Cancer stem cells (CSCs)/cancer initiating cells represent a minor population of tumor cells with the properties of self-renewal or cancer progenitor cells, contributing to tumor progression. To further delineate the molecular mechanisms of prostate cancer progression linked to the expression changes of stem cell-related genes, a prostate cancer progression model was established by orthotopic injection of prostate cancer CWR22Rv1 cells into nude mice. Fourteen weeks after the injection, the tumor cells metastazing into the lung were isolated as 14w CWR22Rv1 cells. Interestingly, the expression level of hepatocyte growth factor activator inhibitor type 2 (HAI-2) in 14w CWR22Rv1 cells was down-regulated, while the expression levels of the stem cell-related transcription factors (Oct-4 and Nanog), the activated level of matriptase and the tyrosine phosphorylation level of c-Met were increased in these cells. To further clarify if HAI-2 played a role in modulating prostate cancer malignancy, we used HAI-2 shRNAs to silence HAI-2 expression, and found that the knockdown of HAI-2 enhanced CWR22Rv1 cell invasion, migration, sphere formation, and the expression levels of Sox2. Moreover, HAI-2 knockdown activated matriptase and the phosphorylation of c-Met, EGFR and ERK. In addition, overexpression of HAI-2 or HAI-1 in 14w CWR22Rv1 cells down-regulated the expression of Sox2 and significantly activated matriptase and the phosphorylation of c-Met. Our data further showed that an increase of matriptase activation by overexpression had similar effects to HAI-2-knockdown cells on Sox2 expression, the phosphorylation of c-Met as well as sphere-forming potentials. Furthermore, inhibition of the c-Met kinase activity in HAI-2-knockdown cells reduced the expression of Sox2. Therefore, our data suggest that HAI-2 may play an inhibitory role in regulating the stem cell-related properties of prostate cancer cells through modulating matriptase and c-Met pathways.