BACKGROUND
Numerous of models have been developed to predict the bone metastasis (BM) risk, however, due to the variety of cancer types, it is difficult for clinicians to Use these models efficiently.
OBJECTIVE
We aimed to perform the pan-cancer analysis to create the cancer classification system for BM, and construct the nomogram for predicting the individualized BM risk.
METHODS
Cancer patients diagnosed between 2010-2018 in the Surveillance, Epidemiology, and End Results (SEER) database were included. Unsupervised hierarchical clustering analysis was performed to create the BM prevalence-based cancer classification system (BM-CCS). Multivariable logistic regression was applied to investigate the possible associated factors for BM and construct a nomogram for BM risk prediction. The patients diagnosed between 2017-2018 in SEER were selected for validating the performance of the BM-CCS and the nomogram, respectively.
RESULTS
A total of 50 cancer types with 243,8680 patients were included in the construction model. Unsupervised hierarchical clustering analysis classified the 50 cancer types into three main phenotypes, namely, categories A, B, and C. The pooled BM prevalence in category A (17.7%; 95%CI: 17.5%-17.8%) was significantly higher than that in category B (5.0%; 95%CI: 4.5%-5.6%) and category C (1.2%; 95%CI: 1.1%-1.4%) (p<0.001). Advanced age, male gender, race, poorly differentiated grade, higher T, N stage, and brain, lung, liver metastasis were significantly associated with BM risk, but the results were not consistent across all cancers. Based on these factors and BM-CCS, we constructed a nomogram for predicting the BM risk. The nomogram showed good calibration and discrimination ability and the decision curve analysis also demonstrated the clinical usefulness.
CONCLUSIONS
The classification system and prediction nomogram may guide the cancer management and individualized BM screening, thus allocating the medical resources to cancer patients. Moreover, it may also have important implications for studying the etiology of BM.