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Mutations missed in early-onset colorectal cancer

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Multigene testing needed for early-onset colorectal cancer

This study illustrates the shortcomings of current algorithms for diagnosing and managing younger patients with CRC. First, although family history is one of the main components used to stratify an individual’s risk for CRC, it is imperfect because only one in five younger patients with CRC reported having a first-degree relative with CRC. Second, although clinical criteria define the phenotypes typically associated with specific gene mutations, variability in penetrance and expressivity can result in overlap among the different hereditary cancer syndromes (e.g., BRCA germline mutations in younger patients with CRC).

The findings of this large population-based study demonstrate that the incorporation of multigene panel genetic testing in the evaluation of patients with CRC will increase the diagnosis of individuals with genetic predisposition to cancer and will expand current knowledge regarding the associated phenotypes, further supporting the cost-effectiveness of testing that can guide management for patients with cancer and their at-risk relatives. The study found germline mutations in one in six patients with CRC and has argued for comprehensive germline genetic testing of patients diagnosed at younger than 50 years.

Eduardo Vilar-Sanchez, MD, PhD, is in the department of clinical cancer prevention and clinical cancer genetics program at The University of Texas MD Anderson Cancer Center, Houston. Elena M. Stoffel, MD, is in the department of internal medicine at the University of Michigan, Ann Arbor. These comments are adapted from an editorial (JAMA Oncology 2016 Dec 15. doi: 10.1001/jamaoncol.2016.5193). No conflicts of interest were declared.


 

FROM JAMA ONCOLOGY

As many as one in six patients with early-onset colorectal cancer (CRC) have a pathogenic genetic mutation, but around one-third of these patients may not have met the criteria for genetic testing for at least one of their mutations under current guidelines, researchers say.

Rachel Pearlman, MS, CGC, of The Ohio State University Comprehensive Cancer Center, and her coauthors reported the results of multigene panel testing of 450 patients aged under 50 years, from 51 institutions, who had been diagnosed with CRC (JAMA Oncol 2016 Dec 15. doi: 10.1001/jamaoncol.2016.5194).

Overall, 16% of patients were found to have a pathogenic or likely pathogenic cancer susceptibility gene mutations, with 83.3% having at least one gene mutation.

Thirty-seven patients had Lynch syndrome; 13 were MLH1, 16 were LSH2, 1 patient was MSH2/monoallelic MUTYH; 2 were MSH6, and 5 were PMS2.

“While the prevalence of Lynch syndrome reported herein (8.4%) is consistent with previous publications, this is the first study to our knowledge to determine the prevalence and spectrum of other hereditary cancer syndromes (8%) found in an unselected series of patients with early-onset CRC,” the authors wrote.

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Forty-eight patients (10.7%) had mismatch repair–deficient tumors, nine of which were in high-penetrance genes linked to CRC risk.

But for 145 patients, their genetic variants were of uncertain significance. Thirteen patients had mutations in high- or moderate-penetrance genes not traditionally associated with CRC, including ATM, ATM/ CHEK2, BRCA1, BRCA2, CDKN2A, and PALB2.

The authors pointed out that the multigene panel testing approach enables identification of hereditary cancer syndromes in patients who might not have otherwise met the criteria for testing.

“Importantly, 24 of 72 patients (33.3%) with pathogenic mutations did not meet NCCN Guidelines for at least 1 of the gene(s) in which they were found to have a mutation,” the researchers noted. These included three patients with MMR-deficient tumors who had additional mutations in genes that would not have been assessed, one patient with an MMR-proficient tumor who was also found to have Lynch syndrome, and six patients with BRCA1/2 mutations.

“Previous studies have reported early-onset CRC in women with BRCA1 mutations and BRCA2 mutations in families with familial colorectal cancer type X,” they noted.

The Ohio Colorectal Cancer Prevention Initiative (OCCPI) is supported by a grant from Pelotonia, and by the National Cancer Institute. Myriad Genetics Inc. donated next-generation sequencing testing. Nine authors disclosed ties with private industry, including Myriad Genetics.

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