作者
Kurt J De Vos, Anna L Chapman, Maria E Tennant, Catherine Manser, Elizabeth L Tudor, Kwok-Fai Lau, Janet Brownlees, Steven Ackerley, Pamela J Shaw, Declan M McLoughlin, Christopher E Shaw, P Nigel Leigh, Christopher CJ Miller, Andrew J Grierson
发表日期
2007/11/15
期刊
Human molecular genetics
卷号
16
期号
22
页码范围
2720-2728
出版商
Oxford University Press
简介
Amyotrophic lateral sclerosis (ALS) is a late-onset neurological disorder characterized by death of motoneurons. Mutations in Cu/Zn superoxide dismutase-1 (SOD1) cause familial ALS but the mechanisms whereby they induce disease are not fully understood. Here, we use time-lapse microscopy to monitor for the first time the effect of mutant SOD1 on fast axonal transport (FAT) of bona fide cargoes in living neurons. We analyzed FAT of mitochondria that are a known target for damage by mutant SOD1 and also of membrane-bound organelles (MBOs) using EGFP-tagged amyloid precursor protein as a marker. We studied FAT in motor neurons derived from SOD1G93A transgenic mice that are a model of ALS and also in cortical neurons transfected with SOD1G93A and three further ALS-associated SOD1 mutants. We find that mutant SOD1 damages transport of both mitochondria and MBOs, and that the …
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KJ De Vos, AL Chapman, ME Tennant, C Manser… - Human molecular genetics, 2007