Yu Gu scite author profile

In a broad genomics analysis to find novel protein targets for antibiotic discovery, MurF was identified as an essential gene product for Streptococcus pneumonia that catalyzes a critical reaction in the biosynthesis of the peptidoglycan in the formation of the cell wall. Lacking close relatives in mammalian biology, MurF presents attractive characteristics as a potential drug target. Initial screening of the Abbott small-molecule compound collection identified several compounds for further validation as pharmaceutical leads. Here we report the integrated efforts of NMR and X-ray crystallography, which reveal the multidomain structure of a MurF-inhibitor complex in a compact conformation that differs dramatically from related structures. The lead molecule is bound in the substrate-binding region and induces domain closure, suggestive of the domain arrangement for the as yet unobserved transition state conformation for MurF enzymes. The results form a basis for directed optimization of the compound lead by structure-based design to explore the suitability of MurF as a pharmaceutical target.

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Design and flight-testing of non-linear formation control laws

Campa

Seanor

et al. 2007

Control Engineering Practice

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Flight-Test Evaluation of Sensor Fusion Algorithms for Attitude Estimation

Gross

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et al. 2012

IEEE Trans. Aerosp. Electron. Syst.

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A Survey of Optical Flow Techniques for Robotics Navigation Applications

Huo

Napolitano

2013

J Intell Robot Syst

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Yu Gu

Design and Flight Testing Evaluation of Formation Control Laws

Structure of MurF from Streptococcus pneumoniae co‐crystallized with a small molecule inhibitor exhibits interdomain closure

Design and flight-testing of non-linear formation control laws

Flight-Test Evaluation of Sensor Fusion Algorithms for Attitude Estimation

A Survey of Optical Flow Techniques for Robotics Navigation Applications

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