Colorectal cancers (CRCs) are rare in adolescents and adults ages 25 years or younger. We analyzed clinical, pathology, and molecular features of colorectal tumors from adolescents and young adults in an effort to improve genetic counseling, surveillance, and, ultimately, treatment and outcomes.
Methods
We analyzed clinical data and molecular and genetic features of colorectal tumor tissues from 139 adolescents or young adults (age, ≤25 y; median age, 23 y; 58% male), collected from 2000 through 2017; tumor tissues and clinical data were obtained from the nationwide network and registry of histopathology and cytopathology and The Netherlands Cancer Registry, respectively. DNA samples from tumors were analyzed for microsatellite instability, mutations in 56 genes, and genome-wide somatic copy number aberrations.
Results
Mucinous and/or signet ring cell components were observed in 33% of tumor samples. A genetic tumor risk syndrome was confirmed for 39% of cases. Factors associated with shorter survival time included younger age at diagnosis, signet ring cell carcinoma, the absence of a genetic tumor risk syndrome, and diagnosis at an advanced stage of disease. Compared with colorectal tumors from patients ages 60 years or older in the Cancer Genome Atlas, higher proportions of tumors from adolescents or young adults were microsatellite stable with nearly diploid genomes, or contained somatic mutations in TP53 and POLE, whereas lower proportions contained mutations in APC.
Conclusions
We found clinical, molecular, and genetic features of CRCs in adolescents or young adults to differ from those of patients older than age 60 years. In 39% of patients a genetic tumor risk syndrome was identified. These findings provide insight into the pathogenesis of CRC in young patients and suggest new strategies for clinical management. Performing genetic and molecular analyses for every individual diagnosed with CRC at age 25 years or younger would aid in this optimization.
Keywords
SCNA
Colon Cancer
MSI
MSS
Abbreviations used in this paper
AYA-CRC
children, adolescents, and young adults with colorectal cancer
Nationwide network and registry of histo- and cytopathology
POLE-exo
POLE exonuclease domain
SCNA
somatic copy number alteration
smMIP
single-molecule molecular inversion probe
SRCC
signet ring cell carcinoma
TCGA
The Cancer Genome Atlas
Cited by (0)
Current address for M.C.J.J.: Princess Maxima Center for Pediatric Oncology, Utrecht, The Netherlands, and Department of Clinical Genetics, University Medical Center Utrecht, Utrecht, The Netherlands
Conflicts of interest The authors disclose no conflicts.
Funding Supported by the Dutch Digestive Foundation FP13-19 (M.J.L.L.). The funding source had no role in the study design, conduct, data analysis and interpretation, or manuscript writing.
