BiomedExperts ProfilePublication Detail
The publication detail shows the title, authors (with indicators showing other profiled authors), information on the publishing organization, abstract and a link to the article in PubMed. This abstract is what is used to create the fingerprint of the publication. If any grants are referenced by the publication, they will be listed here as well.
Loss of the ataxia-telangiectasia gene product causes oxidative damage in target organs.
C Barlow; P A Dennery; M K Shigenaga; M A Smith; J D Morrow; L J Roberts; A Wynshaw-Boris; R L Levine (Profiled Author: Smith, Mark A)
Laboratory of Genetic Disease Research, National Human Genome Research Institute, Bethesda, MD 20892, USA. barlow@salk.edu
Proceedings of the National Academy of Sciences of the United States of America 1999;96(17):9915-9.
Ataxia-telangiectasia (A-T) is characterized by a markedly increased sensitivity to ionizing radiation, increased incidence of cancer, and neurodegeneration, especially of the cerebellar Purkinje cells. Ionizing radiation oxidizes macromolecules and causes tissue damage through the generation of reactive oxygen species (ROS). We therefore hypothesized that A-T is due to oxidative damage resulting from loss of function of the A-T gene product. To assess this hypothesis, we employed an animal model of A-T, the mouse with a disrupted Atm gene. We show that organs which develop pathologic changes in the Atm-deficient mice are targets of oxidative damage, and that cerebellar Purkinje cells are particularly affected. These observations provide a mechanistic basis for the A-T phenotype and lay a rational foundation for therapeutic intervention.
Scientific Context
This section shows information related to the publication - computed using the fingerprint of the publication - including related publications, related experts and related grants with fingerprints representing significant amounts of overlap between their fingerprint and this publication. The red dots indicate whether those experts or terms appear within the publication, thereby showing potential and actual connections.
Related Grants
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1.
MATTSON, MARK
Dietary Modification Of Brain Aging And Neurodegenerative Disorders
NATIONAL INSTITUTE ON AGING
Total Funding: $ 1,876,709
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2.
MATTSON, MARK
Hormesis/Adaptive Stress Responses and Aging
NATIONAL INSTITUTE ON AGING
Total Funding: $ 1,257,830
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3.
PERRY, GEORGE
NEUROFIBRILLARY PATHOLOGY IN ALZHEIMER DISEASE
1 September 1990 - 30 November 2000
NATIONAL INSTITUTE ON AGING
Total Funding: $ 1,191,333
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1.
2004Susan E Browne; L Jackson Roberts; Phyllis A Dennery; Susan R Doctrow; M Flint Beal; Carrolee Barlow; Rodney L Levine
Free radical biology & medicine 2004;36(7):938-42. -
2.
2001B S Wong; T Liu; D Paisley; R Li; T Pan; S G Chen; G Perry; R B Petersen; M A Smith; D W Melton; et al.
Induction of HO-1 and NOS in doppel-expressing mice devoid of PrP: implications for doppel function.
Molecular and cellular neurosciences 2001;17(4):768-75. -
3.
2000M Takahashi; S Doré; C D Ferris; T Tomita; A Sawa; H Wolosker; D R Borchelt; T Iwatsubo; S H Kim; G Thinakaran; et al.
Neuron 2000;28(2):461-73.
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