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      Potent neuroprotection after stroke afforded by a double-knot spider-venom peptide that inhibits acid-sensing ion channel 1a

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          Significance

          Six million people die each year from stroke, and 5 million survivors are left with a permanent disability. Moreover, the neuronal damage caused by stroke often triggers a progressive decline in cognitive function that doubles the risk of dementia for stroke survivors. Despite this massive global disease burden, there are no approved drugs for treating the neuronal injury caused to the brain by the oxygen deprivation occurring during an ischemic stroke. The precipitous drop in brain pH resulting from stroke activates acid-sensing ion channel 1a. We show that inhibition of these channels using a “double-knot” spider venom peptide massively attenuates brain damage after stroke and improves behavioral outcomes, even when the peptide is administered 8 h after stroke onset.

          Abstract

          Stroke is the second-leading cause of death worldwide, yet there are no drugs available to protect the brain from stroke-induced neuronal injury. Acid-sensing ion channel 1a (ASIC1a) is the primary acid sensor in mammalian brain and a key mediator of acidosis-induced neuronal damage following cerebral ischemia. Genetic ablation and selective pharmacologic inhibition of ASIC1a reduces neuronal death following ischemic stroke in rodents. Here, we demonstrate that Hi1a, a disulfide-rich spider venom peptide, is highly neuroprotective in a focal model of ischemic stroke. Nuclear magnetic resonance structural studies reveal that Hi1a comprises two homologous inhibitor cystine knot domains separated by a short, structurally well-defined linker. In contrast with known ASIC1a inhibitors, Hi1a incompletely inhibits ASIC1a activation in a pH-independent and slowly reversible manner. Whole-cell, macropatch, and single-channel electrophysiological recordings indicate that Hi1a binds to and stabilizes the closed state of the channel, thereby impeding the transition into a conducting state. Intracerebroventricular administration to rats of a single small dose of Hi1a (2 ng/kg) up to 8 h after stroke induction by occlusion of the middle cerebral artery markedly reduced infarct size, and this correlated with improved neurological and motor function, as well as with preservation of neuronal architecture. Thus, Hi1a is a powerful pharmacological tool for probing the role of ASIC1a in acid-mediated neuronal injury and various neurological disorders, and a promising lead for the development of therapeutics to protect the brain from ischemic injury.

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          Automated NMR structure calculation with CYANA.

          Peter Güntert (2004)
          This chapter gives an introduction to automated nuclear magnetic resonance (NMR) structure calculation with the program CYANA. Given a sufficiently complete list of assigned chemical shifts and one or several lists of cross-peak positions and columns from two-, three-, or four-dimensional nuclear Overhauser effect spectroscopy (NOESY) spectra, the assignment of the NOESY cross-peaks and the three-dimensional structure of the protein in solution can be calculated automatically with CYANA.
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            Pathophysiology, treatment, and animal and cellular models of human ischemic stroke

            Trent Woodruff, John Thundyil, Sung-Chun Tang (2011)
            Stroke is the world's second leading cause of mortality, with a high incidence of severe morbidity in surviving victims. There are currently relatively few treatment options available to minimize tissue death following a stroke. As such, there is a pressing need to explore, at a molecular, cellular, tissue, and whole body level, the mechanisms leading to damage and death of CNS tissue following an ischemic brain event. This review explores the etiology and pathogenesis of ischemic stroke, and provides a general model of such. The pathophysiology of cerebral ischemic injury is explained, and experimental animal models of global and focal ischemic stroke, and in vitro cellular stroke models, are described in detail along with experimental strategies to analyze the injuries. In particular, the technical aspects of these stroke models are assessed and critically evaluated, along with detailed descriptions of the current best-practice murine models of ischemic stroke. Finally, we review preclinical studies using different strategies in experimental models, followed by an evaluation of results of recent, and failed attempts of neuroprotection in human clinical trials. We also explore new and emerging approaches for the prevention and treatment of stroke. In this regard, we note that single-target drug therapies for stroke therapy, have thus far universally failed in clinical trials. The need to investigate new targets for stroke treatments, which have pleiotropic therapeutic effects in the brain, is explored as an alternate strategy, and some such possible targets are elaborated. Developing therapeutic treatments for ischemic stroke is an intrinsically difficult endeavour. The heterogeneity of the causes, the anatomical complexity of the brain, and the practicalities of the victim receiving both timely and effective treatment, conspire against developing effective drug therapies. This should in no way be a disincentive to research, but instead, a clarion call to intensify efforts to ameliorate suffering and death from this common health catastrophe. This review aims to summarize both the present experimental and clinical state-of-the art, and to guide future research directions.
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              A bivalent tarantula toxin activates the capsaicin receptor, TRPV1, by targeting the outer pore domain.

              Christopher Bohlen, Avi Priel, Sharleen Zhou (2010)
              Toxins have evolved to target regions of membrane ion channels that underlie ligand binding, gating, or ion permeation, and have thus served as invaluable tools for probing channel structure and function. Here, we describe a peptide toxin from the Earth Tiger tarantula that selectively and irreversibly activates the capsaicin- and heat-sensitive channel, TRPV1. This high-avidity interaction derives from a unique tandem repeat structure of the toxin that endows it with an antibody-like bivalency. The "double-knot" toxin traps TRPV1 in the open state by interacting with residues in the presumptive pore-forming region of the channel, highlighting the importance of conformational changes in the outer pore region of TRP channels during activation. Copyright 2010 Elsevier Inc. All rights reserved.
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                Author and article information

                Journal
                Journal ID (nlm-ta): Proc Natl Acad Sci U S A
                Journal ID (iso-abbrev): Proc. Natl. Acad. Sci. U.S.A
                Journal ID (hwp): pnas
                Journal ID (pmc): pnas
                Journal ID (publisher-id): PNAS
                Title: Proceedings of the National Academy of Sciences of the United States of America
                Publisher: National Academy of Sciences
                ISSN (Print): 0027-8424
                ISSN (Electronic): 1091-6490
                Publication date (Print): 4 April 2017
                Publication date (Electronic): 20 March 2017
                Volume: 114
                Issue: 14
                Pages: 3750-3755
                Affiliations
                [1] aInstitute for Molecular Bioscience, The University of Queensland , St. Lucia, QLD 4072, Australia;
                [2] bBiomedicine Discovery Institute, Monash University , Clayton, VIC 3800, Australia;
                [3] cDepartment of Pharmacology, Monash University , Clayton, VIC 3800, Australia;
                [4] dQueensland Brain Institute, The University of Queensland , St. Lucia, QLD 4072, Australia;
                [5] eCentre for Advanced Imaging, The University of Queensland , St. Lucia, QLD 4072, Australia;
                [6] fSchool of Biomedical Sciences, The University of Queensland , St. Lucia, QLD 4072, Australia
                Author notes
                1To whom correspondence may be addressed. Email: l.rash@ 123456uq.edu.au or glenn.king@ 123456imb.uq.edu.au .

                Edited by Solomon H. Snyder, Johns Hopkins University School of Medicine, Baltimore, MD, and approved February 6, 2017 (received for review September 1, 2016)

                Author contributions: I.R.C., C.A.M., A.K., J.W.L., R.E.W., L.D.R., and G.F.K. designed research; I.R.C., C.A.M., Y.K.-Y.C., S.S.P., A.K., M.M., V.P., T.M.D.S., L.D.R., and G.F.K. performed research; I.R.C., C.A.M., Y.K.-Y.C., S.S.P., A.K., J.W.L., R.E.W., L.D.R., and G.F.K. analyzed data; and I.R.C., C.A.M., R.E.W., L.D.R., and G.F.K. wrote the paper.

                Author information
                http://orcid.org/0000-0003-2846-052X
                http://orcid.org/0000-0002-2308-2200
                Article
                Accession ID: PMC5389327 Pmcid ID: PMC5389327 Pmc-uid ID: 5389327 Publisher ID: 201614728
                DOI: 10.1073/pnas.1614728114
                PMC ID: 5389327
                PubMed ID: 28320941
                SO-VID: 8d11d8bc-c78e-48a9-8730-d9da5c4067fb
                History
                Page count
                Pages: 6
                Funding
                Funded by: Department of Health, Australian Government | National Health and Medical Research Council (NHMRC) 501100000925
                Award ID: APP1063798
                Categories
                Subject: Biological Sciences
                Subject: Pharmacology

                Keywords: acid-sensing ion channel 1a,stroke,venom peptide,neuroprotection,ischemia
                Data availability:
                Keywords: acid-sensing ion channel 1a, stroke, venom peptide, neuroprotection, ischemia

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