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The future of antiviral immunotoxins
- Source :
- Spiess , K , Høy Jakobsen , M , Kledal , T N & Rosenkilde , M M 2016 , ' The future of antiviral immunotoxins ' , Journal of Leukocyte Biology , vol. 99 , no. 6 , pp. 911-925 .
- Publication Year :
- 2016
-
Abstract
- There is a constant need for new therapeutic interventions in a wide range of infectious diseases. Over the past few years, the immunotoxins have entered the stage as promising antiviral treatments. Immunotoxins have been extensively explored in cancer treatment and have achieved FDA approval in several cases. Indeed, the design of new anticancer immunotoxins is a rapidly developing field. However, at present, several immunotoxins have been developed targeting a variety of different viruses with high specificity and efficacy. Rather than blocking a viral or cellular pathway needed for virus replication and dissemination, immunotoxins exert their effect by killing and eradicating the pool of infected cells. By targeting a virus-encoded target molecule, it is possible to obtain superior selectivity and drastically limit the side effects, which is an immunotoxin-related challenge that has hindered the success of immunotoxins in cancer treatment. Therefore, it seems beneficial to use immunotoxins for the treatment of virus infections. One recent example showed that targeting of virus-encoded 7 transmembrane (7TM) receptors by immunotoxins could be a future strategy for designing ultraspecific antiviral treatment, ensuring efficient internalization and hence efficient eradication of the pool of infected cells, both in vitro and in vivo. In this review, we provide an overview of the mechanisms of action of immunotoxins and highlight the advantages of immunotoxins as future anti-viral therapies.
Details
- Database :
- OAIster
- Journal :
- Spiess , K , Høy Jakobsen , M , Kledal , T N & Rosenkilde , M M 2016 , ' The future of antiviral immunotoxins ' , Journal of Leukocyte Biology , vol. 99 , no. 6 , pp. 911-925 .
- Notes :
- application/pdf, English
- Publication Type :
- Electronic Resource
- Accession number :
- edsoai.on1020643498
- Document Type :
- Electronic Resource