Abstract Purpose: Describe patients, disease characteristics, and treatment patterns of a nationwide cohort of black men with mCRPC in the largest nationwide integrated health care system in the United States: the VHA. Background: Black men have an increased incidence of prostate cancer, are diagnosed at an earlier age than white men with similar demographic and disease characteristics, and experience worse clinical outcomes (1–4). This study examines disease characteristics and treatment practices among black men with mCRPC over a 10-year period for the first 2 lines of therapy in the VHA. Methods: Patient information was obtained from the Veterans Affairs (VA) Clinical Cancer Registry (VACCR) and the VA Corporate Data Warehouse (CDW) to identify patients who were diagnosed with prostate cancer at the VA and later developed mCRPC, defined as: (1) radiologic evidence of metastasis obtained from radiology reports using a natural language processing algorithm (5); (2) evidence of rising prostate-specific antigen (PSA), i.e., 2 consecutive increases in the PSA concentration over a baseline value, retrieved from the CDW/ VA Informatics and Computing Infrastructure (VINCI) Lab Chemistry package using the Clinical Lab Information Retrieval (CLIR) (6); (3) evidence of ongoing androgen deprivation consisting of a serum testosterone level of ≤ 50 ng/dL (≤ 2.0 nmol/L), retrieved from the CDW/ VINCI Lab Chemistry package using the CLIR pipeline, whereby the values were extracted based on the LOINC code and/or lab test name. Treatments of mCRPC were identified by review of the NCCN Prostate Cancer Guidelines V2.2017. Therapies were extracted from CDW pharmacy dispensation records (docetaxel, abiraterone, enzalutamide, etc.). Race/ethnicity data were obtained from VACCR. Classification of race/ethnicity using VA data was previously validated by Kressin et al (7). Charlson Comorbidity Index (CCI) was calculated using Quan comorbidity mapping (8). Results: 120,374 patients were diagnosed with prostate cancer and treated in the VA from 2006 to 2016; of these, 3,637 developed mCRPC, of whom 2,429 (67%) were white, 1,066 (29%) were black, and 142 (4%) were reported as other. Compared with white men, at diagnosis black men were younger (66 vs. 69 years) and had a higher PSA (92.25 ng/mL vs. 41 ng/mL). Disease characteristics at diagnosis were comparable: Gleason 2-6 (1% vs. 1%), 7 (19% vs. 22%), 8-10 (66% vs. 63%); Stages II (28% vs. 32%), III (5% vs. 4%), IV (61% vs. 60%). Treatment did not differ significantly: radiation (26% vs. 26%), prostatectomy (6% vs. 4%), surgical orchiectomy (2% vs. 1%), castration by agonists (85% vs. 86%), castration by agonists/androgen deprivation (34% vs. 33%). Cytotoxic agent docetaxel was the primary first-line therapy for both black and white men (28% and 27%). More white men received first-line abiraterone acetate (AA; 22%) compared with black men (19%), although more black men than white men received second-line AA (17% vs. 14%). Similar treatment patterns between black and white men were observed when the results were further stratified by time period (2006-2010 vs. 2011-2016). Conclusions: This is the first study of a large, nationwide, contemporary cohort of black men with mCRPC treated in an integrated equal-access health care system, the VHA. Consistent with prior reports, black men with mCRPC were younger and had higher PSA values, although treatment patterns between the 2 groups were similar.