Crystal structure of a human rhinovirus that displays part of the HIV-1 V3 loop and induces neutralizing antibodies against HIV-1

Jianping Ding; Allen D. Smith; Sheila C. Geisler; Xuejun Ma; Gail Ferstandig Arnold; Eddy Arnold

doi:10.1016/S0969-2126(02)00793-1

Crystal structure of a human rhinovirus that displays part of the HIV-1 V3 loop and induces neutralizing antibodies against HIV-1

Jianping Ding
, Allen D. Smith
, Sheila C. Geisler
, Xuejun Ma
, Gail Ferstandig Arnold
, Eddy Arnold

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

30 Scopus citations

Abstract

We report the 2.7 Å resolution structure of a chimeric rhinovirus, MN-III-2, that displays part of the HIV-1 gp120 V3 loop and elicits HIV-neutralizing antibodies. The V3 loop insert is dominated by two type I β turns. The structures of two adjacent tripeptides resemble those of analogous segments in three Fab/V3 loop peptide complexes. Although two of the three corresponding antibodies bind and neutralize MN-III-2 well, only one of the three can bind without significant rearrangement. These results suggest that the V3 loop insert: (1) can share some local conformational similarity to V3 loop sequences presented on different structural frameworks; (2) must be able to adopt multiple conformations, even in a relatively constrained environment; and (3) may mimic the conformational variability of the epitope on HIV-1, increasing the likelihood of eliciting appropriate neutralizing immune responses. Cell Press.

Original language	English (US)
Pages (from-to)	999-1011
Number of pages	13
Journal	Structure
Volume	10
Issue number	7
DOIs	https://doi.org/10.1016/S0969-2126(02)00793-1
State	Published - Jan 1 2002

All Science Journal Classification (ASJC) codes

Structural Biology
Molecular Biology

Keywords

AIDS
Antibody recognition
Chimeric virus
Engineered vaccine
Virus structure

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10.1016/S0969-2126(02)00793-1

Cite this

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title = "Crystal structure of a human rhinovirus that displays part of the HIV-1 V3 loop and induces neutralizing antibodies against HIV-1",

abstract = "We report the 2.7 {\AA} resolution structure of a chimeric rhinovirus, MN-III-2, that displays part of the HIV-1 gp120 V3 loop and elicits HIV-neutralizing antibodies. The V3 loop insert is dominated by two type I β turns. The structures of two adjacent tripeptides resemble those of analogous segments in three Fab/V3 loop peptide complexes. Although two of the three corresponding antibodies bind and neutralize MN-III-2 well, only one of the three can bind without significant rearrangement. These results suggest that the V3 loop insert: (1) can share some local conformational similarity to V3 loop sequences presented on different structural frameworks; (2) must be able to adopt multiple conformations, even in a relatively constrained environment; and (3) may mimic the conformational variability of the epitope on HIV-1, increasing the likelihood of eliciting appropriate neutralizing immune responses. Cell Press.",

keywords = "AIDS, Antibody recognition, Chimeric virus, Engineered vaccine, Virus structure",

author = "Jianping Ding and Smith, \{Allen D.\} and Geisler, \{Sheila C.\} and Xuejun Ma and Arnold, \{Gail Ferstandig\} and Eddy Arnold",

note = "Funding Information: We thank Kalyan Das, Andrew Holmes, Yu Hsiou, Susan Mazzocchi, Deena Oren, Dawn Resnick, Stefan Sarafianos, Sharina Palencia, and Wanyi Zhang for their assistance and valuable discussions. We gratefully acknowledge Dr. Albert Profy, then at Repligen Corporation, for mAbs 50.1 and 59.1, and Dr. Ian Wilson and Dr. Robyn Stanfield at Scripps for the Repligen mAb 58.2. We also thank the staff at the Cornell High Energy Synchrotron Source and at Brookhaven National Laboratory for their support in data collection. This research was supported by NIH grants AI 38221 and AI 45353 to G.F.A. and by CABM and the Keck Foundation. ",

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doi = "10.1016/S0969-2126(02)00793-1",

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T1 - Crystal structure of a human rhinovirus that displays part of the HIV-1 V3 loop and induces neutralizing antibodies against HIV-1

AU - Ding, Jianping

AU - Smith, Allen D.

AU - Geisler, Sheila C.

AU - Ma, Xuejun

AU - Arnold, Gail Ferstandig

AU - Arnold, Eddy

N1 - Funding Information: We thank Kalyan Das, Andrew Holmes, Yu Hsiou, Susan Mazzocchi, Deena Oren, Dawn Resnick, Stefan Sarafianos, Sharina Palencia, and Wanyi Zhang for their assistance and valuable discussions. We gratefully acknowledge Dr. Albert Profy, then at Repligen Corporation, for mAbs 50.1 and 59.1, and Dr. Ian Wilson and Dr. Robyn Stanfield at Scripps for the Repligen mAb 58.2. We also thank the staff at the Cornell High Energy Synchrotron Source and at Brookhaven National Laboratory for their support in data collection. This research was supported by NIH grants AI 38221 and AI 45353 to G.F.A. and by CABM and the Keck Foundation.

PY - 2002/1/1

Y1 - 2002/1/1

N2 - We report the 2.7 Å resolution structure of a chimeric rhinovirus, MN-III-2, that displays part of the HIV-1 gp120 V3 loop and elicits HIV-neutralizing antibodies. The V3 loop insert is dominated by two type I β turns. The structures of two adjacent tripeptides resemble those of analogous segments in three Fab/V3 loop peptide complexes. Although two of the three corresponding antibodies bind and neutralize MN-III-2 well, only one of the three can bind without significant rearrangement. These results suggest that the V3 loop insert: (1) can share some local conformational similarity to V3 loop sequences presented on different structural frameworks; (2) must be able to adopt multiple conformations, even in a relatively constrained environment; and (3) may mimic the conformational variability of the epitope on HIV-1, increasing the likelihood of eliciting appropriate neutralizing immune responses. Cell Press.

AB - We report the 2.7 Å resolution structure of a chimeric rhinovirus, MN-III-2, that displays part of the HIV-1 gp120 V3 loop and elicits HIV-neutralizing antibodies. The V3 loop insert is dominated by two type I β turns. The structures of two adjacent tripeptides resemble those of analogous segments in three Fab/V3 loop peptide complexes. Although two of the three corresponding antibodies bind and neutralize MN-III-2 well, only one of the three can bind without significant rearrangement. These results suggest that the V3 loop insert: (1) can share some local conformational similarity to V3 loop sequences presented on different structural frameworks; (2) must be able to adopt multiple conformations, even in a relatively constrained environment; and (3) may mimic the conformational variability of the epitope on HIV-1, increasing the likelihood of eliciting appropriate neutralizing immune responses. Cell Press.

KW - AIDS

KW - Antibody recognition

KW - Chimeric virus

KW - Engineered vaccine

KW - Virus structure

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Crystal structure of a human rhinovirus that displays part of the HIV-1 V3 loop and induces neutralizing antibodies against HIV-1

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