Antiviral chemotherapy facilitates control of poxvirus infections through inhibition of cellular signal transduction
Hailin Yang, … , Raymond M. Welsh, Ellis L. Reinherz
Hailin Yang, … , Raymond M. Welsh, Ellis L. Reinherz
Published February 1, 2005
Citation Information: J Clin Invest. 2005;115(2):379-387. https://doi.org/10.1172/JCI23220.
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Article Infectious disease

Antiviral chemotherapy facilitates control of poxvirus infections through inhibition of cellular signal transduction

Abstract

The EGF-like domain of smallpox growth factor (SPGF) targets human ErbB-1, inducing tyrosine phosphorylation of certain host cellular substrates via activation of the receptor’s kinase domain and thereby facilitating viral replication. Given these findings, low molecular weight organic inhibitors of ErbB-1 kinases might function as antiviral agents against smallpox. Here we show that CI-1033 and related 4-anilinoquinazolines inhibit SPGF-induced human cellular DNA synthesis, protein tyrosine kinase activation, and c-Cbl association with ErbB-1 and resultant internalization. Infection of monkey kidney BSC-40 and VERO-E6 cells in vitro by variola strain Solaimen is blocked by CI-1033, primarily at the level of secondary viral spreading. In an in vivo lethal vaccinia virus pneumonia model, CI-1033 alone promotes survival of animals, augments systemic T cell immunity and, in conjunction with a single dose of anti-L1R intracellular mature virus particle-specific mAb, fosters virtually complete viral clearance of the lungs of infected mice by the eighth day after infection. Collectively, these findings show that chemical inhibitors of host-signaling pathways exploited by viral pathogens may represent potent antiviral therapies.

Authors

Hailin Yang, Sung-Kwon Kim, Mikyung Kim, Pedro A. Reche, Tiara J. Morehead, Inger K. Damon, Raymond M. Welsh, Ellis L. Reinherz

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Postexposure therapy of VV infection in the C57BL/6 pneumonia model. Mic...
Postexposure therapy of VV infection in the C57BL/6 pneumonia model. Mice were inoculated i.n. with 2 × 104 PFU of VV, and 2 days later were treated with a single dose of mAb L1R or control mAb and/or with CI-1033, the latter given daily until termination of the experiment. Mice were sacrificed on different days after infection and examined for lung weight (A), VV PFU/lung (B), and the number of anti-CD3–induced IFN-γ–producing CD8+ T cells per spleen (C). For days 6, 7, and 8, group sizes of 3–4, 5, or 6 animals, respectively, were employed. At day 8, 2 of 6 anti–L1R-treated mice had undetectable virus, whereas 5 of 6 anti-L1R plus CI-1033–treated mice had undetectable virus. For calculation of mean titers, the lowest detectable titer possible (1 log) was used for mice without detectable virus, such that the means are actually lower values. *P < 0.05.