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Titlebook: Oxidative Phosphorylation in Health and Disease; Jan A. M. Smeitink,Rob C. A. Sengers,J. M. Frans T Book 2005 Springer-Verlag US 2005 DNA.

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ice, is also studied. There are critical reviews of symptoms and signs associated with syndromes, as well as updates on the genetic defects of either the mitochondrial or the nuclear genome responsible for many disorders.978-1-4419-3435-2978-0-387-26992-4
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Biochemical Diagnosis of OXPHOS Disorders, be measured. In the latter case patients with a disturbance in the oxidative phosphorylation not localized in one of the OXPHOS complexes remain undiagnosed. Practical guidelines for the biochemical examinations of muscle are provided. In certain circumstances it is necessary to examine also fibrob
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Mitochondrial DNA and OXPHOS Disorders,ey range from lesions of single tissues or structures, such as the optic nerve in Leber s hereditary optic neuropathy, or the cochlea in maternally-inherited nonsyndromic deafness, to more widespread lesions including myopathies, encephalomyopathies, cardiopathies, or complex multisystem syndromes.
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Prenatal Diagnostics in Oxidative Phosphorylation Disorders,e muscle biopsies with clearly decreased substrate oxidation rates and ATP production rates, all respiratory chain enzymes, complex-V and PDHC show normal activities. In these cases it is impossible at the moment to offer prenatal diagnosis. In the remainder of the biopsies with clearly reduced subs
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