Author: Neef, Anne B.; Pernot, Lucile; Schreier, Verena N.; Scapozza, Leonardo; Luedtke, Nathan W.
Title: A Bioorthogonal Chemical Reporter of Viral Infection Cord-id: bfhasr8l Document date: 2015_6_26
ID: bfhasr8l
Snippet: Pathogenâ€selective labeling was achieved by using the novel gemcitabine metabolite analogue 2′â€deoxyâ€2′,2′â€difluoroâ€5â€ethynyluridine (dFâ€EdU) and click chemistry. Cells infected with Herpes Simplex Virusâ€1 (HSVâ€1), but not uninfected cells, exhibit nuclear staining upon the addition of dFâ€EdU and a fluorescent azide. The incorporation of the dFâ€EdU into DNA depends on its phosphorylation by a herpes virus thymidine kinase (TK). Crystallographic analyses revealed how d
Document: Pathogenâ€selective labeling was achieved by using the novel gemcitabine metabolite analogue 2′â€deoxyâ€2′,2′â€difluoroâ€5â€ethynyluridine (dFâ€EdU) and click chemistry. Cells infected with Herpes Simplex Virusâ€1 (HSVâ€1), but not uninfected cells, exhibit nuclear staining upon the addition of dFâ€EdU and a fluorescent azide. The incorporation of the dFâ€EdU into DNA depends on its phosphorylation by a herpes virus thymidine kinase (TK). Crystallographic analyses revealed how dFâ€EdU is well accommodated in the active site of HSVâ€1 TK, but steric clashes prevent dFâ€EdU from binding human TK. These results provide the first example of pathogenâ€enzymeâ€dependent incorporation and labeling of bioorthogonal functional groups in human cells.
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