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Inhibition of diverse opportunistic viruses by structurally optimized retrograde trafficking inhibitors
Authors:Dhimant Desai  Matthew Lauver  Alexandria Ostman  Linda Cruz  Kevin Ferguson  Ge Jin  Brianne Roper  Daniel Brosius  Aron Lukacher  Shantu Amin  Nick Buchkovich
Affiliation:1. Department of Microbiology & Immunology, Penn State College of Medicine, 500 University Drive, Hershey, PA 17033, United States;2. Department of Pharmacology, Penn State College of Medicine, 500 University Drive, Hershey, PA 17033, United States
Abstract:Opportunistic viruses are a major problem for immunosuppressed individuals, particularly following organ or stem cell transplantation. Current treatments are non-existent or suffer from problems such as high toxicity or development of resistant strains. We previously published that a trafficking inhibitor that targets a host protein greatly reduces the replication of human cytomegalovirus. This inhibitor was also shown to be moderately effective against polyomaviruses, another family of opportunistic viruses. We have developed a panel of analogues for this inhibitor and have shown that these analogues maintain their high efficacy against HCMV, while substantially lowering the concentration required to inhibit polyomavirus replication. By targeting a host protein these compounds are able to inhibit the replication of two very different viruses. These observations open up the possibility of pan-viral inhibitors for immunosuppressed individuals that are effective against multiple, diverse opportunistic viruses.
Keywords:HCMV  human cytomegalovirus  STX5  syntaxin 5  MuPyV  mouse polyomavirus  LT  large tumor antigen  Human cytomegalovirus  Mouse polyomavirus  Antivirals  Syntaxin 5  Retrograde trafficking
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