1994
DOI: 10.1620/tjem.172.355
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Impaired Biliary Excretion of Copper and Lysosomal Enzymes in Long-Evans Cinnamon Rat.

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Cited by 5 publications
(3 citation statements)
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“…Although the cytosolic copper has been discussed to be the reactive species [39], our finding that in LEC rats virtually all cytosolic copper is bound to MT supports the findings by others [40] that cytosolic copper is not directly toxic. There is increasing evidence [25,41] that the toxic form of copper is located in the lysosomes. According to earlier results, this copper is considered to be loosely associated to insoluble polymers of oxidized MT and MT-degradation products and therefore is redox reactive [24,25].…”
Section: Discussionmentioning
confidence: 99%
“…Although the cytosolic copper has been discussed to be the reactive species [39], our finding that in LEC rats virtually all cytosolic copper is bound to MT supports the findings by others [40] that cytosolic copper is not directly toxic. There is increasing evidence [25,41] that the toxic form of copper is located in the lysosomes. According to earlier results, this copper is considered to be loosely associated to insoluble polymers of oxidized MT and MT-degradation products and therefore is redox reactive [24,25].…”
Section: Discussionmentioning
confidence: 99%
“…Interestingly, in hepatocytes exposed to elevated copper levels, one of the copper transporters, Atp7b, moves from the Golgi to lysosomes and imports metal into their lumen [ 52 ]. Moreover, in vivo models of copper overload demonstrated that increased copper loading in the liver leads to increased activity of lysosomal enzymes and reduces their structural integrity [ 53 ]. These data allow us to speculate that in macrophages, copper treatment and the disruption of lysosomal function may exert somewhat similar effects, affecting the stability of Fpn in an iron-independent manner.…”
Section: Discussionmentioning
confidence: 99%
“…ATP7B (WND) expression is highest in liver tissue, with lower expression patterns in the brain and kidney (Bull et al 1993;Tanzi et al 1993;Yamaguchi et al 1994). ATP7A (MNK) expression is observed in most extra-hepatic adult tissues, with high expression in the intestinal mucosa, kidney and neuronal cells (Abe et al 1994;Monty et al 2005). Recent evidence has changed our understanding of expression patterns and the interplay of MNK and WND expressed in the same cells (Linz and Lutsenko 2007).…”
Section: A) Lessons From Co-expressing Cu-atpasesmentioning
confidence: 99%