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Nanobody engineering for SARS-CoV-2 neutralization and detection

Publiceringsår

2024

Upphovspersoner

Hannula, Liina; Kuivanen, Suvi; Lasham, Jonathan; Kant, Ravi; Kareinen, Lauri; Bogacheva, Mariia; Strandin, Tomas; Sironen, Tarja; Hepojoki, Jussi; Sharma, Vivek; Saviranta, Petri; Kipar, Anja; Vapalahti, Olli; Huiskonen, Juha T.; Rissanen, Ilona

Abstrakt

<p>UNLABELLED: In response to the ongoing COVID-19 pandemic, the quest for coronavirus inhibitors has inspired research on a variety of small proteins beyond conventional antibodies, including robust single-domain antibody fragments, i.e., "nanobodies." Here, we explore the potential of nanobody engineering in the development of antivirals and diagnostic tools. Through fusion of nanobody domains that target distinct binding sites, we engineered multimodular nanobody constructs that neutralize wild-type SARS-CoV-2 and the Alpha and Delta variants at high potency, with IC 50 values as low as 50 pM. Despite simultaneous binding to distinct epitopes, Beta and Omicron variants were more resistant to neutralization by the multimodular nanobodies, which highlights the importance of accounting for antigenic drift in the design of biologics. To further explore the applications of nanobody engineering in outbreak management, we present an assay based on fusions of nanobodies with fragments of NanoLuc luciferase that can detect sub-nanomolar quantities of the SARS-CoV-2 spike protein in a single step. Our work showcases the potential of nanobody engineering to combat emerging infectious diseases. </p><p>IMPORTANCE: Nanobodies, small protein binders derived from the camelid antibody, are highly potent inhibitors of respiratory viruses that offer several advantages over conventional antibodies as candidates for specific therapies, including high stability and low production costs. In this work, we leverage the unique properties of nanobodies and apply them as building blocks for new therapeutic and diagnostic tools. We report ultra-potent SARS-CoV-2 inhibition by engineered nanobodies comprising multiple modules in structure-guided combinations and develop nanobodies that carry signal molecules, allowing rapid detection of the SARS-CoV-2 spike protein. Our results highlight the potential of engineered nanobodies in the development of effective countermeasures, both therapeutic and diagnostic, to manage outbreaks of emerging viruses.</p>
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Organisationer och upphovspersoner

Helsingfors universitet

Kipar Anja

Rissanen Ilona

Lasham Jonathan

Huiskonen Juha T.

Hepojoki Jussi

Kareinen Lauri

Hannula Liina

Bogacheva Mariia

Vapalahti Olli

Kant Ravi

Kuivanen Suvi

Sironen Tarja

Strandin Tomas

Sharma Vivek

Helsingforsregionens universitetscentralsjukhus specialupptagningsområde

Kipar Anja

Rissanen Ilona

Lasham Jonathan

Huiskonen Juha T.

Hepojoki Jussi

Kareinen Lauri

Hannula Liina

Bogacheva Mariia

Vapalahti Olli

Kant Ravi

Kuivanen Suvi

Sironen Tarja

Strandin Tomas

Sharma Vivek

Livsmedelsverket

Kareinen Lauri Orcid -palvelun logo

Publikationstyp

Publikationsform

Artikel

Moderpublikationens typ

Tidning

Artikelstyp

En originalartikel

Målgrupp

Vetenskaplig

Kollegialt utvärderad

Kollegialt utvärderad

UKM:s publikationstyp

A1 Originalartikel i en vetenskaplig tidskrift

Publikationskanalens uppgifter

Moderpublikationens namn

Microbiology Spectrum

Volym

12

Nummer

4

Artikelnummer

e0419922

Publikationsforum

86021

Publikationsforumsnivå

2

Öppen tillgång

Öppen tillgänglighet i förläggarens tjänst

Ja

Öppen tillgång till publikationskanalen

Helt öppen publikationskanal

Parallellsparad

Ja

Publiceringsavgift för öppen tillgång €

2412

Övriga uppgifter

Vetenskapsområden

Växtbiologi, mikrobiologi, virologi; Biomedicinska vetenskaper

Nyckelord

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Publiceringsland

Förenta staterna (USA)

Förlagets internationalitet

Internationell

Språk

engelska

Internationell sampublikation

Ja

Sampublikation med ett företag

Nej

DOI

10.1128/spectrum.04199-22

Publikationen ingår i undervisnings- och kulturministeriets datainsamling

Ja