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Your search keyword '"Bernatowska E"' showing total 5 results
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5 results on '"Bernatowska E"'

1. Nijmegen breakage syndrome

Author

Krajewska-Walasek, M., Barbi, G., Bialecka, M., Matsuura, S., Wegner, R.D., Abramczuk, D., Conley, M.E., Sperling, K., Gregorek, H., Concannon, P., Dixon, J., Michalkiewicz, J., Gatti, R.A., Maraschio, P., Perek, D., Marseglia, G.L., Midro, A.T., Green, A., Seemanová, E., Taylor, A.M., Belohradsky, B.H., Kaloustian, V.M. der, Sölder, B., Komatsu, K., Hiel, J.A., Weemaes, C.M., Heuvel, L.P. van den, Engelen, B.G. van, Gabreëls, F.J., Smeets, D.F., Burgt, I. van der, Chrzanovska, K.H., and Bernatowska, E.

Abstract

Background Nijmegen breakage syndrome (NBS) is a rare autosomal recessive disorder. NBS-1, the gene defective in NBS, is located on chromosome 8q21 and has recently been cloned. The gene product, nibrin, is a novel protein, which is member of the hMre11/hRad50 protein complex, suggesting that the gene is involved in DNA double strand break repair. Aims To study the clinical and laboratory features of NBS as well as the genotype-phenotype relation. Methods Fifty five patients with NBS, included in the NBS registry in Nijmegen were evaluated. The majority of the patients were of eastern European ancestry. Most of them had shown a truncating 5 bp deletion 657-661 delACAAA. Four further truncating mutations have been identified in patients with other distinct haplotypes. Results and conclusions Essential features found in NBS were microcephaly, usually without severe retardation, typical facial appearance, immunodeficiency, chromosomal instability, x ray hypersensitivity, and predisposition to malignancy. In 40% of the patients cancer was noted before the age of 21 years. Important additional features were skin abnormalities, particularly café au lait spots and vitiligo, and congenital malformations, particularly clinodactyly and syndactyly. Congenital malformations, immunodeficiency, radiation hypersensitivity, and cancer predispostion were comprehensible in case of dysfunctioning of DNA repair mechanisms. No specific genotype-phenotype relation could be found. Patients with the same genotype may show different phenotypes and patients with different genotypes may express the same phenotype. Specific mutations did not lead to specific clinical features.

Published
2000

2. Four novel mutations in the gene encoding gp91-phox of human NADPH oxidase: consequences for oxidase assembly

Author

Leusen, J. H. W., Meischl, C., Eppink, M. H. M., Hilarius, P. M., de Boer, M., Weening, R. S., Åhlin, A., Sanders, L., Goldblatt, D., Skopczynska, H., Bernatowska, E., Palmblad, J., Verhoeven, A. J., van Berkel, W. J. H., and Roos, D.

Abstract

The superoxide-forming nicotinamide adenine dinucleotide phosphate reduced (NADPH) oxidase of human phagocytes comprises membrane-bound and cytosolic proteins, which, upon cell activation, assemble on the plasma membrane to form the active enzyme. Patients with chronic granulomatous disease (CGD) are defective in one of the phagocyte oxidase (phox) components, p47-phox or p67-phox, which reside in the cytosol of resting phagocytes, or gp91-phox or p22-phox, which constitute the membrane-bound cytochrome b558. In four X-linked CGD patients we have identified novel missense mutations inCYBB, the gene encoding gp91-phox. These mutations were associated with normal amounts of nonfunctional cytochromeb558 in the patients' neutrophils. In phorbol-myristate–stimulated neutrophils and in a cell-free translocation assay with neutrophil membranes and cytosol, the association of p47-phox and p67-phox with the membrane fraction of the cells with Cys369→Arg, Gly408→Glu, and Glu568→ Lys substitutions was strongly disturbed. Only a Thr341→Lys substitution, residing in a region of gp91-phox involved in flavin adenine dinucleotide (FAD) binding, supported a normal translocation. Thus, the introduction or reversal of charge at residues 369, 408, and 568 in gp91-phox destroys the correct binding of p47-phox and p67-phox to cytochrome b558. Based on mutagenesis studies of structurally related flavin-dependent oxidoreductases, we propose that the Thr341→Lys substitution results in impaired hydride transfer from NADPH to FAD. Because we found no electron transfer in solubilized neutrophil plasma membranes from any of the four patients, we conclude that all four amino acid replacements are critical for electron transfer. Apparently, an intimate relation exists between domains of gp91-phox involved in electron transfer and in p47/p67-phox binding.

Published
2000
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3. Primary Immunodeficiency Diseases in Children Treated in the Children's Memorial Hospital, Poland

Author

Bernatowska, E., Madalinski, K., Michalkiewicz, J., and Gregorek, H.

Abstract

One hundred and three cases of primary immunodeficiency diseases were diagnosed among children suffering mainly from chronic and severe infections in the period 1980-1987. Predominantly antibody defects were recognized in 48 patients (46.6%), combined immunodeficiencies in 36 patients (35%), phagocytic disorders in 12 patients (11.6%), complement defects in 6 patients (5.8%), and cell-mediated disease (Di George syndrome) in 1 patient.Allergic complications were observed in 25 patients (24.2%) and malignancy - in 3 patients (2.9%). More detailed immunological studies were performed in children with X-linked agammaglobulinemia in the course of intravenous immunoglobulin therapy and in children with ataxia telangiectasia.

Published
1988
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