Pleiotropic cytotoxicity of VacA toxin in host cells and its impact on immunotherapy.

In the recent decades, a number of studies have highlighted the importance of in the initiation and development of peptic ulcer and gastric cancer. Some potential virulence factors (e.g., urease, CagA, VacA, BabA) are exploited by this microorganism, facilitating its persistence through evading human defense mechanisms. Among these toxins and enzymes, vacuolating toxin A (VacA) is of a great importance in the pathogenesis of H. pylori. VacA toxin shows different pattern of cytotoxicity through binding to different cell surface receptors in various cells. To highlight attempts in treatment for H. pylori infection, here, we discussed the VacA potential as a candidate for development of vaccine and targeted immunotherapy. Furthermore, we reviewed the related literature to provide key insights on association of the genetic variants of VacA with the toxicity of the toxin in cells. A number of investigations on the receptor(s) binding of VacA toxin confirmed the pleiotropic nature of VacA that uses a unique mechanism for internalization through some membrane components such as lipid rafts and glycophosphatidylinositol (GPI)-anchored proteins (GPI-AP). Considering the high potency of VacA toxin in the clinical presentations in infection and assisting persistence and colonization of , it is considered as one of the pivotal components in production vaccines and monoclonal antibodies (mAbs). It is possible to generate mAbs with a considerable potential to convert into secretory immunoglobulins that could penetrate into the niche of and inhibit its normal functionalities. Further, conjugation of targeting Ab fragments with the toxic agents or drug delivery systems (DDSs) offers new generation of treatments.