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Quaternary Solar Cells with 12.5% Efficiency Enabled with Non‐Fullerene and Fullerene Acceptor Guests to Improve Open Circuit Voltage and Film Morphology

DOI:10.1002/marc.201900353 期刊:Macromolecular Rapid Communications 出版年份:2019 更新时间:2025-09-11 14:15:04
摘要: Vaccines and antivirals to combat dengue, Zika, and other flavivirus pathogens present a major, unmet medical need. Vaccine development has been severely challenged by the antigenic diversity of these viruses and the propensity of non-neutralizing, cross-reactive antibodies to facilitate cellular infection and increase disease severity. As an alternative, direct-acting antivirals targeting the flavivirus envelope protein, E, have the potential to act via an analogous mode of action without the risk of antibody-dependent enhancement of infection and disease. We previously discovered that structurally diverse small molecule inhibitors of the dengue virus E protein exhibit varying levels of antiviral activity against other flaviviruses in cell culture. Here, we demonstrate that the broad-spectrum activity of several cyanohydrazones against dengue, Zika, and Japanese encephalitis viruses is due to specific inhibition of E-mediated membrane fusion during viral entry and provide proof of concept for pharmacological inhibition of E as an antiviral strategy in vivo.
作者: Jaebong Jang,Chih-Yun Hsia,Pi-Chun Li,Patrice V. Groomes,Melissanne de Wispelaere,Nathanael S. Gray,Jared D. Pitts,Priscilla L. Yang,Nicholas Kwiatkowski,Wenlong Lian,Jinhua Wang
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To develop small molecule inhibitors targeting the flavivirus envelope protein, E, to combat dengue, Zika, and other flavivirus pathogens without the risk of antibody-dependent enhancement of infection and disease.

The study provides proof of concept for the development of direct-acting antivirals that can block E-mediated membrane fusion of multiple flavivirus pathogens. The cyanohydrazone inhibitors, particularly JBJ-01-162-04, show promise as broad-spectrum antivirals against flaviviruses, with improved in vivo properties and reduced cytotoxicity.

The study acknowledges the potential for nonspecific, E-independent mechanisms, including colloidal compound aggregation or other pan-assay interference (PAINS) properties, to contribute to antiviral activity. Additionally, the modest effect observed in vivo may be due to high levels of plasma-protein binding, limiting the compound's antiviral effect.

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