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Query: UMLS:C0019209 (
hepatomegaly
)
5,798
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
A newborn female, the second child of consanguineous parents, exhibited general muscle hypotonia, apathy,
hepatomegaly
and failure to thrive from birth and signs of craniofacial dysmorphia were present. Pipecolic and trihydroxicoprostanoic acid were excreted in the urine and serum transferrin, ferritin and iron were markedly elevated. At the age of 7 weeks the baby died of respiratory insufficiency. Besides malformations of the brain, renal cysts, liver damage with hypoplastic intrahepatic bile ducts and cholestasis, increased storage of iron and cytochemically proven deficiency of peroxisomes in liver and kidney, morphological studied provided evidence of a mitochondrial myopathy in striated muscle with the accumulation of enlarged bizarre mitochondria, showing only minor structural abnormalities. No defects of NADH-reductase, succinate-dehydrogenase or cytochrome-c-oxidase were demonstrated histochemically. Cytochemical-ultrastructural investigation of
mitochondrial ATPase
revealed activation of the ATP-synthesising enzyme even before the addition of an uncoupler, this indicating loosely coupled oxidative phosphorylation. In addition a high rate of subcellular autophagy with segregation of mitochondria and focal loss of fibrils was present. Muscle damage in Zellweger syndrome appears to be the consequence of complex, interacting metabolic processes. The mitochondrial myopathy thereby induced allows a better understanding of general muscle hypotonia, one of the leading symptoms of this disorder.
...
PMID:Mitochondrial myopathy with loosely coupled oxidative phosphorylation in a case of Zellweger syndrome. A cytochemical-ultrastructural study. 614 41
We report a new type of fatal mitochondrial disorder caused by selective deficiency of mitochondrial
ATP synthase
(
ATPase
). A hypotrophic newborn from a consanguineous marriage presented severe lactic acidosis, cardiomegaly and
hepatomegaly
and died from heart failure after 2 days. The activity of oligomycin-sensitive
ATPase
was only 31-34% of the control, both in muscle and heart, but the activities of cytochrome c oxidase, citrate synthase and pyruvate dehydrogenase were normal. Electrophoretic and western blot analysis revealed selective reduction of
ATPase
complex but normal levels of the respiratory chain complexes I, III and IV. The same selective deficiency of
ATPase
was found in cultured skin fibroblasts which showed similar decreases in
ATPase
content,
ATPase
hydrolytic activity and level of substrate-dependent ATP synthesis (20-25, 18 and 29-33% of the control, respectively). Pulse-chase labelling of patient fibroblasts revealed low incorporation of [(35)S]methionine into assembled
ATPase
complexes, but increased incorporation into immunoprecipitated
ATPase
subunit beta, which had a very short half-life. In contrast, no difference was found in the size and subunit composition of the assembled and newly produced
ATPase
complex. Transmitochondrial cybrids prepared from enucleated fibroblasts of the patient and rho degrees cells derived from 143B. TK(-)human osteosarcoma cells fully restored the
ATPase
activity, ATP synthesis and
ATPase
content, when compared with control cybrids. Likewise, the pattern of [(35)S]methionine labelling of
ATPase
was found to be normal in patient cybrids. We conclude that the generalized deficiency of
mitochondrial ATPase
described is of nuclear origin and is caused by altered biosynthesis of the enzyme.
...
PMID:A novel deficiency of mitochondrial ATPase of nuclear origin. 1048 64
We present clinical and laboratory data from 14 cases with an isolated deficiency of the mitochondrial
ATP synthase
(7-30% of control) caused by nuclear genetic defects. A quantitative decrease of the
ATP synthase
complex was documented by Blue-Native electrophoresis and Western blotting and was supported by the diminished activity of oligomycin/aurovertin-sensitive ATP hydrolysis in fibroblasts (10 cases), muscle (6 of 7 cases), and liver (one case). All patients had neonatal onset and elevated plasma lactate levels. In 12 patients investigated 3-methyl-glutaconic aciduria was detected. Seven patients died, mostly within the first weeks of life and surviving patients showed psychomotor and various degrees of mental retardation. Eleven patients had hypertrophic cardiomyopathy; other clinical signs included hypotonia,
hepatomegaly
, facial dysmorphism and microcephaly. This phenotype markedly differs from the severe central nervous system changes of
ATP synthase
disorders caused by mitochondrial DNA mutations of the ATP6 gene presenting mostly as NARP and MILS.
...
PMID:Deficiency of mitochondrial ATP synthase of nuclear genetic origin. 1705 6
