51. Systemic inflammation and neurodegeneration in a mouse model of multiple sulfatase deficiency
- Author
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Gilda Cobellis, Carmine Settembre, Ester Zito, Daniela Zarcone, Ida Annunziata, Carmine Spampanato, Carlo Tacchetti, Edoardo Nusco, Andrea Ballabio, Maria Pia Cosma, Settembre, Carmine, Annunziata, Ida, Spampanato, Carmine, Zarcone, Daniela, Cobellis, Gilda, Nusco, Edoardo, Zito, Ester, Tacchetti, Carlo, Cosma, Maria Pia, Ballabio, Andrea, C., Settembre, I., Annunziata, C., Spampanato, D., Zarcone, G., Cobelli, E., Nusco, E., Zito, M. P., Cosma, and A., Ballabio
- Subjects
medicine.medical_specialty ,Macrophage ,Inflammation ,Apoptosis ,Mice, Transgenic ,Biology ,Proinflammatory cytokine ,Cell Line ,Mice ,Multiple sulfatase deficiency ,Internal medicine ,medicine ,SUMF1 Gene ,Animals ,Oxidoreductases Acting on Sulfur Group Donors ,Glycosaminoglycans ,Neurons ,Multidisciplinary ,Microglia ,Neurodegenerative Disease ,Animal ,Sulfatase ,Macrophages ,Neurodegeneration ,Apoptosi ,Neurodegenerative Diseases ,Fibroblasts ,Biological Sciences ,Neuron ,medicine.disease ,Cell biology ,Disease Models, Animal ,medicine.anatomical_structure ,Endocrinology ,Phenotype ,Glycosaminoglycan ,Sulfatase-Modifying Factor 1 ,Mutation ,Fibroblast ,medicine.symptom ,Sulfatases - Abstract
Sulfatases are involved in several biological functions such as degradation of macromolecules in the lysosomes. In patients with multiple sulfatase deficiency, mutations in theSUMF1gene cause a reduction of sulfatase activities because of a posttranslational modification defect. We have generated a mouse line carrying a null mutation in theSumf1gene. Sulfatase activities are completely absent inSumf1−/−mice, indicating that Sumf1 is indispensable for sulfatase activation and that mammals, differently from bacteria, have a single sulfatase modification system. Similarly to multiple sulfatase deficiency patients,Sumf1−/−mice display frequent early mortality, congenital growth retardation, skeletal abnormalities, and neurological defects. All examined tissues showed progressive cell vacuolization and significant lysosomal storage of glycosaminoglycans.Sumf1−/−mice showed a generalized inflammatory process characterized by a massive presence of highly vacuolated macrophages, which are the main site of lysosomal storage. Activated microglia were detected in the cerebellum and brain cortex associated with remarkable astroglyosis and neuronal cell loss. Between 4 and 6 months of age, we detected a strong increase in the expression levels of inflammatory cytokines and of apoptotic markers in both the CNS and liver, demonstrating that inflammation and apoptosis occur at the late stage of disease and suggesting that they play an important role in both the systemic and CNS phenotypes observed in lysosomal disorders. This mouse model, in which the function of an entire protein family has been silenced, offers a unique opportunity to study sulfatase function and the mechanisms underlying lysosomal storage diseases.
- Published
- 2007