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dc.creatorBenítez-King, Gloria
dc.creatorDomínguez-Alonso, Aline
dc.creatorRamírez-Rodríguez, Gerardo
dc.date.accessioned2017-06-30T03:42:28Z
dc.date.available2017-06-30T03:42:28Z
dc.date.issued2010es_ES
dc.identifier2143es_ES
dc.identifier.urihttp://repositorio.inprf.gob.mx/handle/123456789/6798
dc.identifier.urihttp://doi.org/ 10.2174/1876528901003010105es_ES
dc.identifier.urihttps://benthamopen.com/ABSTRACT/TONEUROEJ-3-105es_ES
dc.description.abstractNeurons have a highly asymmetric shape and they are constituted by two functional domains: the axonal, and the somatodendritic domains. Axons are cellular processes that make contact with target cells to transmit information, while dendrites located in the somatodendritic domain are specialized in the reception of information. During neurodevelopment, neurons acquire the highly morphofunctional polarization through a dynamic cytoskeletal organization. Melatonin, the main indolamine secreted by the pineal gland has two important properties which play a key role in the maintaining of neuron polarization: it is a potent free radical scavenger, and it is a cytoskeletal modulator. Melatonin stimulates cytoskeletal polarization through PKC and ROCK activation by recruiting cells at early stages of neurodevelopment for later differentiation. At later stages, melatonin induces neurite and microtubule enlargement by a calmodulin antagonism. Moreover, melatonin prevents the asymmetric shape lost induced by oxidative stress, a condition present in neuropsychiatric diseases, and abolishes the cytoskeletal damage caused by prolonged treatment with antipsychotics, restoring the morphofunctional polarization. Moreover, in organotypic cultures, melatonin at nanomolar concentrations enhances the number of dendrites and their complexity in hilar neurons of the hippocampus. In addition, melatonin stimulates the formation of new neurons in vitro and in a rodent model. In this review we will describe current evidences indicative of the melatonin participation in the neuronal morphofunctional differentiation as a cytoskeletal modulator. Also we will discuss the implications of the loss of neuronal polarization in neuropsychiatric diseases and the potential therapeutic utility of melatonin for the treatment of these illnesses.es_ES
dc.language.isoenges_ES
dc.relation3, 105-111 p.es_ES
dc.relationversión del editores_ES
dc.rightsacceso cerradoes_ES
dc.titleNeurocytoskeletal Protective Effect of Melatonin: Importance for Morphofunctional Neuronal Polarizationes_ES
dc.typearticlees_ES
dc.contributor.affiliationInstituto Nacional de Psiquiatría Ramón de la Fuente Muñiz, Calz, México-Xochimilco 101, Col. Sn Lorenzo Huipulco 14370, México, D.F., Mexicoes_ES
dc.contributor.emailbekin@imp.edu.mxes_ES
dc.relation.jnabreviadoOPEN NEUROENDOCRINOL Jes_ES
dc.relation.journalThe Open neuroendocrinology journales_ES
dc.identifier.placeOak Park, ILes_ES
dc.date.published2010es_ES
dc.identifier.organizacionInstituto Nacional de Psiquiatría Ramón de la Fuente Muñiz, México.es_ES
dc.identifier.eissn1876-5289es_ES
dc.subject.kwCitoskeletales_ES
dc.subject.kwNeuritases_ES
dc.subject.kwNeurodesarrolloes_ES
dc.subject.kwDoublecortines_ES
dc.subject.kwMelatoninaes_ES
dc.subject.koCitoskeletales_ES
dc.subject.koNeuriteses_ES
dc.subject.koGrowth coneses_ES
dc.subject.koNeurodevelopmentes_ES
dc.subject.koDoublecortines_ES
dc.subject.koMelatonines_ES


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