Infective endocarditis (IE) is an infectious disease of the cardiovascular system, and carries a high recurrence and mortality rate. Streptococcus mutans, a member of viridans streptococci, is a commensal in the oral cavity and also one of major opportunistic pathogen for causing IE. Escaping immune surveillance and forming biofilm are two determining virulent factors for bacteria to cause IE. Our previous reports demonstrated that one S. mutans protein, AtlA, not only plays the role in enhancing bacterial resistance against neutrophil killing through binding fibronectin in the plasma, but also contributes to bacterial biofilm formation on the heart valve through mediating extracellular DNA release. Interestingly, we identified a AtlA homologous protein (named Ahp) by using polyclonal antibodies against AtlA. Therefore, we hypothesized Ahp may also play similar roles in modulating S. mutans virulence in biofilm formation and immune evasion. By using in vivo rat experimental IE model, we demonstrated the role of Ahp in the pathogenesis of IE. In vitro assays showed that Ahp majorly plays role in mediating bacterial ability to escape neutrophil killing. More interestingly, we found that S. mutans strains can be grouped into two types according to the intactness of Ahp. When the strain UA159, which originally exhibits the truncated form of Ahp, expresses the intact Ahp, its virulence for causing IE will be dramatically increased. The clinical blood isolates of S. mutans with the intact form of Ahp also exhibit higher abilities to escape immune surveillance and cause IE. These data suggested that Ahp mediates S. mutans to escape neutrophil killing, which contributes to the pathogenesis of IE.