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Published in: Virology Journal 1/2010

Open Access 01-12-2010 | Hypothesis

A new therapeutic strategy for lung tissue injury induced by influenza with CR2 targeting complement inhibitior

Authors: Chuanfu Zhang, Yuanyong Xu, Leili Jia, Yutao Yang, Yong Wang, Yansong Sun, Liuyu Huang, Fei Qiao, Stephen Tomlinson, Xuelin Liu, Yusen Zhou, Hongbin Song

Published in: Virology Journal | Issue 1/2010

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Abstract

Background

Influenza is a respiratory disease that seriously threatens human health. In fact, influenza virus itself does not make critical contribution to mortality induced by influenza, but "cytokine storm" produced by the excessive immune response triggered by the virus can result in inflammatory reaction of lung tissues and fatal lung tissue injury, and thus increase influenza mortality. Therefore, besides antiviral drugs, immunosuppression drugs should also be included in infection treatment.

Presentation of the hypothesis

Complement is the center of inflammatory reaction. If complement system is over activated, the body will have strong inflammatory reaction or tissue injury, resulting in pathological process. Many studies have proved that, inflammatory injury of lung tissues caused by influenza virus is closely related to complement activation. Therefore, inhibiting complement activation can significantly reduce inflammatory injury in lung tissues. As complement is both a physiological defense and pathological damage medium, systematic inhibition may result in side effects including infection. Therefore, we design targeting complement inhibitors for complement activation sites, i.e. with CR2 as targeting vector, complement inhibitors like CD59 and Crry are targeted to inflammatory sites to specially inhibit the complement activation in local injury, thus local inflammatory reaction is inhibited.

Testing the hypothesis

CR2-CD59 and CR2-Crry targeting complement inhibitors are fusion-expressed, and their biological activity is examined via in vivo and in vitro tests. CR2 targeting complement inhibitors are used to treat mouse influenza viral pneumonia model, with PBS treatment group as the control. The survival and lung tissue injury of the mice is observed and the effect of CR2 targeting complement inhibitors on pneumonia induced by influenza virus is evaluated.

Implications of the hypothesis

CR2 targeting complement inhibitors are expected to be ideal drugs for viral pneumonia.
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Metadata
Title
A new therapeutic strategy for lung tissue injury induced by influenza with CR2 targeting complement inhibitior
Authors
Chuanfu Zhang
Yuanyong Xu
Leili Jia
Yutao Yang
Yong Wang
Yansong Sun
Liuyu Huang
Fei Qiao
Stephen Tomlinson
Xuelin Liu
Yusen Zhou
Hongbin Song
Publication date
01-12-2010
Publisher
BioMed Central
Published in
Virology Journal / Issue 1/2010
Electronic ISSN: 1743-422X
DOI
https://doi.org/10.1186/1743-422X-7-30

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