A Comprehensive Comparison of Early-Onset and Average-Onset Colorectal Cancers

医学 结直肠癌 内科学 肿瘤科 癌症 儿科
作者
Andrea Cercek,Walid K. Chatila,Rona Yaeger,Henry Walch,Gustavo dos Santos Fernandes,Asha Krishnan,Lerie Palmaira,Anna Maio,Yelena Kemel,Preethi Srinivasan,Chaitanya Bandlamudi,Erin Salo‐Mullen,Prince Ray Tejada,Kimeisha Belanfanti,Jesse Galle,Joseph Vijai,Neil H. Segal,Anna M. Varghese,Diane Reidy‐Lagunes,Jinru Shia,Efsevia Vakiani,Sebastián Mondaca,Robin B. Mendelsohn,Melissa Lumish,Felix Steinruecke,Nancy E. Kemeny,Louise C. Connell,Karuna Ganesh,Arnold J. Markowitz,Garrett M. Nash,José G. Guillem,J. Joshua Smith,Phillip Paty,Liying Zhang,Diana Mandelker,Ozge Birsoy,Mark E. Robson,Kenneth Offit,Barry S. Taylor,Michael F. Berger,David B. Solit,Martin R. Weiser,Leonard Saltz,Julio Garcia‐Aguilar,Nikolaus Schultz,Luis A. Díaz,Zsofia K. Stadler
出处
期刊:Journal of the National Cancer Institute [Oxford University Press]
卷期号:113 (12): 1683-1692 被引量:66
标识
DOI:10.1093/jnci/djab124
摘要

The causative factors for the recent increase in early-onset colorectal cancer (EO-CRC) incidence are unknown. We sought to determine if early-onset disease is clinically or genomically distinct from average-onset colorectal cancer (AO-CRC).Clinical, histopathologic, and genomic characteristics of EO-CRC patients (2014-2019), divided into age 35 years and younger and 36-49 years at diagnosis, were compared with AO-CRC (50 years and older). Patients with mismatch repair deficient tumors, CRC-related hereditary syndromes, and inflammatory bowel disease were excluded from all but the germline analysis. All statistical tests were 2-sided.In total, 759 patients with EO-CRC (35 years, n = 151; 36-49 years, n = 608) and AO-CRC (n = 687) were included. Left-sided tumors (35 years and younger = 80.8%; 36-49 years = 83.7%; AO = 63.9%; P < .001 for both comparisons), rectal bleeding (35 years and younger = 41.1%; 36-49 years = 41.0%; AO = 25.9%; P = .001 and P < .001, respectively), and abdominal pain (35 years and younger = 37.1%; 36-49 years = 34.0%; AO = 26.8%; P = .01 and P = .005, respectively) were more common in EO-CRC. Among microsatellite stable tumors, we found no differences in histopathologic tumor characteristics. Initially, differences in TP53 and Receptor Tyrosine Kinase signaling pathway (RTK-RAS)alterations were noted by age. However, on multivariate analysis including somatic gene analysis and tumor sidedness, no statistically significant differences at the gene or pathway level were demonstrated. Among advanced microsatellite stable CRCs, chemotherapy response and survival were equivalent by age cohorts. Pathogenic germline variants were identified in 23.3% of patients 35 years and younger vs 14.1% of AO-CRC (P = .01).EO-CRCs are more commonly left-sided and present with rectal bleeding and abdominal pain but are otherwise clinically and genomically indistinguishable from AO-CRCs. Aggressive treatment regimens based solely on the age at CRC diagnosis are not warranted.
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