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21 results on '"Alirezaie, Najmeh"'

1. Candidate DNA repair susceptibility genes identified by exome sequencing in high-risk pancreatic cancer

Author

Smith, Alyssa L, Alirezaie, Najmeh, Connor, Ashton, Chan-Seng-Yue, Michelle, Grant, Robert, Selander, Iris, Bascuñana, Claire, Borgida, Ayelet, Hall, Anita, Whelan, Thomas, Holter, Spring, McPherson, Treasa, Cleary, Sean, Petersen, Gloria M, Omeroglu, Atilla, Saloustros, Emmanouil, McPherson, John, Stein, Lincoln D, Foulkes, William D, Majewski, Jacek, Gallinger, Steven, and Zogopoulos, George

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Human Genome, Rare Diseases, Genetics, Orphan Drug, Pancreatic Cancer, Clinical Research, Digestive Diseases, Cancer, Biotechnology, Genetic Testing, Aetiology, 2.1 Biological and endogenous factors, Cell Cycle Proteins, DNA Repair, Exome, Gene Expression Regulation, Neoplastic, Genetic Predisposition to Disease, Humans, NIMA-Related Kinase 1, Pancreatic Neoplasms, Protein Serine-Threonine Kinases, Risk Factors, Sequence Analysis, DNA, Pancreatic adenocarcinoma, Familial pancreatic cancer, Exome sequencing, DNA repair genes, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

The genetic basis underlying the majority of hereditary pancreatic adenocarcinoma (PC) is unknown. Since DNA repair genes are widely implicated in gastrointestinal malignancies, including PC, we hypothesized that there are novel DNA repair PC susceptibility genes. As germline DNA repair gene mutations may lead to PC subtypes with selective therapeutic responses, we also hypothesized that there is an overall survival (OS) difference in mutation carriers versus non-carriers. We therefore interrogated the germline exomes of 109 high-risk PC cases for rare protein-truncating variants (PTVs) in 513 putative DNA repair genes. We identified PTVs in 41 novel genes among 36 kindred. Additional genetic evidence for causality was obtained for 17 genes, with FAN1, NEK1 and RHNO1 emerging as the strongest candidates. An OS difference was observed for carriers versus non-carriers of PTVs with early stage (≤IIB) disease. This adverse survival trend in carriers with early stage disease was also observed in an independent series of 130 PC cases. We identified candidate DNA repair PC susceptibility genes and suggest that carriers of a germline PTV in a DNA repair gene with early stage disease have worse survival.

Published
2016

2. The Mutational Spectrum of Pre- and Post-Neoadjuvant Chemotherapy Triple-Negative Breast Cancers

Author

Aguilar-Mahecha, Adriana, primary, Alirezaie, Najmeh, additional, Lafleur, Josiane, additional, Bareke, Eric, additional, Przybytkowski, Ewa, additional, Lan, Cathy, additional, Cavallone, Luca, additional, Salem, Myriam, additional, Pelmus, Manuela, additional, Aleynikova, Olga, additional, Greenwood, Celia, additional, Lovato, Amanda, additional, Ferrario, Cristiano, additional, Boileau, Jean-François, additional, Mihalcioiu, Catalin, additional, Roy, Josée-Anne, additional, Marcus, Elizabeth, additional, Discepola, Federico, additional, Majewski, Jacek, additional, and Basik, Mark, additional

Published
2023
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3. Exomic and epigenomic analysis of pulmonary blastoma

Author

Alirezaie, Najmeh, Chong, Anne-Laure, Kommoss, Felix K.F., Sabbaghian, Nelly, Camacho Valenzuela, Jose, Pelletier, Dylan, Nadaf, Javad, Kolekar, Shailesh B., Sivapalan, Pradeesh, Evans, Mark G., Thorner, Paul S., Fiset, Pierre-Olivier, von Deimling, Andreas, and Foulkes, William D.

Published
2024
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4. Prognostic and predictive value of circulating tumor DNA during neoadjuvant chemotherapy for triple negative breast cancer

Author

Cavallone, Luca, Aguilar-Mahecha, Adriana, Lafleur, Josiane, Brousse, Susie, Aldamry, Mohammed, Roseshter, Talia, Lan, Cathy, Alirezaie, Najmeh, Bareke, Eric, Majewski, Jacek, Ferrario, Cristiano, Hassan, Saima, Discepola, Federico, Seguin, Carole, Mihalcioiu, Catalin, Marcus, Elizabeth A., Robidoux, André, Roy, Josée-Anne, Pelmus, Manuela, and Basik, Mark

Published
2020
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5. The Mutational Spectrum of Pre- and Post-Neoadjuvant Chemotherapy Triple-Negative Breast Cancers.

Author

Aguilar-Mahecha, Adriana, Alirezaie, Najmeh, Lafleur, Josiane, Bareke, Eric, Przybytkowski, Ewa, Lan, Cathy, Cavallone, Luca, Salem, Myriam, Pelmus, Manuela, Aleynikova, Olga, Greenwood, Celia, Lovato, Amanda, Ferrario, Cristiano, Boileau, Jean-François, Mihalcioiu, Catalin, Roy, Josée-Anne, Marcus, Elizabeth, Discepola, Federico, Majewski, Jacek, and Basik, Mark

Subjects
*TRIPLE-negative breast cancer, *TUBULINS, *TUMOR suppressor genes, *NEOADJUVANT chemotherapy, *BREAST, *CANCER chemotherapy, *LYMPHOCYTE count
Abstract

The response of triple-negative breast cancer (TNBC) patients to pre-operative (neoadjuvant chemotherapy) is a critical factor of their outcome. To determine the effects of chemotherapy on the tumor genome and to identify mutations associated with chemoresistance and sensitivity, we performed whole exome sequencing on pre/post-chemotherapy tumors and matched lymphocytes from 26 patients. We observed great inter-tumoral heterogeneity with no gene mutated recurrently in more than four tumors besides TP53. Although the degree of response to chemotherapy in residual tumors was associated with more subclonal changes during chemotherapy, there was minimal evolution between pre/post-tumors. Indeed, gene sets enriched for mutations in pre- and post-chemotherapy tumors were very similar and reflected genes involved in the biological process of neurogenesis. Somatically mutated genes present in chemosensitive tumors included COL1A2, PRMD15, APOBEC3B, PALB2 and histone protein encoding genes, while BRCA1, ATR, ARID1A, XRCC3 and genes encoding for tubulin-associated proteins were present in the chemoresistant tumors. We also found that the mutational spectrum of post-chemotherapy tumors was more reflective of matching metastatic tumor biopsies than pre-chemotherapy samples. These findings support a portrait of modest ongoing genomic instability with respect to single-nucleotide variants induced by or selected for by chemotherapy in TNBCs. [ABSTRACT FROM AUTHOR]

Published
2024
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6. Mutations in BCOR , a co-repressor of CRX/OTX2 , are associated with early-onset retinal degeneration

Author

Langouët, Maéva, primary, Jolicoeur, Christine, additional, Javed, Awais, additional, Mattar, Pierre, additional, Gearhart, Micah D., additional, Daiger, Stephen P., additional, Bertelsen, Mette, additional, Tranebjærg, Lisbeth, additional, Rendtorff, Nanna D., additional, Grønskov, Karen, additional, Jespersgaard, Catherine, additional, Chen, Rui, additional, Sun, Zixi, additional, Li, Hui, additional, Alirezaie, Najmeh, additional, Majewski, Jacek, additional, Bardwell, Vivian J., additional, Sui, Ruifang, additional, Koenekoop, Robert K., additional, and Cayouette, Michel, additional

Published
2022
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9. Mutations in BCOR, a co-repressor of CRX/OTX2, are associated with early-onset retinal degeneration

Author

Langouët, Maéva, Jolicoeur, Christine, Javed, Awais, Mattar, Pierre, Gearhart, Micah D., Daiger, Stephen P., Bertelsen, Mette, Tranebjærg, Lisbeth, Rendtorff, Nanna D., Grønskov, Karen, Jespersgaard, Catherine, Chen, Rui, Sun, Zixi, Li, Hui, Alirezaie, Najmeh, Majewski, Jacek, Bardwell, Vivian J., Sui, Ruifang, Koenekoop, Robert K., Cayouette, Michel, Langouët, Maéva, Jolicoeur, Christine, Javed, Awais, Mattar, Pierre, Gearhart, Micah D., Daiger, Stephen P., Bertelsen, Mette, Tranebjærg, Lisbeth, Rendtorff, Nanna D., Grønskov, Karen, Jespersgaard, Catherine, Chen, Rui, Sun, Zixi, Li, Hui, Alirezaie, Najmeh, Majewski, Jacek, Bardwell, Vivian J., Sui, Ruifang, Koenekoop, Robert K., and Cayouette, Michel

Abstract

Many transcription factors regulating the production, survival, and function of photoreceptor cells have been identified, but little is known about transcriptional co-regulators in retinal health and disease. Here, we show that BCL6 co-repressor (BCOR), a Polycomb repressive complex 1 factor mutated in various cancers, is involved in photoreceptor degenerative diseases. Using proteomics and transcription assays, we report that BCOR interacts with the transcription factors CRX and OTX2 and reduces their ability to activate the promoters of photoreceptor-specific genes. CUT&RUN sequencing further shows that BCOR shares genome-wide binding profiles with CRX/OTX2, consistent with a general co-repression activity. We also identify missense mutations in human BCOR in five families that have no evidence of cancer but present severe early-onset X-linked retinal degeneration. Last, we show that the human BCOR mutants cause degeneration when expressed in the mouse retina and have enhanced repressive activity on OTX2. These results uncover a role for BCOR in photoreceptors in both health and disease.

Published
2022

10. Exome sequencing identifies mutations in the gene TTC7A in French-Canadian cases with hereditary multiple intestinal atresia

Author

Samuels, Mark E, Majewski, Jacek, Alirezaie, Najmeh, Fernandez, Isabel, Casals, Ferran, Patey, Natalie, Decaluwe, Hélène, Gosselin, Isabelle, Haddad, Elie, Hodgkinson, Alan, Idaghdour, Youssef, Marchand, Valerie, Michaud, Jacques L, Rodrigue, Marc-André, Desjardins, Sylvie, Dubois, Stéphane, Le Deist, Francoise, Awadalla, Philip, Raymond, Vincent, and Maranda, Bruno

Published
2013
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12. Circulating tumor DNA (ctDNA) during and after neoadjuvant chemotherapy and prior to surgery is a powerful prognostic factor in triple-negative breast cancer (TNBC).

Author

Cavallone, Luca, primary, Aguilar, Adriana, additional, Aldamry, Mohammed, additional, Lafleur, Josiane, additional, Brousse, Susie, additional, Lan, Cathy, additional, Alirezaie, Najmeh, additional, Bareke, Eric, additional, Majewski, Jacek, additional, Pelmus, Manuela, additional, Ferrario, Cristiano, additional, Marcus, Elizabeth A., additional, Robidoux, Andre, additional, Discepola, Federico, additional, and Basik, Mark, additional

Published
2019
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15. A region-based gene association study combined with a leave-one-out sensitivity analysis identifies SMG1 as a pancreatic cancer susceptibility gene.

Author

Wong, Cavin, Chen, Fei, Alirezaie, Najmeh, Wang, Yifan, Cuggia, Adeline, Borgida, Ayelet, Holter, Spring, Lenko, Tatiana, Domecq, Celine, null, null, Petersen, Gloria M., Syngal, Sapna, Brand, Randall, Rustgi, Anil K., Cote, Michele L., Stoffel, Elena, Olson, Sara H., Roberts, Nicholas J., Akbari, Mohammad R., and Majewski, Jacek

Subjects
CANCER genes, CANCER susceptibility, PANCREATIC cancer, DNA repair, SENSITIVITY analysis, COMPUTER-assisted drug design
Abstract

Pancreatic adenocarcinoma (PC) is a lethal malignancy that is familial or associated with genetic syndromes in 10% of cases. Gene-based surveillance strategies for at-risk individuals may improve clinical outcomes. However, familial PC (FPC) is plagued by genetic heterogeneity and the genetic basis for the majority of FPC remains elusive, hampering the development of gene-based surveillance programs. The study was powered to identify genes with a cumulative pathogenic variant prevalence of at least 3%, which includes the most prevalent PC susceptibility gene, BRCA2. Since the majority of known PC susceptibility genes are involved in DNA repair, we focused on genes implicated in these pathways. We performed a region-based association study using the Mixed-Effects Score Test, followed by leave-one-out characterization of PC-associated gene regions and variants to identify the genes and variants driving risk associations. We evaluated 398 cases from two case series and 987 controls without a personal history of cancer. The first case series consisted of 109 patients with either FPC (n = 101) or PC at ≤50 years of age (n = 8). The second case series was composed of 289 unselected PC cases. We validated this discovery strategy by identifying known pathogenic BRCA2 variants, and also identified SMG1, encoding a serine/threonine protein kinase, to be significantly associated with PC following correction for multiple testing (p = 3.22x10-7). The SMG1 association was validated in a second independent series of 532 FPC cases and 753 controls (p<0.0062, OR = 1.88, 95%CI 1.17–3.03). We showed segregation of the c.4249A>G SMG1 variant in 3 affected relatives in a FPC kindred, and we found c.103G>A to be a recurrent SMG1 variant associating with PC in both the discovery and validation series. These results suggest that SMG1 is a novel PC susceptibility gene, and we identified specific SMG1 gene variants associated with PC risk. [ABSTRACT FROM AUTHOR]

Published
2019
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16. Abstract 4320: Genomic change in residual triple-negative breast cancers after neoadjuvant chemotherapy

Author

Aguilar-Mahecha, Adriana, primary, Przybytkowski, Ewa, additional, Lafleur, Josiane, additional, Lan, Cathy, additional, Légaré, Stephanie, additional, Alirezaie, Najmeh, additional, Séguin, Carole, additional, Discepola, Federico, additional, Kovacina, Bojan, additional, Mihalcioiu, Catalin, additional, Robidoux, André, additional, Marcus, Elizabeth, additional, Roy, Josée Anne, additional, Pelmus, Manuela, additional, Aleynikova, Olga, additional, Nabavi, Sheida, additional, Majewski, Jacek, additional, and Basik, Mark, additional

Published
2015
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18. Abstract 09: Contribution of known and novel BRCA-mediated DNA repair pathway genes to pancreatic cancer susceptibility

Author

Smith, Alyssa, primary, Grant, Robert, additional, Hall, Anita, additional, Alirezaie, Najmeh, additional, Holter, Spring, additional, Whelan, Thomas, additional, Selander, Iris, additional, McPherson, Treasa, additional, McPherson, John, additional, Omeroglu, Atilla, additional, Majewski, Jacek, additional, Foulkes, William, additional, Gallinger, Steven, additional, and Zogopoulos, George, additional

Published
2014
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19. Exome sequencing identifies mutations in the geneTTC7Ain French-Canadian cases with hereditary multiple intestinal atresia

Author

Samuels, Mark E, primary, Majewski, Jacek, additional, Alirezaie, Najmeh, additional, Fernandez, Isabel, additional, Casals, Ferran, additional, Patey, Natalie, additional, Decaluwe, Hélène, additional, Gosselin, Isabelle, additional, Haddad, Elie, additional, Hodgkinson, Alan, additional, Idaghdour, Youssef, additional, Marchand, Valerie, additional, Michaud, Jacques L, additional, Rodrigue, Marc-André, additional, Desjardins, Sylvie, additional, Dubois, Stéphane, additional, Le Deist, Francoise, additional, Awadalla, Philip, additional, Raymond, Vincent, additional, and Maranda, Bruno, additional

Published
2013
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21. Genetic analysis of a combined small cell carcinoma and adenocarcinoma of the lung.

Author

Lach, Katherine D., Alirezaie, Najmeh S., Majewski, Jacek, Camilleri-Broet, Sophie, Fraser, Richard, Spicer, Jonathan D., and Fiset, Pierre O.

Subjects
LUNG cancer & genetics, SMALL cell carcinoma, ADENOCARCINOMA, IMMUNOHISTOCHEMISTRY, NUCLEIC acid isolation methods
Abstract

Background: Combined small cell lung carcinoma consists of small cell carcinoma and another histologic type of nonsmall cell lung carcinoma. Little is known of the mutation spectrum of this malignancy, and whether it results from a common precursor or from two independent tumours. We present a case of a 73-year old male ex-smoker who presented with hemoptysis. Investigations revealed a left lower lobe mass and a left mainstem endobronchial tumour. Surgical resection of the lower lobe tumour showed a combined small cell carcinoma and adenocarcinoma. The endobronchial tumour showed only small cell carcinoma. Foci of metastatic adenocarcinoma were found in regional lymph nodes. Methods: Immunohistochemistry (cytokeratin 7, Napsin A, TTF-1, CD56, synaptophysin and chromogranin) and mucin stains (PAS, PAS-D and mucicarmine) were performed. DNA was extracted from formalin-fixed paraffin-embedded tissue, targeting morphologically distinct areas. The DNA was analyzed using whole-exome sequencing (WES). Results: Neuroendocrine staining was limited to the small cell carcinoma, while epithelial marker and mucin stains were positive in the adenocarcinoma only. WES showed that the small cell component of both the primary and metastatic site harbored characteristic mutations including RB1, TP53 and EP300. By comparison, the adenocarcinoma component showed mutations in KRAS and EYA1. Conclusions: This is a rare case of a surgically resected combined small cell carcinoma and adenocarcinoma, with distinct histologic and immunohistochemical phenotypes. With whole exome sequencing, two distinct genetic phenotypes were present providing evidence that the tumour was a collision tumour. [ABSTRACT FROM AUTHOR]

Published
2018

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