Medical Education - Research Publications

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Multiomic analysis of homologous recombination-deficient end-stage high-grade serous ovarian cancer

Burdett, NL ; Willis, MO ; Alsop, K ; Hunt, AL ; Pandey, A ; Hamilton, PT ; Abulez, T ; Liu, X ; Hoang, T ; Craig, S ; Fereday, S ; Hendley, J ; Garsed, DW ; Milne, K ; Kalaria, S ; Marshall, A ; Hood, BL ; Wilson, KN ; Conrads, KA ; Pishas, K ; Ananda, S ; Scott, CL ; Antill, Y ; McNally, O ; Mileshkin, L ; Hamilton, A ; Au-Yeung, G ; Devereux, L ; Thorne, H ; Bild, A ; Bateman, NW ; Maxwell, GL ; Chang, JT ; Conrads, TPP ; Nelson, BH ; Bowtell, DDL ; Christie, ELL (NATURE PORTFOLIO, 2023-03)

High-grade serous ovarian cancer (HGSC) is frequently characterized by homologous recombination (HR) DNA repair deficiency and, while most such tumors are sensitive to initial treatment, acquired resistance is common. We undertook a multiomics approach to interrogate molecular diversity in end-stage disease, using multiple autopsy samples collected from 15 women with HR-deficient HGSC. Patients had polyclonal disease, and several resistance mechanisms were identified within most patients, including reversion mutations and HR restoration by other means. We also observed frequent whole-genome duplication and global changes in immune composition with evidence of immune escape. This analysis highlights diverse evolutionary changes within HGSC that evade therapy and ultimately overwhelm individual patients.
A comparison of DNA sequencing and gene expression profiling to assist tissue of origin diagnosis in cancer of unknown primary

Posner, A ; Prall, OW ; Sivakumaran, T ; Etemadamoghadam, D ; Thio, N ; Pattison, A ; Balachander, S ; Fisher, K ; Webb, S ; Wood, C ; DeFazio, A ; Wilcken, N ; Gao, B ; Karapetis, CS ; Singh, M ; Collins, IM ; Richardson, G ; Steer, C ; Warren, M ; Karanth, N ; Wright, G ; Williams, S ; George, J ; Hicks, RJ ; Boussioutas, A ; Gill, AJ ; Solomon, BJ ; Xu, H ; Fellowes, A ; Fox, SB ; Schofield, P ; Bowtell, D ; Mileshkin, L ; Tothill, RW (WILEY, 2023-01)
CCNE1 Amplification as a Therapeutic Target

Au-Yeung, G ; Mileshkin, L ; Bowtell, DDL (LIPPINCOTT WILLIAMS & WILKINS, 2023-03-20)
Immune and genomic biomarkers of immunotherapy response in cancer of unknown primary

Posner, A ; Sivakumaran, T ; Pattison, A ; Etemadmoghadam, D ; Thio, N ; Wood, C ; Fisher, K ; Webb, S ; DeFazio, A ; Wilcken, N ; Gao, B ; Karapetis, CS ; Singh, M ; Collins, IM ; Richardson, G ; Steer, C ; Warren, M ; Karanth, N ; Fellowes, A ; Fox, SB ; Hicks, RJ ; Schofield, P ; Bowtell, D ; Prall, OWJ ; Tothill, RW ; Mileshkin, L (BMJ PUBLISHING GROUP, 2023-01)

BACKGROUND: Cancer of unknown primary (CUP) is a heterogeneous group of metastatic cancers where a primary tissue of origin (TOO) is uncertain. Most patients with CUP have limited treatment options and poor survival outcomes. Immune checkpoint inhibitors (ICIs) can be efficacious in some patients with CUP, but the optimal predictive biomarkers are unknown. We therefore assessed immune and genomic biomarkers as well as predicted TOO in patients with CUP, including a subset treated with ICIs. METHODS: Patients with CUP were subject to gene-expression profiling (GEP) and DNA panel sequencing. Immune and stromal-related gene expression was explored by NanoString, including genes associated with immunotherapy response (IR) in other solid malignancies. ICI responsive cancer types were assigned based on Food and Drug Administration-approved indications, and either detection of a latent primary tumor or the TOO was suspected based on genomics informed pathology review. Tumor mutation burden (TMB) and gene mutations were also assessed. RESULTS: A total of 219 patients with CUP were included, 215 assessed for TOO in a previous study, with the majority (163) receiving both RNA and DNA tests. Of GEP profiled cases, 33% (59/175) had a high IR gene-expression score. Of the DNA sequenced cases, 16% (32/203) had high TMB (>10 mutations/Mb), including two with mismatch repair deficiency. Low correlation was observed between TMB and an IR score (R=0.26, p<0.001). Among 110 CUPs with a latent primary or suspected TOO, 47% (52/110) belonged to ICI-responsive cancer types. More than half of the CUPs had at least one feature that may predict ICI response (high IR score, high TMB, ICI-responsive cancer type). Among patients with CUP treated with ICIs, 8/28 (29%) responded (2 complete responses and 6 partial responses). Among non-responders, 9 had stable and 11 had progressive disease. All responders had a high IR score (7/8) and/or high TMB (3/8), while most (5/8) belonged to ICI-responsive cancer types. These features were detected at a lower frequency in non-responders and mostly in patients with stable disease. CONCLUSIONS: A significant fraction of CUP tumors had genomic features previously associated with ICI response. High IR score was the most sensitive predictive feature of ICI response, warranting evaluation in a larger patient series.
Uncertainty and the unmet informational needs of patients with cancer of unknown primary (CUP): a cross-sectional multi-site study

Guccione, L ; Fisher, K ; Mileshkin, L ; Tothill, R ; Bowtell, D ; Quinn, S ; DeFazio, A ; Karapetis, CS ; Wilcken, N ; Singh, M ; Steer, C ; Gao, B ; Warren, M ; Collins, IM ; Karanth, N ; Bryant, C ; Schofield, P (SPRINGER, 2022-10)

OBJECTIVE: This study aimed to determine the healthcare experiences, quality of life, and psychosocial needs of patients with cancer of unknown primary (CUP) early after diagnosis; comparing their experiences to patients with advanced cancer of a known primary (non-CUP control patients) and published general population reference data where available. METHODS: This study was a cross-sectional, multi-site study comparing CUP patients (n = 139) compared to non-CUP controls (n = 45). Demographic, clinical information and patient-reported outcome questionnaire data were collected at baseline. RESULTS: Differences in healthcare experienced were found between CUP and non-CUP controls with CUP patients reporting higher scores for unmet medical communication/information needs compared with non-CUP control patients (p = 0.013) as well as greater uncertainty in illness (p = 0.042). Whilst no differences were found between CUP and non-CUP controls on the EORTC and PROMIS measures, of those that 'received written information about your cancer…' and asked '…how useful was it?' fewer CUP patients reported finding the information useful 40% vs 61%, and more were likely to not have received written information at all 59% vs 32%; (p = 0.002). Additionally, of those that found information about their cancer online, fewer patients with CUP reported finding it useful 32% vs 48% control patients (p = 0.005). CONCLUSIONS: CUP patients have unmet medical communication/information needs and greater uncertainty in illness but do not differ in health-related quality of life domains compared to patients with advanced cancer of a known primary.
Psychological distress, understanding of cancer and illness uncertainty in patients with Cancer of Unknown Primary

Wolyniec, K ; Sharp, J ; Fisher, K ; Tothill, RW ; Bowtell, D ; Mileshkin, L ; Schofield, P (WILEY, 2022-11)

OBJECTIVE: Patients diagnosed with Cancer of Unknown Primary (CUP) experience high levels of psychological distress and report poor understanding of their cancer. We aimed to investigate: (1) if CUP patients with poorer understanding of their cancer diagnosis and testing experience more symptoms of psychological distress than those with better understanding; (2) if the relationship between patients' understanding of their cancer and psychological distress is mediated by illness uncertainty; and (3) explore whether patients' degree of understanding of their cancer can be predicted by clinical and socio-demographic factors. METHODS: 209 CUP patients completed a questionnaire measuring anxiety, depression, illness uncertainty, fatigue, pain, sleep and understanding of their cancer. Using an apriori theoretical framework, we employed structural equation modelling to investigate predictors of patient's understanding of their cancer and psychological distress and the relationships between understanding, illness uncertainty and distress. RESULTS: The structural equation model displayed good fit indices and supported the hypothesised relationship of patient's understanding of their cancer and the extent of psychological distress, which was mediated via illness uncertainty. Physical symptoms were positively associated with psychological distress and illness uncertainty. Younger age was predictive of lower patient's understanding of their cancer and higher levels of psychological distress. CONCLUSIONS: Patients with CUP, particularly those who are younger and experiencing more physical symptoms, report higher levels of psychological distress and may require additional mental health support. Our findings highlight a need to improve CUP patient's understanding about their illness, which could help reduce their illness uncertainty and alleviate psychological distress.
Endometriosis and menopausal hormone therapy impact the hysterectomy-ovarian cancer association.

Khoja, L ; Weber, RP ; Australian Ovarian Cancer Study Group, ; Webb, PM ; Jordan, SJ ; Muthukumar, A ; Chang-Claude, J ; Fortner, RT ; Jensen, A ; Kjaer, SK ; Risch, H ; Doherty, JA ; Harris, HR ; Goodman, MT ; Modugno, F ; Moysich, K ; Berchuck, A ; Schildkraut, JM ; Cramer, D ; Terry, KL ; Anton-Culver, H ; Ziogas, A ; Phung, MT ; Hanley, GE ; Wu, AH ; Mukherjee, B ; McLean, K ; Cho, K ; Pike, MC ; Pearce, CL ; Lee, AW (Elsevier BV, 2022-01)

OBJECTIVE: To evaluate the association between hysterectomy and ovarian cancer, and to understand how hormone therapy (HT) use and endometriosis affect this association. METHODS: We conducted a pooled analysis of self-reported data from 11 case-control studies in the Ovarian Cancer Association Consortium (OCAC). Women with (n = 5350) and without ovarian cancer (n = 7544) who never used HT or exclusively used either estrogen-only therapy (ET) or estrogen+progestin therapy (EPT) were included. Risk of invasive epithelial ovarian cancer adjusted for duration of ET and EPT use and stratified on history of endometriosis was determined using odds ratios (ORs) with 95% confidence intervals (CIs). RESULTS: Overall and among women without endometriosis, there was a positive association between ovarian cancer risk and hysterectomy (OR = 1.19, 95% CI 1.09-1.31 and OR = 1.20, 95% CI 1.09-1.32, respectively), but no association upon adjusting for duration of ET and EPT use (OR = 1.04, 95% CI 0.94-1.16 and OR = 1.06, 95% CI 0.95-1.18, respectively). Among women with a history of endometriosis, there was a slight inverse association between hysterectomy and ovarian cancer risk (OR = 0.93, 95% CI 0.69-1.26), but this association became stronger and statistically significant after adjusting for duration of ET and EPT use (OR = 0.69, 95% CI 0.48-0.99). CONCLUSIONS: The hysterectomy-ovarian cancer association is complex and cannot be understood without considering duration of ET and EPT use and history of endometriosis. Failure to take these exposures into account in prior studies casts doubt on their conclusions. Overall, hysterectomy is not risk-reducing for ovarian cancer, however the inverse association among women with endometriosis warrants further investigation.
REZOLVE (ANZGOG-1101): A phase 2 trial of intraperitoneal bevacizumab to treat symptomatic ascites in patients with chemotherapy-resistant, epithelial ovarian cancer

Sjoquist, KM ; Espinoza, D ; Mileshkin, L ; Ananda, S ; Shannon, C ; Yip, S ; Goh, J ; Bowtell, D ; Harrison, M ; Friedlander, ML (ACADEMIC PRESS INC ELSEVIER SCIENCE, 2021-05)

BACKGROUND: The primary aim of this study was to evaluate the activity of intraperitoneal bevacizumab (IP-bev) in delaying re-accumulation of malignant ascites in women with chemotherapy-resistant epithelial ovarian cancer (CR-EOC) who have ceased chemotherapy. Secondary outcomes were safety and quality of life. METHODS: Women with CR-EOC and malignant ascites that reaccumulated within 28 days of their last paracentesis (P-1) were administered IP-bev 5 mg/kg following their first therapeutic paracentesis on study (P0). Additional doses of IP-bev were allowed at each subsequent paracentesis (P1, P2, etc) provided the interval from the last dose was 42 days or greater (median time from first to second therapeutic ascitic drainage). RESULTS: 24 participants (median age 67 years [range 38-86]; median 4.5 lines prior systemic treatment [range 1-12]; ECOG performance status of 0 in 1, 1 in 8, and 2-3 in 15) were recruited. The doses of IP-bev administered were 1 in 13 participants, 2 in 5, 3 in 2, 4 in 1, and 5 in 1. The proportion with a TTP of >42 days using competing risk analysis was 77% (95% CI 58-92). Median time from P0 to P1 or death was 48 days (range 8-248). Median paracentesis-free interval (P0-P1 or death) was 4.29-fold (95% CI 2.4-5.8) higher following a first dose of IP-bev compared with the time between paracenteses prior to study entry (P-1-P0). CONCLUSION: IP-bev was safe, active, and warrants further study as a palliative intervention for recurrent ascites in CR-EOC patients receiving best supportive care.
Pan-cancer analysis of whole genomes

Campbell, PJ ; Getz, G ; Korbel, JO ; Stuart, JM ; Jennings, JL ; Stein, LD ; Perry, MD ; Nahal-Bose, HK ; Ouellette, BFF ; Li, CH ; Rheinbay, E ; Nielsen, GP ; Sgroi, DC ; Wu, C-L ; Faquin, WC ; Deshpande, V ; Boutros, PC ; Lazar, AJ ; Hoadley, KA ; Louis, DN ; Dursi, LJ ; Yung, CK ; Bailey, MH ; Saksena, G ; Raine, KM ; Buchhalter, I ; Kleinheinz, K ; Schlesner, M ; Zhang, J ; Wang, W ; Wheeler, DA ; Ding, L ; Simpson, JT ; O'Connor, BD ; Yakneen, S ; Ellrott, K ; Miyoshi, N ; Butler, AP ; Royo, R ; Shorser, S ; Vazquez, M ; Rausch, T ; Tiao, G ; Waszak, SM ; Rodriguez-Martin, B ; Shringarpure, S ; Wu, D-Y ; Demidov, GM ; Delaneau, O ; Hayashi, S ; Imoto, S ; Habermann, N ; Segre, A ; Garrison, E ; Cafferkey, A ; Alvarez, EG ; Maria Heredia-Genestar, J ; Muyas, F ; Drechsel, O ; Bruzos, AL ; Temes, J ; Zamora, J ; Baez-Ortega, A ; Kim, H-L ; Mashl, RJ ; Ye, K ; DiBiase, A ; Huang, K-L ; Letunic, I ; McLellan, MD ; Newhouse, SJ ; Shmaya, T ; Kumar, S ; Wedge, DC ; Wright, MH ; Yellapantula, VD ; Gerstein, M ; Khurana, E ; Marques-Bonet, T ; Navarro, A ; Bustamante, CD ; Siebert, R ; Nakagawa, H ; Easton, DF ; Ossowski, S ; Tubio, JMC ; De La Vega, FM ; Estivill, X ; Yuen, D ; Mihaiescu, GL ; Omberg, L ; Ferretti, V ; Sabarinathan, R ; Pich, O ; Gonzalez-Perez, A ; Weiner, AT ; Fittall, MW ; Demeulemeester, J ; Tarabichi, M ; Roberts, ND ; Van Loo, P ; Cortes-Ciriano, I ; Urban, L ; Park, P ; Bin, Z ; Pitkaenen, E ; Li, Y ; Saini, N ; Klimczak, LJ ; Weischenfeldt, J ; Sidiropoulos, N ; Alexandrov, LB ; Rabionet, R ; Escaramis, G ; Bosio, M ; Holik, AZ ; Susak, H ; Prasad, A ; Erkek, S ; Calabrese, C ; Raeder, B ; Harrington, E ; Mayes, S ; Turner, D ; Juul, S ; Roberts, SA ; Song, L ; Koster, R ; Mirabello, L ; Hua, X ; Tanskanen, TJ ; Tojo, M ; Chen, J ; Aaltonen, LA ; Ratsch, G ; Schwarz, RF ; Butte, AJ ; Brazma, A ; Chanock, SJ ; Chatterjee, N ; Stegle, O ; Harismendy, O ; Bova, GS ; Gordenin, DA ; Haan, D ; Sieverling, L ; Feuerbach, L ; Chalmers, D ; Joly, Y ; Knoppers, B ; Molnar-Gabor, F ; Phillips, M ; Thorogood, A ; Townend, D ; Goldman, M ; Fonseca, NA ; Xiang, Q ; Craft, B ; Pineiro-Yanez, E ; Munoz, A ; Petryszak, R ; Fullgrabe, A ; Al-Shahrour, F ; Keays, M ; Haussler, D ; Weinstein, J ; Huber, W ; Valencia, A ; Papatheodorou, I ; Zhu, J ; Fan, Y ; Torrents, D ; Bieg, M ; Chen, K ; Chong, Z ; Cibulskis, K ; Eils, R ; Fulton, RS ; Gelpi, JL ; Gonzalez, S ; Gut, IG ; Hach, F ; Heinold, M ; Hu, T ; Huang, V ; Hutter, B ; Jaeger, N ; Jung, J ; Kumar, Y ; Lalansingh, C ; Leshchiner, I ; Livitz, D ; Ma, EZ ; Maruvka, YE ; Milovanovic, A ; Nielsen, MM ; Paramasivam, N ; Pedersen, JS ; Puiggros, M ; Sahinalp, SC ; Sarrafi, I ; Stewart, C ; Stobbe, MD ; Wala, JA ; Wang, J ; Wendl, M ; Werner, J ; Wu, Z ; Xue, H ; Yamaguchi, TN ; Yellapantula, V ; Davis-Dusenbery, BN ; Grossman, RL ; Kim, Y ; Heinold, MC ; Hinton, J ; Jones, DR ; Menzies, A ; Stebbings, L ; Hess, JM ; Rosenberg, M ; Dunford, AJ ; Gupta, M ; Imielinski, M ; Meyerson, M ; Beroukhim, R ; Reimand, J ; Dhingra, P ; Favero, F ; Dentro, S ; Wintersinger, J ; Rudneva, V ; Park, JW ; Hong, EP ; Heo, SG ; Kahles, A ; Kjong-Van, L ; Soulette, CM ; Shiraishi, Y ; Liu, F ; He, Y ; Demircioglu, D ; Davidson, NR ; Greger, L ; Li, S ; Liu, D ; Stark, SG ; Zhang, F ; Amin, SB ; Bailey, P ; Chateigner, A ; Frenkel-Morgenstern, M ; Hou, Y ; Huska, MR ; Kilpinen, H ; Lamaze, FC ; Li, C ; Li, X ; Li, X ; Liu, X ; Marin, MG ; Markowski, J ; Nandi, T ; Ojesina, A ; Pan-Hammarstrom, Q ; Park, PJ ; Pedamallu, CS ; Su, H ; Tan, P ; Teh, BT ; Wang, J ; Xiong, H ; Ye, C ; Yung, C ; Zhang, X ; Zheng, L ; Zhu, S ; Awadalla, P ; Creighton, CJ ; Wu, K ; Yang, H ; Goke, J ; Zhang, Z ; Brooks, AN ; Martincorena, I ; Rubio-Perez, C ; Juul, M ; Schumacher, S ; Shapira, O ; Tamborero, D ; Mularoni, L ; Hornshoj, H ; Deu-Pons, J ; Muinos, F ; Bertl, J ; Guo, Q ; Bazant, W ; Barrera, E ; Al-Sedairy, ST ; Aretz, A ; Bell, C ; Betancourt, M ; Buchholz, C ; Calvo, F ; Chomienne, C ; Dunn, M ; Edmonds, S ; Green, E ; Gupta, S ; Hutter, CM ; Jegalian, K ; Jones, N ; Lu, Y ; Nakagama, H ; Nettekoven, G ; Planko, L ; Scott, D ; Shibata, T ; Shimizu, K ; Stratton, MR ; Yugawa, T ; Tortora, G ; VijayRaghavan, K ; Zenklusen, JC ; Knoppers, BM ; Aminou, B ; Bartolome, J ; Boroevich, KA ; Boyce, R ; Buchanan, A ; Byrne, NJ ; Chen, Z ; Cho, S ; Choi, W ; Clapham, P ; Dow, MT ; Dursi, LJ ; Eils, J ; Farcas, C ; Fayzullaev, N ; Flicek, P ; Heath, AP ; Hofmann, O ; Hong, JH ; Hudson, TJ ; Huebschmann, D ; Ivkovic, S ; Jeon, S-H ; Jiao, W ; Kabbe, R ; Kerssemakers, JNA ; Kim, H ; Kim, J ; Koscher, M ; Koures, A ; Kovacevic, M ; Lawerenz, C ; Liu, J ; Mijalkovic, S ; Mijalkovic-Lazic, AM ; Miyano, S ; Nastic, M ; Nicholson, J ; Ocana, D ; Ohi, K ; Ohno-Machado, L ; Pihl, TD ; Prinz, M ; Radovic, P ; Short, C ; Sofia, HJ ; Spring, J ; Struck, AJ ; Tijanic, N ; Vicente, D ; Wang, Z ; Williams, A ; Woo, Y ; Wright, AJ ; Yang, L ; Hamilton, MP ; Johnson, TA ; Kahraman, A ; Kellis, M ; Polak, P ; Sallari, R ; Sinnott-Armstrong, N ; von Mering, C ; Beltran, S ; Gerhard, DS ; Gut, M ; Trotta, J-R ; Whalley, JP ; Niu, B ; Espiritu, SMG ; Gao, S ; Huang, Y ; Lalansingh, CM ; Teague, JW ; Wendl, MC ; Abascal, F ; Bader, GD ; Bandopadhayay, P ; Barenboim, J ; Brunak, S ; Fita, JC ; Chakravarty, D ; Chan, CWY ; Choi, JK ; Diamanti, K ; Fink, JL ; Frigola, J ; Gambacorti-Passerini, C ; Garsed, DW ; Haradhvala, NJ ; Harmanci, AO ; Helmy, M ; Herrmann, C ; Hobolth, A ; Hodzic, E ; Hong, C ; Isaev, K ; Izarzugaza, JMG ; Johnson, R ; Juul, RI ; Kim, J ; Kim, JK ; Komorowski, J ; Lanzos, A ; Larsson, E ; Lee, D ; Li, S ; Li, X ; Lin, Z ; Liu, EM ; Lochovsky, L ; Lou, S ; Madsen, T ; Marchal, K ; Fundichely, AM ; McGillivray, PD ; Meyerson, W ; Paczkowska, M ; Park, K ; Park, K ; Pons, T ; Pulido-Tamayo, S ; Reyes Salazar, I ; Reyna, MA ; Rubin, MA ; Salichos, L ; Sander, C ; Schumacher, SE ; Shackleton, M ; Shen, C ; Shrestha, R ; Shuai, S ; Tsunoda, T ; Umer, HM ; Uuskula-Reimand, L ; Verbeke, LPC ; Wadelius, C ; Wadi, L ; Warrell, J ; Wu, G ; Yu, J ; Zhang, J ; Zhang, X ; Zhang, Y ; Zhao, Z ; Zou, L ; Lawrence, MS ; Raphael, BJ ; Bailey, PJ ; Craft, D ; Goldman, MJ ; Aburatani, H ; Binder, H ; Dinh, HQ ; Heath, SC ; Hoffmann, S ; Imbusch, CD ; Kretzmer, H ; Laird, PW ; Martin-Subero, J ; Nagae, G ; Shen, H ; Wang, Q ; Weichenhan, D ; Zhou, W ; Berman, BP ; Brors, B ; Plass, C ; Akdemir, KC ; Bowtell, DDL ; Burns, KH ; Busanovich, J ; Chan, K ; Dueso-Barroso, A ; Edwards, PA ; Etemadmoghadam, D ; Haber, JE ; Jones, DTW ; Ju, YS ; Kazanov, MD ; Koh, Y ; Kumar, K ; Lee, EA ; Lee, JJ-K ; Lynch, AG ; Macintyre, G ; Markowetz, F ; Navarro, FCP ; Pearson, J ; Rippe, K ; Scully, R ; Villasante, I ; Waddell, N ; Yang, L ; Yao, X ; Yoon, S-S ; Zhang, C-Z ; Bergstrom, EN ; Boot, A ; Covington, K ; Fujimoto, A ; Huang, MN ; Islam, SMA ; McPherson, JR ; Morganella, S ; Mustonen, V ; Ng, AWT ; Prokopec, SD ; Vazquez-Garcia, I ; Wu, Y ; Yousif, F ; Yu, W ; Rozen, SG ; Rudneva, VA ; Shringarpure, SS ; Turner, DJ ; Xia, T ; Atwal, G ; Chang, DK ; Cooke, SL ; Faltas, BM ; Haider, S ; Kaiser, VB ; Karlic, R ; Kato, M ; Kubler, K ; Margolin, A ; Martin, S ; Nik-Zainal, S ; P'ng, C ; Semple, CA ; Smith, J ; Sun, RX ; Thai, K ; Wright, DW ; Yuan, K ; Biankin, A ; Garraway, L ; Grimmond, SM ; Adams, DJ ; Anur, P ; Cao, S ; Christie, EL ; Cmero, M ; Cun, Y ; Dawson, KJ ; Dentro, SC ; Deshwar, AG ; Donmez, N ; Drews, RM ; Gerstung, M ; Ha, G ; Haase, K ; Jerman, L ; Ji, Y ; Jolly, C ; Lee, J ; Lee-Six, H ; Malikic, S ; Mitchell, TJ ; Morris, QD ; Oesper, L ; Peifer, M ; Peto, M ; Rosebrock, D ; Rubanova, Y ; Salcedo, A ; Sengupta, S ; Shi, R ; Shin, SJ ; Spiro, O ; Vembu, S ; Wintersinger, JA ; Yang, T-P ; Yu, K ; Zhu, H ; Spellman, PT ; Weinstein, JN ; Chen, Y ; Fujita, M ; Han, L ; Hasegawa, T ; Komura, M ; Li, J ; Mizuno, S ; Shimizu, E ; Wang, Y ; Xu, Y ; Yamaguchi, R ; Yang, F ; Yang, Y ; Yoon, CJ ; Yuan, Y ; Liang, H ; Alawi, M ; Borozan, I ; Brewer, DS ; Cooper, CS ; Desai, N ; Grundhoff, A ; Iskar, M ; Su, X ; Zapatka, M ; Lichter, P ; Alsop, K ; Bruxner, TJC ; Christ, AN ; Cordner, SM ; Cowin, PA ; Drapkin, R ; Fereday, S ; George, J ; Hamilton, A ; Holmes, O ; Hung, JA ; Kassahn, KS ; Kazakoff, SH ; Kennedy, CJ ; Leonard, CR ; Mileshkin, L ; Miller, DK ; Arnau, GM ; Mitchell, C ; Newell, F ; Nones, K ; Patch, A-M ; Quinn, MC ; Taylor, DF ; Thorne, H ; Traficante, N ; Vedururu, R ; Waddell, NM ; Waring, PM ; Wood, S ; Xu, Q ; DeFazio, A ; Anderson, MJ ; Antonello, D ; Barbour, AP ; Bassi, C ; Bersani, S ; Cataldo, I ; Chantrill, LA ; Chiew, Y-E ; Chou, A ; Cingarlini, S ; Cloonan, N ; Corbo, V ; Davi, MV ; Duthie, FR ; Gill, AJ ; Graham, JS ; Harliwong, I ; Jamieson, NB ; Johns, AL ; Kench, JG ; Landoni, L ; Lawlor, RT ; Mafficini, A ; Merrett, ND ; Miotto, M ; Musgrove, EA ; Nagrial, AM ; Oien, KA ; Pajic, M ; Pinese, M ; Robertson, AJ ; Rooman, I ; Rusev, BC ; Samra, JS ; Scardoni, M ; Scarlett, CJ ; Scarpa, A ; Sereni, E ; Sikora, KO ; Simbolo, M ; Taschuk, ML ; Toon, CW ; Vicentini, C ; Wu, J ; Zeps, N ; Behren, A ; Burke, H ; Cebon, J ; Dagg, RA ; De Paoli-Iseppi, R ; Dutton-Regester, K ; Field, MA ; Fitzgerald, A ; Hersey, P ; Jakrot, V ; Johansson, PA ; Kakavand, H ; Kefford, RF ; Lau, LMS ; Long, G ; Pickett, HA ; Pritchard, AL ; Pupo, GM ; Saw, RPM ; Schramm, S-J ; Shang, CA ; Shang, P ; Spillane, AJ ; Stretch, JR ; Tembe, V ; Thompson, JF ; Vilain, RE ; Wilmott, JS ; Yang, JY ; Hayward, NK ; Mann, GJ ; Scolyer, RA ; Bartlett, J ; Bavi, P ; Chadwick, DE ; Chan-Seng-Yue, M ; Cleary, S ; Connor, AA ; Czajka, K ; Denroche, RE ; Dhani, NC ; Eagles, J ; Gallinger, S ; Grant, RC ; Hedley, D ; Hollingsworth, MA ; Jang, GH ; Johns, J ; Kalimuthu, S ; Liang, S-B ; Lungu, I ; Luo, X ; Mbabaali, F ; McPherson, TA ; Miller, JK ; Moore, MJ ; Notta, F ; Pasternack, D ; Petersen, GM ; Roehrl, MHA ; Sam, M ; Selander, I ; Serra, S ; Shahabi, S ; Thayer, SP ; Timms, LE ; Wilson, GW ; Wilson, JM ; Wouters, BG ; McPherson, JD ; Beck, TA ; Bhandari, V ; Collins, CC ; Fleshner, NE ; Fox, NS ; Fraser, M ; Heisler, LE ; Lalonde, E ; Livingstone, J ; Meng, A ; Sabelnykova, VY ; Shiah, Y-J ; Van Der Kwast, T ; Bristow, RG ; Ding, S ; Fan, D ; Li, L ; Nie, Y ; Xiao, X ; Xing, R ; Yang, S ; Yu, Y ; Zhou, Y ; Banks, RE ; Bourque, G ; Brennan, P ; Letourneau, L ; Riazalhosseini, Y ; Scelo, G ; Vasudev, N ; Viksna, J ; Lathrop, M ; Tost, J ; Ahn, S-M ; Aparicio, S ; Arnould, L ; Aure, MR ; Bhosle, SG ; Birney, E ; Borg, A ; Boyault, S ; Brinkman, AB ; Brock, JE ; Broeks, A ; Borresen-Dale, A-L ; Caldas, C ; Chin, S-F ; Davies, H ; Desmedt, C ; Dirix, L ; Dronov, S ; Ehinger, A ; Eyfjord, JE ; Fatima, A ; Foekens, JA ; Futreal, PA ; Garred, O ; Giri, DD ; Glodzik, D ; Grabau, D ; Hilmarsdottir, H ; Hooijer, GK ; Jacquemier, J ; Jang, SJ ; Jonasson, JG ; Jonkers, J ; Kim, H-Y ; King, TA ; Knappskog, S ; Kong, G ; Krishnamurthy, S ; Lakhani, SR ; Langerod, A ; Larsimont, D ; Lee, HJ ; Lee, J-Y ; Lee, MTM ; Lingjaerde, OC ; MacGrogan, G ; Martens, JWM ; O'Meara, S ; Pauporte, I ; Pinder, S ; Pivot, X ; Provenzano, E ; Purdie, CA ; Ramakrishna, M ; Ramakrishnan, K ; Reis-Filho, J ; Richardson, AL ; Ringner, M ; Rodriguez, JB ; Rodriguez-Gonzalez, FG ; Romieu, G ; Salgado, R ; Sauer, T ; Shepherd, R ; Sieuwerts, AM ; Simpson, PT ; Smid, M ; Sotiriou, C ; Span, PN ; Stefansson, OA ; Stenhouse, A ; Stunnenberg, HG ; Sweep, F ; Tan, BKT ; Thomas, G ; Thompson, AM ; Tommasi, S ; Treilleux, I ; Tutt, A ; Ueno, NT ; Van Laere, S ; Van den Eynden, GG ; Vermeulen, P ; Viari, A ; Vincent-Salomon, A ; Wong, BH ; Yates, L ; Zou, X ; van Deurzen, CHM ; van de Vijver, MJ ; van't Veer, L ; Ammerpohl, O ; Aukema, S ; Bergmann, AK ; Bernhart, SH ; Borkhardt, A ; Borst, C ; Burkhardt, B ; Claviez, A ; Goebler, ME ; Haake, A ; Haas, S ; Hansmann, M ; Hoell, J ; Hummel, M ; Karsch, D ; Klapper, W ; Kneba, M ; Kreuz, M ; Kube, D ; Kueppers, R ; Lenze, D ; Loeffler, M ; Lopez, C ; Mantovani-Loeffler, L ; Moeller, P ; Ott, G ; Radlwimmer, B ; Richter, J ; Rohde, M ; Rosenstiel, PC ; Rosenwald, A ; Schilhabel, MB ; Schreiber, S ; Stadler, PF ; Staib, P ; Stilgenbauer, S ; Sungalee, S ; Szczepanowski, M ; Toprak, UH ; Truemper, LHP ; Wagener, R ; Zenz, T ; Hovestadt, V ; von Kalle, C ; Kool, M ; Korshunov, A ; Landgraf, P ; Lehrach, H ; Northcott, PA ; Pfister, SM ; Reifenberger, G ; Warnatz, H-J ; Wolf, S ; Yaspo, M-L ; Assenov, Y ; Gerhauser, C ; Minner, S ; Schlomm, T ; Simon, R ; Sauter, G ; Sueltmann, H ; Biswas, NK ; Maitra, A ; Majumder, PP ; Sarin, R ; Barbi, S ; Bonizzato, G ; Cantu, C ; Dei Tos, AP ; Fassan, M ; Grimaldi, S ; Luchini, C ; Malleo, G ; Marchegiani, G ; Milella, M ; Paiella, S ; Pea, A ; Pederzoli, P ; Ruzzenente, A ; Salvia, R ; Sperandio, N ; Arai, Y ; Hama, N ; Hiraoka, N ; Hosoda, F ; Nakamura, H ; Ojima, H ; Okusaka, T ; Totoki, Y ; Urushidate, T ; Fukayama, M ; Ishikawa, S ; Katai, H ; Katoh, H ; Komura, D ; Rokutan, H ; Saito-Adachi, M ; Suzuki, A ; Taniguchi, H ; Tatsuno, K ; Ushiku, T ; Yachida, S ; Yamamoto, S ; Aikata, H ; Arihiro, K ; Ariizumi, S-I ; Chayama, K ; Furuta, M ; Gotoh, K ; Hayami, S ; Hirano, S ; Kawakami, Y ; Maejima, K ; Nakamura, T ; Nakano, K ; Ohdan, H ; Sasaki-Oku, A ; Tanaka, H ; Ueno, M ; Yamamoto, M ; Yamaue, H ; Choo, SP ; Cutcutache, I ; Khuntikeo, N ; Ong, CK ; Pairojkul, C ; Popescu, I ; Ahn, KS ; Aymerich, M ; Lopez-Guillermo, A ; Lopez-Otin, C ; Puente, XS ; Campo, E ; Amary, F ; Baumhoer, D ; Behjati, S ; Bjerkehagen, B ; Futreal, PA ; Myklebost, O ; Pillay, N ; Tarpey, P ; Tirabosco, R ; Zaikova, O ; Flanagan, AM ; Boultwood, J ; Bowen, DT ; Cazzola, M ; Green, AR ; Hellstrom-Lindberg, E ; Malcovati, L ; Nangalia, J ; Papaemmanuil, E ; Vyas, P ; Ang, Y ; Barr, H ; Beardsmore, D ; Eldridge, M ; Gossage, J ; Grehan, N ; Hanna, GB ; Hayes, SJ ; Hupp, TR ; Khoo, D ; Lagergren, J ; Lovat, LB ; MacRae, S ; O'Donovan, M ; O'Neill, JR ; Parsons, SL ; Preston, SR ; Puig, S ; Roques, T ; Sanders, G ; Sothi, S ; Tavare, S ; Tucker, O ; Turkington, R ; Underwood, TJ ; Welch, I ; Fitzgerald, RC ; Berney, DM ; De Bono, JS ; Cahill, D ; Camacho, N ; Dennis, NM ; Dudderidge, T ; Edwards, SE ; Fisher, C ; Foster, CS ; Ghori, M ; Gill, P ; Gnanapragasam, VJ ; Gundem, G ; Hamdy, FC ; Hawkins, S ; Hazell, S ; Howat, W ; Isaacs, WB ; Karaszi, K ; Kay, JD ; Khoo, V ; Kote-Jarai, Z ; Kremeyer, B ; Kumar, P ; Lambert, A ; Leongamornlert, DA ; Livni, N ; Lu, Y-J ; Luxton, HJ ; Marsden, L ; Massie, CE ; Matthews, L ; Mayer, E ; McDermott, U ; Merson, S ; Neal, DE ; Ng, A ; Nicol, D ; Ogden, C ; Rowe, EW ; Shah, NC ; Thomas, S ; Thompson, A ; Verrill, C ; Visakorpi, T ; Warren, AY ; Whitaker, HC ; Zhang, H ; van As, N ; Eeles, RA ; Abeshouse, A ; Agrawal, N ; Akbani, R ; Al Ahmadie, H ; Albert, M ; Aldape, K ; Ally, A ; Appelbaum, EL ; Armenia, J ; Asa, S ; Auman, JT ; Balasundaram, M ; Balu, S ; Barnholtz-Sloan, J ; Bathe, OF ; Baylin, SB ; Benz, C ; Berchuck, A ; Berrios, M ; Bigner, D ; Birrer, M ; Bodenheimer, T ; Boice, L ; Bootwalla, MS ; Bosenberg, M ; Bowlby, R ; Boyd, J ; Broaddus, RR ; Brock, M ; Brooks, D ; Bullman, S ; Caesar-Johnson, SJ ; Carey, TE ; Carlsen, R ; Cerfolio, R ; Chandan, VS ; Chen, H-W ; Cherniack, AD ; Chien, J ; Cho, J ; Chuah, E ; Cibulskis, C ; Cope, L ; Cordes, MG ; Curley, E ; Czerniak, B ; Danilova, L ; Davis, IJ ; Defreitas, T ; Demchok, JA ; Dhalla, N ; Dhir, R ; Doddapaneni, H ; El-Naggar, A ; Felau, I ; Ferguson, ML ; Finocchiaro, G ; Fong, KM ; Frazer, S ; Friedman, W ; Fronick, CC ; Fulton, LA ; Gabriel, SB ; Gao, J ; Gehlenborg, N ; Gershenwald, JE ; Ghossein, R ; Giama, NH ; Gibbs, RA ; Gomez, C ; Govindan, R ; Hayes, DN ; Hegde, AM ; Heiman, D ; Heins, Z ; Hepperla, AJ ; Holbrook, A ; Holt, RA ; Hoyle, AP ; Hruban, RH ; Hu, J ; Huang, M ; Huntsman, D ; Huse, J ; Donahue, CAI ; Ittmann, M ; Jayaseelan, JC ; Jefferys, SR ; Jones, CD ; Jones, SJM ; Juhl, H ; Kang, KJ ; Karlan, B ; Kasaian, K ; Kebebew, E ; Kim, HK ; Korchina, V ; Kundra, R ; Lai, PH ; Lander, E ; Le, X ; Lee, D ; Levine, DA ; Lewis, L ; Ley, T ; Li, HI ; Lin, P ; Linehan, WM ; Liu, FF ; Lu, Y ; Lype, L ; Ma, Y ; Maglinte, DT ; Mardis, ER ; Marks, J ; Marra, MA ; Matthew, TJ ; Mayo, M ; McCune, K ; Meier, SR ; Meng, S ; Mieczkowski, PA ; Mikkelsen, T ; Miller, CA ; Mills, GB ; Moore, RA ; Morrison, C ; Mose, LE ; Moser, CD ; Mungall, AJ ; Mungall, K ; Mutch, D ; Muzny, DM ; Myers, J ; Newton, Y ; Noble, MS ; O'Donnell, P ; O'Neill, BP ; Ochoa, A ; Park, J-W ; Parker, JS ; Pass, H ; Pastore, A ; Pennell, NA ; Perou, CM ; Petrelli, N ; Potapova, O ; Rader, JS ; Ramalingam, S ; Rathmell, WK ; Reuter, V ; Reynolds, SM ; Ringel, M ; Roach, J ; Roberts, LR ; Robertson, AG ; Sadeghi, S ; Saller, C ; Sanchez-Vega, F ; Schadendorf, D ; Schein, JE ; Schmidt, HK ; Schultz, N ; Seethala, R ; Senbabaoglu, Y ; Shelton, T ; Shi, Y ; Shih, J ; Shmulevich, I ; Shriver, C ; Signoretti, S ; Simons, J ; Singer, S ; Sipahimalani, P ; Skelly, TJ ; McCune, KS ; Socci, ND ; Soloway, MG ; Sood, AK ; Tam, A ; Tan, D ; Tarnuzzer, R ; Thiessen, N ; Thompson, RH ; Thorne, LB ; Tsao, M ; Umbricht, C ; Van Den Berg, DJ ; Van Meir, EG ; Veluvolu, U ; Voet, D ; Wang, L ; Weinberger, P ; Weisenberger, DJ ; Wigle, D ; Wilkerson, MD ; Wilson, RK ; Winterhoff, B ; Wiznerowicz, M ; Wong, T ; Wong, W ; Xi, L ; Yau, C ; Zhang, H ; Zhang, H ; Zhang, J (NATURE PUBLISHING GROUP, 2020-02-06)

Cancer is driven by genetic change, and the advent of massively parallel sequencing has enabled systematic documentation of this variation at the whole-genome scale1-3. Here we report the integrative analysis of 2,658 whole-cancer genomes and their matching normal tissues across 38 tumour types from the Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium of the International Cancer Genome Consortium (ICGC) and The Cancer Genome Atlas (TCGA). We describe the generation of the PCAWG resource, facilitated by international data sharing using compute clouds. On average, cancer genomes contained 4-5 driver mutations when combining coding and non-coding genomic elements; however, in around 5% of cases no drivers were identified, suggesting that cancer driver discovery is not yet complete. Chromothripsis, in which many clustered structural variants arise in a single catastrophic event, is frequently an early event in tumour evolution; in acral melanoma, for example, these events precede most somatic point mutations and affect several cancer-associated genes simultaneously. Cancers with abnormal telomere maintenance often originate from tissues with low replicative activity and show several mechanisms of preventing telomere attrition to critical levels. Common and rare germline variants affect patterns of somatic mutation, including point mutations, structural variants and somatic retrotransposition. A collection of papers from the PCAWG Consortium describes non-coding mutations that drive cancer beyond those in the TERT promoter4; identifies new signatures of mutational processes that cause base substitutions, small insertions and deletions and structural variation5,6; analyses timings and patterns of tumour evolution7; describes the diverse transcriptional consequences of somatic mutation on splicing, expression levels, fusion genes and promoter activity8,9; and evaluates a range of more-specialized features of cancer genomes8,10-18.
Sex differences in oncogenic mutational processes

Li, CH ; Prokopec, SD ; Sun, RX ; Yousif, F ; Schmitz, N ; Boutros, PC (NATURE PORTFOLIO, 2020-08-28)

Sex differences have been observed in multiple facets of cancer epidemiology, treatment and biology, and in most cancers outside the sex organs. Efforts to link these clinical differences to specific molecular features have focused on somatic mutations within the coding regions of the genome. Here we report a pan-cancer analysis of sex differences in whole genomes of 1983 tumours of 28 subtypes as part of the ICGC/TCGA Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium. We both confirm the results of exome studies, and also uncover previously undescribed sex differences. These include sex-biases in coding and non-coding cancer drivers, mutation prevalence and strikingly, in mutational signatures related to underlying mutational processes. These results underline the pervasiveness of molecular sex differences and strengthen the call for increased consideration of sex in molecular cancer research.

Medical Education - Research Publications

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