Abstract P-14: Cryo-Electron Tomography Pipeline on the Example of Structural Analysis of Polyribosomes

Background: Cryo-electron tomography (cryo-ET) is currently the only technique that can be used for quaternary structure determination of polyribosomal complexes under near physiological conditions. Here we describe, in more detail, the cryo-ET pipeline from a sample preparation for data processing...

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Main Authors: Timur N. Baymukhametov, Yury M. Chesnokov, Zhanna A. Afonina, Alexander L. Vasiliev
Format: Article
Language:English
Published: International Medical Research and Development Corporation 2019-06-01
Series:International Journal of Biomedicine
Subjects:
Online Access:http://ijbm.org/articles/IJBM_2019_9_S1_P14.pdf
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spelling doaj-834ea325d5fe4625b5e1e078b73722242020-11-25T01:51:59ZengInternational Medical Research and Development CorporationInternational Journal of Biomedicine2158-05102158-05292019-06-019Suppl_1S22S2310.21103/IJBM.9.Suppl_1.P14Abstract P-14: Cryo-Electron Tomography Pipeline on the Example of Structural Analysis of PolyribosomesTimur N. Baymukhametov0Yury M. Chesnokov1Zhanna A. Afonina2Alexander L. Vasiliev3National Research Center «Kurchatov Institute», Moscow, RussiaNational Research Center «Kurchatov Institute», Moscow, RussiaInstitute of Protein Research RAS, Pushchino, RussiaNational Research Center «Kurchatov Institute», Moscow, Russia; Shubnikov Institute of Crystallography of FSRC «Crystallography and Photonics» RAS, Moscow, RussiaBackground: Cryo-electron tomography (cryo-ET) is currently the only technique that can be used for quaternary structure determination of polyribosomal complexes under near physiological conditions. Here we describe, in more detail, the cryo-ET pipeline from a sample preparation for data processing from the poster talk “Cryo-ET structural analysis of polyribosomes from HeLa cells” by Zhanna A. Afonina. Methods: The investigations were carried out in a Titan Krios 60-300 TEM/STEM (FEI, USA), equipped with Falcon II DED (FEI, USA) and Cs-image corrector (CEOS, Germany). Data acquisition were done automatically using FEI Tomography software. All data processing stages including sub-tomogram averaging after tomographic reconstruction using IMOD were carried out using computing resources of the Federal Collective Usage Center Complex for Simulation and Data Processing for Mega-Science Facilities at NRC “Kurchatov Institute”. Results: Cryo-ET with sub-tomogram averaging was allowed us to determine spatial structure of polyribosomes with 17.5Å resolution. The relative orientations of ribosomes in polyribosomes and the mRNA pathways in each individual polyribosome were determined. Conclusion: Cryo-ET in combination with sub-tomographic averaging is the most promising technique in cryo-electron microscopy. This approach in comparison of single particle analysis imposes additional requirements both at the stages of data acquisition and data processing. On the example of this work we demonstrated all the stages of the Cryo-ET pipeline. Taking into account the experimental equipment used, bottlenecks and possible solutions were shown. http://ijbm.org/articles/IJBM_2019_9_S1_P14.pdfcryo-EMcryo-ETpolyribosomes
collection DOAJ
language English
format Article
sources DOAJ
author Timur N. Baymukhametov
Yury M. Chesnokov
Zhanna A. Afonina
Alexander L. Vasiliev
spellingShingle Timur N. Baymukhametov
Yury M. Chesnokov
Zhanna A. Afonina
Alexander L. Vasiliev
Abstract P-14: Cryo-Electron Tomography Pipeline on the Example of Structural Analysis of Polyribosomes
International Journal of Biomedicine
cryo-EM
cryo-ET
polyribosomes
author_facet Timur N. Baymukhametov
Yury M. Chesnokov
Zhanna A. Afonina
Alexander L. Vasiliev
author_sort Timur N. Baymukhametov
title Abstract P-14: Cryo-Electron Tomography Pipeline on the Example of Structural Analysis of Polyribosomes
title_short Abstract P-14: Cryo-Electron Tomography Pipeline on the Example of Structural Analysis of Polyribosomes
title_full Abstract P-14: Cryo-Electron Tomography Pipeline on the Example of Structural Analysis of Polyribosomes
title_fullStr Abstract P-14: Cryo-Electron Tomography Pipeline on the Example of Structural Analysis of Polyribosomes
title_full_unstemmed Abstract P-14: Cryo-Electron Tomography Pipeline on the Example of Structural Analysis of Polyribosomes
title_sort abstract p-14: cryo-electron tomography pipeline on the example of structural analysis of polyribosomes
publisher International Medical Research and Development Corporation
series International Journal of Biomedicine
issn 2158-0510
2158-0529
publishDate 2019-06-01
description Background: Cryo-electron tomography (cryo-ET) is currently the only technique that can be used for quaternary structure determination of polyribosomal complexes under near physiological conditions. Here we describe, in more detail, the cryo-ET pipeline from a sample preparation for data processing from the poster talk “Cryo-ET structural analysis of polyribosomes from HeLa cells” by Zhanna A. Afonina. Methods: The investigations were carried out in a Titan Krios 60-300 TEM/STEM (FEI, USA), equipped with Falcon II DED (FEI, USA) and Cs-image corrector (CEOS, Germany). Data acquisition were done automatically using FEI Tomography software. All data processing stages including sub-tomogram averaging after tomographic reconstruction using IMOD were carried out using computing resources of the Federal Collective Usage Center Complex for Simulation and Data Processing for Mega-Science Facilities at NRC “Kurchatov Institute”. Results: Cryo-ET with sub-tomogram averaging was allowed us to determine spatial structure of polyribosomes with 17.5Å resolution. The relative orientations of ribosomes in polyribosomes and the mRNA pathways in each individual polyribosome were determined. Conclusion: Cryo-ET in combination with sub-tomographic averaging is the most promising technique in cryo-electron microscopy. This approach in comparison of single particle analysis imposes additional requirements both at the stages of data acquisition and data processing. On the example of this work we demonstrated all the stages of the Cryo-ET pipeline. Taking into account the experimental equipment used, bottlenecks and possible solutions were shown.
topic cryo-EM
cryo-ET
polyribosomes
url http://ijbm.org/articles/IJBM_2019_9_S1_P14.pdf
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