2012
DOI: 10.1523/jneurosci.6153-11.2012
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Toxic Role of K+Channel Oxidation in Mammalian Brain

Abstract: Potassium (K ϩ ) channels are essential to neuronal signaling and survival. Here we show that these proteins are targets of reactive oxygen species in mammalian brain and that their oxidation contributes to neuropathy. Thus, the KCNB1 (Kv2.1) channel, which is abundantly expressed in cortex and hippocampus, formed oligomers upon exposure to oxidizing agents. These oligomers were ϳ10-fold more abundant in the brain of old than young mice. Oxidant-induced oligomerization of wild-type KCNB1 enhanced apoptosis in … Show more

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Cited by 70 publications
(109 citation statements)
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“…We previously proposed that the lost GFP phenotype reflects neuronal apoptosis (Cotella et al 2012;Duan and Sesti 2013). Here, we sought to corroborate this notion by genetic and pharmacological evidence.…”
Section: Resultsmentioning
confidence: 79%
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“…We previously proposed that the lost GFP phenotype reflects neuronal apoptosis (Cotella et al 2012;Duan and Sesti 2013). Here, we sought to corroborate this notion by genetic and pharmacological evidence.…”
Section: Resultsmentioning
confidence: 79%
“…For these studies, we employed the FDX25 worm that expresses human Ab 42 -a potent neurodegenerative factor (Mattson 2004)-in ASE sensory neurons (Cotella et al 2012). In addition, we labeled the right ASE neuron (ASER) with a specific GFP reporter (P gcy-5 ::GFP) (Yu et al 1997).…”
Section: Resultsmentioning
confidence: 99%
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“…With our protocols we study the effects of human Aβ 42 oligomer on neuronal function 8 . A fragment encoding human Aβ 42 and the artificial signal peptide coding sequence of Fire vector pPD50.52 was amplified from construct PCL12 9 using primers that introduced a Sma 1 restriction endonuclease site at the ends.…”
Section: Representative Resultsmentioning
confidence: 99%
“…The fragment was then inserted into a construct containing a 2,481-bp flp-6 promoter sequence in the pPD95.75 Fire vector between the unique Sma 1 site 10 . Using the transformation techniques described in protocol 1 we constructed a transgenic worm expressing Aβ 42 in the ASE neurons (FDX(ses25) strain) 8 . To mark positive transformants we used the P gcy-5 ::GFP reporter which specifically drives GFP expression in the ASE right (ASER) neuron 11 .…”
Section: Representative Resultsmentioning
confidence: 99%