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Structure-guided changes at the V2 apex of HIV-1 clade C trimer enhance elicitation of autologous neutralizing and broad V1V2-scaffold antibodies.

Authors :
Sahoo A
Hodge EA
LaBranche CC
Styles TM
Shen X
Cheedarla N
Shiferaw A
Ozorowski G
Lee WH
Ward AB
Tomaras GD
Montefiori DC
Irvine DJ
Lee KK
Amara RR
Source :
Cell reports [Cell Rep] 2022 Mar 01; Vol. 38 (9), pp. 110436.
Publication Year :
2022

Abstract

HIV-1 clade C envelope immunogens that elicit both neutralizing and non-neutralizing V1V2-scaffold-specific antibodies (protective correlates from RV144 human trial) are urgently needed due to the prevalence of this clade in the most impacted regions worldwide. To achieve this, we introduce structure-guided changes followed by consensus-C-sequence-guided optimizations at the V2 region to generate UFO-v2-RQH <superscript>173</superscript> trimer. This improves the abundance of well-formed trimers. Following the immunization of rabbits, the wild-type protein fails to elicit any autologous neutralizing antibodies, but UFO-v2-RQH <superscript>173</superscript> elicits both autologous neutralizing and broad V1V2-scaffold antibodies. The variant with a 173Y modification in the V2 region, most prevalent among HIV-1 sequences, shows decreased ability in displaying a native-like V1V2 epitope with time in vitro and elicited antibodies with lower neutralizing and higher V1V2-scaffold activities. Our results identify a stabilized clade C trimer capable of eliciting improved neutralizing and V1V2-scaffold antibodies and reveal the importance of the V2 region in tuning this.<br />Competing Interests: Declaration of interests A patent has been filed on the C.1086 UFO trimers developed in the study, and R.R.A., A. Sahoo, and T.M.S. are co-inventors of this technology. The other authors declare no competing interests.<br /> (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Details

Language :
English
ISSN :
2211-1247
Volume :
38
Issue :
9
Database :
MEDLINE
Journal :
Cell reports
Publication Type :
Academic Journal
Accession number :
35235790
Full Text :
https://doi.org/10.1016/j.celrep.2022.110436