Your search keyword '"P. Andrew Futreal"' showing total 4 results

1. Comparative genomics of high grade neuroendocrine carcinoma of the cervix

Author

Won-Chul Lee, Elizabeth M. Swisher, Preetha Ramalingam, P. Andrew Futreal, Michael Frumovitz, Junya Fujimoto, Robert J. Cardnell, Mario M. Leitao, Jianjun Zhang, R. Tyler Hillman, and Lauren Averett Byers

Subjects

0301 basic medicine, medicine.medical_treatment, Cancer Treatment, Uterine Cervical Neoplasms, Squamous Cell Lung Carcinoma, Cervix Uteri, medicine.disease_cause, Cervix, Lung and Intrathoracic Tumors, Targeted therapy, Cohort Studies, Small Cell Lung Cancer, 0302 clinical medicine, Basic Cancer Research, GTP-Binding Protein alpha Subunits, Gs, Medicine and Health Sciences, Cervical cancer, Multidisciplinary, Neuroendocrine carcinoma of the cervix, biology, Squamous Cell Carcinomas, Genomics, Middle Aged, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Medicine, Female, KRAS, Anatomy, Genital Anatomy, Research Article, Adult, DNA Copy Number Variations, Class I Phosphatidylinositol 3-Kinases, Science, Carcinomas, Small-cell carcinoma, Proto-Oncogene Proteins p21(ras), 03 medical and health sciences, Cancer Genomics, Genomic Medicine, Exome Sequencing, Chromogranins, Genetics, medicine, GNAS complex locus, Carcinoma, Humans, business.industry, Reproductive System, Cancers and Neoplasms, Biology and Life Sciences, Computational Biology, Comparative Genomics, medicine.disease, Carcinoma, Neuroendocrine, 030104 developmental biology, Mutation, Cancer research, biology.protein, Somatic Mutation, Tumor Suppressor Protein p53, business

Abstract

In order to improve treatment selection for high grade neuroendocrine carcinomas of the cervix (NECC), we performed a comparative genomic analysis between this rare tumor type and other cervical cancer types, as well as extra-cervical neuroendocrine small cell carcinomas of the lung and bladder. We performed whole exome sequencing on fresh-frozen tissue from 15 NECCs and matched normal tissue. We then identified mutations and copy number variants using standard analysis pipelines. Published mutation tables from cervical cancers and extra-cervical small cell carcinomas were used for comparative analysis. Descriptive statistical methods were used and a two-sided threshold of P < .05 was used for significance. In the NECC cohort, we detected a median of 1.7 somatic mutations per megabase (range 1.0–20.9). PIK3CA p.E545K mutations were the most frequency observed oncogenic mutation (4/15 tumors, 27%). Activating MAPK pathway mutations in KRAS (p.G12D) and GNAS (p.R201C) co-occurred in two tumors (13%). In total we identified PI3-kinase or MAPK pathway activating mutations in 67% of NECC. When compared to NECC, lung and bladder small cell carcinomas exhibited a statistically significant higher rate of coding mutations (P < .001 for lung; P = .001 for bladder). Mutation of TP53 was uncommon in NECC (13%) and was more frequent in both lung (103 of 110 tumors [94%], P < .001) and bladder (18 of 19 tumors [95%], P < .001) small cell carcinoma. These comparative genomics data suggest that NECC may be genetically more similar to common cervical cancer subtypes than to extra-cervical small cell neuroendocrine carcinomas of the lung and bladder. These results may have implications for the selection of cytotoxic and targeted therapy regimens for this rare disease.

Published

2020

2. Amplification and Overexpression of Hsa-miR-30b, Hsa-miR-30d and KHDRBS3 at 8q24.22-q24.23 in Medulloblastoma

Author

David W. Ellison, Steven C. Clifford, Sarra Ryan, Graham R. Bignell, David J. Elliott, Yuan-Yuan Lu, Simon Bailey, and P. Andrew Futreal

Subjects

Male, lcsh:Medicine, RNA-binding protein, In situ hybridization, Bioinformatics, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Pathogenesis, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, microRNA, Gene duplication, medicine, Humans, lcsh:Science, Gene, In Situ Hybridization, Fluorescence, 030304 developmental biology, Oncology/Neuro-Oncology, Medulloblastoma, 0303 health sciences, Multidisciplinary, business.industry, Brain Neoplasms, lcsh:R, Gene targeting, RNA-Binding Proteins, medicine.disease, 3. Good health, MicroRNAs, Oncology, 030220 oncology & carcinogenesis, Cancer research, lcsh:Q, Oncology/Pediatric Oncology, Female, business, Research Article, Chromosomes, Human, Pair 8

Abstract

Background Medulloblastoma is the most common malignant brain tumour of childhood. The identification of critical genes involved in its pathogenesis will be central to advances in our understanding of its molecular basis, and the development of improved therapeutic approaches. Methodology/Principal Findings We performed a SNP-array based genome-wide copy number analysis in medulloblastoma cell lines, to identify regions of genomic amplification and homozygous deletion, which may harbour critical disease genes. A series of novel and established medulloblastoma defects were detected (MYC amplification (n = 4), 17q21.31 high-level gain (n = 1); 9p21.1–p21.3 (n = 1) and 6q23.1 (n = 1) homozygous deletion). Most notably, a novel recurrent region of genomic amplification at 8q24.22–q24.23 was identified (n = 2), and selected for further investigation. Additional analysis by interphase fluorescence in situ hybridisation (iFISH), PCR-based mapping and SNP-array revealed this novel amplification at 8q24.22–q24.23 is independent of MYC amplification at 8q24.21, and is unique to medulloblastoma in over 800 cancer cell lines assessed from different tumour types, suggesting it contains key genes specifically involved in medulloblastoma development. Detailed mapping identified a 3Mb common minimal region of amplification harbouring 3 coding genes (ZFAT1, LOC286094, KHDRBS3) and two genes encoding micro-RNAs (hsa-miR-30b, hsa-miR-30d). Of these, only expression of hsa-miR-30b, hsa-miR-30d and KHDRBS3 correlated with copy number status, and all three of these transcripts also displayed evidence of elevated expression in sub-sets of primary medulloblastomas, measured relative to the normal cerebellum. Conclusions/Significance These data implicate hsa-miR-30b, hsa-miR-30d and KHDRBS3 as putative oncogenic target(s) of a novel recurrent medulloblastoma amplicon at 8q24.22–q24.23. Our findings suggest critical roles for these genes in medulloblastoma development, and further support the contribution of micro-RNA species to medulloblastoma pathogenesis.

Published

2009

3. Comparative genomics of high grade neuroendocrine carcinoma of the cervix.

Author

R Tyler Hillman, Robert Cardnell, Junya Fujimoto, Won-Chul Lee, Jianjun Zhang, Lauren A Byers, Preetha Ramalingam, Mario Leitao, Elizabeth Swisher, P Andrew Futreal, and Michael Frumovitz

Subjects

Medicine, Science

Abstract

In order to improve treatment selection for high grade neuroendocrine carcinomas of the cervix (NECC), we performed a comparative genomic analysis between this rare tumor type and other cervical cancer types, as well as extra-cervical neuroendocrine small cell carcinomas of the lung and bladder. We performed whole exome sequencing on fresh-frozen tissue from 15 NECCs and matched normal tissue. We then identified mutations and copy number variants using standard analysis pipelines. Published mutation tables from cervical cancers and extra-cervical small cell carcinomas were used for comparative analysis. Descriptive statistical methods were used and a two-sided threshold of P < .05 was used for significance. In the NECC cohort, we detected a median of 1.7 somatic mutations per megabase (range 1.0-20.9). PIK3CA p.E545K mutations were the most frequency observed oncogenic mutation (4/15 tumors, 27%). Activating MAPK pathway mutations in KRAS (p.G12D) and GNAS (p.R201C) co-occurred in two tumors (13%). In total we identified PI3-kinase or MAPK pathway activating mutations in 67% of NECC. When compared to NECC, lung and bladder small cell carcinomas exhibited a statistically significant higher rate of coding mutations (P < .001 for lung; P = .001 for bladder). Mutation of TP53 was uncommon in NECC (13%) and was more frequent in both lung (103 of 110 tumors [94%], P < .001) and bladder (18 of 19 tumors [95%], P < .001) small cell carcinoma. These comparative genomics data suggest that NECC may be genetically more similar to common cervical cancer subtypes than to extra-cervical small cell neuroendocrine carcinomas of the lung and bladder. These results may have implications for the selection of cytotoxic and targeted therapy regimens for this rare disease.

Published

2020

4. Amplification and overexpression of Hsa-miR-30b, Hsa-miR-30d and KHDRBS3 at 8q24.22-q24.23 in medulloblastoma.

Author

Yuan Lu, Sarra L Ryan, David J Elliott, Graham R Bignell, P Andrew Futreal, David W Ellison, Simon Bailey, and Steven C Clifford

Subjects

Medicine, Science

Abstract

Medulloblastoma is the most common malignant brain tumour of childhood. The identification of critical genes involved in its pathogenesis will be central to advances in our understanding of its molecular basis, and the development of improved therapeutic approaches.We performed a SNP-array based genome-wide copy number analysis in medulloblastoma cell lines, to identify regions of genomic amplification and homozygous deletion, which may harbour critical disease genes. A series of novel and established medulloblastoma defects were detected (MYC amplification (n = 4), 17q21.31 high-level gain (n = 1); 9p21.1-p21.3 (n = 1) and 6q23.1 (n = 1) homozygous deletion). Most notably, a novel recurrent region of genomic amplification at 8q24.22-q24.23 was identified (n = 2), and selected for further investigation. Additional analysis by interphase fluorescence in situ hybridisation (iFISH), PCR-based mapping and SNP-array revealed this novel amplification at 8q24.22-q24.23 is independent of MYC amplification at 8q24.21, and is unique to medulloblastoma in over 800 cancer cell lines assessed from different tumour types, suggesting it contains key genes specifically involved in medulloblastoma development. Detailed mapping identified a 3Mb common minimal region of amplification harbouring 3 coding genes (ZFAT1, LOC286094, KHDRBS3) and two genes encoding micro-RNAs (hsa-miR-30b, hsa-miR-30d). Of these, only expression of hsa-miR-30b, hsa-miR-30d and KHDRBS3 correlated with copy number status, and all three of these transcripts also displayed evidence of elevated expression in sub-sets of primary medulloblastomas, measured relative to the normal cerebellum.These data implicate hsa-miR-30b, hsa-miR-30d and KHDRBS3 as putative oncogenic target(s) of a novel recurrent medulloblastoma amplicon at 8q24.22-q24.23. Our findings suggest critical roles for these genes in medulloblastoma development, and further support the contribution of micro-RNA species to medulloblastoma pathogenesis.

Published

2009