TY - JOUR
T1 - Hollow Octadecameric Self-Assembly of Collagen-like Peptides
AU - Yu, Le Tracy
AU - Hancu, Maria C.
AU - Kreutzberger, Mark A.B.
AU - Henrickson, Amy
AU - Demeler, Borries
AU - Egelman, Edward H.
AU - Hartgerink, Jeffrey D.
N1 - Funding Information:
L.T.Y. thanks Caroline M. Peterson and Adam C. Farsheed for their help in instrument training. The cryo-EM data were collected at the Molecular Electron Microscopy Core (MEMC) at the University of Virginia. We would like to thank Dr. Michael Purdy at the MEMC for his assistance with the imaging. This work was supported by the NSF CHE grant number 2203937 (awarded to J.D.H.) and NIH GM122510 (to E.H.E.). AUC analysis was supported by the Canada 150 Research Chairs program (C150-2017-00015), the Canada Foundation for Innovation (CFI-37589), the National Institutes of Health (1R01GM120600), and the Canadian Natural Science and Engineering Research Council (DG-RGPIN-2019-05637). UltraScan supercomputer calculations were supported through NSF/XSEDE grant TG-MCB070039N and University of Texas grant TG457201 (awarded to B.D.). The Canadian Natural Science and Engineering Research Council supported A.H. through a scholarship grant.
Funding Information:
This work was supported by the NSF CHE grant number 2203937 (awarded to J.D.H.) and NIH GM122510 (to E.H.E.). AUC analysis was supported by the Canada 150 Research Chairs program (C150-2017-00015), the Canada Foundation for Innovation (CFI-37589), the National Institutes of Health (1R01GM120600), and the Canadian Natural Science and Engineering Research Council (DG-RGPIN-2019-05637). UltraScan supercomputer calculations were supported through NSF/XSEDE grant TG-MCB070039N and University of Texas grant TG457201 (awarded to B.D.). The Canadian Natural Science and Engineering Research Council supported A.H. through a scholarship grant.
Publisher Copyright:
© 2023 American Chemical Society.
PY - 2023/3/8
Y1 - 2023/3/8
N2 - The folding of collagen is a hierarchical process that starts with three peptides associating into the characteristic triple helical fold. Depending on the specific collagen in question, these triple helices then assemble into bundles reminiscent of α-helical coiled-coils. Unlike α-helices, however, the bundling of collagen triple helices is very poorly understood with almost no direct experimental data available. In order to shed light on this critical step of collagen hierarchical assembly, we have examined the collagenous region of complement component 1q. Thirteen synthetic peptides were prepared to dissect the critical regions allowing for its octadecameric self-assembly. We find that short peptides (under 40 amino acids) are able to self-assemble into specific (ABC)6 octadecamers. This requires the ABC heterotrimeric composition as the self-assembly subunit, but does not require disulfide bonds. Self-assembly into this octadecamer is aided by short noncollagenous sequences at the N-terminus, although they are not entirely required. The mechanism of self-assembly appears to begin with the very slow formation of the ABC heterotrimeric helix, followed by rapid bundling of triple helices into progressively larger oligomers, terminating in the formation of the (ABC)6 octadecamer. Cryo-electron microscopy reveals the (ABC)6 assembly as a remarkable, hollow, crown-like structure with an open channel approximately 18 Å at the narrow end and 30 Å at the wide end. This work helps to illuminate the structure and assembly mechanism of a critical protein in the innate immune system and lays the groundwork for the de novo design of higher order collagen mimetic peptide assemblies.
AB - The folding of collagen is a hierarchical process that starts with three peptides associating into the characteristic triple helical fold. Depending on the specific collagen in question, these triple helices then assemble into bundles reminiscent of α-helical coiled-coils. Unlike α-helices, however, the bundling of collagen triple helices is very poorly understood with almost no direct experimental data available. In order to shed light on this critical step of collagen hierarchical assembly, we have examined the collagenous region of complement component 1q. Thirteen synthetic peptides were prepared to dissect the critical regions allowing for its octadecameric self-assembly. We find that short peptides (under 40 amino acids) are able to self-assemble into specific (ABC)6 octadecamers. This requires the ABC heterotrimeric composition as the self-assembly subunit, but does not require disulfide bonds. Self-assembly into this octadecamer is aided by short noncollagenous sequences at the N-terminus, although they are not entirely required. The mechanism of self-assembly appears to begin with the very slow formation of the ABC heterotrimeric helix, followed by rapid bundling of triple helices into progressively larger oligomers, terminating in the formation of the (ABC)6 octadecamer. Cryo-electron microscopy reveals the (ABC)6 assembly as a remarkable, hollow, crown-like structure with an open channel approximately 18 Å at the narrow end and 30 Å at the wide end. This work helps to illuminate the structure and assembly mechanism of a critical protein in the innate immune system and lays the groundwork for the de novo design of higher order collagen mimetic peptide assemblies.
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U2 - 10.1021/jacs.2c12931
DO - 10.1021/jacs.2c12931
M3 - Article
C2 - 36812303
AN - SCOPUS:85148770312
SN - 0002-7863
VL - 145
SP - 5285
EP - 5296
JO - Journal of the American Chemical Society
JF - Journal of the American Chemical Society
IS - 9
ER -