Combining native and ‘omics’ mass spectrometry to identify endogenous ligands bound to membrane proteins
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作者:
Joseph Gault
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机构:University of Oxford,Department of Chemistry
Joseph Gault
Idlir Liko
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机构:University of Oxford,Department of Chemistry
Idlir Liko
Michael Landreh
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机构:University of Oxford,Department of Chemistry
Michael Landreh
Denis Shutin
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机构:University of Oxford,Department of Chemistry
Denis Shutin
Jani Reddy Bolla
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机构:University of Oxford,Department of Chemistry
Jani Reddy Bolla
Damien Jefferies
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机构:University of Oxford,Department of Chemistry
Damien Jefferies
Mark Agasid
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机构:University of Oxford,Department of Chemistry
Mark Agasid
Hsin-Yung Yen
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机构:University of Oxford,Department of Chemistry
Hsin-Yung Yen
Marcus J. G. W. Ladds
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机构:University of Oxford,Department of Chemistry
Marcus J. G. W. Ladds
David P. Lane
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机构:University of Oxford,Department of Chemistry
David P. Lane
Syma Khalid
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机构:University of Oxford,Department of Chemistry
Syma Khalid
Christopher Mullen
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机构:University of Oxford,Department of Chemistry
Christopher Mullen
Philip M. Remes
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机构:University of Oxford,Department of Chemistry
Philip M. Remes
Romain Huguet
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机构:University of Oxford,Department of Chemistry
Romain Huguet
Graeme McAlister
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机构:University of Oxford,Department of Chemistry
Graeme McAlister
Michael Goodwin
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机构:University of Oxford,Department of Chemistry
Michael Goodwin
Rosa Viner
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机构:University of Oxford,Department of Chemistry
Rosa Viner
John E.P. Syka
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机构:University of Oxford,Department of Chemistry
John E.P. Syka
Carol V. Robinson
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机构:University of Oxford,Department of Chemistry
Carol V. Robinson
机构:
[1] University of Oxford,Department of Chemistry
[2] OMass Therapeutics,Department of Microbiology
[3] Tumor and Cell Biology,School of Chemistry
[4] Biomedicum,undefined
[5] Karolinska Institutet,undefined
[6] University of Southampton,undefined
[7] Thermo Fisher Scientific,undefined
来源:
Nature Methods
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2020年
/
17卷
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摘要:
Ligands bound to protein assemblies provide critical information for function, yet are often difficult to capture and define. Here we develop a top-down method, ‘nativeomics’, unifying ‘omics’ (lipidomics, proteomics, metabolomics) analysis with native mass spectrometry to identify ligands bound to membrane protein assemblies. By maintaining the link between proteins and ligands, we define the lipidome/metabolome in contact with membrane porins and a mitochondrial translocator to discover potential regulators of protein function.