Intracellular bacteria
Viruses
Parasite

ABMA protects cells against four bacterial toxins ( Corynebacterium diphtheriae (DT; EC ₅₀ of 62.9 μM), Bacillus anthracis (LT), Clostridium difficile toxin B (TcdB; EC ₅₀ of 73.3?μM), Clostridium sordellii lethal toxin (TcsL; EC ₅₀ of 86.7 μM)), three viruses (Ebola (EC ₅₀ of 3.3?μM), rabies (EC ₅₀ of 19.4?μM), dengue-4 virus ( EC ₅₀ of 8.2?μM)), two species of Chlamydiales intracellular bacteria ( Simkania negevensis and Chlamydia trachomatis ), and the parasite Leishmania infantum (EC ₅₀ of 7.1?μM) at micromolar level.
In A549 cells, ABMA treatment induces a decrease in ricin cytotoxicity with an EC ₅₀ of 3.8?μM, and a protection factor (R) at 30?μM ranging from 5 to 10. ABMA retained almost 100% of its biological activity against ricin-induced cytotoxicity up to six days.

ABMA (2-200 mg/kg; intraperitoneal injection; female BALB/c mice) treatment protects mice from nasal instillation of an LD ₉₀ of ricin.