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The cumulative lifetime risk for prostate cancer was twice as high in patients with Lynch syndrome compared with the general population, according to study results.
“Recently the US Preventive Services Task Force recommended against prostate cancer screening in asymptomatic men under age 50,” lead researcher Victoria M. Raymond, MS, a certified genetic counselor with the University of Michigan’s Cancer Genetics Clinic, told HemOnc Today. “While these recommendations may be appropriate for men at average risk, men with an increased risk for prostate cancer, either due to a family history of prostate cancer or an inherited predisposition to cancer (Lynch syndrome, mutation in HOXB13 or mutation in BRCA2) should be considered for prostate cancer screening.”
Previous studies have assessed prostate cancer risk in patients with Lynch syndrome but led to conflicting results. For this reason, Raymond and colleagues set out to assess cancer history in probands and their first to fourth-degree relatives for 198 independent mutation-positive Lynch syndrome families included in two US cancer registries.
The researchers compared the cumulative lifetime risks and HR estimates for prostate cancer with that of the general population.
Out of 4,127 men, there were 97 prostate cancer cases. Median age at prostate cancer diagnosis was 65 years; 11.53% were diagnosed before age 50.
The cumulative risk for prostate cancer at age 60 years was 6.3% among patients with Lynch syndrome compared with 2.59% for the general population. The cumulative lifetime risk by age 80 was 30% among patients with Lynch syndrome vs. 17.84% for the general population.
Overall, the HR for prostate cancer in those with Lynch syndrome was 1.99 (95% CI, 1.31-3.03).
“It is important to personalize the medical care of individuals, query the family history, and consider genetic consultation and/or genetic testing where appropriate to ensure each patient is receiving the most appropriate management care guidelines,” Raymond said.
In an accompanying editorial, Himisha Beltran, MD, of Weill Cornell Medical College, wrote: “These findings not only have important clinical implications for screening, but also highlight the role of DNA mismatch repair [MMR] in tumor diagnosis. Germline susceptibility of seemingly unrelated tumor types within the spectrum of Lynch syndrome suggests that defects in MMR play key roles in tumor initiation, but additional tissue-specific driving events may also occur throughout tumor progression. Identifying patients with either germline or somatic defects in MMR has prognostic and therapeutic implications, long recognized in colon cancer, which may be applicable to other tumor types, such as prostate cancer.”
For more information:
Beltran H. J Clin Oncol. 2013;doi:10.1200/JCO.2012.48.4667.
Raymond VM. J Clin Oncol. 2013;doi:10.1200/JCO.2012.44.1238.
Victoria M. Raymond, MS, can be reached at University of Michigan, 300 N. Ingalls, Ann Arbor, MI 48109-5419; vraymond@umich.edu.
Disclosure: The researchers report consultant fees from Myriad Genetics and Quest Diagnostics. Beltran reports no relevant financial disclosures.
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