Lysosomal dysfunction, cellular pathology and clinical symptoms: basic principles

Between 40 and 50 lysosomal storage disorders are known at present. Fine details of the pathogenic process involved are in general not known. This overview highlights the basic principles of lysosomal pathogenesis and the clinical consequences of defective genes involved in lysosomal functions. The...

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Bibliographic Details
Published inActa pædiatrica (Oslo) Vol. 95; no. 451; pp. 77 - 82
Main Authors Reuser, Arnold, Drost, Maarten
Format Journal Article
LanguageEnglish
Published Norway 01.04.2006
Subjects
Animals
beta-Galactosidase - deficiency
Gaucher Disease - metabolism
Gaucher Disease - pathology
Gaucher Disease - physiopathology
Glycogen Storage Disease Type II - pathology
Glycogen Storage Disease Type II - physiopathology
Humans
Liver - metabolism
Lysosomal Storage Diseases - pathology
Lysosomal Storage Diseases - physiopathology
Lysosomes - physiology
Macrophages - metabolism
Mucopolysaccharidoses - pathology
Mucopolysaccharidoses - physiopathology
Muscle Contraction - physiology
Muscle, Skeletal - pathology
Myofibrils - pathology
Sarcomeres - pathology
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ISSN0803-5253
0803-5326
DOI10.1080/08035320600618957

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Summary:Between 40 and 50 lysosomal storage disorders are known at present. Fine details of the pathogenic process involved are in general not known. This overview highlights the basic principles of lysosomal pathogenesis and the clinical consequences of defective genes involved in lysosomal functions. The subject is discussed in the context of the possibility of prevention and reversal of cellular and organ damage by enzyme replacement therapy. Also presented is a mechanical model for the muscle pathology observed in Pompe disease. Direct mechanical effects of the non-contractile inclusions - glycogen-loaded lysosomes - seem to be a key factor in the loss of force during both early and late stages of the disease. Each lysosomal storage disorder and each patient with a given lysosomal disorder has unique molecular, pathological and clinical features. But, the order of pathological events is largely the same. Mutations in a gene cause lysosomal dysfunction which, in turn, results in cellular pathology affecting organ structure and function. Clinical symptoms are the ultimate manifestation. The reversibility of symptoms with enzyme replacement therapy will vary according to the disease, as well as the nature and stage of organ pathology.
ISSN:0803-5253
0803-5326
DOI:10.1080/08035320600618957