Clinical and ultrastructural spectrum of diffuse lung disease associated with surfactant protein C mutations

Genetic defects of surfactant metabolism are associated with a broad range of clinical manifestations, from neonatal respiratory distress syndrome to adult interstitial lung disease. Early therapies may improve symptoms but diagnosis is often delayed owing to phenotype and genotype variability. Our...

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Published in:	European journal of human genetics : EJHG Vol. 23; no. 8; pp. 1033 - 1041
Main Authors:	Peca, Donatella, Boldrini, Renata, Johannson, Jan, Shieh, Joseph T, Citti, Arianna, Petrini, Stefania, Salerno, Teresa, Cazzato, Salvatore, Testa, Raffaele, Messina, Francesco, Onofri, Alfredo, Cenacchi, Giovanna, Westermark, Per, Ullmann, Nicola, Ullman, Nicola, Cogo, Paola, Cutrera, Renato, Danhaive, Olivier
Format:	Journal Article
Language:	English
Published:	England Nature Publishing Group 01-08-2015
Subjects:	Adult Biopsy Child Children Electron microscopy Female Gene expression Genetics Genotypes Heterozygote Homeostasis Hospitals Humans Infant, Newborn Intensive care Lung Lung - pathology Lung - ultrastructure Lung diseases Lung Diseases, Interstitial - genetics Lung Diseases, Interstitial - pathology Male Medicin och hälsovetenskap Metabolism Microscopy, Electron, Transmission Morphology Mutation Neonates Neurosciences Pediatrics Peptides Phenotype Phenotypes Pneumonia Protein C Protein C - genetics Protein folding Proteins Pulmonary Surfactant-Associated Protein C - genetics Respiratory distress syndrome Rodents Surfactant protein C Surfactants Transgenic animals Ultrastructure Italy San Francisco California Sweden California United States > US
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Summary:	Genetic defects of surfactant metabolism are associated with a broad range of clinical manifestations, from neonatal respiratory distress syndrome to adult interstitial lung disease. Early therapies may improve symptoms but diagnosis is often delayed owing to phenotype and genotype variability. Our objective was to characterize the cellular/ultrastructural correlates of surfactant protein C (SP-C) mutations in children with idiopathic diffuse lung diseases. We sequenced SFTPC - the gene encoding SP-C - SFTPB and ABCA3, and analyzed morphology, ultrastructure and SP expression in lung tissue when available. We identified eight subjects who were heterozygous for SP-C mutations. Median age at onset and clinical course were variable. None of the mutations were located in the mature peptide-encoding region, but were either in the pro-protein BRICHOS or linker C-terminal domains. Although lung morphology was similar to other genetic surfactant metabolism disorders, electron microscopy studies showed specific anomalies, suggesting surfactant homeostasis disruption, plus trafficking defects in the four subjects with linker domain mutation and protein misfolding in the single BRICHOS mutation carrier in whom material was available. Immunolabeling studies showed increased proSP-C staining in all cases. In two cases, amyloid deposits could be identified. Immunochemistry and ultrastructural studies may be useful for diagnostic purposes and for genotype interpretation.
Bibliography:	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23
ISSN:	1018-4813 1476-5438 1476-5438
DOI:	10.1038/ejhg.2015.45