Your search keyword '"RECEPTOR ANTAGONIST"' showing total 20,561 results

1. Full-length and N-terminally truncated recombinant interleukin-38 variants are similarly inefficient in antagonizing interleukin-36 and interleukin-1 receptors.

Author

Diaz-Barreiro, Alejandro, Talabot-Ayer, Dominique, Huard, Arnaud, Cereghetti, Gea, Tonacini, Jenna, Maillasson, Mike, Francés-Monerris, Antonio, Mortier, Erwan, and Palmer, Gaby

Subjects

*RECOMBINANT proteins, *LIFE sciences, *SURFACE plasmon resonance, *INTERLEUKIN-1 receptors, *CYTOLOGY, KERATINOCYTE differentiation

Abstract

Background: Interleukin (IL)-38 is an IL-1 family cytokine that was proposed to exert anti-inflammatory effects. However, its mechanisms of action are not well understood and the identity of the IL-38 receptor(s) remains debated. Proposed candidates include the IL-1 receptor (IL-1R1), the IL-36 receptor (IL-36R) and the orphan receptor IL-1RAPL1. Yet, in literature, IL-38 is often presented as an IL-36R antagonist. Methods: The N-terminus of the IL-38 protein produced in a human keratinocyte cell line and of endogenous epidermal IL-38 isolated from healthy human skin was characterized by mass spectrometry. The effects of various recombinant forms of IL-38 on IL-36R- and IL-1R1-mediated responses were assessed in IL-36R HEK Blue reporter cells and in a normal human keratinocyte cell line. IL-8 and IL-6 production was quantified by ELISA. Binding of recombinant IL-38 proteins to the IL-36R was assessed by surface plasmon resonance. Results: Analysis of its native N-terminus revealed that the IL-38 protein produced by human keratinocytes starts at cysteine 2. In cell-based assays, neither full-length amino acid 2-152 IL-38 nor two N-terminally truncated forms of the protein showed efficient antagonist activity on IL-36R- and IL-1R1-mediated responses. The recombinant IL-38 proteins bound to the IL-36R with only moderate affinity, which may provide a mechanistic explanation for inefficient IL-36R antagonism. Conclusions: Our results argue against meaningful inhibitory effects of any of the recombinant IL-38 variants tested on IL-36R or IL-1R1-mediated responses. The mechanisms underlying reported anti-inflammatory effects of IL-38 are thus still unclear, but seem unlikely to be mediated by classical IL-36R or IL-1R1 antagonism. [ABSTRACT FROM AUTHOR]

Published

2025

2. The inhibitory effect of type V transforming growth factor-β receptor antagonist on the proliferation of keloid fibroblasts by suppressing insulin-like growth factor-binding protein 3-interleukin-6 signaling

Author

Boya Zhou, Xunxun Lin, Lingling Xia, Zhen Gao, Meihua Di, Xiaoli Wu, and Wenbo Wang

Subjects

cell proliferation, insulin-like growth factor-binding protein 3, interleukin-6, keloid fibroblasts, type v transforming growth factor-β, receptor antagonist, Dermatology, RL1-803

Abstract

Background: Hyperplasia of fibroblasts is critical in keloid pathogenesis. Insulin-like growth factor-binding protein 3 (IGFBP3) is an important factor in the regulation of cell growth and type V transforming growth factor-β receptor (TβR-V) is a specific receptor of IGFBP3. However, the role of IGFBP3 in keloid development has not been reported. Objectives: This study aimed to investigate the role of IGFBP3 in keloid pathogenesis and evaluate the effects of TβR-V antagonist on keloid fibroblasts (KFs) activities. Methods: IGFBP3 expression in keloids and its impact on KF proliferation were examined. The effects of TβR-V antagonist on KF cell proliferation, migration, and invasion were also investigated. Differentially expressed genes (DEGs) between TβR-V antagonist treated and nontreated KFs were identified through RNA-sequencing (RNA-seq), followed by Gene Ontology (GO), Kyoto Encyclopedia of Genes and Genomes (KEGG), and protein–protein interaction (PPI) network analyses. Results: IGFBP3 was overexpressed in keloids and could promote KF proliferation. TβR-V antagonist suppressed KFs proliferation, migration, and invasion. GO and KEGG analyses showed that the downregulated DEGs revealed by RNA-seq were significantly enriched in terms related to cell proliferation. Interleukin-6 (IL-6) was identified as the only gene interacting with IGFBP3 in the PPI network and was associated with nine hub genes. In vitro assay confirmed the suppression of IL-6 by TβR-V antagonist in KFs. Conclusion: Our study demonstrated that TβR-V antagonist could inhibit keloid growth likely through suppressing IGFBP3-IL-6 signaling activation. These findings suggest that targeting TβR-V could be a potential therapeutic strategy for keloid treatment.

Published

2024

3. Peptide Radioligands in Cancer Theranostics: Agonists and Antagonists.

Author

Nock, Berthold A., Kanellopoulos, Panagiotis, Joosten, Lieke, Mansi, Rosalba, and Maina, Theodosia

Subjects

*PEPTIDES, *COMPANION diagnostics, *SOMATOSTATIN receptors, *SOMATOSTATIN, *GASTRIN, *CANCER patients

Abstract

The clinical success of radiolabeled somatostatin analogs in the diagnosis and therapy—"theranostics"—of tumors expressing the somatostatin subtype 2 receptor (SST2R) has paved the way for the development of a broader panel of peptide radioligands targeting different human tumors. This approach relies on the overexpression of other receptor-targets in different cancer types. In recent years, a shift in paradigm from internalizing agonists to antagonists has occurred. Thus, SST2R-antagonist radioligands were first shown to accumulate more efficiently in tumor lesions and clear faster from the background in animal models and patients. The switch to receptor antagonists was soon adopted in the field of radiolabeled bombesin (BBN). Unlike the stable cyclic octapeptides used in the case of somatostatin, BBN-like peptides are linear, fast to biodegradable and elicit adverse effects in the body. Thus, the advent of BBN-like antagonists provided an elegant way to obtain effective and safe radiotheranostics. Likewise, the pursuit of gastrin and exendin antagonist-based radioligands is advancing with exciting new outcomes on the horizon. In the present review, we discuss these developments with a focus on clinical results, commenting on challenges and opportunities for personalized treatment of cancer patients by means of state-of-the-art antagonist-based radiopharmaceuticals. [ABSTRACT FROM AUTHOR]

Published

2023

4. Effects of Boletus Poisoning on Estrogen Receptors and Neurotransmitters in Rats Based on ERk1/2 Pathway.

Author

Gui, Hongzhen, Wang, Zhenhui, Li, Jiming, Guo, Li, Wang, Chunxia, Liu, Sainan, Yan, Song, and Ao, Jinping

Subjects

ESTROGEN receptors, POISONS, MITOGEN-activated protein kinases, POISONING, AMINO acid residues, ORAL drug administration, ANDROGEN receptors, MITOGENS

Abstract

Estrogen is primarily an endocrine hormone produced by the ovaries and, to a lesser degree, glands of the adrenal cortex's zona reticularis layer. However, it can be synthesized from other tissues and can possess both autocrine and paracrine activities of the target tissue or organ. Its activities, only possible through ligand(estrogen)-receptor interaction, range from reproduction health to skeletal development. These activities can, however, be modulated by using an antagonist. An antagonist is anything that binds to the receptors to prevent the action of a particular hormone, neurotransmitter, or enzyme.The antagonist can specifically bind to the pituitary GnRH receptor, thus blocking the effect of GnRH on the pituitary and reducing the secretion of pituitary GN.Notwithstanding its numerous physiological activities, estrogen is also implicated in some cancers' pathophysiology, specifically estrogen (E2)-induced growth factor-related breast cancers. Androgen receptor, a member of the nuclear receptor superfamily, is encoded by a full-length 90 kb gene from the long arm of X chromosome 11.2–12, which contains 7 introns and 7 exons. There are two isomers of messenger RNA encoding 920 and 388 amino acid residues, respectively.This is because estrogen acts as a mediator for mitogen-activated protein kinase (MAPK/ERk) activation, facilitating cell proliferation, which can progress autonomously. This research investigates the effects of boletus poisoning on estrogen receptors and neurotransmitters in rats based on the ERk 1/2 pathway. A prospective study was conducted for which two sets of experimental studies were performed using albino rats. The first experiment was to determine the toxic dose. This is the dosage for which the saturation point will be reached and the existing estrogen on the receptors displaced. The second set of the experiment was to determine the pathophysiology of this poisoning on the albino rats. A 200 mg/100 kg b.wt oral administration of boletus spp juice and 250 mg/100 kg b.wt of alcohol extracts were administered using an oral gavage to the test specimens. The toxic effects were then recorded for the next 24 h of administration. The results indicated low levels of breast cancer markers in test specimens than those of control specimens. This is because the BoletusBoletus acted as an antagonist blocking the action of E2 on estrogen receptors (ERs). [ABSTRACT FROM AUTHOR]

Published

2023

5. Dose-Response Analysis: Identification of Threshold Levels for Chemicals

Author

Heim, Hans-Karl, Mayer, Peter, Reichl, Franz-Xaver, editor, and Schwenk, Michael, editor

Published

2021

6. The in‐vitro effect of gonadotropin‐releasing hormones, GnRH‐I and GnRH‐II, on the motility, vitality and acrosome integrity of Vervet monkey (Chlorocebus aethiops) spermatozoa.

Author

de Villiers, Charon, Maree, Liana, Katz, Arieh A., and van der Horst, Gerhard

Subjects

*MALE reproductive organs, *CERCOPITHECUS aethiops, *GONADOTROPIN releasing hormone, *FROZEN semen, *GENITALIA, *SPERMATOZOA, *LUTEINIZING hormone releasing hormone receptors, *SPERMATOZOA analysis

Abstract

Two isoforms of the gonadotropin‐releasing hormone (GnRH), GnRH‐I and GnRH‐II, are expressed in mammals, and the presence of one or more GnRH‐like peptides has been demonstrated in the male reproductive tract. GnRH and its receptors (GnRHR) are present in human and non‐human primate testis, prostate, epididymis, seminal vesicle, spermatozoa and seminal human plasma. GnRH‐II is site‐specific and acts directly in an inhibitory or stimulatory fashion. Previous studies speculated that GnRH‐II could disrupt specific sperm processes, such as sperm motility or capacitation and could be utilized as an effective contraceptive agent. Our study aimed to investigate the in‐vitro effects of GnRH‐I and GnRH‐II on Vervet monkey sperm function. Electro‐ejaculated semen samples from 10 Vervet monkeys (Chlorocebus aethiops) were used to select motile sperm populations. Sperm aliquots were incubated with GnRH‐I and GnRH‐II at different concentrations for 1 h, where after sperm motility and kinematic parameters were assessed using the automated Sperm Class Analyser. Additional sperm aliquots were incubated with two 10‐amino acid control peptides, a non‐related peptide and an inactive peptide to exclude the possible influence on sperm motility from other peptides with a structure similar to GnRH. Additionally, a GnRHR‐I antagonist (GnRHR‐A), Cetrorelix, was tested to establish its antagonistic capability on GnRH. The effect of selected concentrations of GnRH‐I and GnRH‐II on sperm vitality and acrosome intactness was also evaluated after 10‐ and 60 min exposure. Analysis of the percentage total sperm motility revealed that different concentrations for GnRH‐I and GnRH‐II inhibited sperm motility significantly. While sperm progressiveness was also notably affected and a trend of decreased sperm kinematics were evident, no effect was found on sperm vitality or acrosome intactness. The non‐related and inactive peptides had no impact on sperm motility. The GnRHR‐A demonstrated no effect on sperm motility and effectively blocked the inhibitory outcome on the motility of both GnRH isoforms. While GnRH‐I or GnRH‐II at low‐dose concentrations resulted in in‐vitro inhibition of sperm motility, it appears to have no adverse effects on other sperm functional parameters evaluated. These collective observations possibly indicate an essential role for GnRH in the in‐vivo process of sperm selection in the female reproductive tract. [ABSTRACT FROM AUTHOR]

Published

2022

7. Introduction and Pharmacodynamics

Author

Seifert, Roland and Seifert, Roland

Published

2019

8. In vivo Evidence for Brain Region-Specific Molecular Interactions Between Cannabinoid and Orexin Receptors.

Author

Kim, Hye Ji J., Zagzoog, Ayat, Smolyakova, Anna Maria, Ezeaka, Udoka C., Benko, Michael J., Holt, Teagan, and Laprairie, Robert B.

Subjects

CANNABINOID receptors, MOLECULAR interactions, BODY temperature, SLEEP, DRUG interactions, PAIN, REWARD (Psychology)

Abstract

The endocannabinoid and orexin neuromodulatory systems serve key roles in many of the same biological functions such as sleep, appetite, pain processing, and emotional behaviors related to reward. The type 1 cannabinoid receptor (CB1R) and both subtypes of the orexin receptor, orexin receptor type 1 (OX1R) and orexin receptor type 2 (OX2R) are not only expressed in the same brain regions modulating these functions, but physically interact as heterodimers in recombinant and neuronal cell cultures. In the current study, male and female C57BL/6 mice were co-treated with the cannabinoid receptor agonist CP55,940 and either the OX2R antagonist TCS-OX2-29 or the dual orexin receptor antagonist (DORA) TCS-1102. Mice were then evaluated for catalepsy, body temperature, thermal anti-nociception, and locomotion, after which their brains were collected for receptor colocalization analysis. Combined treatment with the DORA TCS-1102 and CP55,940 potentiated catalepsy more than CP55,940 alone, but this effect was not observed for changes in body temperature, nociception, locomotion, or via selective OX2R antagonism. Co-treatment with CP55,940 and TCS-1102 also led to increased CB1R-OX1R colocalization in the ventral striatum. This was not seen following co-treatment with TCS-OX2-29, nor in CB1R-OX2R colocalization. The magnitude of effects following co-treatment with CP55,940 and either the DORA or OX2R-selective antagonist was greater in males than females. These data show that CB1R-OX1R colocalization in the ventral striatum underlies cataleptic additivity between CP55,940 and the DORA TCS-1102. Moreover, cannabinoid-orexin receptor interactions are sex-specific with regards to brain region and functionality. Physical or molecular interactions between these two systems may provide valuable insight into drug-drug interactions between cannabinoid and orexin drugs for the treatment of insomnia, pain, and other disorders. [ABSTRACT FROM AUTHOR]

Published

2021

9. In vivo Evidence for Brain Region-Specific Molecular Interactions Between Cannabinoid and Orexin Receptors

Author

Hye Ji J. Kim, Ayat Zagzoog, Anna Maria Smolyakova, Udoka C. Ezeaka, Michael J. Benko, Teagan Holt, and Robert B. Laprairie

Subjects

cannabinoid, cannabinoid receptor, receptor antagonist, orexin receptor, heterodimerization, colocalization, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The endocannabinoid and orexin neuromodulatory systems serve key roles in many of the same biological functions such as sleep, appetite, pain processing, and emotional behaviors related to reward. The type 1 cannabinoid receptor (CB1R) and both subtypes of the orexin receptor, orexin receptor type 1 (OX1R) and orexin receptor type 2 (OX2R) are not only expressed in the same brain regions modulating these functions, but physically interact as heterodimers in recombinant and neuronal cell cultures. In the current study, male and female C57BL/6 mice were co-treated with the cannabinoid receptor agonist CP55,940 and either the OX2R antagonist TCS-OX2-29 or the dual orexin receptor antagonist (DORA) TCS-1102. Mice were then evaluated for catalepsy, body temperature, thermal anti-nociception, and locomotion, after which their brains were collected for receptor colocalization analysis. Combined treatment with the DORA TCS-1102 and CP55,940 potentiated catalepsy more than CP55,940 alone, but this effect was not observed for changes in body temperature, nociception, locomotion, or via selective OX2R antagonism. Co-treatment with CP55,940 and TCS-1102 also led to increased CB1R-OX1R colocalization in the ventral striatum. This was not seen following co-treatment with TCS-OX2-29, nor in CB1R-OX2R colocalization. The magnitude of effects following co-treatment with CP55,940 and either the DORA or OX2R-selective antagonist was greater in males than females. These data show that CB1R-OX1R colocalization in the ventral striatum underlies cataleptic additivity between CP55,940 and the DORA TCS-1102. Moreover, cannabinoid-orexin receptor interactions are sex-specific with regards to brain region and functionality. Physical or molecular interactions between these two systems may provide valuable insight into drug-drug interactions between cannabinoid and orexin drugs for the treatment of insomnia, pain, and other disorders.

Published

2021

10. Effects of second-generation H1-antihistamine drugs on angiogenesis in in vivo chick chorioallantoic membrane model

Author

Nilay Duman, Reşat Duman, and Ayhan Vurmaz

Subjects

angiogenesis, Second-generation H1-antihistamines, desloratadine, rupatadine, Receptor Antagonist, General Medicine, in vivo chick chorioallantoic membrane model, cetirizine, Toxicology, Platelet-Activating-Factor, Tumor-Cells, Cancer

Abstract

BackgroundLiterature on the effects of second-generation H1-antihistamines on angiogenesis is limited.ObjectivesTo investigate the effects of cetirizine, desloratadine, and rupatadine (second-generation H1-antihistamines commonly used in dermatology clinics) on angiogenesis in an in vivo chick chorioallantoic membrane (CAM) model.MethodsThe study was approved by the local ethics committee on animal experimentation. Forty fertilized specific pathogen free eggs were incubated and kept under appropriate temperature and humidity control. Drug solutions were prepared in identical concentrations by dissolving powders in phosphate-buffered saline (PBS). On the third day of the incubation, a small window was opened on the CAM and 0.1 mL desloratadine (1.5 mu g/0.1 mL) in the first group, 0.1 mL cetirizine (1.5 mu g/0.1 mL) in the second group, 0.1 mL rupatadine in the third group (1.5 mu g/0.1 mL), and PBS (0.1 mL) in the fourth group were administered by injection. On the eighth day of incubation, the vascular structures of the CAMs were macroscopically examined and standard digital photographs were taken. The digital images were analyzed and data including mean vessel density, thickness, and number were compared between groups. p < 0.05 was considered statistically significant.ResultsVessel densities were similar in the desloratadine, cetirizine, and control groups, whereas they were significantly less in the rupatadine group (p = 0.01). Furthermore, the rupatadine group had significantly lower vessel thickness and number compared with the other groups (p < 0.05 for both).ConclusionsRupatadine showed anti-angiogenic effects in the chick CAM model, compared with desloratadine and cetirizine. The anti-angiogenic effect of rupatadine could be due to its platelet-activating factor (PAF) receptor inhibition. Thus, rupatadine could be a treatment agent in pathological processes in which angiogenesis is responsible. Further studies with larger series are needed to clarify this potential., Afyon Kocatepe University Scientific Research Foundation; [17.KARIYER.172], Afyon Kocatepe University Scientific Research Foundation (17.KARIYER.172) provided financial support for the conduct of the research.

Published

2022

11. Increased Meal Size but Reduced Meal-Stimulated Plasma Cholecystokinin Concentrations in Women With Obesity

Author

Geary, Nori, Asarian, Lori, Graf, Gwendolyn, Gobbi, Susanna, Tobler, Philippe N., Rehfeld, Jens F., Leeners, Brigitte, Geary, Nori, Asarian, Lori, Graf, Gwendolyn, Gobbi, Susanna, Tobler, Philippe N., Rehfeld, Jens F., and Leeners, Brigitte

Abstract

To better understand the physiological basis of obesity in women, we investigated whether obesity or menstrual cycle phase affects laboratory test-meal size or meal-stimulated plasma cholecystokinin (CCK) concentration. Women with healthy weight (body mass index [BMI] of 18.5-24.9 kg/m(2), N = 16) or obesity (BMI 30-39.9 kg/m(2), N = 20) were tested once in the late-follicular or peri-ovulatory phase (LF/PO) and once in the mid-luteal phase (ML). Meals of ham sandwiches were offered and blood was sampled. Menstrual cycle phases were verified with participants' reports of menses and measurements of progesterone and luteinizing hormone (LH) concentrations. Women with obesity ate significantly larger meals than women with healthy weight, (mean, 711 [95% CI, 402-1013] kJ, P = 0.001, during the LF/PO and 426 [105-734] kJ, P = 0.027, larger during the ML). Women with healthy weight ate smaller meals during LF/PO than ML (decrease, 510 [192-821 kJ], P = 0.008), but women with obesity did not (decrease, 226 [-87-542] kJ, P = 0.15). CCK concentrations 18 to 30 minutes after meal onset were lower in women with obesity than in women with healthy weight during LF/PO (3.6 [3.1-4.1] vs 6.1 [4.5-7.7] pmol/L; P = 0.004), but not during ML, with a significant interaction effect (1.8 [1.2-2.4] pmol/L, P = 0.048). Women with obesity consumed larger meals than women with healthy weight but displayed reduced meal-stimulated plasma CCK concentrations. These data are consistent with the hypothesis that a defect in CCK secretion compromises satiation in obese women and contributes to the development or maintenance of obesity.

Published

2023

12. Soluble PD-L1 generated by endogenous retroelement exaptation is a receptor antagonist

Author

Kevin W Ng, Jan Attig, George R Young, Eleonora Ottina, Spyros I Papamichos, Ioannis Kotsianidis, and George Kassiotis

Subjects

PD-L1, LINE, retroelement, receptor antagonist, Medicine, Science, Biology (General), QH301-705.5

Abstract

Immune regulation is a finely balanced process of positive and negative signals. PD-L1 and its receptor PD-1 are critical regulators of autoimmune, antiviral and antitumoural T cell responses. Although the function of its predominant membrane-bound form is well established, the source and biological activity of soluble PD-L1 (sPD-L1) remain incompletely understood. Here, we show that sPD-L1 in human healthy tissues and tumours is produced by exaptation of an intronic LINE-2A (L2A) endogenous retroelement in the CD274 gene, encoding PD-L1, which causes omission of the transmembrane domain and the regulatory sequence in the canonical 3’ untranslated region. The alternatively spliced CD274-L2A transcript forms the major source of sPD-L1 and is highly conserved in hominids, but lost in mice and a few related species. Importantly, CD274-L2A-encoded sPD-L1 lacks measurable T cell inhibitory activity. Instead, it functions as a receptor antagonist, blocking the inhibitory activity of PD-L1 bound on cellular or exosomal membranes.

Published

2019

13. Eritoran Attenuates Hepatic Inflammation and Fibrosis in Mice with Chronic Liver Injury

Author

Yun-Cheng Hsieh, Kuei-Chuan Lee, Pei-Shan Wu, Teh-Ia Huo, Yi-Hsiang Huang, Ming-Chih Hou, and Han-Chieh Lin

Subjects

toll-like receptor 4, receptor antagonist, hepatic stellate cell, chronic liver disease, animal model, Cytology, QH573-671

Abstract

Toll-like receptor 4 (TLR4) signaling plays a key role in liver inflammation and fibrosis. The therapeutic effects of eritoran, a TLR4 antagonist, in mice with chronic liver injury remained unclear. C57BL/6 mice were fed a fast-food diet (FFD) or treated with carbon tetrachloride (CCl4) to induce chronic liver injury. Eritoran (10 mg/kg) or a vehicle was randomly intraperitoneally administered to the FFD-fed mice and the CCl4-injured mice. Primary mouse liver cells were cultured with lipopolysaccharide (LPS) or eritoran. In both FFD and CCl4 mouse models, eritoran significantly reduced serum ALT levels and decreased hepatic inflammatory cell infiltration without altering hepatic steatosis. Additionally, eritoran attenuated liver fibrosis by decreasing hepatic stellate cells (HSCs) activation and the abundance of α-smooth muscle actin and transforming growth factor-β1. Hepatic TLR4 downstream signaling including MyD88 expression, NF-κB p65 nuclear translocation, p38 and JNK phosphorylation were successfully inhibited by eritoran. In the in vitro study, LPS-induced nuclear translocation of NF-κB in primary HSCs and Kupffer cells was significantly suppressed by eritoran. In conclusion, eritoran attenuated hepatic inflammation and fibrosis by inhibition of the TLR4 signaling pathway in mice with chronic liver injury. Eritoran may serve as a potential drug for chronic liver disease.

Published

2021

14. Biological Activities of Lasso Peptides and Structure–Activity Relationships

Author

Li, Yanyan, Zirah, Séverine, Rebuffat, Sylvie, Li, Yanyan, Zirah, Séverine, and Rebuffat, Sylvie

Published

2015

15. The antagonist of CXCR1 and CXCR2 protects db/db mice from metabolic diseases through modulating inflammation.

Author

Siyuan Cui, Lu Qiao, Shanshan Yu, Lili Men, Yu Li, Fang Li, and Jianling Du

Abstract

Interleukin-8 (IL-8, also named CXCL8) binds to its receptors (CXCR1 and CXCR2) with subsequent recruitment of neutrophils and enhancement of their infiltration into inflamed sites, which exaggerates inflammation in many diseases. Recent studies have proposed that metabolic disorders can be attenuated by counteracting certain inflammatory signal pathways. In this study, we examined whether intervention with G31P, an antagonist of CXCL8, could attenuate tissue inflammation and development of metabolic disorders in db/db mice. The db/m and db/db mice were subcutaneously injected with G31P or equivalent normal saline once a day for 6 wk. The physical and metabolic parameters, glucose tolerance, insulin sensitivity, hepatic lipid accumulation, and inflammation markers were measured. G31P improved hepatic insulin sensitivity by modulating expression of genes related to gluconeogenesis and phosphorylated Akt levels. The expressions of several genes encoding proteins involved in de novo lipogenesis were decreased in G31P-treated db/db mice. Meanwhile, immune cell infiltration and cytokine release were attenuated in db/db mice with G31P treatment. G31P also improved the ratio of proinflammatory M1 and antiinflammatory M2 macrophages. Furthermore, G31P ameliorates metabolic disturbances via inhibition of CXCR1 and CXCR2 pathways in db/db mice. These data suggest that the selective inhibition of CXC chemokines may have therapeutic effects on symptoms associated with obesity and diabetes. [ABSTRACT FROM AUTHOR]

Published

2019

16. Autoimmune thrombocytopenia: Current treatment options in adults with a focus on novel drugs.

Author

Witkowski, Michał, Witkowska, Magdalena, and Robak, Tadeusz

Subjects

*IDIOPATHIC thrombocytopenic purpura, *THROMBOPOIETIN receptors, *ANTINEOPLASTIC agents, *INTRAVENOUS immunoglobulins, *DRUGS

Abstract

Immune thrombocytopenia (ITP) is an autoimmune disease characterized by platelet destruction and reduced platelet production resulting in decreased platelet level and an increased risk of bleeding. Based on the immunologic mechanism of ITP, front‐line standard therapy consists of corticosteroids and intravenous immunoglobulins (IVIG). If patients do not respond to the first‐line treatment, or if continuous therapy is required, the disorder is called refractory ITP, and second‐line therapy is indicated. This treatment may consist of rituximab, thrombopoietin receptor agonists, splenectomy, or cytotoxic drugs. Despite significant advances, many patients do not respond to any the treatments listed below, and new treatment options need to be developed for this relapsed and refractory group. Recent clinical studies have indicated promising outcomes for novel drugs, either as single agents or in combination with traditional drugs. This review discusses the latest and the most promising novel drugs for ITP in adults. [ABSTRACT FROM AUTHOR]

Published

2019

17. Interactions of Noradrenergic, Glucocorticoid and Endocannabinoid Systems Intensify and Generalize Fear Memory Traces

Author

Reinaldo N. Takahashi, Lucas Gazarini, Leandro J. Bertoglio, and Cristina A.J. Stern

Subjects

AM251, medicine.medical_specialty, Epinephrine, medicine.drug_class, Stimulation, Context (language use), Norepinephrine, chemistry.chemical_compound, Memory, Corticosterone, Internal medicine, medicine, Animals, Inverse agonist, Rats, Wistar, Glucocorticoids, Cannabinoid Receptor Agonists, business.industry, General Neuroscience, Fear, Receptor antagonist, Rats, Endocrinology, chemistry, Memory consolidation, business, Glucocorticoid, Endocannabinoids, medicine.drug

Abstract

Systemic administration of drugs that activate the noradrenergic or glucocorticoid system potentiates aversive memory consolidation and reconsolidation. The opposite happens with the stimulation of endocannabinoid signaling under certain conditions. An unbalance of these interacting neurotransmitters can lead to the formation and maintenance of traumatic memories, whose strength and specificity attributes are often maladaptive. Here we aimed to investigate whether originally low-intensity and precise contextual fear memories would turn similar to traumatic ones in rats systemically administered with adrenaline, corticosterone, and/or the cannabinoid type-1 receptor antagonist/inverse agonist AM251 during consolidation or reconsolidation. The high dose of each pharmacological agent evaluated significantly increased freezing times at test in the conditioning context one and nine days later when given alone post-acquisition or post-retrieval. Their respective low dose produced no relative changes when given separately, but co-treatment of adrenaline with corticosterone or AM251 and the three drugs combined, but not corticosterone with AM251, produced results equivalent to those mentioned initially. Neither the high nor the low dose of adrenaline, corticosterone, or AM251 altered freezing times at test in a novel, neutral context two and ten days later. In contrast, animals receiving the association of their low dose exhibited significantly higher freezing times than controls. Together, the results indicate that newly acquired and destabilized threat memory traces become more intense and generalized after a combined interference acting synergistically and mimicking that reported in patients presenting stress-related psychiatric conditions.

Published

2022

18. Visualization of the binding between gintonin, a Panax ginseng-derived LPA receptor ligand, and the LPA receptor subtypes and transactivation of the EGF receptor

Author

Seung-Yeol Nah, Hyewhon Rhim, Hongik Hwang, Hyoung-Chun Kim, Do-Geun Kim, Ik-Hyun Cho, Sung Hee Hwang, Ra Mi Lee, Han-Sung Cho, and Sun-Hye Choi

Subjects

medicine.drug_class, Receptor antagonist, Ligand (biochemistry), Biochemistry, Genetics and Molecular Biology (miscellaneous), Cell biology, Transactivation, chemistry.chemical_compound, Complementary and alternative medicine, chemistry, Epidermal growth factor, Lysophosphatidic acid, medicine, Phosphorylation, Binding site, Receptor, Biotechnology

Abstract

Background Gintonin is a ginseng-derived exogenous G-protein-coupled lysophosphatidic acid (LPA) receptor ligand. Gintonin exerts its neuronal and non-neuronal in vitro and in vivo effects through LPA receptor subtypes. However, it is unknown whether gintonin can bind to the plasma membrane of cells and can transactivate the epidermal growth factor (EGF) receptor. In the present study, we examined whether gintonin-biotin conjugates directly bound to LPA receptors and transactivated the EGF receptor. Methods We designed gintonin-biotin conjugates through gintonin biotinylation and examined whether gintonin-biotin conjugate binding sites co-localized with the LPA receptor subtype binding sites. We further examined whether gintonin-biotin transactivated the EGF receptor via LPA receptor regulation via phosphor-EGF and cell migration assays. Results Gintonin-biotin conjugates elicit [Ca2+]i transient similar to that observed with unbiotinylated gintonin in cultured PC3 cells, suggesting that biotinylation does not affect physiological activity of gintonin. We proved that gintonin-biotin conjugate binding sites co-localized with the LPA1/6 receptor binding sites. Gintonin-biotin binding to the LPA1 receptor transactivates the epidermal growth factor (EGF) receptor through phosphorylation, while the LPA1/3 receptor antagonist, Ki16425, blocked phosphorylation of the EGF receptor. Additionally, an EGF receptor inhibitor AG1478 blocked gintonin-biotin conjugate-mediated cell migration. Conclusions We observed the binding between ginseng-derived gintonin and the plasma membrane target proteins corresponding to the LPA1/6 receptor subtypes. Moreover, gintonin transactivated EGF receptors via LPA receptor regulation. Our results suggest that gintonin directly binds to the LPA receptor subtypes and transactivates the EGF receptor. It may explain the molecular basis of ginseng physiology/pharmacology in biological systems.

Published

2022

19. Effects of microsomal prostaglandin E synthase‐1 inhibition on resistance artery tone in patients with end stage kidney disease

Author

Per-Johan Jakobsson, Karin Larsson, Peter Stenvinkel, Jabin Jahan, Neja Mudrovcic, Karolina Kublickiene, Marina Korotkova, Lars Wennberg, Julia Steinmetz-Späh, and Samsul Arefin

Subjects

medicine.drug_class, Thromboxane, Receptor expression, Prostaglandin, Adrenergic, Vasodilation, Pharmacology, Etoricoxib, chemistry.chemical_compound, Adrenergic Agents, medicine, Humans, Nitrobenzenes, Prostaglandin-E Synthases, Sulfonamides, Cyclooxygenase 2 Inhibitors, Arteries, Receptor antagonist, medicine.anatomical_structure, chemistry, Cyclooxygenase 2, Microvessels, Cyclooxygenase 1, Prostaglandins, Kidney Failure, Chronic, lipids (amino acids, peptides, and proteins), medicine.symptom, Vasoconstriction, Artery

Abstract

Background Inhibition of the microsomal prostaglandin (PG) E2 synthase (mPGES-1) introduces a promising anti-inflammatory treatment approach by specifically reducing PGE2 . The microvasculature is a central target organ for early manifestations of cardiovascular disease. Therefore, a better understanding of the prostaglandin system and characterising the effects of mPGES-1 inhibition in this vascular bed are of interest. Experimental approach The effects of mPGES-1 inhibition on constriction and relaxation of resistance arteries (O100-400μm) from patients with end stage kidney disease (ESKD) and controls (Non-ESKD) were studied using wire-myography in combination with immunological and mass-spectrometry based analyses. Key results Inhibition of mPGES-1 in arteries from ESKD patients and Non-ESKD controls significantly reduced adrenergic vasoconstriction, which was not affected by the COX-2 inhibitors NS-398 and Etoricoxib or the COX-1/COX-2 inhibitor Indomethacin, tested in Non-ESKD controls. Correspondingly, a significant increase of acetylcholine-induced dilatation was observed for mPGES-1 inhibition only. In IL-1β treated arteries, inhibition of mPGES-1 significantly reduced PGE2 levels while PGI2 levels remained unchanged. In contrast, COX-2 inhibition blocked the formation of both prostaglandins. Blockage of PGI2 signaling with an IP receptor antagonist did not restore the reduced constriction, neither did blocking of PGE2 -EP4 or signaling through PPARγ. A biphasic effect was observed for PGE2 , inducing dilatation at nmol and constriction at μmol concentrations. Immunohistochemistry demonstrated expression of mPGES-1, COX-1, PGIS, weak expression for COX-2 as well as receptor expression for PGE2 (EP1-4), thromboxane (TP) and PGI2 (IP) in ESKD and Non-ESKD. Conclusion Our study demonstrates vasodilating effects following mPGES-1 inhibition in human microvasculature and suggests that several pathways besides shunting to PGI2 may be involved.

Published

2022

20. Glucosylsphingosine evokes pruritus via activation of 5‐HT 2A receptor and TRPV4 in sensory neurons

Author

Earl Carstens, Myung-Hyun Song, Babina Sanjel, Won-Sik Shim, and Bo Hyun Kim

Subjects

Pharmacology, TRPV4, Ketanserin, Phospholipase C, medicine.drug_class, Chemistry, Receptor antagonist, medicine.anatomical_structure, Dorsal root ganglion, Knockout mouse, medicine, Receptor, Protein kinase C, medicine.drug

Abstract

Background and purpose Glucosylsphingosine (GS), an endogenous sphingolipid, is highly accumulated in the epidermis of patients with atopic dermatitis (AD) due to abnormal ceramide metabolism. More importantly, GS can evoke scratching behaviors. However, the precise molecular mechanism by which GS induces pruritus has been elusive. Thus, the present study aimed to elucidate the molecular signaling pathway of GS, especially at the peripheral sensory neuronal levels. Experimental approach Calcium imaging was used to investigate the responses of HEK293T cells or mouse dorsal root ganglion (DRG) neurons to application of GS. Scratching behavior tests were also performed with wild-type and Trpv4 knockout mice. Key results GS activated DRG neurons in a manner involving both the 5-HT2A receptor and TRPV4. Furthermore, GS-induced responses were significantly suppressed by various inhibitors, including ketanserin (5-HT2A receptor antagonist), YM254890 (Gαq/11 inhibitor), gallein (Gβγ complex inhibitor), U73122 (phospholipase C inhibitor), bisindolylmaleimide I (PKC inhibitor), and HC067047 (TRPV4 antagonist). Moreover, DRG neurons from Trpv4 knockout mice exhibited significantly reduced responses to GS. Additionally, GS-evoked scratching behaviors were greatly decreased by pretreatment with inhibitors of either 5-HT2A receptor or TRPV4. As expected, GS-evoked scratching behavior was also significantly decreased in Trpv4 knockout mice. Conclusion and implications Overall, the present study provides evidence for a novel molecular signaling pathway for GS-evoked pruritus, which utilizes both 5-HT2A receptor and TRPV4 in mouse sensory neurons. Considering the high accumulation of GS in the epidermis of patients with AD, GS could be another pruritogen in patients with AD.

Published

2022

21. Protective effects of remote ischemic preconditioning against spinal cord ischemia–reperfusion injury in rats

Author

Takashi Mori, Tomoharu Funao, Koichi Suehiro, Kiyonobu Nishikawa, Akira Mukai, Aya Kimura, and Yohei Fujimoto

Subjects

Pulmonary and Respiratory Medicine, Microdialysis, microdialysis, medicine.drug_class, Glutamic Acid, glutamate, 030204 cardiovascular system & hematology, Receptors, N-Methyl-D-Aspartate, Rats, Sprague-Dawley, 03 medical and health sciences, マイクロダイアリシス, 0302 clinical medicine, Cerebrospinal fluid, Anterior Horn Cells, medicine, Animals, Ischemic Preconditioning, グルタミン酸, Spinal Cord Ischemia, business.industry, Glutamate receptor, Receptor antagonist, Spinal cord, medicine.disease, Rats, Neuroprotective Agents, Treatment Outcome, medicine.anatomical_structure, Spinal Cord, 030228 respiratory system, Reperfusion Injury, Anesthesia, Ischemic preconditioning, NMDA receptor, Surgery, N-methyl-D-aspartate receptor, remote ischemic preconditioning, Dizocilpine Maleate, Cardiology and Cardiovascular Medicine, business, Reperfusion injury

Abstract

We aimed to investigate the protective effect of remote ischemic preconditioning against spinal cord ischemia and find a clue to its mechanism by measuring glutamate concentrations in the spinal ventral horn.Male Sprague-Dawley rats were divided into 5 groups (n = 6 in each group) as follows: sham; SCI (only spinal cord ischemia); RIPC/SCI (perform remote ischemic preconditioning before spinal cord ischemia); MK-801/RIPC/SCI (administer MK-801, N-methyl-D-aspartate receptor antagonist, before remote ischemic preconditioning); and MK-801/SCI (administer MK-801 without remote ischemic preconditioning). Remote ischemic preconditioning was achieved by brief limb ischemia 80 minutes before spinal cord ischemia. MK-801 (1 mg/kg, intravenous) was administered 60 minutes before remote ischemic preconditioning. The glutamate concentration in the ventral horn was measured by microdialysis for 130 minutes after spinal cord ischemia. Immunofluorescence was also performed to evaluate the expression of N-methyl-D-aspartate receptor 2B subunit in the ventral horn 130 minutes after spinal cord ischemia.The glutamate concentrations in the spinal cord ischemia group were significantly higher than in the sham group at all time points (P .01). Remote ischemic preconditioning attenuated the spinal cord ischemia-induced glutamate increase. When MK-801 was preadministered before remote ischemic preconditioning, glutamate concentration was increased after spinal cord ischemia (P .01). Immunofluorescence showed that remote ischemic preconditioning prevented the increase in the expression of N-methyl-D-aspartate receptor 2B subunit on the surface of motor neurons (P = .047).Our results showed that remote ischemic preconditioning prevented spinal cord ischemia-induced extracellular glutamate increase in ventral horn and suppressed N-methyl-D-aspartate receptor 2B subunit expression.

Published

2022

22. Does mismatch negativity have utility for NMDA receptor drug development in depression?

Author

Mark A. Smith, Sidra Iqbal, Alan C. Swann, Marijn Lijffijt, Nithya Ramakrishnan, Sanjay J. Mathew, Tabish Iqbal, Brittany Vo-Le, Brittany O'Brien, Bylinda Vo-Le, and Nicholas Murphy

Subjects

lanicemine mismatch negativity for NMDAR drug development, ketamine, Mismatch negativity, medicine.drug_class, RC435-571, Receptors, N-Methyl-D-Aspartate, NMDA-receptor, 03 medical and health sciences, 0302 clinical medicine, Drug Development, Animals, Humans, Medicine, Psychiatry, Depressive Disorder, Major, Depression, business.industry, medicine.disease, Receptor antagonist, 030227 psychiatry, AV-101, Clinical trial, Psychiatry and Mental health, Drug development, Lanicemine, Antidepressant, Major depressive disorder, NMDA receptor, business, Neuroscience, 030217 neurology & neurosurgery

Abstract

Rapid antidepressant effects associated with ketamine have shifted the landscape for the development of therapeutics to treat major depressive disorder (MDD) from a monoaminergic to glutamatergic model. Treatment with ketamine, an N-methyl-D-aspartate (NMDA) receptor antagonist, may be effective, but has many non-glutamatergic targets, and clinical and logistical problems are potential challenges. These factors underscore the importance of manipulations of binding mechanics to produce antidepressant effects without concomitant clinical side effects. This will require identification of efficient biomarkers to monitor target engagement. The mismatch negativity (MMN) is a widely used electrophysiological signature linked to the activity of NMDA receptors (NMDAR) in humans and animals and validated in pre-clinical and clinical studies of ketamine. In this review, we explore the flexibility of the MMN and its capabilities for reliable use in drug development for NMDAR antagonists in MDD. We supplement this with findings from our own research with three distinct NMDAR antagonists. The research described illustrates that there are important distinctions between the mechanisms of NMDAR antagonism, which are further crystallized when considering the paradigm used to study the MMN. We conclude that the lack of standardized methodology currently prevents MMN from being ready for common use in drug discovery. Clinical trial registration: This manuscript describes data collected from the following National Institutes of Health (NIH) and Veterans Affairs (VA) studies: AV-101, NCT03583554; lanicemine, NCT03166501; ketamine, NCT02556606.

Published

2022

23. The mechanism behind activation of the Nod-like receptor family protein 3 inflammasome in Parkinson’s disease

Author

Jin-Ni Fang, Fei-Fei Hua, Jing Wang, Anmu Xie, Xiaona Zhang, Zeng-Qiang Yuan, and Jing-Yang Han

Subjects

medicine.drug_class, Receptor expression, Parkinson's disease, Substantia nigra, atp, neurodegenerative disorder, neuroinflammation, neuroinflammatory response, nlrp3, p2x4, parkinson’s disease, Developmental Neuroscience, NLRP3, medicine, RC346-429, Neuroinflammation, integumentary system, business.industry, Pars compacta, Neurodegeneration, NOD-like receptor, Inflammasome, medicine.disease, Receptor antagonist, ATP, P2X4, Cancer research, Neurology. Diseases of the nervous system, business, medicine.drug, Research Article

Abstract

Previous studies have shown that the ATP-P2X4 receptor signaling pathway mediates the activation of the Nod-like receptor family protein 3 (NLRP3) inflammasome. The NLRP3 inflammasome may promote renal interstitial inflammation in diabetic nephropathy. As inflammation also plays an important role in the pathogenesis of Parkinson's disease, we hypothesized that the ATP-P2X4 receptor signaling pathway may activate the NLRP3 inflammasome in Parkinson's disease. A male rat model of Parkinson's disease was induced by stereotactic injection of 6-hydroxydopamine into the pars compacta of the substantia nigra. The P2X4 receptor and the NLRP3 inflammasome (interleukin-1β and interleukin-18) were activated. Intracerebroventricular injection of the selective P2X4 receptor antagonist 5-(3-bromophenyl)-1,3-dihydro-2H-benzofuro[3,2-e]-1,4-diazepin-2-one (5-BDBD) or knockdown of P2X4 receptor expression by siRNA inhibited the activation of the NLRP3 inflammasome and alleviated dopaminergic neurodegeneration and neuroinflammation. Our results suggest that the ATP-P2X4 receptor signaling pathway mediates NLRP3 inflammasome activation, dopaminergic neurodegeneration, and dopamine levels. These findings reveal a novel role of the ATP-P2X4 axis in the molecular mechanisms underlying Parkinson's disease, thus providing a new target for treatment. This study was approved by the Animal Ethics Committee of Qingdao University, China, on March 5, 2015 (approval No. QYFYWZLL 26119).

Published

2022

24. Histamine 2 receptor antagonists do not improve the outcomes of hospitalized COVID-19 patients

Author

Adnan Malik, Sultan Mahmood, Waseem Amjad, Faisal Kamal, and Ritu Singh

Subjects

medicine.medical_specialty, ARDS, Coronavirus disease 2019 (COVID-19), medicine.drug_class, business.industry, Gastroenterology, medicine.disease, Receptor antagonist, Obesity, Coronary artery disease, Famotidine, Diabetes mellitus, Internal medicine, medicine, Observational study, business, medicine.drug

Abstract

Introduction: Some observational studies have demonstrated the benefit of famotidine in COVID-19-infected individuals. The preference of using an H-2 receptor antagonist (H(2)RA) over proton pump inhibitors (PPI) during the COVID-19 pandemic has been questioned by clinicians. Aim: To compare the outcomes of hospitalized patients who were taking H(2)RA vs. PPI. Material and methods: We conducted a retrospective review of patients admitted for COVID-19 infection from 1 March until 31 July 2020. We included 396 patients admitted during the study period. Of the total, 39 (9.8%) received H(2)RA and 86 (21.7%) were taking PPI as home medications;6 patients were taking both H(2)RA and PPI. Results: The baseline characteristics and comorbid conditions were similar in both groups. The mean age was 57.79 +/- 17.36 years, 43.2% were female, and 48.7% were Caucasian. The common comorbid conditions included HTN (56.8%), obesity (44.4%), diabetes mellitus (38.6%), and coronary artery disease (30.1%). Smoking was more prevalent in the PPI group (42.5% vs. 18.2%, p = 0.03). Gastrointestinal symptoms were seen on initial presentation in 31.1%, and 43.9% had elevated liver enzymes. The H(2)RA group had similar mortality (HR = 0.84, 95% CI: 0.35-2.05) to the non-H2B group. It remained non-significant as compared to PPI (HR = 0.34-3.19, 95% CI: 0.34-3.19). The secondary outcomes including readmission, ICU admission, and severe COVID infections (including ARDS and thromboembolism) were similar in these groups. Conclusions: The H-2 receptor antagonist used as a home medication did not show benefit over the PPI in patients admitted for COVID-19 infections.

Published

2022

25. Exercise tolls the bell for key mediators of low-grade inflammation in dysmetabolic conditions

Author

Lucio Della Guardia and Roberto Codella

Subjects

medicine.medical_specialty, medicine.drug_class, Endocrinology, Diabetes and Metabolism, Immunology, Anti-Inflammatory Agents, Adipose tissue, Inflammation, General Biochemistry, Genetics and Molecular Biology, Insulin resistance, Immune system, Internal medicine, medicine, Humans, Immunology and Allergy, Obesity, Exercise, business.industry, Skeletal muscle, medicine.disease, Receptor antagonist, Pathophysiology, Endocrinology, medicine.anatomical_structure, Cytokines, Tumor necrosis factor alpha, Inflammation Mediators, medicine.symptom, business

Abstract

Metabolic conditions share a common low-grade inflammatory milieu, which represents a key-factor for their ignition and maintenance. Exercise is instrumental for warranting systemic cardio-metabolic balance, owing to its regulatory effect on inflammation. This review explores the effect of physical activity in the modulation of sub-inflammatory framework characterizing dysmetabolic conditions. Regular exercise suppresses plasma levels of TNFα, IL-1β, FFAs and MCP-1, in dysmetabolic subjects. In addition, a single session of training increases the anti-inflammatory IL-10, IL-1 receptor antagonist (IL-1ra), and muscle-derived IL-6, mitigating low-grade inflammation. Resting IL-6 levels are decreased in trained-dysmetabolic subjects, compared to sedentary. On the other hand, the acute release of muscle-IL-6, after exercise, seems to exert a regulatory effect on the metabolic and inflammatory balance. In fact, muscle-released IL-6 is presumably implicated in fat loss and boosts plasma levels of IL-10 and IL-1ra. The improvement of adipose tissue functionality, following regular exercise, is also critical for the mitigation of sub-inflammation. This effect is likely mediated by muscle-released IL-15 and IL-6 and partly relies on the brown-shifting of white adipocytes, induced by exercise. In obese-dysmetabolic subjects, moderate training is shown to restore gut-microbiota health, and this mitigates the translocation of bacterial-LPS into bloodstream. Finally, regular exercise can lower plasma advanced glycated endproducts. The articulated physiology of circulating mediators and the modulating effect of the pathophysiological background, render the comprehension of the exercise-regulatory effect on sub-inflammation a key issue, in dysmetabolism.

Published

2021

26. CXCR4 Antagonism Reduces Cardiac Fibrosis and Improves Cardiac Performance in Dilated Cardiomyopathy.

Author

Chu, Po-Yin, Joshi, Mandar S., Horlock, Duncan, Kiriazis, Helen, and Kaye, David M.

Subjects

HEART fibrosis, DILATED cardiomyopathy, CHEMICAL inhibitors, ALDOSTERONE, ANGIOTENSIN II

Abstract

Background: Myocardial fibrosis is a key pathologic finding in the failing heart and is implicated as a cause of increased ventricular stiffness and susceptibility to ventricular arrhythmia. Neurohormonal mediators such as aldosterone and angiotensin II are known to cause fibrosis in experimental models, however, clinical evidence for the reversal of fibrosis with relevant antagonists is limited. Recent studies suggest that inflammatory mediators may contribute to fibrosis. In dilated cardiomyopathy the mechanism for myocardial fibrosis is unclear and its implications on systolic function are not known. Methods and Results: We studied the effect of a highly selective antagonist of SDF-1/CXCR4 signaling, AMD3100, on the development of cardiac fibrosis and cardiac function in mice with dilated cardiomyopathy due to cardiac-specific transgenic overexpression of the stress-kinase, Mst1. AMD3100 significantly attenuated the progression of myocardial fibrosis and this was accompanied by significant improvements in diastolic and systolic performance as evaluated in isolated Langendorff perfused hearts. AMD3100 reduced BNP mRNA expression but did not alter the expression of Ca2+ handling genes. CXCR4 antagonism also reduced the abundance of splenic CD4+ T cells. Conclusion: This study demonstrates that CXCR4 pathway contributes to pathogenesis of cardiac fibrosis in dilated cardiomyopathy, and it represents a new potential therapeutic target in heart failure. The data also demonstrate that anti-fibrotic strategies can improve systolic performance. [ABSTRACT FROM AUTHOR]

Published

2019

27. Endothelin and the heart in health and diseases.

Author

Miyauchi, Takashi and Sakai, Satoshi

Subjects

*ENDOTHELINS, *HEART diseases, *VASOCONSTRICTION, *HEART cells, *KIDNEY diseases, *VASOCONSTRICTORS

Abstract

Graphical abstract Highlights • Endothelin-1 (ET-1) causes potent vasoconstriction and vasoproliferation. • Cardiomyocytes produce ET-1, which causes a hypertrophic activity of cardiomyocytes. • ET-1 acts via activation of two receptor subtypes, ET A and ET B receptors. • ET receptor antagonists (ERA) are currently in clinical use for pulmonary hypertension. • Heart failure, renal diseases, hypertension, etc are further target diseases of ERA. Abstract Endothelin-1 (ET-1), a 21-amino acid peptide, was initially identified in 1988 as a potent vasoconstrictor and pressor substance isolated from the culture supernatant of porcine aortic endothelial cells. From human genomic DNA analysis, two other family peptides, ET-2 and ET-3, were found. They showed different effects and distribution, suggesting that each peptide may play separate roles in different organs. In the heart, ET-1 also causes positive inotropic and chronotropic responses and hypertrophic activity of the cardiomyocytes. ETs act via activation of two receptor subtypes, ET A and ET B receptors, both of which are coupled to various GTP-binding proteins depending on cell types. Endogenous ET-1 may be involved in progression of various cardiovascular diseases. ET antagonists are currently used clinically in the treatment for patients with pulmonary hypertension, and are considered to have further target diseases as heart failure, cardiac hypertrophy and other cardiac diseases, renal diseases, systemic hypertension, and cerebral vasospasm. [ABSTRACT FROM AUTHOR]

Published

2019

28. Targeting cysteinyl-leukotrienes in abdominal aortic aneurysm.

Author

Araújo, Ana Carolina, Tang, Xiao, and Haeggström, Jesper Z.

Subjects

*CYSTEINYL-transfer RNA, *LEUKOTRIENES, *MONTELUKAST, *AORTIC aneurysms, *LIPOXYGENASES

Abstract

Highlights • Abdominal aortic aneurysm is a life-threatening vascular disorder. • Cys-LT and the CysLT1 are involved in abdominal aortic aneurysm development. • Asthma associates with human abdominal aortic aneurysm and rupture. • The anti-asthma drug montelukast may be used in abdominal aortic aneurysm. • Safe and affordable montelukast holds promise to treat abdominal aortic aneurysm. Abstract Abdominal aortic aneurysm (AAA) is an asymptomatic dilatation of the vessel wall exceeding the normal vessel diameter by 50%, accompanied by intramural thrombus formation. Since the aneurysm can rupture, AAA is a life-threatening vascular disease, which may be amenable to surgical repair. At present, no pharmacological therapy for AAA is available. The 5-lipoxygenase (5-LOX) pathway of arachidonic acid metabolism leads to biosynthesis of leukotrienes (LTs), potent lipid mediators with pro-inflammatory biological actions. Among the LTs, cysteinyl-leukotrienes (cys-LT) are well-recognized signaling molecules in human asthma and allergic rhinitis. However, the effects of these molecules in cardiovascular diseases have only recently been explored. Drugs antagonizing the CysLT1 receptor, termed lukasts and typified by montelukast, are established therapeutics for clinical management of asthma. Lukasts are safe, well-tolerated drugs that can be administered during long time periods. Here we describe recent data indicating that montelukast may be used for prevention and treatment of AAA, thus representing a promising pharmacological tool for a deadly vascular disease with significant socio-economic impact. [ABSTRACT FROM AUTHOR]

Published

2018

29. Long-term use of naldemedine in the treatment of opioid-induced constipation in patients with chronic noncancer pain: a randomized, double-blind, placebo-controlled phase 3 study.

Author

Webster, Lynn R., Nalamachu, Srinivas, Morlion, Bart, Reddy, Jyotsna, Yuko Baba, Tadaaki Yamada, Ferreira, Juan C. Arjona, Baba, Yuko, Yamada, Tadaaki, and Arjona Ferreira, Juan C

Subjects

*OPIOID-induced constipation, *DRUG efficacy, *CHRONIC pain, *RECEPTOR antibodies, *PLACEBOS, *THERAPEUTIC use of narcotics, *ANALGESICS, *COMPARATIVE studies, *CONSTIPATION, *RESEARCH methodology, *MEDICAL cooperation, *NALTREXONE, *NARCOTIC antagonists, *NARCOTICS, *QUALITY of life, *RESEARCH, *EVALUATION research, *RANDOMIZED controlled trials, *TREATMENT effectiveness, *BLIND experiment, *FERRANS & Powers Quality of Life Index, *THERAPEUTICS

Abstract

The long-term safety of naldemedine, a peripherally acting µ-opioid receptor antagonist, was evaluated in patients with opioid-induced constipation and chronic noncancer pain in a 52-week, randomized, double-blind, phase 3 study. Eligible adults who could be on a routine laxative regimen were randomized 1:1 to receive once-daily oral naldemedine 0.2 mg (n = 623) or placebo (n = 623). The primary endpoint was summary measures of treatment-emergent adverse events (AEs). Additional endpoints included opioid withdrawal on the Clinical Opiate Withdrawal Scale and the Subjective Opiate Withdrawal Scale, pain intensity on Numeric Rating Scale, frequency of bowel movements, and constipation-related symptoms and quality of life on the Patient Assessment of Constipation Symptoms and Patient Assessment of Constipation Quality of Life scales, respectively. Treatment-emergent AEs (naldemedine, 68.4% vs placebo, 72.1%; difference: -3.6% [95% confidence interval: -8.7 to 1.5]) and treatment-emergent AEs leading to study discontinuation (6.3% vs 5.8%; difference: 0.5% [-2.2 to 3.1)] were reported for similar proportions of patients. Diarrhea was reported more frequently with naldemedine (11.0%) vs placebo (5.3%; difference: 5.6% [2.6-8.6]). There were no meaningful differences between groups in opioid withdrawal or pain intensity. Sustained significant improvements in bowel movement frequency and overall constipation-related symptoms and quality of life were observed with naldemedine (P ≤ 0.0001 vs placebo at all time points). Naldemedine was generally well tolerated for 52 weeks and did not interfere with opioid-mediated analgesia or precipitate opioid withdrawal. Naldemedine significantly increased bowel movement frequency, improved symptomatic burden of opioid-induced constipation, and increased patients' quality of life vs placebo. [ABSTRACT FROM AUTHOR]

Published

2018

30. Pharmacological Effects of Amiodarone and Dronedarone on Cardiac Thyroid Hormone Receptors

Author

Wiersinga, Wilmar M., Iervasi, Giorgio, editor, and Pingitore, Alessandro, editor

Published

2009

31. Exercise-Induced Adrenocorticotropic Hormone Response Is Cooperatively Regulated by Hypothalamic Arginine Vasopressin and Corticotrophin-Releasing Hormone

Author

Jang Soo Yook, Masahiro Okamoto, Subrina Jesmin, Takeru Shima, Kanako Takahashi, Hideaki Soya, Tsuyoshi Saito, Mariko Soya, and Hikaru Koizumi

Subjects

Male, endocrine system, medicine.medical_specialty, Vasopressin, Arginine, Corticotropin-Releasing Hormone, medicine.drug_class, Endocrinology, Diabetes and Metabolism, Hypothalamus, Adrenocorticotropic hormone, Cellular and Molecular Neuroscience, Endocrinology, Adrenocorticotropic Hormone, Physical Conditioning, Animal, Internal medicine, medicine, Animals, Humans, Aerobic exercise, Rats, Wistar, Endocrine and Autonomic Systems, business.industry, Antagonist, Receptor antagonist, Rats, Arginine Vasopressin, nervous system, business, hormones, hormone substitutes, and hormone antagonists, Hormone

Abstract

Introduction: Exercise becomes a stress when performed at an intensity above the lactate threshold (LT) because at that point the plasma adrenocorticotropic hormone (ACTH), a marker of stress response, increases. It is possible that the exercise-induced ACTH response is regulated at least by arginine vasopressin (AVP) and possibly by corticotropin-releasing hormone (CRH), but this remains unclear. To clarify the involvement of these factors, it is useful to intervene pharmacologically in the regulatory mechanisms, with a physiologically acceptable exercise model. Methods: We used a special stress model of treadmill running (aerobic exercise) for male Wistar rats, which mimic the human physiological response, where plasma ACTH levels increase at just above the LT for 30 min. Animals were administered the AVP V1b receptor antagonist SSR149415 (SSR) and/or the CRH type 1 receptor antagonist CP154526 (CP) intraperitoneally before the exercise, which allowed the monitoring of exercise-induced ACTH response. Immunohistochemical evaluation of activated AVP and CRH neurons with exercise was performed for the animals’ hypothalami. Results: A single injection of either antagonist, SSR or CP, resulted in inhibited ACTH levels after exercise stress. Moreover, the combined injection of SSR and CP strongly suppressed ACTH secretion during treadmill running to a greater extent than each alone. The running-exercise-induced activation of both AVP and CRH neurons in the hypothalamus was also confirmed. Conclusion: These results lead us to hypothesize that AVP and CRH are cooperatively involved in exercise-induced ACTH response just above the LT. This may also reflect the stress response with moderate-intensity exercise in humans.

Published

2021

32. Neuromedin B modulates phosphate-induced vascular calcification

Author

Hyung Joon Kim, Mi-Kyoung Kim, Yeon Sook Kim, Soo-Kyung Bae, Hyun-Joo Park, and Moon-Kyoung Bae

Subjects

Male, medicine.medical_specialty, Vascular smooth muscle, Neurokinin B, medicine.drug_class, Biochemistry, Article, Muscle, Smooth, Vascular, Phosphates, Osteogenesis, Internal medicine, Vascular smooth muscle cells, medicine, Animals, Rats, Wistar, Renal Insufficiency, Chronic, Vascular Calcification, Receptor, Wnt Signaling Pathway, Molecular Biology, Cells, Cultured, Vascular tissue, Neuromedin B receptor, Chemistry, Wnt signaling pathway, Cell Differentiation, General Medicine, Neuromedin B, Receptor antagonist, medicine.disease, Rats, Receptors, Bombesin, Arterial calcification, Endocrinology, Calcium, Bombesin-like peptides, Calcification

Abstract

Vascular calcification is the heterotopic accumulation of calcium phosphate salts in the vascular tissue and is highly correlated with increased cardiovascular morbidity and mortality. In this study, we found that the expression of neuromedin B (NMB) and NMB receptor is upregulated in phosphate-induced calcification of vascular smooth muscle cells (VSMCs). Silencing of NMB or treatment with NMB receptor antagonist, PD168368, inhibited the phosphate-induced osteogenic differentiation of VSMCs by inhibiting Wnt/β-catenin signaling and VSMC apoptosis. PD168368 also attenuated the arterial calcification in cultured aortic rings and in a rat model of chronic kidney disease. The results of this study suggest that NMB-NMB receptor axis may have potential therapeutic value in the diagnosis and treatment of vascular calcification. [BMB Reports 2021; 54(11): 569-574].

Published

2021

33. Bioactive compounds and therapeutic role ofBrassica oleraceaL. seeds in rheumatoid arthritis ratsviaregulating inflammatory signalling pathways and antagonizing interleukin-1 receptor action

Author

Asmaa F. Aboul Naser, Mona E Aboutabl, Wagdy K. B. Khalil, Ali M. El-Hagrassi, Wessam M Aziz, Entesar E. S. Hassan, Ayman A. Farghaly, Abeer F. Osman, and Manal A. Hamed

Subjects

Autoimmune disease, medicine.drug_class, business.industry, Health, Toxicology and Mutagenesis, medicine.medical_treatment, Clinical Biochemistry, Arthritis, Interleukin-1 receptor, Pharmacology, medicine.disease, Receptor antagonist, medicine.disease_cause, Biochemistry, Rheumatoid arthritis, medicine, Polyarthritis, business, Adjuvant, Oxidative stress

Abstract

Rheumatoid arthritis (RA) is a chronic, progressive autoimmune disease characterized by aggressive and systematic polyarthritis. Objective: The present study aimed to isolate and identify the phenolic constituents in Brassica oleracea L. (Brassicaceae) seeds methanolic extract and evaluates its effect against rheumatoid arthritis in rats referring to the new therapy; interleukin-1 receptor antagonist (IL-1RA). Materiald and Methods: The GC/MS profiling of the plant was determined. Arthritis induction was done using complete Freund's adjuvant. Arthritis severity was assessed by percentage of edema and arthritis index. IL-1 receptor type I gene expression, IL-1β, oxidative stress markers, protein content, inflammatory mediators, prostaglandin-E2 (PGE2), genetic abnormalities and the histopathological features of ankle joint were evaluated. Results: For the first time twelve phenolic compounds had been isolated from the seeds extract. Treatment with extract and IL-1RA improved the tested parameters by variable degrees. Conclusions: RA is an irreversible disease, where its severity increase with the time of induction. Brassica oleracea L. seeds extract is considered as a promising anti-arthritis agent. IL-1 RA may be consider as an unusual therapeutic agent for RA disease. More studies are needed to consider the seeds extract as a nutraceutical agent and to recommend IL-1RA as a new RA drug.

Published

2021

34. Synergistic Effect of Ketamine and Buprenorphine Observed in the Treatment of Buprenorphine Precipitated Opioid Withdrawal in a Patient With Fentanyl Use

Author

Mark K. Greenwald, Joshua Luftig, Melena Outhay, Andrew A. Herring, Amy Liang, Erik Anderson, Steve Shoptaw, Christian Hailozian, Mariah M Kalmin, and Monish Ullal

Subjects

Male, Narcotics, Agonist, medicine.drug_class, Receptors, Opioid, mu, Fentanyl, medicine, Humans, Pharmacology (medical), Ketamine, Prospective Studies, business.industry, Opioid-Related Disorders, Receptor antagonist, Buprenorphine, Substance Withdrawal Syndrome, Clonidine, Analgesics, Opioid, Psychiatry and Mental health, Anesthesia, Hyperalgesia, Antidepressant, medicine.symptom, business, medicine.drug

Abstract

Background Optimal treatment of buprenorphine precipitated opioid withdrawal (BPOW) is unclear. Full agonist treatment of BPOW is limited by buprenorphine's high-affinity blockade at mu-opioid receptors (μORs). Buprenorphine's partial agonism (low intrinsic efficacy) at μORs can limit the effectiveness of even massive doses once BPOW has begun. Adjunct medications, such as clonidine, are rarely effective in severe BPOW. Ketamine is an N-methyl-D-aspartate receptor antagonist with a potentially ideal pharmacologic profile for treatment of BPOW. Ketamine reduces opioid withdrawal symptoms independently of direct μOR binding, synergistically potentiates the effectiveness of buprenorphine μOR signaling, reverses (resensitizes) fentanyl induced μOR receptor desensitization, and inhibits descending pathways of hyperalgesia and central sensitization. Ketamine's rapid antidepressant effects potentially address depressive symptoms and subjective distress that often accompanies BPOW. Ketamine is inexpensive, safe, and available in emergency departments. To date, neither ketamine as treatment for BPOW nor to support uncomplicated buprenorphine induction has been described. Case description We report a case of an illicit fentanyl-using OUD patient who experienced severe BPOW during an outpatient low-dose cross taper buprenorphine induction (ie, "microdose"). The BPOW was successfully treated in the emergency department with a combination of ketamine (0.6 mg/kg intravenous over 1 hour) combined with high-dose buprenorphine (16 mg sublingual single dose); 3 days later he was administered a month-long dose of extended-release subcutaneous buprenorphine which was repeated monthly (300 mg). At 90 days the patient remained in treatment and reported continuous abstinence from fentanyl use. Conclusions This single case observation raises important questions about the potential therapeutic role of ketamine as a treatment for BPOW. BPOW is an important clinical problem for which there is currently only limited guidance and no universally accepted approach. Prospective study comparing the effectiveness of differing pharmacologic approaches to treat BPOW is urgently needed.

Published

2021

35. The Sigma‐2 Receptor/TMEM97 Agonist PB28 Suppresses Cell Proliferation and Invasion by Regulating the PI3K‐AKT‐mTOR Signalling Pathway in Renal Cancer

Author

Yuanjun Jiang, Xiao Dong, Bo Zhan, Chiyuan Piao, Chuize Kong, Yang Du, and Zhe Zhang

Subjects

medicine.drug_class, Drug Resistance, Sigma-2 receptor, PI3K‐AKT‐mTOR pathway, Piperazines, Mice, Phosphatidylinositol 3-Kinases, Cell Movement, Cell Line, Tumor, medicine, Animals, Humans, Receptors, sigma, Receptor, Carcinoma, Renal Cell, Protein kinase B, PI3K/AKT/mTOR pathway, Cell Proliferation, Dose-Response Relationship, Drug, Chemistry, Cell growth, TOR Serine-Threonine Kinases, EMT, Membrane Proteins, Cancer, Original Articles, Cell Biology, Receptor antagonist, medicine.disease, Xenograft Model Antitumor Assays, Sigma‐2/TMEM97, Disease Models, Animal, Renal cancer, PB28, Cancer cell, Cancer research, Molecular Medicine, Original Article, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

Sigma‐2 receptor/TMEM97 is overexpressed in many tumours, and sigma‐2 receptor ligands are under investigation for cancer therapy. We intended to evaluate the effect of PB28 on renal cancer in proliferation, migration and invasion in vitro and in vivo. Invasive renal cancer cell lines treated with PB28 (or sigma‐2 receptor antagonist 1) were subjected to cell proliferation, migration and invasion assays. The therapeutic effect of PB28 was performed on nude mice. Western blot for proteins in the PI3K‐AKT‐mTOR signalling pathway was conducted. A CCK‐8 assay was used to examine the effect of the combination of PB28 and cisplatin on renal cancer cells. Significant inhibitory effects were observed on proliferation, migration and invasion of 786‐O and ACHN cells after culturing with PB28. But, the outcomes of sigma‐2 receptor antagonist 1 presented the opposite tendency. PB28 significantly inhibited the proliferative and invasive ability of OS‐RC‐2 cells in vivo. Treatment resulted in decreased phosphorylation of constituents of the PI3K‐AKT‐mTOR pathway. The combination of PB28 and cisplatin showed enhanced efficacy in the inhibition of renal cancer cell proliferation. Taken together, PB28 inhibited the tumorigenic behaviours of renal cancer cells by regulating the PI3K‐AKT‐mTOR signalling pathway and was expected to be a sensitizer of cisplatin.

Published

2021

36. A Review on Heteroaryl Substituted Pyrazolines with their Pharmacological Activity and SAR Studies

Author

Meena Chandran, Geetha Elias, and Anatt Treesa Mathew

Subjects

chemistry.chemical_compound, Chalcone, Chemistry, Drug discovery, medicine.drug_class, Chemical structure, medicine, Biological activity, Pyrazole, Ligand (biochemistry), Receptor antagonist, Receptor, Combinatorial chemistry

Abstract

In step with the development of organic chemistry, heterocyclic compounds play an important part. Electron-rich nitrogen containing heterocyclic compounds and their derivatives play key role in diverse biological activities. The wide-ranging functionality and stereochemical complexity in a five-member ring structure is shown by the pyrazole nucleus, which has two nitrogen atoms and exhibit aromatic character. The medicinal chemists have been using the relationship between chemical structure and biological activity of a molecule in drug discovery as the driving force to guide synthetic efforts, to design new chemical derivatives. It has been reported that pyrazoline derivatives possess a broad spectrum of biological activities such as antibacterial, antimicrobial, anti-inflammatory, antioxidant, antidiabetic, anticancer, antifungal, antitubercular, antidepressant, anticonvulsant and analgesic activities. They also possess some potent receptor selective biological activities like monoamine oxidases (MAOs) inhibitor, Nitric oxide synthase (NOS) inhibitor, Angiotensin converting enzyme (ACE) inhibitor, cholecystokinin-1 receptor antagonist and estrogen receptor (ER) ligand activity. Hence in this article, we focus on the pyrazole derivatives having heteroaryl substituents and their pharmacological activities along with their structure–activity relationships in order to create opportunities to explore the full potential of these compounds. Keywords: Heterocyclic compounds, Pyrazolines, Claisen-Schmidt condensation, Chalcone.

Published

2021

37. Simulation of the oxidative metabolization pattern of netupitant, an NK1 receptor antagonist, by electrochemistry coupled to mass spectrometry

Author

Radu Oprean, Ede Bodoki, Valentin Zaharia, Ruxandra Chira, Ioan-Ovidiu Neaga, Jens Fangmeyer, and Uwe Karst

Subjects

medicine.drug_class, Pharmaceutical Science, 02 engineering and technology, Pharmacy, Oxidative phosphorylation, RM1-950, Mass spectrometry, 01 natural sciences, Redox, Analytical Chemistry, Hydroxylation, chemistry.chemical_compound, In vivo, Drug Discovery, Electrochemistry, medicine, Netupitant, Spectroscopy, Chemistry, 010401 analytical chemistry, 021001 nanoscience & nanotechnology, Receptor antagonist, Combinatorial chemistry, In vitro, 0104 chemical sciences, EC/LC/MS, Oxidative metabolism, Neurokinin-1 antagonist, Original Article, Therapeutics. Pharmacology, 0210 nano-technology

Abstract

Considering the frequent use of netupitant in polytherapy, the elucidation of its oxidative metabolization pattern is of major importance. However, there is a lack of published research on the redox behavior of this novel neurokinin-1 receptor antagonist. Therefore, this study was performed to simulate the intensive hepatic biotransformation of netupitant using an electrochemically driven method. Most of the known enzyme-mediated reactions occurring in the liver (i.e., N-dealkylation, hydroxylation, and N-oxidation) were successfully mimicked by the electrolytic cell using a boron-doped diamond working electrode. The products were separated by reversed-phase high-performance liquid chromatography and identified by high-resolution mass spectrometry. Aside from its ability to pinpoint formerly unknown metabolites that could be responsible for the known side effects of netupitant or connected with any new perspective concerning future therapeutic indications, this electrochemical process also represents a facile alternative for the synthesis of oxidation products for further in vitro and in vivo studies., Graphical abstract Image 1, Highlights • Study of the electrochemical behavior of netupitant, an NK1 receptor antagonist. • Electrochemical simulation of the phase I oxidative metabolization of netupitant. • Identification of the generated oxidation species by LC/ESI(+)-MS. • Separation and identification of electrochemically generated isomers.

Published

2021

38. Memantine Improves Recovery After Spreading Depolarization in Brain Slices and can be Considered for Future Clinical Trials

Author

Andrew P. Carlson, Kevin C. Brennan, Alanna Humphrey, C. William Shuttleworth, and Katelyn M. Reinhart

Subjects

medicine.medical_specialty, Neurology, business.industry, medicine.drug_class, Memantine, Brain, Critical Care and Intensive Care Medicine, Receptor antagonist, Receptors, N-Methyl-D-Aspartate, Article, Mice, Electrophysiology, Slice preparation, Anesthesia, Cortical spreading depression, Animals, Medicine, NMDA receptor, Ketamine, Neurology (clinical), business, Excitatory Amino Acid Antagonists, medicine.drug

Abstract

Spreading depolarization (SD) has been identified as a key mediator of secondary lesion progression after acute brain injuries, and clinical studies are beginning to pharmacologically target SDs. Although initial work has focused on the N-Methyl-D-aspartate receptor antagonist ketamine, there is also interest in alternatives that may be better tolerated. We recently showed that ketamine can inhibit mechanisms linked to deleterious consequences of SD in brain slices. The present study tested the hypothesis that memantine improves recovery of brain slices after SD and explored the effects of memantine in a clinical case targeting SD. For mechanistic studies, electrophysiological and optical recordings were made from hippocampal area CA1 in acutely prepared brain slices from mice. SDs were initiated by localized microinjection of K+ in conditions of either normal or reduced metabolic substrate availability. Memantine effects were assessed from intrinsic optical signals and extracellular potential recordings. For the clinical report, a subdural strip electrode was used for continuous electrocorticographic recording after the surgical evacuation of a chronic subdural hematoma. In brain slice studies, memantine (10–300 µM) did not prevent the initiation of SD, but impaired SD propagation rate and recovery from SD. Memantine reduced direct current (DC) shift duration and improved recovery of synaptic potentials after SD. In brain slices with reduced metabolic substrate availability, memantine reduced the evidence of structural disruption after the passage of SD. In our clinical case, memantine did not noticeably immediately suppress SD; however, it was associated with a significant reduction of SD duration and a reduction in the electrocorticographic (ECoG) suppression that occurs after SD. SD was completely suppressed, with improvement in neurological examination with the addition of a brief course of ketamine. These data extend recent work showing that N-Methyl-D-aspartate receptor antagonists can improve recovery from SD. These results suggest that memantine could be considered for future clinical trials targeting SD, and in some cases as an adjunct or alternative to ketamine.

Published

2021

39. Antidepressant and anxiolytic compounds isolated from Salvia elegans interact with serotonergic drugs

Author

Enrique Jiménez-Ferrer, Rubén Román-Ramos, Manasés González-Cortazar, Gabriela Belen Martínez-Hernández, Gabriela Vargas-Villa, Jaime Tortoriello, and Maribel Herrera-Ruiz

Subjects

Pharmacology, Agonist, Elevated plus maze, biology, Chemistry, medicine.drug_class, Antagonist, General Medicine, Receptor antagonist, biology.organism_classification, Anxiolytic, Open field, medicine, Salvia elegans, Behavioural despair test

Abstract

Salvia elegans belongs to a genus plants with biological activities in central nervous system. In this work, the purpose was to evaluate the anxiolytic and antidepressant effects of fractions and compounds isolated from S. elegans and its interaction with serotoninergic drugs by using behavioral tests in mice. Fractions from aerial parts of S. elegans were obtained by column chromatography, SeF1, SeF2, SeF3, and SeF4. Each of them was administered to 25 mg/k in ICR mice subject to forced swimming test (FST), or elevated plus maze test (EPM), or open field test (OFT). The most active fractions were chemically separated until compounds, which were analyzed as anxiolytic or antidepressant and the coadministration of these treatments with 5-HT1A and 5-HT2 drugs was measured in the different biological tests. All fractions were anxiolytic and antidepressant, oleanolic acid (OA) was found in SeF2, and from SeF3, a mixture of terpenes was found; a GC–MS analysis confirmed the presence of two main compounds: rosifoliol and agaraspirol (TM, mixture of terpenes). TM (doses-response curve, 0.01, 0.1, 0.5, 1.0, and 2.0 mg/kg) and OA (5 mg/kg) were also evaluated demonstrating an antidepressant and anxiolytic effect, respectively. The combination of TM (0.5 mg/kg) with 8-OH (selective 5-HT1A receptor agonist) induced an increment of antidepressant activity, while with the antagonist WAY-100635, the effect diminished. But with DOI (5-HT1c/5-HT2 receptor agonist), there was no change, and with KET (5-HT2 receptor antagonist), the activity was increased. When OA is co-administered with 8-OH or with DOI, the anxiolytic activity of this terpene, diminished; but with the combination with antagonists, the effect of OA shows no change. TM and OA were antidepressant and anxiolytic, respectively, on mice exposed to different tests, and these are able to interact with serotoninergic drugs.

Published

2021

40. Postnatal Cytokine Trajectories in Very Preterm Infants

Author

Abigail B. Shoben, Rita H. Pickler, Marliese Dion Nist, Deborah K. Steward, and Tondi M. Harrison

Subjects

Chemokine, medicine.drug_class, medicine.medical_treatment, Period (gene), Physiology, Inflammation, medicine, Humans, General Nursing, biology, Interleukin-6, business.industry, Monocyte, Interleukin-8, Infant, Newborn, Infant, Receptor antagonist, Very preterm, Cytokine, medicine.anatomical_structure, biology.protein, Cytokines, Tumor necrosis factor alpha, medicine.symptom, business, Infant, Premature

Abstract

Inflammation often accompanies preterm birth and contributes to poor neurodevelopment in preterm infants. The purpose of this study was to describe postnatal cytokine trajectories among non-infected very preterm infants during the first weeks of life. Blood samples for cytokine analysis were collected weekly from infants born between 28 and 31 weeks post-menstrual age. We used linear mixed models to calculate slopes for each cytokine and allowed the slopes to differ by infant biological sex and post-menstrual age at birth. Levels of interleukin-6, interleukin-8, and interleukin-1 receptor antagonist decreased, on average, during the neonatal period. Monocyte chemoattractant protein-1 levels increased over time, and tumor necrosis factor-alpha levels were stable. Interleukin-6 and interleukin-8 slopes differed by post-menstrual age at birth but were unaffected by infant sex. Knowledge of average cytokine trajectories may be useful in identifying infants with unresolving inflammation that increases their risk for poor neurodevelopment.

Published

2021

41. Resolvins as potential candidates for the treatment of major depressive disorder

Author

Katsuyuki Kaneda, Masabumi Minami, and Satoshi Deyama

Subjects

0301 basic medicine, Mechanistic target of rapamycin complex 1, Docosahexaenoic Acids, medicine.drug_class, Prefrontal Cortex, RM1-950, Pharmacology, Dissociative, 03 medical and health sciences, Mice, 0302 clinical medicine, Neurotrophic factors, medicine, Animals, Ketamine, Rapid antidepressant, Specialized pro-resolving lipid mediator, Depressive Disorder, Major, business.industry, Depression, Psychotomimetic, Receptor antagonist, medicine.disease, Antidepressive Agents, Omega-3 polyunsaturated fatty acid, Disease Models, Animal, 030104 developmental biology, Monoamine neurotransmitter, Eicosapentaenoic Acid, Molecular Medicine, Major depressive disorder, Antidepressant, Therapeutics. Pharmacology, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

In contrast with the delayed onset of therapeutic responses and relatively low efficacy of currently available monoamine-based antidepressants, a single subanesthetic dose of ketamine, an N-methyl-D-aspartate receptor antagonist, produces rapid and sustained antidepressant actions even in patients with treatment-resistant depression. However, since the clinical use of ketamine as an antidepressant is limited owing to its adverse effects, such as psychotomimetic/dissociative effects and abuse potential, there is an unmet need for novel rapid-acting antidepressants with fewer side effects. Preclinical studies have revealed that the antidepressant actions of ketamine are mediated via the release of brain-derived neurotrophic factor and vascular endothelial growth factor, with the subsequent activation of mechanistic target of rapamycin complex 1 (mTORC1) in the medial prefrontal cortex. Recently, we demonstrated that resolvins (RvD1, RvD2, RvE1, RvE2 and RvE3), endogenous lipid mediators generated from n-3 polyunsaturated fatty acids (docosahexaenoic and eicosapentaenoic acids), exert antidepressant effects in a rodent model of depression, and that the antidepressant effects of RvD1, RvD2, and RvE1 necessitate mTORC1 activation. In this review, we first provide an overview of the mechanisms underlying the antidepressant effects of ketamine and other rapid-acting agents. We then discuss the possibility of using resolvins as novel therapeutic candidates for depression.

Published

2021

42. Vascular sympathetic neurotransmission and its serotonergic regulation are modified by chronic fluoxetine treatment

Author

Juan Francisco Fernández-González, Cristina López, María Luisa Martín, Mónica García-Domingo, José Ángel García-Pedraza, and Asunción Morán

Subjects

0301 basic medicine, Agonist, Male, Serotonin, Sympathetic Nervous System, Sympathetic neurotransmission, medicine.drug_class, 5-HT, Ritanserin, Stimulation, RM1-950, Pharmacology, Serotonergic, Synaptic Transmission, 03 medical and health sciences, Norepinephrine, 0302 clinical medicine, Fluoxetine, medicine, Animals, Receptor, Serotonin, 5-HT2A, Rats, Wistar, Receptor, 5-HT receptor, Vascular tone, Chemistry, Antagonist, Receptor antagonist, Antidepressive Agents, Electric Stimulation, 030104 developmental biology, Vasoconstriction, Noradrenaline, Molecular Medicine, Blood Vessels, Therapeutics. Pharmacology, 030217 neurology & neurosurgery, medicine.drug

Abstract

Given the interconnection between depressive and cardiovascular disorders, we investigated whether antidepressant treatment (fluoxetine) modifies the serotonergic influence on rat vascular noradrenergic outflow. Twelve-week-old male Wistar rats received fluoxetine treatment (10 mg/kg/day; p.o.) for 14 days; then, they were pithed and prepared for sympathetic stimulation. Vasopressor responses were obtained by electrical stimulation of the sympathetic outflow (0.1, 0.5, 1, and 5 Hz) or i.v. noradrenaline (NA; 0.01, 0.05, 0.1, and 0.5 μg/kg). In fluoxetine-treated group, the electrical-induced vasoconstrictions were lower compared to non-treated rats. Intravenous infusion of 5-HT (10 μg/kg/min) inhibited the sympathetically-induced vasoconstrictions. Only 5-CT, 8-OH-DPAT and L-694,247 (5-HT1/7, 5-HT1A and 5-HT1D agonists, respectively) mimicked 5-HT-induced inhibition, while α-methyl-5-HT (5-HT2 agonist) increased the vasopressor responses. The inhibitory effect of 5-HT was: a) no modified by SB269970 (5-HT7 antagonist); b) abolished by WAY-100,635 (5-HT1A antagonist) plus LY310762 (5-HT1D antagonist); and c) potentiated by ritanserin (5-HT2A receptor antagonist). The vasoconstrictions induced by exogenous NA were not modified by 5-CT but were increased by α-methyl-5-HT. Our results suggest that fluoxetine treatment decreases NA release at vascular level and changes 5-HT modulation on rat vascular noradrenergic neurotransmission, inducing sympatho-inhibition via prejunctional 5-HT1A/1D receptors, and sympatho-potentiation via pre and/or postjunctional 5-HT2A receptors.

Published

2021

43. Clozapine, nimodipine and endosulfan differentially suppress behavioral defects caused by gain-of-function mutations in a two-pore domain K+ channel (UNC-58)

Author

Merve Kasap and Donard S. Dwyer

Subjects

0301 basic medicine, Membrane potential, Chemistry, medicine.drug_class, General Neuroscience, Loxapine, Depolarization, General Medicine, Amoxapine, Forward locomotion, Receptor antagonist, Potassium channel, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine, Nimodipine, 030217 neurology & neurosurgery, medicine.drug

Abstract

Two-pore domain K+ channels (K2Ps) regulate the resting membrane potential in excitable cells and determine ease of depolarization. Gain-of-function (gf) mutations in one of these channels (unc-58) in C. elegans switch it to a Na+ conductance channel and cause tremors, paralysis and other defects. We hypothesized that it should be possible to identify drugs that corrected these defects in unc-58(gf) mutant animals by blocking or modulating the over-active channels. We examined dispersal of animals on food because the absence of effective forward locomotion is the most obvious defect. In addition, we quantified egg release over 24 h. Starting with a known inhibitor of mammalian K2Ps and directed structure-based screening, we evaluated numerous drugs in these assays. Loratadine, which inhibits human KCNK18, significantly improved movement as did methiothepin. We confirmed that endosulfan, a GABA-A receptor antagonist, corrected locomotion in the unc-58(gf) strains. Based on structural similarities to other hits, we found that clozapine, loxapine and amoxapine potently suppressed abnormal phenotypes. Curiously, nimodipine, a Ca++-channel blocker, dramatically improved movement and egg laying in unc-58(e665), but not unc-58(n495) animals. Molecular modeling provided initial insights into a possible basis for this difference based on the location of the e665 and n495 mutations. This research may lead to identification of novel K2P modulators and potential leads for drug discovery.

Published

2021

44. 5-HT1A receptors mediate the analgesic effect of rosavin in a mouse model of oxaliplatin-induced peripheral neuropathic pain

Author

Dae Sik Jang, Sangwon Park, Kyungjoon Lee, Sun Kwang Kim, and Daxian Li

Subjects

Pharmacology, biology, Physiology, business.industry, medicine.drug_class, Analgesic, Antagonist, Rosavin, (+)-Naloxone, Receptor antagonist, biology.organism_classification, chemistry.chemical_compound, Rhodiola rosea, Allodynia, chemistry, Opioid receptor, Medicine, medicine.symptom, business

Abstract

Oxaliplatin, a third-generation platinum derivative, is the mainstay of current antineoplastic medications for advanced colorectal cancer therapy. However, peripheral neuropathic complications, especially cold allodynia, undermine the lifeprolonging outcome of this anti-cancer agent. Rosavin, a phenylpropanoid derived originally from Rhodiola rosea, exhibits a wide range of therapeutic properties. The present study explored whether and how rosavin alleviates oxaliplatin-induced cold hypersensitivity in mice. In the acetone drop test, cold allodynia behavior was observed from days 3 to 5 after a single injection of oxaliplatin (6 mg/kg, i.p.). Cold allodynia was significantly attenuated following rosavin treatment (10 mg/kg, i.p.). Specific endogenous 5-HT depletion by three consecutive pretreatments with parachlorophenylalanine (150 mg/kg/day, i.p.) abolished the analgesic action of rosavin; this effect was not observed following pretreatment with naloxone (opioid receptor antagonist, 10 mg/kg, i.p.). Furthermore, 5-HT1A receptor antagonist WAY-100635 (0.16 mg/kg, i.p.), but not 5-HT3 receptor antagonist MDL-72222 (1 mg/kg, i.p.), blocked rosavin-induced analgesia. These results suggest that rosavin may provide a novel approach to alleviate oxaliplatin-induced cold allodynia by recruiting the activity of 5-HT1A receptors.

Published

2021

45. Establishing a high throughput drug screening system for cerebral ischemia using zebrafish larvae

Author

Toshiaki Kume, Yasuhiko Izumi, Yuki Takada-Takatori, Masahito Sawahata, Mami Matsumoto, and Moeri Miyamoto

Subjects

0301 basic medicine, medicine.drug_class, Nitrogen, Ischemia, Drug Evaluation, Preclinical, RM1-950, Pharmacology, Neuroprotection, Receptors, N-Methyl-D-Aspartate, Brain Ischemia, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Edaravone, medicine, Animals, Hypoxia, Cell damage, Zebrafish, chemistry.chemical_classification, Neurons, Reactive oxygen species, biology, Cell Death, Brain, Free Radical Scavengers, Cerebral ischemia, Free radical scavenger, medicine.disease, Receptor antagonist, biology.organism_classification, Disease Models, Animal, 030104 developmental biology, chemistry, Drug screening, N-methyl-D-aspartate (NMDA) receptor, Larva, Molecular Medicine, Gases, Therapeutics. Pharmacology, Dizocilpine Maleate, 030217 neurology & neurosurgery

Abstract

We previously generated an ischemic stroke in a zebrafish model using N2 gas perfusion; however, this model was an unsuitable drug screening system due to low throughput. In this study, we examined a zebrafish ischemic stroke model using an oxygen absorber to assess drug effects. Hypoxic exposure more than 2 h using the oxygen absorber significantly induced cell death in the brain and damage to the neuronal cells. To confirm the utility of the ischemic model induced by the oxygen absorber, we treated zebrafish with neuroprotective agents. MK-801, an N-methyl- d -aspartate (NMDA) receptor antagonist, significantly suppressed cell death in the brain, and edaravone, a free radical scavenger, significantly reduced the number of dead cells. These results suggest that the activation of NMDA receptors and the production of reactive oxygen species induce neuronal cell damage in accordance with previous mammalian reports. We demonstrate the suitability of an ischemic stroke model in zebrafish larvae using the oxygen absorber, enabling a high throughput drug screening.

Published

2021

46. Inhibition of A2A Adenosine Receptor Signaling in Cancer Cells Proliferation by the Novel Antagonist TP455

Author

Stefania Gessi, Serena Bencivenni, Enrica Battistello, Fabrizio Vincenzi, Vittoria Colotta, Daniela Catarzi, Flavia Varano, Stefania Merighi, Pier Andrea Borea, and Katia Varani

Subjects

A2A adenosine receptor, cancer cell proliferation, intracellular signaling pathways, Drug Discovery and Therapy, receptor antagonist, Therapeutics. Pharmacology, RM1-950

Abstract

Several evidences indicate that the ubiquitous nucleoside adenosine, acting through A1, A2A, A2B, and A3 receptor (AR) subtypes, plays crucial roles in tumor development. Adenosine has contrasting effects on cell proliferation depending on the engagement of different receptor subtypes in various tumors. The involvement of A2AARs in human A375 melanoma, as well as in human A549 lung and rat MRMT1 breast carcinoma proliferation has been evaluated in view of the availability of a novel A2AAR antagonist, with high affinity and selectivity, named as 2-(2-furanyl)-N5-(2-methoxybenzyl)[1,3]thiazolo[5,4-d]pyrimidine-5,7-diammine (TP455). Specifically, the signaling pathways triggered in the cancer cells of different origin and the antagonist effect of TP455 were investigated. The A2AAR protein expression was evaluated through receptor binding assays. Furthermore, the effect of A2AAR activation on cell proliferation at 24, 48 and 72 hours was studied. The selective A2AAR agonist 2-p-(2-carboxyethyl)phenethylamino-5′-N-ethylcarboxamidoadenosine hydrochloride (CGS21680), concentration-dependently induced cell proliferation in A375, A549, and MRMT1 cancer cells and the effect was potently antagonized by the A2AAR antagonist TP455, as well as by the reference A2AAR blocker 4-(2-[7-amino-2-(2-furyl)[1,2,4]triazolo[2,3-a][1,3,5]triazin-5-ylamino]ethyl)phenol (ZM241385). As for the signaling pathway recruited in this response we demonstrated that, by using the specific inhibitors of signal transduction pathways, the effect of A2AAR stimulation was induced through phospholipase C (PLC) and protein kinase C-delta (PKC-δ). In addition, we evaluated, through the AlphaScreen SureFire phospho(p) protein assay, the kinases enrolled by A2AAR to stimulate cell proliferation and we found the involvement of protein kinase B (AKT), extracellular regulated kinases (ERK1/2), and c-Jun N-terminal kinases (JNKs). Indeed, we demonstrated that the CGS21680 stimulatory effect on kinases was strongly reduced in the presence of the new potent compound TP455, as well as by ZM241385, confirming the role of the A2AAR. In conclusion, the A2AAR activation stimulates proliferation of A375, A549, and MRMT1 cancer cells and importantly TP455 reveals its capability to counteract this effect, suggesting selective A2AAR antagonists as potential new therapeutics.

Published

2017

47. Blocking of interleukin-1 suppresses angiotensin II-induced renal injury

Author

Sarasa Isobe, Kazunori Shimada, Koji Akita, Motoaki Sano, Tohru Minamino, Yoichiro Iwakura, Tomiharu Niida, Kikuo Isoda, Yayoi Sato-Okabayashi, and Fumie Ohtomo

Subjects

Endothelin Receptor Antagonists, medicine.medical_specialty, medicine.drug_class, Interleukin-1beta, Renal function, Blood Pressure, Inflammation, Kidney, Antibodies, Proinflammatory cytokine, Fibrosis, Internal medicine, Renin–angiotensin system, medicine, Animals, Humans, Mice, Knockout, Endothelin-1, business.industry, Angiotensin II, Interleukin, Bosentan, General Medicine, Receptor antagonist, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Interleukin 1 Receptor Antagonist Protein, Endocrinology, Hypertension, Kidney Diseases, medicine.symptom, business, Signal Transduction

Abstract

Clinical hypertension (HT) is associated with renal inflammation and elevated circulating levels of proinflammatory cytokines. Interleukin (IL)-1 receptor antagonist (IL-1Ra) is one of the most important anti-inflammatory cytokines and plays a crucial role in inflammation. Inhibition of IL-1 may contribute to modulation of the Angiotensin II (Ang II)-induced HT response. The present study aimed to elucidate the effects of IL-1Ra and anti-IL-1β antibody (01BSUR) on Ang II-induced renal injury. To determine the contribution of IL-1Ra to Ang II-induced renal inflammation, male wildtype (WT) and IL-1Ra-deficient (IL-1Ra−/−) mice were infused with Ang II (1000 ng/kg/min) using subcutaneous osmotic pump for 14 days. We checked renal function, histological change, and several mRNA expressions 14 days after infusion. Fourteen days after infusion, systolic blood pressure (197 ± 5 vs 169 ± 9 mmHg, P

Published

2021

48. Targeting cannabinoid receptor 2 (CB2) limits collagen production—An in vitro study in a primary culture of human fibroblasts

Author

Maria Augusta Vieira-Coelho, Marisa Marques, Paula Serrão, Vera A. Machado, Inês Correia-Sá, Sofia O. Carvalho, and Cláudia Carvalho

Subjects

Pharmacology, Cannabinoid receptor, medicine.drug_class, Chemistry, medicine.medical_treatment, Fibroblasts, Receptor antagonist, Fibrosis, Molecular biology, Receptor, Cannabinoid, CB2, chemistry.chemical_compound, medicine.anatomical_structure, medicine, Cannabinoid receptor type 2, Humans, lipids (amino acids, peptides, and proteins), Pharmacology (medical), Collagen, Cannabinoid, Fibroblast, Receptor, Wound healing, Sirius Red, Cells, Cultured

Abstract

Background Previous studies showed that cannabinoid 2 (CB2) receptor is involved in skin inflammation, fibrogenesis and re-epithelialization in mice, indicating that this receptor may be implicated in wound healing. Thus, topical use of cannabinoids may have a role in local fibrotic and wound healing diseases such as scars or keloids. We investigate the effect of the CB2 selective receptor agonist (6aR,10aR)-3-(1,1-Dimethylbutyl)-6a,7,10,10a-tetrahydro-6,6,9-trimethyl-6H-dibenzo[b,d]pyran (JWH133) and the CB2 selective receptor antagonist (6-Iodo-2-methyl-1-[2-(4-morpholinyl)ethyl]-1H-indol-3-yl)(4-methoxyphenyl)-methanone (AM630), on primary cultures of human fibroblasts. Material and methods Primary cultures of adult human fibroblasts were obtained from abdominal human skin samples. Fibroblasts pretreated with JWH133 and/or AM630 were stimulated with TGF-β (10 ng/mL). Fibroblast activation into myofibroblasts was quantified by the expression of alpha-smooth muscle actin (α-SMA) using Immunocytochemistry and Western Blot assays. Collagen content was quantified with the Sirius red staining assay. Results Upon human fibroblasts stimulation with TGF-β, a significant increase on α-SMA and CB2 receptor expression was observed. In these cells, JWH133 decreased α-SMA expression and collagen content. However, this effect was not observed in resting human fibroblasts. AM630 decreased α-SMA expression and collagen content in both resting and activated fibroblasts. This effect was time- and concentration-dependent with an IC50 value of 11 μM. Conclusion The CB2 receptor appears to be involved in fibroblast repair during skin wound healing in humans, as TGF-β increases CB2 receptor expression and JWH133 produces an anti-fibrotic effect in human fibroblasts. AM630 also showed an anti-fibrotic effect hypothesizing that other cannabinoid receptors, such as TRPV, may be involved in this response.

Published

2021

49. Rapid response to secukinumab in a 5‐year‐old with deficiency of the interleukin‐36 receptor antagonist (DITRA) with severe scalp and nail involvement

Author

Zhang Zhen Ying, Guo Jing, and Wang Bin

Subjects

medicine.medical_specialty, business.industry, medicine.drug_class, Dermatology, Receptor antagonist, medicine.disease, Systemic inflammation, medicine.anatomical_structure, Interleukin 36 receptor antagonist, Scalp, Pediatrics, Perinatology and Child Health, Generalized pustular psoriasis, Nail (anatomy), Medicine, Secukinumab, Leukocytosis, medicine.symptom, business

Abstract

Deficiency of the interleukin-36 receptor antagonist (DITRA) is an autosomal recessive disease caused by mutations of the IL36RN gene. DITRA is characterized by acute generalized pustular psoriasis (GPP), fever, systemic inflammation, and leukocytosis. We report the case of a 5-year-old girl with severe scalp and nail involvement with a rapid response to secukinumab.

Published

2021

50. Effect of Empagliflozin and Liraglutide on the Nucleotide-Binding and Oligomerization Domain-Like Receptor Family Pyrin Domain-Containing 3 Inflammasome in a Rodent Model of Type 2 Diabetes Mellitus

Author

Patrick Meagher, Mark Gordon, and Kim A. Connelly

Subjects

Male, Inflammasomes, medicine.drug_class, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Type 2 diabetes, Pharmacology, Pyrin domain, Glucagon-Like Peptide-1 Receptor, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Glucosides, NLR Family, Pyrin Domain-Containing 3 Protein, Internal Medicine, medicine, Empagliflozin, Animals, 030212 general & internal medicine, Benzhydryl Compounds, Receptor, Sodium-Glucose Transporter 2 Inhibitors, Liraglutide, business.industry, Type 2 Diabetes Mellitus, Inflammasome, General Medicine, medicine.disease, Receptor antagonist, Rats, Disease Models, Animal, Diabetes Mellitus, Type 2, Female, business, medicine.drug

Abstract

Objectives Chronic inflammation has been identified as an important driver of cardiovascular disease in type 2 diabetes (T2D) and can lead to a higher risk of cardiovascular events and rehospitalization. Empagliflozin or liraglutide represent 2 classes of drugs with proven efficacy in the treatment of T2D to reduce macrovascular complications; however, the exact mechanism behind their cardioprotective properties remains incompletely understood. The nucleotide-binding and oligomerization domain-like receptor family pyrin domain-containing 3 (NLRP3) inflammasome is implicated in the progression of cardiovascular disease and linked to the progression of cardiovascular risk factors, such as T2D. Methods We set out to determine whether the sodium-glucose cotransporter-2 inhibitor, empagliflozin, or the glucagon-like peptide-1 receptor antagonist, liraglutide, modified components of NLRP3 in a rodent model of T2D, which recapitulates many of the features of humans with T2D. Empagliflozin and liraglutide were used for 8 weeks in a 32-week-old rat model of T2D and compared with an age- and sex-matched control. After treatment, left ventricular tissue samples and blood plasma were obtained for immunoblotting and an interleukin-1β enzyme-linked immunossay. NLRP3, apoptosis-associated speck-like protein, pro-caspase-1 as well as the cleaved caspase-1 subunits p12 and p10 were assessed by Western blot. Results Goto-Kakizaki rats demonstrated increased NLRP3 inflammasome activation, but neither empagliflozin nor liraglutide demonstrated any impact across the NLRP3 inflammasome pathways or interleukin-1β levels. Conclusions The data suggest that the cardioprotective benefits demonstrated by sodium-glucose cotransporter-2 inhibitors and glucagon-like peptide-1 receptor antagonists occur independently of the NLRP3 inflammasome.

Published

2021