Discovery and characterization of single-domain antibodies for polymeric Ig receptor-mediated mucosal delivery of biologics

Maruthachalam, Bharathikumar Vellalore; Zwolak, Adam; Lin-Schmidt, Xiefan; Keough, Edward; Tamot, Ninkka; Venkataramani, Sathya; Geist, Brian; Singh, Sanjaya; Ganesan, Rajkumar

doi:10.1080/19420862.2019.1708030

Cited by 7 publications

(7 citation statements)

References 36 publications

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“…We previously identified a panel of heavy chain only (VHH) antibodies that could bind human pIgR with affinities ranging from ~4 to 500 nM. 41 Of these, VHH2 and VHH6 were included in this analysis since VHH2 displayed cross-reactivity to mouse pIgR and both displayed strong transcytosis in an MDCK monolayer-based assay and in a human epithelial airway model. To mediate binding to the SARS-CoV-2 spike glycoprotein, we identified 2 antibodies that were reported to display neutralization activity – D001 (Sino Biological cat.…”

Section: Resultsmentioning

confidence: 99%

“…Bifunctional molecules containing VHH2 (CV19B283, CV19B307, and CV19B308) bound to pIgR with Kd values ~5 nM, consistent with our previous findings. 41 Bifunctional molecules containing VHH6 (CV19B277 and CV19B301) bound with Kd ~ 0.2 mM or 265 nM, respectively. The significantly weaker binding by CV19B277 may have been due to its being fused in tandem on the N-terminus of ACE2, although the mechanism for its reduced binding was unknown.…”

Section: Resultsmentioning

confidence: 99%

“…The anti-pIgR VHH modules could mediate transcytosis across both MDCK cell bilayers and in a human epithelial microtissue model, and we thus asked whether this pIgR-mediated transcytosis could occur in vivo . 41 We selected VHH2, and VHH6 for pharmacokinetic analysis in either monovalent or bivalent format in C57BL/6 mice ( Supplementary Fig. S4, Supplementary Table S1 ).…”

Section: Resultsmentioning

confidence: 99%

“… 40 We and others have developed anti-pIgR single-domain antibodies (VHH) that can exploit pIgR-mediated transcytosis to deliver IgG across the endothelium into the lung mucosa. 41 , 42 We have shown that molecules harboring the anti-pIgR domains displayed increased level of transport across Madin-Darby canine kidney (MDCK) cell-derived monolayers and across human-derived lung epithelial layers by >30-fold compared to conventional IgG. 41 This platform, which we call BRING-IT ( B i-di r ect i o n al polymeric I g receptor med i ated t ransport of biologics), has the potential to deliver IgG into the mucosal lumen, where it can target and neutralize mucosal antigens or pathogens such as SARS-CoV-2.…”

Section: Introductionmentioning

confidence: 99%

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Bifunctional molecules targeting SARS-CoV-2 spike and the polymeric Ig receptor display neutralization activity and mucosal enrichment

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Tamot

Doddareddy

et al. 2021

mAbs

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The global health crisis and economic tolls of COVID-19 necessitate a panoply of strategies to treat SARS-CoV-2 infection. To date, few treatment options exist, although neutralizing antibodies against the spike glycoprotein have proven to be effective. Because infection is initiated at the mucosa and propagates mainly at this site throughout the course of the disease, blocking the virus at the mucosal milieu should be effective. However, administration of biologics to the mucosa presents a substantial challenge. Here, we describe bifunctional molecules combining single-domain variable regions that bind to the polymeric Ig receptor (pIgR) and to the SARS-CoV-2 spike protein via addition of the ACE2 extracellular domain (ECD). The hypothesis behind this design is that pIgR will transport the molecule from the circulation to the mucosal surface where the ACE ECD would act as a decoy receptor for the nCoV2. The bifunctional molecules bind SARS-Cov-2 spike glycoprotein in vitro and efficiently transcytose across the lung epithelium in human tissue-based analyses. Designs featuring ACE2 tethered to the C-terminus of the Fc do not induce antibody-dependent cytotoxicity against pIgR-expressing cells. These molecules thus represent a potential therapeutic modality for systemic administration of neutralizing anti-SARS-CoV-2 molecules to the mucosa.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Bifunctional molecules targeting SARS-CoV-2 spike and the polymeric Ig receptor display neutralization activity and mucosal enrichment

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Tamot

Doddareddy

et al. 2021

mAbs

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“…[1][2][3] The ability of nanobodies to specifically target unique epitopes with subnanomolar affinity, and to penetrate dense solid tumours make them a powerful tool in medical therapeutic procedures and in tumour pathobiology. 2,[5][6][7] Improvements in drug delivery and monitoring of diseases in biotherapeutics…”

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Improvements in drug delivery and monitoring of diseases in biotherapeutics

Melrose¹

2020

JSRT

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VHH nanobodies were discovered almost 25 years ago and have been used to specifically target cells in cancer therapy and to develop novel antimicrobials. [1][2][3][4] Nanobodies, recombinant, antigen-specific, singledomain, variable Ig fragments of Camelid (Camelus dromarius, Camelus bactrianus, Lama glama, Lama pacos, Lama guanicoe and Lama vicugna) heavy chain-only antibodies are affinity bioreagents that have been produced in high yield in a broad range of expression systems. [1][2][3] The ability of nanobodies to specifically target unique epitopes with subnanomolar affinity, and to penetrate dense solid tumours make them a powerful tool in medical therapeutic procedures and in tumour pathobiology. 2,[5][6][7] Improvements in drug delivery and monitoring of diseases in biotherapeutics

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A Biomolecular Toolbox for Precision Nanomotors

et al. 2023

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Figure 2. Chemically propelled nanomotors. a) Pt/Cr coated Janus nanomotors loaded with doxorubicin and functionalized with folic acid. Reproduced with permission. [54] Copyright 2014, John Wiley and Sons; b) pH-responsive ZIF-L nanomotors encapsulated with catalase and succinylated β-lactoglobulin, reproduced with permission. [55] Copyright 2019, John Wiley and Sons; c) vertically driven pH-responsive ZIF-L nanomotors encapsulating catalase and PDPA. Reproduced with permission. [34] Copyright 2019, Elsevier; d) Nanomotors constructed out of heparin, folic acid, and L-arginine were loaded with doxorubicin for the nitric oxide-mediated treatment of solid tumors. Reproduced under terms of the CC-BY license. [45] Copyright 2022, John Wiley and Sons; e) ZIF-8-coated up-conversion nanoparticles functionalised with glucose oxidase and catalase for photodynamic and oxygen starvation therapy of cancer cells. Reproduced with permission. [43] Copyright 2019, Elsevier; f) A jellyfish-shaped multi-metallic shell micromotor for DNA detection. Reproduced with permission. [57] Copyright 2014, John Wiley and Sons. g) Magnesium-based micromotor coated with titanium, PLGA embedded with clarithromycin and chitosan for the treatment of a stomach infection. Reproduced under terms of the CC-BY license. [59] Copyright 2017, Springer Nature; h) Mesoporous silica nanoparticles functionalized with urease and anti-FGFR3 for bladder treatment. Reproduced with permission. [60]

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Discovery and characterization of single-domain antibodies for polymeric Ig receptor-mediated mucosal delivery of biologics

Cited by 7 publications

References 36 publications

Bifunctional molecules targeting SARS-CoV-2 spike and the polymeric Ig receptor display neutralization activity and mucosal enrichment

Bifunctional molecules targeting SARS-CoV-2 spike and the polymeric Ig receptor display neutralization activity and mucosal enrichment

Improvements in drug delivery and monitoring of diseases in biotherapeutics

A Biomolecular Toolbox for Precision Nanomotors

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