCN1 neurons are deeply implicated in stress-related disorders, we hypothesized that TRPA1/UCN1 neurons are also affected in posttraumatic stress disorder (PTSD). We examined male Trpa1 wild type (WT) and gene-deficient (KO) mice in the single prolonged stress (SPS) model of PTSD. Two weeks later the behavioral changes were monitored by forced swim test (FST) and restraint. The Trpa1 and Ucn1 mRNA expression and the UCN1 peptide content were assessed by RNAscope in situ hybridization technique combined with immunofluorescence labeling in the EWcp. SPS-induced immobility was lower in Trpa1 KO compared to WT animals, both in the FST and restraint, corresponding to diminished depression-like behavior. The copy number of Trpa1 mRNA decreased significantly in EWcp of WT animals in response to SPS. Higher basal Ucn1 mRNA expression was observed in the EWcp of KO animals, that was not affected by SPS exposure. EWcp neurons of WT animals responded to SPS with substantially increased amount of UCN1 peptide content compared to control animals, whereas such changes were not observable in KO mice. The decreased Trpa1 mRNA expression in the SPS model of PTSD associated with increased neuronal UCN1 peptide content suggests that this cation channel might be involved in the regulation of stress adaptation and may contribute to the pathomechanism of PTSD.

Published

2022

7. Plasma Somatostatin Levels Increase during Scoliosis Surgery, but Not Herniated Disc Operations: Results of a Pilot Study

Author

Balázs Sütő, Bálint Kolumbán, Éva Szabó, Sára Pásztor, Timea Németh, Teréz Bagoly, Bálint Botz, Erika Pintér, and Zsuzsanna Helyes

Subjects

neuropeptides, pain, inflammation, tissue damage, scoliosis and disc herniation, Cobb angle, Biology (General), QH301-705.5

Abstract

Somatostatin (SST) released from capsaicin-sensitive sensory nerves in response to stimulation exerts systemic anti-inflammatory, analgesic actions. Its elevation correlates with the extent of tissue injury. We measured plasma SST alterations during spine operations (scoliosis and herniated disc) to determine whether its release might be a general protective mechanism during painful conditions. Sampling timepoints were baseline (1), after: soft tissue retraction (2), osteotomy (3), skin closure (4), the following morning (5). Plasma SST-like immunoreactivity (SST-LI) determined by radioimmunoassay was correlated with pain intensity and the correction angle (Cobb angle). In scoliosis surgery, postoperative pain intensity (VAS 2.) 1 day after surgery significantly increased (from 1.44 SEM ± 0.68 to 6.77 SEM ± 0.82, p = 0.0028) and positively correlated with the Cobb angle (p = 0.0235). The baseline Cobb degree negatively correlated (p = 0.0459) with the preoperative SST-LI. The plasma SST-LI significantly increased in fraction 3 compared to the baseline (p < 0.05), and significantly decreased thereafter (p < 0.001). In contrast, in herniated disc operations no SST-LI changes were observed in either group. The VAS decreased after surgery both in the traditional (mean 6.83 to 2.29, p = 0.0005) and microdiscectomy groups (mean 7.22 to 2.11, p = 0.0009). More extensive and destructive scoliosis surgery might cause greater tissue damage with greater pain (inflammation), which results in a significant SST release into the plasma from the sensory nerves. SST is suggested to be involved in an endogenous postoperative analgesic (anti-inflammatory) mechanism.

Published

2023

8. Personalised health education against health damage of COVID-19 epidemic in the elderly Hungarian population (PROACTIVE-19): protocol of an adaptive randomised controlled clinical trial

Author

Bálint Erőss, Zsolt Molnár, Zsolt Szakács, Noémi Zádori, Lajos Szakó, Szilárd Váncsa, Márk Félix Juhász, Klementina Ocskay, Nóra Vörhendi, Katalin Márta, Andrea Szentesi, Andrea Párniczky, Péter J. Hegyi, Szabolcs Kiss, Mária Földi, Fanni Dembrovszky, Anna Kanjo, Piroska Pázmány, András Varró, Árpád Csathó, Zsuzsanna Helyes, Zoltán Péterfi, László Czopf, István Kiss, Antal Zemplényi, Dóra Czapári, Eszter Hegyi, Dalma Dobszai, Emőke Miklós, Attila Márta, Dominika Tóth, Richard Farkas, Nelli Farkas, Béla Birkás, Erika Pintér, Gábor Pethő, Borbála Zsigmond, Andrea Sárközi, Anikó Nagy, and Péter Hegyi

Subjects

COVID-19, SARS-CoV-2, nCov-2019, Public health, Randomised controlled trial, Prevention, Medicine (General), R5-920

Abstract

Abstract Background Early reports indicate that COVID-19 may require intensive care unit (ICU) admission in 5–26% and overall mortality can rise to 11% of the recognised cases, particularly affecting the elderly. There is a lack of evidence-based targeted pharmacological therapy for its prevention and treatment. We aim to compare the effects of a World Health Organization recommendation-based education and a personalised complex preventive lifestyle intervention package (based on the same WHO recommendation) on the outcomes of the COVID-19. Methods PROACTIVE-19 is a pragmatic, randomised controlled clinical trial with adaptive “sample size re-estimation” design. Hungarian population over the age of 60 years without confirmed COVID-19 will be approached to participate in a telephone health assessment and lifestyle counselling voluntarily. Volunteers will be randomised into two groups: (A) general health education and (B) personalised health education. Participants will go through questioning and recommendation in 5 fields: (1) mental health, (2) smoking habits, (3) physical activity, (4) dietary habits, and (5) alcohol consumption. Both groups A and B will receive the same line of questioning to assess habits concerning these topics. Assessment will be done weekly during the first month, every second week in the second month, then monthly. The composite primary endpoint will include the rate of ICU admission, hospital admission (longer than 48 h), and mortality in COVID-19-positive cases. The estimated sample size is 3788 subjects per study arm. The planned duration of the follow-up is a minimum of 1 year. Discussion These interventions may boost the body’s cardiovascular and pulmonary reserve capacities, leading to improved resistance against the damage caused by COVID-19. Consequently, lifestyle changes can reduce the incidence of life-threatening conditions and attenuate the detrimental effects of the pandemic seriously affecting the older population. Trial registration The study has been approved by the Scientific and Research Ethics Committee of the Hungarian Medical Research Council (IV/2428- 2 /2020/EKU) and has been registered at clinicaltrials.gov ( NCT04321928 ) on 25 March 2020.

Published

2020

9. Development of Capsaicin-Containing Analgesic Silicone-Based Transdermal Patches

Author

Szabolcs László, István Z. Bátai, Szilvia Berkó, Erzsébet Csányi, Ágnes Dombi, Gábor Pozsgai, Kata Bölcskei, Lajos Botz, Ödön Wagner, and Erika Pintér

Subjects

transdermal therapeutic system, capsaicin, silicone, addition polymer, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Transdermal therapeutic systems (TTSs) enable convenient dosing in drug therapy. Modified silicone-polymer-based patches are well-controlled and cost-effective matrix diffusion systems. In the present study, we investigated the substance release properties, skin penetration, and analgesic effect of this type of TTS loaded with low-dose capsaicin. Release properties were measured in Franz diffusion cell and continuous flow-through cell approaches. Capsaicin was detected with HPLC-UV and UV spectrophotometry. Raman spectroscopy was conducted on human skin samples exposed to the TTS. A surgical incision or carrageenan injection was performed on one hind paw of male Wistar rats. TTSs were applied to the epilated dorsal skin. Patches were kept on the animals for 6 h. The thermal hyperalgesia and mechanical pain threshold of the hind paws were detected. Patches exhibited controlled, zero-order kinetic capsaicin release. According to the Raman mapping, capsaicin penetrated into the epidermis and dermis of human skin, where the target receptors are expressed. The thermal pain threshold drop of the operated rat paws was reversed by capsaicin treatment compared to that of animals treated with control patches. It was concluded that our modified silicone-polymer-based capsaicin-containing TTS is suitable for the relief of traumatic and inflammatory pain.

Published

2022

10. Development of a Silicone-Based Polymer Matrix as a Suitable Transdermal Therapeutic System for Diallyl Disulfide

Author

Szabolcs László, Zsófia Hajna, Attila Egyed, Erika Pintér, and Ödön Wagner

Subjects

diallyl disulfide, hydrogen sulfide, TRPA1 receptor, transdermal therapeutic systems, silicone, membrane diffusion, Medicine, Pharmacy and materia medica, RS1-441

Abstract

There is an unmet need for novel therapeutic tools relieving chronic pain. Hydrogen sulfide (H2S) is highly involved in pain processes; however, the development of ideal matrices for sulfide donor compounds remains a great pharmaceutical challenge. We aimed to establish a suitable transdermal therapeutic system (TTS) using the H2S donor diallyl disulfide (DADS) as a model compound. After the preparation of DADS, its solubility was investigated in different liquid excipients (propylene glycol, polyethylene glycol, silicone oil) and its membrane diffusivity was assessed in silicone matrices of different compositions. Drug-releasing properties of DADS-containing patches with different silicone oil contents were determined with Franz and flow-through cells. We found a correlation between the liquid excipient content of the patch and the diffusion rate of DADS. DADS showed the best solubility in dimethyl silicone oil, and the diffusion constant was proportional to the amount of oil above the 3 m/m% threshold value. The 8-day-old patch showed a significantly lower, but better-regulated, drug release over time than the 4-day-old one. In conclusion, the silicone-based polymer matrix developed in this study is suitable for stable storage and optimal release of DADS, providing a good basis for a TTS applied in chronic pain.

Published

2022

11. Effects of Angiotensin-Converting Enzyme Inhibitors and Angiotensin Receptor Blockers on Angiotensin-Converting Enzyme 2 Levels: A Comprehensive Analysis Based on Animal Studies

Author

Gábor Kriszta, Zsófia Kriszta, Szilárd Váncsa, Péter Jenő Hegyi, Levente Frim, Bálint Erőss, Péter Hegyi, Gábor Pethő, and Erika Pintér

Subjects

SARS-CoV-2, angiotensin converrting enzyme, angiotensin receptor blocker, ACE2, animal study, Therapeutics. Pharmacology, RM1-950

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS‐CoV‐2), the pathogen of coronavirus disease 2019 (COVID‐19), caused the outbreak escalated to pandemic. Reports suggested that near 1–3% of COVID‐19 cases have a fatal outcome. Angiotensin-converting enzyme inhibitors (ACEIs) and angiotensin receptor blockers (ARBs) are widely used in hypertension, heart failure and chronic kidney disease. These drugs have been reported to upregulate angiotensin converting enzyme 2 (ACE2) which produces Ang (1–7), the main counter-regulatory mediator of angiotensin II. This enzyme is also known as the receptor of SARS‐CoV‐2 promoting the cellular uptake of the virus in the airways, however, ACE2 itself proved to be protective in several experimental models of lung injury. The present study aimed to systematically review the relationship between ACEI/ARB administration and ACE2 expression in experimental models. After a comprehensive search and selection, 27 animal studies investigating ACE2 expression in the context of ACEI and ARB were identified. The majority of these papers reported increased ACE2 levels in response to ACEI/ARB treatment. This result should be interpreted in the light of the dual role of ACE2 being a promoter of viral entry to cells and a protective factor against oxidative damage in the lungs.

Published

2021

12. Protective effects of the novel amine-oxidase inhibitor multi-target drug SZV 1287 on streptozotocin-induced beta cell damage and diabetic complications in rats

Author

Valéria Tékus, Ádám István Horváth, Kata Csekő, Krisztina Szabadfi, Andrea Kovács-Valasek, Bese Dányádi, László Deres, Róbert Halmosi, Éva Sághy, Zoltán V. Varga, Ernest Adeghate, Tamás Kőszegi, Péter Mátyus, Róbert Gábriel, Péter Ferdinandy, Erika Pintér, and Zsuzsanna Helyes

Subjects

Semicarbazide-sensitive amine oxidase, Vascular adhesion protein 1, Streptozotocin, Diabetic neuropathy, Diabetic retinopathy, LJP 1207, Therapeutics. Pharmacology, RM1-950

Abstract

Diabetes mellitus is a common metabolic disease leading to hyperglycemia due to insufficient pancreatic insulin production or effect. Amine oxidase copper containing 3 (AOC3) is an enzyme that belongs to the semicarbazide-sensitive amine oxidase family, which may be a novel therapeutic target to treat diabetic complications. We aimed to explore the effects of AOC3 inhibition and to test the actions of our novel AOC3 inhibitor multi-target drug candidate, SZV 1287, compared to a selective reference compound, LJP 1207, in an 8-week long insulin-controlled streptozotocin (STZ)-induced (60 mg/kg i.p.) rat diabetes model. Both AOC3 inhibitors (20 mg/kg, daily s.c. injections) were protective against STZ-induced pancreatic beta cell damage determined by insulin immunohistochemistry and radioimmunoassay, neuropathic cold hypersensitivity measured by paw withdrawal latency decrease from 0 °C water, and retinal dysfunction detected by electroretinography. SZV 1287 showed greater inhibitory effects on beta cell damage, and reduced retinal apoptosis shown by histochemistry. Mechanical hypersensitivity measured by aesthesiometry, cardiac dysfunction and nitrosative stress determined by echocardiography and immunohistochemistry/Western blot, respectively, serum Na+, K+, fructosamine, and urine microalbumin, creatinine, total protein/creatinine ratio alterations did not develop in response to diabetes. None of these parameters were influenced by the treatments except for SZV 1287 reducing serum fructosamine and LJP 1207 increasing urine creatinine. We provide the first evidence for protective effects of AOC3 inhibition on STZ-induced pancreatic beta cell damage, neuropathic cold hypersensitivity and diabetic retinal dysfunction. Long-term treatment with our novel multi-target analgesic candidate, SZV 1287, is safe and effective also under diabetic conditions.

Published

2021

13. In Silico, In Vitro and In Vivo Pharmacodynamic Characterization of Novel Analgesic Drug Candidate Somatostatin SST4 Receptor Agonists

Author

Boglárka Kántás, Éva Szőke, Rita Börzsei, Péter Bánhegyi, Junaid Asghar, Lina Hudhud, Anita Steib, Ágnes Hunyady, Ádám Horváth, Angéla Kecskés, Éva Borbély, Csaba Hetényi, Gábor Pethő, Erika Pintér, and Zsuzsanna Helyes

Subjects

neuropathic pain, drug discovery, G protein coupled receptor, somatostatin, somatostatin receptor subtype 4, molecular, Therapeutics. Pharmacology, RM1-950

Abstract

Background: Somatostatin released from the capsaicin-sensitive sensory nerves mediates analgesic and anti-inflammatory effects via its receptor subtype 4 (SST4) without influencing endocrine functions. Therefore, SST4 is considered to be a novel target for drug development in pain, especially chronic neuropathy which is a great unmet medical need.Purpose and Experimental Approach: Here, we examined the in silico binding, SST4-linked G protein activation and β-arrestin activation on stable SST4 expressing cells and the effects of our novel pyrrolo-pyrimidine molecules (20, 100, 500, 1,000, 2,000 µg·kg−1) on partial sciatic nerve ligation-induced traumatic mononeuropathic pain model in mice.Key Results: The novel compounds bind to the high affinity binding site of SST4 the receptor and activate the G protein. However, unlike the reference SST4 agonists NNC 26-9100 and J-2156, they do not induce β-arrestin activation responsible for receptor desensitization and internalization upon chronic use. They exert 65–80% maximal anti-hyperalgesic effects in the neuropathy model 1 h after a single oral administration of 100–500 µg·kg−1 doses.Conclusion and Implications: The novel orally active compounds show potent and effective SST4 receptor agonism in vitro and in vivo. All four novel ligands proved to be full agonists based on G protein activation, but failed to recruit β-arrestin. Based on their potent antinociceptive effect in the neuropathic pain model following a single oral administration, they are promising candidates for drug development.

Published

2021

14. Investigation of the Role of the TRPA1 Ion Channel in Conveying the Effect of Dimethyl Trisulfide on Vascular and Histological Changes in Serum-Transfer Arthritis

Author

István Z. Bátai, Ágnes Dombi, Éva Borbély, Ádám Fehér, Ferenc Papp, Zoltan Varga, Attila Mócsai, Zsuzsanna Helyes, Erika Pintér, and Gábor Pozsgai

Subjects

dimethyl trisulfide, K/BxN serum-transfer arthritis, TRPA1 ion channel, plasma extravasation, fibroblast-like synoviocyte, cartilage destruction, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Rheumatoid arthritis (RA) is one of the most prevalent autoimmune diseases. Its therapy is often challenging, even in the era of biologicals. Previously, we observed the anti-inflammatory effects of garlic-derived organic polysulfide dimethyl trisulfide (DMTS). Some of these effects were mediated by activation of the TRPA1 ion channel. TRPA1 was mostly expressed in a subset of nociceptor neurons. We decided to investigate the action of DMTS in K/BxN serum-transfer arthritis, which is a relevant model of RA. TRPA1 gene knockout (KO) and wild-type (WT) mice were used. The interaction of DMTS and TRPA1 was examined using a patch clamp in CHO cells. Arthritis was characterized by mechanical hyperalgesia, paw swelling, movement range of the ankle joint, hanging performance, plasma extravasation rate, myeloperoxidase activity, and histological changes in the tibiotarsal joint. DMTS activated TRPA1 channels dose-dependently. DMTS treatment reduced paw swelling and plasma extravasation in both TRPA1 WT and KO animals. DMTS-treated TRPA1 KO animals developed milder collagen deposition in the inflamed joints than WT ones. TRPA1 WT mice did not exhibit significant cartilage damage compared to ones administered a vehicle. We concluded that DMTS and related substances might evolve into novel complementary therapeutic aids for RA patients.

Published

2022

15. Presence of TRPA1 Modifies CD4+/CD8+ T Lymphocyte Ratio and Activation

Author

Katalin Szabó, Ágnes Kemény, Noémi Balázs, Esam Khanfar, Zoltán Sándor, Ferenc Boldizsár, Rolland Gyulai, József Najbauer, Erika Pintér, and Tímea Berki

Subjects

TRPA1, lymphocytes, monocytes, CD4+ cells, CD8+ cells, B cells, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Transient Receptor Potential Ankyrin 1 (TRPA1) has been reported to influence neuroinflammation and lymphocyte function. We analysed the immune phenotype and activation characteristics of TRPA1-deficient mice (knockout—KO) generated by targeted deletion of the pore-loop domain of the ion channel. We compared TRPA1 mRNA and protein expression in monocyte and lymphocyte subpopulations isolated from primary and secondary lymphatic organs of wild type (WT) and KO mice. qRT-PCR and flow cytometric studies indicated a higher level of TRPA1 in monocytes than in lymphocytes, but both were orders of magnitude lower than in sensory neurons. We found lower CD4+/CD8+ thymocyte ratios, diminished CD4/CD8 rates, and B cell numbers in the KO mice. Early activation marker CD69 was lower in CD4+ T cells of KO, while the level of CD8+/CD25+ cells was higher. In vitro TcR-mediated activation did not result in significant differences in CD69 level between WT and KO splenocytes, but lower cytokine (IL-1β, IL-6, TNF-α, IL-17A, IL-22, and RANTES) secretion was observed in KO splenocytes. Basal intracellular Ca2+ level and TcR-induced Ca2+ signal in T lymphocytes did not differ significantly, but interestingly, imiquimod-induced Ca2+ level in KO thymocytes was higher. Our results support the role of TRPA1 in the regulation of activation, cytokine production, and T and B lymphocytes composition in mice.

Published

2022

16. The Role of TRPA1 Channels in the Central Processing of Odours Contributing to the Behavioural Responses of Mice

Author

János Konkoly, Viktória Kormos, Balázs Gaszner, Zoltán Sándor, Angéla Kecskés, Ammar Alomari, Alíz Szilágyi, Beatrix Szilágyi, Dóra Zelena, and Erika Pintér

Subjects

TRPA1, social behaviour, innate fear, piriform cortex, olfactory bulb, olfactory epithelium, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Transient receptor potential ankyrin 1 (TRPA1), a nonselective cation channel, contributes to several (patho)physiological processes. Smell loss is an early sign in several neurodegenerative disorders, such as multiple sclerosis, Parkinson’s and Alzheimer’s diseases; therefore, we focused on its role in olfaction and social behaviour with the aim to reveal its potential therapeutic use. The presence of Trpa1 mRNA was studied along the olfactory tract of mice by combined RNAscope in situ hybridisation and immunohistochemistry. The aversive effects of fox and cat odour were examined in parallel with stress hormone levels. In vitro calcium imaging was applied to test if these substances can directly activate TRPA1 receptors. The role of TRPA1 in social behaviour was investigated by comparing Trpa1 wild-type and knockout mice (KO). Trpa1 mRNA was detected in the olfactory bulb and piriform cortex, while its expression was weak in the olfactory epithelium. Fox, but not cat odour directly activated TRPA1 channels in TRPA1-overexpressing Chinese Hamster Ovary cell lines. Accordingly, KO animals showed less aversion against fox, but not cat odour. The social interest of KO mice was reduced during social habituation–dishabituation and social interaction, but not during resident–intruder tests. TRPA1 may contribute to odour processing at several points of the olfactory tract and may play an important role in shaping the social behaviour of mice. Thus, TRPA1 may influence the development of certain social disorders, serving as a potential drug target in the future.

Published

2021

17. Prerequisite Binding Modes Determine the Dynamics of Action of Covalent Agonists of Ion Channel TRPA1

Author

Balázs Zoltán Zsidó, Rita Börzsei, Erika Pintér, and Csaba Hetényi

Subjects

TRPA1 receptor, prerequisite binding, covalent binding, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Transient receptor potential ankyrin 1 (TRPA1) is a transmembrane protein channeling the influx of calcium ions. As a polymodal nocisensor, TRPA1 can be activated by thermal, mechanical stimuli and a wide range of chemically damaging molecules including small volatile environmental toxicants and endogenous algogenic lipids. After activation by such compounds, the ion channel opens up, its central pore widens allowing calcium influx into the cytosol inducing signal transduction pathways. Afterwards, the calcium influx desensitizes irritant evoked responses and results in an inactive state of the ion channel. Recent experimental determination of structures of apo and holo forms of TRPA1 opened the way towards the design of new agonists, which can activate the ion channel. The present study is aimed at the elucidation of binding dynamics of agonists using experimental structures of TRPA1-agonist complexes at the atomic level applying molecular docking and dynamics methods accounting for covalent and non-covalent interactions. Following a test of docking methods focused on the final, holo structures, prerequisite binding modes were detected involving the apo forms. It was shown how reversible interactions with prerequisite binding sites contribute to structural changes of TRPA1 leading to covalent bonding of agonists. The proposed dynamics of action allowed a mechanism-based forecast of new, druggable binding sites of potent agonists.

Published

2021

18. TRPA1 Ion Channel Determines Beneficial and Detrimental Effects of GYY4137 in Murine Serum-Transfer Arthritis

Author

István Z. Bátai, Cecília Pápainé Sár, Ádám Horváth, Éva Borbély, Kata Bölcskei, Ágnes Kemény, Zoltán Sándor, Balázs Nemes, Zsuzsanna Helyes, Anikó Perkecz, Attila Mócsai, Gábor Pozsgai, and Erika Pintér

Subjects

GYY4137, TRPA1, K/BxN serum-transfer model, arthritis, hydrogen sulphide, polysulfide, Therapeutics. Pharmacology, RM1-950

Abstract

Modulation of nociception and inflammation by sulfide in rheumatoid arthritis and activation of transient receptor potential ankyrin 1 (TRPA1) ion channels by sulfide compounds are well documented. The present study aims to investigate TRPA1-mediated effects of sulfide donor GYY4137 in K/BxN serum-transfer arthritis, a rodent model of rheumatoid arthritis. TRPA1 and somatostatin sst4 receptor wild-type (WT) and knockout mice underwent K/BxN serum transfer and were treated daily with GYY4137. Functional and biochemical signs of inflammation were recorded, together with histological characterization. These included detection of hind paw mechanical hyperalgesia by dynamic plantar esthesiometry, hind paw volume by plethysmometry, and upside-down hanging time to failure. Hind paw erythema, edema, and passive movement range of tibiotarsal joints were scored. Somatostatin release from sensory nerve endings of TRPA1 wild-type and knockout mice in response to polysulfide was detected by radioimmunoassay. Polysulfide formation from GYY4137 was uncovered by cold cyanolysis. GYY4137 aggravated mechanical hyperalgesia in TRPA1 knockout mice but ameliorated it in wild-type ones. Arthritis score was lowered by GYY4137 in TRPA1 wild-type animals. Increased myeloperoxidase activity, plasma extravasation, and subcutaneous MIP-2 levels of hind paws were detected in TRPA1 knockout mice upon GYY4137 treatment. Genetic lack of sst4 receptors did not alter mechanical hyperalgesia, edema formation, hanging performance, arthritis score, plasma extravasation, or myeloperoxidase activity. TRPA1 WT animals exhibited smaller cartilage destruction upon GYY4137 administration. Sodium polysulfide caused TRPA1-dependent somatostatin release from murine nerve endings. Sulfide released from GYY4137 is readily converted into polysulfide by hypochlorite. Polysulfide potently activates human TRPA1 receptors expressed in Chinese hamster ovary (CHO) cells. According to our data, the protective effect of GYY4137 is mediated by TRPA1, while detrimental actions are independent of the ion channel in the K/BxN serum-transfer arthritis model in mice. At acidic pH in inflamed tissue sulfide is released from GYY4137 and reacts with neutrophil-derived hypochlorite. Resulting polysulfide might be responsible for TRPA1-mediated antinociceptive and anti-inflammatory as well as TRPA1-independent pro-inflammatory effects.

Published

2019

19. Investigation of Cuprizone-Induced Demyelination in mGFAP-Driven Conditional Transient Receptor Potential Ankyrin 1 (TRPA1) Receptor Knockout Mice

Author

Gábor Kriszta, Balázs Nemes, Zoltán Sándor, Péter Ács, Sámuel Komoly, Zoltán Berente, Kata Bölcskei, and Erika Pintér

Subjects

transient receptor potential ankyrin 1, cuprizone, demyelination, astrocyte, conditional knockout, magnetic resonance imaging, Cytology, QH573-671

Abstract

Transient receptor potential ankyrin 1 (TRPA1) receptors are non-selective cation channels responsive to a variety of exogenous irritants and endogenous stimuli including products of oxidative stress. It is mainly expressed by primary sensory neurons; however, expression of TRPA1 by astrocytes and oligodendrocytes has recently been detected in the mouse brain. Genetic deletion of TRPA1 was shown to attenuate cuprizone-induced oligodendrocyte apoptosis and myelin loss in mice. In the present study we aimed at investigating mGFAP-Cre conditional TRPA1 knockout mice in the cuprizone model. These animals were generated by crossbreeding GFAP-Cre+/− and floxed TRPA1 (TRPA1Fl/Fl) mice. Cuprizone was administered for 6 weeks and demyelination was followed by magnetic resonance imaging (MRI). At the end of the treatment, demyelination and glial activation was also investigated by histological methods. The results of the MRI showed that demyelination was milder at weeks 3 and 4 in both homozygous (GFAP-Cre+/− TRPA1Fl/Fl) and heterozygous (GFAP-Cre+/− TRPA1Fl/−) conditional knockout animals compared to Cre−/− control mice. However, by week 6 of the treatment the difference was not detectable by either MRI or histological methods. In conclusion, TRPA1 receptors on astrocytes may transiently contribute to the demyelination induced by cuprizone, however, expression and function of TRPA1 receptors by other cells in the brain (oligodendrocytes, microglia, neurons) warrant further investigation.

Published

2019

20. Role of Transient Receptor Potential Ankyrin 1 Ion Channel and Somatostatin sst4 Receptor in the Antinociceptive and Anti-inflammatory Effects of Sodium Polysulfide and Dimethyl Trisulfide

Author

István Z. Bátai, Ádám Horváth, Erika Pintér, Zsuzsanna Helyes, and Gábor Pozsgai

Subjects

transient receptor potential ankyrin 1, sst4, somatostatin, dimethyl trisulfide, polysulfide, carrageenan, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Transient receptor potential ankyrin 1 (TRPA1) non-selective ligand-gated cation channels are mostly expressed in primary sensory neurons. Polysulfides (POLYs) are Janus-faced substances interacting with numerous target proteins and associated with both protective and detrimental processes. Activation of TRPA1 in sensory neurons, consequent somatostatin (SOM) liberation and action on sst4 receptors have recently emerged as mediators of the antinociceptive effect of organic trisulfide dimethyl trisulfide (DMTS). In the frame of the present study, we set out to compare the participation of this mechanism in antinociceptive and anti-inflammatory effects of inorganic sodium POLY and DMTS in carrageenan-evoked hind-paw inflammation. Inflammation of murine hind paws was induced by intraplantar injection of carrageenan (3% in 30 µL saline). Animals were treated intraperitoneally with POLY (17 µmol/kg) or DMTS (250 µmol/kg) or their respective vehicles 30 min prior paw challenge and six times afterward every 60 min. Mechanical pain threshold and swelling of the paws were measured by dynamic plantar aesthesiometry and plethysmometry at 2, 4, and 6 h after initiation of inflammation. Myeloperoxidase (MPO) activity in the hind paws were detected 6 h after challenge by luminescent imaging. Mice genetically lacking TRPA1 ion channels, sst4 receptors and their wild-type counterparts were used to examine the participation of these proteins in POLY and DMTS effects. POLY counteracted carrageenan-evoked mechanical hyperalgesia in a TRPA1 and sst4 receptor-dependent manner. POLY did not influence paw swelling and MPO activity. DMTS ameliorated all examined inflammatory parameters. Mitigation of mechanical hyperalgesia and paw swelling by DMTS were mediated through sst4 receptors. These effects were present in TRPA1 knockout animals, too. DMTS inhibited MPO activity with no participation of the sensory neuron–SOM axis. While antinociceptive effects of POLY are transmitted by activation of peptidergic nerves via TRPA1, release of SOM and its effect on sst4 receptors, those of DMTS partially rely on SOM release triggered by other routes. SOM is responsible for the inhibition of paw swelling by DMTS, but TRPA1 does not contribute to its release. Modulation of MPO activity by DMTS is independent of TRPA1 and sst4.

Published

2018

21. Upregulation of the transient receptor potential ankyrin 1 ion channel in the inflamed human and mouse colon and its protective roles.

Author

József Kun, István Szitter, Agnes Kemény, Anikó Perkecz, László Kereskai, Krisztina Pohóczky, Aron Vincze, Szilárd Gódi, Imre Szabó, János Szolcsányi, Erika Pintér, and Zsuzsanna Helyes

Subjects

Medicine, Science

Abstract

Transient Receptor Potential Ankyrin 1 (TRPA1) channels are localized on sensory nerves and several non-neural cells, but data on their functional significance are contradictory. We analysed the presence and alterations of TRPA1 in comparison with TRP Vanilloid 1 (TRPV1) at mRNA and protein levels in human and mouse intact and inflamed colons. The role of TRPA1 in a colitis model was investigated using gene-deficient mice. TRPA1 and TRPV1 expressions were investigated in human colon biopsies of healthy subjects and patients with inflammatory bowel diseases (IBD: ulcerative colitis, Crohn's disease) with quantitative PCR and immunohistochemistry. Mouse colitis was induced by oral 2% dextran-sulphate (DSS) for 10 days. For investigating the functions of TRPA1, Disease Activity Index (weight loss, stool consistency, blood content) was determined in C57BL/6-based Trpa1-deficient (knockout: KO) and wildtype (WT) mice. Sensory neuropeptides, their receptors, and inflammatory cytokines/chemokines were determined with qPCR or Luminex. In human and mouse colons TRPA1 and TRPV1 are located on epithelial cells, macrophages, enteric ganglia. Significant upregulation of TRPA1 mRNA was detected in inflamed samples. In Trpa1 KO mice, Disease Activity Index was significantly higher compared to WTs. It could be explained by the greater levels of substance P, neurokinins A and B, neurokinin 1 receptor, pituitary adenylate-cyclase activating polypeptide, vasoactive intestinal polypeptide, and also interleukin-1beta, macrophage chemoattractant protein-1, monokine induced by gamma interferon-1, tumor necrosis factor-alpha and B-lymphocyte chemoattractant in the distal colon. TRPA1 is upregulated in colitis and its activation exerts protective roles by decreasing the expressions of several proinflammatory neuropeptides, cytokines and chemokines.

Published

2014

22. Role of tachykinin 1 and 4 gene-derived neuropeptides and the neurokinin 1 receptor in adjuvant-induced chronic arthritis of the mouse.

Author

Eva Borbély, Zsófia Hajna, Katalin Sándor, László Kereskai, István Tóth, Erika Pintér, Péter Nagy, János Szolcsányi, John Quinn, Andreas Zimmer, James Stewart, Christopher Paige, Alexandra Berger, and Zsuzsanna Helyes

Subjects

Medicine, Science

Abstract

Substance P, encoded by the Tac1 gene, is involved in neurogenic inflammation and hyperalgesia via neurokinin 1 (NK1) receptor activation. Its non-neuronal counterpart, hemokinin-1, which is derived from the Tac4 gene, is also a potent NK1 agonist. Although hemokinin-1 has been described as a tachykinin of distinct origin and function compared to SP, its role in inflammatory and pain processes has not yet been elucidated in such detail. In this study, we analysed the involvement of tachykinins derived from the Tac1 and Tac4 genes, as well as the NK1 receptor in chronic arthritis of the mouse.Complete Freund's Adjuvant was injected intraplantarly and into the tail of Tac1(-/-), Tac4(-/-), Tacr1(-/-) (NK1 receptor deficient) and Tac1(-/-/)Tac4(-/-) mice. Paw volume was measured by plethysmometry and mechanosensitivity using dynamic plantar aesthesiometry over a time period of 21 days. Semiquantitative histopathological scoring and ELISA measurement of IL-1β concentrations of the tibiotarsal joints were performed.Mechanical hyperalgesia was significantly reduced from day 11 in Tac4(-/-) and Tacr1(-/-) animals, while paw swelling was not altered in any strain. Inflammatory histopathological alterations (synovial swelling, leukocyte infiltration, cartilage destruction, bone damage) and IL-1β concentration in the joint homogenates were significantly smaller in Tac4(-/-) and Tac1(-/-/)Tac4(-/-) mice.Hemokinin-1, but not substance P increases inflammation and hyperalgesia in the late phase of adjuvant-induced arthritis. While NK1 receptors mediate its antihyperalgesic actions, the involvement of another receptor in histopathological changes and IL-1β production is suggested.

Published

2013

23. The triple function of the capsaicin-sensitive sensory neurons: In memoriam János Szolcsányi

Author

Erika Pintér, Zsuzsanna Helyes, Éva Szőke, Kata Bölcskei, Angéla Kecskés, and Gábor Pethő

Subjects

Physiology, Physiology (medical)

Published

2022

24. Megelőzhető-e a ciklosporin A okozta fogíny-hyperplasia a dentalis plakk eltávolításával?

Author

Bernadett, Schönfeld, András, Szabadi, Erika, Pintér, József, Kun, and Ágnes, Bán

Subjects

Hyperplasia, Gingival Hyperplasia, Cyclosporine, Prevalence, Humans, General Medicine, Kidney Transplantation

Abstract

Hazánkban mintegy 3500 ember él transzplantált szervvel, az összes donáció meghaladja az évi 400-at, ebből a vesetranszplantációk száma például évente 250–300 között van. Az immunszuppresszió és a sebészi technikák fejlődésének köszönhetően a páciensek túlélési aránya nő, ezért a fogorvosoknak is egyre gyakrabban kell szembesülniük veseelégtelenségből származó orodentalis elváltozások mellett az immunszuppresszív terápia miatt kialakuló gingiva-hyperplasiával. A ciklosporin A alkalmazása esetén kialakult gingiva-hyperplasia prevalenciája a 90%-ot is elérheti. Tanulmányunk célja felhívni a figyelmet a dentalis plakk jelentőségére a ciklosporin A okozta gingiva-hyperplasia kialakulásában, illetve hangsúlyozni, hogy a gingiva-hyperplasia, valamint a szervkilökődés veszélye megelőzhető vagy nagymértékben csökkenthető megfelelő individuális szájhigénia kialakításával és sikeres parodontológiai oki terápia elvégzésével. Különös figyelmet érdemel az interdiszciplináris együttműködés fontossága és a páciensek rendszeres gondozása. Vizsgálatainkat és kezeléseinket a Pécsi Tudományegyetem Fogászati és Szájsebészeti Klinikájának Parodontológiai Osztályán végeztük. Orv Hetil. 2022; 163(42): 1663–1669.

Published

2022

25. Peptidergic neurons of the Edinger–Westphal nucleus express TRPA1 ion channel that is downregulated both upon chronic variable mild stress in male mice and in humans who died by suicide

Author

Viktória Kormos, Angéla Kecskés, József Farkas, Tamás Gaszner, Valér Csernus, Ammar Alomari, Dániel Hegedüs, Éva Renner, Miklós Palkovits, Dóra Zelena, Zsuzsanna Helyes, Erika Pintér, and Balázs Gaszner

Subjects

Male, Mice, Knockout, Neurons, Ion Channels, Edinger-Westphal Nucleus, Mice, Suicide, Psychiatry and Mental health, Animals, Humans, Female, Pharmacology (medical), RNA, Messenger, TRPA1 Cation Channel, Urocortins, Biological Psychiatry

Abstract

Transient receptor potential ankyrin 1 (TRPA1), a cation channel, is expressed predominantly in primary sensory neurons, but its central distribution and role in mood control are not well understood. We investigated whether TRPA1 is expressed in the urocortin 1 (UCN1)-immunoreactive centrally projecting Edinger-Westphal nucleus (EWcp), and we hypothesized that chronic variable mild stress (CVMS) would reduce its expression in mice. We anticipated thatWe exposedDevelopmental compensations and the global lack of TRPA1 may have influenced our findings. Because experimental data came from male brains only, we have no evidence for whether findings would be similar in female brains. Because a TRPA1-specific antibody is lacking, we have provided mRNA data only. Limited access to high-quality human tissues restricted sample size.TRPA1 in EWcp/UCN1 neurons might contribute to the regulation of depression-like behaviour and stress adaptation response in mice. In humans, TRPA1 might contribute to mood control via EWcp/UCN1 neurons.

Published

2022

26. The anti-inflammatory effect of dimethyl trisulfide in experimental acute pancreatitis

Author

Erik Márk Orján, Eszter Sára Kormányos, Gabriella Mihalekné Fűr, Ágnes Dombi, Emese Réka Bálint, Zsolt Balla, Beáta Adél Balog, Ágnes Dágó, Ahmad Totonji, Zoárd István Bátai, Gábor Pozsgai, Erika Pintér, Zoltán Rakonczay, and Lóránd Kiss

Abstract

Several organosulfur compounds, such as dimethyl trisulfide (DMTS), exhibit anti-inflammatory properties. Our aims were to investigate the effects of DMTS on acute pancreatitis (AP) and its mechanism of action in both in vivo and in vitro studies. AP was induced in FVB/n mice or Wistar rats by caerulein or L-ornithine-HCl, respectively. DMTS treatments were applied subcutaneously. AP severity was evaluated with histological scoring of the pancreas, pancreatic water content and myeloperoxidase activity measurements. The behaviour of animals were followed. Western blot was performed to determine the extent of pancreatic heat shock protein 72 (HSP72) expression. In vitro acinar viability, reactive oxygen species (ROS) production, and intracellular Ca2+ concentrations were determined in isolated pancreatic acinar cells. DMTS dose dependently reduced the severity of AP. It decreased the pancreatic infiltration of leukocytes, myeloperoxidase activity and cellular damage in mice, but it was less effective in rats. During AP, DMTS upregulated the HSP72 expression. DMTS showed cytoprotection against H2O2 and AP inducing agents, it reduced the level of ROS, and altered the caerulein-evoked Ca2+ signals. Overall, DMTS significantly ameliorated the severity of AP and protected pancreatic acinar cells. Our results suggest that DMTS have anti-inflammatory effects, so organosulfur compounds are worth further investigation in this potentially lethal disease.

Published

2022

27. From capsaicin to TRPV1: The 'hot' legacy of János Szolcsányi

Author

Erika Pintér, Andras Garami, and Arpad Szallasi

Subjects

Physiology, Physiology (medical)

Published

2023

28. A 2021. évi orvosi-élettani Nobel-díjjal elismert kutatások és azok magyar előzményei • Nobel Prize in Physiology or Medicine 2021: The Hungarian Contribution

Author

György Helyes, Zsuzsanna Helyes, Zsuzsanna Sántha, Péter Sántha, Péter Pintér, Erika Pintér, Erika Pethő, Gábor Pethő, Gábor Barthó, Loránd Barthó, Loránd Dux, Mária Dux, Mária Jancsó, and Gábor Jancsó

Published

2022

29. The heptapeptide somatostatin analogue TT-232 exerts analgesic and anti-inflammatory actions via SST4 receptor activation: In silico, in vitro and in vivo evidence in mice

Author

Rita Börzsei, Éva Borbély, Boglárka Kántás, Lina Hudhud, Ádám Horváth, Éva Szőke, Csaba Hetényi, Zsuzsanna Helyes, and Erika Pintér

Subjects

Pharmacology, Biochemistry

Published

2023

30. Drug Delivery through the Psoriatic Epidermal Barrier—A “Skin-On-A-Chip” Permeability Study and Ex Vivo Optical Imaging

Author

Erdő, Dorottya Kocsis, Szabina Horváth, Ágnes Kemény, Zsófia Varga-Medveczky, Csaba Pongor, Rózsa Molnár, Anna Mihály, Dániel Farkas, Bese Márton Naszlady, András Fülöp, András Horváth, Balázs Rózsa, Erika Pintér, Rolland Gyulai, and Franciska

Subjects

psoriasis, skin permeability, skin-on-a-chip diffusion cells, TEWL, imiquimod, TRPA1 knock out, TRPV1 knock out, scanning electron microscopy, epidermal barrier

Abstract

Psoriasis is a chronic inflammatory disease with unmet medical needs. To clarify potential therapeutic targets, different animal models have been developed. In the current study, imiquimod-induced psoriasiform dermatitis was used for monitoring the changes in skin thickness, transepidermal water loss, body weight, blood perfusion and drug permeability for a topical cream formulation of caffeine, both in wild type and in knock out mice. Morphological characterization of control and diseased tissues was performed by scanning electron microscopy and two-photon microscopy. The chemically induced psoriatic group showed increased skin permeability for the model drug during disease progression. In wild type and TRPA1 KO mice, however, enhanced skin thickness and hyperkeratosis blocked further increase of drug penetration at the late phase (96 h). These results indicate that topical drug therapy can be more effective in early phases of plaque development, when skin thickness is lower. Although paracellular connections (tight junctions) are looser in the advanced phase, hyperkeratosis blocks drug delivery through the transappendageal routes. Novel drug formulations may have the potency for effective drug delivery across the epidermal barrier even in the advanced phase. For development of more effective topical drugs, further research is proposed to explore drug penetration both in healthy and diseased conditions.

Published

2022

31. Drug Delivery through the Psoriatic Epidermal Barrier-A 'Skin-On-A-Chip' Permeability Study and Ex Vivo Optical Imaging

Author

Dorottya Kocsis, Szabina Horváth, Ágnes Kemény, Zsófia Varga-Medveczky, Csaba Pongor, Rózsa Molnár, Anna Mihály, Dániel Farkas, Bese Márton Naszlady, András Fülöp, András Horváth, Balázs Rózsa, Erika Pintér, Rolland Gyulai, and Franciska Erdő

Subjects

Organic Chemistry, Optical Imaging, General Medicine, Catalysis, Permeability, Computer Science Applications, Inorganic Chemistry, Disease Models, Animal, Mice, Lab-On-A-Chip Devices, Animals, Psoriasis, Physical and Theoretical Chemistry, Epidermis, Molecular Biology, Spectroscopy, Skin

Abstract

Psoriasis is a chronic inflammatory disease with unmet medical needs. To clarify potential therapeutic targets, different animal models have been developed. In the current study, imiquimod-induced psoriasiform dermatitis was used for monitoring the changes in skin thickness, transepidermal water loss, body weight, blood perfusion and drug permeability for a topical cream formulation of caffeine, both in wild type and in knock out mice. Morphological characterization of control and diseased tissues was performed by scanning electron microscopy and two-photon microscopy. The chemically induced psoriatic group showed increased skin permeability for the model drug during disease progression. In wild type and TRPA1 KO mice, however, enhanced skin thickness and hyperkeratosis blocked further increase of drug penetration at the late phase (96 h). These results indicate that topical drug therapy can be more effective in early phases of plaque development, when skin thickness is lower. Although paracellular connections (tight junctions) are looser in the advanced phase, hyperkeratosis blocks drug delivery through the transappendageal routes. Novel drug formulations may have the potency for effective drug delivery across the epidermal barrier even in the advanced phase. For development of more effective topical drugs, further research is proposed to explore drug penetration both in healthy and diseased conditions.

Published

2022

32. A Central Role for TRPM4 in Ca2+-Signal Amplification and Vasoconstriction

Author

Tóth, Tamás Csípő, Ágnes Czikora, Gábor Á. Fülöp, Hajnalka Gulyás, Ibolya Rutkai, Enikő Pásztorné Tóth, Róbert Pórszász, Andrea Szalai, Kata Bölcskei, Zsuzsanna Helyes, Erika Pintér, Zoltán Papp, Zoltán Ungvári, and Attila

Subjects

transient receptor potential, transient receptor potential melastatin-4, blood pressure regulation, vascular smooth muscle, Ca2+ signaling

Abstract

Transient receptor potential melastatin-4 (TRPM4) is activated by an increase in intracellular Ca2+ concentration and is expressed on smooth muscle cells (SMCs). It is implicated in the myogenic constriction of cerebral arteries. We hypothesized that TRPM4 has a general role in intracellular Ca2+ signal amplification in a wide range of blood vessels. TRPM4 function was tested with the TRPM4 antagonist 9-phenanthrol and the TRPM4 activator A23187 on the cardiovascular responses of the rat, in vivo and in isolated basilar, mesenteric, and skeletal muscle arteries. TRPM4 inhibition by 9-phenanthrol resulted in hypotension and a decreased heart rate in the rat. TRPM4 inhibition completely antagonized myogenic tone development and norepinephrine-evoked vasoconstriction, and depolarization (high extracellular KCl concentration) evoked vasoconstriction in a wide range of peripheral arteries. Vasorelaxation caused by TRPM4 inhibition was accompanied by a significant decrease in intracellular Ca2+ concentration, suggesting an inhibition of Ca2+ signal amplification. Immunohistochemistry confirmed TRPM4 expression in the smooth muscle cells of the peripheral arteries. Finally, TRPM4 activation by the Ca2+ ionophore A23187 was competitively inhibited by 9-phenanthrol. In summary, TRPM4 was identified as an essential Ca2+-amplifying channel in peripheral arteries, contributing to both myogenic tone and agonist responses. These results suggest an important role for TRPM4 in the circulation. The modulation of TRPM4 activity may be a therapeutic target for hypertension. Furthermore, the Ca2+ ionophore A23187 was identified as the first high-affinity (nanomolar) direct activator of TRPM4, acting on the 9-phenanthrol binding site.

Published

2022

33. A Central Role for TRPM4 in Ca2+-Signal Amplification and Vasoconstriction

Author

Tamás Csípő, Ágnes Czikora, Gábor Á. Fülöp, Hajnalka Gulyás, Ibolya Rutkai, Enikő Pásztorné Tóth, Róbert Pórszász, Andrea Szalai, Kata Bölcskei, Zsuzsanna Helyes, Erika Pintér, Zoltán Papp, Zoltán Ungvári, and Attila Tóth

Subjects

Chemistry, transient receptor potential, vascular smooth muscle, Ca2+ signaling, QH301-705.5, transient receptor potential melastatin-4, blood pressure regulation, Biology (General), QD1-999

Abstract

Transient receptor potential melastatin-4 (TRPM4) is activated by an increase in intracellular Ca2+ concentration and is expressed on smooth muscle cells (SMCs). It is implicated in the myogenic constriction of cerebral arteries. We hypothesized that TRPM4 has a general role in intracellular Ca2+ signal amplification in a wide range of blood vessels. TRPM4 function was tested with the TRPM4 antagonist 9-phenanthrol and the TRPM4 activator A23187 on the cardiovascular responses of the rat, in vivo and in isolated basilar, mesenteric, and skeletal muscle arteries. TRPM4 inhibition by 9-phenanthrol resulted in hypotension and a decreased heart rate in the rat. TRPM4 inhibition completely antagonized myogenic tone development and norepinephrine-evoked vasoconstriction, and depolarization (high extracellular KCl concentration) evoked vasoconstriction in a wide range of peripheral arteries. Vasorelaxation caused by TRPM4 inhibition was accompanied by a significant decrease in intracellular Ca2+ concentration, suggesting an inhibition of Ca2+ signal amplification. Immunohistochemistry confirmed TRPM4 expression in the smooth muscle cells of the peripheral arteries. Finally, TRPM4 activation by the Ca2+ ionophore A23187 was competitively inhibited by 9-phenanthrol. In summary, TRPM4 was identified as an essential Ca2+-amplifying channel in peripheral arteries, contributing to both myogenic tone and agonist responses. These results suggest an important role for TRPM4 in the circulation. The modulation of TRPM4 activity may be a therapeutic target for hypertension. Furthermore, the Ca2+ ionophore A23187 was identified as the first high-affinity (nanomolar) direct activator of TRPM4, acting on the 9-phenanthrol binding site.

Published

2022

34. A Central Role for TRPM4 in Ca

Author

Tamás, Csípő, Ágnes, Czikora, Gábor Á, Fülöp, Hajnalka, Gulyás, Ibolya, Rutkai, Enikő Pásztorné, Tóth, Róbert, Pórszász, Andrea, Szalai, Kata, Bölcskei, Zsuzsanna, Helyes, Erika, Pintér, Zoltán, Papp, Zoltán, Ungvári, and Attila, Tóth

Subjects

Male, Ionophores, Myocytes, Smooth Muscle, TRPM Cation Channels, Blood Pressure, Arteries, Phenanthrenes, Muscle Development, Muscle, Smooth, Vascular, Potassium Chloride, Norepinephrine, Heart Rate, Vasoconstriction, Animals, Administration, Intravenous, Calcium, Calcium Signaling, Endothelium, Vascular, Rats, Wistar, Muscle, Skeletal, Calcimycin

Abstract

Transient receptor potential melastatin-4 (TRPM4) is activated by an increase in intracellular Ca

Published

2021

35. The Hypothermic Effect of Hydrogen Sulfide Is Mediated by the Transient Receptor Potential Ankyrin-1 Channel in Mice

Author

Erika Pintér, Patrik Keringer, Balázs Gaszner, Eszter Pakai, Valéria Tékus, András Garami, Hannah Wilson, Viktória Kormos, Kata Fekete, Leonardo Kelava, Emoke Olah, Julie Keeble, Margit Solymár, Zoltan Rumbus, and Matthew Whiteman

Subjects

medicine.medical_specialty, Hydrogen sulfide, Pharmaceutical Science, TRPA1, Article, H2S, Transient receptor potential channel, chemistry.chemical_compound, Pharmacy and materia medica, Internal medicine, GYY4137, Drug Discovery, medicine, Ankyrin, chemistry.chemical_classification, Messenger RNA, thermoregulation, food and beverages, Thermoregulation, Hypothermia, equipment and supplies, RS1-441, Endocrinology, chemistry, Molecular targets, Molecular Medicine, Medicine, medicine.symptom, hypothermia, Thermogenesis, psychological phenomena and processes

Abstract

Hydrogen sulfide (H2S) has been shown in previous studies to cause hypothermia and hypometabolism in mice, and its thermoregulatory effects were subsequently investigated. However, the molecular target through which H2S triggers its effects on deep body temperature has remained unknown. We investigated the thermoregulatory response to fast-(Na2S) and slow-releasing (GYY4137) H2S donors in C57BL/6 mice, and then tested whether their effects depend on the transient receptor potential ankyrin-1 (TRPA1) channel in Trpa1 knockout (Trpa1−/−) and wild-type (Trpa1+/+) mice. Intracerebroventricular administration of Na2S (0.5–1 mg/kg) caused hypothermia in C57BL/6 mice, which was mediated by cutaneous vasodilation and decreased thermogenesis. In contrast, intraperitoneal administration of Na2S (5 mg/kg) did not cause any thermoregulatory effect. Central administration of GYY4137 (3 mg/kg) also caused hypothermia and hypometabolism. The hypothermic response to both H2S donors was significantly (p &lt, 0.001) attenuated in Trpa1−/− mice compared to their Trpa1+/+ littermates. Trpa1 mRNA transcripts could be detected with RNAscope in hypothalamic and other brain neurons within the autonomic thermoeffector pathways. In conclusion, slow- and fast-releasing H2S donors induce hypothermia through hypometabolism and cutaneous vasodilation in mice that is mediated by TRPA1 channels located in the brain, presumably in hypothalamic neurons within the autonomic thermoeffector pathways.

Published

2021

36. Important regulatory function of transient receptor potential ankyrin 1 receptors in age-related learning and memory alterations of mice

Author

Maja Payrits, Éva Borbély, Ágnes Hunyady, Erika Pintér, and Gréta Mező

Subjects

Aging, medicine.medical_specialty, Morris water navigation task, Hippocampus, Biology, TRPA1, Transient receptor potential channel, Memory, Internal medicine, medicine, Learning, Animals, Ankyrin, Maze Learning, Receptor, TRPA1 Cation Channel, Mice, Knockout, chemistry.chemical_classification, Memory Disorders, Radial arm maze, food and beverages, Cortex (botany), Disease Models, Animal, Endocrinology, chemistry, Hypothalamus, Exploratory Behavior, Original Article, Dementia, Geriatrics and Gerontology, Locomotion, psychological phenomena and processes

Abstract

Expression of the transient receptor potential ankyrin 1 (TRPA1) receptor has been demonstrated not only in the dorsal root and trigeminal ganglia but also in different brain regions (e.g., hippocampus, hypothalamus, and cortex). However, data concerning their role in neurodegenerative and age-related diseases of the CNS is still indistinct. The aim of our study was to investigate the potential role of TRPA1 in a mouse model of senile dementia. For the investigation of changes during aging, we used male young (3–4-month-old) and old (18-month-old) wild-type (TRPA1+/+;WT) and TRPA1 receptor gene-deleted (TRPA1−/−) mice. Novel object recognition (NOR) test as well as Y maze (YM), radial arm maze (RAM), and Morris water maze (MWM) tests were used to assess the decline of memory and learning skills. In the behavioral studies, significant memory loss was detected in aged TRPA1+/+ mice with the NOR and RAM, but there was no difference measured by YM and MWM tests regarding the age and gene. TRPA1−/− showed significantly reduced memory loss, which could be seen as higher discrimination index in the NOR and less exploration time in the RAM. Furthermore, young TRPA1−/− animals showed significantly less reference memory error in the RAM and notably higher mobility in NOR, RAM, and YM compared with the age-matched WTs. Our present work has provided the first evidence that TRPA1 receptors mediate deteriorating effects in the old age memory decline. Understanding the underlying mechanisms could open new perspectives in the pharmacotherapy of dementia.

Published

2019

37. Methodological refinement of Aldara-induced psoriasiform dermatitis model in mice

Author

Erika Pintér, Anikó Perkecz, R. Komlódi, Rolland Gyulai, S. Horváth, and Ágnes Kemény

Subjects

0301 basic medicine, medicine.medical_specialty, Petrolatum, medicine.medical_treatment, lcsh:Medicine, Inflammation, Imiquimod, Dermatitis, Article, Vaseline, 03 medical and health sciences, 0302 clinical medicine, Psoriasis, medicine, Animals, lcsh:Science, Psoriasiform Dermatitis, Multidisciplinary, CD11b Antigen, integumentary system, business.industry, lcsh:R, Histology, medicine.disease, Dermatology, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Cytokine, Cytokines, Female, lcsh:Q, medicine.symptom, business, Perfusion, 030217 neurology & neurosurgery, medicine.drug

Abstract

Imiquimod (IMQ)-induced skin inflammation is currently the most widely accepted psoriasis animal model, however, it features several limitations. We have modified the IMQ-model to minimize its systemic effects towards effectively maintaining the characteristic skin reactions. The original protocol (OP) uses 62.5 mg Aldara cream (or vaseline) on the shaved back skin of mice for 4 days. In contrast, in our modified protocol (MP) 25 mg Aldara and vaseline are applied simultaneously in separate Finn chambers over the dorsal skin of mice. In both the OP and MP groups, histology showed unequivocal hallmarks of psoriasiform dermatitis. Additionally, skin scaling and blood perfusion values were similar. While Aldara elicited significantly increased skin thickness in the MP group, significant weight loss, spleen enlargement, increased inflammatory cytokine levels in plasma, and treatment related death were only observed in the OP group. Our new method reproduces psoriatic skin alterations highlighting considerably reduced systemic inflammatory reactions. Possessing psoriasiform and control skin areas on the same mouse also reduces inter-individual differences. Additionally, the new method permits prolonged IMQ treatment studies to mimic the chronic nature of psoriasis. Finally, our experimental approach may also be used in other mouse models, to prevent the undesired systemic effects of topically applied drugs.

Published

2019

38. Human Somatostatin SST4 Receptor Transgenic Mice: Construction and Brain Expression Pattern Characterization

Author

Viktória Kormos, Timea Aczél, Zoltán Sándor, Balázs Nemes, Kata Bölcskei, Zsuzsanna Helyes, Erika Pintér, Dániel Hegedüs, Angéla Kecskés, and Balázs Gaszner

Subjects

Genetically modified mouse, endocrine system, Sstr4 KO mice, CA2 Region, Hippocampal, Hippocampus, Mice, Transgenic, Biology, somatostatin, Article, Catalysis, Inorganic Chemistry, lcsh:Chemistry, Glutamatergic, Mice, ligation-mediated PCR, Piriform cortex, PiggyBac (PB) transposon vector, Animals, Humans, SSTR4 humanized mice, Receptors, Somatostatin, Physical and Theoretical Chemistry, Molecular Biology, CA1 Region, Hippocampal, lcsh:QH301-705.5, Spectroscopy, Neurons, Reporter gene, Somatostatin receptor, Organic Chemistry, General Medicine, RNAscope in situ hybridization, Computer Science Applications, Cell biology, Olfactory bulb, Gene Expression Regulation, lcsh:Biology (General), lcsh:QD1-999, Humanized mouse, hormones, hormone substitutes, and hormone antagonists

Abstract

Somatostatin receptor subtype 4 (SST4) has been shown to mediate analgesic, antidepressant and anti-inflammatory functions without endocrine actions, therefore, it is proposed to be a novel target for drug development. To overcome the species differences of SST4 receptor expression and function between humans and mice, we generated an SST4 humanized mouse line to serve as a translational animal model for preclinical research. A transposon vector containing the hSSTR4 and reporter gene construct driven by the hSSTR4 regulatory elements were created. The vector was randomly inserted in Sstr4-deficient mice. hSSTR4 expression was detected by bioluminescent in vivo imaging of the luciferase reporter predominantly in the brain. RT-qPCR confirmed the expression of the human gene in the brain and various peripheral tissues consistent with the in vivo imaging. RNAscope in situ hybridization revealed the presence of hSSTR4 transcripts in glutamatergic excitatory neurons in the CA1 and CA2 regions of the hippocampus, in the GABAergic interneurons in the granular layer of the olfactory bulb and in both types of neurons in the primary somatosensory cortex, piriform cortex, prelimbic cortex and amygdala. This novel SST4 humanized mouse line might enable us to investigate the differences of human and mouse SST4 receptor expression and function and assess the effects of SST4 receptor agonist drug candidates.

Published

2021

39. Dimethyl Trisulfide Diminishes Traumatic Neuropathic Pain Acting on TRPA1 Receptors in Mice

Author

Gábor Pozsgai, Angéla Kecskés, Csenge Sánta, Viktória Kormos, Valéria Tékus, Krisztina Pohóczky, István Bátai, Kata Bölcskei, Ágnes Dombi, and Erika Pintér

Subjects

Male, microglia, sciatic nerve, partial ligation, Pharmacology, Sulfides, somatostatin, TRPA1, Catalysis, Article, Inorganic Chemistry, lcsh:Chemistry, Mice, Dorsal root ganglion, Spinal Cord Dorsal Horn, Ganglia, Spinal, Medicine, Animals, RNA, Messenger, Physical and Theoretical Chemistry, Molecular Biology, TRPA1 Cation Channel, lcsh:QH301-705.5, RNAscope, Spectroscopy, Mice, Knockout, neuropathic pain, Microscopy, Confocal, Microglia, business.industry, Organic Chemistry, dimethyl trisulfide, General Medicine, SST4, Computer Science Applications, Mice, Inbred C57BL, medicine.anatomical_structure, Somatostatin, lcsh:Biology (General), lcsh:QD1-999, Hyperalgesia, Neuropathic pain, Nociceptor, Neuralgia, Sciatic nerve, business, Free nerve ending

Abstract

Pharmacotherapy of neuropathic pain is still challenging. Our earlier work indicated an analgesic effect of dimethyl trisulfide (DMTS), which was mediated by somatostatin released from nociceptor nerve endings acting on SST4 receptors. Somatostatin release occurred due to TRPA1 ion channel activation. In the present study, we investigated the effect of DMTS in neuropathic pain evoked by partial ligation of the sciatic nerve in mice. Expression of the mRNA of Trpa1 in murine dorsal-root-ganglion neurons was detected by RNAscope. Involvement of TRPA1 ion channels and SST4 receptors was tested with gene-deleted animals. Macrophage activity at the site of the nerve lesion was determined by lucigenin bioluminescence. Density and activation of microglia in the spinal cord dorsal horn was verified by immunohistochemistry and image analysis. Trpa1 mRNA is expressed in peptidergic and non-peptidergic neurons in the dorsal root ganglion. DMTS ameliorated neuropathic pain in Trpa1 and Sstr4 WT mice, but not in KO ones. DMTS had no effect on macrophage activity around the damaged nerve. Microglial density in the dorsal horn was reduced by DMTS independently from TRPA1. No effect on microglial activation was detected. DMTS might offer a novel therapeutic opportunity in the complementary treatment of neuropathic pain.

Published

2021

40. Protective effects of the novel amine-oxidase inhibitor multi-target drug SZV 1287 on streptozotocin-induced beta cell damage and diabetic complications in rats

Author

Péter Mátyus, Bese Danyadi, Erika Pintér, Péter Ferdinandy, Zsuzsanna Helyes, Krisztina Szabadfi, Laszlo Deres, Ernest Adeghate, Kata Csekő, Robert Halmosi, Éva Sághy, Robert Gábriel, Valéria Tékus, Andrea Kovács-Valasek, Zoltán Varga, Tamás Kőszegi, and Ádám Horváth

Subjects

0301 basic medicine, Male, Diabetic neuropathy, AOC3, medicine.medical_treatment, Vascular adhesion protein 1, LJP 1207, Pharmacology, Rats, Sprague-Dawley, chemistry.chemical_compound, 0302 clinical medicine, Diabetic retinopathy, Insulin-Secreting Cells, Oximes, Insulin, Diabetic Nephropathies, Oxazoles, Analgesics, Streptozotocin, Amine oxidase (copper-containing), General Medicine, Fructosamine, Hydrazines, 030220 oncology & carcinogenesis, Amine Oxidase (Copper-Containing), Beta cell, medicine.drug, Monoamine Oxidase Inhibitors, Semicarbazide-sensitive amine oxidase, RM1-950, Streptozocin, Diabetes Mellitus, Experimental, Diabetes Complications, 03 medical and health sciences, Diabetes mellitus, medicine, Animals, Humans, Creatinine, business.industry, medicine.disease, Rats, 030104 developmental biology, chemistry, Therapeutics. Pharmacology, business, Cell Adhesion Molecules

Abstract

Diabetes mellitus is a common metabolic disease leading to hyperglycemia due to insufficient pancreatic insulin production or effect. Amine oxidase copper containing 3 (AOC3) is an enzyme that belongs to the semicarbazide-sensitive amine oxidase family, which may be a novel therapeutic target to treat diabetic complications. We aimed to explore the effects of AOC3 inhibition and to test the actions of our novel AOC3 inhibitor multi-target drug candidate, SZV 1287, compared to a selective reference compound, LJP 1207, in an 8-week long insulin-controlled streptozotocin (STZ)-induced (60 mg/kg i.p.) rat diabetes model. Both AOC3 inhibitors (20 mg/kg, daily s.c. injections) were protective against STZ-induced pancreatic beta cell damage determined by insulin immunohistochemistry and radioimmunoassay, neuropathic cold hypersensitivity measured by paw withdrawal latency decrease from 0 °C water, and retinal dysfunction detected by electroretinography. SZV 1287 showed greater inhibitory effects on beta cell damage, and reduced retinal apoptosis shown by histochemistry. Mechanical hypersensitivity measured by aesthesiometry, cardiac dysfunction and nitrosative stress determined by echocardiography and immunohistochemistry/Western blot, respectively, serum Na+, K+, fructosamine, and urine microalbumin, creatinine, total protein/creatinine ratio alterations did not develop in response to diabetes. None of these parameters were influenced by the treatments except for SZV 1287 reducing serum fructosamine and LJP 1207 increasing urine creatinine. We provide the first evidence for protective effects of AOC3 inhibition on STZ-induced pancreatic beta cell damage, neuropathic cold hypersensitivity and diabetic retinal dysfunction. Long-term treatment with our novel multi-target analgesic candidate, SZV 1287, is safe and effective also under diabetic conditions.

Published

2021

41. Nitrosopersulfide (SSNO-) is a unique cysteine polysulfidating agent with reduction-resistant bioactivity

Author

Klaudia Galambos, Virág Bogdándi, Péter Buglyó, István Bátai, Zoltán Sándor, Péter Nagy, Martin Feelisch, Anita Vasas, Tamás Ditrói, Erika Pintér, and Magdalena Minnion

Subjects

0301 basic medicine, chemistry.chemical_classification, Reactive oxygen species, 030102 biochemistry & molecular biology, Sulfide, Physiology, Hydrogen sulfide, Clinical Biochemistry, Cell Biology, Biochemistry, Combinatorial chemistry, Nitric oxide, Reduction (complexity), 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, chemistry, General Earth and Planetary Sciences, Molecular Biology, General Environmental Science, Cysteine

Abstract

Aims: The aim of the present study was to investigate the biochemical properties of nitrosopersulfide (SSNO -), a key intermediate of the nitric oxide (NO)/sulfide cross talk. Results: We obtained corroborating evidence that SSNO - is indeed a major product of the reaction of S-nitrosothiols with hydrogen sulfide (H 2S). It was found to be relatively stable (t 1/2 *1 h at room temperature) in aqueous solution of physiological pH, stabilized by the presence of excess sulfide and resistant toward reduction by other thiols. Furthermore, we here show that SSNO - escapes the reducing power of the NADPH-driven biological reducing machineries, the thioredoxin and glutathione reductase systems. The slow decomposition of SSNO - produces inorganic polysulfide species, which effectively induce per/polysulfidation on glutathione or protein cysteine (Cys) residues. Our data also demonstrate that, in contrast to the transient activation by inorganic polysulfides, SSNO - induces long-term potentiation of TRPA1 (transient receptor potential ankyrin 1) channels, which may be due to its propensity to generate a slow flux of polysulfide in situ. Innovation: The characterized properties of SSNO - would seem to represent unique features in cell signaling by enabling sulfur and nitrogen trafficking within the reducing environment of the cytosol, with targeted release of both NO and polysulfide equivalents. Conclusion: SSNO - is a surprisingly stable bioactive product of the chemical interaction of S-nitrosothiol species and H 2S that is resistant to reduction by the thioredoxin and glutathione systems. As well as generating NO, it releases inorganic polysulfides, enabling transfer of sulfane sulfur species to peptide/protein Cys residues. The sustained activation of TRPA1 channels by SSNO - is most likely linked to all these properties. Antioxid. Redox Signal. 33, 1277–1294.

Published

2020

42. Personalised health education against health damage of COVID-19 epidemic in the elderly hungarian population (PROACTIVE-19): protocol of an adaptive randomised controlled clinical trial

Author

Borbála Zsigmond, Márk Félix Juhász, Lajos Szakó, Anikó Nagy, Andrea Sárközi, Nelli Farkas, Eszter Hegyi, Zsolt Szakács, Bálint Erőss, Antal Zemplényi, Péter Hegyi, Dominika Tóth, László Czopf, Gábor Pethő, Attila Márta, András Varró, Zoltán Péterfi, Szabolcs Kiss, Noémi Zádori, Anna Kanjo, Szilárd Váncsa, Richárd Farkas, Dalma Dobszai, Andrea Szentesi, Andrea Párniczky, Erika Pintér, Emőke Miklós, Piroska Pázmány, Fanni Dembrovszky, Zsuzsanna Helyes, Zsolt Molnár, Béla Birkás, Klementina Ocskay, Dóra Czapári, István Kiss, Katalin Márta, Mária Földi, Árpád Csathó, Nóra Vörhendi, and Péter Jenő Hegyi

Subjects

Male, Health Knowledge, Attitudes, Practice, Health Status, Psychological intervention, Medicine (miscellaneous), 030204 cardiovascular system & hematology, law.invention, Study Protocol, 0302 clinical medicine, Randomized controlled trial, law, Risk Factors, Clinical endpoint, Medicine, Pharmacology (medical), 030212 general & internal medicine, Health Education, Aged, 80 and over, Randomised controlled trial, lcsh:R5-920, education.field_of_study, Public health, Adaptive Clinical Trials as Topic, Smoking, Age Factors, Middle Aged, Mental Health, Host-Pathogen Interactions, Health education, Female, lcsh:Medicine (General), Coronavirus Infections, medicine.medical_specialty, Alcohol Drinking, Population, Pneumonia, Viral, Risk Assessment, 03 medical and health sciences, Betacoronavirus, Pragmatic Clinical Trials as Topic, Humans, education, Exercise, Pandemics, Aged, Hungary, business.industry, SARS-CoV-2, nCov-2019, Prevention, COVID-19, Feeding Behavior, Protective Factors, Mental health, Clinical trial, Family medicine, business, Risk Reduction Behavior

Abstract

Background Early reports indicate that COVID-19 may require intensive care unit (ICU) admission in 5–26% and overall mortality can rise to 11% of the recognised cases, particularly affecting the elderly. There is a lack of evidence-based targeted pharmacological therapy for its prevention and treatment. We aim to compare the effects of a World Health Organization recommendation-based education and a personalised complex preventive lifestyle intervention package (based on the same WHO recommendation) on the outcomes of the COVID-19. Methods PROACTIVE-19 is a pragmatic, randomised controlled clinical trial with adaptive “sample size re-estimation” design. Hungarian population over the age of 60 years without confirmed COVID-19 will be approached to participate in a telephone health assessment and lifestyle counselling voluntarily. Volunteers will be randomised into two groups: (A) general health education and (B) personalised health education. Participants will go through questioning and recommendation in 5 fields: (1) mental health, (2) smoking habits, (3) physical activity, (4) dietary habits, and (5) alcohol consumption. Both groups A and B will receive the same line of questioning to assess habits concerning these topics. Assessment will be done weekly during the first month, every second week in the second month, then monthly. The composite primary endpoint will include the rate of ICU admission, hospital admission (longer than 48 h), and mortality in COVID-19-positive cases. The estimated sample size is 3788 subjects per study arm. The planned duration of the follow-up is a minimum of 1 year. Discussion These interventions may boost the body’s cardiovascular and pulmonary reserve capacities, leading to improved resistance against the damage caused by COVID-19. Consequently, lifestyle changes can reduce the incidence of life-threatening conditions and attenuate the detrimental effects of the pandemic seriously affecting the older population. Trial registration The study has been approved by the Scientific and Research Ethics Committee of the Hungarian Medical Research Council (IV/2428- 2 /2020/EKU) and has been registered at clinicaltrials.gov (NCT04321928) on 25 March 2020.

Published

2020

43. Personalised health education against the health damage of COVID-19 epidemic in Hungary (PROACTIVE-19): protocol of an adaptive randomised controlled clinical trial

Author

Bálint Erőss, Zsolt Molnár, Zsolt Szakács, Noémi Zádori, Lajos Szakó, Szilárd Váncsa, Félix Juhász, Klementina Ocskay, Nóra Vörhendi, Katalin Márta, Andrea Szentesi, Andrea Párniczky, Péter J. Hegyi, Szabolcs Kiss, Mária Földi, Fanni Dembrovszky, Anna Kanjo, Piroska Pázmány, András Varró, Árpád Csathó, Zsuzsanna Helyes, Zoltán Péterfi, László Czopf, István Kiss, Antal Zemplényi, Dóra Czapári, Eszter Hegyi, Dalma Dobszai, Emőke Miklós, Attila Márta, Dominika Tóth, Richard Farkas, Nelli Farkas, Béla Birkás, Erika Pintér, Gábor Pethő, Borbála Zsigmond, Andrea Sárközi, Anikó Nagy, and Péter Hegyi

Abstract

Background: Early reports indicate that COVID-19 may require intensive care unit (ICU) admission in 5-26% and overall mortality can rise to 11% of the recognized cases, particularly affecting the elderly. There is a lack of evidence-based targeted pharmacological therapy for prevention and treatment alike. We aim to compare the effects of a World Health Organisation (WHO) recommendations’ based education and a personalised complex preventive lifestyle intervention package (based on the same WHO recommendation) on the outcomes of the COVID-19.Methods: PROACTIVE-19 is a pragmatic, randomized controlled clinical trial with adaptive “sample size re-estimation” design. Hungarian population over the age of 60 years without confirmed COVID-19 will be approached to participate in a telephone health assessment and lifestyle counselling voluntarily. Volunteers will be randomized into two groups: (A) general health education; (B) personalized health education. Participants will go through questioning and recommendation in 5 fields: (1) mental health, (2) smoking habits, (3) physical activity, (4) dietary habits, (5) alcohol consumption. Both groups A and B will receive the same line of questioning to assess habits concerning these topics. Assessment will be done weekly during the first month, every second week in the second month, then monthly. The composite primary endpoint will include the rate of ICU admission, hospital admission (longer han 48 hours) and mortality in COVID-19 positive cases. The estimated sample size is 3788 subjects per study arm. The planned duration of the follow-up is a minimum of one year.Discussion: These interventions may boost the body’s cardiovascular and pulmonary reserve capacities, leading to improved resistance against the damage caused by COVID-19. Consequently, lifestyle changes can reduce the incidence of life-threatening conditions and attenuate the detrimental effects of the pandemic seriously affecting the older population. Trial registration: The study has been approved by the Scientific and Research Ethics Committee of the Hungarian Medical Research Council (IV/2428- 2 /2020/EKU) and has been registered at clinicaltrials.gov (NCT04321928) on 25 March, 2020.

Published

2020

44. A Localized Aldara (5% Imiquimod)-Induced Psoriasiform Dermatitis Model in Mice Using Finn Chambers

Author

Erika Pintér, Rolland Gyulai, S. Horváth, and Ágnes Kemény

Subjects

0301 basic medicine, medicine.medical_specialty, Imiquimod, Dermatitis, Systemic inflammation, 03 medical and health sciences, Psoriatic skin, Mice, 0302 clinical medicine, Psoriasis, medicine, Animals, Psoriasiform Dermatitis, Skin, integumentary system, business.industry, Functional measurement, General Medicine, medicine.disease, Dermatology, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Research studies, Female, medicine.symptom, business, Perfusion, 030217 neurology & neurosurgery, medicine.drug

Abstract

The expanding number of research studies utilizing the imiquimod-induced psoriasiform dermatitis model attests to the usefulness of this procedure. Advantages of this model include rapid development of the skin response and cost-effectiveness. A major limitation is that application of imiquimod cream over large areas of skin, as well as licking and ingestion of the cream, may lead to severe systemic inflammation, which can cause a general decline in health, splenomegaly, and death. In this protocol, Finn chambers are used to localize the imiquimod cream to a small area of the skin. This results in production of severe and reproducible psoriatic skin reactions with significantly less imiquimod, greatly reducing the possibility of untoward systemic effects. Moreover, having psoriasiform and control skin areas on the same mice decreases inter-animal differences. The protocol can be readily adapted for other skin disease models involving topical application of test agents. This article also details functional measurements performed during assays, including skin thickness, blood perfusion, semiquantitative histopathological evaluation, determination of scaling score to monitor psoriatic symptoms, and collection of spleen and body weight data to identify systemic effects. © 2020 The Authors. Basic Protocol: Use of Finn chambers to induce psoriasiform skin reactions with imiquimod Support Protocol 1: Measurement of double-fold dorsal skin thickness Support Protocol 2: Measurement of blood perfusion Support Protocol 3: Determination of scaling score Support Protocol 4: Semiquantitative histopathological scoring Support Protocol 5: Assessment of systemic side effects in response to imiquimod application.

Published

2020

45. Complex Regulatory Role of the TRPA1 Receptor in Acute and Chronic Airway Inflammation Mouse Models

Author

Zsófia Hajna, István Szitter, Béla Kocsis, Anikó Perkecz, Zsuzsanna Helyes, Erika Pintér, László Kereskai, Tamás Kiss, Kata Csekő, and Ágnes Kemény

Subjects

Lipopolysaccharides, Male, Chronic bronchitis, Pharmacology, bronchitis, lcsh:Chemistry, whole body plethysmography, Respiratory system, Lung, TRPA1 Cation Channel, lcsh:QH301-705.5, Spectroscopy, Tidal volume, COPD, cigarette smoke, pneumonitis, food and beverages, General Medicine, Computer Science Applications, Respiratory Function Tests, Bronchitis, Chronic, medicine.anatomical_structure, emphysema, Pulmonary Emphysema, Bronchitis, Female, Bronchoalveolar Lavage Fluid, psychological phenomena and processes, LPS, Catalysis, Article, Cigarette Smoking, Inorganic Chemistry, medicine, Animals, Physical and Theoretical Chemistry, Molecular Biology, Pneumonitis, Peroxidase, Plethysmography, Whole Body, business.industry, Organic Chemistry, Pneumonia, medicine.disease, Mice, Mutant Strains, Mice, Inbred C57BL, Disease Models, Animal, lcsh:Biology (General), lcsh:QD1-999, business, Respiratory minute volume

Abstract

The Transient Receptor Potential Ankyrin 1 (TRPA1) cation channel expressed on capsaicin-sensitive afferents, immune and endothelial cells is activated by inflammatory mediators and exogenous irritants, e.g., endotoxins, nicotine, crotonaldehyde and acrolein. We investigated its involvement in acute and chronic pulmonary inflammation using Trpa1 gene-deleted (Trpa1&minus, /&minus, ) mice. Acute pneumonitis was evoked by intranasal Escherichia coli endotoxin (lipopolysaccharide: LPS) administration, chronic bronchitis by daily cigarette smoke exposure (CSE) for 4 months. Frequency, peak inspiratory/expiratory flows, minute ventilation determined by unrestrained whole-body plethysmography were significantly greater, while tidal volume, inspiratory/expiratory/relaxation times were smaller in Trpa1&minus, mice. LPS-induced bronchial hyperreactivity, myeloperoxidase activity, frequency-decrease were significantly greater in Trpa1&minus, mice. CSE significantly decreased tidal volume, minute ventilation, peak inspiratory/expiratory flows in wildtypes, but not in Trpa1&minus, mice. CSE remarkably increased the mean linear intercept (histopathology), as an emphysema indicator after 2 months in wildtypes, but only after 4 months in Trpa1&minus, mice. Semiquantitative histopathological scores were not different between strains in either models. TRPA1 has a complex role in basal airway function regulation and inflammatory mechanisms. It protects against LPS-induced acute pneumonitis and hyperresponsiveness, but is required for CSE-evoked emphysema and respiratory deterioration. Further research is needed to determine TRPA1 as a potential pharmacological target in the lung.

Published

2020

46. Effect of angiotensin-converting enzyme inhibitors and angiotensin receptor blockers on the angiotensin-converting enzyme 2 levels in experimental models, and clinical outcomes of COVID-19 in humans

Author

Gábor Kriszta, Zsófia Kriszta, Bálint Erőss, Gabriella Pár, Péter Jenő Hegyi, Szilárd Váncsa, Szabolcs Kiss, Katalin Márta, Levente Frim, Lóránd Kiss, Margit Solymár, Gábor Pethő, László Czopf, Zsolt Szakács, Péter Hegyi, and Erika Pintér

Subjects

angiotensin-converting enzyme inhibitor, SARS-CoV-2, pandemic, coronavirus, angiotensin-converting enzyme-2, COVID-19, severity, angiotensin receptor blocker, hormones, hormone substitutes, and hormone antagonists, animal models

Abstract

Introduction A new coronavirus, the severe acute respiratory syndrome coronavirus 2 (SARS-CoV2), was first reported to cause human infection in Wuhan, China, in December 2019. The virus by now has been detected in all continents except Antarctica. The name represents the form of “corona,” from the many crown-like spike proteins on the surface of the virus. These spikes thought to be the main domain in connection to angiotensin-converting enzyme 2 (ACE2) on the cell surface; therefore, the mechanism of virus entry is already hypothesized. There are disagreements about the use of the renin-angiotensin-aldosterone system (RAAS) inhibitors that may alter ACE2 expression. Therefore, the use of angiotensin-converting enzyme inhibitors (ACEIs) and angiotensin receptor blockers (ARBs) and the consequent dynamics in ACE2 expression might affect the virulence and the outcome of the infection. Coronavirus disease-19 (COVID-19) is a pandemic with significant mortality. One of the critical comorbidities leading to adverse outcomes is cardiovascular disease (CVD). Patients with cardiovascular diseases (CVDs) are often treated with ACEIs and ARBs acting on RAAS. ACEIs and ARBs might upregulate the expression of ACE2, providing more gates to the virus to enter the cells; they also exert beneficial hemodynamic, anti-inflammatory, and tissue-protective effects. Given the frequent use of ACEIs and ARBs worldwide, evidence-based recommendations on the use of these agents in patients with COVID-19 is urgently needed. Aim First, we aim to investigate the effects of ACEIs and ARBs on ACE2 activity and expression in experimental in vitro and in vivo animal models. Second, we will examine the impact of ACEIs and ARBs on the reported outcomes of COVID-19 involving patients’ data. Scientific questions in the systematic review on experimental data are: Whether the angiotensin-converting enzyme inhibitors and angiotensin receptor blockers could influence the expression of the ACE2? What is the tissue distribution of ACE2? What is the role of ACE2 in different pathological conditions (myocardial hypoxia, hypertension, heart failure, inflammatory diseases, oxidative stress, etc.)? How does ACE2 influence the expression dynamics of angiotensin-like peptide levels (Angiotensin 1-7, Angiotensin 1-9)? Scientific questions in the systematic review or meta-analysis on clinical data is: Do ACEIs and ARBs have any effect on the outcome of the infection? Finally, we aim to integrate the findings of both systematic reviews and interpret the experimental data in light of the clinical result. Methods Two separate systematic reviews and -if possible -a clinical meta-analysis will be performed to answer the questions mentioned above. Data We plan to include published data in peer-reviewed scientific papers. In consideration of the contemporary importance of COVID-19, we keep on systematic screening the publications daily and involve relevant papers to our study. Two independent review teams will perform each systematic review. In each independent review team, two independent reviewers will make the selection by title, abstract, and full text. The disagreements between the independent reviewers will be resolved through consensus and discussion involving the senior leaders of each systematic review team.

Published

2020

47. Nitrosopersulfide (SSNO

Author

Virág, Bogdándi, Tamás, Ditrói, István Zoárd, Bátai, Zoltán, Sándor, Magdalena, Minnion, Anita, Vasas, Klaudia, Galambos, Péter, Buglyó, Erika, Pintér, Martin, Feelisch, and Péter, Nagy

Subjects

Cysteine, Hydrogen Sulfide, Sulfides, Nitric Oxide, Oxidation-Reduction, Protein Processing, Post-Translational, Signal Transduction

Published

2020

48. Effects of sulfide and polysulfides transmitted by direct or signal transduction-mediated activation of TRPA1 channels

Author

István Bátai, Gábor Pozsgai, and Erika Pintér

Subjects

0301 basic medicine, Pharmacology, chemistry.chemical_classification, Sulfide, Hydrogen sulfide, 03 medical and health sciences, chemistry.chemical_compound, Transient receptor potential channel, Crosstalk (biology), 030104 developmental biology, 0302 clinical medicine, Mediator, chemistry, Biophysics, Signal transduction, 030217 neurology & neurosurgery, Polysulfide, Ion channel

Abstract

Hydrogen sulfide (H2 S) is a gaseous mediator in various physiological and pathological processes, including neuroimmune modulation, metabolic pathways, cardiovascular system, tumour growth, inflammation and pain. Now the hydrogen polysulfides (H2 Sn ) have been recognised as signalling molecules modulating ion channels, transcription factors and protein kinases. Transient receptor potential (TRP) cation channels can be activated by mechanical, thermal or chemical triggers. Here, we review the current literature regarding the biological actions of sulfide and polysulfide compounds mediated by TRP channels with special emphasis on the role of TRPA1, best known as ion channels in nociceptors. However, the non-neuronal TRPA1 channels should also be considered to play regulatory roles. Although sulfide and polysulfide effects in different pathological circumstances and TRPA1-mediated processes have been investigated intensively, our review attempts to present the first comprehensive overview of the potential crosstalk between TRPA1 channels and sulfide-activated signalling pathways. LINKED ARTICLES: This article is part of a themed section on Chemical Biology of Reactive Sulfur Species. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v176.4/issuetoc.

Published

2018

49. Complex Role of Capsaicin-Sensitive Afferents in the Collagen Antibody-Induced Autoimmune Arthritis of the Mouse

Author

János Szolcsányi, Krisztina Szabadfi, Éva Borbély, Erika Pintér, Tamás Kiss, Zsuzsanna Helyes, and Bálint Botz

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Resiniferatoxin, Arthritis, lcsh:Medicine, Severity of Illness Index, Bone resorption, Antibodies, Article, 03 medical and health sciences, chemistry.chemical_compound, Mice, Edema, Internal medicine, medicine, Animals, Neurons, Afferent, lcsh:Science, Multidisciplinary, business.industry, Body Weight, lcsh:R, X-Ray Microtomography, medicine.disease, Arthritis, Experimental, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Allodynia, Endocrinology, chemistry, Capsaicin, Hyperalgesia, Rheumatoid arthritis, lcsh:Q, medicine.symptom, Diterpenes, business, Ankle Joint

Abstract

Capsaicin-sensitive afferents have complex regulatory functions in the joints orchestrated via neuropeptides. This study aimed to determine their role in the collagen-antibody induced rheumatoid arthritis model. Capsaicin-sensitive nerves were defunctionalized by the capsaicin receptor agonist resiniferatoxin in C57Bl/6 mice. Arthritis was induced by the ArithroMab antibody cocktail and adjuvant. Arthritis was monitored by measuring body weight, joint edema by plethysmometry, arthritis severity by clinical scoring, mechanonociceptive threshold by plantar esthesiometry, thermonociceptive threshold by hot plate, cold tolerance by paw withdrawal latency from 0 °C water. Grasping ability was determined by the wire-grid grip test. Bone structure was evaluated by in vivo micro-CT and histology. Arthritic animals developed a modest joint edema, mechanical and cold hyperalgesia, weight loss, and a diminished grasping function, while thermal hyperalgesia is absent in the model. Desensitised mice displayed reduced arthritis severity, edema, and mechanical hyperalgesia, however, cold hyperalgesia was significantly greater in this group. Arthritic controls displayed a transient decrease of bone volume and an increased porosity, while bone density and trabecularity increased in desensitised mice. The activation of capsaicin-sensitive afferents increases joint inflammation and mechanical hyperalgesia, but decreases cold allodynia. It also affects inflammatory bone structural changes by promoting bone resorption.

Published

2018

50. Upregulation of extraneuronal TRPV1 expression in chronic rhinosinusitis with nasal polyps

Author

Tamás Tornóczky, Ágnes Kemény, Imre Gerlinger, Anikó Perkecz, József Kun, Józsefné Kneif, Eszter Tóth, Erika Pintér, Zalán Piski, Krisztián Katona, and János Szolcsányi

Subjects

Adult, 0301 basic medicine, Allergy, Adolescent, Biopsy, Population, TRPV1, TRPV Cation Channels, Plasma cell, Polymerase Chain Reaction, Pathogenesis, 03 medical and health sciences, Nasal Polyps, Downregulation and upregulation, medicine, Humans, Nasal polyps, Sinusitis, Receptor, education, TRPA1 Cation Channel, Aged, Rhinitis, education.field_of_study, business.industry, musculoskeletal, neural, and ocular physiology, food and beverages, General Medicine, Middle Aged, medicine.disease, Immunohistochemistry, Up-Regulation, 030104 developmental biology, medicine.anatomical_structure, nervous system, Otorhinolaryngology, Case-Control Studies, Chronic Disease, Immunology, Cytokines, lipids (amino acids, peptides, and proteins), business, psychological phenomena and processes

Abstract

Background Chronic rhinosinusitis (CRS) is a multifactorial upper airway disease with unclear etiology. Neuronal Transient Receptor Potential Vanilloid 1 (TRPV1) and Ankyrin 1 (TRPA1) channels have been implicated in the pathogenesis of CRS. We aimed to detect the expression of extraneuronal TRPV1 and TRPA1 receptors in nasal polyp (NP) tissue samples. Methodology Samples were obtained from fourty-two CRS pateints with nasal polyp and sixteen healthy controls to measure receptor gene expression by quantitative PCR, protein localization by immunohistochemistry and cytokine profile by multiplex bead immunoassay. Results Non-neuronal TRPV1, TRPA1 receptors were expressed in biopsy samples of NP. A population of mast cells and macrophages were immunopositive for TRPV1 and TRPA1. A fraction of plasma cells expressed TRPV1 but not TRPA1 and neither receptor was present on eosinophils. The local gene expression of extraneuronal TRPV1, TRPA1 receptors was also proven. TRPV1 mRNA levels were significantly increased in CRSwNP patients with asthma and allergic rhinitis compared to their NP counterparts. Conclusions Elevated TRPV1 levels in comorbid asthma and allergy may have a function in CRSwNP. Subpopulation-specific TRPV1 presence on plasma and mast cells can indicate delicate roles in regulating activation and release of inflammatory mediators.

Published

2018