Your search keyword '"Mirko Rivara"' showing total 49 results

1. New ALKBH2 and ALKBH5 inhibitors for treating glioblastoma

Author

Mirko Rivara, Gabriella Nicolini, Alessio Malacrida, Francesca Re, Matteo Incerti, Giulia Russo, and Valentina Zuliani

Subjects

Brain cancer, Glioblastoma, ALKBH2 inhibitors, ALKBH5 inhibitors, Chemistry, QD1-999

Abstract

Purpose: Glioblastoma is an aggressive brain tumor with high mortality and a median survival of about 15 months. Starting from our previous published compound, MV1035 that inhibited migration and invasiveness of glioblastoma U87 cells, and also exhibited a synergic effect in combination with the alkylating agent Temozolomide, we identified new active molecules, with the aim to understand the key motifs responsible for MV1035 activity against the DNA repair protein ALKBH2 and the RNA demethylase ALKBH5. Materials and methods: We modified the original structure of MV1035, synthesizing new molecules that have been tested through MTT assay, cell-free ALKBH2 assay and cell-free ALKBH5 assay. Results: We found that compound 6 is able to reduce the activity of both ALKBH2 and ALKBH5. Conclusion: We obtained important information about the key motifs responsible for the activity of these inhibitors. However, considering the complexity, heterogeneity and plasticity of GBM and GSC cells, the new identified compound will need to be validated in vivo.

Published

2024

2. Chemico-Physical Properties of Some 1,1′-Bis-alkyl-2,2′-hexane-1,6-diyl-bispyridinium Chlorides Hydrogenated and Partially Fluorinated for Gene Delivery

Author

Michele Massa, Mirko Rivara, Thelma A. Pertinhez, Carlotta Compari, Gaetano Donofrio, Luigi Cristofolini, Davide Orsi, Valentina Franceschi, and Emilia Fisicaro

Subjects

heterocyclic gemini cationic surfactants, non-viral vectors, gene delivery, partially fluorinated gemini surfactants, atomic force microscopy on DNA, DNA-surfactant interaction, Organic chemistry, QD241-441

Abstract

The development of very efficient and safe non-viral vectors, constituted mainly by cationic lipids bearing multiple charges, is a landmark for in vivo gene-based medicine. To understand the effect of the hydrophobic chain’s length, we here report the synthesis, and the chemico-physical and biological characterization, of a new term of the homologous series of hydrogenated gemini bispyridinium surfactants, the 1,1′-bis-dodecyl-2,2′-hexane-1,6-diyl-bispyridinium chloride (GP12_6). Moreover, we have collected and compared the thermodynamic micellization parameters (cmc, changes in enthalpy, free energy, and entropy of micellization) obtained by isothermal titration calorimetry (ITC) experiments for hydrogenated surfactants GP12_6 and GP16_6, and for the partially fluorinated ones, FGPn (where n is the spacer length). The data obtained for GP12_6 by EMSA, MTT, transient transfection assays, and AFM imaging show that in this class of compounds, the gene delivery ability strictly depends on the spacer length but barely on the hydrophobic tail length. CD spectra have been shown to be a useful tool to verify the formation of lipoplexes due to the presence of a “tail” in the 288–320 nm region attributed to a chiroptical feature named ψ-phase. Ellipsometric measurements suggest that FGP6 and FGP8 (showing a very interesting gene delivery activity, when formulated with DOPE) act in a very similar way, and dissimilar from FGP4, exactly as in the case of transfection, and confirm the hypothesis suggested by previously obtained thermodynamic data about the requirement of a proper length of the spacer to allow the molecule to form a sort of molecular tong able to intercalate DNA.

Published

2023

3. NaV1.1 and NaV1.6 selective compounds reduce the behavior phenotype and epileptiform activity in a novel zebrafish model for Dravet Syndrome.

Author

Wout J Weuring, Sakshi Singh, Linda Volkers, Martin B Rook, Ruben H van 't Slot, Marjolein Bosma, Marco Inserra, Irina Vetter, Nanda M Verhoeven-Duif, Kees P J Braun, Mirko Rivara, and Bobby P C Koeleman

Subjects

Medicine, Science

Abstract

Dravet syndrome is caused by dominant loss-of-function mutations in SCN1A which cause reduced activity of Nav1.1 leading to lack of neuronal inhibition. On the other hand, gain-of-function mutations in SCN8A can lead to a severe epileptic encephalopathy subtype by over activating NaV1.6 channels. These observations suggest that Nav1.1 and Nav1.6 represent two opposing sides of the neuronal balance between inhibition and activation. Here, we hypothesize that Dravet syndrome may be treated by either enhancing Nav1.1 or reducing Nav1.6 activity. To test this hypothesis we generated and characterized a novel DS zebrafish model and tested new compounds that selectively activate or inhibit the human NaV1.1 or NaV1.6 channel respectively. We used CRISPR/Cas9 to generate two separate Scn1Lab knockout lines as an alternative to previous zebrafish models generated by random mutagenesis or morpholino oligomers. Using an optimized locomotor assay, spontaneous burst movements were detected that were unique to Scn1Lab knockouts and disappear when introducing human SCN1A mRNA. Besides the behavioral phenotype, Scn1Lab knockouts show sudden, electrical discharges in the brain that indicate epileptic seizures in zebrafish. Scn1Lab knockouts showed increased sensitivity to the GABA antagonist pentylenetetrazole and a reduction in whole organism GABA levels. Drug screenings further validated a Dravet syndrome phenotype. We tested the NaV1.1 activator AA43279 and two novel NaV1.6 inhibitors MV1369 and MV1312 in the Scn1Lab knockouts. Both type of compounds significantly reduced the number of spontaneous burst movements and seizure activity. Our results show that selective inhibition of NaV1.6 could be just as efficient as selective activation of NaV1.1 and these approaches could prove to be novel potential treatment strategies for Dravet syndrome and other (genetic) epilepsies. Compounds tested in zebrafish however, should always be further validated in other model systems for efficacy in mammals and to screen for potential side effects.

Published

2020

4. MV1035 Overcomes Temozolomide Resistance in Patient-Derived Glioblastoma Stem Cell Lines

Author

Alessio Malacrida, Alessandro Di Domizio, Angela Bentivegna, Giacomo Cislaghi, Eleonora Messuti, Silvia Maria Tabano, Carlo Giussani, Valentina Zuliani, Mirko Rivara, and Gabriella Nicolini

Subjects

glioblastoma, temozolomide, patient-derived GSCs, ALKBH2, Biology (General), QH301-705.5

Abstract

Glioblastoma (GBM, grade IV glioma) represents the most aggressive brain tumor and patients with GBM have a poor prognosis. Until now surgical resection followed by radiotherapy and temozolomide (TMZ) treatment represents the standard strategy for GBM. We showed that the imidazobenzoxazin-5-thione MV1035 is able to significantly reduce GBM U87-MG cells migration and invasiveness through inhibition of the RNA demethylase ALKBH5. In this work, we focus on the DNA repair protein ALKBH2, a further MV1035 target resulting from SPILLO-PBSS proteome-wide scale in silico analysis. Our data demonstrate that MV1035 inhibits the activity of ALKBH2, known to be involved in GBM TMZ resistance. MV1035 was used on both U87-MG and two patient-derived (PD) glioma stem cells (GSCs): in combination with TMZ, it has a significant synergistic effect in reducing cell viability and sphere formation. Moreover, MV1035 induces a reduction in MGMT expression in PD-GSCs cell lines most likely through a mechanism that acts on MGMT promoter methylation. Taken together our data show that MV1035 could act as an inhibitor potentially helpful to overcome TMZ resistance and able to reduce GBM migration and invasiveness.

Published

2022

5. Subtype-Selective Small Molecule Inhibitors Reveal a Fundamental Role for Nav1.7 in Nociceptor Electrogenesis, Axonal Conduction and Presynaptic Release.

Author

Aristos J Alexandrou, Adam R Brown, Mark L Chapman, Mark Estacion, Jamie Turner, Malgorzata A Mis, Anna Wilbrey, Elizabeth C Payne, Alex Gutteridge, Peter J Cox, Rachel Doyle, David Printzenhoff, Zhixin Lin, Brian E Marron, Christopher West, Nigel A Swain, R Ian Storer, Paul A Stupple, Neil A Castle, James A Hounshell, Mirko Rivara, Andrew Randall, Sulayman D Dib-Hajj, Douglas Krafte, Stephen G Waxman, Manoj K Patel, Richard P Butt, and Edward B Stevens

Subjects

Medicine, Science

Abstract

Human genetic studies show that the voltage gated sodium channel 1.7 (Nav1.7) is a key molecular determinant of pain sensation. However, defining the Nav1.7 contribution to nociceptive signalling has been hampered by a lack of selective inhibitors. Here we report two potent and selective arylsulfonamide Nav1.7 inhibitors; PF-05198007 and PF-05089771, which we have used to directly interrogate Nav1.7's role in nociceptor physiology. We report that Nav1.7 is the predominant functional TTX-sensitive Nav in mouse and human nociceptors and contributes to the initiation and the upstroke phase of the nociceptor action potential. Moreover, we confirm a role for Nav1.7 in influencing synaptic transmission in the dorsal horn of the spinal cord as well as peripheral neuropeptide release in the skin. These findings demonstrate multiple contributions of Nav1.7 to nociceptor signalling and shed new light on the relative functional contribution of this channel to peripheral and central noxious signal transmission.

Published

2016

6. Gene-Delivery Ability of New Hydrogenated and Partially Fluorinated Gemini bispyridinium Surfactants with Six Methylene Spacers

Author

Michele Massa, Mirko Rivara, Gaetano Donofrio, Luigi Cristofolini, Erica Peracchia, Carlotta Compari, Franco Bacciottini, Davide Orsi, Valentina Franceschi, and Emilia Fisicaro

Subjects

Inorganic Chemistry, heterocyclic gemini cationic surfactants, nonviral vectors, gene delivery, gene therapy, partially fluorinated gemini surfactants, atomic force microscopy on DNA, DNA-surfactant interaction, Organic Chemistry, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Computer Science Applications

Abstract

The pandemic emergency determined by the spreading worldwide of the SARS-CoV-2 virus has focused the scientific and economic efforts of the pharmaceutical industry and governments on the possibility to fight the virus by genetic immunization. The genetic material must be delivered inside the cells by means of vectors. Due to the risk of adverse or immunogenic reaction or replication connected with the more efficient viral vectors, non-viral vectors are in many cases considered as a preferred strategy for gene delivery into eukaryotic cells. This paper is devoted to the evaluation of the gene delivery ability of new synthesized gemini bis-pyridinium surfactants with six methylene spacers, both hydrogenated and fluorinated, in comparison with compounds with spacers of different lengths, previously studied. Results from MTT proliferation assay, electrophoresis mobility shift assay (EMSA), transient transfection assay tests and atomic force microscopy (AFM) imaging confirm that pyridinium gemini surfactants could be a valuable tool for gene delivery purposes, but their performance is highly dependent on the spacer length and strictly related to their structure in solution. All the fluorinated compounds are unable to transfect RD-4 cells, if used alone, but they are all able to deliver a plasmid carrying an enhanced green fluorescent protein (EGFP) expression cassette, when co-formulated with 1,2-dioleyl-sn-glycero-3-phosphoethanolamine (DOPE) in a 1:2 ratio. The fluorinated compounds with spacers formed by six (FGP6) and eight carbon atoms (FGP8) give rise to a very interesting gene delivery activity, greater to that of the commercial reagent, when formulated with DOPE. The hydrogenated compound GP16_6 is unable to sufficiently compact the DNA, as shown by AFM images.

Published

2022

7. Innovative 3D proteome-wide scale identification of ALKBH5 target for MV1035 small molecule able to reduce migration and invasiveness in U87 glioblastoma cell lines by SPILLO-PBSS

Author

Omar Ben Mariem, Gabriella Nicolini, Mariarosaria Miloso, Valentina Zuliani, Alessio Malacrida, Mirko Rivara, Giacomo Cislaghi, and Alessandro Di Domizio

Subjects

Glioblastoma cell, Scale (ratio), Proteome, Identification (biology), General Medicine, Computational biology, U87, Biology, Small molecule

Abstract

The innovative in silico technologies developed at SPILLOproject,1 e.g., the SPILLO potential binding sites searcher (SPILLO-PBSS) software,2,3 allow to identify targets and off-targets of any small molecule on a multiple-organism proteomewide scale, and to perform an accurate multilevel cross-organism transferability analysis (MCOTA) aimed at rationalising animal testing. SPILLO-PBSS has been successfully used in several research projects, such as a study in which a compound (MV1035) was found to reduce migration and invasiveness in U87 glioblastoma (GBM) cell lines: the human structural proteome was analyzed and the RNA demethylase ALKBH5 has been identified as a target responsible for the observed effects (target experimentally validated). Another top-ranked target identified by SPILLO-PBSS, the DNA repair protein AlkB homolog 2 (ALKBH2), abundantly expressed in GBM cell lines, resulted particularly interesting for its pivotal role in the onset of resistance to Temozolomide (TMZ), the standard firstline treatment for GBM.2

Published

2021

8. NaV1.1 and NaV1.6 selective compounds reduce the behavior phenotype in a novel zebrafish model for Dravet Syndrome

Author

Marco Inserra, Wout J. Weuring, Kees P.J. Braun, Linda Volkers, Nanda M. Verhoeven-Duif, Ruben van 't Slot, Irina Vetter, Sakshi Singh, Bobby P. C. Koeleman, Mirko Rivara, Martin B. Rook, and Marjolein Bosma

Subjects

biology, Dravet syndrome, Activator (genetics), NAV1, Convulsant, medicine, CRISPR, biology.organism_classification, medicine.disease, Zebrafish, Phenotype, Gene knockout, Cell biology

Abstract

Dravet syndrome is caused by dominant loss-of-function mutations in SCN1A which cause reduced activity of Nav1.1 leading to lack of neuronal inhibition. On the other hand, gain-of-function mutations in SCN8A can lead to a severe epileptic encephalopathy subtype by over activating NaV1.6 channels. These observations suggest that Nav1.1 and Nav1.6 represent two opposing sides of the neuronal balance between inhibition and activation. Here, we hypothesize that Dravet syndrome may be treated by either enhancing Nav1.1 or reducing Nav1.6 activity. To test this hypothesis we generated and characterized a novel DS zebrafish model and tested new compounds that selectively activate or inhibit the human NaV1.1 or NaV1.6 channel respectively. We used CRISPR/Cas9 to generate two separate Scn1Lab knockout lines as an alternative to previous knock-down models. Using an optimized locomotor assay, spontaneous burst movements were detected that were unique to Scn1Lab knockouts and disappear when introducing human SCN1A mRNA. Besides the behavioral phenotype, Scn1Lab knockouts show sudden, electrical discharges in the brain that indicate epileptic seizures in zebrafish. Scn1Lab knockouts showed increased sensitivity to the convulsant pentylenetetrazole and a reduction in whole organism GABA levels. Drug screenings further validated a Dravet syndrome phenotype. We tested the NaV1.1 activator AA43279 and our newly synthesized NaV1.6 inhibitors MV1369 and MV1312 in the Scn1Lab knockouts. Both type of compounds significantly reduced the number of burst movements. Our results show that selective inhibition of NaV1.6 could be just as efficient as selective activation of NaV1.1 and these approaches could prove to be novel potential treatment strategies for Dravet syndrome and other (genetic) epilepsies. Compounds tested in zebrafish however, should always be further validated in other model systems, preferably human derived.

Published

2019

9. Sodium Channel Blocking Activity and In-vivo Testing of New Phenylimidazole Derivatives

Author

Manoj K. Patel, Valentina Zuliani, Mirko Rivara, and Alberto Rapalli

Subjects

Chemistry, In vivo, Blocking (radio), Sodium channel, Drug Discovery, Biophysics, Pharmaceutical Science, Molecular Medicine

Published

2016

10. NaV1.1 and NaV1.6 selective compounds reduce the behavior phenotype and epileptiform activity in a novel zebrafish model for Dravet Syndrome

Author

Sakshi Singh, Bobby P. C. Koeleman, Martin B. Rook, Marjolein Bosma, Marco Inserra, Mirko Rivara, Kees P.J. Braun, Linda Volkers, Ruben van 't Slot, Nanda M. Verhoeven-Duif, Irina Vetter, and Wout J. Weuring

Subjects

0301 basic medicine, Life Cycles, Embryology, Morpholino, Physiology, Action Potentials, Epilepsies, Myoclonic, Biochemistry, Ion Channels, Morpholinos, Epilepsy, Larvae, 0302 clinical medicine, Medicine and Health Sciences, Zebrafish, gamma-Aminobutyric Acid, Neurons, Voltage-Gated Sodium Channel Blockers, Multidisciplinary, biology, Physics, Eukaryota, Animal Models, Phenotype, Cell biology, Electrophysiology, Experimental Organism Systems, Neurology, Osteichthyes, Vertebrates, Physical Sciences, Medicine, Anticonvulsants, Locomotion, RNA, Guide, Kinetoplastida, Research Article, Science, Biophysics, Neurophysiology, Research and Analysis Methods, Membrane Potential, 03 medical and health sciences, Model Organisms, Dravet syndrome, medicine, Animals, Humans, RNA, Messenger, Swimming, Gene knockout, Biological Locomotion, Embryos, Organisms, Biology and Life Sciences, Proteins, Voltage-Gated Sodium Channel Agonists, Zebrafish Proteins, GABA receptor antagonist, medicine.disease, biology.organism_classification, NAV1.1 Voltage-Gated Sodium Channel, Disease Models, Animal, Fish, 030104 developmental biology, Mutagenesis, NAV1.6 Voltage-Gated Sodium Channel, NAV1, Animal Studies, Pentylenetetrazole, 030217 neurology & neurosurgery, Developmental Biology, Neuroscience

Abstract

Dravet syndrome is caused by dominant loss-of-function mutations in SCN1A which cause reduced activity of Nav1.1 leading to lack of neuronal inhibition. On the other hand, gain-of-function mutations in SCN8A can lead to a severe epileptic encephalopathy subtype by over activating NaV1.6 channels. These observations suggest that Nav1.1 and Nav1.6 represent two opposing sides of the neuronal balance between inhibition and activation. Here, we hypothesize that Dravet syndrome may be treated by either enhancing Nav1.1 or reducing Nav1.6 activity. To test this hypothesis we generated and characterized a novel DS zebrafish model and tested new compounds that selectively activate or inhibit the human NaV1.1 or NaV1.6 channel respectively. We used CRISPR/Cas9 to generate two separate Scn1Lab knockout lines as an alternative to previous zebrafish models generated by random mutagenesis or morpholino oligomers. Using an optimized locomotor assay, spontaneous burst movements were detected that were unique to Scn1Lab knockouts and disappear when introducing human SCN1A mRNA. Besides the behavioral phenotype, Scn1Lab knockouts show sudden, electrical discharges in the brain that indicate epileptic seizures in zebrafish. Scn1Lab knockouts showed increased sensitivity to the GABA antagonist pentylenetetrazole and a reduction in whole organism GABA levels. Drug screenings further validated a Dravet syndrome phenotype. We tested the NaV1.1 activator AA43279 and two novel NaV1.6 inhibitors MV1369 and MV1312 in the Scn1Lab knockouts. Both type of compounds significantly reduced the number of spontaneous burst movements and seizure activity. Our results show that selective inhibition of NaV1.6 could be just as efficient as selective activation of NaV1.1 and these approaches could prove to be novel potential treatment strategies for Dravet syndrome and other (genetic) epilepsies. Compounds tested in zebrafish however, should always be further validated in other model systems for efficacy in mammals and to screen for potential side effects.

Published

2020

11. 3D proteome-wide scale screening and activity evaluation of a new ALKBH5 inhibitor in U87 glioblastoma cell line

Author

Gabriella Nicolini, Giacomo Cislaghi, Valentina Zuliani, Alessio Malacrida, Mirko Rivara, Alessandro Di Domizio, Mariarosaria Miloso, Malacrida, A, Rivara, M, Di Domizio, A, Cislaghi, G, Miloso, M, Zuliani, V, and Nicolini, G

Subjects

Proteome, Cell Survival, In silico, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Imidazobenzoxazin-5-thione scaffold, 01 natural sciences, Biochemistry, Structure-Activity Relationship, Cell Movement, Transcription (biology), Cell Line, Tumor, Drug Discovery, Humans, Enzyme Inhibitors, U87, neoplasms, Molecular Biology, Dose-Response Relationship, Drug, Molecular Structure, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, Off-target interaction, AlkB Homolog 5, RNA Demethylase, RNA, ALKBH5, In vitro, Benzoxazines, nervous system diseases, 0104 chemical sciences, Cell biology, 010404 medicinal & biomolecular chemistry, Cell culture, biology.protein, Molecular Medicine, Demethylase, Glioblastoma

Abstract

The imidazobenzoxazin-5-thione MV1035, synthesized as a new sodium channel blocker, has been tested on tumoral cells that differ for origin and for expressed NaV pool (U87-MG, H460 and A549). In this paper we focus on the effect of MV1035 in reducing U87 glioblastoma cell line migration and invasiveness. Since the effect of this compound on U87-MG cells seemed not dependent on its sodium channel blocking capability, alternative off-target interaction for MV1035 have been identified using SPILLO-PBSS software. This software performs a structure-based in silico screening on a proteome-wide scale, that allows to identify off-target interactions. Among the top-ranked off-targets of MV1035, we focused on the RNA demethylase ALKBH5 enzyme, known for playing a key role in cancer. In order to prove the effect of MV1035 on ALKBH5 in vitro coincubation of MV1035 and ALKBH5 has been performed demonstrating a consequent increase of N6-methyladenosine (m6A) RNA. To further validate the pathway involving ALKBH5 inhibition by MV1035 in U87-MG reduced migration and invasiveness, we evaluated CD73 as possible downstream protein. CD73 is an extrinsic protein involved in the generation of adenosine and is overexpressed in several tumors including glioblastoma. We have demonstrated that treating U87-MG with MV1035, CD73 protein expression was reduced without altering CD73 transcription. Our results show that MV1035 is able to significantly reduce U87 cell line migration and invasiveness inhibiting ALKBH5, an RNA demethylase that can be considered an interesting target in fighting glioblastoma aggressiveness. Our data encourage to further investigate the MV1035 inhibitory effect on glioblastoma.

Published

2020

12. Drug repurposing approaches to fight Dengue virus infection and related diseases

Author

Lorenzo Botta, Marco Radi, Mirko Rivara, and Valentina Zuliani

Subjects

0301 basic medicine, Drug, Serotype, viruses, media_common.quotation_subject, Drug repurposing, Dengue virus, medicine.disease_cause, Virus Replication, Antiviral Agents, Dengue fever, Settore CHIM/06, Dengue, 03 medical and health sciences, Drug Discovery, medicine, Animals, Humans, Pathogen, Repurposing, media_common, business.industry, Drug Repositioning, Neglected Diseases, Dengue Virus, medicine.disease, Virology, Drug repositioning, 030104 developmental biology, Viral disease, business

Abstract

Dengue is a mosquito-borne viral disease caused by four antigenically distinct serotypes of Dengue Virus (DENV), namely DENV1-4 and is currently considered the most important arthropod-born viral disease in the world. An effective antiviral therapy to treat Dengue Virus infection is still missing and a number of replicative cycle inhibitors are currently under study. Considering the rapid spreading of DENV and the common timeframe required for bringing a new drug on the market, the repurposing of approved drugs used for different diseases to identify novel inhibitors of this pathogen represents an attractive approach for a rapid therapeutic intervention. Herein, we will describe the most recent drug repurposing approaches to fight DENV infection and their implications in antiviral drug-discovery.

Published

2018

13. Novel sodium channel antagonists in the treatment of neuropathic pain

Author

Mirko Rivara and Valentina Zuliani

Subjects

0301 basic medicine, Action Potentials, Disease, Bioinformatics, Sodium Channels, 03 medical and health sciences, 0302 clinical medicine, Sodium channel blocker, medicine, Animals, Humans, Pharmacology (medical), Molecular Targeted Therapy, Pharmacology, business.industry, Sodium channel, General Medicine, medicine.disease, Sodium Channel Antagonists, 030104 developmental biology, Drug Design, Anesthesia, Neuropathic pain, Quality of Life, Neuralgia, business, 030217 neurology & neurosurgery, Signal Transduction, Sodium Channel Blockers

Abstract

Effective and safe drugs for the treatment of neuropathic pain are still an unmet clinical need. Neuropathic pain, caused by a lesion or disease that affects the somatosensory system, is a debilitating and hampering condition that has a great economic cost and, above all, a tremendous impact on the quality of life. Sodium channels are one of the major players in generating and propagating action potentials. They represent an appealing target for researchers involved in the development of new and safer drugs useful in the treatment of neuropathic pain. The actual goal for researchers is to target sodium channels selectively to stop the abnormal signaling that characterizes neuropathic pain while leaving normal somatosensory functions intact.This review covers the most recent publications regarding sodium channel blockers and their development as new treatments for neuropathic pain. The main areas discussed are the natural sources of new blockers, such as venom extracts and the recent efforts from many pharmaceutical companies in the field.There have been serious efforts by both the pharmaceutical industry and academia to develop new and safer therapeutic options for neuropathic pain. A number of different strategies have been undertaken; the main efforts directed towards the identification of selective blockers starting from both natural products or screening chemical libraries. At this time, researchers have identified and characterized selective compounds against NaV1.7 or NaV1.8 voltage-gated sodium channels but only time will tell if they reach the market.

Published

2015

14. Subtype-Selective Small Molecule Inhibitors Reveal a Fundamental Role for Nav1.7 in Nociceptor Electrogenesis, Axonal Conduction and Presynaptic Release

Author

Edward B. Stevens, Zhixin Lin, Anna Wilbrey, Stephen G. Waxman, Peter J. Cox, Sulayman D. Dib-Hajj, Mark L. Chapman, Malgorzata A. Mis, Christopher William West, R. Ian Storer, Stupple Paul Anthony, Elizabeth C. Payne, Manoj K. Patel, David Printzenhoff, Andrew D. Randall, James A. Hounshell, Douglas S. Krafte, Jamie Turner, Nigel Alan Swain, Aristos J. Alexandrou, Richard P. Butt, Adam R. Brown, Mark Estacion, Brian E. Marron, Alex Gutteridge, Neil A. Castle, Rachel Doyle, and Mirko Rivara

Subjects

Male, 0301 basic medicine, Sensory Receptors, Patch-Clamp Techniques, Physiology, Action Potentials, Social Sciences, lcsh:Medicine, Nervous System, Biochemistry, Ion Channels, Sodium Channels, Mice, 0302 clinical medicine, Animal Cells, Ganglia, Spinal, Medicine and Health Sciences, Psychology, lcsh:Science, Membrane Electrophysiology, Neurons, Sulfonamides, Multidisciplinary, Organic Compounds, Chemistry, Physics, Phenyl Ethers, Monosaccharides, NAV1.7 Voltage-Gated Sodium Channel, Nociceptors, Anatomy, Electrophysiology, Bioassays and Physiological Analysis, Nociception, Spinal Cord, Physical Sciences, Nociceptor, Cell lines, Sensory Perception, Cellular Types, Biological cultures, Research Article, Signal Transduction, Carbohydrates, Biophysics, Presynaptic Terminals, Neurophysiology, Neurotransmission, Membrane Potential, 03 medical and health sciences, Animals, Humans, Patch clamp, Sodium channel, Organic Chemistry, HEK 293 cells, Electrophysiological Techniques, lcsh:R, Chemical Compounds, Biology and Life Sciences, Proteins, Cell Biology, Axons, Research and analysis methods, Neuroanatomy, Glucose, HEK293 Cells, 030104 developmental biology, nervous system, Cellular Neuroscience, NAV1, lcsh:Q, Patch Clamp Techniques, Neuroscience, 030217 neurology & neurosurgery

Abstract

Human genetic studies show that the voltage gated sodium channel 1.7 (Nav1.7) is a key molecular determinant of pain sensation. However, defining the Nav1.7 contribution to nociceptive signalling has been hampered by a lack of selective inhibitors. Here we report two potent and selective arylsulfonamide Nav1.7 inhibitors; PF-05198007 and PF-05089771, which we have used to directly interrogate Nav1.7's role in nociceptor physiology. We report that Nav1.7 is the predominant functional TTX-sensitive Nav in mouse and human nociceptors and contributes to the initiation and the upstroke phase of the nociceptor action potential. Moreover, we confirm a role for Nav1.7 in influencing synaptic transmission in the dorsal horn of the spinal cord as well as peripheral neuropeptide release in the skin. These findings demonstrate multiple contributions of Nav1.7 to nociceptor signalling and shed new light on the relative functional contribution of this channel to peripheral and central noxious signal transmission.

Published

2016

15. Inhibition of NaV1.6 sodium channel currents by a novel series of 1,4-disubstituted-triazole derivatives obtained via copper-catalyzed click chemistry

Author

Valentina Zuliani, Manoj K. Patel, Mirko Rivara, and Laura Amori

Subjects

Stereochemistry, Clinical Biochemistry, Substituent, Triazole, Pharmaceutical Science, Ring (chemistry), Biochemistry, Article, Catalysis, chemistry.chemical_compound, Drug Discovery, Animals, Humans, Molecule, Imidazole, Molecular Biology, Voltage-Gated Sodium Channel Blockers, Aryl, Organic Chemistry, Triazoles, Cycloaddition, Rats, HEK293 Cells, chemistry, NAV1.6 Voltage-Gated Sodium Channel, Click chemistry, Molecular Medicine, Click Chemistry, Copper

Abstract

We have synthesized and evaluated a series of 1,4-disubstituted-triazole derivatives for inhibition of the rat Na(V)1.6 sodium channel isoform, an isoform thought to play an important role in controlling neuronal firing. Starting from a series of 2,4(1H)-diarylimidazoles previously published, we decided to extend the SAR study by replacing the imidazole with a different heterocyclic scaffold and by varying the aryl substituents on the central aromatic ring. The 1,4-disubstituted 1,2,3-triazoles were prepared employing the copper-catalyzed azide-alkyne cycloaddition (CuAAC). Many of the new molecules were able to block the rNa(v)1.6 currents at 10 μM by over 20%, displaying IC(50) values ranging in the low micromolar, thus indicating that triazole can efficiently replace the central heterocyclic core. Moreover, the introduction of a long chain at C4 of the central triazole seems beneficial for increased rNa(v)1.6 current block, whereas the length of N1 substituent seems less crucial for inhibition, as long as a phenyl ring is not direcly connected to the triazole. These results provide additional information on the structural features necessary for block of the voltage-gated sodium channels. These new data will be exploited in the preparation of new compounds and could result in potentially useful AEDs.

Published

2012

16. In vivo screening of diarylimidazoles as anticonvulsant agents

Author

Valentina Zuliani and Mirko Rivara

Subjects

Phenylglyoxal, medicine.medical_treatment, Organic Chemistry, Neurotoxicity, Pharmacology, medicine.disease, Epilepsy, chemistry.chemical_compound, Anticonvulsant Agent, Anticonvulsant, chemistry, In vivo, Toxicity, medicine, General Pharmacology, Toxicology and Pharmaceutics, Ammonium acetate

Abstract

In this study, the anticonvulsant activity evaluation of a series of new 2,4(1H)-diarylimidazoles, characterized by the presence of different substituents on the aryl rings, was described. The anticonvulsant activity profile of those compounds was determined by Maximal Electroshock Seizure (MES), subcutaneous Metrazol Seizure (scMet) tests, and 6-Hz seizure model, whereas their neurotoxicity was examined using rotarod test. The trifluoromethoxy derivative, obtained starting from phenylglyoxal, p-OCF3-benzaldehyde, and ammonium acetate in methanol (r.t.), exhibited a great ability to prevent the seizures induced in the 6-Hz test, becoming a new promising molecule to develop for the treatment of therapy-resistant partial seizures.

Published

2011

17. Anticonvulsant activity of 2,4(1H)-diarylimidazoles in mice and rats acute seizure models

Author

James P. Stables, Manoj K. Patel, Mirko Rivara, Aradhya Nigam, Marco Fantini, and Valentina Zuliani

Subjects

medicine.drug_class, Stereochemistry, medicine.medical_treatment, Clinical Biochemistry, Administration, Oral, Pharmaceutical Science, Motor Activity, Pharmacology, Biochemistry, Article, Sodium Channels, Cell Line, Mice, Structure-Activity Relationship, Epilepsy, Sodium channel blocker, Seizures, Oral administration, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Molecular Biology, Chemistry, Sodium channel, Organic Chemistry, Imidazoles, Neurotoxicity, medicine.disease, Rats, Disease Models, Animal, Anticonvulsant, Sedative, Molecular Medicine, Anticonvulsants, Sodium Channel Blockers

Abstract

2,4(1H)-Diarylimidazoles have been previously shown to inhibit hNa(V)1.2 sodium (Na) channel currents. Since many of the clinically used anticonvulsants are known to inhibit Na channels as an important mechanism of their action, these compounds were tested in two acute rodent seizure models for anticonvulsant activity (MES and scMet) and for sedative and ataxic side effects. Compounds exhibiting antiepileptic activity were further tested to establish a dose response curve (ED(50)). The experimental data identified four compounds with anticonvulsant activity in the MES acute seizure rodent model (compound 10, ED(50)=61.7mg/kg; compound 13, ED(50)=46.8mg/kg, compound 17, ED(50)=129.5mg/kg and compound 20, ED(50)=136.7mg/kg). Protective indexes (PI=TD(50)/ED(50)) ranged from 2.1 (compound 10) to greater than 3.6 (compounds 13, 17 and 20). All four compounds were shown to inhibit hNa(V)1.2 in a dose dependant manner. Even if a correlation between sodium channel inhibition and anticonvulsant activity was unclear, these studies identify four Na channel antagonists with anticonvulsant activity, providing evidence that these derivatives could be potential drug candidates for development as safe, new and effective antiepileptic drugs (AEDs).

Published

2010

18. 5-Benzylidene-hydantoins: Synthesis and antiproliferative activity on A549 lung cancer cell line

Author

Valentina Zuliani, Maricla Galetti, Caterina Carmi, Mirko Rivara, Federica Vacondio, Pier Giorgio Petronini, Marco Mor, Roberta Alfieri, Marco Fantini, Pier Vincenzo Plazzi, Fabrizio Bordi, Alessio Lodola, and Andrea Cavazzoni

Subjects

Lung Neoplasms, Stereochemistry, Hydantoin, Antineoplastic Agents, Adenocarcinoma, Benzylidene Compounds, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Cell Line, Tumor, Drug Discovery, medicine, Humans, Cell Proliferation, Pharmacology, A549 cell, Cell growth, Hydantoins, Organic Chemistry, Autophosphorylation, Biological activity, General Medicine, Cell cycle, ErbB Receptors, Gene Expression Regulation, Neoplastic, Mechanism of action, chemistry, Tumor Suppressor Protein p53, medicine.symptom, DNA Damage

Abstract

Benzylidene hydantoins have been recently reported as a new class of EGFR inhibitors. We describe here a simple and efficient methodology for the parallel solution-phase synthesis of a library of 5-benzylidene hydantoins, which were evaluated for antiproliferative activity on the human lung adenocarcinoma A549 cell line. Various substituents at positions 1, 3 and 5 on the hydantoin nucleus were examined. In the presence of a 5-benzylidene group and of a lipophilic substituent at position 1, most of the tested compounds inhibited cell proliferation at a concentration of 20 μM. Compound 7 (UPR1024), bearing 1-phenethyl and (E)-5-p-OH-benzylidene substituents, was found to be the most active derivative of the series. It inhibited EGFR autophosphorylation and induced DNA damage in A549 cells. Compound 7 and other synthesized 5-benzylidene hydantoin derivatives increased p53 levels, suggesting that the dual mechanism of action was a common feature shared by compound 7 and other member of the series.

Published

2009

19. 2,4(5)-Diarylimidazoles as inhibitors of hNaV1.2 sodium channels: Pharmacological evaluation and structure–property relationships

Author

Claudia Silva, Natasha Singh, Christopher L. Kalmar, Chiara Ghiron, Federica Vacondio, Aparna R. Baheti, Manoj K. Patel, Marco Fantini, Mirko Rivara, Ravi Katari, Valentina Zuliani, Ellen C. Merrick, and Giuseppe Cocconcelli

Subjects

Stereochemistry, Sodium, Clinical Biochemistry, Pharmaceutical Science, chemistry.chemical_element, Biochemistry, Chemical synthesis, Sodium Channels, Cell Line, Inhibitory Concentration 50, Structure-Activity Relationship, chemistry.chemical_compound, Sodium channel blocker, Drug Discovery, Humans, Structure–activity relationship, Molecular Biology, Chemistry, Sodium channel, Organic Chemistry, Imidazoles, Biological activity, Electrophysiology, Lipophilicity, Molecular Medicine, Lead compound, Sodium Channel Blockers

Abstract

Sodium (Na) channels continue to represent an important target for the development of novel anticonvulsants. We have synthesized and evaluated a series of 2,4(5)-diarylimidazoles for inhibition of the human neuronal Na(V)1.2 Na channel isoform. Starting with the unsubstituted lead compound previously published 3, SAR studies were performed introducing substituents with different physico-chemical properties. Lipophilicity (log D(7.4)) and basicity (pK(a)) of the compounds were measured and submitted for QSPR investigations. Some of the active compounds described had IC(50) values that were considerably lower than our lead compound. In particular, the m-CF(3) disubstituted 22 was the most active compound, inhibiting hNa(V)1.2 currents within the nanomolar concentration range (IC(50)=200 nM). In comparison, lamotrigine and phenytoin, two clinically used anticonvulsant drugs known to inhibit Na channels, had IC(50)'s values that were greater than 100 microM.

Published

2009

20. Chiral NMR discrimination of the diastereoisomeric salts of the H3 -antagonist 2-[3-(1H-imidazol-4-ylmethyl)piperidin-1-yl]-1H-benzimidazole

Author

Elisa Dallaturca, Marco Fantini, Marco Mor, Mirko Rivara, and Valentina Zuliani

Subjects

NMR spectra database, Benzimidazole, chemistry.chemical_compound, Trifluoromethyl, chemistry, Stereochemistry, Diastereomer, Imidazole, General Materials Science, General Chemistry, Piperidine, Enantiomer, Phenylacetic acid

Abstract

Diastereomeric salts with optically pure (S)-α-methoxy-α-(trifluoromethyl)phenylacetic acid (MTPA) were used to discriminate the enantiomers of the chiral H3-antagonist 2-[3-(1H-imidazol-4-ylmethyl)piperidin-1-yl]-1H-benzimidazole. Chemical-shift differences (Δδ) in NMR spectra strongly depend on solvent and stoichiometric ratio. The better observable differentiation occurred for the proton at the 2-position of the imidazole ring. Copyright © 2009 John Wiley & Sons, Ltd.

Published

2009

21. Synthesis and structure–activity relationships for biphenyl H3 receptor antagonists with moderate anti-cholinesterase activity

Author

Vigilio Ballabeni, Marco Mor, Giovanni Morini, Fabrizio Bordi, Pier Vincenzo Plazzi, Simona Bertoni, Francesca Saccani, Mirko Rivara, Silvia Rivara, Lisa Flammini, Elisabetta Barocelli, and Mara Comini

Subjects

Stereochemistry, Guinea Pigs, Clinical Biochemistry, Histamine Antagonists, Pharmaceutical Science, Biochemistry, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Histamine receptor, Piperidines, Drug Discovery, Animals, Humans, Receptors, Histamine H3, Structure–activity relationship, Receptor, Molecular Biology, Cells, Cultured, Cholinesterase, biology, Chemistry, Biphenyl Compounds, Organic Chemistry, Acetylcholinesterase, Rats, biology.protein, Molecular Medicine, Cholinesterase Inhibitors, Piperidine, Histamine H3 receptor

Abstract

The combination of antagonism at histamine H 3 receptors and inhibition of acetylcholinesterase has been recently proposed as an approach to devise putative new therapeutic agents for cognitive diseases. The 4,4′-biphenyl fragment has been reported by us as a rigid scaffold leading to potent and selective non-imidazole H 3 -antagonists. Starting from these premises, the current work presents an expanded series of histamine H 3 receptor antagonists, characterized by a central 4,4′-biphenyl scaffold, where the structure–activity profile of both mono-basic and di-basic compounds is further explored and their ability to inhibit rat brain cholinesterase activity is determined. The steric properties and basicity of the terminal groups were modulated in symmetrical compounds, carrying identical substituents, and in asymmetrical compounds, having a piperidine ring at one end and different groups at the other. The length of the linker connecting the biphenyl scaffold to the terminal groups was also modulated. Binding studies at rat and human H 3 receptors evidenced the highest binding affinities for di-basic compounds, in the order of nM concentrations, and that the steric requirements for the two terminal groups are different. Many potent compounds showed good selectivity profiles over the other histamine receptors. Interestingly, some derivatives displayed a moderate ability to inhibit rat brain cholinesterase, for example compound 12 (1-[2-(4′-piperidinomethyl-biphenyl-4-yl)ethyl]piperidine) has a pIC 50 = 5.96 for cholinesterase inhibition and high H 3 receptor binding affinity and antagonist potency (p K i = 8.70; p K B = 9.28). These compounds can be considered as rigid analogs of a recently reported class of dual-acting compounds and as a promising starting point for the design of new H 3 -antagonists with anti-cholinesterase activity.

Published

2008

22. In vitro and in vivo pharmacological analysis of imidazole-free histamine H3 receptor antagonists: promising results for a brain-penetrating H3 blocker with weak anticholinesterase activity

Author

Giovanni Morini, Vigilio Ballabeni, Simona Bertoni, Mara Comini, Elisabetta Barocelli, Giuseppe Domenichini, Mirko Rivara, Lisa Flammini, and Francesca Saccani

Subjects

Cell Survival, Guinea Pigs, In Vitro Techniques, Pharmacology, Receptors, G-Protein-Coupled, Histamine receptor, chemistry.chemical_compound, Ileum, Memory, In vivo, Avoidance Learning, Animals, Humans, Potency, Cells, Cultured, Receptors, Histamine H4, Cholinesterase, biology, Imidazoles, Brain, Heart, General Medicine, Electric Stimulation, In vitro, chemistry, Data Interpretation, Statistical, biology.protein, Receptors, Histamine, Cholinesterase Inhibitors, Histamine H3 receptor, Histamine, Ex vivo, Histamine H3 Antagonists

Abstract

The pharmacological profiling of potent histamine H(3)-ligands initiated in a previous study is completed here. In vitro functional and binding studies revealed that several derivatives were selective H(3)-antagonists with nanomolar potency at human and guinea-pig histamine receptors, able to inhibit rat brain cholinesterase at micromolar concentrations and devoid of any cytotoxicity on cultured cells. Ex vivo binding experiments in rats showed that the most potent H(3)-antagonist, compound 5, had a prompt and long-lasting presence in the central nervous system (CNS), inhibiting [(3)H](R)-alpha-methylhistamine cortical binding [ED(50) (dose that elicits a 50% response) = 0.63 mg/kg intraperitoneally (i.p.)]. In the passive-avoidance test, compound 5, at 1.25 mg/kg i.p., was as effective as the anti-Alzheimer drug donepezil in attenuating scopolamine-induced amnesia in rats. These results suggest that a good CNS penetration and multitarget activity could account for the antiamnesic effect of this weak cholinesterase inhibitor and potent H(3)-antagonist (compound 5). This result represents a potential benchmark for the development of non-imidazole H(3)-antagonists/cholinesterase inhibitors with therapeutic potential in cognitive disorders.

Published

2008

23. Development and validation of a LC–MS method with electrospray ionization for the determination of the imidazole H3 antagonist ROS203 in rat plasma

Author

Elisabetta Barocelli, Alessandro Fioni, Mirko Rivara, Claudia Silva, Vigilio Ballabeni, Lisa Flammini, Fabrizio Bordi, Federica Vacondio, and Marco Mor

Subjects

Spectrometry, Mass, Electrospray Ionization, Electrospray, Calibration curve, Electrospray ionization, Scopolamine, Clinical Biochemistry, Histamine Antagonists, Analytical chemistry, Pharmaceutical Science, Mass spectrometry, High-performance liquid chromatography, Analytical Chemistry, Liquid chromatography–mass spectrometry, Drug Discovery, Avoidance Learning, Animals, Receptors, Histamine H3, Benzothiazoles, Least-Squares Analysis, Rats, Wistar, Quadrupole mass analyzer, Spectroscopy, Chromatography, Behavior, Animal, Molecular Structure, Chemistry, Imidazoles, Reproducibility of Results, Rats, Calibration, Female, Quantitative analysis (chemistry), Injections, Intraperitoneal, Chromatography, Liquid

Abstract

A rapid, simple and sensitive liquid chromatography-mass spectrometry (LC-MS) method was developed and validated for the determination of the imidazole H(3) antagonist ROS203 in rat plasma, using the superior homologue ROS287 as internal standard. Analyses were performed on an Agilent 1100 Series HPLC system employing a Supelco Ascentis C(18) column and isocratic elution with acetonitrile-10mM ammonium acetate buffer pH 4.0 (30:70, v/v) at a flow rate of 0.25 mL/min. An Applied Biosystems/MDS Sciex 150-EX single quadrupole mass spectrometer, equipped with an electrospray ionization interface was employed, operating in the positive ion mode. Plasma samples were deproteinized with acetonitrile (1:2), evaporated under nitrogen stream, reconstituted in the mobile phase and 5 microL were injected into the system. The retention times of ROS203 and IS were 2.20 and 2.90 min, respectively. Calibration curves in spiked plasma were linear over the concentration range of 2610-2.61 ng/mL with determination coefficients >0.99. The lower limit of quantification (LLOQ) was 2.61 ng/mL. The accuracy of the method was within 15%. Intra- and inter-day relative standard deviations were less or equal to 9.50% or 7.19%, respectively. The applicability of the LC-MS method was tested employing plasma samples obtained after i.p. administration of ROS203 to female Wistar rats to support a behavioral in vivo study. The specificity of the method was confirmed by the absence of interferences from endogenous substances. The reported method can provide the necessary sensitivity, linearity, precision, accuracy and specificity to allow the determination of ROS203 in rat plasma samples to support further pharmacokinetic assays.

Published

2008

24. Discovery of antitubercular 2,4-diphenyl-1H-imidazoles from chemical library repositioning and rational design

Author

Baojie Wan, Mirko Rivara, Valentina Zuliani, Gabriele Costantino, Marco Pieroni, and Scott G. Franzblau

Subjects

Tuberculosis, Antitubercular Agents, Disease, Microbial Sensitivity Tests, Pharmacology, Chemical library, Mycobacterium tuberculosis, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Tuberculosis, Multidrug-Resistant, Medicine, biology, Latent tuberculosis, Dose-Response Relationship, Drug, Molecular Structure, business.industry, Organic Chemistry, Rational design, Drug Repositioning, General Medicine, biology.organism_classification, medicine.disease, Virology, Multiple drug resistance, Drug repositioning, chemistry, Drug Design, business

Abstract

TB, caused by Mycobacterium tuberculosis, is one of the deadliest infections worldwide. The co-infection with HIV and the emergence of multidrug-resistant tuberculosis (MDR-TB) and extensively drug-resistant tuberculosis (XDR-TB) strains have further increased the burden for this disease. In the attempt to respond to the constant need of novel therapeutic options, we herein report the discovery of 2,4-diphenyl-1H-imidazoles as effective antitubercular agents, with MIC in the low micromolar range against actively replicating and persistent M. tuberculosis strains. The good activity, along with the lack of toxicity and the feasible synthesis, underscore their value as novel scaffolds for the development of new anti-TB drugs.

Published

2015

25. Synthesis and biological evaluation of new non-imidazole H3-receptor antagonists of the 2-aminobenzimidazole series

Author

Giuseppe Cocconcelli, Mara Comini, Vigilio Ballabeni, Giovanni Morini, Fabrizio Bordi, Marco Mor, Simona Bertoni, Mirko Rivara, Elisabetta Barocelli, Pier Vincenzo Plazzi, Silvia Rivara, and Valentina Zuliani

Subjects

Benzimidazole, Stereochemistry, Clinical Biochemistry, Histamine Antagonists, Substituent, Pharmaceutical Science, Ring (chemistry), Biochemistry, Chemical synthesis, Structure-Activity Relationship, chemistry.chemical_compound, Piperidines, Drug Discovery, Animals, Receptors, Histamine H3, Moiety, Imidazole, Molecular Biology, Cells, Cultured, Binding Sites, Bicyclic molecule, Organic Chemistry, Imidazoles, Brain, Rats, chemistry, Molecular Medicine, Benzimidazoles, Piperidine, Chlorophenols

Abstract

A novel series of non-imidazole H(3)-receptor antagonists was developed, by chemical modification of a potent lead H(3)-antagonist composed by an imidazole ring connected through an alkyl spacer to a 2-aminobenzimidazole moiety (e.g., 2-[[3-[4(5)-imidazolyl]propyl]amino]benzimidazole), previously reported by our research group. We investigated whether the removal of the imidazole ring could allow retaining high affinity for the H(3)-receptor, thanks to the interactions undertaken by the 2-aminobenzimidazole moiety at the binding site. The imidazole ring of the lead was replaced by a basic piperidine or by a lipophilic p-chlorophenoxy substituent, modulating the spacer length from three to eight methylene groups; moreover, the substituents were moved to the 5(6) position of the benzimidazole nucleus. Within both the 2-alkylaminobenzimidazole series and the 5(6)-alkoxy-2-aminobenzimidazole one, the greatest H(3)-receptor affinity was obtained for the piperidine-substituted compounds, while the presence of the p-chlorophenoxy group resulted in a drop in affinity. The optimal chain length was different in the two series. Even if the new compounds did not reach the high receptor affinity shown by the imidazole-containing lead compound, it was possible to get good H(3)-antagonist potencies with 2-aminobenzimidazoles having a tertiary amino group at appropriate distance.

Published

2006

26. Validation of a histamine H3 receptor model through structure–activity relationships for classical H3 antagonists

Author

Silvia Rivara, Elisabetta Barocelli, Marco Mor, Simone Lorenzi, Mirko Rivara, Giovanni Morini, Fabrizio Bordi, Simona Bertoni, Pier Vincenzo Plazzi, and Vigilio Ballabeni

Subjects

Models, Molecular, Rhodopsin, Time Factors, Molecular model, G protein, Stereochemistry, Molecular Sequence Data, Clinical Biochemistry, Histamine Antagonists, Quantitative Structure-Activity Relationship, Pharmaceutical Science, Crystallography, X-Ray, Binding, Competitive, Biochemistry, chemistry.chemical_compound, Drug Discovery, Animals, Receptors, Histamine H3, Amino Acid Sequence, Binding site, Molecular Biology, G protein-coupled receptor, Molecular Structure, Chemistry, Organic Chemistry, Rats, Docking (molecular), Molecular Medicine, Cattle, Pharmacophore, Histamine H3 receptor, Sequence Alignment, Histamine

Abstract

Histamine H(3) receptor is a G protein-coupled receptor whose activation inhibits the synthesis and release of histamine and other neurotransmitters from nerve endings and is involved in the modulation of different central nervous system functions. H(3) antagonists have been proposed for their potential usefulness in diseases characterized by impaired neurotransmission and they have demonstrated beneficial effects on learning and food intake in animal models. In the present work, a 3D model of the rat histamine H(3) receptor, built by comparative modeling from the crystallographic coordinates of bovine rhodopsin, is presented with the discussion of its ability to predict the potency of known and new H(3) antagonists. A putative binding site for classical, imidazole-derived H(3) antagonists was identified by molecular docking. Comparison with a known pharmacophore model and the binding affinity of a new rigid H(3) antagonist (compound 1, pK(i)=8.02) allowed the characterization of a binding scheme which could also account for the different affinities observed in a recently reported series of potent H(3) antagonists, characterized by a 2-aminobenzimidazole moiety. Molecular dynamics simulations were employed to assess the stability and reliability of the proposed binding mode. Two new conformationally constrained benzimidazole derivatives were prepared and their binding affinity was tested on rat brain membranes; compound 9, designed to reproduce the conformation of a known potent H(3) antagonist, showed higher potency than compound 8, as expected from the binding scheme hypothesized.

Published

2005

27. The role of HB-donor groups in the heterocyclic polar fragment of H3-antagonists

Author

Valentina Zuliani, Federica Vacondio, Simona Bertoni, Mirko Rivara, Silvia Rivara, Pier Vincenzo Plazzi, Elisabetta Barocelli, Francesca Magnanini, Vigilio Ballabeni, Giovanni Morini, Fabrizio Bordi, and Claudia Silva

Subjects

chemistry.chemical_classification, Bicyclic molecule, Hydrogen bond, Stereochemistry, Pharmaceutical Science, Chemical synthesis, chemistry.chemical_compound, chemistry, Drug Discovery, Imidazole, Moiety, Binding site, Guanidine, Alkyl

Abstract

It has been recently reported that compounds composed of an imidazole connected through an alkyl spacer to a 2-aminobenzimidazole showed high affinity towards the H(3)-receptor. The guanidine fragment of the 2-aminobenzimidazole is probably involved in hydrogen bond interactions at the binding site, and is referred to as the 'polar fragment'. In the present work, starting from 2-aminobenzimidazole derivatives with a di-methylene spacer 1 (pK(i)=7.25) or a tri-methylene one 2 (pK(i)=8.90), we investigated the importance of the hydrogen bond (HB) donor groups at the polar fragment in the interaction with the H(3)-receptor. The replacement of 2-aminobenzimidazoles with different moieties [2-aminobenzothiazole, 3, 4; 2-thiobenzimidazole, 5, 6; 2-thiobenzothiazole, 7, 8; 2-thio-4-phenyl- or 2-thio-5-phenyl-N-methylimidazoles, 9-12] highlighted the effect of the polar group basicity on the optimal length of the alkyl chain: longer spacers were preferred with polar groups of moderate basicity whereas, in the presence of neutral polar groups, the best affinity values were obtained with di-methylene chains. Moreover, N-methylation at the 2-aminobenzimidazole moiety 13-16 revealed different behaviour for compounds having different spacer lengths. In fact, methylation of the exocyclic NH group maintained high affinity for the tri-methylene 2-aminobenzimidazole derivative, while a drop in affinity was observed for the annular N-methylation. An opposite trend characterised di-methylene derivatives. These observed SAR suggest that, within this class of compounds, the number of HB-donor groups can be lowered while maintaining high receptor affinity. Since the presence of HB-donor groups strongly affects brain access, this observation could be useful to design and prepare new H(3)-antagonists.

Published

2003

28. ChemInform Abstract: Inhibition of Nav1.6 Sodium Channel Currents by a Novel Series of 1,4-Disubstituted-triazole Derivatives Obtained via Copper-Catalyzed Click Chemistry

Author

Laura Amori, Manoj K. Patel, Mirko Rivara, and Valentina Zuliani

Subjects

chemistry.chemical_compound, chemistry, Aryl, Triazole, Substituent, Click chemistry, Molecule, Imidazole, General Medicine, Ring (chemistry), Combinatorial chemistry, Cycloaddition

Abstract

We have synthesized and evaluated a series of 1,4-disubstituted-triazole derivatives for inhibition of the rat Na(V)1.6 sodium channel isoform, an isoform thought to play an important role in controlling neuronal firing. Starting from a series of 2,4(1H)-diarylimidazoles previously published, we decided to extend the SAR study by replacing the imidazole with a different heterocyclic scaffold and by varying the aryl substituents on the central aromatic ring. The 1,4-disubstituted 1,2,3-triazoles were prepared employing the copper-catalyzed azide-alkyne cycloaddition (CuAAC). Many of the new molecules were able to block the rNa(v)1.6 currents at 10 μM by over 20%, displaying IC(50) values ranging in the low micromolar, thus indicating that triazole can efficiently replace the central heterocyclic core. Moreover, the introduction of a long chain at C4 of the central triazole seems beneficial for increased rNa(v)1.6 current block, whereas the length of N1 substituent seems less crucial for inhibition, as long as a phenyl ring is not direcly connected to the triazole. These results provide additional information on the structural features necessary for block of the voltage-gated sodium channels. These new data will be exploited in the preparation of new compounds and could result in potentially useful AEDs.

Published

2013

29. Advances in Design and Development of Sodium Channel Blockers

Author

Laura Amori, Valentina Zuliani, and Mirko Rivara

Subjects

Gene isoform, Electrophysiology, Epilepsy, Sodium channel blocker, business.industry, Sodium channel, State selective, Chronic pain, medicine, Cellular excitability, medicine.disease, business, Neuroscience

Abstract

The voltage-gated sodium channels (VGSCs) play a fundamental role in controlling cellular excitability. Abnormal activity of sodium channels is related to several pathological processes, including cardiac arrhythmias, epilepsy, chronic pain, neurodegenerative diseases, and spasticity. In view of this, VGSCs are considered important therapeutic targets for the treatment of these disorders. To date, nine functional VGSC isoforms have been identified and have a distinct pattern of expression within the human body. In addition, VGSC also have distinct electrophysiological profiles with differing activation and inactivation states. As such, there is a concerted effort to develop not only isoform selective blockers, but also blockers that exhibit state selectivity, particularly to the inactivated state of the channel. This article provides a brief historical perspective and primarily focuses on recent advances in the development of isoform specific and state selective sodium channel blockers and the medicinal chemistry involved, surveying the emerging therapeutic fields.

Published

2011

30. ChemInform Abstract: Microwave Assisted Efficient Synthesis of Imidazole-Based Privileged Structures

Author

Mirko Rivara, Marco Fantini, Mario A. Spotti, and Valentina Zuliani

Subjects

chemistry.chemical_compound, Scope (project management), chemistry, Microwave heating, Molecule, Imidazole, Nanotechnology, General Medicine, Microwave assisted

Abstract

A simple and efficient microwave assisted synthesis of imidazobenzoxazines, imidazobenzoxazin-5-ones, and imidazobenzoxazin-5-thiones with broad chemistry scope is described. The molecules were prepared both under conventional as well as microwave heating conditions, to provide in high yields with clean and scalable reactions a small library of imidazole-based privileged structures for drug discovery.

Published

2010

31. Sodium channel blockers for neuropathic pain

Author

Mirko Rivara, Valentina Zuliani, Marco Fantini, and Gabriele Costantino

Subjects

Diabetic neuropathy, Sodium Channels, Patents as Topic, Epilepsy, Sodium channel blocker, Drug Delivery Systems, Trigeminal neuralgia, Drug Discovery, Medicine, Animals, Humans, Spasticity, Spinal cord injury, Pharmacology, Analgesics, business.industry, Sodium channel, General Medicine, medicine.disease, Anesthesia, Drug Design, Neuropathic pain, Chronic Disease, Neuralgia, medicine.symptom, business, Sodium Channel Blockers

Abstract

The voltage-gated sodium channels (VGSCs) play a fundamental role in controlling cellular excitability and their abnormal activity is related to several pathological processes, including cardiac arrhythmias, epilepsy, neurodegenerative diseases, spasticity, chronic and neuropathic pain. In particular, neuropathic pain (e.g., postherpetic and trigeminal neuralgia, diabetic neuropathy and spinal cord injury) is a serious clinical problem that affects a high percentage of the world population. Because an altered sodium channel isoform expression profile has been considered one reason for the changes in neuronal excitability, there is a continuous quest for new selective molecules targeting sodium channels for the treatment of chronic pain.PubMed, http://www.sciencedirect.com/ , SciFinder Scholar and http://ep.espacenet.com/ were used as sources for this review and patents between 2007 and September 2009 were taken into account for the sodium channel blockers molecular classes reviewed and discussed herein.The sodium channel blockers reported in this review have been categorized into different molecular classes on the basis of their wide structural diversity. This classification, somewhat arbitrary, does not necessarily reflect the presence of pharmacophoric elements but offers a useful way to discuss and comment on structurally homogenous classes of chemotypes recently patented.The continuous discoveries in the field of sodium channel blockers, highlighted by the increasing numbers of patent applications published in the last few years and by the numbers of compounds currently in clinical development, underline the importance of this target for the treatment of neuropathic pain. The great difficulty in the design of new selective and active structures, not obtained from old VGSC blockers that are often associated with high risk of adverse effects, is a strong challenge for medicinal chemistry research.

Published

2010

32. NMR analysis of a series of imidazobenzoxazines

Author

Domenico Acquotti, Marco Fantini, Valentina Zuliani, and Mirko Rivara

Subjects

Magnetic Resonance Spectroscopy, Nuclear magnetic resonance, Models, Chemical, Series (mathematics), Chemistry, Computational chemistry, Structural isomer, General Materials Science, General Chemistry, Carbon-13 NMR, Two-dimensional nuclear magnetic resonance spectroscopy, Heteronuclear single quantum coherence spectroscopy, Benzoxazines

Abstract

The complete 1H and 13C NMR assignment of a series of imidazobenzoxazines by a combination of one- and two-dimensional experiments (COSY, HSQC and HMBC) is studied. Moreover, 2D NOESY and 1D selective NOESY are reported. This procedure allows the identification of the regioisomers obtained. Copyright © 2010 John Wiley & Sons, Ltd.

Published

2010

33. Microwave assisted efficient synthesis of imidazole-based privileged structures

Author

Mirko Rivara, Marco Fantini, Valentina Zuliani, and Mario A. Spotti

Subjects

chemistry.chemical_compound, Molecular Structure, Chemistry, Microwave heating, Imidazoles, Imidazole, Molecule, Combinatorial Chemistry Techniques, Nanotechnology, General Chemistry, Microwaves, Microwave assisted, Combinatorial chemistry

Abstract

A simple and efficient microwave assisted synthesis of imidazobenzoxazines, imidazobenzoxazin-5-ones, and imidazobenzoxazin-5-thiones with broad chemistry scope is described. The molecules were prepared both under conventional as well as microwave heating conditions, to provide in high yields with clean and scalable reactions a small library of imidazole-based privileged structures for drug discovery.

Published

2009

34. ChemInform Abstract: A Short and Efficient Synthesis of the Selective H4Receptor Agonist 4-Methylhistamine

Author

Mirko Rivara, Fabrizio Bordi, P. V. Plazzi, and Valentina Zuliani

Subjects

Agonist, chemistry.chemical_compound, Stereochemistry, Chemistry, medicine.drug_class, medicine, General Medicine, Histamine H4 receptor, Combinatorial chemistry, 4-Methylhistamine

Published

2009

35. Chiral NMR discrimination of the diastereoisomeric salts of the H3-antagonist 2-[3-(1H-imidazol-4-ylmethyl)piperidin-1-yl]-1H-benzimidazole

Author

Mirko, Rivara, Valentina, Zuliani, Marco, Fantini, Elisa, Dallaturca, and Marco, Mor

Subjects

Magnetic Resonance Spectroscopy, Piperidines, Benzimidazoles, Stereoisomerism, Reference Standards, Histamine H3 Antagonists

Abstract

Diastereomeric salts with optically pure (S)-alpha-methoxy-alpha-(trifluoromethyl)phenylacetic acid (MTPA) were used to discriminate the enantiomers of the chiral H(3)-antagonist 2-[3-(1H-imidazol-4-ylmethyl)piperidin-1-yl]-1H-benzimidazole. Chemical-shift differences (Delta delta) in NMR spectra strongly depend on solvent and stoichiometric ratio. The better observable differentiation occurred for the proton at the 2-position of the imidazole ring.

Published

2009

36. 2,4(5)-Diarylimidazoles: synthesis and biological evaluation of a new class of sodium channel blockers against hNa(v)1.2

Author

Mirko Rivara, Aparna Baheti, Natasha Singh, Christopher L. Kalmar, Valentina Zuliani, Ellen C. Merrick, Marco Fantini, Giuseppe Cocconcelli, Manoj K. Patel, and Chiara Ghiron

Subjects

Stereochemistry, Chemistry, Pharmaceutical, Clinical Biochemistry, Pharmaceutical Science, Nerve Tissue Proteins, Biochemistry, Sodium Channels, chemistry.chemical_compound, Structure-Activity Relationship, Sodium channel blocker, Drug Discovery, Humans, Protein Isoforms, Molecular Biology, Biological evaluation, NAV1.2 Voltage-Gated Sodium Channel, Molecular Structure, Sodium channel, Organic Chemistry, Sodium, Imidazoles, chemistry, Models, Chemical, Drug Design, Molecular Medicine, Lead compound, Ion Channel Gating, Sodium Channel Blockers

Abstract

A small family of novel 2,4(5)-diarylimidazoles were prepared through a simple and efficient synthesis and evaluated as potential inhibitors of hNa(v)1.2 sodium channel currents. One member of this series (4) exhibited profound inhibition of Na(v)1.2 currents, emerging as a promising lead compound for further structure-activity relationship studies for the development of novel sodium channel blockers.

Published

2008

37. Synthesis and stability in biological media of 1H-imidazole-1-carboxylates of ROS203, an antagonist of the histamine H3 receptor

Author

Elisabetta Barocelli, Valentina Zuliani, Pier Vincenzo Plazzi, Marco Fantini, Vigilio Ballabeni, Mirko Rivara, Simona Bertoni, Claudia Lucia Martins Silva, Lisa Flammini, Fabrizio Bordi, Marco Mor, and Federica Vacondio

Subjects

Stereochemistry, Swine, Carboxylic Acids, Drug Evaluation, Preclinical, Bioengineering, Biochemistry, Esterase, Catalysis, chemistry.chemical_compound, Structure-Activity Relationship, Drug Stability, Enzymatic hydrolysis, Structure–activity relationship, Animals, Receptors, Histamine H3, Benzothiazoles, Bovine serum albumin, Molecular Biology, biology, Molecular Structure, Hydrolysis, Esterases, Imidazoles, Serum Albumin, Bovine, Stereoisomerism, General Chemistry, General Medicine, Hydrogen-Ion Concentration, Ligand (biochemistry), Rats, chemistry, Liver, Lipophilicity, Injections, Intravenous, biology.protein, Molecular Medicine, Ethyl carbamate, Chemical stability, Cattle, Histamine H3 Antagonists

Abstract

A series of carbamate derivatives of the H(3) antagonist ROS203 (1) were prepared, and their lipophilicity and steric hindrance were modulated by introducing linear or branched alkyl chains of various lengths. In vitro stability studies were conducted to evaluate how structural modulations affect the intrinsic reactivity of the carbamoyl moiety and its recognition by metabolic enzymes. Linear alkyl carbamates were the most susceptible to enzymatic hydrolysis, with bioconversion rates being higher in rat liver and plasma. Chain ramification significantly enhanced the enzymatic stability of the set, with two derivatives (1g and 1h) being more stable by a factor of 8-40 than the ethyl carbamate 1a. Incubation with bovine serum albumin (BSA) showed a protective role of proteins on chemical and porcine-liver esterase (PLE)-catalyzed hydrolysis. Ex vivo binding data after i.v. administration of 1h revealed prolonged displacement of the labeled ligand [(3)H]-(R)-alpha-methylhistamine ([(3)H]RAMHA) from rat-brain cortical membranes, when compared to 1. However, the high rates of bioconversion in liver, as well as the chemical instability of 1h, suggest that further work is needed to optimize the enzymatic and chemical stability of these compounds.

Published

2008

38. A Practical Synthesis of 2,4(5)-Diarylimidazoles from Simple Building Blocks

Author

Chiara Ghiron, Mirko Rivara, Marco Fantini, Giuseppe Cocconcelli, and Valentiani Zuliani

Subjects

Reaction conditions, Simple (abstract algebra), Chemistry, Yield (chemistry), Organic Chemistry, Benzene Derivatives, Imidazoles, General Medicine, Selectivity, Chemical synthesis, Combinatorial chemistry

Abstract

A simple and efficient approach to selectively obtain 2,4(5)-diarylimidazoles suppressing formation of 2-aroyl-4(5)-arylimidazoles is described. The yield of each of the two products strongly depends on the reaction conditions employed. This reaction provides a simple method to prepare small libraries of biologically active compounds by parallel synthesis.

Published

2007

39. WITHDRAWN: A short and efficient synthesis of the selective H4 receptor agonist 4-methylhistamine

Author

Mirko Rivara, Fabrizio Bordi, and Valentina Zuliani

Subjects

Agonist, chemistry.chemical_compound, Chemistry, medicine.drug_class, Organic Chemistry, Drug Discovery, medicine, Nanotechnology, Histamine H4 receptor, Pharmacology, Biochemistry, 4-Methylhistamine

Abstract

This article has been withdrawn consistent with Elsevier Policy on Article Withdrawal ( http:www.elsevier.com/locate/withdrawalpolicy ). The Publisher apologizes for any inconvenience this may cause.

Published

2007

40. Dibasic non-imidazole histamine H3 receptor antagonists with a rigid biphenyl scaffold

Author

Marco Mor, Mara Comini, Lisa Flammini, Simona Bertoni, Vigilio Ballabeni, Simone Lorenzi, Silvia Rivara, Mirko Rivara, Giovanni Morini, Fabrizio Bordi, Pier Vincenzo Plazzi, and Elisabetta Barocelli

Subjects

Models, Molecular, Molecular model, Tertiary amine, Stereochemistry, Clinical Biochemistry, Guinea Pigs, Histamine Antagonists, Pharmaceutical Science, Biochemistry, Cell Line, chemistry.chemical_compound, Histamine receptor, Drug Discovery, Imidazole, Animals, Humans, Receptors, Histamine H3, Molecular Biology, Dibasic acid, Organic Chemistry, Imidazoles, Rats, chemistry, Docking (molecular), Molecular Medicine, Amine gas treating, Histamine H3 receptor

Abstract

A class of rigid, dibasic, non-imidazole H 3 antagonists was developed, starting from a series of previously described flexible compounds. The original polymethylene chain between two tertiary amine groups was replaced by a rigid scaffold, composed by a phenyl ring or a biphenyl fragment. Modulation of the distance between the two amine groups, and of their alkyl substituents, was driven by superposition of molecular models and docking into a receptor model, resulting in the identification of 1,1′-[biphenyl-4,4′-diylbis(methylene)]bis-piperidine ( 5 ) as a subtype-selective H 3 antagonist with high binding affinity (p K i = 9.47) at human H 3 histamine receptor.

Published

2006

41. Synthesis, antioxidant activity and structure-activity relationships for a new series of 2-(N-acylaminoethyl)indoles with melatonin-like cytoprotective activity

Author

Davide Franceschini, Claudia Silva, Giuseppe Diamantini, Marco Mor, Morena Zusso, Federica Vacondio, Annalida Bedini, Gilberto Spadoni, Pier Vincenzo Plazzi, Pietro Giusti, Mirko Rivara, and Giorgio Tarzia

Subjects

Antioxidant, medicine.medical_treatment, Antioxidants, Melatonin, chemistry.chemical_compound, Inhibitory Concentration 50, Structure-Activity Relationship, Endocrinology, In vivo, Cerebellum, medicine, Structure–activity relationship, Animals, Cells, Cultured, Indole test, Neurons, ABTS, Cytoprotection, Lipids, Tryptamines, Biochemistry, chemistry, Solubility, Lipophilicity, medicine.drug

Abstract

5-Methoxy-2-(N-acetylaminoethyl)indole (5d), a melatonin analogue derived from the transposition of the acetylaminoethyl side chain from C3 to C2 of the indole nucleus, had been previously characterized as a low affinity antagonist at MT1 and MT2 membrane receptors; this molecule is endowed with good in vitro antioxidant and cytoprotective potency in rat cerebellar cell cultures, comparable to or better than those of melatonin. In order to further investigate the role of structure-antioxidant activity relationships in cytoprotection, the structure of 5d was systematically modulated to design a new series of compounds. The 5-methoxy group was replaced by substituents with different electronic and lipophilic properties and it was moved to a different position on the indole ring. Other modifications of the lead structure involved the methylation of the indole nitrogen or its replacement by a sulfur atom. The side chain was also modified either increasing its lipophilicity or introducing an ionisable acid group. The antioxidant activity of this set of compounds was evaluated by the ABTS and conjugated dienes (CD) assays, while their cytoprotection was evaluated against kainate-induced cytotoxicity in cultured cerebellar neurons. In both antioxidant assays, the shift of the 5-methoxy group to the 4-position of the indole nucleus led to the most active radical scavenger (9), more potent than the parent compound and melatonin in the antioxidant tests, but much less effective as a cytoprotectant. Sharp structure-activity relationships were registered for cytoprotection, where the maintenance of the 5-alkoxy-2-(N-acylaminoethyl)indole scaffold appeared as the key feature to confer both antioxidant and cytoprotective activity to the structure. Some derivatives of the set, however, together with the most potent 5d, maintained a significant antioxidant and cytoprotective effect and could be employed as tools for in vivo pharmacological investigations on neuroprotective efficacy of melatonin-related indoles.

Published

2006

42. Antioxidant and cytoprotective activity of indole derivatives related to melatonin

Author

Marco, Mor, Gilberto, Spadoni, Giuseppe, Diamantini, Annalida, Bedini, Giorgio, Tarzia, Claudia, Silva, Federica, Vacondio, Mirko, Rivara, Pier Vincenzo, Plazzi, Davide, Franceschini, Morena, Zusso, and Pietro, Giusti

Subjects

Indoles, Quantitative Structure-Activity Relationship, In Vitro Techniques, Thiobarbituric Acid Reactive Substances, Antioxidants, Rats, Rats, Sprague-Dawley, Cytoprotection, Cerebellum, Animals, Female, Benzothiazoles, Rats, Wistar, Sulfonic Acids, Cells, Cultured, Melatonin

Abstract

Melatonin (MLT) is known for its radical scavenger activity, which had been related to its ability to protect neuronal cells from different kinds of oxidative stress. In particular, MLT protects rat cerebellum granular cells from kainate-induced necrosis at concentrations higher than 100 microM, and is able to reduce lipoperoxidation induced by radical stress in rat brain homogenate at similar concentrations. On the other hand, MLT has nanomolar affinity for its membrane receptors (MT1 and MT2), and these are completely saturated at the high concentrations employed when the cytoprotective effect is observed. Other indole derivatives are also known to possess antioxidant and cytoprotective activity. In order to dissociate the cytoprotective effect of MLT from its receptor affinity, and to investigate the structure-activity relationships (SAR) between this effect and some potentially relevant chemical properties, we prepared a series of indole derivatives, where the structure of MLT was gradually modulated, varying the 5-methoxy group nature and position, the acylaminoethyl chain position, and by the introduction of lipophilic groups. These modifications resulted in a set of compounds having different receptor affinity and intrinsic activity, different lipophilicity, and different substitution at the indole nucleus. The compounds were tested for their antioxidant potency by the ABTS test and by inhibition of rat brain homogenate lipoperoxidation; their cytoprotective effect was also estimated from the inhibition of kainate-induced cellular death on rat cerebellum granular cells, and the results were evaluated by SAR comparison and QSAR analysis. An isomer of MLT resulted more potent and effective than MLT itself in the cytoprotection test, although it showed similar potency in the peroxidation test, and it was devoid of the ability to stimulate MT1 and MT2 receptors. This compound was selected as the lead compound for a further SAR study, devoted to the optimization of the cytoprotective effect and to the investigation on its mechanism.

Published

2004

43. Imidazole H3-antagonists: relationship between structure and ex vivo binding to rat brain H3-receptors

Author

Fabrizio Bordi, Marco Mor, Mirko Rivara, Vigilio Ballabeni, Elisabetta Barocelli, Simona Bertoni, Valentina Zuliani, Federica Vacondio, Pierre-Alain Carrupt, Silvia Rivara, Bernard Testa, Francesca Magnanini, Claudia Silva, and Pier Vincenzo Plazzi

Subjects

Chemical Phenomena, Histamine Antagonists, Pharmaceutical Science, Histamine Agonists/metabolism, Histamine Antagonists/*pharmacokinetics/*pharmacology, Imidazoles/*pharmacokinetics/*pharmacology, Lipids/chemistry, In Vitro Techniques, Binding, Competitive, Histamine Agonists, chemistry.chemical_compound, Structure-Activity Relationship, Methylhistamines/metabolism, Biotransformation, Potency, Imidazole, Receptors, Histamine H3, Animals, Rats, Wistar, Receptor, ddc:615, Chemistry, Physical, Methylhistamines, Antagonist, Imidazoles, Brain, Hydrogen Bonding, Physicochemical Phenomena, Binding, Competitive/drug effects, Brain/drug effects/*metabolism, Hydrogen-Ion Concentration, Receptors, Histamine H3/*drug effects, Lipids, In vitro, Liver/drug effects/metabolism, Rats, chemistry, Biochemistry, Liver, Solubility, Lipophilicity, Potentiometry, Female, Ex vivo

Abstract

H3-antagonists possess promising pharmacological effects on awakening, learning and memory, but few data on their access to the central nervous system (CNS) have been reported so far. The purpose of this work was to investigate the relationships between structure and brain penetration of a series of H3-antagonists, using ex vivo binding experiments in rats. H3-antagonists belonging to different chemical classes but all having an imidazole ring, an alkyl spacer, a polar fragment and a lipophilic ending group, were selected among the numerous H3-antagonists recently described by us. Ex vivo binding studies were performed by inhibiting specific [3H]-(R)-alpha-methylhistamine ([3H]-RAMHA) binding to rat cerebral cortical membranes following H3-antagonist peripheral administration. Ionization constants and partition coefficients in n-octanol/water and 1,2-dichloroethane/water were determined by the potentiometric pH-metric method and were compared to the ex vivo binding potencies to analyse structure-property relationships (SPR). In the ex vivo assay, the H3-antagonists showed different potencies (pED50) not correlated to their in vitro H3-receptor binding affinities (pKi). Compound 4a, having a benzothiazol-2-yl-thioethyl chain, showed high ex vivo potency (ED50=1.35 mg kg(-1) i.p.) and a fast brain penetration, eliciting maximal displacement of [3H]-RAMHA already 5 min after i.v. or i.p. administration. Ex vivo binding assays of three compounds, following i.v. and i.p. administration, showed that the observed i.p. ex vivo potencies were not significantly affected by biotransformation. Within the set of compounds, those having a better ability to reach the CNS had a logDoct(7.4) in the range 2-3.5, and a DeltalogPoct-dce < 2. The combined use of two easily measurable physicochemical descriptors, namely logDoct(7.4) (apparent lipophilicity at pH 7.4) and DeltalogPoct-dce (a descriptor of H-bond donor capacity) allowed to model brain permeation of the majority of the compounds examined.

Published

2004

44. Synthesis, biological activity, QSAR and QSPR study of 2-aminobenzimidazole derivatives as potent H3-antagonists

Author

Elisabetta Barocelli, Vigilio Ballabeni, Mariannina Impicciatore, Silvia Rivara, Simona Bertoni, Mirko Rivara, Federica Vacondio, Valentina Zuliani, Fabrizio Bordi, Claudia Silva, Francesca Magnanini, Pier Vincenzo Plazzi, and Marco Mor

Subjects

Benzimidazole, Quantitative structure–activity relationship, Intrinsic activity, Stereochemistry, Clinical Biochemistry, Histamine Antagonists, Pharmaceutical Science, Quantitative Structure-Activity Relationship, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Drug Discovery, Electronic effect, Moiety, Animals, Receptors, Histamine H3, Rats, Wistar, Molecular Biology, Bicyclic molecule, Molecular Structure, Methylhistamines, Organic Chemistry, Cell Membrane, Brain, Rats, chemistry, Drug Design, Lipophilicity, Molecular Medicine, Benzimidazoles

Abstract

We report the design, synthesis, QSPR and QSAR of a new class of H(3)-antagonists, having a 2-aminobenzimidazole moiety connected to the 4(5) position of an imidazole ring through di- or tri-methylene chains. Eleven substituents, selected by experimental design to obtain broad and non-correlated variation in their lipophilic, electronic and steric properties, were introduced at the 5(6) position of the benzimidazole nucleus. The compounds were tested for their H(3)-receptor affinity, by displacement of [(3)H]-(R)-alpha-methylhistamine ([(3)H]-RAMHA) binding to rat brain membranes (pK(i)), for intrinsic activity, evaluating their effect on [(35)S]GTPgammaS binding to rat brain membranes, and for H(3)-antagonist potency, on electrically stimulated guinea-pig ileum (pK(B)). The pK(i) values of the derivatives with longer chain (5a-k) ranged over 2 orders of magnitude, with the 5(6)-methoxy derivative 5d endowed with sub-nanomolar affinity (pK(i)=9.37). The series having two methylene groups in the chain spacer (4a-k), showing a small variation in affinity, revealed to be somewhat insensitive to ring substitution. Lipophilicity (log P) and basicity (pK(a)) of the newly synthesized compounds were measured and related to receptor affinity in a QSAR study. Multiple regression analysis (MRA) showed an approximate parabolic dependence of pK(i) on log P, while an additional electronic effect of the substituents on benzimidazole tautomerism is suspected.

Published

2003

45. Recent Advances in the Medicinal Chemistry of Sodium Channel Blockers and their Therapeutic Potential

Author

Marco Fantini, Mirko Rivara, Manoj K. Patel, and Valentina Zuliani

Subjects

Gene isoform, Chemistry, Chemistry, Pharmaceutical, State selective, Sodium channel, Chronic pain, General Medicine, Pharmacology, medicine.disease, Medicinal chemistry, Sodium Channels, Structure-Activity Relationship, Epilepsy, Electrophysiology, Sodium channel blocker, Drug Discovery, Cellular excitability, medicine, Humans, Protein Isoforms, Sodium Channel Blockers

Abstract

The voltage-gated sodium channels (VGSCs) play a fundamental role in controlling cellular excitability. Abnormal activity of sodium channels is related to several pathological processes, including cardiac arrhythmias, epilepsy, chronic pain, neurodegenerative diseases and spasticity. In view of this, VGSCs are considered important therapeutic targets for the treatment of these disorders. To date, nine VGSC isoforms have been identified and have a distinct pattern of expression within the human body. In addition, VGSCs also have distinct electrophysiological profiles with differing activation and inactivation states. As such, there is a concerted effort to develop not only isoform selective antagonists, but also antagonists that exhibit state selectivity, particularly to the inactivated state of the channel. This review will provide a brief historical prospective and will primarily focus on recent advances in the development of isoform specific and state selective sodium channel antagonists and the medicinal chemistry involved, surveying the emerging therapeutic fields.

46. A Short and Efficient Synthesis of the Selective H-4 Receptor Agonist 4-Methylhistamine

Author

P. V. Plazzi, Valentina Zuliani, Fabrizio Bordi, and Mirko Rivara

Subjects

Agonist, chemistry.chemical_compound, chemistry, medicine.drug_class, Organic Chemistry, medicine, Histamine H4 receptor, Pharmacology, Biochemistry, 4-Methylhistamine

47. Antioxidant and cytoprotective activity of indole derivatives related to melatonin

Author

Giorgio Tarzia, Morena Zussot, Pietro Giusti, Mirko Rivara, Gilberto Spadoni, Federica Vacondio, Annalida Bedini, Marco Mor, Davide Franceschinit, Claudia Silva, Giuseppe Diamantini, and Pier Vincenzo Plazzi

Subjects

Indole test, ABTS, Antioxidant, Intrinsic activity, medicine.medical_treatment, Melatonin receptor, Melatonin, chemistry.chemical_compound, chemistry, Biochemistry, Lipophilicity, medicine, Receptor, medicine.drug

Abstract

Melatonin (MLT) is known for its radical scavenger activity, which had been related to its ability to protect neuronal cells from different kinds of oxidative stress. In particular, MLT protects rat cerebellum granular cells from kainate-induced necrosis at concentrations higher than 100 µM, and is able to reduce lipoperoxidation induced by radical stress in rat brain homogenate at similar concentrations. On the other hand, MLT has nanomolar affinity for its membrane receptors (MT’and MT2), and these are completely saturated at the high concentrations employed when the cytoprotective effect is observed. Other indole derivatives are also known to possess antioxidant and cytoprotective activity. In order to dissociate the cytoprotective effect of MLT from its receptor affinity, and to investigate the structure-activity relationships (SAR) between this effect and some potentially relevant chemical properties, we prepared a series of indole derivatives, where the structure of MLT was gradually modulated, varying the 5methoxy group nature and position, the acylaminoethyl chain position, and by the introduction of lipophilic groups. These modifications resulted in a set of compounds having different receptor affinity and intrinsic activity, different lipophilicity, and different substitution at the indole nucleus. The compounds were tested for their antioxidant potency by the ABTS test and by inhibition of rat brain homogenate kainate

48. Biological Evaluation of Imidazobenzoxazines, Imidazobenzoxazin-5-ones and Imidazobenzoxazin-5-thiones as Sodium Channel Blockers

Author

Mirko Rivara, Valentina Zuliani, and Manoj K. Patel

Subjects

Sodium channel blocker, Chemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Combinatorial chemistry, Biological evaluation

49. Microwave Assisted Efficient Synthesis of Imidazole-Based Privileged Structures.

Author

Marco Fantini, Valentina Zuliani, Mario A. Spotti, and Mirko Rivara

Subjects

*IMIDAZOLES, *MICROWAVE heating, *ORGANIC synthesis, *HETEROCYCLIC compounds, *MOLECULAR structure, *DRUG development, *CHEMICAL reactions

Abstract

A simple and efficient microwave assisted synthesis of imidazobenzoxazines, imidazobenzoxazin-5-ones, and imidazobenzoxazin-5-thiones with broad chemistry scope is described. The molecules were prepared both under conventional as well as microwave heating conditions, to provide in high yields with clean and scalable reactions a small library of imidazole-based privileged structures for drug discovery. [ABSTRACT FROM AUTHOR]

Published

2010