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In vivo Cross-Linking MS of the Complement System MAC Assembled on Live Gram-Positive Bacteria.


ABSTRACT: Protein-protein interactions are central in many biological processes, but they are challenging to characterize, especially in complex samples. Protein cross-linking combined with mass spectrometry (MS) and computational modeling is gaining increased recognition as a viable tool in protein interaction studies. Here, we provide insights into the structure of the multicomponent human complement system membrane attack complex (MAC) using in vivo cross-linking MS combined with computational macromolecular modeling. We developed an affinity procedure followed by chemical cross-linking on human blood plasma using live Streptococcus pyogenes to enrich for native MAC associated with the bacterial surface. In this highly complex sample, we identified over 100 cross-linked lysine-lysine pairs between different MAC components that enabled us to present a quaternary model of the assembled MAC in its native environment. Demonstrating the validity of our approach, this MAC model is supported by existing X-ray crystallographic and electron cryo-microscopic models. This approach allows the study of protein-protein interactions in native environment mimicking their natural milieu. Its high potential in assisting and refining data interpretation in electron cryo-tomographic experiments will be discussed.

SUBMITTER: Khakzad H 

PROVIDER: S-EPMC7820895 | biostudies-literature | 2020

REPOSITORIES: biostudies-literature

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<i>In vivo</i> Cross-Linking MS of the Complement System MAC Assembled on Live Gram-Positive Bacteria.

Khakzad Hamed H   Happonen Lotta L   Tran Van Nhieu Guy G   Malmström Johan J   Malmström Lars L  

Frontiers in genetics 20210108


Protein-protein interactions are central in many biological processes, but they are challenging to characterize, especially in complex samples. Protein cross-linking combined with mass spectrometry (MS) and computational modeling is gaining increased recognition as a viable tool in protein interaction studies. Here, we provide insights into the structure of the multicomponent human complement system membrane attack complex (MAC) using <i>in vivo</i> cross-linking MS combined with computational m  ...[more]

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