News Release

Younger age associated with increased likelihood of targetable genotype in lung cancer

Peer-Reviewed Publication

JAMA Network

Patients younger than 50 diagnosed with non-small-cell lung cancer (NSCLC) had a higher likelihood of having a targetable genomic alteration for which therapies exist, according to an article published online by JAMA Oncology.

NSCLC in young patients is rare and the clinical characteristics of the disease are poorly understood. A definition for young age describing this unique population has not been established.

Geoffrey R. Oxnard, M.D., of the Dana-Farber Cancer Institute, Boston, and coauthors examined the relationship between young age at diagnosis and the presence of a potentially targetable genomic alteration and prognosis.

The study included 2,237 patients with NSCLC who underwent genotyping between 2002 and 2014. Of the patients, 1,939 (87 percent) had histologically confirmed adenocarcinoma, 269 (12 percent) has NSCLC not otherwise specified, and 29 (1 percent) had squamous histologic findings. About 63 percent (1,396 patients) had either stage IIIB or stage IV cancers; the median age was 62 years and 27 percent (594 patients) had never smoked.

Across the entire group of patients, 712 of them (32 percent) had a targetable genomic alteration for which approved therapies exist or where compelling clinical trial data suggest the potential for targeted therapy.

Among 1,325 patients tested for all five targetable genomic alterations, younger age was associated with an increased likelihood of a targetable genotype. Patients diagnosed younger than 50 had a 59 percent increased chance of detecting a targetable alteration compared with an older patient, according to the results. Lowest overall median survival was in patients younger than 40 (18.2 months) and those patients older than 70 (13.6 months), the study indicates.

The authors note study limitations, including the retrospective or historical nature of the data, as well as limited comprehensive data on individual patient treatment.

"Despite the aforementioned limitations, the findings of this study expand the current understanding of the genetics and biology of lung cancer in young patients. These patients possess a uniquely high incidence of targetable genomic alterations paired with an unexpectedly poor prognosis. This combination of opportunity and risk defines the treatment of NSCLC in young patients and requires unique therapeutic and research strategies," the study concludes.

Editor's Note: Young Patients with Lung Cancer

"While these results and conclusions are limited by the referral bias to a center of excellence to which younger patients and those with an identified mutation likely gravitated, almost certainly creating a skewed study population that is not necessarily generalizable to the broader lung cancer population, this work provides an invaluable early step toward identifying the youngest patients with lung cancer as a subgroup that deserves more study and special consideration as a distinct clinical demographic most likely to benefit from a more extensive search for targetable driver mutations," writes Howard (Jack) West, M.D., web editor of JAMA Oncology in a related Editor's Note.

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(JAMA Oncol. Published online December 17, 2015. doi:10.1001/jamaoncol.2015.4482. Available pre-embargo to the media at http://media.jamanetwork.com.)

Editor's Note: The study includes conflict of interest and funding/support disclosures. Please see the article for additional information, including other authors, author contributions and affiliations, financial disclosures, funding and support, etc.

Media Advisory: To contact corresponding author Geoffrey R. Oxnard, M.D., call Anne Doerr at 617-632-4090 or email anne_doerr@dfci.harvard.edu. To contact editor's note author Howard (Jack) West, M.D., email mediarelations@jamanetwork.org


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