Adenomas from individuals with pathogenic biallelic variants in the MUTYH and NTHL1 genes demonstrate base excision repair tumour mutational signature profiles similar to colorectal cancers, expanding potential diagnostic and variant classification applications
Colorectal cancers (CRCs) from people with biallelic germline likely pathogenic/pathogenic variants in or exhibit specific single base substitution (SBS) mutational signatures, namely combined SBS18 and SBS36 (SBS18+SBS36), and SBS30, respectively. The aim was to determine if adenomas from biallelic...
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| Published in | medRxiv : the preprint server for health sciences |
|---|---|
| Main Authors | , , , , , , , , , , , , , , , , , , , , , , , , , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
United States
09.08.2024
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| Subjects | |
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| Abstract | Colorectal cancers (CRCs) from people with biallelic germline likely pathogenic/pathogenic variants in
or
exhibit specific single base substitution (SBS) mutational signatures, namely combined SBS18 and SBS36 (SBS18+SBS36), and SBS30, respectively. The aim was to determine if adenomas from biallelic cases demonstrated these mutational signatures at diagnostic levels.
Whole-exome sequencing of FFPE tissue and matched blood-derived DNA was performed on 9 adenomas and 15 CRCs from 13 biallelic
cases, on 7 adenomas and 2 CRCs from 5 biallelic
cases and on 27 adenomas and 26 CRCs from 46 non-hereditary (sporadic) participants. All samples were assessed for COSMIC v3.2 SBS mutational signatures.
In biallelic
cases, SBS18+SBS36 signature proportions in adenomas (mean±standard deviation, 65.6%±29.6%) were not significantly different to those observed in CRCs (76.2%±20.5%,
=0.37), but were significantly higher compared with non-hereditary adenomas (7.6%±7.0%,
=3.4×10
). Similarly, in biallelic
cases, SBS30 signature proportions in adenomas (74.5%±9.4%) were similar to those in CRCs (78.8%±2.4%) but significantly higher compared with non-hereditary adenomas (2.8%±3.6%,
=5.1×10
). Additionally, a compound heterozygote with the c.1187G>A p.(Gly396Asp) pathogenic variant and the c.533G>C p.(Gly178Ala) variant of unknown significance (VUS) in
demonstrated high levels of SBS18+SBS36 in four adenomas and one CRC, providing evidence for reclassification of the VUS to pathogenic.
SBS18+SBS36 and SBS30 were enriched in adenomas at comparable proportions observed in CRCs from biallelic
and biallelic
cases, respectively. Therefore, testing adenomas may improve the identification of biallelic cases and facilitate variant classification, ultimately enabling opportunities for CRC prevention. |
|---|---|
| AbstractList | Colorectal cancers (CRCs) from people with biallelic germline likely pathogenic/pathogenic variants in
or
exhibit specific single base substitution (SBS) mutational signatures, namely combined SBS18 and SBS36 (SBS18+SBS36), and SBS30, respectively. The aim was to determine if adenomas from biallelic cases demonstrated these mutational signatures at diagnostic levels.
Whole-exome sequencing of FFPE tissue and matched blood-derived DNA was performed on 9 adenomas and 15 CRCs from 13 biallelic
cases, on 7 adenomas and 2 CRCs from 5 biallelic
cases and on 27 adenomas and 26 CRCs from 46 non-hereditary (sporadic) participants. All samples were assessed for COSMIC v3.2 SBS mutational signatures.
In biallelic
cases, SBS18+SBS36 signature proportions in adenomas (mean±standard deviation, 65.6%±29.6%) were not significantly different to those observed in CRCs (76.2%±20.5%,
=0.37), but were significantly higher compared with non-hereditary adenomas (7.6%±7.0%,
=3.4×10
). Similarly, in biallelic
cases, SBS30 signature proportions in adenomas (74.5%±9.4%) were similar to those in CRCs (78.8%±2.4%) but significantly higher compared with non-hereditary adenomas (2.8%±3.6%,
=5.1×10
). Additionally, a compound heterozygote with the c.1187G>A p.(Gly396Asp) pathogenic variant and the c.533G>C p.(Gly178Ala) variant of unknown significance (VUS) in
demonstrated high levels of SBS18+SBS36 in four adenomas and one CRC, providing evidence for reclassification of the VUS to pathogenic.
SBS18+SBS36 and SBS30 were enriched in adenomas at comparable proportions observed in CRCs from biallelic
and biallelic
cases, respectively. Therefore, testing adenomas may improve the identification of biallelic cases and facilitate variant classification, ultimately enabling opportunities for CRC prevention. |
| Author | Pachter, Nicholas Joo, Jihoon E Healey, Emma Georgeson, Peter Winship, Ingrid M Pope, Bernard J Buchanan, Daniel D Medeiros, Ana B D Clendenning, Mark Bernatowicz, Krzysztof Gallinger, Steven Jenkins, Mark A Macrae, Finlay A Groves, Alexandra Joseland, Sharelle Murillo, Brenely V Win, Aung K Mahmood, Khalid Torrezan, Giovana T Spigelman, Allan D Hopper, John L Walker, Romy Gleeson, Margaret Grant, Robert C Como, Julia Poplawski, Nicola Andrews, Lesley Rosty, Christophe Sweet, Kevin Preston, Susan G |
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Camargo Cancer Centre, Sao Paulo, 01508-010, Brazil – sequence: 10 givenname: Brenely V surname: Murillo fullname: Murillo, Brenely V organization: Genetic Services of Western Australia, King Edward Memorial Hospital, Perth, WA, 6008, Australia – sequence: 11 givenname: Nicholas surname: Pachter fullname: Pachter, Nicholas organization: School of Medicine, Curtin University, Perth, WA, 6845, Australia – sequence: 12 givenname: Kevin surname: Sweet fullname: Sweet, Kevin organization: Division of Human Genetics, Department of Internal Medicine, College of Medicine, The Ohio State University, Columbus, OH, 43210, USA – sequence: 13 givenname: Allan D surname: Spigelman fullname: Spigelman, Allan D organization: Surgical Professorial Unit, UNSW Clinical School of Clinical Medicine, Sydney, NSW, 2052, Australia – sequence: 14 givenname: Alexandra surname: Groves fullname: Groves, Alexandra organization: Hunter Family Cancer Service, Newcastle, NSW, 2298, Australia – sequence: 15 givenname: Margaret surname: Gleeson fullname: Gleeson, Margaret organization: Hunter Family Cancer Service, Newcastle, NSW, 2298, Australia – sequence: 16 givenname: Krzysztof surname: Bernatowicz fullname: Bernatowicz, Krzysztof organization: Adult Genetics Unit, Royal Adelaide Hospital, Adelaide, SA 5000, Australia – sequence: 17 givenname: Nicola surname: Poplawski fullname: Poplawski, Nicola organization: Adelaide Medical School, University of Adelaide, Adelaide, South Australia, Australia – sequence: 18 givenname: Lesley surname: Andrews fullname: Andrews, Lesley organization: School of Medicine and Public Health, University of Newcastle, Callaghan, New South Wales, Australia – sequence: 19 givenname: Emma surname: Healey fullname: Healey, Emma organization: Illawarra Cancer Care Centre, Wollongong Hospital, Wollongong, New South Wales 2500 Australia – sequence: 20 givenname: Steven surname: Gallinger fullname: Gallinger, Steven organization: Lunenfeld Tanenbaum Research Institute, Mount Sinai Hospital, University of Toronto, Toronto, ON, Canada – sequence: 21 givenname: Robert C surname: Grant fullname: Grant, Robert C organization: Division of Medical Oncology and Hematology, Princess Margaret Cancer Centre, University Health Network, Toronto, ON, Canada – sequence: 22 givenname: Aung K surname: Win fullname: Win, Aung K organization: Centre for Epidemiology and Biostatistics, Melbourne School of Population and Global Health, VIC, 3053, Australia – sequence: 23 givenname: John L orcidid: 0000-0002-8567-173X surname: Hopper fullname: Hopper, John L organization: Centre for Epidemiology and Biostatistics, Melbourne School of Population and Global Health, VIC, 3053, Australia – sequence: 24 givenname: Mark A surname: Jenkins fullname: Jenkins, Mark A organization: Centre for Epidemiology and Biostatistics, Melbourne School of Population and Global Health, VIC, 3053, Australia – sequence: 25 givenname: Giovana T surname: Torrezan fullname: Torrezan, Giovana T organization: National Institute of Science and Technology in Oncogenomics and Therapeutic Innovation, Sao Paulo 01508-010, Brazil – sequence: 26 givenname: Christophe orcidid: 0000-0001-7671-2651 surname: Rosty fullname: Rosty, Christophe organization: University of Queensland, Brisbane, QLD, 4072, Australia – sequence: 27 givenname: Finlay A orcidid: 0000-0003-4035-9678 surname: Macrae fullname: Macrae, Finlay A organization: Colorectal Medicine and Genetics, The Royal Melbourne Hospital, Parkville, VIC, 3000, Australia – sequence: 28 givenname: Ingrid M surname: Winship fullname: Winship, Ingrid M organization: Department of Medicine, The University of Melbourne, Parkville, VIC, 3000, Australia – sequence: 29 givenname: Daniel D orcidid: 0000-0003-2225-6675 surname: Buchanan fullname: Buchanan, Daniel D organization: Genomic Medicine and Family Cancer Clinic, Royal Melbourne Hospital, Parkville, VIC, 3000, Australia – sequence: 30 givenname: Peter orcidid: 0000-0002-5096-4735 surname: Georgeson fullname: Georgeson, Peter organization: University of Melbourne Centre for Cancer Research, Victorian Comprehensive Cancer Centre, Parkville, VIC, 3010, Australia |
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| Keywords | SBS30 hereditary cancer predisposition adenoma NTHL1 Colorectal cancer SBS36 SBS18 variant of uncertain clinical significance MUTYH mutational signature |
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| Snippet | Colorectal cancers (CRCs) from people with biallelic germline likely pathogenic/pathogenic variants in
or
exhibit specific single base substitution (SBS)... |
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| Title | Adenomas from individuals with pathogenic biallelic variants in the MUTYH and NTHL1 genes demonstrate base excision repair tumour mutational signature profiles similar to colorectal cancers, expanding potential diagnostic and variant classification applications |
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