Sp1-regulated expression of p11 contributes to motor neuron degeneration by membrane insertion of TASK1.

Garcia-Morales, Victoria; Rodriguez-Bey, Guillermo; Gomez-Perez, Laura; Dominguez-Vias, German; Gonzalez-Forero, David; Portillo, Federico; Campos-Caro, Antonio; Gento-Caro, Angela; Issaoui, Noura; Soler, Rosa M; Garcera, Ana; Moreno-Lopez, Bernardo

Publication:
Sp1-regulated expression of p11 contributes to motor neuron degeneration by membrane insertion of TASK1.

dc.contributor.author	Garcia-Morales, Victoria
dc.contributor.author	Rodriguez-Bey, Guillermo
dc.contributor.author	Gomez-Perez, Laura
dc.contributor.author	Dominguez-Vias, German
dc.contributor.author	Gonzalez-Forero, David
dc.contributor.author	Portillo, Federico
dc.contributor.author	Campos-Caro, Antonio
dc.contributor.author	Gento-Caro, Angela
dc.contributor.author	Issaoui, Noura
dc.contributor.author	Soler, Rosa M
dc.contributor.author	Garcera, Ana
dc.contributor.author	Moreno-Lopez, Bernardo
dc.contributor.funder	MICINN/FEDER
dc.contributor.funder	MICINN
dc.contributor.funder	MINECO/FEDER
dc.contributor.funder	Junta de Andalucía, Spain
dc.date.accessioned	2023-01-25T13:39:52Z
dc.date.available	2023-01-25T13:39:52Z
dc.date.issued	2019-07-25
dc.description.abstract	Disruption in membrane excitability contributes to malfunction and differential vulnerability of specific neuronal subpopulations in a number of neurological diseases. The adaptor protein p11, and background potassium channel TASK1, have overlapping distributions in the CNS. Here, we report that the transcription factor Sp1 controls p11 expression, which impacts on excitability by hampering functional expression of TASK1. In the SOD1-G93A mouse model of ALS, Sp1-p11-TASK1 dysregulation contributes to increased excitability and vulnerability of motor neurons. Interference with either Sp1 or p11 is neuroprotective, delaying neuron loss and prolonging lifespan in this model. Nitrosative stress, a potential factor in human neurodegeneration, stimulated Sp1 expression and human p11 promoter activity, at least in part, through a Sp1-binding site. Disruption of Sp1 or p11 also has neuroprotective effects in a traumatic model of motor neuron degeneration. Together our work suggests the Sp1-p11-TASK1 pathway is a potential target for treatment of degeneration of motor neurons.
dc.description.sponsorship	Funding grants: SAF2008-01415 (MICINN/FEDER), SAF2011-23633 (MICINN), BFU2015-71422-R (MINECO/FEDER), PI14/00060 (ISCIII/FEDER) from Spain’s Government, as well as P07-CTS-02606, P09-CTS-5445, and P11-CTS-7281 (CICE/FEDER) from Junta de Andalucía, Spain. We thank Dr. Douglas A. Bayliss (University of Virginia, USA) for kindly providing the knock-out mice, Drs. Carmen Castro (University of Cadiz, Spain) and Sergey Kasparov (University of Bristol, UK) for supervision on the initial western blotting experiments and on viral constructions and production, respectively, and Ms. Lucia Molanes, Ms. Eugenia Gomez and Mr. Antonio Torres for their skillful technical assistance. We thank Elaine Lilly, Ph.D. (Writer's First Aid), for English language revision.
dc.description.version	Si
dc.identifier.citation	García-Morales V, Rodríguez-Bey G, Gómez-Pérez L, Domínguez-Vías G, González-Forero D, Portillo F, et al. Sp1-regulated expression of p11 contributes to motor neuron degeneration by membrane insertion of TASK1. Nat Commun. 2019 Aug 22;10(1):3784.
dc.identifier.doi	10.1038/s41467-019-11637-4
dc.identifier.essn	2041-1723
dc.identifier.pmc	PMC6706379
dc.identifier.pmid	31439839
dc.identifier.pubmedURL	https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6706379/pdf
dc.identifier.unpaywallURL	https://www.nature.com/articles/s41467-019-11637-4.pdf
dc.identifier.uri	http://hdl.handle.net/10668/14432
dc.issue.number	1
dc.journal.title	Nature communications
dc.journal.titleabbreviation	Nat Commun
dc.language.iso	en
dc.organization	Hospital Universitario Puerta del Mar
dc.organization	Instituto de Investigación e Innovación en Ciencias Biomédicas
dc.page.number	23
dc.provenance	Realizada la curación de contenido 06/09/2024
dc.publisher	Nature Publishing Group
dc.pubmedtype	Journal Article
dc.pubmedtype	Research Support, Non-U.S. Gov't
dc.relation.projectID	SAF2008-01415
dc.relation.projectID	SAF2011-23633
dc.relation.projectID	BFU2015-71422-R
dc.relation.projectID	PI14/00060
dc.relation.projectID	P07-CTS-02606
dc.relation.projectID	P09-CTS-5445
dc.relation.projectID	P11-CTS-7281
dc.relation.publisherversion	https://doi.org/10.1038/s41467-019-11637-4
dc.rights	Attribution 4.0 International
dc.rights.accessRights	open access
dc.rights.uri	http://creativecommons.org/licenses/by/4.0/
dc.subject	Amyotrophic lateral sclerosis
dc.subject	Ion channels in the nervous system
dc.subject.decs	Anexina A2
dc.subject.decs	Animales
dc.subject.decs	Cultivo primario de células
dc.subject.decs	Células HEK293
dc.subject.decs	Degeneración nerviosa
dc.subject.decs	Esclerosis amiotrófica lateral
dc.subject.decs	Membrana celular
dc.subject.decs	Médula espinal
dc.subject.decs	Proteínas S100
dc.subject.decs	Proteínas del tejido nervioso
dc.subject.decs	Ratones transgénicos
dc.subject.decs	Regulación de la expresión génica
dc.subject.mesh	Amyotrophic Lateral Sclerosis
dc.subject.mesh	Animals
dc.subject.mesh	Annexin A2
dc.subject.mesh	Cell Membrane
dc.subject.mesh	Disease Models, Animal
dc.subject.mesh	Female
dc.subject.mesh	Gene Expression Regulation
dc.subject.mesh	Gene Knockdown Techniques
dc.subject.mesh	HEK293 Cells
dc.subject.mesh	Humans
dc.subject.mesh	Male
dc.subject.mesh	Membrane Potentials
dc.subject.mesh	Mice
dc.subject.mesh	Mice, Transgenic
dc.subject.mesh	Motor Neurons
dc.subject.mesh	Nerve Degeneration
dc.subject.mesh	Nerve Tissue Proteins
dc.subject.mesh	Potassium Channels, Tandem Pore Domain
dc.subject.mesh	Primary Cell Culture
dc.subject.mesh	Promoter Regions, Genetic
dc.subject.mesh	Rats
dc.subject.mesh	S100 Proteins
dc.subject.mesh	Sp1 Transcription Factor
dc.subject.mesh	Spinal Cord
dc.title	Sp1-regulated expression of p11 contributes to motor neuron degeneration by membrane insertion of TASK1.
dc.type	research article
dc.type.hasVersion	VoR
dc.volume.number	10
dspace.entity.type	Publication