Control óptico de ensambles neuronales patológicos en un modelo de la enfermedad de parkinson

Zamora Ursulo, Miguel Ángel

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dc.contributor	NADIA SADERI;257613	es_MX
dc.contributor.advisor	Saderi, Nadia	es_MX
dc.contributor.advisor	Carrillo Reid, Luis	es_MX
dc.contributor.advisor	Castillo Martin del Campo, Claudia	es_MX
dc.contributor.advisor	Salgado Delgado, Roberto Carlos	es_MX
dc.contributor.advisor	Ibáñez Sandoval, Osvaldo	es_MX
dc.contributor.advisor	Téllez Lima, Luis	es_MX
dc.contributor.author	Zamora Ursulo, Miguel Ángel	es_MX
dc.coverage.spatial	México. San Luis Potosí. San Luis Potosí	es_MX
dc.creator	MIGUEL ANGEL ZAMORA URSULO;770504	es_MX
dc.date.accessioned	2024-03-05T17:30:02Z
dc.date.available	2024-03-05T17:30:02Z
dc.date.issued	2024-02
dc.identifier.uri	https://repositorioinstitucional.uaslp.mx/xmlui/handle/i/8563
dc.identifier.uri	https://doi.org/10.1371/journal.pone.0290317	es_MX
dc.description.abstract	Motor deficits observed in Parkinson’s disease (PD) are caused by the loss of dopaminergic neurons and the subsequent dopamine depletion in different brain areas. The most common therapy to treat motor symptoms for patients with this disorder is the systemic intake of L- DOPA that increases dopamine levels in all the brain, making it difficult to discern the main locus of dopaminergic action in the alleviation of motor control. Caged compounds are molecules with the ability to release neuromodulators locally in temporary controlled conditions using light. In the present study, we measured the turning behavior of unilateral dopamine depleted mice before and after dopamine uncaging. The optical delivery of dopamine in the striatum of lesioned mice produced contralateral turning behavior that resembled, to a lesser extent, the contralateral turning behavior evoked by a systemic injection of apomorphine. Contralateral turning behavior induced by dopamine uncaging was temporarily tied to the transient elevation of dopamine concentration and was reversed when dopamine decreased to pathological levels. Remarkably, contralateral turning behavior was tuned by changing the power and frequency of light stimulation, opening the possibility to modulate dopamine fluctuations using different light stimulation protocols. Moreover, striatal dopamine uncaging recapitulated the motor effects of a low concentration of systemic L-DOPA, but with better temporal control of dopamine levels. Finally, dopamine uncaging reduced the pathological synchronization of striatal neuronal ensembles that characterize unilateral dopamine- depleted mice. We conclude that optical delivery of dopamine in the striatum resembles the motor effects induced by systemic injection of dopaminergic agonists in unilateral dopamine-depleted mice. Future experiments using this approach could help to elucidate the role of dopamine in different brain nuclei in normal and pathological conditions.	es_MX
dc.description.statementofresponsibility	Investigadores	es_MX
dc.description.statementofresponsibility	Estudiantes	es_MX
dc.language	Inglés	es_MX
dc.publisher	Facultad de Medicina	es_MX
dc.relation.ispartof	REPOSITORIO NACIONAL CONACYT	es_MX
dc.rights	Acceso Abierto	es_MX
dc.rights.uri	http://creativecommons.org/licenses/by-nc-sa/4.0	es_MX
dc.subject	Parkinson´s disease	es_MX
dc.subject	Caged compound	es_MX
dc.subject	Movement disorders	es_MX
dc.subject	Dopamine	es_MX
dc.subject	optical stimulation	es_MX
dc.subject	Enfermedad de parkinson (bvs)	es_MX
dc.subject	Dopamina (bvs)	es_MX
dc.subject.other	MEDICINA Y CIENCIAS DE LA SALUD	es_MX
dc.title	Control óptico de ensambles neuronales patológicos en un modelo de la enfermedad de parkinson	es_MX
dc.title.alternative	Reversal of pathological motor behavior in a model of Parkinson’s disease by striatal dopamine uncaging	es_MX
dc.type	Tesis de doctorado	es_MX
dc.degree.name	Doctorado en Ciencias Biomédicas Básicas	es_MX
dc.degree.department	Facultad de Medicina	es_MX