Anginosus group streptococci (AGS) and Mitis group streptococci (MGS) are commensal streptococci habitual in the oral cavity of human. Except for typical human pathogen S. pneumoniae, most of the species/strains belonging to AGS and MGS are recognized as an opportunistic pathogen, and clinical importance is often underestimated. However, a part of species/strains belonging to these groups of human origin shows β-hemolysis and two kinds of β-hemolysin are known among them. One is the protein toxin generally called cholesterol-dependent cytolysin (CDC), and another is the homologs of streptolysin S (SLS) that is a post-translationally modified peptide toxin. Interestingly, there are structural- and functional-diversity among the β-hemolysins of AGS and MGS, compared to the representative streptococcal β-hemolysins such as streptolysin O and SLS from Pyogenic group streptococci such as S. pyogenes. Especially, CDCs produced from S. intermedius of AGS and from a part of strains of S. mitis and S. pseudopneumoniae of MGS shows human-specific and -preferential activity, respectively. These specificities thought to be important for the pathogenicity toward human. Based on our studies, I intend to introduce the information on the diversities of the β-hemolysins produced by β-hemolytic AGS and MGS and their contribution to the potential pathogenicity of β-hemolytic AGS and MGS.