Your search keyword '"Niknafs, Noushin"' showing total 8 results

1. Durvalumab with platinum-pemetrexed for unresectable pleural mesothelioma: survival, genomic and immunologic analyses from the phase 2 PrE0505 trial

Author

Forde, Patrick M., Anagnostou, Valsamo, Sun, Zhuoxin, Dahlberg, Suzanne E., Kindler, Hedy L., Niknafs, Noushin, and Purcell, Thomas

Subjects

T cells -- Analysis, Radioimmunotherapy -- Methods, Mesothelioma -- Diagnosis -- Care and treatment -- Risk factors, Pemetrexed -- Dosage and administration, Biological sciences, Health

Abstract

Mesothelioma is a rare and fatal cancer with limited therapeutic options until the recent approval of combination immune checkpoint blockade. Here we report the results of the phase 2 PrE0505 trial (NCT02899195) of the anti-PD-L1 antibody durvalumab plus platinum-pemetrexed chemotherapy for 55 patients with previously untreated, unresectable pleural mesothelioma. The primary endpoint was overall survival compared to historical control with cisplatin and pemetrexed chemotherapy; secondary and exploratory endpoints included safety, progression-free survival and biomarkers of response. The combination of durvalumab with chemotherapy met the pre-specified primary endpoint, reaching a median survival of 20.4 months versus 12.1 months with historical control. Treatment-emergent adverse events were consistent with known side effects of chemotherapy, and all adverse events due to immunotherapy were grade 2 or lower. Integrated genomic and immune cell repertoire analyses revealed that a higher immunogenic mutation burden coupled with a more diverse T cell repertoire was linked to favorable clinical outcome. Structural genome-wide analyses showed a higher degree of genomic instability in responding tumors of epithelioid histology. Patients with germline alterations in cancer predisposing genes, especially those involved in DNA repair, were more likely to achieve long-term survival. Our findings indicate that concurrent durvalumab with platinum-based chemotherapy has promising clinical activity and that responses are driven by the complex genomic background of malignant pleural mesothelioma. In a phase 2 trial, the combination of chemotherapy with durvalumab, an anti-PD-L1 antibody, exhibited promising clinical activity in patients with previously untreated, unresectable mesothelioma, with additional analyses providing insights into genomic and immunologic features potentially associated with response., Author(s): Patrick M. Forde [sup.1] [sup.2] , Valsamo Anagnostou [sup.1] [sup.2] , Zhuoxin Sun [sup.3] [sup.4] , Suzanne E. Dahlberg [sup.5] , Hedy L. Kindler [sup.6] , Noushin Niknafs [sup.1] [...]

Published

2021

2. The genomic landscape of response to EGFR blockade in colorectal cancer

Author

Bertotti, Andrea, Papp, Eniko, Jones, Sian, Adleff, Vilmos, Anagnostou, Valsamo, Lupo, Barbara, Sausen, Mark, Phallen, Jillian, Hruban, Carolyn A., Tokheim, Collin, Niknafs, Noushin, Nesselbush, Monica, Lytle, Karli, Sassi, Francesco, Cottino, Francesca, Migliardi, Giorgia, Zanella, Eugenia R., Riberof, Dario, Russolillo, Nadia, Mellano, Alfredo, Muratore, Andrea, Paraluppi, Gianluca, Salizzoni, Mauro, Marsoni, Silvia, Kragh, Michael, Lantto, Johan, Cassingena, Andrea, Li, Qing Kay, Karchin, Rachel, Scharpf, Robert, Sartore-Bianchi, Andrea, Siena, Salvatore, Diaz, Jr., Luis A., Trusolino, Livio, and Velculescu, Victor E.

Subjects

Gene mutations -- Identification and classification -- Health aspects, Drug metabolism -- Genetic aspects, Colorectal cancer -- Genetic aspects -- Care and treatment, Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

Colorectal cancer is the third most common cancer worldwide, with 1.2 million patients diagnosed annually. In late-stage colorectal cancer, the most commonly used targeted therapies are the monoclonal antibodies cetuximab [...]

Published

2015

3. Genomic characterization of malignant progression in neoplastic pancreatic cysts

Author

Pathologie Groep Brosens, Cancer, Pathologie Pathologen staf, Noë, Michaël, Niknafs, Noushin, Fischer, Catherine G, Hackeng, Wenzel M, Beleva Guthrie, Violeta, Hosoda, Waki, Debeljak, Marija, Papp, Eniko, Adleff, Vilmos, White, James R, Luchini, Claudio, Pea, Antonio, Scarpa, Aldo, Butturini, Giovanni, Zamboni, Giuseppe, Castelli, Paola, Hong, Seung-Mo, Yachida, Shinichi, Hiraoka, Nobuyoshi, Gill, Anthony J, Samra, Jaswinder S, Offerhaus, G Johan A, Hoorens, Anne, Verheij, Joanne, Jansen, Casper, Adsay, N Volkan, Jiang, Wei, Winter, Jordan, Albores-Saavedra, Jorge, Terris, Benoit, Thompson, Elizabeth D, Roberts, Nicholas J, Hruban, Ralph H, Karchin, Rachel, Scharpf, Robert B, Brosens, Lodewijk A A, Velculescu, Victor E, Wood, Laura D, Pathologie Groep Brosens, Cancer, Pathologie Pathologen staf, Noë, Michaël, Niknafs, Noushin, Fischer, Catherine G, Hackeng, Wenzel M, Beleva Guthrie, Violeta, Hosoda, Waki, Debeljak, Marija, Papp, Eniko, Adleff, Vilmos, White, James R, Luchini, Claudio, Pea, Antonio, Scarpa, Aldo, Butturini, Giovanni, Zamboni, Giuseppe, Castelli, Paola, Hong, Seung-Mo, Yachida, Shinichi, Hiraoka, Nobuyoshi, Gill, Anthony J, Samra, Jaswinder S, Offerhaus, G Johan A, Hoorens, Anne, Verheij, Joanne, Jansen, Casper, Adsay, N Volkan, Jiang, Wei, Winter, Jordan, Albores-Saavedra, Jorge, Terris, Benoit, Thompson, Elizabeth D, Roberts, Nicholas J, Hruban, Ralph H, Karchin, Rachel, Scharpf, Robert B, Brosens, Lodewijk A A, Velculescu, Victor E, and Wood, Laura D

Published

2020

4. Genome-wide cell-free DNA fragmentation in patients with cancer

Author

Cristiano, Stephen, Leal, Alessandro, Phallen, Jillian, Fiksel, Jacob, Adleff, Vilmos, Bruhm, Daniel C, Jensen, Sarah Østrup, Medina, Jamie E, Hruban, Carolyn, White, James R, Palsgrove, Doreen N, Niknafs, Noushin, Anagnostou, Valsamo, Forde, Patrick, Naidoo, Jarushka, Marrone, Kristen, Brahmer, Julie, Woodward, Brian D, Husain, Hatim, van Rooijen, Karlijn L, Ørntoft, Mai-Britt Worm, Madsen, Anders Husted, van de Velde, Cornelis J H, Verheij, Marcel, Cats, Annemieke, Punt, Cornelis J A, Vink, Geraldine R, van Grieken, Nicole C T, Koopman, Miriam, Fijneman, Remond J A, Johansen, Julia S, Nielsen, Hans Jørgen, Meijer, Gerrit A, Andersen, Claus Lindbjerg, Scharpf, Robert B, Velculescu, Victor E, Cristiano, Stephen, Leal, Alessandro, Phallen, Jillian, Fiksel, Jacob, Adleff, Vilmos, Bruhm, Daniel C, Jensen, Sarah Østrup, Medina, Jamie E, Hruban, Carolyn, White, James R, Palsgrove, Doreen N, Niknafs, Noushin, Anagnostou, Valsamo, Forde, Patrick, Naidoo, Jarushka, Marrone, Kristen, Brahmer, Julie, Woodward, Brian D, Husain, Hatim, van Rooijen, Karlijn L, Ørntoft, Mai-Britt Worm, Madsen, Anders Husted, van de Velde, Cornelis J H, Verheij, Marcel, Cats, Annemieke, Punt, Cornelis J A, Vink, Geraldine R, van Grieken, Nicole C T, Koopman, Miriam, Fijneman, Remond J A, Johansen, Julia S, Nielsen, Hans Jørgen, Meijer, Gerrit A, Andersen, Claus Lindbjerg, Scharpf, Robert B, and Velculescu, Victor E

Published

2019

5. Genome-wide cell-free DNA fragmentation in patients with cancer

Author

Unit Opleiding Aios, Cancer, MS Medische Oncologie, Cristiano, Stephen, Leal, Alessandro, Phallen, Jillian, Fiksel, Jacob, Adleff, Vilmos, Bruhm, Daniel C, Jensen, Sarah Østrup, Medina, Jamie E, Hruban, Carolyn, White, James R, Palsgrove, Doreen N, Niknafs, Noushin, Anagnostou, Valsamo, Forde, Patrick, Naidoo, Jarushka, Marrone, Kristen, Brahmer, Julie, Woodward, Brian D, Husain, Hatim, van Rooijen, Karlijn L, Ørntoft, Mai-Britt Worm, Madsen, Anders Husted, van de Velde, Cornelis J H, Verheij, Marcel, Cats, Annemieke, Punt, Cornelis J A, Vink, Geraldine R, van Grieken, Nicole C T, Koopman, Miriam, Fijneman, Remond J A, Johansen, Julia S, Nielsen, Hans Jørgen, Meijer, Gerrit A, Andersen, Claus Lindbjerg, Scharpf, Robert B, Velculescu, Victor E, Unit Opleiding Aios, Cancer, MS Medische Oncologie, Cristiano, Stephen, Leal, Alessandro, Phallen, Jillian, Fiksel, Jacob, Adleff, Vilmos, Bruhm, Daniel C, Jensen, Sarah Østrup, Medina, Jamie E, Hruban, Carolyn, White, James R, Palsgrove, Doreen N, Niknafs, Noushin, Anagnostou, Valsamo, Forde, Patrick, Naidoo, Jarushka, Marrone, Kristen, Brahmer, Julie, Woodward, Brian D, Husain, Hatim, van Rooijen, Karlijn L, Ørntoft, Mai-Britt Worm, Madsen, Anders Husted, van de Velde, Cornelis J H, Verheij, Marcel, Cats, Annemieke, Punt, Cornelis J A, Vink, Geraldine R, van Grieken, Nicole C T, Koopman, Miriam, Fijneman, Remond J A, Johansen, Julia S, Nielsen, Hans Jørgen, Meijer, Gerrit A, Andersen, Claus Lindbjerg, Scharpf, Robert B, and Velculescu, Victor E

Published

2019

6. 3D genomic mapping reveals multifocality of human pancreatic precancers.

Author

Braxton AM, Kiemen AL, Grahn MP, Forjaz A, Parksong J, Mahesh Babu J, Lai J, Zheng L, Niknafs N, Jiang L, Cheng H, Song Q, Reichel R, Graham S, Damanakis AI, Fischer CG, Mou S, Metz C, Granger J, Liu XD, Bachmann N, Zhu Y, Liu Y, Almagro-Pérez C, Jiang AC, Yoo J, Kim B, Du S, Foster E, Hsu JY, Rivera PA, Chu LC, Liu F, Fishman EK, Yuille A, Roberts NJ, Thompson ED, Scharpf RB, Cornish TC, Jiao Y, Karchin R, Hruban RH, Wu PH, Wirtz D, and Wood LD

Subjects

Adult, Female, Humans, Male, Clone Cells metabolism, Clone Cells pathology, Exome Sequencing, Machine Learning, Mutation, Pancreas anatomy & histology, Pancreas cytology, Pancreas metabolism, Pancreas pathology, Workflow, Disease Progression, Early Detection of Cancer, Oncogenes genetics, Genetic Heterogeneity, Genomics, Imaging, Three-Dimensional, Pancreatic Neoplasms genetics, Pancreatic Neoplasms pathology, Precancerous Conditions genetics, Precancerous Conditions pathology, Single-Cell Analysis

Abstract

Pancreatic intraepithelial neoplasias (PanINs) are the most common precursors of pancreatic cancer, but their small size and inaccessibility in humans make them challenging to study 1 . Critically, the number, dimensions and connectivity of human PanINs remain largely unknown, precluding important insights into early cancer development. Here, we provide a microanatomical survey of human PanINs by analysing 46 large samples of grossly normal human pancreas with a machine-learning pipeline for quantitative 3D histological reconstruction at single-cell resolution. To elucidate genetic relationships between and within PanINs, we developed a workflow in which 3D modelling guides multi-region microdissection and targeted and whole-exome sequencing. From these samples, we calculated a mean burden of 13 PanINs per cm 3 and extrapolated that the normal intact adult pancreas harbours hundreds of PanINs, almost all with oncogenic KRAS hotspot mutations. We found that most PanINs originate as independent clones with distinct somatic mutation profiles. Some spatially continuous PanINs were found to contain multiple KRAS mutations; computational and in situ analyses demonstrated that different KRAS mutations localize to distinct cell subpopulations within these neoplasms, indicating their polyclonal origins. The extensive multifocality and genetic heterogeneity of PanINs raises important questions about mechanisms that drive precancer initiation and confer differential progression risk in the human pancreas. This detailed 3D genomic mapping of molecular alterations in human PanINs provides an empirical foundation for early detection and rational interception of pancreatic cancer., (© 2024. The Author(s), under exclusive licence to Springer Nature Limited.)

Published

2024

7. Multimodal genomic features predict outcome of immune checkpoint blockade in non-small-cell lung cancer.

Author

Anagnostou V, Niknafs N, Marrone K, Bruhm DC, White JR, Naidoo J, Hummelink K, Monkhorst K, Lalezari F, Lanis M, Rosner S, Reuss JE, Smith KN, Adleff V, Rodgers K, Belcaid Z, Rhymee L, Levy B, Feliciano J, Hann CL, Ettinger DS, Georgiades C, Verde F, Illei P, Li QK, Baras AS, Gabrielson E, Brock MV, Karchin R, Pardoll DM, Baylin SB, Brahmer JR, Scharpf RB, Forde PM, and Velculescu VE

Subjects

Biomarkers, Tumor genetics, Humans, Immune Checkpoint Inhibitors pharmacology, Immunotherapy methods, Carcinoma, Non-Small-Cell Lung drug therapy, Lung Neoplasms drug therapy

Abstract

Despite progress in immunotherapy, identifying patients that respond has remained a challenge. Through analysis of whole-exome and targeted sequence data from 5,449 tumors, we found a significant correlation between tumor mutation burden (TMB) and tumor purity, suggesting that low tumor purity tumors are likely to have inaccurate TMB estimates. We developed a new method to estimate a corrected TMB (cTMB) that was adjusted for tumor purity and more accurately predicted outcome to immune checkpoint blockade (ICB). To identify improved predictive markers together with cTMB, we performed whole-exome sequencing for 104 lung tumors treated with ICB. Through comprehensive analyses of sequence and structural alterations, we discovered a significant enrichment in activating mutations in receptor tyrosine kinase (RTK) genes in nonresponding tumors in three immunotherapy treated cohorts. An integrated multivariable model incorporating cTMB, RTK mutations, smoking-related mutational signature and human leukocyte antigen status provided an improved predictor of response to immunotherapy that was independently validated.

Published

2020

8. Genome-wide cell-free DNA fragmentation in patients with cancer.

Author

Cristiano S, Leal A, Phallen J, Fiksel J, Adleff V, Bruhm DC, Jensen SØ, Medina JE, Hruban C, White JR, Palsgrove DN, Niknafs N, Anagnostou V, Forde P, Naidoo J, Marrone K, Brahmer J, Woodward BD, Husain H, van Rooijen KL, Ørntoft MW, Madsen AH, van de Velde CJH, Verheij M, Cats A, Punt CJA, Vink GR, van Grieken NCT, Koopman M, Fijneman RJA, Johansen JS, Nielsen HJ, Meijer GA, Andersen CL, Scharpf RB, and Velculescu VE

Subjects

Case-Control Studies, Cohort Studies, DNA Mutational Analysis, Humans, Machine Learning, Mutation, Neoplasms blood, Neoplasms pathology, Circulating Tumor DNA blood, Circulating Tumor DNA genetics, DNA Fragmentation, Genome, Human genetics, Neoplasms diagnosis, Neoplasms genetics

Abstract

Cell-free DNA in the blood provides a non-invasive diagnostic avenue for patients with cancer 1 . However, characteristics of the origins and molecular features of cell-free DNA are poorly understood. Here we developed an approach to evaluate fragmentation patterns of cell-free DNA across the genome, and found that profiles of healthy individuals reflected nucleosomal patterns of white blood cells, whereas patients with cancer had altered fragmentation profiles. We used this method to analyse the fragmentation profiles of 236 patients with breast, colorectal, lung, ovarian, pancreatic, gastric or bile duct cancer and 245 healthy individuals. A machine learning model that incorporated genome-wide fragmentation features had sensitivities of detection ranging from 57% to more than 99% among the seven cancer types at 98% specificity, with an overall area under the curve value of 0.94. Fragmentation profiles could be used to identify the tissue of origin of the cancers to a limited number of sites in 75% of cases. Combining our approach with mutation-based cell-free DNA analyses detected 91% of patients with cancer. The results of these analyses highlight important properties of cell-free DNA and provide a proof-of-principle approach for the screening, early detection and monitoring of human cancer.

Published

2019