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Piai, Alessandro

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Piai

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Alessandro

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Piai, Alessandro

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2017 - 20182

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Author's Publications: search.filters.isAuthorOfPublication.cd6b73cd-a739-4e19-b853-1c47c93fa6bd

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    HIV envelope V3 region mimic embodies key features of a broadly neutralizing antibody lineage epitope

    (Nature Publishing Group UK, 2018) Fera, Daniela; Lee, Matthew; Wiehe, Kevin; Meyerhoff, R. Ryan; Piai, Alessandro; Bonsignori, Mattia; Aussedat, Baptiste; Walkowicz, William E.; Ton, Therese; Zhou, Jeffrey O.; Danishefsky, Samuel; Haynes, Barton F.; Harrison, Stephen

    HIV-1 envelope (Env) mimetics are candidate components of prophylactic vaccines and potential therapeutics. Here we use a synthetic V3-glycopeptide (“Man9-V3”) for structural studies of an HIV Env third variable loop (V3)-glycan directed, broadly neutralizing antibody (bnAb) lineage (“DH270”), to visualize the epitope on Env and to study how affinity maturation of the lineage proceeded. Unlike many previous V3 mimetics, Man9-V3 encompasses two key features of the V3 region recognized by V3-glycan bnAbs—the conserved GDIR motif and the N332 glycan. In our structure of an antibody fragment of a lineage member, DH270.6, in complex with the V3 glycopeptide, the conformation of the antibody-bound glycopeptide conforms closely to that of the corresponding segment in an intact HIV-1 Env trimer. An additional structure identifies roles for two critical mutations in the development of breadth. The results suggest a strategy for use of a V3 glycopeptide as a vaccine immunogen.

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    An Exhaustive Search Algorithm to Aid NMR-Based Structure Determination of Rotationally Symmetric Transmembrane Oligomers

    (Nature Publishing Group UK, 2017) Yang, Jing; Piai, Alessandro; Shen, Hong-Bin; Chou, James

    Nuclear magnetic resonance (NMR) has been an important source of structural restraints for solving structures of oligomeric transmembrane domains (TMDs) of cell surface receptors and viral membrane proteins. In NMR studies, oligomers are assembled using inter-protomer distance restraints. But, for oligomers that are higher than dimer, these distance restraints all have two-fold directional ambiguity, and resolving such ambiguity often requires time-consuming trial-and-error calculations using restrained molecular dynamics (MD) with simulated annealing (SA). We report an Exhaustive Search algorithm for Symmetric Oligomer (ExSSO), which can perform near-complete search of the symmetric conformational space in a very short time. In this approach, the predetermined protomer model is subject to full angular and spatial search within the symmetry space. This approach, which can be applied to any rotationally symmetric oligomers, was validated using the structures of the Fas death receptor, the HIV-1 gp41 fusion protein, the influenza proton channel, and the MCU pore. The algorithm is able to generate approximate oligomer solutions quickly as initial inputs for further refinement using the MD/SA method.