Your search keyword '"Leora Witkowski"' showing total 5 results

1. Author Correction: SMARCA4/2 loss inhibits chemotherapy-induced apoptosis by restricting IP3R3-mediated Ca2+ flux to mitochondria

Author

Yibo Xue, Jordan L. Morris, Kangning Yang, Zheng Fu, Xianbing Zhu, Fraser Johnson, Brian Meehan, Leora Witkowski, Amber Yasmeen, Tunde Golenar, Mackenzie Coatham, Geneviève Morin, Anie Monast, Virginie Pilon, Pierre Olivier Fiset, Sungmi Jung, Anne V. Gonzalez, Sophie Camilleri-Broet, Lili Fu, Lynne-Marie Postovit, Jonathan Spicer, Walter H. Gotlieb, Marie-Christine Guiot, Janusz Rak, Morag Park, William Lockwood, William D. Foulkes, Julien Prudent, and Sidong Huang

Subjects

Multidisciplinary, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology

Published

2023

2. Malignant teratoid tumor of the thyroid gland: an aggressive primitive multiphenotypic malignancy showing organotypical elements and frequent DICER1 alterations—is the term 'thyroblastoma' more appropriate?

Author

Manuel Sobrinho-Simões, Alfred Brütting, Randa M S Amin, Leora Witkowski, Abbas Agaimy, Markus Bährle, Robert Stoehr, Samir S. Amr, Joseph Christopher Castillo Cuenca, Arndt Hartmann, Catarina Eloy, William D. Foulkes, Markus Metzler, Konstantinos Mantsopoulos, and Carlos Alberto González-Muller

Subjects

Male, Ribonuclease III, 0301 basic medicine, Pathology, medicine.medical_specialty, Thyroblastoma, Adolescent, DICER1, Teratocarcinosarcoma, Biology, Malignant teratoma, Pathology and Forensic Medicine, DEAD-box RNA Helicases, Head and neck, 03 medical and health sciences, 0302 clinical medicine, Terminology as Topic, Rhabdomyosarcoma, Germ cell tumor, medicine, Humans, Thyroid Neoplasms, ddc:610, Molecular Biology, Aged, DICER1 Syndrome, Thyroid, Teratoma, Wilms' tumor, Cell Biology, General Medicine, Middle Aged, medicine.disease, Teratoid tumor, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Mutation, Blastoma, Female, Original Article, PAX8, Germ cell

Abstract

Primary thyroid teratomas are exceedingly rare. Mature and immature variants recapitulate their gonadal counterparts (predilection for infants/children, triphasic germ layer differentiation, and favorable outcome). On the other hand, the so-called malignant teratomas affect predominantly adults and elderly, are highly aggressive, and, according to a few published cases, harbor DICER1 mutations. We describe three highly aggressive sporadic malignant teratoid thyroid tumors in 2 females (17 and 45 years) and one male (17 years). Histology showed triphasic neoplasms composed of solid nests of small primitive monomorphic cells embedded in a cellular stroma with primitive immature rhabdomyosarcoma-like (2) or pleomorphic sarcoma-like (1) phenotype. The third component was represented by TTF1+/PAX8+ primitive teratoid epithelial tubules reminiscent of primitive thyroid follicles and/or Wilms tumor, admixed with scattered respiratory- or enteric-type tubules, neuroepithelial rosettes, and fetal-type squamoid nests. Foci of cartilage were seen in two cases, but none contained mature organoid adult-type tissue or skin adnexa. SALL4 was expressed in the small cell (2) and stromal (1) component. Other germ cell markers were negative. Molecular testing revealed a known “hotspot” pathogenic DICER1 mutation in two cases. In addition, case 1 had a missense TP53 variant. This type of thyroid malignancy is distinct from genuine teratomas. The immunoprofile suggests primitive thyroid- or branchial cleft-like differentiation. Given that “blastoma” is a well-accepted terminology in the spectrum of DICER1-associated malignancies, the term “thyroblastoma” might be more convenient for these malignant teratoid tumors of the thyroid gland. Relationship of thyroblastoma to the DICER1 syndrome remains to be addressed. Electronic supplementary material The online version of this article (10.1007/s00428-020-02853-1) contains supplementary material, which is available to authorized users.

Published

2020

3. Germline and somatic SMARCA4 mutations characterize small cell carcinoma of the ovary, hypercalcemic type

Author

Avi Saskin, Jocelyne Arseneau, Lawrence M. Roth, Anna Margiolaki, François Plourde, Janez Lamovec, Barbara Rivera, Rachel Silva-Smith, Steffen Albrecht, Reiner Siebert, Vassilis Georgoulias, Helen J. Mackay, Andrew Berchuck, William D. Foulkes, Emmanouil Saloustros, Jacek Majewski, W Glenn McCluggage, Sharon M. Castellino, Madeleine Arseneault, Kitty Pavlakis, Ester Castellsagué, Yasser Riazalhosseini, Somayyeh Fahiminiya, Nancy Hamel, Thomas M. Ulbright, Inga Nagel, Elizabeth A. Reilly, Frederick R. Ueland, Tracey A Bender, Mona Wu, Javad Nadaf, Blaise A. Clarke, David Grynspan, Eva Tomiak, Catherine Gilpin, Leora Witkowski, Colin J.R. Stewart, Michel Longy, Marc Tischkowitz, Rouzan G. Karabakhtsian, Martin Hasselblatt, and Jian Carrot-Zhang

Subjects

Genetics, Mutation, Somatic cell, Biology, medicine.disease, medicine.disease_cause, Germline, Germline mutation, Carcinoma, medicine, Allele, Ovarian cancer, Exome sequencing

Abstract

Small cell carcinoma of the ovary, hypercalcemic type (SCCOHT) is the most common undifferentiated ovarian malignancy in women under 40 years of age. We sequenced the exomes of six individuals from three families with SCCOHT. After discovering segregating deleterious germline mutations in SMARCA4 in all three families, we tested DNA from a fourth affected family, which also carried a segregating SMARCA4 germline mutation. All the familial tumors sequenced harbored either a somatic mutation or loss of the wild-type allele. Immunohistochemical analysis of these cases and additional familial and non-familial cases showed loss of SMARCA4 (BRG1) protein in 38 of 40 tumors overall. Sequencing of cases with available DNA identified at least one germline or somatic deleterious SMARCA4 mutation in 30 of 32 cases. Additionally, the SCCOHT cell line BIN-67 had biallelic deleterious mutations in SMARCA4. Our findings identify alterations in SMARCA4 as the major cause of SCCOHT, which could lead to improvements in genetic counseling and new treatment approaches.

Published

2014

4. DICER1 hotspot mutations in non-epithelial gonadal tumours

Author

Nicholas Coleman, Jocelyne Arseneau, Dominik T. Schneider, Gabriele Calaminus, Jorge S. Reis-Filho, David G. Huntsman, Colin J.R. Stewart, Matthew J. Murray, James Nicholson, W G McCluggage, Leora Witkowski, Stefan Schönberger, Catherine S. Choong, William D. Foulkes, and J. Mattina

Subjects

Male, Ribonuclease III, Cancer Research, Pathology, Somatic cell, DNA Mutational Analysis, Sex Cord-Gonadal Stromal Tumors, DICER1, DEAD-box RNA Helicases, 0302 clinical medicine, Gene Frequency, Child, Ovarian Neoplasms, Sanger sequencing, 0303 health sciences, microRNA, Middle Aged, Neoplasms, Germ Cell and Embryonal, medicine.anatomical_structure, Oncology, Child, Preschool, 030220 oncology & carcinogenesis, symbols, Female, Germ cell, Adult, endocrine system, medicine.medical_specialty, Adolescent, RNase P, germ cell tumours, Biology, Young Adult, 03 medical and health sciences, symbols.namesake, Testicular Neoplasms, medicine, ovarian, Humans, Gene, Allele frequency, Aged, 030304 developmental biology, DICER1 Syndrome, Infant, Newborn, Infant, Genetics and Genomics, testicular, Mutation, Cancer research, sex cord-stromal tumours

Abstract

Background: Non-epithelial gonadal tumours largely comprise sex cord-stromal tumours (SCSTs) and germ cell tumours (GCTs). Specific somatic mutations in DICER1, a microRNA maturation pathway gene, have been identified in these tumours. We conducted a study that aimed to confirm, refine and extend the previous observations. Methods: We used Sanger sequencing to sequence the RNase IIIa and IIIb domains of DICER1 in 154 gonadal tumours from 135 females and 19 males, as well as 43 extra-gonadal GCTs from 26 females and 17 males. Results: We identified heterozygous non-synonymous mutations in the RNase IIIb domain of DICER1 in 14/197 non-epithelial tumours (7.1%). Mutations were found in 9/28 SCSTs (32%), 5/118 gonadal GCTs (4.2%), 0/43 extra-gonadal GCTs and 0/8 miscellaneous tumours. The 14 mutations affected only five residues: E1705, D1709, E1788, D1810 and E1813. In all five patients where matched and constitutional DNA was available, the mutations were only somatic. There were no mutations found in the RNase IIIa domain. Conclusion: More than half (8/15) of Sertoli–Leydig cell tumours (SLCTs) harbour DICER1 mutations in the RNase IIIb domain, while mutations are rarely found in GCTs. Genetic alterations in SLCTs may aid in classification and provide new approaches to therapy.

Published

2013

5. Erratum: DICER1 hotspot mutations in non-epithelial gonadal tumours

Author

Colin J.R. Stewart, Gabriele Calaminus, Jorge S. Reis-Filho, David G. Huntsman, Leora Witkowski, Nicholas Coleman, Stefan Schönberger, J Mattina, James Nicholson, Jocelyne Arseneau, Catherine S. Choong, W G McCluggage, Matthew J. Murray, Dominik T. Schneider, and William D. Foulkes

Subjects

Cancer Research, History, Oncology, Genealogy

Abstract

Correction to: British Journal of Cancer (2013) 109, 2744–2750. doi:10.1038/bjc.2013.637 Owing to an error on the authors' part, the fifth named author (Dr C S Choong) was omitted from the author listing when the paper was originally published. The full, correct author listing is now shown above.

Published

2013