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Selective dendritic susceptibility to bioenergetic, excitotoxic and redox perturbations in cortical neurons

Author: Abramov
Al-Mubarak
Andrabi
Ankarcrona
Arundine
Bading
Baughman
Bell
Bell
Bell
Bell
Bonfoco
Brennan
Camacho
Chen
Choi
Choi
Choi
Choi
Csordas
Dawson
De Stefani
Dickstein
Do
Dryanovski
Duan
Duchen
Duchen
Fan
Frustaci
Gawryluk
Gellerich
Ghanizadeh
Giles E. Hardingham
Glancy
Gomez-Isla
Greenwood
Greenwood
Grima
Gupta
Gupta
Gupta
Gutscher
Gysin
Hall
Halliwell
Hardingham
Hardingham
Hardingham
Hardingham
Harris
Hung
Imamura
Ittner
Jing Qiu
Johnson
Johri
Kalia
Keelan
Khatri
Kulak
Lau
Lipton
Lipton
Llorente-Folch
Lucas
Luebke
Mairet-Coello
Mao
Martel
Matsuzawa
Mehta
Melo
Milnerwood
Mizielinska
Nakamura
Nicholls
Nicholls
Okamoto
Olney
Papadia
Parsons
Philip Hasel
Puddifoot
Qiu
Rardin
Rocher
Sean Mckay
Siskova
Soriano
Spires
Wahl
Wyllie
Yu
Zundorf
Publication venue: 'Elsevier BV'
Publication date: 01/09/2015
Field of study

AbstractNeurodegenerative and neurological disorders are often characterised by pathological changes to dendrites, in advance of neuronal death. Oxidative stress, energy deficits and excitotoxicity are implicated in many such disorders, suggesting a potential vulnerability of dendrites to these situations. Here we have studied dendritic vs. somatic responses of primary cortical neurons to these types of challenges in real-time.Using a genetically encoded indicator of intracellular redox potential (Grx1-roGFP2) we found that, compared to the soma, dendritic regions exhibited more dramatic fluctuations in redox potential in response to sub-lethal ROS exposure, and existed in a basally more oxidised state. We also studied the responses of dendritic and somatic regions to excitotoxic NMDA receptor activity. Both dendritic and somatic regions experienced similar increases in cytoplasmic Ca2+. Interestingly, while mitochondrial Ca2+ uptake and initial mitochondrial depolarisation were similar in both regions, secondary delayed mitochondrial depolarisation was far weaker in dendrites, potentially as a result of less NADH depletion. Despite this, ATP levels were found to fall faster in dendritic regions. Finally we studied the responses of dendritic and somatic regions to energetically demanding action potential burst activity. Burst activity triggered PDH dephosphorylation, increases in oxygen consumption and cellular NADH:NAD ratio. Compared to somatic regions, dendritic regions exhibited a smaller degree of mitochondrial Ca2+ uptake, lower fold-induction of NADH and larger reduction in ATP levels. Collectively, these data reveal that dendritic regions of primary neurons are vulnerable to greater energetic and redox fluctuations than the cell body, which may contribute to disease-associated dendritic damage. This article is part of a Special Issue entitled: 13th European Symposium on Calcium

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