HIV-1 Envelope Recognition by Polyreactive and Cross-Reactive Intestinal B Cells

Planchais, Cyril; Kök, Ayrin; Kanyavuz, Alexia; Lorin, Valérie; Bruel, Timothée; Guivel‐Benhassine, Florence; Rollenske, Tim; Prigent, Julie; Hieu, Thierry; Prazuck, Thiérry; Lefrou, Laurent; Wardemann, Hedda; Dimitrov, Jordan D.; Hocqueloux, Laurent; Mouquet, Hugo

doi:10.1016/j.celrep.2019.03.032

Cited by 23 publications

(47 citation statements)

References 78 publications

(164 reference statements)

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“…This implies the existence of antibodies whose primary function is to act as polyreactive sentries in the gut, yet the downstream effects of polyreactive antibodies coating commensal bacteria is so far unclear. Similar polyreactive IgA and IgG mucosal antibodies were found in the gut of human immunodeficiency virus (HIV)-infected patients, but these antibodies either had low affinity to the virus or lacked neutralization capabilities ( Planchais et al, 2019 ). The benefit of singular antibody sequences with the ability to sample large portions of the commensal population may represent an improvement in efficiency of the homeostatic machinery of the gut.…”

Section: Introductionmentioning

confidence: 90%

Biochemical patterns of antibody polyreactivity revealed through a bioinformatics-based analysis of CDR loops

Boughter

Borowska

Guthmiller

et al. 2020

eLife

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Antibodies are critical components of adaptive immunity, binding with high affinity to pathogenic epitopes. Antibodies undergo rigorous selection to achieve this high affinity, yet some maintain an additional basal level of low affinity, broad reactivity to diverse epitopes, a phenomenon termed 'polyreactivity'. While polyreactivity has been observed in antibodies isolated from various immunological niches, the biophysical properties that allow for promiscuity in a protein selected for high affinity binding to a single target remain unclear. Using a database of over 1,000 polyreactive and non-polyreactive antibody sequences, we created a bioinformatic pipeline to isolate key determinants of polyreactivity. These determinants, which include an increase in inter-loop crosstalk and a propensity for a neutral binding surface, are sufficient to generate a classifier able to identify polyreactive antibodies with over 75% accuracy. The framework from which this classifier was built is generalizable, and represents a powerful, automated pipeline for future immune repertoire analysis.

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Section: Introductionmentioning

confidence: 90%

Biochemical patterns of antibody polyreactivity revealed through a bioinformatics-based analysis of CDR loops

Boughter

Borowska

Guthmiller

et al. 2020

eLife

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“…Recent work identified monoclonal antibodies produced by B cells in the gastrointestinal tract that target the HIV1 envelope, but also cross-react with a number of intestinal proteins. Sequence and/or structural homology was proposed as the molecular basis for this phenomenon (Planchais et al, 2019). We propose that the BCR on the surface of dual-specific B cells recognizes an epitope on the external aspect of the capsid that is shared among different RV strains.…”

Section: Discussionmentioning

confidence: 96%

T-bet+ Memory B Cells Link to Local Cross-Reactive IgG upon Human Rhinovirus Infection

Eccles¹,

Turner²,

Kirk³

et al. 2020

Cell Reports

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“…Notably, the context and antigen can change the role and characteristics of polyreactive mAbs. HIV-binding polyreactive mAbs are low affinity and non-neutralizing and derive from intestinal B cells ( Planchais et al., 2019 ; Liao et al., 2011 ). However, HIV-binding polyreactive mAbs can become potently neutralizing against HIV through affinity maturation ( Liao et al., 2011 ; Prigent et al., 2018 ).…”

Section: Discussionmentioning

confidence: 99%

Polyreactive Broadly Neutralizing B cells Are Selected to Provide Defense against Pandemic Threat Influenza Viruses

et al. 2020

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Summary Polyreactivity is the ability of a single antibody to bind to multiple molecularly distinct antigens and is a common feature of antibodies induced upon pathogen exposure. However, little is known about the role of polyreactivity during anti-influenza virus antibody responses. By analyzing more than 500 monoclonal antibodies (mAbs) derived from B cells induced by numerous influenza virus vaccines and infections, we found mAbs targeting conserved neutralizing influenza virus hemagglutinin epitopes were polyreactive. Polyreactive mAbs were preferentially induced by novel viral exposures due to their broad viral binding breadth. Polyreactivity augmented mAb viral binding strength by increasing antibody flexibility, allowing for adaption to imperfectly conserved epitopes. Lastly, we found affinity-matured polyreactive B cells were typically derived from germline polyreactive B cells that were preferentially selected to participate in B cell responses over time. Together, our data reveal that polyreactivity is a beneficial feature of antibodies targeting conserved epitopes.

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HIV-1 Envelope Recognition by Polyreactive and Cross-Reactive Intestinal B Cells

Cited by 23 publications

References 78 publications

Biochemical patterns of antibody polyreactivity revealed through a bioinformatics-based analysis of CDR loops

Biochemical patterns of antibody polyreactivity revealed through a bioinformatics-based analysis of CDR loops

T-bet+ Memory B Cells Link to Local Cross-Reactive IgG upon Human Rhinovirus Infection

Polyreactive Broadly Neutralizing B cells Are Selected to Provide Defense against Pandemic Threat Influenza Viruses

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