TRPM4 Expression during postnatal developmental of mouse CA1 pyramidal neurons
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Riquelme, Denise
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TRPM4 Expression during postnatal developmental of mouse CA1 pyramidal neurons
Abstract
TRPM4 is a non-selective cation channel activated by intracellular calcium and
permeable to monovalent cations. This channel participates in the control of neuronal
firing, neuronal plasticity, and neuronal death. TRPM4 depolarizes dendritic spines and
is critical for the induction of NMDA receptor-dependent long-term potentiation in CA1
pyramidal neurons. Despite its functional importance, no subcellular localization or
expression during postnatal development has been described in this area. To examine
the localization and expression of TRPM4, we performed duplex immunofluorescence
and patch-clamp in brain slices at different postnatal ages in C57BL/6J mice. At P0
we found TRPM4 is expressed with a somatic pattern. At P7, P14, and P35, TRPM4
expression extended from the soma to the apical dendrites but was excluded from
the axon initial segment. Patch-clamp recordings showed a TRPM4-like current active
at the resting membrane potential from P0, which increased throughout the postnatal
development. This current was dependent on intracellular Ca2C (ICAN) and sensitive to 9-
phenanthrol (9-Ph). Inhibiting TRPM4 with 9-Ph hyperpolarized the membrane potential
at P14 and P35, with no effect in earlier stages. Together, these results show that TRPM4
is expressed in CA1 pyramidal neurons in the soma and apical dendrites and associated
with a TRPM4-like current, which depolarizes the neurons. The expression, localization,
and function of TRPM4 throughout postnatal development in the CA1 hippocampal
may underlie an important mechanism of control of membrane potential and action
potential firing during critical periods of neuronal development, particularly during the
establishment of circuits.
Patrocinador
Pontificia Universidad Catolica de Chile animal facility PIA-CONICYT ECM-07
Programa de Equipamiento Cientifico y Tecnologico (FONDEQUIP) EQM150069
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Artículo de publícación WoS Artículo de publicación SCOPUS
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Frontiers in Neuroanatomy April 2021 Volume 15 Article 643287
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