Bi-paratopic and multivalent VH domains block ACE2 binding and neutralize SARS-CoV-2

Bracken, Colton; Lim, Shion A.; Solomon, Paige; Rettko, Nicholas J.; Nguyen, Duy; Zha, Beth Shoshana; Byrnes, James R.; Zhou, Jie; Lui, Irene; Liu, Jia; Pance, Katarina; Brilot, Axel F.; Lopez, Kyle E.; Melo, Arthur A.; Moss, Frank R.; Rizo, Alexandrea N.; Sun, Ming; Thomas, Paul; Wang, Feng; Braxton, Julian R.; Chio, Un Seng; Dickinson, Miles Sasha; Li, Fēi; Li, Junrui; Liu, Yanxin; Nguyen, Henry C.; Pospiech, Thomas H.; Trinidad, Donovan; Zhang, Kaihua; Billesboelle, Christian; Bowen, Alisa; Campbell, Melody G.; Diwanji, Devan; Hoppe, Nick; Li, Yen-Li; Nguyen, Phuong T.; Nowotny, Carlos; Puchades, Cristina; Safari, Mali; Sangwan, Smriti; Smith, Amber M.; Trenker, Raphael; Whitis, Natalie; Zhao, Jianhua; Asarnow, Daniel; Azumaya, Caleigh M.; Chio, Cynthia M.; Faust, Bryan; Kim, Kate; Moritz, Michelle; Owens, Tristan W.; Peters, Jessica K.; Pourmal, Sergei; Schaefer, Kaitlin; Tsui, Tsz Kin Martin; Biel, J.T.; Deshpande, Ishan; Herrera, Nadia; Liu, Xi; Schulze‐Gahmen, Ursula; Young, Iris D.; Chen, Jen; Diallo, Amy; Doan, Loan; Flores, Sebastián; Gupta, Meghna; Jin, Mingliang; Kratochvil, Huong T.; Lam, Victor; Yang, Li; Lo, Megan; Merz, Gregory E.; Paulino, Joana; Thwin, Aye C.; Titus, Erron W.; Yu, Zanlin; Zhou, Fengbo; Zhang, Yang; Bulkley, David; Joves, Arceli; Joves, Almarie; McKay, Liam; Tabios, Mariano; Tse, Eric; Agard, David A.; Cheng, Yifan; Fraser, James S.; Frost, Adam; Jura, Natalia; Kortemme, Tanja; Krogan, Nevan J.; Manglik, Aashish; Rosenberg, Oren S.; Southworth, Daniel R.; Stroud, Robert M.; Verba, Kliment A.; Zhou, Xin; Leung, Kevin; Wells, James A.

doi:10.1038/s41589-020-00679-1

Cited by 85 publications

(104 citation statements)

References 58 publications

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“…VH domains that bind outside of the ACE2 binding site were not identified with this selection campaign. 8 Here, we used an in-house Fab-phage library to identify unbiased Fab binders that recognize Spike-RBD. Briefly, for each round of selection, the Fab-phage pool was pre-cleared with biotinylated Fc immobilized on streptavidin (SA)-coated magnetic beads before incubating with SA-beads conjugated with biotinylated Spike-RBD-Fc ( Figure 1a).…”

Section: Identification and Characterization Of Fabs Against Sars-covmentioning

confidence: 99%

“…The epitope of VH B01 was determined previously by cryo-EM. 8 In the absence of a high-resolution structure of Fab D01 bound to Spike, we used the structure of CR3022 12 as a surrogate to model how the two arms on Bis4 could engage Spike. We find that in the context of the same RBD, the VH and Fab bind at separate, non-overlapping epitopes ( Supplementary Figure 6a-b).…”

Section: Structural Modeling Of the Epitopes Targeted By Bispecific Imentioning

confidence: 99%

“…SARS-CoV-2 has emerged as a global health concern and effective therapeutics are necessary to curb the COVID-19 pandemic. Many potential therapeutic options for treating COVID-19 have been explored, including small molecules, 1 convalescent patient sera, 2 decoy receptors, [3][4][5][6] neutralizing antibodies, [7][8][9][10][11][12][13][14][15][16][17][18] and other protein scaffolds. [19][20][21] In particular, antibodies are advantageous due to their specific and potent binding, demonstrated pharmacokinetics, and ability to be recombinantly produced and manufactured at scale.…”

Section: Introductionmentioning

confidence: 99%

“…SARS-CoV-2 antibodies have been derived from several sources, including B-cells of convalescent patients 7,12,13,17 and people with prior coronavirus infections, 14,15 animal immunization, 10,18 and synthetic libraries or de novo design. 8,9,11,16,19 Most of the antibodies reported to date potently target the receptor-binding domain (RBD) in the trimeric Spike protein on the surface of SARS-CoV-2, 7,13,[22][23][24] which is highly immunogenic and is the key protein that mediates cellular entry via interaction with the host angiotensin-converting enzyme II (ACE2) receptor. 25 However, given the widespread global impact of this pandemic and limitations in biologic manufacturing capacities, means to further increase the potency of these antibodies and thereby decrease the dose required will be critical in meeting the global demand for therapeutics.…”

Section: Introductionmentioning

confidence: 99%

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Bispecific VH/Fab antibodies targeting neutralizing and non-neutralizing Spike epitopes demonstrate enhanced potency against SARS-CoV-2

Lim

Gramespacher

Pance

et al. 2021

mAbs

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Numerous neutralizing antibodies that target SARS-CoV-2 have been reported, and most directly block binding of the viral Spike receptor-binding domain (RBD) to angiotensin-converting enzyme II (ACE2). Here, we deliberately exploit non-neutralizing RBD antibodies, showing they can dramatically assist in neutralization when linked to neutralizing binders. We identified antigen-binding fragments (Fabs) by phage display that bind RBD, but do not block ACE2 or neutralize virus as IgGs. When these nonneutralizing Fabs were assembled into bispecific VH/Fab IgGs with a neutralizing VH domain, we observed a ~ 25-fold potency improvement in neutralizing SARS-CoV-2 compared to the mono-specific bi-valent VH-Fc alone or the cocktail of the VH-Fc and IgG. This effect was epitope-dependent, reflecting the unique geometry of the bispecific antibody toward Spike. Our results show that a bispecific antibody that combines both neutralizing and non-neutralizing epitopes on Spike-RBD is a promising and rapid engineering strategy to improve the potency of SARS-CoV-2 antibodies.

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Section: Identification and Characterization Of Fabs Against Sars-covmentioning

confidence: 99%

Section: Structural Modeling Of the Epitopes Targeted By Bispecific Imentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Bispecific VH/Fab antibodies targeting neutralizing and non-neutralizing Spike epitopes demonstrate enhanced potency against SARS-CoV-2

Lim

Gramespacher

Pance

et al. 2021

mAbs

Self Cite

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show abstract

“…Single, as well as multiple targeting, can be achieved through the use of an engineered antibody. Multivalent antibodies not only block signaling but also overcome resistance through multiple targets [57].…”

Section: Intrinsic Therapeutic Effectmentioning

confidence: 99%

Targeted Cancer Therapy Using Nanoparticles and Antibody Fragments

Bhattacharya¹,

Gore²

2021

Advances in Precision Medicine Oncology

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Cancer is caused by an uncontrolled cell division, forming a tumor capable of metastasis. Cancer is the second leading cause of death worldwide. Conventional treatments kill healthy cells, causing side effects. Recently, nanomaterials are explored due to properties such as as- nano-size, high loading, and ligands’ attachment for a selective delivery. Apart from normal body cells, cancer cells express many receptors in excess, which serve as ‘targets’ for attacking the cells. Various ligands like proteins, peptides, polysaccharides can be attached to nanoparticles to allow proper and specific reach to the tumor. Such nanoparticles go to their desired site and stick onto the receptors, taken inside the cells by various methods. Antibodies are natural proteins that bind to foreign substances and remove them. IgG being the most explored antibody, suffers from many disadvantages such as non-specificity for required antigen, limited binding sites, low tumor penetration. Hence many researchers experimented by removing and adjusting the binding sites, using only the binding sites, enhancing the valency of naturally available IgG. It gave many benefits such as enhanced penetration, reduced immunogenicity, better delivery of drugs with fewer side effects. Continuing advancements in the field of protein engineering will help scientists to come up with better solutions. The properties allow easy surface interaction and entry, achieve better biodistribution, and reduce the amount of drug required. Targeting is based on Paul Ehrlich’s ‘magic bullet, ‘where the therapeutic moiety has two parts-one to identify the target and the second to eliminate it. This concept is revised to incorporate a third component, a carrier. Many nanocarriers can be used to target cancer cells containing ligands to identify malignant cells. Approaches to targeting are passive, active and physical targeting. Many such nanoparticles are in clinical trials and can be a better solution to cancer therapy.

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A SARS‐CoV‐2 Spike Binding DNA Aptamer that Inhibits Pseudovirus Infection by an RBD‐Independent Mechanism**

et al. 2021

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The receptor binding domain (RBD) of the spike glycoprotein of the coronavirus SARS-CoV-2 (CoV2-S) binds to the human angiotensin-converting enzyme 2( ACE2) representing the initial contact point for leveraging the infection cascade.W eu sed an automated selection process and identified an aptamer that specifically interacts with CoV2-S. The aptamer does not bind to the RBD of CoV2-S and does not blockthe interaction of CoV2-S with ACE2. Nevertheless, infection studies revealed potent and specific inhibition of pseudoviral infection by the aptamer.The present study opens up new vistas in developing SARS-CoV2 infection inhibitors, independent of blocking the ACE2 interaction of the virus,and harnesses aptamers as potential drug candidates and tools to disentangle hitherto inaccessible infection modalities,w hichi s of particular interest in light of the increasing number of escape mutants that are currently being reported.

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Bi-paratopic and multivalent VH domains block ACE2 binding and neutralize SARS-CoV-2

Cited by 85 publications

References 58 publications

Bispecific VH/Fab antibodies targeting neutralizing and non-neutralizing Spike epitopes demonstrate enhanced potency against SARS-CoV-2

Bispecific VH/Fab antibodies targeting neutralizing and non-neutralizing Spike epitopes demonstrate enhanced potency against SARS-CoV-2

Targeted Cancer Therapy Using Nanoparticles and Antibody Fragments

A SARS‐CoV‐2 Spike Binding DNA Aptamer that Inhibits Pseudovirus Infection by an RBD‐Independent Mechanism**

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