Your search keyword '"Ahmet Zehir"' showing total 10 results

1. The context-specific role of germline pathogenicity in tumorigenesis

Author

Marc Ladanyi, Gowtham Jayakumaran, Karen Cadoo, Ahmet Zehir, Philip Jonsson, Xiang Li, Jason Hwee, Meera Prasad, Michael Walsh, Jinru Shia, Allison Richards, Alexander V Penson, Aijazuddin Syed, Joseph Vijai, Roy Cambria, Michael F. Berger, Barry S. Taylor, Mark E. Robson, Semanti Mukherjee, Chaitanya Bandlamudi, Jianjiong Gao, Christopher J. Fong, Ozge Ceyhan-Birsoy, Maria I. Carlo, Liying Zhang, David M. Hyman, Preethi Srinivasan, Ino de Bruijn, Diana Mandelker, Jesse Galle, Selcuk Onur Sumer, Craig M. Bielski, Kenneth Offit, Shweta S. Chavan, Nikolaus Schultz, Yelena Kemel, David B. Solit, and Zsofia K. Stadler

Subjects

Heterozygote, DNA Copy Number Variations, Carcinogenesis, Somatic cell, Biology, medicine.disease_cause, DNA Mismatch Repair, Medical and Health Sciences, Germline, Rare Diseases, Clinical Research, Neoplasms, Genetics, medicine, Humans, 2.1 Biological and endogenous factors, Genetic Predisposition to Disease, Aetiology, Allele, Gene, Germ-Line Mutation, Cancer, Human Genome, Biological Sciences, medicine.disease, Phenotype, Penetrance, Developmental Biology

Abstract

Human cancers arise from environmental, heritable and somatic factors, but how these mechanisms interact in tumorigenesis is poorly understood. Studying 17,152 prospectively sequenced patients with cancer, we identified pathogenic germline variants in cancer predisposition genes, and assessed their zygosity and co-occurring somatic alterations in the concomitant tumors. Two major routes to tumorigenesis were apparent. In carriers of pathogenic germline variants in high-penetrance genes (5.1% overall), lineage-dependent patterns of biallelic inactivation led to tumors exhibiting mechanism-specific somatic phenotypes and fewer additional somatic oncogenic drivers. Nevertheless, 27% of cancers in these patients, and most tumors in patients with pathogenic germline variants in lower-penetrance genes, lacked particular hallmarks of tumorigenesis associated with the germline allele. The dependence of tumors on pathogenic germline variants is variable and often dictated by both penetrance and lineage, a finding with implications for clinical management. A study of 17,152 patients with cancer identified pathogenic germline variants in cancer predisposition genes. Although tumors showed biallelic inactivation for high-penetrance genes, this was not the case in most patients with pathogenic variants in low-penetrance genes, suggesting alternative routes to tumorigenesis.

Published

2021

2. Diagnostic yield and clinical relevance of expanded genetic testing for cancer patients

Author

Ozge Ceyhan-Birsoy, Gowtham Jayakumaran, Yelena Kemel, Maksym Misyura, Umut Aypar, Sowmya Jairam, Ciyu Yang, Yirong Li, Nikita Mehta, Anna Maio, Angela Arnold, Erin Salo-Mullen, Margaret Sheehan, Aijazuddin Syed, Michael Walsh, Maria Carlo, Mark Robson, Kenneth Offit, Marc Ladanyi, Jorge S. Reis-Filho, Zsofia K. Stadler, Liying Zhang, Alicia Latham, Ahmet Zehir, and Diana Mandelker

Subjects

Cohort Studies, Male, Genetics, Humans, Prostatic Neoplasms, Molecular Medicine, Genetic Predisposition to Disease, Genetic Testing, Colorectal Neoplasms, Molecular Biology, Germ-Line Mutation, Genetics (clinical)

Abstract

Background Genetic testing (GT) for hereditary cancer predisposition is traditionally performed on selected genes based on established guidelines for each cancer type. Recently, expanded GT (eGT) using large hereditary cancer gene panels uncovered hereditary predisposition in a greater proportion of patients than previously anticipated. We sought to define the diagnostic yield of eGT and its clinical relevance in a broad cancer patient population over a 5-year period. Methods A total of 17,523 cancer patients with a broad range of solid tumors, who received eGT at Memorial Sloan Kettering Cancer Center between July 2015 to April 2020, were included in the study. The patients were unselected for current GT criteria such as cancer type, age of onset, and/or family history of disease. The diagnostic yield of eGT was determined for each cancer type. For 9187 patients with five common cancer types frequently interrogated for hereditary predisposition (breast, colorectal, ovarian, pancreatic, and prostate cancer), the rate of pathogenic/likely pathogenic (P/LP) variants in genes that have been associated with each cancer type was analyzed. The clinical implications of additional findings in genes not known to be associated with a patients’ cancer type were investigated. Results 16.7% of patients in a broad cancer cohort had P/LP variants in hereditary cancer predisposition genes identified by eGT. The diagnostic yield of eGT in patients with breast, colorectal, ovarian, pancreatic, and prostate cancer was 17.5%, 15.3%, 24.2%, 19.4%, and 15.9%, respectively. Additionally, 8% of the patients with five common cancers had P/LP variants in genes not known to be associated with the patient’s current cancer type, with 0.8% of them having such a variant that confers a high risk for another cancer type. Analysis of clinical and family histories revealed that 74% of patients with variants in genes not associated with their current cancer type but which conferred a high risk for another cancer did not meet the current GT criteria for the genes harboring these variants. One or more variants of uncertain significance were identified in 57% of the patients. Conclusions Compared to targeted testing approaches, eGT can increase the yield of detection of hereditary cancer predisposition in patients with a range of tumors, allowing opportunities for enhanced surveillance and intervention. The benefits of performing eGT should be weighed against the added number of VUSs identified with this approach.

Published

2022

3. Clinical sequencing of soft tissue and bone sarcomas delineates diverse genomic landscapes and potential therapeutic targets

Author

Benjamin A. Nacev, Francisco Sanchez-Vega, Shaleigh A. Smith, Cristina R. Antonescu, Evan Rosenbaum, Hongyu Shi, Cerise Tang, Nicholas D. Socci, Satshil Rana, Rodrigo Gularte-Mérida, Ahmet Zehir, Mrinal M. Gounder, Timothy G. Bowler, Anisha Luthra, Bhumika Jadeja, Azusa Okada, Jonathan A. Strong, Jake Stoller, Jason E. Chan, Ping Chi, Sandra P. D’Angelo, Mark A. Dickson, Ciara M. Kelly, Mary Louise Keohan, Sujana Movva, Katherine Thornton, Paul A. Meyers, Leonard H. Wexler, Emily K. Slotkin, Julia L. Glade Bender, Neerav N. Shukla, Martee L. Hensley, John H. Healey, Michael P. La Quaglia, Kaled M. Alektiar, Aimee M. Crago, Sam S. Yoon, Brian R. Untch, Sarah Chiang, Narasimhan P. Agaram, Meera R. Hameed, Michael F. Berger, David B. Solit, Nikolaus Schultz, Marc Ladanyi, Samuel Singer, and William D. Tap

Subjects

Osteosarcoma, Multidisciplinary, Humans, General Physics and Astronomy, Bone Neoplasms, Sarcoma, Soft Tissue Neoplasms, Genomics, General Chemistry, General Biochemistry, Genetics and Molecular Biology

Abstract

The genetic, biologic, and clinical heterogeneity of sarcomas poses a challenge for the identification of therapeutic targets, clinical research, and advancing patient care. Because there are > 100 sarcoma subtypes, in-depth genetic studies have focused on one or a few subtypes. Herein, we report a comparative genetic analysis of 2,138 sarcomas representing 45 pathological entities. This cohort is prospectively analyzed using targeted sequencing to characterize subtype-specific somatic alterations in targetable pathways, rates of whole genome doubling, mutational signatures, and subtype-agnostic genomic clusters. The most common alterations are in cell cycle control and TP53, receptor tyrosine kinases/PI3K/RAS, and epigenetic regulators. Subtype-specific associations include TERT amplification in intimal sarcoma and SWI/SNF alterations in uterine adenosarcoma. Tumor mutational burden, while low compared to other cancers, varies between and within subtypes. This resource will improve sarcoma models, motivate studies of subtype-specific alterations, and inform investigations of genetic factors and their correlations with treatment response.

Published

2022

4. Clonal hematopoiesis is associated with risk of severe Covid-19

Author

Youngil Koh, Ross L. Levine, Marc Ladanyi, Eu Suk Kim, Choong Hyun Sun, Kelly L. Bolton, Mini Kamboj, Michael J. Rauh, Hong Bin Kim, Hogune Im, Michael F. Berger, Michael B. Foote, Han Song, Ji Yeon Lee, Minal Patel, Anton Safonov, Lior Z. Braunstein, Elli Papaemmanuil, Chang Kyung Kang, Kaitlyn Tkachuk, Nam Joong Kim, Myoung Don Oh, Brian J. Wiley, Ireaneus C. Chan, Larry Norton, Andriy Derkach, Philip Awadalla, Justin Jee, Erika Gedvilaite, Ahmet Zehir, Sugyeong Kim, Vijai Joseph, Joon Ho Moon, Kenneth Offit, Luis A. Diaz, N. Esther Babady, Melissa S. Pessin, Wan Beom Park, Pyoeng Gyun Choe, Ryan Ptashkin, Teng Gao, Mitchell J. Machiela, Pradeep Natarajan, Kyoung Ho Song, and Jongtak Jung

Subjects

Male, Oncology, Somatic cell, General Physics and Astronomy, Disease, medicine.disease_cause, Severity of Illness Index, Cohort Studies, Risk Factors, Neoplasms, Child, Aged, 80 and over, Multidisciplinary, biology, Streptococcus, musculoskeletal, neural, and ocular physiology, Genomics, Middle Aged, Clostridium difficile, Haematopoiesis, Child, Preschool, Infectious diseases, Female, Clonal Hematopoiesis, Cohort study, Adult, medicine.medical_specialty, Adolescent, Coronavirus disease 2019 (COVID-19), Science, macromolecular substances, Article, General Biochemistry, Genetics and Molecular Biology, Internal medicine, Severity of illness, medicine, Humans, Progenitor cell, Aged, SARS-CoV-2, business.industry, Infant, Newborn, COVID-19, Infant, General Chemistry, biology.organism_classification, Hematopoietic Stem Cells, nervous system, Enterococcus, Immunology, Mutation, business

Abstract

Acquired somatic mutations in hematopoietic stem and progenitor cells (clonal hematopoiesis or CH) are associated with advanced age, increased risk of cardiovascular and malignant diseases, and decreased overall survival. These adverse sequelae may be mediated by altered inflammatory profiles observed in patients with CH. A pro-inflammatory immunologic profile is also associated with worse outcomes of certain infections, including SARS-CoV-2 and its associated disease Covid-19. Whether CH predisposes to severe Covid-19 or other infections is unknown. Among 525 individuals with Covid-19 from Memorial Sloan Kettering (MSK) and the Korean Clonal Hematopoiesis (KoCH) consortia, we show that CH is associated with severe Covid-19 outcomes (OR = 1.85, 95%=1.15–2.99, p = 0.01), in particular CH characterized by non-cancer driver mutations (OR = 2.01, 95% CI = 1.15–3.50, p = 0.01). We further explore the relationship between CH and risk of other infections in 14,211 solid tumor patients at MSK. CH is significantly associated with risk of Clostridium Difficile (HR = 2.01, 95% CI: 1.22–3.30, p = 6×10−3) and Streptococcus/Enterococcus infections (HR = 1.56, 95% CI = 1.15–2.13, p = 5×10−3). These findings suggest a relationship between CH and risk of severe infections that warrants further investigation., Clonal haematopoiesis (CH) has been associated with altered inflammatory profiles and increased risk of cardiovascular and malignant diseases. Here, the authors analyze patient data from two different cohorts and show that CH is associated with severe infections and severe Covid19.

Published

2021

5. Tumour lineage shapes BRCA-mediated phenotypes

Author

Marc Ladanyi, Ozge Birsoy, David M. Hyman, Nikolaus Schultz, Agnes Viale, S. Duygu Selcuklu, Ezra Y. Rosen, José Baselga, Mark E. Robson, Allison Richards, Kenneth Offit, Michael L. Cheng, Preethi Srinivasan, Wassim Abida, Barry S. Taylor, Craig M. Bielski, Noah D. Friedman, Shweta S. Chavan, Philip Jonsson, Liying Zhang, Michael F. Berger, Diana Mandelker, Chaitanya Bandlamudi, Nancy Bouvier, Eileen M. O'Reilly, Ahmet Zehir, Zsofia K. Stadler, Nicholas D. Socci, Mark T.A. Donoghue, David B. Solit, and Howard I. Scher

Subjects

0301 basic medicine, Heterozygote, Lineage (genetic), endocrine system diseases, Zygote, Genes, BRCA2, Genes, BRCA1, Poly(ADP-ribose) Polymerase Inhibitors, Biology, medicine.disease_cause, Germline, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, medicine, Humans, Cell Lineage, Allele, skin and connective tissue diseases, Alleles, Mutation, Multidisciplinary, Cancer, medicine.disease, Penetrance, Phenotype, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, Haploinsufficiency, Carcinogenesis

Abstract

Mutations in BRCA1 and BRCA2 predispose individuals to certain cancers1–3, and disease-specific screening and preventative strategies have reduced cancer mortality in affected patients4,5. These classical tumour-suppressor genes have tumorigenic effects associated with somatic biallelic inactivation, although haploinsufficiency may also promote the formation and progression of tumours6,7. Moreover, BRCA1/2-mutant tumours are often deficient in the repair of double-stranded DNA breaks by homologous recombination8–13, and consequently exhibit increased therapeutic sensitivity to platinum-containing therapy and inhibitors of poly-(ADP-ribose)-polymerase (PARP)14,15. However, the phenotypic and therapeutic relevance of mutations in BRCA1 or BRCA2 remains poorly defined in most cancer types. Here we show that in the 2.7% and 1.8% of patients with advanced-stage cancer and germline pathogenic or somatic loss-of-function alterations in BRCA1/2, respectively, selective pressure for biallelic inactivation, zygosity-dependent phenotype penetrance, and sensitivity to PARP inhibition were observed only in tumour types associated with increased heritable cancer risk in BRCA1/2 carriers (BRCA-associated cancer types). Conversely, among patients with non-BRCA-associated cancer types, most carriers of these BRCA1/2 mutation types had evidence for tumour pathogenesis that was independent of mutant BRCA1/2. Overall, mutant BRCA is an indispensable founding event for some tumours, but in a considerable proportion of other cancers, it appears to be biologically neutral—a difference predominantly conditioned by tumour lineage—with implications for disease pathogenesis, screening, design of clinical trials and therapeutic decision-making. Analysis of more than 17,000 tumours suggests that the contribution of germline and somatic mutations in the BRCA1 and BRCA2 genes to oncogenesis depends on tumour lineage.

Published

2019

6. Tumor fraction-guided cell-free DNA profiling in metastatic solid tumor patients

Author

Maha Shady, Nicholas D. Socci, Julie L. Yang, Helen Won, Maria E. Arcila, Marc Ladanyi, Gopa Iyer, Michael L. Cheng, Xiaohong Jing, Hongxin Zhang, Jonathan Rosenberg, Ahmet Zehir, Pedram Razavi, Kety Huberman, Agnes Viale, Fanli Meng, Darren R. Feldman, Debyani Chakravarty, Michael F. Berger, Venkatraman E. Seshan, S. Duygu Selcuklu, Dennis Stephens, Wassim Abida, Maysun Hasan, Dana E. Rathkopf, Dean F. Bajorin, Erika Gedvilaite, Dana W.Y. Tsui, Preethi Srinivasan, Howard I. Scher, David B. Solit, Juber Patel, Samuel Funt, Ryma Benayed, Ian Johnson, Bob T. Li, and Brian Houck-Loomis

Subjects

DNA Copy Number Variations, Somatic cell, QH426-470, Noninvasive, Molecular diagnostic, Circulating Tumor DNA, Neoplasms, Exome Sequencing, Biomarkers, Tumor, Genetics, medicine, Sequencing, Humans, Liquid biopsy, Molecular Biology, Gene, Genetics (clinical), Exome sequencing, Cancer, Whole genome sequencing, Whole Genome Sequencing, business.industry, Research, Genomics, Assay sensitivity, medicine.disease, Plasma DNA, ROC Curve, Cell-free fetal DNA, Mutation, Cancer research, Medicine, Molecular Medicine, business

Abstract

BackgroundCell-free DNA (cfDNA) profiling is increasingly used to guide cancer care, yet mutations are not always identified. The ability to detect somatic mutations in plasma depends on both assay sensitivity and the fraction of circulating DNA in plasma that is tumor-derived (i.e., cfDNA tumor fraction). We hypothesized that cfDNA tumor fraction could inform the interpretation of negative cfDNA results and guide the choice of subsequent assays of greater genomic breadth or depth.MethodsPlasma samples collected from 118 metastatic cancer patients were analyzed with cf-IMPACT, a modified version of the FDA-authorized MSK-IMPACT tumor test that can detect genomic alterations in 410 cancer-associated genes. Shallow whole genome sequencing (sWGS) was also performed in the same samples to estimate cfDNA tumor fraction based on genome-wide copy number alterations usingz-score statistics. Plasma samples with no somatic alterations detected by cf-IMPACT were triaged based on sWGS-estimated tumor fraction for analysis with either a less comprehensive but more sensitive assay (MSK-ACCESS) or broader whole exome sequencing (WES).ResultscfDNA profiling using cf-IMPACT identified somatic mutations in 55/76 (72%) patients for whom MSK-IMPACT tumor profiling data were available. A significantly higher concordance of mutational profiles and tumor mutational burden (TMB) was observed between plasma and tumor profiling for plasma samples with a high tumor fraction (z-score≥5). In the 42 patients from whom tumor data was not available, cf-IMPACT identified mutations in 16/42 (38%). In total, cf-IMPACT analysis of plasma revealed mutations in 71/118 (60%) patients, with clinically actionable alterations identified in 30 (25%), including therapeutic targets of FDA-approved drugs. Of the 47 samples without alterations detected and low tumor fraction (z-scorez-score≥5) were analyzed by WES, which identified mutational signatures and alterations in potential oncogenic drivers not covered by the cf-IMPACT panel. Overall, we identified mutations in 90/118 (76%) patients in the entire cohort using the three complementary plasma profiling approaches.ConclusionscfDNA tumor fraction can inform the interpretation of negative cfDNA results and guide the selection of subsequent sequencing platforms that are most likely to identify clinically-relevant genomic alterations.

Published

2021

7. A quick guide for clinical oncology

Author

Ahmet Zehir and Michael F. Berger

Subjects

Clinical Oncology, Set (abstract data type), Cancer Research, Oncology, Computer science, Interpretation (philosophy), medicine, Cancer, Molecular Profile, Computational biology, medicine.disease, Selection (genetic algorithm)

Abstract

Clinical interpretation of cancer genomes for therapy selection and clinical hypothesis generation is an urgent and complex endeavor. A new study brings together a diverse set of data sources to automatically prioritize first- and second-order genomic alterations to provide a meaningful set of interpretations based on a patient’s molecular profile.

Published

2021

8. Mutational landscape of metastatic cancer revealed from prospective clinical sequencing of 10,000 patients

Author

Helen Won, James J. Harding, David S. Klimstra, Andrea Cercek, Nitya Raj, Emmet Jordan, Darren R. Feldman, Michael F. Berger, Barry S. Taylor, Meera Hameed, Jacklyn Casanova, Jesse Galle, Meera Prasad, Sumit Middha, Pedram Razavi, Philip Jonsson, Jaclyn F. Hechtman, Ritika Kundra, David B. Solit, Yelena Y. Janjigian, Jonathan A. Coleman, Lisa Stewart, Antonio Omuro, Stacy B. Thomas, Anoop Balakrishnan Rema, Snjezana Dogan, Preethi Srinivasan, Ryan Ptashkin, Dara S. Ross, Mrinal M. Gounder, Bernard H. Bochner, Dalicia N. Reales, Hikmat Al-Ahmadie, Michael H. Eubank, Hsiao-Wei Chen, Mustafa H Syed, Donavan T. Cheng, Jinjuan Yao, Gowtham Jayakumaran, Ryma Benayed, David M. Hyman, Deborah DeLair, Howard I. Scher, Sean M. Devlin, Justyna Sadowska, Rona Yaeger, Anna M. Varghese, Matthew D. Hellmann, Matthew T. Chang, Zachary J. Heins, José Baselga, Tara Soumerai, Alexander N. Shoushtari, Ahmet Zehir, Alison M. Schram, Debyani Chakravarty, Efsevia Vakiani, Leonard B. Saltz, Maria E. Arcila, Gregory J. Riely, Gopa Iyer, Ruben Bacares, Tessara Baldi, Hyunjae R. Kim, Robert Durany, Sarah Phillips, Maeve A. Lowery, Mark E. Robson, A. Ari Hakimi, Niedzica Camacho, Jiaojiao Wang, Khedoudja Nafa, Hongxin Zhang, Marc Ladanyi, Alexander V Penson, Iwona Kiecka, Aijazuddin Syed, Jianjiong Gao, Jonathan Wills, Raghu Chandramohan, Nikolaus Schultz, Kerry Mullaney, Laetitia Borsu, Diana Mandelker, Julie B Son, Wassim Abida, Ciara Marie Kelly, Benjamin Gross, Adam Abeshouse, Roy Cambria, Luc G. T. Morris, Neerav Shukla, Paul Sabbatini, Zhen Y Liu, Ronak Shah, Anna Razumova, Abhinita Mohanty, Stuart Gardos, David Barron, and Angelica Ochoa

Subjects

Male, 0301 basic medicine, Sequence analysis, Genomics, Computational biology, Biology, Gene mutation, Bioinformatics, General Biochemistry, Genetics and Molecular Biology, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Biomarkers, Tumor, Data Mining, Humans, Prospective Studies, Neoplasm Metastasis, Prospective cohort study, Gene, High-Throughput Nucleotide Sequencing, DNA, Neoplasm, Sequence Analysis, DNA, General Medicine, 3. Good health, Clinical trial, 030104 developmental biology, 030220 oncology & carcinogenesis, Mutation, Feasibility Studies, Female, Normal sequence, Cohort study

Abstract

Tumor molecular profiling is a fundamental component of precision oncology, enabling the identification of genomic alterations in genes and pathways that can be targeted therapeutically. The existence of recurrent targetable alterations across distinct histologically defined tumor types, coupled with an expanding portfolio of molecularly targeted therapies, demands flexible and comprehensive approaches to profile clinically relevant genes across the full spectrum of cancers. We established a large-scale, prospective clinical sequencing initiative using a comprehensive assay, MSK-IMPACT, through which we have compiled tumor and matched normal sequence data from a unique cohort of more than 10,000 patients with advanced cancer and available pathological and clinical annotations. Using these data, we identified clinically relevant somatic mutations, novel noncoding alterations, and mutational signatures that were shared by common and rare tumor types. Patients were enrolled on genomically matched clinical trials at a rate of 11%. To enable discovery of novel biomarkers and deeper investigation into rare alterations and tumor types, all results are publicly accessible.

Published

2017

9. Universal screening for microsatellite instability in colorectal cancer in the clinical genomics era: new recommendations, methods, and considerations

Author

Jaclyn F. Hechtman, Marc Ladanyi, Martin R. Weiser, Jinru Shia, Efsevia Vakiani, David S. Klimstra, Ahmet Zehir, Zsofia K. Stadler, Leonard B. Saltz, Sumit Middha, and Michael F. Berger

Subjects

0301 basic medicine, Cancer Research, Colorectal cancer, Genomics, Biology, Bioinformatics, DNA Mismatch Repair, DNA sequencing, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Humans, Genetics (clinical), Clinical genomics, High-Throughput Nucleotide Sequencing, Microsatellite instability, medicine.disease, Lynch syndrome, Human genetics, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Microsatellite Instability, DNA mismatch repair, Colorectal Neoplasms

Published

2017

10. Author Correction: Tumour lineage shapes BRCA-mediated phenotypes

Author

Kenneth Offit, Ezra Y. Rosen, Marc Ladanyi, Nikolaus Schultz, Liying Zhang, Mark E. Robson, Philip Jonsson, Michael L. Cheng, Ahmet Zehir, David B. Solit, David M. Hyman, Chaitanya Bandlamudi, Michael F. Berger, Eileen M. O'Reilly, José Baselga, Nicholas D. Socci, Mark T.A. Donoghue, Noah D. Friedman, Zsofia K. Stadler, Agnes Viale, Allison Richards, Preethi Srinivasan, Nancy Bouvier, Wassim Abida, Howard I. Scher, Diana Mandelker, Ozge Birsoy, Craig M. Bielski, Shweta S. Chavan, Barry S. Taylor, and S. Duygu Selcuklu

Subjects

Genetics, Multidisciplinary, Lineage (genetic), Biology, Phenotype

Published

2019