Biochemical Study on the Critical Period for Treatment of the Mottled Brindled Mouse

Fujii, Tatsuya; Ito, Masako; Tsuda, Hideo; Mikawa, Harukí

doi:10.1111/j.1471-4159.1990.tb04574.x

Cited by 26 publications

(11 citation statements)

References 23 publications

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“…The recovery of Cu,Zn-SOD activity after addition of CuSO 4 to Trien-treated cells, together with Cytox rescue, improved cell viability, indicating that impairment of copper-dependent enzymes is a causal factor in the induction of cell death. Indeed, copper supplementation by injection prevents the neurological disturbances present in the Mottled/Brindled mouse [54]. Bcl-2 levels also revert to control ones; the different response of Mn-SOD is probably due to a different turnover of this protein or to an additional specific effect of Trien.…”

Section: Discussionmentioning

confidence: 84%

Prolonged copper depletion induces expression of antioxidants and triggers apoptosis in SH-SY5Y neuroblastoma cells

Lombardo

Ciriolo

Rotilio

et al. 2003

Cellular and Molecular Life Sciences (CMLS)

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SH-SY5Y neuroblastoma cells were cultured for up to three serial passages in the presence of the copper chelator triethylene tetramine (Trien). The copper-depleted neuroblastoma cell line obtained showed decreased activities of the copper enzymes Cu, Zn super-oxide dismutase and cytochrome c oxidase with concomitant increases in reactive oxygen species. Mitochondrial antioxidants (Mn superoxide dismutase and Bcl-2)were up-regulated. Overexpression and activation of p53 were early responses, leading to an increase in p21. Eventually, copper-depleted cells detached from the monolayer and underwent apoptosis. Activation of upstream caspase-9, but not caspase-8, suggested that apoptosis proceeds via a mitochondrial pathway, followed by caspase-3 activation. The addition of copper sulfate to the copper-depleted cells restored copper enzymes, normalized antioxidant levels and improved cell viability. We conclude that prolonged copper starvation in these replicating cells leads to mitochondrial damage and oxidative stress and ultimately, apoptosis.

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Section: Discussionmentioning

confidence: 84%

Prolonged copper depletion induces expression of antioxidants and triggers apoptosis in SH-SY5Y neuroblastoma cells

Lombardo

Ciriolo

Rotilio

et al. 2003

Cellular and Molecular Life Sciences (CMLS)

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“…Fujii et al [11] have recently demonstrated that in creases in the activity of the copper-dependent mitochon drial enzyme, cytochrome c oxidase, are associated with improvement of the neurological symptoms of the mice. Based upon these data, they have argued that cyto chrome c oxidase deficiency is the mechanism whereby neuronal damage occurs.…”

Section: Discussionmentioning

confidence: 99%

“…These injections attenuate the neuronal degener ation of the cerebrum, and make the neuronal mitochon drial changes far less conspicuous [10]. More recently, Fujii et al [11] demonstrated that increases in the activity of the copper-dependent, mitochondrial enzyme cy tochrome c oxidase, specifically, are associated with im provement of the neurological symptoms of the mice, as indicated by fur color, body weight, brain weight and ataxia. They also demonstrated that increases in cy tochrome c oxidase activity occur only if copper treat ment is given before day 12.…”

Section: Introductionmentioning

confidence: 99%

The Female Brindled Mouse as a Model of Menkes' Disease: The Relationship of Fur Pattern to Behavioral and Neurochemical Abnormalities

Martin¹,

Irino²,

Suzuki³

et al. 1991

Dev Neurosci

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The brindled mottled mutant mouse, a model of Menkes'' disease, has alterations in copper homeostasis which cause, among other sequelae, neuronal degeneration in selected areas of brain. This work examined the neurochemical changes at postnatal days (PND) 15, 30 and 60 in females heterozygous for the sex-linked brindled mutation. These data were compared to behavioral alterations and to fur coat color at these same time points. The brindled heterozygotic females had lower concentrations of norepinephrine (NE) in the cingulate cortex, and higher levels of dopamine or dopamine metabolites in the cingulate cortex, thalamus and hypothalamus across all ages, although the difference was greatest at PND 15. The brindled females were much less active than their normal littermates at PND 15, but the differences were no longer evident at PND 30 and 60. Mottling of the fur is believed to result from low tyrosinase activity caused by abnormalities in copper metabolism. The fur pattern and behavior of the brindled mice were highly correlated with NE levels in the cingulate cortex and thalamus. These data show that female brindled mice have neurochemical abnormalities similar to (if less severe than) the male hemizygotes, that these abnormalities are regionally specific, are most apparent prior to 30 days of age, and are linked to behavioral deficits. These data also show that the extent of such deficits can be predicted by a quantitative analysis of the fur pattern of these females.

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“…[47][48][49][50] When Mo br is treated with copper injections within the first week of postnatal period the mice survive and do not develop neurological symptoms. 51 Furthermore, transgenic expression of human ATP7A in Mo br could correct the phenotype even though copper defect was not completely corrected. 52 The mottled blotchy (Mo blo ) phenotype resembles OHS by showing predominantly connective tissue manifestations.…”

Section: Animal Modelsmentioning

confidence: 99%

Menkes disease

Tümer

Møller²

2009

Eur J Hum Genet

310

276

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Biochemical Study on the Critical Period for Treatment of the Mottled Brindled Mouse

Cited by 26 publications

References 23 publications

Prolonged copper depletion induces expression of antioxidants and triggers apoptosis in SH-SY5Y neuroblastoma cells

Prolonged copper depletion induces expression of antioxidants and triggers apoptosis in SH-SY5Y neuroblastoma cells

The Female Brindled Mouse as a Model of Menkes' Disease: The Relationship of Fur Pattern to Behavioral and Neurochemical Abnormalities

Menkes disease

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