Because the process of macropinocytosis is non-specific, many
pathogens take advantage of macropinosomes to infect their target cells. In this way, pathogens internalized in macropinosomes avoid barriers and obstructions that the plasma membrane, cytoplasmic crowding and cortical cytoskeleton pose when moving deeper into the cytoplasm.
Vaccinia virus (VACV), a member of
Poxviridae family, has also been shown to partially utilize macropinocytosis for infectious cell entry. Here, both infectious forms of VACV, mature virion (MV) and enveloped virion (EV), induce their own macropinocytosis by binding to the cell surface and triggering an actin-mediated plasma membrane protrusion that eventually collapses back onto the plasma membrane sealing the attached virion inside a macropinosome, which then goes through a maturation program that leads to core activation and genome release.
Shiga toxin produced by
enterohemorrhagic E. coli has been shown to enter target cells via macropinocytosis, causing
gastrointestinal tract complications. Other pathogens that have been shown to utilize this mechanism are
Kaposi's sarcoma-associated herpesvirus and
Salmonella. == References ==