Journal
CELL REPORTS
Volume 40, Issue 1, Pages -Publisher
CELL PRESS
DOI: 10.1016/j.celrep.2022.111030
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Funding
- Chinese Academy of Medical Sciences (CAMS) Innovation Fund for Medical Sciences [2021-I2M-1-043]
- CRP-ICGEB Research Grant 2019 [CRP/CHN19-02]
- National Natural Science Foundation of China [82072291, 81772207, 81572005, 32072831]
- Gansu Science Foundation for Distinguished Young Scholars [21JR7RA026]
- Key Technologies R&D Program of Gansu Province [21ZD3NA001]
- Chinese Academy of Agricultural Science and Technology Innovation Project [CAAS-ASTIP-2021-LVRI]
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The crystal structure of an FMDV 2C fragment reveals its similarity with enterovirus 2C protein. An anti-FMDV peptide derived from 2C protein disrupts its activity and shows anti-FMDV activity in cells.
The foot-and-mouth disease virus (FMDV) 2C protein shares conserved motifs with enterovirus 2Cs despite low sequence identity. Here, we determine the crystal structure of an FMDV 2C fragment to 1.83 A?? resolution, which comprises an ATPase domain, a region equivalent to the enterovirus 2C zinc-finger (ZFER), and a C-terminal domain harboring a loop (PBL) that occupies a hydrophobic cleft (Pocket) in an adjacent 2C mole-cule. Mutations at ZFER, PBL, and Pocket affect FMDV 2C ATPase activity and are lethal to FMDV infectious clones. Because the PBL-Pocket interaction between FMDV 2C molecules is essential for its functions, we design an anti-FMDV peptide derived from PBL (PBL-peptide). PBL-peptide inhibits FMDV 2C ATPase activ-ity, binds FMDV 2C with nanomolar affinity, and disrupts FMDV 2C oligomerization. FMDV 2C targets lipid droplets (LDs) and induces LD clustering in cells, and PBL-peptide disrupts FMDV 2C-induced LD clustering. Finally, we demonstrate that PBL-peptide exhibits anti-FMDV activity in cells.
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