Similarities and differences in the structures and proteoform profiles of the complement proteins C6 and C7

Marie V Lukassen; Vojtech Franc; Johannes F Hevler; Albert J R Heck

doi:10.1002/pmic.202000310

Similarities and differences in the structures and proteoform profiles of the complement proteins C6 and C7

Marie V Lukassen, Vojtech Franc, Johannes F Hevler, Albert J R Heck

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

The human complement system provides a first line of defence against pathogens. It requires a well-orchestrated sequential assembly of an array of terminal complement components (C5, C6, C7, C8, and C9), ultimately forming the membrane attack complex (MAC). Although much information about MAC assembly is available, the structure of the soluble C7 has remained elusive. The complement proteins C7 and C6 share very high sequence homology and exhibit several conserved domains, disulphide bridges, and C-mannosylation sites. Here, we used an integrative structural MS-based approach combining native MS, glycopeptide-centric MS, in-gel cross-linking MS (IGX-MS) and structural modelling to describe structural features, including glycosylation, of human serum soluble C7. We compare this data with structural and glycosylation data for human serum C6. The new structural model for C7 shows that it adopts a compact conformation in solution. Although C6 and C7 share many similarities, our data reveals distinct O-, and N-linked glycosylation patterns in terms of location and glycan composition. Cumulatively, our data provide valuable new insight into the structure and proteoforms of C7, solving an essential piece of the puzzle in our understanding of MAC assembly.

Original language	English
Article number	2000310
Pages (from-to)	1-11
Journal	Proteomics
Volume	21
Issue number	21-22
Early online date	9 Jul 2021
DOIs	https://doi.org/10.1002/pmic.202000310
Publication status	Published - Nov 2021

Bibliographical note

Funding Information:
The authors acknowledge support from the Netherlands Organization for Scientific Research (NWO) funding the Netherlands Proteomics Centre through the X‐omics Road Map program (project 184.034.019) and the EU Horizon 2020 program INFRAIA project Epic‐XS (Project 823839). MVL further acknowledges fellowship support from the Independent Research Fund Denmark (Project 9036‐00007B).

Publisher Copyright:
© 2021 The Authors. Proteomics published by Wiley-VCH GmbH

Keywords

complement
cross-linking
glycosylation
mass spectrometry
proteoforms

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Proteomics - 2021 - Lukassen - Similarities and differences in the structures and proteoform profiles of the complementFinal published version, 1.62 MBLicence: CC BY-NC

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title = "Similarities and differences in the structures and proteoform profiles of the complement proteins C6 and C7",

abstract = "The human complement system provides a first line of defence against pathogens. It requires a well-orchestrated sequential assembly of an array of terminal complement components (C5, C6, C7, C8, and C9), ultimately forming the membrane attack complex (MAC). Although much information about MAC assembly is available, the structure of the soluble C7 has remained elusive. The complement proteins C7 and C6 share very high sequence homology and exhibit several conserved domains, disulphide bridges, and C-mannosylation sites. Here, we used an integrative structural MS-based approach combining native MS, glycopeptide-centric MS, in-gel cross-linking MS (IGX-MS) and structural modelling to describe structural features, including glycosylation, of human serum soluble C7. We compare this data with structural and glycosylation data for human serum C6. The new structural model for C7 shows that it adopts a compact conformation in solution. Although C6 and C7 share many similarities, our data reveals distinct O-, and N-linked glycosylation patterns in terms of location and glycan composition. Cumulatively, our data provide valuable new insight into the structure and proteoforms of C7, solving an essential piece of the puzzle in our understanding of MAC assembly.",

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author = "Lukassen, {Marie V} and Vojtech Franc and Hevler, {Johannes F} and Heck, {Albert J R}",

note = "Funding Information: The authors acknowledge support from the Netherlands Organization for Scientific Research (NWO) funding the Netherlands Proteomics Centre through the X‐omics Road Map program (project 184.034.019) and the EU Horizon 2020 program INFRAIA project Epic‐XS (Project 823839). MVL further acknowledges fellowship support from the Independent Research Fund Denmark (Project 9036‐00007B). Publisher Copyright: {\textcopyright} 2021 The Authors. Proteomics published by Wiley-VCH GmbH",

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N1 - Funding Information: The authors acknowledge support from the Netherlands Organization for Scientific Research (NWO) funding the Netherlands Proteomics Centre through the X‐omics Road Map program (project 184.034.019) and the EU Horizon 2020 program INFRAIA project Epic‐XS (Project 823839). MVL further acknowledges fellowship support from the Independent Research Fund Denmark (Project 9036‐00007B). Publisher Copyright: © 2021 The Authors. Proteomics published by Wiley-VCH GmbH

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N2 - The human complement system provides a first line of defence against pathogens. It requires a well-orchestrated sequential assembly of an array of terminal complement components (C5, C6, C7, C8, and C9), ultimately forming the membrane attack complex (MAC). Although much information about MAC assembly is available, the structure of the soluble C7 has remained elusive. The complement proteins C7 and C6 share very high sequence homology and exhibit several conserved domains, disulphide bridges, and C-mannosylation sites. Here, we used an integrative structural MS-based approach combining native MS, glycopeptide-centric MS, in-gel cross-linking MS (IGX-MS) and structural modelling to describe structural features, including glycosylation, of human serum soluble C7. We compare this data with structural and glycosylation data for human serum C6. The new structural model for C7 shows that it adopts a compact conformation in solution. Although C6 and C7 share many similarities, our data reveals distinct O-, and N-linked glycosylation patterns in terms of location and glycan composition. Cumulatively, our data provide valuable new insight into the structure and proteoforms of C7, solving an essential piece of the puzzle in our understanding of MAC assembly.

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Similarities and differences in the structures and proteoform profiles of the complement proteins C6 and C7

Abstract

Bibliographical note

Keywords

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