Structural basis of nanobody recognition of grapevine fanleaf virus and of virus resistance loss

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Orlov, Igor | Hemmer, Caroline | Ackerer, Léa | Lorber, Bernard | Ghannam, Ahmed | Poignavent, Vianney | Hleibieh, Kamal | Sauter, Claude | Schmitt-Keichinger, Corinne | Belval, Lorène | Hily, Jean-Michel | Marmonier, Aurélie | Komar, Véronique | Gersch, Sophie | Schellenberger, Pascale | Bron, Patrick | Vigne, Emmanuelle | Muyldermans, Serge | Lemaire, Olivier | Demangeat, Gérard | Ritzenthaler, Christophe | Klaholz, Bruno

Edité par CCSD ; National Academy of Sciences -

International audience. Grapevine fanleaf virus (GFLV) is a picorna-like plant virus transmitted by nematodes that affects vineyards worldwide. Nanobody (Nb)-mediated resistance against GFLV has been created recently, and shown to be highly effective in plants, including grapevine, but the underlying mechanism is unknown. Here we present the high-resolution cryo electron microscopy structure of the GFLV-Nb23 complex, which provides the basis for molecular recognition by the Nb. The structure reveals a composite binding site bridging over three domains of one capsid protein (CP) monomer. The structure provides a precise mapping of the Nb23 epitope on the GFLV capsid in which the antigen loop is accommodated through an induced-fit mechanism. Moreover, we uncover and characterize several resistance-breaking GFLV isolates with amino acids mapping within this epitope, including C-terminal extensions of the CP, which would sterically interfere with Nb binding. Escape variants with such extended CP fail to be transmitted by nematodes linking Nb-mediated resistance to vector transmission. Together, these data provide insights into the molecular mechanism of Nb23-mediated recognition of GFLV and of virus resistance loss.

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