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Titlebook: Biology of Brain Dysfunction; Volume 1 Gerald E. Gaull Book 1973 Plenum Press, New York 1973 biology.brain.growth.information.molecular bio

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Cytogenetic Aspects of Brain Dysfunction,rations. This difference is now understandable on the basis that only one X chromosome is genetically active in somatic cells and any extra X chromosome material in excess of one is inactivated during early life..
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Kommunikation und Kommunikationsmodelle,galactose metabolism is blocked also gives rise to accumulation of galactose-1-phosphate. With this type, the pathophysiology is particularly complex in that it includes mental retardation, a symptom not found in galactokinase deficiency. The pathophysiology of galactosemia has been studied extensiv
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Galactosemia: Biochemistry, Genetics, Pathophysiology, and Developmental Aspects,galactose metabolism is blocked also gives rise to accumulation of galactose-1-phosphate. With this type, the pathophysiology is particularly complex in that it includes mental retardation, a symptom not found in galactokinase deficiency. The pathophysiology of galactosemia has been studied extensiv
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Book 1973ifference in the rate at which various authors work. Therefore, the following strategy has been adopted: multiple small volumes and a relatively flexible format, with publication in order of receipt and as soon as enough chapters are assembled to make publication practical and economical. In this wa
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Galactosemia: Biochemistry, Genetics, Pathophysiology, and Developmental Aspects,mia” means simply “galactose in the blood.” In animals, galactosemia can be achieved by overloading the organism with this sugar by feeding a diet rich in galactose. In man, one has encountered two types of congenital disease, both called “galactosemia.” One type of hereditary galactosemia is caused
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