Your search keyword '"Limon, Janusz"' showing total 3 results

1. Cornelia de Lange syndrome with NIPBL mutation and mosaic Turner syndrome in the same individual

Author

Wierzba Jolanta, Gil-Rodríguez María, Polucha Anna, Puisac Beatriz, Arnedo María, Teresa-Rodrigo María, Winnicka Dorota, Hegardt Fausto G, Ramos Feliciano J, Limon Janusz, and Pié Juan

Subjects

Cornelia de Lange syndrome, CdLS, NIPBL, Turner syndrome, TS, Monosomy X mosaicism, Mosaic 45,X/46,XX karyotype, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Cornelia de Lange syndrome (CdLS) is a dominantly inherited disorder characterized by facial dysmorphism, growth and cognitive impairment, limb malformations and multiple organ involvement. Mutations in NIPBL gene account for about 60% of patients with CdLS. This gene encodes a key regulator of the Cohesin complex, which controls sister chromatid segregation during both mitosis and meiosis. Turner syndrome (TS) results from the partial or complete absence of one of the X chromosomes, usually associated with congenital lymphedema, short stature, and gonadal dysgenesis. Case presentation Here we report a four-year-old female with CdLS due to a frameshift mutation in the NIPBL gene (c.1445_1448delGAGA), who also had a tissue-specific mosaic 45,X/46,XX karyotype. The patient showed a severe form of CdLS with craniofacial dysmorphism, pre- and post-natal growth delay, cardiovascular abnormalities, hirsutism and severe psychomotor retardation with behavioural problems. She also presented with minor clinical features consistent with TS, including peripheral lymphedema and webbed neck. The NIPBL mutation was present in the two tissues analysed from different embryonic origins (peripheral blood lymphocytes and oral mucosa epithelial cells). However, the percentage of cells with monosomy X was low and variable in tissues. These findings indicate that, ontogenically, the NIPBL mutation may have appeared before the mosaic monosomy X. Conclusions The coexistence in several patients of these two rare disorders raises the issue of whether there is indeed a cause-effect association. The detailed clinical descriptions indicate predominant CdLS phenotype, although additional TS manifestations may appear in adolescence.

Published

2012

2. High Resolution Melting analysis as a rapid and efficient method of screening for small mutations in the STK11gene in patients with Peutz-Jeghers syndrome

Author

Borun, Pawel, primary, Bartkowiak, Anna, additional, Banasiewicz, Tomasz, additional, Nedoszytko, Boguslaw, additional, Nowakowska, Dorota, additional, Teisseyre, Mikolaj, additional, Limon, Janusz, additional, Lubinski, Jan, additional, Kubaszewski, Lukasz, additional, Walkowiak, Jaroslaw, additional, Czkwianianc, Elzbieta, additional, Siolek, Monika, additional, Kedzia, Agnieszka, additional, Krokowicz, Piotr, additional, Cichy, Wojciech, additional, and Plawski, Andrzej, additional

Published

2013

3. High Resolution Melting analysis as a rapid and efficient method of screening for small mutations in the STK11 gene in patients with Peutz-Jeghers syndrome.

Author

Borun, Pawel, Bartkowiak, Anna, Banasiewicz, Tomasz, Nedoszytko, Boguslaw, Nowakowska, Dorota, Teisseyre, Mikolaj, Limon, Janusz, Lubinski, Jan, Kubaszewski, Lukasz, Walkowiak, Jaroslaw, Czkwianianc, Elzbieta, Siolek, Monika, Kedzia, Agnieszka, Krokowicz, Piotr, Cichy, Wojciech, and Plawski, Andrzej

Subjects

PEUTZ-Jeghers syndrome, CANCER risk factors, MEDICAL screening, EXONS (Genetics), NUCLEOTIDE sequence, GENETIC disorders

Abstract

Background: Peutz-Jeghers syndrome (PJS) is a rare hereditary syndrome characterized by the occurrence of hamartomatous polyps in the gastrointestinal tract, mucocutaneous pigmentation and increased risk of cancer in multiple internal organs. Depending on the studied population, its incidence has been estimated to range from 1:200 000 even up to 1:50 000 births. Being an autosomal disease, PJS is caused in most cases by mutations in the STK11 gene. Methods: The majority of causative DNA changes identified in patients with PJS are small mutations and, therefore, developing a method of their detection is a key aspect in the advancement of genetic diagnostics of PJS patients. We designed 13 pairs of primers, which amplify at the same temperature and enable examination of all coding exons of the STK11 gene by the HRM analysis. Results: In our group of 41 families with PJS small mutations of the STK11 gene were detected in 22 families (54%). In the remaining cases all of the coding exons were sequenced. However, this has not allowed to detect any additional mutations. Conclusions: The developed methodology is a rapid and cost-effective screening tool for small mutations in PJS patients and makes it possible to detect all the STK11 gene sequence changes occurring in this group. [ABSTRACT FROM AUTHOR]

Published

2013