Your search keyword '"Chin SF"' showing total 6 results

1. Integration of genomic, transcriptomic and proteomic data identifies two biologically distinct subtypes of invasive lobular breast cancer

Author

Michaut, M (author), Chin, SF (author), Majewski, I (author), Severson, TM (author), Bismeijer, T (author), de Koning, L (author), Peeters, JK (author), Schouten, PC (author), Rueda, OM (author), Bosma, AJ (author), Wessels, L.F.A. (author), Michaut, M (author), Chin, SF (author), Majewski, I (author), Severson, TM (author), Bismeijer, T (author), de Koning, L (author), Peeters, JK (author), Schouten, PC (author), Rueda, OM (author), Bosma, AJ (author), and Wessels, L.F.A. (author)

Abstract

Invasive lobular carcinoma (ILC) is the second most frequently occurring histological breast cancer subtype after invasive ductal carcinoma (IDC), accounting for around 10% of all breast cancers. The molecular processes that drive the development of ILC are still largely unknown. We have performed a comprehensive genomic, transcriptomic and proteomic analysis of a large ILC patient cohort and present here an integrated molecular portrait of ILC. Mutations in CDH1 and in the PI3K pathway are the most frequent molecular alterations in ILC. We identified two main subtypes of ILCs: (i) an immune related subtype with mRNA up-regulation of PD-L1, PD-1 and CTLA-4 and greater sensitivity to DNA-damaging agents in representative cell line models; (ii) a hormone related subtype, associated with Epithelial to Mesenchymal Transition (EMT), and gain of chromosomes 1q and 8q and loss of chromosome 11q. Using the somatic mutation rate and eIF4B protein level, we identified three groups with different clinical outcomes, including a group with extremely good prognosis. We provide a comprehensive overview of the molecular alterations driving ILC and have explored links with therapy response. This molecular characterization may help to tailor treatment of ILC through the application of specific targeted, chemo- and/or immune-therapies., Pattern Recognition and Bioinformatics

Published

2016

2. Integration of genomic, transcriptomic and proteomic data identifies two biologically distinct subtypes of invasive lobular breast cancer

Author

Michaut, M (author), Chin, SF (author), Majewski, I (author), Severson, TM (author), Bismeijer, T (author), de Koning, L (author), Peeters, JK (author), Schouten, PC (author), Rueda, OM (author), Bosma, AJ (author), Wessels, L.F.A. (author), Michaut, M (author), Chin, SF (author), Majewski, I (author), Severson, TM (author), Bismeijer, T (author), de Koning, L (author), Peeters, JK (author), Schouten, PC (author), Rueda, OM (author), Bosma, AJ (author), and Wessels, L.F.A. (author)

Abstract

Invasive lobular carcinoma (ILC) is the second most frequently occurring histological breast cancer subtype after invasive ductal carcinoma (IDC), accounting for around 10% of all breast cancers. The molecular processes that drive the development of ILC are still largely unknown. We have performed a comprehensive genomic, transcriptomic and proteomic analysis of a large ILC patient cohort and present here an integrated molecular portrait of ILC. Mutations in CDH1 and in the PI3K pathway are the most frequent molecular alterations in ILC. We identified two main subtypes of ILCs: (i) an immune related subtype with mRNA up-regulation of PD-L1, PD-1 and CTLA-4 and greater sensitivity to DNA-damaging agents in representative cell line models; (ii) a hormone related subtype, associated with Epithelial to Mesenchymal Transition (EMT), and gain of chromosomes 1q and 8q and loss of chromosome 11q. Using the somatic mutation rate and eIF4B protein level, we identified three groups with different clinical outcomes, including a group with extremely good prognosis. We provide a comprehensive overview of the molecular alterations driving ILC and have explored links with therapy response. This molecular characterization may help to tailor treatment of ILC through the application of specific targeted, chemo- and/or immune-therapies., Pattern Recognition and Bioinformatics

Published

2016

3. Common germline polymorphisms associated with breast cancer-specific survival

Author

Pirie, A, Guo, Q, Kraft, P, Canisius, S, Eccles, DM, Rahman, N, Nevanlinna, H, Chen, C (Christopher Li Hsian), Khan, Salima, Tyrer, J, Bolla, MK, Wang, Q (Qing), Dennis, J, Michailidou, K, Lush, M, Dunning, AM, Shah, M, Czene, K, Darabi, H, Eriksson, M, Lambrechts, D, Weltens, C, Leunen, K, Van Ongeval, C, Nordestgaard, BG, Nielsen, SF, Flyger, H, Rudolph, A, Seibold, P, Flesch-Janys, D, Blomqvist, C, Aittomaaki, K, Fagerholm, R, Muranen, TA, Olsen, JE, Hallberg, E, Vachon, C, Knight, JA, Glendon, G, Mulligan, AM, Broeks, A, Cornelissen, S, Haiman, CA, Henderson, BE, Schumacher, F, Le Marchand, L, Hopper, JL, Tsimiklis, H, Apicella, C, Southey, MC, Cross, SS, Reed, MWR, Giles, GG, Milne, RL, McLean, C, Winqvist, R, Pylkas, K, Jukkola-Vuorinen, A, Grip, M, Hooning, Maartje, Hollestelle, Antoinette, Martens, John, van den Ouweland, Ans, Marme, F, Schneeweiss, A, Yang, RX, Burwinkel, B, Figueroa, J, Chanock, SJ, Lissowska, J, Sawyer, EJ, Tomlinson, I, Kerin, MJ, Miller, N, Brenner, H, Butterbach, K, Holleczek, B, Kataja, V, Kosma, VM, Hartikainen, JM, Li, JM, Brand, JS, Humphreys, K, Devilee, P, Tollenaar, RAEM, Seynaeve, Caroline, Radice, P, Peterlongo, P, Manoukian, S, Ficarazzi, F, Beckmann, MW, Hein, A, Ekici, AB, Balleine, R, Phillips, KA, Benitez, J, Zamora, MP, Perez, JIA, Menendez, P, Jakubowska, A, Lubinski, J, Gronwald, J, Durda, K, Hamann, U, Kabisch, M, Ulmer, HU, Rudiger, T, Margolin, S, Kristensen, V, Nord, S, Evans, DG, Abraham, J, Earl, H, Poole, CJ, Hiller, L, Dunn, JA, Bowden, S, Yang, R, Campa, D, Diver, WR, Gapstur, SM, Gaudet, MM, Hankinson, S, Hoover, RN, Husing, A, Kaaks, R, Machiela, MJ, Willett, W, Barrdahl, M, Canzian, F, Chin, SF, Caldas, C, Hunter, DJ, Lindstrom, S, Garcia-Closas, M, Couch, FJ, Chenevix-Trench, G, Mannermaa, A, Andrulis, IL, Hall, P, Chang-Claude, J, Easton, DF, Bojesen, SE, Cox, A, Fasching, PA, Pharoah, PDP, Schmidt, MK (Marjanka), Pirie, A, Guo, Q, Kraft, P, Canisius, S, Eccles, DM, Rahman, N, Nevanlinna, H, Chen, C (Christopher Li Hsian), Khan, Salima, Tyrer, J, Bolla, MK, Wang, Q (Qing), Dennis, J, Michailidou, K, Lush, M, Dunning, AM, Shah, M, Czene, K, Darabi, H, Eriksson, M, Lambrechts, D, Weltens, C, Leunen, K, Van Ongeval, C, Nordestgaard, BG, Nielsen, SF, Flyger, H, Rudolph, A, Seibold, P, Flesch-Janys, D, Blomqvist, C, Aittomaaki, K, Fagerholm, R, Muranen, TA, Olsen, JE, Hallberg, E, Vachon, C, Knight, JA, Glendon, G, Mulligan, AM, Broeks, A, Cornelissen, S, Haiman, CA, Henderson, BE, Schumacher, F, Le Marchand, L, Hopper, JL, Tsimiklis, H, Apicella, C, Southey, MC, Cross, SS, Reed, MWR, Giles, GG, Milne, RL, McLean, C, Winqvist, R, Pylkas, K, Jukkola-Vuorinen, A, Grip, M, Hooning, Maartje, Hollestelle, Antoinette, Martens, John, van den Ouweland, Ans, Marme, F, Schneeweiss, A, Yang, RX, Burwinkel, B, Figueroa, J, Chanock, SJ, Lissowska, J, Sawyer, EJ, Tomlinson, I, Kerin, MJ, Miller, N, Brenner, H, Butterbach, K, Holleczek, B, Kataja, V, Kosma, VM, Hartikainen, JM, Li, JM, Brand, JS, Humphreys, K, Devilee, P, Tollenaar, RAEM, Seynaeve, Caroline, Radice, P, Peterlongo, P, Manoukian, S, Ficarazzi, F, Beckmann, MW, Hein, A, Ekici, AB, Balleine, R, Phillips, KA, Benitez, J, Zamora, MP, Perez, JIA, Menendez, P, Jakubowska, A, Lubinski, J, Gronwald, J, Durda, K, Hamann, U, Kabisch, M, Ulmer, HU, Rudiger, T, Margolin, S, Kristensen, V, Nord, S, Evans, DG, Abraham, J, Earl, H, Poole, CJ, Hiller, L, Dunn, JA, Bowden, S, Yang, R, Campa, D, Diver, WR, Gapstur, SM, Gaudet, MM, Hankinson, S, Hoover, RN, Husing, A, Kaaks, R, Machiela, MJ, Willett, W, Barrdahl, M, Canzian, F, Chin, SF, Caldas, C, Hunter, DJ, Lindstrom, S, Garcia-Closas, M, Couch, FJ, Chenevix-Trench, G, Mannermaa, A, Andrulis, IL, Hall, P, Chang-Claude, J, Easton, DF, Bojesen, SE, Cox, A, Fasching, PA, Pharoah, PDP, and Schmidt, MK (Marjanka)

Abstract

Introduction: Previous studies have identified common germline variants nominally associated with breast cancer survival. These associations have not been widely replicated in further studies. The purpose of this study was to evaluate the association of previously reported SNPs with breast cancer-specific survival using data from a pooled analysis of eight breast cancer survival genome-wide association studies (GWAS) from the Breast Cancer Association Consortium. Methods: A literature review was conducted of all previously published associations between common germline variants and three survival outcomes: breast cancer-specific survival, overall survival and disease-free survival. All associations that reached the nominal significance level of P value <0.05 were included. Single nucleotide polymorphisms that had been previously reported as nominally associated with at least one survival outcome were evaluated in the pooled analysis of over 37,000 breast cancer cases for association with breast cancer-specific survival. Previous associations were evaluated using a one-sided test based on the reported direction of effect. Results: Fifty-six variants from 45 previous publications were evaluated in the meta-analysis. Fifty-four of these were evaluated in the full set of 37,954 breast cancer cases with 2,900 events and the two additional variants were evaluated in a reduced sample size of 30,000 samples in order to ensure independence from the previously published studies. Five variants reached nominal significance (P <0.05) in the pooled GWAS data compared to 2.8 expected under the null hypothesis. Seven additional variants were associated (P <0.05) with ER-positive disease. Conclusions: Although no variants reached genome-wide significance (P <5 x 10(-8)), these results suggest that there is some evidence of association between candidate common germline variants and breast cancer prognosis. Larger studies from multinational collaborations are necessary to

Published

2015

4. Identification of Novel Genetic Markers of Breast Cancer Survival

Author

Guo, Q, Schmidt, MK (Marjanka), Kraft, P, Canisius, S, Chen, C (Christopher Li Hsian), Khan, Salima, Tyrer, J, Bolla, MK, Wang, Q (Qing), Dennis, J, Michailidou, K, Lush, M, Kar, S, Beesley, J, Dunning, AM, Shah, M, Czene, K, Darabi, H, Eriksson, M, Lambrechts, D, Weltens, C, Leunen, K, Bojesen, SE, Nordestgaard, BG, Nielsen, SF, Flyger, H, Chang-Claude, J, Rudolph, A, Seibold, P, Flesch-Janys, D, Blomqvist, C, Aittomaki, K, Fagerholm, R, Muranen, TA, Couch, FJ, Olson, JE, Vachon, C, Andrulis, IL, Knight, JA, Glendon, G, Mulligan, AM, Broeks, A, Hogervorst, FB, Haiman, CA, Henderson, BE, Schumacher, F, Le Marchand, L, Hopper, JL, Tsimiklis, H, Apicella, C, Southey, MC, Cox, A, Cross, SS, Reed, MWR, Giles, GG, Milne, RL, McLean, C, Winqvist, R, Pylkas, K, Jukkola-Vuorinen, A, Grip, M, Hooning, Maartje, Hollestelle, Antoinette, Martens, John, van den Ouweland, Ans, Marme, F, Schneeweiss, A, Yang, RX, Burwinkel, B, Figueroa, J, Chanock, SJ, Lissowska, J, Sawyer, EJ, Tomlinson, I, Kerin, MJ, Miller, N, Brenner, H, Dieffenbach, AK, Arndt, V, Holleczek, B, Mannermaa, A, Kataja, V, Kosma, VM, Hartikainen, JM, Li, JM, Brand, JS, Humphreys, K, Devilee, P, Tollenaar, RAEM, Seynaeve, Caroline, Radice, P, Peterlongo, P, Bonanni, B, Mariani, P, Fasching, PA, Beckmann, MW, Hein, A, Ekici, AB, Chenevix-Trench, G, Balleine, R, Phillips, KA, Benitez, J, Zamora, MP, Perez, JIA, Menendez, P, Jakubowska, A, Lubinski, J, Jaworska-Bieniek, K, Durda, K, Hamann, U, Kabisch, M, Ulmer, HU, Rudiger, T, Margolin, S, Kristensen, V, Nord, S, Evans, DG, Abraham, JE, Earl, HM, Hiller, L, Dunn, JA, Bowden, S, Berg, Conny, Campa, D, Diver, WR, Gapstur, SM, Gaudet, MM, Hankinson, SE, Hoover, RN, Husing, A, Kaaks, R, Machiela, MJ, Willett, W, Barrdahl, M, Canzian, F, Chin, SF, Caldas, C, Hunter, DJ, Lindstrom, S, Garcia-Closas, M, Hall, P, Easton, DF, Eccles, DM, Rahman, N, Nevanlinna, H, Pharoah, PDP, Guo, Q, Schmidt, MK (Marjanka), Kraft, P, Canisius, S, Chen, C (Christopher Li Hsian), Khan, Salima, Tyrer, J, Bolla, MK, Wang, Q (Qing), Dennis, J, Michailidou, K, Lush, M, Kar, S, Beesley, J, Dunning, AM, Shah, M, Czene, K, Darabi, H, Eriksson, M, Lambrechts, D, Weltens, C, Leunen, K, Bojesen, SE, Nordestgaard, BG, Nielsen, SF, Flyger, H, Chang-Claude, J, Rudolph, A, Seibold, P, Flesch-Janys, D, Blomqvist, C, Aittomaki, K, Fagerholm, R, Muranen, TA, Couch, FJ, Olson, JE, Vachon, C, Andrulis, IL, Knight, JA, Glendon, G, Mulligan, AM, Broeks, A, Hogervorst, FB, Haiman, CA, Henderson, BE, Schumacher, F, Le Marchand, L, Hopper, JL, Tsimiklis, H, Apicella, C, Southey, MC, Cox, A, Cross, SS, Reed, MWR, Giles, GG, Milne, RL, McLean, C, Winqvist, R, Pylkas, K, Jukkola-Vuorinen, A, Grip, M, Hooning, Maartje, Hollestelle, Antoinette, Martens, John, van den Ouweland, Ans, Marme, F, Schneeweiss, A, Yang, RX, Burwinkel, B, Figueroa, J, Chanock, SJ, Lissowska, J, Sawyer, EJ, Tomlinson, I, Kerin, MJ, Miller, N, Brenner, H, Dieffenbach, AK, Arndt, V, Holleczek, B, Mannermaa, A, Kataja, V, Kosma, VM, Hartikainen, JM, Li, JM, Brand, JS, Humphreys, K, Devilee, P, Tollenaar, RAEM, Seynaeve, Caroline, Radice, P, Peterlongo, P, Bonanni, B, Mariani, P, Fasching, PA, Beckmann, MW, Hein, A, Ekici, AB, Chenevix-Trench, G, Balleine, R, Phillips, KA, Benitez, J, Zamora, MP, Perez, JIA, Menendez, P, Jakubowska, A, Lubinski, J, Jaworska-Bieniek, K, Durda, K, Hamann, U, Kabisch, M, Ulmer, HU, Rudiger, T, Margolin, S, Kristensen, V, Nord, S, Evans, DG, Abraham, JE, Earl, HM, Hiller, L, Dunn, JA, Bowden, S, Berg, Conny, Campa, D, Diver, WR, Gapstur, SM, Gaudet, MM, Hankinson, SE, Hoover, RN, Husing, A, Kaaks, R, Machiela, MJ, Willett, W, Barrdahl, M, Canzian, F, Chin, SF, Caldas, C, Hunter, DJ, Lindstrom, S, Garcia-Closas, M, Hall, P, Easton, DF, Eccles, DM, Rahman, N, Nevanlinna, H, and Pharoah, PDP

Abstract

Background: Survival after a diagnosis of breast cancer varies considerably between patients, and some of this variation may be because of germline genetic variation. We aimed to identify genetic markers associated with breast cancer-specific survival. Methods: We conducted a large meta-analysis of studies in populations of European ancestry, including 37 954 patients with 2900 deaths from breast cancer. Each study had been genotyped for between 200 000 and 900 000 single nucleotide polymorphisms (SNPs) across the genome; genotypes for nine million common variants were imputed using a common reference panel from the 1000 Genomes Project. We also carried out subtype-specific analyses based on 6881 estrogen receptor (ER)-negative patients (920 events) and 23 059 ER-positive patients (1333 events). All statistical tests were two-sided. Results: We identified one new locus (rs2059614 at 11q24.2) associated with survival in ER-negative breast cancer cases (hazard ratio [HR] = 1.95, 95% confidence interval [CI] = 1.55 to 2.47, P = 1.91 x 10(-8)). Genotyping a subset of 2113 case patients, of which 300 were ER negative, provided supporting evidence for the quality of the imputation. The association in this set of case patients was stronger for the observed genotypes than for the imputed genotypes. A second locus (rs148760487 at 2q24.2) was associated at genome-wide statistical significance in initial analyses; the association was similar in ER-positive and ER-negative case patients. Here the results of genotyping suggested that the finding was less robust. Conclusions: This is currently the largest study investigating genetic variation associated with breast cancer survival. Our results have potential clinical implications, as they confirm that germline genotype can provide prognostic information in addition to standard tumor prognostic factors.

Published

2015

5. High-resolution aCGH and expression profiling identifies a novel genomic subtype of ER negative breast cancer.

Author

Chin, SF, Teschendorff, AE, Marioni, JC, Wang, Y, Barbosa-Morais, NL, Thorne, NP, Costa, JL, Pinder, SE, van de Wiel, MA, Green, AR, Ellis, IO, Porter, PL, Tavaré, S, Brenton, JD, Ylstra, B, Caldas, C, Chin, SF, Teschendorff, AE, Marioni, JC, Wang, Y, Barbosa-Morais, NL, Thorne, NP, Costa, JL, Pinder, SE, van de Wiel, MA, Green, AR, Ellis, IO, Porter, PL, Tavaré, S, Brenton, JD, Ylstra, B, and Caldas, C

Abstract

BACKGROUND: The characterization of copy number alteration patterns in breast cancer requires high-resolution genome-wide profiling of a large panel of tumor specimens. To date, most genome-wide array comparative genomic hybridization studies have used tumor panels of relatively large tumor size and high Nottingham Prognostic Index (NPI) that are not as representative of breast cancer demographics. RESULTS: We performed an oligo-array-based high-resolution analysis of copy number alterations in 171 primary breast tumors of relatively small size and low NPI, which was therefore more representative of breast cancer demographics. Hierarchical clustering over the common regions of alteration identified a novel subtype of high-grade estrogen receptor (ER)-negative breast cancer, characterized by a low genomic instability index. We were able to validate the existence of this genomic subtype in one external breast cancer cohort. Using matched array expression data we also identified the genomic regions showing the strongest coordinate expression changes ('hotspots'). We show that several of these hotspots are located in the phosphatome, kinome and chromatinome, and harbor members of the 122-breast cancer CAN-list. Furthermore, we identify frequently amplified hotspots on 8q22.3 (EDD1, WDSOF1), 8q24.11-13 (THRAP6, DCC1, SQLE, SPG8) and 11q14.1 (NDUFC2, ALG8, USP35) associated with significantly worse prognosis. Amplification of any of these regions identified 37 samples with significantly worse overall survival (hazard ratio (HR) = 2.3 (1.3-1.4) p = 0.003) and time to distant metastasis (HR = 2.6 (1.4-5.1) p = 0.004) independently of NPI. CONCLUSION: We present strong evidence for the existence of a novel subtype of high-grade ER-negative tumors that is characterized by a low genomic instability index. We also provide a genome-wide list of common copy number alteration regions in breast cancer that show strong coordinate aberrant expression, and further identify novel frequ

Published

2007

6. Molecular cytogenetic analysis of breast cancer cell lines

Author

Davidson, JM, Gorringe, KL, Chin, SF, Orsetti, B, Besret, C, Courtay-Cahen, C, Roberts, I, Theillet, C, Caldas, C, Edwards, PAW, Davidson, JM, Gorringe, KL, Chin, SF, Orsetti, B, Besret, C, Courtay-Cahen, C, Roberts, I, Theillet, C, Caldas, C, and Edwards, PAW

Abstract

The extensive chromosome rearrangements of breast carcinomas must contribute to tumour development, but have been largely intractable to classical cytogenetic banding. We report here the analysis by 24-colour karyotyping and comparative genomic hybridization (CGH) of 19 breast carcinoma cell lines and one normal breast epithelial cell line, which provide model examples of karyotype patterns and translocations present in breast carcinomas. The CGH was compared with CGH of 106 primary breast cancers. The lines varied from perfectly diploid to highly aneuploid. Translocations were very varied and over 98% were unbalanced. The most frequent in the carcinomas were 8;11 in five lines; and 8;17, 1;4 and 1;10 in four lines. The most frequently involved chromosome was 8. Several lines showed complex multiply-translocated chromosomes. The very aneuploid karyotypes appeared to fall into two groups that evolved by different routes: one that steadily lost chromosomes and at one point doubled their entire karyotype; and another that steadily gained chromosomes, together with abnormalities. All karyotypes fell within the range seen in fresh material and CGH confirmed that the lines were broadly representative of fresh tumours. The karyotypes provide a resource for the cataloguing and analysis of translocations in these tumours, accessible at http://www.path.cam.ac.uk/ approximately pawefish.

Published

2000