Jihong Zhu scite author profile

Binding of precursor tRNAs (ptRNAs) by bacterial ribonuclease P (RNase P) involves an encounter complex (ES) that isomerizes to a catalytic conformation (ES*). However, the structures of intermediates and the conformational changes that occur during binding are poorly understood. Here, we show that pairing between the 5′ leader and 3′RCCA extending the acceptor stem of ptRNA inhibits ES* formation. Cryo-electron microscopy single particle analysis reveals a dynamic enzyme that becomes ordered upon formation of ES* in which extended acceptor stem pairing is unwound. Comparisons of structures with alternative ptRNAs reveals that once unwinding is completed RNase P primarily uses stacking interactions and shape complementarity to accommodate alternative sequences at its cleavage site. Our study reveals active site interactions and conformational changes that drive molecular recognition by RNase P and lays the foundation for understanding how binding interactions are linked to helix unwinding and catalysis.

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Reaching self-stabilising distributed synchronisation with COTS Ethernet components: the WALDEN approach

Zhu

Yang

2021

Real-Time Syst

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Jihong Zhu

Aerodynamic shape optimization using a novel optimizer based on machine learning techniques

Design of Five-Phase Modular Flux-Switching Permanent-Magnet Machines for High Reliability Applications

H∞ Tracking Control for Linear Discrete-Time Systems: Model-Free Q-Learning Designs

Structural and mechanistic basis for recognition of alternative tRNA precursor substrates by bacterial ribonuclease P

Reaching self-stabilising distributed synchronisation with COTS Ethernet components: the WALDEN approach

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