Identification of a drug target profile is crucial for clearly understanding of the drug mechanism of action, improvement of the drug efficacy, new indications of the drug, or reduction of side effects. BI1 is one of the second-generation Bruton’s tyrosine kinase (BTK) inhibitors and currently used in clinic for the treatment of CLL. Although BI1 exhibits a good efficacy on CLL, it still remains elusive because of its no or low cytotoxicity on BTK-positive CLL cancer cells at the physiological concentrations. The purpose of this study is to identify a novel drug target profile of BI1 and to understand its mechanism of action in human cancer. I found that the inhibitory efficacy of BI1 on the cancer cell proliferation and mobility is not dependent on the BTK levels in the B cell and prostate cancer cells, and encouraged us to identify novel target(s) of BI1. We collaborated with Dr. Geen-Dong Chang and used an antibody-based approach to pull down the BI1-labeled proteins in human B cell and prostate cancer cells, and applied LC-MS/MS analysis to reveal the identity of the target candidates. With this approach, I isolated L-plastin to be a novel target of BI1. BI1 can form a covalent linkage with L-plastin and suppress its actin-bundling function. The data indicate that L-plastin is a novel target for BI1 to suppress prostate cancer cell invasion. This findings provide more insights into the mechanism which lays behind the drug actions of this newly-developed BTK inhibitor, and give a new opportunity for indication of BI1 against prostate cancer.