Abstract C078: Comprehensive evaluation for contribution of molecular, socioeconomic and disease covariates to colorectal cancer racial survival disparity of 47,178 patients

Background: Racial disparities in survival of Colorectal cancer (CRC), as well as differing frequency of driver gene mutation, have been observed before. Here we observe that self-reported race is associated with overall survival (OS) in a single institutional cohort of 47,178 patients with CRC. we...

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Published in:Cancer epidemiology, biomarkers & prevention biomarkers & prevention, 2023-12, Vol.32 (12_Supplement), p.C078-C078
Main Authors: Yousef, Mahmoud, Yousef, Abdelrahman, Zeineddine, Mohammad, Chowdhury, Saikat, Fanaeian, Mohammad, Little-Jackson, Naoko, Knafl, Mark, Alfaro-Munoz, Kristin, Uppal, Abinheet, Kopetz, Scott, Wang, Wenyi, Willis, Jason, Shen, John Paul
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Language:English
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Summary:Background: Racial disparities in survival of Colorectal cancer (CRC), as well as differing frequency of driver gene mutation, have been observed before. Here we observe that self-reported race is associated with overall survival (OS) in a single institutional cohort of 47,178 patients with CRC. we conducted a systematic investigation of molecular, Socioeconomic (SES) and Disease covariates to quantitate the degree to which each influences OS. Methods: Under an approved IRB protocol, the Palantir-Foundry software system was used to query the MD Anderson (MDA) patient database to identify CRC patients and extract outcomes data and covariates. Genetic mutations that showed significant difference were included with other SES and Disease covariates in Cox-proportional hazard regression model for OS. Preliminary mediation analysis was done to quantify the contribution of each covariate to the OS disparity. Results: 47,178 patients with CRC adenocarcinoma diagnosed between 1973 and 2023 were identified and race (self-reported) was extracted (Asian 1433, 3.0%; African American (AA) 4126, 8.7%; Hispanic 4166, 8.8%; non-Hispanic White (NHW) 37453, 79.4%). Relative to NHW, AA had worse OS (HR=1.22, P= 8.03E-8), while Asians and Hispanics had better OS (HR=0.68, P= 1.06E-8 and HR=0.88, P= 7E-4). Restricting to stage 4 patients, these disparities persisted; AA HR 1.2 (p=1.7E-4) Asian HR 0.67 (p= 1.64E-5), Hispanic HR 0.88 (p= 1.4E-2) relative to NHW. Among 7,628 patients with clinical mutational testing, five genes had significant differences in mutation frequency; APC (45% Asian, 62% AA, 44% NHW, 57% Hispanics, P= 5.83E-3), KRAS (43%, 57%, 44%, 50%, P=3.43E-9), PIK3CA (13%, 23%, 17%, 17%, P=3.37E-3), BRAF (8%, 3%, 8%, 4%, P=1.15E-8), KIT (3%, 2%, 5%, 2%, p=0.046). In multivariate analysis the survival difference between Asians, Hispanics or AA compared to NHW was no longer significant (HR= 0.91, P=0.59, HR= 0.87, P=0.21 and HR=1.14, P= 0.18). In contrast KRAS (HR= 1.5, P=9.22E-9), BRAF (HR= 1.64, P=1E-4) APC mutation (HR= 0.77, P=1E-4) were independently associated with OS, as was higher ECOG (HR= 1.39, P=7.14E-23), higher stage (HR= 1.5, P=3.57E-20), higher national area deprivation index (ADI) quantile (HR=1.08, P= 2.7E-3), being married (HR=1.2, P= 1.52E-2), right side colon tumor (HR=1.22, P= 1.03E-2), poorly differentiated tumors (HR= 1.2, P=1.47E-2), undergoing surgical intervention (HR= 0.47, P=1.54E-29) and MSI-high (HR= 0.41, P=2.16E-6). In our single instit
ISSN:1538-7755
1538-7755
DOI:10.1158/1538-7755.DISP23-C078