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Literature DB >> 29656089

Microbiology catches the cryo-EM bug.

Lesley A Earl¹, Veronica Falconieri¹, Sriram Subramaniam².

Abstract

Over the past few years, the advances in technology and methods that have revolutionized cryo-EM are allowing for key insights in a variety of areas in biology, and microbiology is no exception. A wide range of important macromolecular assemblies in prokaryotic and eukaryotic cells, as well as intact viruses, have now become accessible to investigation by new methods in 3D electron microscopy. We focus here on selected examples that illustrate this breadth, and review the application of methods in single particle cryo-EM and cryo-electron tomography to progress in the structural biology of CRISPR systems, visualization of small molecule drugs in membrane proteins, in situ visualization of bacterial nanomachines, and the analysis of antigen-antibody interactions to drive vaccine design. Published by Elsevier Ltd.

Entities: Chemical Disease Gene Species

Mesh：

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Year: 2018 PMID： 29656089 PMCID： PMC6005731 DOI： 10.1016/j.mib.2018.02.012

Source DB: PubMed Journal: Curr Opin Microbiol ISSN： 1369-5274 Impact factor: 7.934

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References

49 in total

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Authors: Zachary Lee Johnson; Jue Chen
Journal: Cell Date: 2017-02-23 Impact factor: 41.582

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Review 4. Resolution advances in cryo-EM enable application to drug discovery.

Authors: Sriram Subramaniam; Lesley A Earl; Veronica Falconieri; Jacqueline Ls Milne; Edward H Egelman
Journal: Curr Opin Struct Biol Date: 2016-08-20 Impact factor: 6.809

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Journal: Cell Date: 2017-09-21 Impact factor: 41.582

Microbiology catches the cryo-EM bug.

1. Structural Basis of Substrate Recognition by the Multidrug Resistance Protein MRP1.

2. Structure Reveals Mechanisms of Viral Suppressors that Intercept a CRISPR RNA-Guided Surveillance Complex.

Review 3. Recent progress in structure and dynamics of dual-membrane-spanning bacterial nanomachines.

Review 4. Resolution advances in cryo-EM enable application to drug discovery.

5. A Human Bi-specific Antibody against Zika Virus with High Therapeutic Potential.

6. 2.2 Å resolution cryo-EM structure of β-galactosidase in complex with a cell-permeant inhibitor.

7. The 3.8 Å resolution cryo-EM structure of Zika virus.

8. Structure of the transporter associated with antigen processing trapped by herpes simplex virus.

9. Disabling Cas9 by an anti-CRISPR DNA mimic.

10. DNA Targeting by a Minimal CRISPR RNA-Guided Cascade.