Fig 2: The central domain of the conserved host protein, RNF214 , is sufficient for IpaH4-mediated ubiquitination and degradation.A. Schematic of human RNF214 with mapping of prey clones collectively identified in two yeast two-hybrid screens using IpaH4 bait [14]. Numbers indicate RNF214 a.a. encoded by each prey clone. B. Schematic displaying the relative conservation and length of RNF214 across indicated organisms. C. PhyloTv2-generated phylogenetic tree of RNF214 orthologs. D. Table of RNF214 orthologs in various vertebrate and invertebrate species generated via reciprocal BLAST analysis. E. AlphaFold2predicted structure of human RNF214. F. Representative immunoblot of degradation assay using Flag-tagged RNF214 co-transfected into U2OS cells with GFP-IpaH4 (WT) or GFP-IpaH4C339S (C339S) catalytic mutant expression vectors. G-H. Representative immunoblot of degradation assays using Flag-tagged RNF214 truncations, RNF2141−275 (G) or RNF214276−504 (H), co-transfected into U2OS cells with GFP-IpaH4 (WT) or GFP-IpaH4C339S (C339S) vectors. I-J. Representative immunoblot of in vitro ubiquitination assay showing direct IpaH4-mediated ubiquitination of purified, recombinant human Flag-RNF214 (I) and Flag-RNF214276−504 (J) proteins.

Fig 3: Depletion of RNF214 enhances arbovirus replication in bat and human cells.A. Representative fluorescence microscopy images (GFP channel) of R06E cells transfected with firefly luciferase (Luc)or RNF214-targeting siRNAs. 48 h post-knockdown, cells were infected with RRV-GFP (MOI=0.001) for 20 h. Cells were then stained with CellTracker Orange, imaged, and fold-change in GFP signal compared to the Luc control was calculated. Supernatants were also collected to assess viral titers by plaque assay. B-C. Similar experiments were performed as in A but for VSVM51R-GFP (MOI=0.0001) (B) and ONNV-GFP (MOI=0.001) (C). D. Representative immunoblot of endogenous bat RNF214 levels following siRNA knockdown in R06E cells for 48 h. E. Representative immunoblot of endogenous human RNF214 levels following in U2OS cells transduced with control lentivirus (C) or lentivirus expressing guide RNAs targeting RNF214 (KO). F. Representative fluorescence microscopy images (GFP channel) in control or ΔRNF214 U2OS cells infected with RRV-GFP (MOI=0.001) 20 h. Cells were then stained with CellTracker Orange, imaged, and fold-change in GFP signal compared to Control U2OS cell infections was calculated. Supernatants were also collected to assess viral titers by plaque assay. G-I. Similar experiments were performed as in F but for VSVM51R-GFP (MOI=0.0001) (G), ONNV-GFP (MOI=0.001) and SINV-GFP (MOI=0.001) (H). Data are means ± SEM; n=3. Statistical significance for A-C was determined with One-way ANOVA and with unpaired student’s t-test for F-I; ns (not significant), *=P<0.05, **=P<0.01, ***=P<0.001, ****=P<0.0001. Scalebars indicate 200 μm on all microscopy images.