T-cell-independent resistance to infection and generation of immunity to Francisella tularensis.

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Infect Immun. 1993 March; 61(3): 823-829

T-cell-independent resistance to infection and generation of immunity to Francisella tularensis.

K L Elkins, T Rhinehart-Jones, C A Nacy, R K Winegar and A H Fortier

Department of Cellular Immunology, Walter Reed Army Institute of Research, Rockville, Maryland 20850.

ABSTRACT

The intraperitoneal 50% lethal dose (LD50) for Francisella tularensisLVS in both normal control heterozygote BALB/c nu/+ mice andBALB/c nu/nu mice was 2 x 10(0). Both nu/+ and nu/nu mice given10(7) LVS bacteria or more intradermally (i.d.) died, with amean time to death of about 7 to 8 days. On the other hand,nu/+ mice given 10(6) LVS bacteria or less survived for morethan 60 days and cleared systemic bacteria, while nu/nu micegiven 10(6) LVS bacteria or less survived for more than 10 daysbut died between days 25 and 30. Thus, the short-term (i.e.,< 10-day) i.d. LD50 of both nu/nu and nu/+ mice was 3 x 10(6),but the long-term (i.e., > 10-day) i.d. LD50 of nu/nu micewas less than 7 x 10(0). The short-term survival of i.d. infectionwas dependent on tumor necrosis factor and gamma interferon:treatment of nu/nu mice with anti-tumor necrosis factor or anti-gammainterferon at the time of i.d. infection resulted in death frominfection 7 to 8 days later, whereas control infected nu/numice survived for 26 days. nu/nu mice infected with LVS i.d.generated LVS-specific serum antibodies, which were predominantlyimmunoglobulin M: titers peaked 7 days after i.d. infectionbut declined sharply by day 21, after which mice died. Surprisingly,nu/nu mice given 10(3) LVS bacteria i.d. became resistant toa lethal challenge (5,000 LD50s) of LVS intraperitoneally within2 days after i.d. infection; nu/nu mice similarly infected withLVS i.d. and challenged with Salmonella typhimurium (10 LD50s)were not protected. nu/nu mice given nu/+ spleen cells intravenouslyas a source of mature T cells survived i.d. infection for morethan 60 days and cleared bacteria. Taken together, these studiesdemonstrate that i.d. infection of nu/nu mice with LVS rapidlygenerates T-cell-independent, short-term, specific protectiveimmunity against lethal challenge, but T lymphocytes are essentialfor long-term survival.

Infect Immun. 1993 March; 61(3): 823-829

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