Therapeutic Approaches to Genetic Ion Channelopathies and Perspectives in Drug Discovery

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Abstract

In the human genome more than 400 genes encode ion channels, which are transmembrane proteins mediating ion fluxes across membranes. Being expressed in all cell types, they are involved in almost all physiological processes, including sense perception, neurotransmission, muscle contraction, secretion, immune response, cell proliferation, and differentiation. Due to the widespread tissue distribution of ion channels and their physiological functions, mutations in genes encoding ion channel subunits, or their interacting proteins, are responsible for inherited ion channelopathies. These diseases can range from common to very rare disorders and their severity can be mild, disabling, or life-threatening. In spite of this, ion channels are the primary target of only about 5% of the marketed drugs suggesting their potential in drug discovery. The current review summarizes the therapeutic management of the principal ion channelopathies of central and peripheral nervous system, heart, kidney, bone, skeletal muscle and pancreas, resulting from mutations in calcium, sodium, potassium, and chloride ion channels. For most channelopathies the therapy is mainly empirical and symptomatic, often limited by lack of efficacy and tolerability for a significant number of patients. Other channelopathies can exploit ion channel targeted drugs, such as marketed sodium channel blockers. Developing new and more specific therapeutic approaches is therefore required. To this aim, a major advancement in the pharmacotherapy of channelopathies has been the discovery that ion channel mutations lead to change in biophysics that can in turn specifically modify the sensitivity to drugs: this opens the way to a pharmacogenetics strategy, allowing the development of a personalized therapy with increased efficacy and reduced side effects. In addition, the identification of disease modifiers in ion channelopathies appears an alternative strategy to discover novel druggable targets.

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Pathophysiology of migraine.

Daniela Pietrobon, Michael A. Moskowitz (2013)

Migraine is a collection of perplexing neurological conditions in which the brain and its associated tissues have been implicated as major players during an attack. Once considered exclusively a disorder of blood vessels, compelling evidence has led to the realization that migraine represents a highly choreographed interaction between major inputs from both the peripheral and central nervous systems, with the trigeminovascular system and the cerebral cortex among the main players. Advances in in vivo and in vitro technologies have informed us about the significance to migraine of events such as cortical spreading depression and activation of the trigeminovascular system and its constituent neuropeptides, as well as about the importance of neuronal and glial ion channels and transporters that contribute to the putative cortical excitatory/inhibitory imbalance that renders migraineurs susceptible to an attack. This review focuses on emerging concepts that drive the science of migraine in both a mechanistic direction and a therapeutic direction.

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Osteopetrosis: genetics, treatment and new insights into osteoclast function.

Cristina Sobacchi, Ansgar Schulz, Fraser Coxon … (2013)

Osteopetrosis is a genetic condition of increased bone mass, which is caused by defects in osteoclast formation and function. Both autosomal recessive and autosomal dominant forms exist, but this Review focuses on autosomal recessive osteopetrosis (ARO), also known as malignant infantile osteopetrosis. The genetic basis of this disease is now largely uncovered: mutations in TCIRG1, CLCN7, OSTM1, SNX10 and PLEKHM1 lead to osteoclast-rich ARO (in which osteoclasts are abundant but have severely impaired resorptive function), whereas mutations in TNFSF11 and TNFRSF11A lead to osteoclast-poor ARO. In osteoclast-rich ARO, impaired endosomal and lysosomal vesicle trafficking results in defective osteoclast ruffled-border formation and, hence, the inability to resorb bone and mineralized cartilage. ARO presents soon after birth and can be fatal if left untreated. However, the disease is heterogeneous in clinical presentation and often misdiagnosed. This article describes the genetics of ARO and discusses the diagnostic role of next-generation sequencing methods. The management of affected patients, including guidelines for the indication of haematopoietic stem cell transplantation (which can provide a cure for many types of ARO), are outlined. Finally, novel treatments, including preclinical data on in utero stem cell treatment, RANKL replacement therapy and denosumab therapy for hypercalcaemia are also discussed.

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Gain-of-function Nav1.8 mutations in painful neuropathy.

Catharina G Faber, Giuseppe Lauria, Ingemar Merkies … (2012)

Painful peripheral neuropathy often occurs without apparent underlying cause. Gain-of-function variants of sodium channel Na(v)1.7 have recently been found in ∼30% of cases of idiopathic painful small-fiber neuropathy. Here, we describe mutations in Na(v)1.8, another sodium channel that is specifically expressed in dorsal root ganglion (DRG) neurons and peripheral nerve axons, in patients with painful neuropathy. Seven Na(v)1.8 mutations were identified in 9 subjects within a series of 104 patients with painful predominantly small-fiber neuropathy. Three mutations met criteria for potential pathogenicity based on predictive algorithms and were assessed by voltage and current clamp. Functional profiling showed that two of these three Na(v)1.8 mutations enhance the channel's response to depolarization and produce hyperexcitability in DRG neurons. These observations suggest that mutations of Na(v)1.8 contribute to painful peripheral neuropathy.

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Author and article information

Contributors

Paola Imbrici: URI : http://loop.frontiersin.org/people/72516/overview

Antonella Liantonio: URI : http://loop.frontiersin.org/people/21119/overview

Michela De Bellis: URI : http://loop.frontiersin.org/people/251137/overview

Sabata Pierno: URI : http://loop.frontiersin.org/people/251115/overview

Journal

Journal ID (nlm-ta): Front Pharmacol

Journal ID (iso-abbrev): Front Pharmacol

Journal ID (publisher-id): Front. Pharmacol.

Title: Frontiers in Pharmacology

Publisher: Frontiers Media S.A.

ISSN (Electronic): 1663-9812

Publication date (Electronic): 10 May 2016

Publication date Collection: 2016

Volume: 7

Electronic Location Identifier: 121

Affiliations

[1] ¹Department of Pharmacy – Drug Sciences, University of Bari “Aldo Moro” Bari, Italy

[2] ²Department of Basic Medical Sciences, Neurosciences and Sense Organs, University of Bari “Aldo Moro” Bari, Italy

[3] ³Department of Biomedical Sciences and Human Oncology, University of Bari “Aldo Moro” Bari, Italy

Author notes

Edited by: Maria Cristina D’Adamo, University of Perugia, Italy

Reviewed by: Mirko Baruscotti, University of Milano, Italy; Adrien Moreau, Institut Neuromyogene – École Normale Supérieure de Lyon, France

*Correspondence: Paola Imbrici, paola.imbrici@ 123456uniba.it

This article was submitted to Pharmacology of Ion Channels and Channelopathies, a section of the journal Frontiers in Pharmacology

Article

DOI: 10.3389/fphar.2016.00121

PMC ID: 4861771

PubMed ID: 27242528

SO-VID: a04f5946-536c-485d-bb1a-4a245be28342

License:

This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

History

Date received : 27 February 2016

Date accepted : 25 April 2016

Page count

Figures: 4, Tables: 6, Equations: 0, References: 285, Pages: 28, Words: 0

Funding

Funded by: Fondazione Telethon 10.13039/501100002426

Award ID: GGP14096

Funded by: AFM-Téléthon 10.13039/501100004923

Award ID: 19027

Funded by: Ministero della Salute 10.13039/501100003196

Award ID: GR-2009-1580433

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Most cited references 235

Pathophysiology of migraine.

Osteopetrosis: genetics, treatment and new insights into osteoclast function.

Gain-of-function Nav1.8 mutations in painful neuropathy.

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