Racial differences in endometrial cancer molecular portraits in The Cancer Genome Atlas
Endometrial cancer (EC) is now the most prevalent gynaecological malignancy in the Western world. Black or African American women (BoAA) have double the mortality of Caucasian women, and their tumours tend to be of higher grade. Despite these disparities, little is known regarding the mutational lan...
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| Veröffentlicht in: | Oncotarget 2018-03, Vol.9 (24), p.17093-17103 |
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| creator | Guttery, David S Blighe, Kevin Polymeros, Konstantinos Symonds, R Paul Macip, Salvador Moss, Esther L |
| description | Endometrial cancer (EC) is now the most prevalent gynaecological malignancy in the Western world. Black or African American women (BoAA) have double the mortality of Caucasian women, and their tumours tend to be of higher grade. Despite these disparities, little is known regarding the mutational landscape of EC between races. Hence, we wished to investigate the molecular features of ECs within The Cancer Genome Atlas (TCGA) dataset by racial groupings. In total 374 Caucasian, 109 BoAA and 20 Asian patients were included in the analysis. Asian women were diagnosed at younger age, 54.2 years versus 64.5 years for Caucasian and 64.9 years for BoAA women (OR 3.432; p=0.011); BoAA women were more likely to have serous type tumors (OR 2.061; p=0.008). No difference in overall survival was evident. The most frequently mutated gene in Caucasian and Asian tumours was
(63% and 85%), unlike BoAA cases where it was
(49%). Mutation and somatic copy number alteration (SCNA) analysis revealed an enrichment of
mutations in BoAAs; whereas
and
mutations were more frequent in Caucasians. Major recurrent SCNA racial differences were observed at chromosomes 3p, 8, 10, and 16, which clustered BoAA tumors into 4 distinct groups and Caucasian tumors into 5 groups. There was a significantly higher frequency of somatic mutations in DNA mismatch repair genes in Asian tumours, in particular
(p=0.0036). In conclusion, inherent racial disparities appear to be present in the molecular profile of EC, which could have potential implications on clinical management. |
| doi_str_mv | 10.18632/oncotarget.24907 |
| format | Article |
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(63% and 85%), unlike BoAA cases where it was
(49%). Mutation and somatic copy number alteration (SCNA) analysis revealed an enrichment of
mutations in BoAAs; whereas
and
mutations were more frequent in Caucasians. Major recurrent SCNA racial differences were observed at chromosomes 3p, 8, 10, and 16, which clustered BoAA tumors into 4 distinct groups and Caucasian tumors into 5 groups. There was a significantly higher frequency of somatic mutations in DNA mismatch repair genes in Asian tumours, in particular
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(63% and 85%), unlike BoAA cases where it was
(49%). Mutation and somatic copy number alteration (SCNA) analysis revealed an enrichment of
mutations in BoAAs; whereas
and
mutations were more frequent in Caucasians. Major recurrent SCNA racial differences were observed at chromosomes 3p, 8, 10, and 16, which clustered BoAA tumors into 4 distinct groups and Caucasian tumors into 5 groups. There was a significantly higher frequency of somatic mutations in DNA mismatch repair genes in Asian tumours, in particular
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(63% and 85%), unlike BoAA cases where it was
(49%). Mutation and somatic copy number alteration (SCNA) analysis revealed an enrichment of
mutations in BoAAs; whereas
and
mutations were more frequent in Caucasians. Major recurrent SCNA racial differences were observed at chromosomes 3p, 8, 10, and 16, which clustered BoAA tumors into 4 distinct groups and Caucasian tumors into 5 groups. There was a significantly higher frequency of somatic mutations in DNA mismatch repair genes in Asian tumours, in particular
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| title | Racial differences in endometrial cancer molecular portraits in The Cancer Genome Atlas |
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