TY - JOUR
T1 - Prevention of rift valley fever in rhesus monkeys with interferon-a
AU - Morrill, John C.
AU - Jennings, Gerald B.
AU - Cosgriff, Thomas M.
AU - Gibbs, Paul H.
AU - Peters, C. J.
PY - 1989/5
Y1 - 1989/5
N2 - Prophylactic and therapeutic efficacy of recombinant leukocyte A interferon (rIFN-aA) and Sendai virus-induced human leukocyte interferon (HuIFN-a) administered intramuscularly to Rift Valley fever virus (RVFV)-infected rhesus monkeys was studied. Clinical, virologic, immunologic, and hemostatic parameters were monitored. Five daily inoculations of 5 x 10s units of either interferon product per kilogram of body weight, initiated 24 hours before or 6 hours after RVFV infection, prevented or greatly suppressed viremia. No clinical signs of disease or laboratory evidence of impaired hemostasis was observed. Serum neutralizing antibody to RVFV was detected within 6 days of virus inoculation. Prophylactic administration of 5 x 104 or 5 x 103 units of rIFN-aA per kilogram also limited viremia, hepatocellular damage, and hemostatic derangement. Untreated, RVFV- infected, control monkeys developed high-titered viremia, clinical disease, and impaired hemostasis. These data suggest that rIFN-aA and HuIFN-a are effective in protecting RVFV-infected rhesus monkeys from viremia and hepatocellular damage and may be beneficial in human RVF infection.
AB - Prophylactic and therapeutic efficacy of recombinant leukocyte A interferon (rIFN-aA) and Sendai virus-induced human leukocyte interferon (HuIFN-a) administered intramuscularly to Rift Valley fever virus (RVFV)-infected rhesus monkeys was studied. Clinical, virologic, immunologic, and hemostatic parameters were monitored. Five daily inoculations of 5 x 10s units of either interferon product per kilogram of body weight, initiated 24 hours before or 6 hours after RVFV infection, prevented or greatly suppressed viremia. No clinical signs of disease or laboratory evidence of impaired hemostasis was observed. Serum neutralizing antibody to RVFV was detected within 6 days of virus inoculation. Prophylactic administration of 5 x 104 or 5 x 103 units of rIFN-aA per kilogram also limited viremia, hepatocellular damage, and hemostatic derangement. Untreated, RVFV- infected, control monkeys developed high-titered viremia, clinical disease, and impaired hemostasis. These data suggest that rIFN-aA and HuIFN-a are effective in protecting RVFV-infected rhesus monkeys from viremia and hepatocellular damage and may be beneficial in human RVF infection.
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U2 - 10.1093/clinids/11.Supplement_4.S815
DO - 10.1093/clinids/11.Supplement_4.S815
M3 - Article
C2 - 2546250
AN - SCOPUS:0000652119
SN - 0162-0886
VL - 11
SP - S815-S825
JO - Reviews of infectious diseases
JF - Reviews of infectious diseases
ER -