TY - JOUR
T1 - TNFα, interferon, and stress response induction as a function of age- related susceptibility to fatal sindbis virus infection of mice
AU - Trgovcich, Joanne
AU - Aronson, Judith F.
AU - Eldridge, J. Charles
AU - Johnston, Robert E.
N1 - Funding Information:
We acknowledge Kate Ryman for helpful suggestions and criticisms in the preparation of the manuscript. We also thank Pam Extrom, Cherice Connor, and Travis Knott for excellent technical assistance. This work was supported by PHS-NIH Grant AI22186, and J.T. was supported by an Augmentation Award for Science and Engineering Research Training, DAAL03-92-G-0084.
PY - 1999/10/25
Y1 - 1999/10/25
N2 - The age-related acquisition of resistance to fatal Sindbis virus infection was examined using a molecularly cloned laboratory strain of the AR339 isolate designated TRSB. TRSB caused 100% mortality in mice up to 5 days of age. Resistance to fatal infection developed abruptly between 5 and 9 days of age. Lethal Sindbis virus infection of mice inoculated at 4 days of age was characterized by high levels of virus replication, induction of high levels of interferon-α/β and TNF-α and severe thymic involution indicative of a systemic stress response. These changes correlated with predominantly noninflammatory lesions. In contrast, TRSB infection of older mice was characterized by survival, more limited virus replication, reduced cytokine induction, and the development of inflammatory responses leading to encephalitis, myositis, and myocarditis. Previous studies utilized infections of neonatal mice with TRSB and an attenuated mutant of TRSB to compare fatal and nonfatal Sindbis infection (Trgovcich et al., 1996. Virology 224, 73-83). The experiments reported here utilize mouse age at the time of infection to create conditions for examination of fatal and nonfatal TRSB infections. Both experiments suggest that fatal infection is associated with a shock-like syndrome and little or no inflammatory pathology, while survival is correlated with greatly reduced cytokine levels and inflammatory lesions.
AB - The age-related acquisition of resistance to fatal Sindbis virus infection was examined using a molecularly cloned laboratory strain of the AR339 isolate designated TRSB. TRSB caused 100% mortality in mice up to 5 days of age. Resistance to fatal infection developed abruptly between 5 and 9 days of age. Lethal Sindbis virus infection of mice inoculated at 4 days of age was characterized by high levels of virus replication, induction of high levels of interferon-α/β and TNF-α and severe thymic involution indicative of a systemic stress response. These changes correlated with predominantly noninflammatory lesions. In contrast, TRSB infection of older mice was characterized by survival, more limited virus replication, reduced cytokine induction, and the development of inflammatory responses leading to encephalitis, myositis, and myocarditis. Previous studies utilized infections of neonatal mice with TRSB and an attenuated mutant of TRSB to compare fatal and nonfatal Sindbis infection (Trgovcich et al., 1996. Virology 224, 73-83). The experiments reported here utilize mouse age at the time of infection to create conditions for examination of fatal and nonfatal TRSB infections. Both experiments suggest that fatal infection is associated with a shock-like syndrome and little or no inflammatory pathology, while survival is correlated with greatly reduced cytokine levels and inflammatory lesions.
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U2 - 10.1006/viro.1999.9913
DO - 10.1006/viro.1999.9913
M3 - Article
C2 - 10544107
AN - SCOPUS:0033604155
SN - 0042-6822
VL - 263
SP - 339
EP - 348
JO - Virology
JF - Virology
IS - 2
ER -