Spn7 is responsible for ~2 million

Spn7 is responsible for ~2 million childhood deaths annually in children ,5 y of age, mostly in low-income countries. Approx- imately 90% of these deaths occur in infants with pneumonia (1). The pathogen also accounts for a high burden of early childhood sepsis, meningitis, and otitis media. In developing countries, undernutrition increases susceptibility to severe dis-
ease(2,3). Efforts tocontrol bacterial infections focus onprompt treatment with first-line antibiotics. However, the rapid spread of antibiotic-resistant strains has threatened to decrease the efficacy and increase the cost of treatment (4). The problem is of greatest significance in low-income countries where many bacterial infections are resistant to first-line antibiotics (5,6). Furthermore, second-line therapies are often unavailable or unaffordable, making these infections difficult to treat, ulti- mately facilitating the spread of drug-resistant strains. The nasopharynx is the primary reservoir for Spn in the human body and is the main source of infection (7,8). Spn conjugate vaccines are efficacious in preventing invasive disease and in lowering the horizontal spread of infection by reducing NP carriage of vaccine strains (9,10). However, concerns about the highcostofthesevaccines,thelimited-serotypeprotection,andthe threat of replacement colonization with potentially pathogenic nonvaccine strains prevent their widespread use in developing countries (7,11–13). In addition, the first dose of these vaccines cannot be administered before the second month of life, leaving young infants with partial, if any, immunity to Spn. Research on complementary strategies to prevent bacterial infection and block disease transmission in early infancy is needed. VA plays a critical role as a modulator of the immune re- sponse; however, its role in the prevention of bacterial infections