Divergent mutational processes distinguish hypoxic and normoxic tumours

Aaltonen, Lauri A.; Abascal, Federico; Abeshouse, Adam; Aburatani, Hiroyuki; Adams, David J.; Agrawal, Nishant; Ahn, Keun Soo; Ahn, Sung-Min; Aikata, Hiroshi; Akbani, Rehan; Akdemir, Kadir C.; Al‐Ahmadie, Hikmat; Al‐Sedairy, Sultan T.; Al‐Shahrour, Fátima; Alawi, Malik; Albert, Monique; Aldape, Kenneth; Alexandrov, Ludmil B.; Ally, Adrian; Alsop, Kathryn; Alvarez, Eva G.; Amary, Fernanda; Amin, Samirkumar B.; Aminou, Brice; Ammerpohl, Ole; Anderson, Matthew; Ang, Yeng; Antonello, Davide; Anur, Pavana; Aparício, Samuel; Appelbaum, Elizabeth L.; Arai, Yasuhito; Aretz, Axel; Arihiro, Koji; Ariizumi, Shun‐ichi; Armenia, Joshua; Arnould́, Laurent; Asa, Sylvia; Assenov, Yassen; Atwal, Gurnit; Aukema, Sietse M.; Auman, J. Todd; Aure, Miriam Ragle; Awadalla, Philip; Aymerich, Marta; Bader, Gary D.; Baez‐Ortega, Adrian; Bailey, Matthew H.; Bailey, Peter J.; Balasundaram, Miruna; Balu, Saianand; Bandopadhayay, Pratiti; Banks, Rosamonde E.; Barbi, Stefano; Barbour, Andrew P.; Barenboim, Jonathan; Barnholtz‐Sloan, Jill S.; Barr, Hugh; Barrera, Elisabet; Bartlett, John M.S.; Bartolomé, Javier; Bassi, Claudio; Bathe, Oliver F.; Baumhoer, Daniel; Bavi, Prashant; Baylin, Stephen B.; Bażant, Wojciech; Beardsmore, Duncan; Beck, Timothy A.; Behjati, Sam; Behren, Andreas; Niu, Beifang; Bell, Cindy; Beltrán, Sergi; Benz, Christopher C.; Berchuck, Andrew; Bergmann, Anke; Bergstrom, Erik N.; Berman, Benjamin P.; Berney, Daniel M.; Bernhart, Stephan H.; Beroukhim, Rameen; Berríos, Mario; Bersani, Samantha; Bertl, Johanna; Betancourt, Miguel; Bhandari, Vinayak; Bhosle, Shriram G.; Biankin, Andrew V.; Bieg, Matthias; Bigner, Darell D.; Binder, Hans; Birney, Ewan; Birrer, Michael J.; Biswas, Nidhan K.; Bjerkehagen, Bodil; Bodenheimer, Tom; Boice, Lori; Bonizzato, Giada; Bono, Johann S. de; Boot, Arnoud; Bootwalla, Moiz S.; Borg, Åke; Borkhardt, Arndt; Boroevich, Keith A.; Borozan, Ivan; Borst, Christoph; Bosenberg, Marcus W.; Bosio, Mattia; Boultwood, Jacqueline; Bourque, Guillaume; Boutros, Paul C.; Bova, G. 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C.; Bruzos, Alicia L.; Buchanan, Alex; Buchhalter, Ivo; Buchholz, Christiane; Bullman, Susan; Burke, Hazel; Burkhardt, Birgit; Burns, Kathleen H.; Busanovich, John; Bustamante, Carlos D.; Butler, Adam; Butte, Atul J.; Byrne, Niall J.; Børresen‐Dale, Anne‐Lise; Caesar-Johnson, Samantha J.; Cafferkey, Andy; Cahill, Declan; Calabrese, Claudia; Caldas, Carlos; Calvo, Fabien; Camacho, Niedzica; Campbell, Peter J.; Campo, Elı́as; Cantù, Cinzia; Cao, Shaolong; Carey, Thomas E.; Carlevaro-Fita, Joana; Carlsen, Rebecca; Cataldo, Ivana; Cazzola, Mario; Cebon, Jonathan; Cerfolio, Robert; Chadwick, Dianne; Chakravarty, Dimple; Chalmers, Don; Chan, Calvin Wing Yiu; Chan, Kin; Chan-Seng-Yue, Michelle; Chandan, Vishal S.; Chang, David K.; Chanock, Stephen J.; Chantrill, Lorraine A.; Chateigner, Aurélien; Chatterjee, Nilanjan; Chayama, Kazuaki; Chen, Hsiao‐Wei; Chen, Jieming; Chen, Ken; Chen, Yiwen; Chen, Zhaohong; Cherniack, Andrew D.; Chien, Jeremy; Chiew, Yoke-Eng; Chin, Suet-Feung; Cho, Juok; Cho, Sunghoon; Choi, Jung Kyoon; Choi, Wan; Chomienne, Christine; Chong, Zechen; Choo, Su Pin; Chou, Angela; Christ, Angelika N.; Christie, Elizabeth L.; Chuah, Eric; Cibulskis, Carrie; Cibulskis, Kristian; Cingarlini, Sara; Clapham, Peter; Claviez, Alexander; Cleary, Sean P.; Cloonan, Nicole; Cmero, Marek; Collins, Colin C.; Connor, Ashton A.; Cooke, Susanna L.; Cooper, Colin S.; Cope, Leslie; Corbo, Vincenzo; Cordes, Matthew G.; Cordner, Stephen; Cortés-Ciriano, Isidro; Covington, Kyle R.; Cowin, Prue A.; Craft, Brian; Craft, David; Creighton, Chad J.; Cun, Yupeng; Curley, Erin; Cutcutache, Ioana; Czajka, Karolina; Czerniak, Bogdan; Dagg, Rebecca A.; Danilova, Ludmila; Davì, Maria Vittoria; Davidson, Natalie R.; Davies, Helen; Davis, Ian J.; Davis‐Dusenbery, Brandi N.; Dawson, Kevin J.; Vega, Francisco; Paoli-Iseppi, Ricardo De; DeFreitas, Timothy; Tos, Angelo Paolo Dei; Delaneau, Olivier; Demchok, John A.; Demeulemeester, Jonas; Demidov, German; Demircioğlu, Deniz; Dennis, Nening M.; Denroche, Robert E.; Dentro, Stefan C.; Desai, Nikita; Deshpande, Vikram; Deshwar, Amit G.; Desmedt, Christine; Deu-Pons, Jordi; Dhalla, Noreen; Dhani, Neesha C.; Dhingra, Priyanka; Dhir, Rajiv; DiBiase, Anthony; Diamanti, Klev; Li, Ding; Ding, Shuai; Dinh, Huy Q.; Dirix, Luc; Doddapaneni, HarshaVardhan; Donmez, Nilgun; Dow, Michelle; Drapkin, Ronny; Drechsel, Oliver; Drews, Ruben M.; Serge, Serge; Dudderidge, Tim; Dueso-Barroso, Ana; Dunford, Andrew; Dunn, Michael; Dursi, Lewis Jonathan; Duthie, Fraser; Dutton‐Regester, Ken; Eagles, Jenna; Easton, Douglas F.; Edmonds, Stuart; Edwards, Paul A.W.; Edwards, Sandra E.; Eeles, Rosalind A.; Ehinger, Anna; Eils, Juergen; Eils, Roland; El‐Naggar, Adel K.; Eldridge, Matthew; Ellrott, Kyle; Erkek, Serap; Escaramís, Geòrgia; Espiritu, Shadrielle M. 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doi:10.1038/s41467-019-14052-x

Cited by 90 publications

(53 citation statements)

References 50 publications

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“…However, a recent study suggested that large number of mutations were identified in patients with hypoxic tumors with higher incidence in deletions, duplications, and single nucleotide changes. 27 The authors also identified mutational signatures from single base substitutions and frameshift mutations correlating with defective DNA repair (homologous recombination and mismatch repair), suggestive of hypoxic contribution to such genotypes. 27 An increase in insertions and deletions was observed in comparison to single nucleotide variations.…”

Section: Discussionmentioning

confidence: 98%

“…27 The authors also identified mutational signatures from single base substitutions and frameshift mutations correlating with defective DNA repair (homologous recombination and mismatch repair), suggestive of hypoxic contribution to such genotypes. 27 An increase in insertions and deletions was observed in comparison to single nucleotide variations. Rospo and coworkers demonstrated that the incidence of insertions and deletions was much more prevalent in colorectal cancers having DNA repair defects like polymerase E mutations and high microsatellite instability.…”

Section: Discussionmentioning

confidence: 98%

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Hypoxia increases mutational load of breast cancer cells through frameshift mutations

et al. 2020

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Tumor hypoxia-induced downregulation of DNA repair pathways and enhanced replication stress are potential sources of genomic instability. A plethora of genetic changes such as point mutations, large deletions and duplications, microsatellite and chromosomal instability have been discovered in cells under hypoxic stress. However, the influence of hypoxia on the mutational burden of the genome is not fully understood. Here, we attempted to elucidate the DNA damage response and repair patterns under different types of hypoxic stress. In addition, we examined the pattern of mutations exclusively induced under chronic and intermittent hypoxic conditions in two breast cancer cell lines using exome sequencing. Our data indicated that hypoxic stress resulted in transcriptional downregulation of DNA repair genes which can impact the DNA repair induced during anoxic as well as reoxygenated conditions. In addition, our findings demonstrate that hypoxic conditions increased the mutational burden, characterized by an increase in frameshift insertions and deletions. The somatic mutations were random and nonrecurring, as huge variations within the technical duplicates were recognized. Hypoxia also resulted in an increase in the formation of potential neoantigens in both cell lines. More importantly, these data indicate that hypoxic stress mitigates DNA damage repair pathways and causes an increase in the mutational burden of tumor cells, thereby interfering with hypoxic cancer cell immunogenicity.

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Section: Discussionmentioning

confidence: 98%

Section: Discussionmentioning

confidence: 98%

Hypoxia increases mutational load of breast cancer cells through frameshift mutations

et al. 2020

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“…Interestingly, active immune infiltration in fTME seemed to increase hypoxia level. Recently, elevated hypoxia was also found to be associated with increased TMB across cancer types including GC ( 40 ). Because high TMB promotes immune infiltration by producing more novel peptide epitopes or neoantigens ( 41 ), this finding indicated again the association between immune infiltration and hypoxia.…”

Section: Discussionmentioning

confidence: 99%

Tumor Microenvironment Status Predicts the Efficacy of Postoperative Chemotherapy or Radiochemotherapy in Resected Gastric Cancer

Duan

Zeng

et al. 2021

Front. Immunol.

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PurposeChemotherapy (CT) and radiochemotherapy (RCT) are currently the standard postoperative treatments for resected gastric cancer (GC). However, owing to a lack of predictive biomarkers, their efficacy is currently suboptimal. As tumor microenvironment (TME) has the potential to determine treatment response, we investigated the association of TME status with the efficacy of fluoropyrimidine (FU)-based postoperative CT/RCT in resected GC.MethodsPatients with transcriptome data were screened and selected in three independent cohorts. Favorable (fTME) and poor TME (pTME) were defined by a transcriptome-based TME qualification method. Immune infiltration and hypoxia were assessed.ResultsA total of 535 patients were eligible. fTME, indicating the presence of immune activation, was characterized by NK cell rather than CD8+ T cell infiltration. However, postoperative CT/RCT improved overall survival and disease-free survival time more evidently in patients with pTME GC than those with fTME GC. Stratified by stage in fTME GC, stage III patients benefited from postoperative CT/RCT while stage Ib/II patients did not. In comparison, patients with pTME GC benefited from postoperative CT/RCT, regardless of stage. Furthermore, fTME was more hypoxic than pTME, accompanied by a stronger expression of thymidylate synthase (TS)—the target of FU. Stage Ib/II fTME GC was the most hypoxic and had the strongest TS expression across all the subgroups stratified by TME status and stage.ConclusionsWe found that fTME, with the enrichment of NK cells, may predict the lack of postoperative CT/RCT efficacy in stage Ib/II GC, which may be associated with hypoxia and TS expression. Further validations and mechanism researches are needed.

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“…The Supplemental Materials and the scores for intratumor hypoxia were downloaded from Bhandari et al and Buffa et. al, respectively [ 57 , 58 , 69 ]. Mann-Whitney U tests with FDR adjustment were used to compare intercohort scores [ 11 , 52 ].…”

Section: Methodsmentioning

confidence: 99%

Analysis of the TCGA Dataset Reveals that Subsites of Laryngeal Squamous Cell Carcinoma Are Molecularly Distinct

Sorgini

Kim

Zeng

et al. 2020

Cancers

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Laryngeal squamous cell carcinoma (LSCC) from different subsites have distinct presentations and prognosis. In this study, we carried out a multiomic comparison of LSCC subsites. The Cancer Genome Atlas (TCGA) LSCC cohort was analyzed in the R statistical environment for differences between supraglottic and glottic cancers in single nucleotide variations (SNVs), copy number alterations (CNAs), mRNA abundance, protein abundance, pathway overrepresentation, tumor microenvironment (TME), hypoxia status, and patient outcome. Supraglottic cancers had significantly higher overall and smoking-associated SNV mutational load. Pathway analysis revealed upregulation of muscle related pathways in glottic cancer and neural pathways in supraglottic cancer. Proteins involved in cancer relevant signaling pathways including PI3K/Akt/mTOR, the cell cycle, and PDL1 were differentially abundant between subsites. Glottic and supraglottic tumors have different molecular profiles, which may partially account for differences in presentation and response to therapy.

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Divergent mutational processes distinguish hypoxic and normoxic tumours

Cited by 90 publications

References 50 publications

Hypoxia increases mutational load of breast cancer cells through frameshift mutations

Hypoxia increases mutational load of breast cancer cells through frameshift mutations

Tumor Microenvironment Status Predicts the Efficacy of Postoperative Chemotherapy or Radiochemotherapy in Resected Gastric Cancer

Analysis of the TCGA Dataset Reveals that Subsites of Laryngeal Squamous Cell Carcinoma Are Molecularly Distinct

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