Your search keyword '"Single-domain antibodies"' showing total 73 results

1. rAAV expressing recombinant antibody for emergency prevention and long-term prophylaxis of COVID-19.

Author

Esmagambetov, Ilias B., Ryabova, Ekaterina I., Derkaev, Artem A., Shcheblyakov, Dmitry V., Dolzhikova, Inna V., Favorskaya, Irina A., Grousova, Daria M., Dovgiy, Mikhail A., Prokofiev, Vladimir V., Gosudarev, Andrey I., Byrikhina, Daria V., Zorkov, Ilia D., Iliukhina, Anna A., Kovyrshina, Anna V., Shelkov, Artem Y., Naroditsky, Boris S., Logunov, Denis Y., and Gintsburg, Alexander L.

Subjects

RECOMBINANT antibodies, SARS-CoV-2 Omicron variant, GENETIC vectors, SARS-CoV-2, COVID-19

Abstract

Introduction: Numerous agents for prophylaxis of SARS-CoV-2-induced diseases are currently registered for the clinical use. Formation of the immunity happens within several weeks following vaccine administration which is their key disadvantage. In contrast, drugs based on monoclonal antibodies, enable rapid passive immunization and therefore can be used for emergency pre- and postexposure prophylaxis of COVID-19. However rapid elimination of antibody-based drugs from the circulation limits their usage for prolonged pre-exposure prophylaxis. Methods: In current work we developed a recombinant adeno-associated viral vector (rAAV), expressing a SARS-CoV-2 spike receptor-binding domain (RBD)- specific antibody P2C5 fused with a human IgG1 Fc fragment (P2C5-Fc) using methods of molecular biotechnology and bioprocessing. Results and discussions: A P2C5-Fc antibody expressed by a proposed rAAV (rAAV-P2C5-Fc) was shown to circulate within more than 300 days in blood of transduced mice and protect animals from lethal SARS-CoV-2 virus (B.1.1.1 and Omicron BA.5 variants) lethal dose of 105 TCID50. In addition, rAAV-P2C5-Fc demonstrated 100% protective activity as emergency prevention and long-term prophylaxis, respectively. It was also demonstrated that high titers of neutralizing antibodies to the SARS-CoV-2 virus were detected in the blood serum of animals that received rAAV-P2C5-Fc for more than 10 months from the moment of administration. Our data therefore indicate applicability of an rAAV for passive immunization and induction of a rapid long-term protection against various SARSCoV-2 variants. [ABSTRACT FROM AUTHOR]

Published

2023

2. rAAV expressing recombinant antibody for emergency prevention and long-term prophylaxis of COVID-19

Author

Ilias B. Esmagambetov, Ekaterina I. Ryabova, Artem A. Derkaev, Dmitry V. Shcheblyakov, Inna V. Dolzhikova, Irina A. Favorskaya, Daria M. Grousova, Mikhail A. Dovgiy, Vladimir V. Prokofiev, Andrey I. Gosudarev, Daria V. Byrikhina, Ilia D. Zorkov, Anna A. Iliukhina, Anna V. Kovyrshina, Artem Y. Shelkov, Boris S. Naroditsky, Denis Y. Logunov, and Alexander L. Gintsburg

Subjects

recombinant adeno-associated viral vector (rAAV), single-domain antibodies, VHH, COVID-19, SARS-CoV-2, passive immunization, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionNumerous agents for prophylaxis of SARS-CoV-2-induced diseases are currently registered for the clinical use. Formation of the immunity happens within several weeks following vaccine administration which is their key disadvantage. In contrast, drugs based on monoclonal antibodies, enable rapid passive immunization and therefore can be used for emergency pre- and post-exposure prophylaxis of COVID-19. However rapid elimination of antibody-based drugs from the circulation limits their usage for prolonged pre-exposure prophylaxis.MethodsIn current work we developed a recombinant adeno-associated viral vector (rAAV), expressing a SARS-CoV-2 spike receptor-binding domain (RBD)-specific antibody P2C5 fused with a human IgG1 Fc fragment (P2C5-Fc) using methods of molecular biotechnology and bioprocessing.Results and discussionsA P2C5-Fc antibody expressed by a proposed rAAV (rAAV-P2C5-Fc) was shown to circulate within more than 300 days in blood of transduced mice and protect animals from lethal SARS-CoV-2 virus (B.1.1.1 and Omicron BA.5 variants) lethal dose of 105 TCID50. In addition, rAAV-P2C5-Fc demonstrated 100% protective activity as emergency prevention and long-term prophylaxis, respectively. It was also demonstrated that high titers of neutralizing antibodies to the SARS-CoV-2 virus were detected in the blood serum of animals that received rAAV-P2C5-Fc for more than 10 months from the moment of administration.Our data therefore indicate applicability of an rAAV for passive immunization and induction of a rapid long-term protection against various SARS-CoV-2 variants.

Published

2023

3. Single-Domain Antibodies Efficiently Neutralize SARS-CoV-2 Variants of Concern.

Author

Favorskaya, Irina A., Shcheblyakov, Dmitry V., Esmagambetov, Ilias B., Dolzhikova, Inna V., Alekseeva, Irina A., Korobkova, Anastasia I., Voronina, Daria V., Ryabova, Ekaterina I., Derkaev, Artem A., Kovyrshina, Anna V., Iliukhina, Anna A., Botikov, Andrey G., Voronina, Olga L., Egorova, Daria A., Zubkova, Olga V., Ryzhova, Natalia N., Aksenova, Ekaterina I., Kunda, Marina S., Logunov, Denis Y., and Naroditsky, Boris S.

Subjects

SARS-CoV-2, SARS-CoV-2 Omicron variant, SARS-CoV-2 Delta variant, IMMUNOGLOBULINS, COVID-19 treatment

Abstract

Virus-neutralizing antibodies are one of the few treatment options for COVID-19. The evolution of SARS-CoV-2 virus has led to the emergence of virus variants with reduced sensitivity to some antibody-based therapies. The development of potent antibodies with a broad spectrum of neutralizing activity is urgently needed. Here we isolated a panel of single-domain antibodies that specifically bind to the receptor-binding domain of SARS-CoV-2 S glycoprotein. Three of the selected antibodies exhibiting most robust neutralization potency were used to generate dimeric molecules. We observed that these modifications resulted in up to a 200-fold increase in neutralizing activity. The most potent heterodimeric molecule efficiently neutralized each of SARS-CoV-2 variant of concern, including Alpha, Beta, Gamma, Delta and Omicron variants. This heterodimeric molecule could be a promising drug candidate for a treatment for COVID-19 caused by virus variants of concern. [ABSTRACT FROM AUTHOR]

Published

2022

4. Single-Domain Antibodies Efficiently Neutralize SARS-CoV-2 Variants of Concern

Author

Irina A. Favorskaya, Dmitry V. Shcheblyakov, Ilias B. Esmagambetov, Inna V. Dolzhikova, Irina A. Alekseeva, Anastasia I. Korobkova, Daria V. Voronina, Ekaterina I. Ryabova, Artem A. Derkaev, Anna V. Kovyrshina, Anna A. Iliukhina, Andrey G. Botikov, Olga L. Voronina, Daria A. Egorova, Olga V. Zubkova, Natalia N. Ryzhova, Ekaterina I. Aksenova, Marina S. Kunda, Denis Y. Logunov, Boris S. Naroditsky, and Alexandr L. Gintsburg

Subjects

SARS-CoV-2, COVID-19, single-domain antibodies, VHH, VOC, neutralizing antibodies, Immunologic diseases. Allergy, RC581-607

Abstract

Virus-neutralizing antibodies are one of the few treatment options for COVID-19. The evolution of SARS-CoV-2 virus has led to the emergence of virus variants with reduced sensitivity to some antibody-based therapies. The development of potent antibodies with a broad spectrum of neutralizing activity is urgently needed. Here we isolated a panel of single-domain antibodies that specifically bind to the receptor-binding domain of SARS-CoV-2 S glycoprotein. Three of the selected antibodies exhibiting most robust neutralization potency were used to generate dimeric molecules. We observed that these modifications resulted in up to a 200-fold increase in neutralizing activity. The most potent heterodimeric molecule efficiently neutralized each of SARS-CoV-2 variant of concern, including Alpha, Beta, Gamma, Delta and Omicron variants. This heterodimeric molecule could be a promising drug candidate for a treatment for COVID-19 caused by virus variants of concern.

Published

2022

5. Serum immunoglobulin or albumin binding single-domain antibodies that enable tailored half-life extension of biologics in multiple animal species.

Author

Harmsen MM, Ackerschott B, and de Smit H

Subjects

Animals, Humans, Dogs, Horses, Swine, Immunoglobulin Heavy Chains, Albumins, Immunoglobulin G, Single-Domain Antibodies, Biological Products, Antitoxins

Abstract

Single-domain antibody fragments (sdAbs) can be isolated from heavy-chain-only antibodies that occur in camelids or the heavy chain of conventional antibodies, that also occur in camelids. Therapeutic application of sdAbs is often complicated by their low serum half-life. Fusion to sdAb that bind to long-lived serum proteins albumin or IgG can prolong serum half-life of fusion partners. Such studies mostly focused on human application. For half-life prolongation in multiple animal species novel species cross-reacting sdAb are needed. We here describe the isolation from immunized llamas of sdAbs G6 and G13 that bound IgG of 9-10 species analysed, including horse, dog, cat, and swine, as well as sdAb A12 that bound horse, dog, swine and cat albumin. A12 bound albumin with 13 to 271 nM affinity dependent on the species. G13 affinity was difficult to determine by biolayer interferometry due to low and heterogeneous signals. G13 and G6 compete for the same binding domain on Fab fragments. Furthermore, they both lack the hallmark residues typical of camelid sdAbs derived from heavy-chain antibodies and had sequence characteristics typical of human sdAbs with high solubility and stability. This suggests they are derived from conventional llama antibodies. They most likely bind IgG through pairing with VL domains at the VH-VL interface rather than a paratope involving complementarity determining regions. None of the isolated sdAb interfered with FcRn binding to albumin or IgG, and thus do not prevent endosomal albumin/IgG-sdAb complex recycling. Fusions of albumin-binding sdAb A12 to several tetanus neurotoxin (TeNT) binding sdAbs prolonged the terminal serum half-life in piglets to about 4 days, comparable to authentic swine albumin. However, G13 conferred a much lower half-life of 0.84 days. Similarly, in horse, G13 prolonged half-life to only 1.2 days whereas A12 fused to two TeNT binding domains (T6T16A12) had a half-life of 21 days. The high half-life of T6T16A12, which earlier proved to be a highly potent TeNT antitoxin, further supports its therapeutic value. Furthermore, we have identified several additional sdAbs that enable tailored half-life extension of biologicals in multiple animal species., Competing Interests: BA and HS were employed by Smivet B.V. while performing the work described here. A patent application was filed describing part of this work. The remaining author declares that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest. The authors declare that the study was funded by Smivet B.V.. The funder (HS) had the following involvement in the study: conceptualization, study design, supervision, validation, decision to publish, and preparation of the manuscript., (Copyright © 2024 Harmsen, Ackerschott and de Smit.)

Published

2024

6. Nanobodies: a promising approach to treatment of viral diseases.

Author

Minatel VM, Prudencio CR, Barraviera B, and Ferreira RS Jr

Subjects

Humans, Tissue Distribution, Antibodies metabolism, Epitopes metabolism, Single-Domain Antibodies, Virus Diseases

Abstract

Since their discovery in the 1990s, heavy chain antibodies have garnered significant interest in the scientific community. These antibodies, found in camelids such as llamas and alpacas, exhibit distinct characteristics from conventional antibodies due to the absence of a light chain in their structure. Furthermore, they possess a single antigen-binding domain known as VHH or Nanobody (Nb). With a small size of approximately 15 kDa, these Nbs demonstrate improved characteristics compared to conventional antibodies, including greater physicochemical stability and enhanced biodistribution, enabling them to bind inaccessible epitopes more effectively. As a result, Nbs have found numerous applications in various medical and veterinary fields, particularly in diagnostics and therapeutics. Advances in biotechnology have made the production of recombinant antibodies feasible and compatible with large-scale manufacturing. Through the construction of immune phage libraries that display VHHs and subsequent selection through biopanning, it has become possible to isolate specific Nbs targeting pharmaceutical targets of interest, such as viruses. This review describes the processes involved in nanobody production, from hyperimmunization to purification, with the aim of their application in the pharmaceutical industry., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Minatel, Prudencio, Barraviera and Ferreira.)

Published

2024

7. Prediction of antigen-responding VHH antibodies by tracking the evolution of antibody along the time course of immunization.

Author

Matsuda T, Akazawa-Ogawa Y, Komaba LK, Kiyose N, Miyazaki N, Mizuguchi Y, Fukuta T, Ito Y, and Hagihara Y

Subjects

Animals, Immunization, Vaccination, Antigens, Immunoglobulin G, Single-Domain Antibodies, Camelids, New World

Abstract

Antibody maturation is the central function of the adaptive immune response. This process is driven by the repetitive selection of mutations that increase the affinity toward antigens. We hypothesized that a precise observation of this process by high-throughput sequencing along the time course of immunization will enable us to predict the antibodies reacting to the immunized antigen without any additional in vitro screening. An alpaca was immunized with IgG fragments using multiple antigen injections, and the antibody repertoire development was traced via high-throughput sequencing periodically for months. The sequences were processed into clusters, and the antibodies in the 16 most abundant clusters were generated to determine whether the clusters included antigen-binding antibodies. The sequences of most antigen-responsive clusters resembled those of germline cells in the early stages. These sequences were observed to accumulate significant mutations and also showed a continuous sequence turnover throughout the experimental period. The foregoing characteristics gave us >80% successful prediction of clusters composed of antigen-responding VHHs against IgG fragment. Furthermore, when the prediction method was applied to the data from other alpaca immunized with epidermal growth factor receptor, the success rate exceeded 80% as well, confirming the general applicability of the prediction method. Superior to previous studies, we identified the immune-responsive but very rare clusters or sequences from the immunized alpaca without any empirical screening data., Competing Interests: Authors YM and TF were employed by JSR Corporation. Authors NK and NM were employed by ARK Resource. Co., Ltd. Kyoto University, AIST, ARK Resource Co. Ltd., and Kagoshima University applied for patents Nos. JP/2019/080434. TM, YA-O, NM, TF, YI, and YH were listed as the inventors. Kyoto University applied for patents Nos. WO/2020/213730. TM, YA-O, NM, TF, YI, and YH were listed as the inventors. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Matsuda, Akazawa-Ogawa, Komaba, Kiyose, Miyazaki, Mizuguchi, Fukuta, Ito and Hagihara.)

Published

2024

8. The GEM-handle as convenient labeling strategy for bimodal single-domain antibody-based tracers carrying 99m Tc and a near-infrared fluorescent dye for intra-operative decision-making.

Author

Declerck NB, Huygen C, Mateusiak L, Stroet MCM, and Hernot S

Subjects

Animals, Mice, Fluorescent Dyes, Tissue Distribution, Tomography, Emission-Computed, Single-Photon methods, Single-Domain Antibodies, Neoplasms diagnostic imaging

Abstract

Intra-operative fluorescence imaging has demonstrated its ability to improve tumor lesion identification. However, the limited tissue penetration of the fluorescent signals hinders the detection of deep-lying or occult lesions. Integrating fluorescence imaging with SPECT and/or intra-operative gamma-probing synergistically combines the deep tissue penetration of gamma rays for tumor localization with the precision of fluorescence imaging for precise tumor resection. In this study, we detail the use of a genetically encoded multifunctional handle, henceforth referred to as a GEM-handle, for the development of fluorescent/radioactive bimodal single-domain antibody (sdAb)-based tracers. A sdAb that targets the urokinase plasminogen activator receptor (uPAR) was engineered to carry a GEM-handle containing a carboxy-terminal hexahistidine-tag and cysteine-tag. A two-step labeling strategy was optimized and applied to site-specifically label IRDye800CW and 99m Tc to the sdAb. Bimodal labeling of the sdAbs proved straightforward and successful. 99m Tc activity was however restricted to 18.5 MBq per nmol fluorescently-labeled sdAb to prevent radiobleaching of IRDye800CW without impeding SPECT/CT imaging. Subsequently, the in vivo biodistribution and tumor-targeting capacity of the bimodal tracer were evaluated in uPAR-positive tumor-bearing mice using SPECT/CT and fluorescence imaging. The bimodal sdAb showed expected renal background signals due to tracer clearance, along with slightly elevated non-specific liver signals. Four hours post-injection, both SPECT/CT and fluorescent images achieved satisfactory tumor uptake and contrast, with significantly higher values observed for the anti-uPAR bimodal sdAb compared to a control non-targeting sdAb. In conclusion, the GEM-handle is a convenient method for designing and producing bimodal sdAb-based tracers with adequate in vivo characteristics., Competing Interests: LM and SH acknowledge that they hold a patent for ‘Anti-urokinase plasminogen activator receptor immunoglobulin single variable domains’, under EP22199885.9. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Declerck, Huygen, Mateusiak, Stroet and Hernot.)

Published

2023

9. Applications of nanobodies in brain diseases

Author

Fang, Zheng, Yucheng, Pang, Luyao, Li, Yuxing, Pang, Jiaxin, Zhang, Xinyi, Wang, and Geert, Raes

Subjects

Blood-Brain Barrier, Alzheimer Disease, Genetic Vectors, Immunology, Humans, Brain, Immunology and Allergy, Single-Domain Antibodies

Abstract

Nanobodies are antibody fragments derived from camelids, naturally endowed with properties like low molecular weight, high affinity and low immunogenicity, which contribute to their effective use as research tools, but also as diagnostic and therapeutic agents in a wide range of diseases, including brain diseases. Also, with the success of Caplacizumab, the first approved nanobody drug which was established as a first-in-class medication to treat acquired thrombotic thrombocytopenic purpura, nanobody-based therapy has received increasing attention. In the current review, we first briefly introduce the characterization and manufacturing of nanobodies. Then, we discuss the issue of crossing of the brain-blood-barrier (BBB) by nanobodies, making use of natural methods of BBB penetration, including passive diffusion, active efflux carriers (ATP-binding cassette transporters), carrier-mediated influx via solute carriers and transcytosis (including receptor-mediated transport, and adsorptive mediated transport) as well as various physical and chemical methods or even more complicated methods such as genetic methods via viral vectors to deliver nanobodies to the brain. Next, we give an extensive overview of research, diagnostic and therapeutic applications of nanobodies in brain-related diseases, with emphasis on Alzheimer’s disease, Parkinson’s disease, and brain tumors. Thanks to the advance of nanobody engineering and modification technologies, nanobodies can be linked to toxins or conjugated with radionuclides, photosensitizers and nanoparticles, according to different requirements. Finally, we provide several perspectives that may facilitate future studies and whereby the versatile nanobodies offer promising perspectives for advancing our knowledge about brain disorders, as well as hopefully yielding diagnostic and therapeutic solutions.

Published

2022

10. Antibody or Antibody Fragments: Implications for Molecular Imaging and Targeted Therapy of Solid Tumors

Author

Katerina T. Xenaki, Sabrina Oliveira, and Paul M. P. van Bergen en Henegouwen

Subjects

molecular imaging, cancer therapy, antibody, antibody fragments, single-domain antibodies, nanobody, Immunologic diseases. Allergy, RC581-607

Abstract

The use of antibody-based therapeutics has proven very promising for clinical applications in cancer patients, with multiple examples of antibodies and antibody–drug conjugates successfully applied for the treatment of solid tumors and lymphomas. Given reported recurrence rates, improvements are clearly still necessary. A major factor limiting the efficacy of antibody-targeted cancer therapies may be the incomplete penetration of the antibody or antibody–drug conjugate into the tumor. Incomplete tumor penetration also affects the outcome of molecular imaging, when using such targeting agents. From the injection site until they arrive inside the tumor, targeting molecules are faced with several barriers that impact intratumoral distribution. The primary means of antibody transport inside tumors is based on diffusion. The diffusive penetration inside the tumor is influenced by both antibody properties, such as size and binding affinity, as well as tumor properties, such as microenvironment, vascularization, and targeted antigen availability. Engineering smaller antibody fragments has shown to improve the rate of tumor uptake and intratumoral distribution. However, it is often accompanied by more rapid clearance from the body and in several cases also by inherent destabilization and reduction of the binding affinity of the antibody. In this perspective, we discuss different cancer targeting approaches based on antibodies or their fragments. We carefully consider how their size and binding properties influence their intratumoral uptake and distribution, and how this may affect cancer imaging and therapy of solid tumors.

Published

2017

11. Intracellular Crosslinking of Filoviral Nucleoproteins with Xintrabodies Restricts Viral Packaging

Author

Tamarand Lee Darling, Laura Jo Sherwood, and Andrew Hayhurst

Subjects

single-domain antibodies, VHH, Marburg, Ebola, nucleoprotein, crosslinker, Immunologic diseases. Allergy, RC581-607

Abstract

Viruses assemble large macromolecular repeat structures that become part of the infectious particles or virions. Ribonucleocapsids (RNCs) of negative strand RNA viruses are a prime example where repetition of nucleoprotein (NP) along the genome creates a core polymeric helical scaffold that accommodates other nucleocapsid proteins including viral polymerase. The RNCs are transported through the cytosol for packaging into virions through association with viral matrix proteins at cell membranes. We hypothesized that RNC would be ideal targets for crosslinkers engineered to promote aberrant protein–protein interactions, thereby blocking their orderly transport and packaging. Previously, we had generated single-domain antibodies (sdAbs) against Filoviruses that have all targeted highly conserved C-terminal regions of NP known to be repetitively exposed along the length of the RNCs of Marburgvirus (MARV) and Ebolavirus (EBOV). Our crosslinker design consisted of dimeric sdAb expressed intracellularly, which we call Xintrabodies (X- for crosslinking). Electron microscopy of purified NP polymers incubated with purified sdAb constructs showed NP aggregation occurred in a genus-specific manner with dimeric and not monomeric sdAb. A virus-like particle (VLP) assay was used for initial evaluation where we found that dimeric sdAb inhibited NP incorporation into VP40-based VLPs whereas monomeric sdAb did not. Inhibition of NP packaging was genus specific. Confocal microscopy revealed dimeric sdAb was diffuse when expressed alone but focused on pools of NP when the two were coexpressed, while monomeric sdAb showed ambivalent partition. Infection of stable Vero cell lines expressing dimeric sdAb specific for either MARV or EBOV NP resulted in smaller plaques and reduced progeny of cognate virus relative to wild-type Vero cells. Though the impact was marginal at later time-points, the collective data suggest that viral replication can be reduced by crosslinking intracellular NP using relatively small amounts of dimeric sdAb to restrict NP packaging. The stoichiometry and ease of application of the approach would likely benefit from transitioning away from intracellular expression of crosslinking sdAb to exogenous delivery of antibody. By retuning sdAb specificity, the approach of crosslinking highly conserved regions of assembly critical proteins may well be applicable to inhibiting replication processes of a broad spectrum of viruses.

Published

2017

12. Single Domain Antibody application in bacterial infection diagnosis and neutralization

Author

Qin, Qian, Liu, Hao, He, Wenbo, Guo, Yucheng, Zhang, Jiaxin, She, Junjun, Zheng, Fang, Zhang, Sicai, Muyldermans, Serge, and Wen, Yurong

Subjects

Immunology, Animals, Humans, Immunology and Allergy, Bacterial Infections, Single-Domain Antibodies, Immunoglobulin Heavy Chains, Camelids, New World, Antibodies

Abstract

Increasing antibiotic resistance to bacterial infections causes a serious threat to human health. Efficient detection and treatment strategies are the keys to preventing and reducing bacterial infections. Due to the high affinity and antigen specificity, antibodies have become an important tool for diagnosis and treatment of various human diseases. In addition to conventional antibodies, a unique class of “heavy-chain-only” antibodies (HCAbs) were found in the serum of camelids and sharks. HCAbs binds to the antigen through only one variable domain Referred to as VHH (variable domain of the heavy chain of HCAbs). The recombinant format of the VHH is also called single domain antibody (sdAb) or nanobody (Nb). Sharks might also have an ancestor HCAb from where SdAbs or V-NAR might be engineered. Compared with traditional Abs, Nbs have several outstanding properties such as small size, high stability, strong antigen-binding affinity, high solubility and low immunogenicity. Furthermore, they are expressed at low cost in microorganisms and amenable to engineering. These superior properties make Nbs a highly desired alternative to conventional antibodies, which are extensively employed in structural biology, unravelling biochemical mechanisms, molecular imaging, diagnosis and treatment of diseases. In this review, we summarized recent progress of nanobody-based approaches in diagnosis and neutralization of bacterial infection and further discussed the challenges of Nbs in these fields.

Published

2022

13. Generation of high affinity ICAM-1-specific nanobodies and evaluation of their suitability for allergy treatment

Author

Ines Zettl, Tatiana Ivanova, Mohammed Zghaebi, Marina V. Rutovskaya, Isabella Ellinger, Oksana Goryainova, Jessica Kollárová, Sergio Villazala-Merino, Christian Lupinek, Christina Weichwald, Anja Drescher, Julia Eckl-Dorna, Sergei V. Tillib, and Sabine Flicker

Subjects

Camelus, Immunology, Hypersensitivity, Immunology and Allergy, Animals, Humans, Rhinitis, Allergic, Seasonal, Single-Domain Antibodies, Allergens, Intercellular Adhesion Molecule-1

Abstract

The nasal cavity is an important site of allergen entry. Hence, it represents an organ where trans-epithelial allergen penetration and subsequent IgE-mediated allergic inflammation can potentially be inhibited. Intercellular adhesion molecule 1 (ICAM-1) is highly expressed on the surface of respiratory epithelial cells in allergic patients. It was identified as a promising target to immobilize antibody conjugates bispecific for ICAM-1 and allergens and thereby block allergen entry. We have previously characterized a nanobody specific for the major birch pollen allergen Bet v 1 and here we report the generation and characterization of ICAM-1-specific nanobodies. Nanobodies were obtained from a camel immunized with ICAM-1 and a high affinity binder was selected after phage display (Nb44). Nb44 was expressed as recombinant protein containing HA- and His-tags in Escherichia coli (E.coli) and purified via affinity chromatography. SDS-PAGE and Western blot revealed a single band at approximately 20 kDa. Nb44 bound to recombinant ICAM-1 in ELISA, and to ICAM-1 expressed on the human bronchial epithelial cell line 16HBE14o- as determined by flow cytometry. Experiments conducted at 4°C and at 37°C, to mimic physiological conditions, yielded similar percentages (97.2 ± 1.2% and 96.7 ± 1.5% out of total live cells). To confirm and visualize binding, we performed immunofluorescence microscopy. While Texas Red Dextran was rapidly internalized Nb44 remained localized on the cell surface. Additionally, we determined the strength of Nb44 and ICAM-1 interaction using surface plasmon resonance (SPR). Nb44 bound ICAM-1 with high affinity (10-10 M) and had slow off-rates (10-4 s-1). In conclusion, our results showed that the selected ICAM-1-specific nanobody bound ICAM-1 with high affinity and was not internalized. Thus, it could be further used to engineer heterodimers with allergen-specific nanobodies in order to develop topical treatments of pollen allergy.

Published

2022

14. Tripartite split-GFP assay to identify selective intracellular nanobody that suppresses GTPase RHOA subfamily downstream signaling

Author

Laura, Keller, Claudine, Tardy, Laetitia, Ligat, Soazig, Le Pennec, Nicolas, Bery, Faten, Koraïchi, Patrick, Chinestra, Mélissa, David, Rémi, Gence, Gilles, Favre, Stéphanie, Cabantous, and Aurélien, Olichon

Subjects

rac1 GTP-Binding Protein, Immunology, ras Proteins, Immunology and Allergy, Guanosine Triphosphate, Single-Domain Antibodies, Actins, Signal Transduction

Abstract

Strategies based on intracellular expression of artificial binding domains present several advantages over manipulating nucleic acid expression or the use of small molecule inhibitors. Intracellularly-functional nanobodies can be considered as promising macrodrugs to study key signaling pathways by interfering with protein-protein interactions. With the aim of studying the RAS-related small GTPase RHOA family, we previously isolated, from a synthetic phage display library, nanobodies selective towards the GTP-bound conformation of RHOA subfamily proteins that lack selectivity between the highly conserved RHOA-like and RAC subfamilies of GTPases. To identify RHOA/ROCK pathway inhibitory intracellular nanobodies, we implemented a stringent, subtractive phage display selection towards RHOA-GTP followed by a phenotypic screen based on F-actin fiber loss. Intracellular interaction and intracellular selectivity between RHOA and RAC1 proteins was demonstrated by adapting the sensitive intracellular protein-protein interaction reporter based on the tripartite split-GFP method. This strategy led us to identify a functional intracellular nanobody, hereafter named RH28, that does not cross-react with the close RAC subfamily and blocks/disrupts the RHOA/ROCK signaling pathway in several cell lines without further engineering or functionalization. We confirmed these results by showing, using SPR assays, the high specificity of the RH28 nanobody towards the GTP-bound conformation of RHOA subfamily GTPases. In the metastatic melanoma cell line WM266-4, RH28 expression triggered an elongated cellular phenotype associated with a loss of cellular contraction properties, demonstrating the efficient intracellular blocking of RHOA/B/C proteins downstream interactions without the need of manipulating endogenous gene expression. This work paves the way for future therapeutic strategies based on protein-protein interaction disruption with intracellular antibodies.

Published

2022

15. NanoNet: Rapid and accurate end-to-end nanobody modeling by deep learning

Author

Cohen, Tomer, Halfon, Matan, and Schneidman-Duhovny, Dina

Subjects

Deep Learning, Immunology, Immunology and Allergy, Amino Acid Sequence, Single-Domain Antibodies, Complementarity Determining Regions, Antibodies

Abstract

Antibodies are a rapidly growing class of therapeutics. Recently, single domain camelid VHH antibodies, and their recognition nanobody domain (Nb) appeared as a cost-effective highly stable alternative to full-length antibodies. There is a growing need for high-throughput epitope mapping based on accurate structural modeling of the variable domains that share a common fold and differ in the Complementarity Determining Regions (CDRs). We develop a deep learning end-to-end model, NanoNet, that given a sequence directly produces the 3D coordinates of the backbone and Cβ atoms of the entire VH domain. For the Nb test set, NanoNet achieves 3.16Å average RMSD for the most variable CDR3 loops and 2.65Å, 1.73Å for the CDR1, CDR2 loops, respectively. The accuracy for antibody VH domains is even higher: 2.38Å RMSD for CDR3 and 0.89Å, 0.96Å for the CDR1, CDR2 loops, respectively. NanoNet run times allow generation of ∼1M nanobody structures in less than 4 hours on a standard CPU computer enabling high-throughput structure modeling. NanoNet is available at GitHub: https://github.com/dina-lab3D/NanoNet

Published

2022

16. CD38-specific nanobodies allow

Author

Luca Julius, Pape, Julia, Hambach, Anna Josephine, Gebhardt, Björn, Rissiek, Tobias, Stähler, Natalie, Tode, Cerusch, Khan, Katja, Weisel, Gerhard, Adam, Friedrich, Koch-Nolte, and Peter, Bannas

Subjects

Mice, Epitopes, Humans, Animals, Single-Domain Antibodies, Multiple Myeloma, ADP-ribosyl Cyclase 1, Fluorescent Dyes

Abstract

Recent studies have demonstrated the feasibility of CD38-specific antibody constructs forWe conjugated the CD38-specific nanobody JK36 to the near-infrared fluorescent dye Alexa Fluor 680. The capacity of JK36Fluorochrome-labeled nanobody JK36Our study demonstrates that a nanobody recognizing a distinct, non-overlapping epitope of CD38 allows the specific detection of myeloma cells under daratumumab therapy

Published

2022

17. Fluorescently tagged nanobodies and NanoBRET to study ligand-binding and agonist-induced conformational changes of full-length EGFR expressed in living cells

Author

Dehan Comez, Jacqueline Glenn, Stephanie M. Anbuhl, Raimond Heukers, Martine J. Smit, Stephen J. Hill, Laura E. Kilpatrick, Medicinal chemistry, and AIMMS

Subjects

Epidermal Growth Factor, EGFR, Immunology, Single-Domain Antibodies, Transforming Growth Factor alpha, Ligands, NanoBiT, ErbB Receptors, nanobody, HEK293 Cells, SDG 3 - Good Health and Well-being, Immunology and Allergy, Humans, BRET, fluorescence, Coloring Agents, Immunoglobulin Heavy Chains

Abstract

IntroductionThe Epidermal Growth Factor Receptor is a member of the Erb receptor tyrosine kinase family. It binds several ligands including EGF, betacellulin (BTC) and TGF-α, controls cellular proliferation and invasion and is overexpressed in various cancer types. Nanobodies (VHHs) are the antigen binding fragments of heavy chain only camelid antibodies. In this paper we used NanoBRET to compare the binding characteristics of fluorescent EGF or two distinct fluorescently labelled EGFR directed nanobodies (Q44c and Q86c) to full length EGFR.MethodsLiving HEK293T cells were stably transfected with N terminal NLuc tagged EGFR. NanoBRET saturation, displacement or kinetics experiments were then performed using fluorescently labelled EGF ligands (EGF-AF488 or EGF-AF647) or fluorescently labelled EGFR targeting nanobodies (Q44c-HL488 and Q86c-HL488).ResultsThese data revealed that the EGFR nanobody Q44c was able to inhibit EGF binding to full length EGFR, while Q86c was able to recognise agonist bound EGFR and act as a conformational sensor. The specific binding of fluorescent Q44c-HL488 and EGF-AF488 was inhibited by a range of EGFR ligands (EGF> BTC>TGF-α).DiscussionEGFR targeting nanobodies are powerful tools for studying the role of the EGFR in health and disease and allow real time quantification of ligand binding and distinct ligand induced conformational changes.

Published

2022

18. Programmable Attenuation of Antigenic Sensitivity for a Nanobody-Based EGFR Chimeric Antigen Receptor Through Hinge Domain Truncation

Author

McComb, Scott, Nguyen, Tina, Shepherd, Alex, Henry, Kevin A., Bloemberg, Darin, Marcil, Anne, Maclean, Susanne, Zafer, Ahmed, Gilbert, Rénald, Gadoury, Christine, Pon, Robert A., Sulea, Traian, Zhu, Qin, and Weeratna, Risini D.

Subjects

Receptors, Chimeric Antigen, Receptor, ErbB-2, T-Lymphocytes, EGFR, Immunology, Single-Domain Antibodies, Immunotherapy, Adoptive, cellular immunotherapy, CAR-T, ErbB Receptors, Epitopes, cancer selectivity, hinge domain, Humans, Immunology and Allergy, cell therapy, CAR optimization

Abstract

Epidermal growth factor family receptor (EGFR) is commonly overexpressed in many solid tumors and an attractive target for chimeric antigen receptor (CAR)-T therapy, but as EGFR is also expressed at lower levels in healthy tissues a therapeutic strategy must balance antigenic responsiveness against the risk of on-target off-tumor toxicity. Herein, we identify several camelid single-domain antibodies (also known as nanobodies) that are effective EGFR targeting moieties for CARs (EGFR-sdCARs) with very strong reactivity to EGFR-high and EGFR-low target cells. As a strategy to attenuate their potent antigenic sensitivity, we performed progressive truncation of the human CD8 hinge commonly used as a spacer domain in many CAR constructs. Single amino acid hinge-domain truncation progressively decreased both EGFR-sdCAR-Jurkat cell binding to EGFR-expressing targets and expression of the CD69 activation marker. Attenuated signaling in hinge-truncated EGFR-sdCAR constructs increased selectivity for antigen-dense EGFR-overexpressing cells over an EGFR-low tumor cell line or healthy donor derived EGFR-positive fibroblasts. We also provide evidence that epitope location is critical for determining hinge-domain requirement for CARs, as hinge truncation similarly decreased antigenic sensitivity of a membrane-proximal epitope targeting HER2-CAR but not a membrane-distal EGFRvIII-specific CAR. Hinge-modified EGFR-sdCAR cells showed clear functional attenuation in Jurkat-CAR-T cells and primary human CAR-T cells from multiple donors in vitro and in vivo. Overall, these results indicate that hinge length tuning provides a programmable strategy for throttling antigenic sensitivity in CARs targeting membrane-proximal epitopes, and could be employed for CAR-optimization and improved tumor selectivity.

Published

2022

19. Mucosal nanobody IgA as inhalable and affordable prophylactic and therapeutic treatment against SARS-CoV-2 and emerging variants

Author

Qi Li, Fiachra Humphries, Roxie C. Girardin, Aaron Wallace, Monir Ejemel, Alla Amcheslavsky, Conor T. McMahon, Zachary A. Schiller, Zepei Ma, John Cruz, Alan P. Dupuis, Anne F. Payne, Arooma Maryam, Nese Kurt Yilmaz, Kathleen A. McDonough, Brian G. Pierce, Celia A. Schiffer, Andrew C. Kruse, Mark S. Klempner, Lisa A. Cavacini, Katherine A. Fitzgerald, and Yang Wang

Subjects

SARS-CoV-2, Immunology, COVID-19, Single-Domain Antibodies, Antibodies, Viral, Immunoglobulin A, Epitopes, Mice, Immunoglobulin G, Spike Glycoprotein, Coronavirus, Immunology and Allergy, Animals, Humans, Angiotensin-Converting Enzyme 2

Abstract

Anti-COVID antibody therapeutics have been developed but not widely used due to their high cost and escape of neutralization from the emerging variants. Here, we describe the development of VHH-IgA1.1, a nanobody IgA fusion molecule as an inhalable, affordable and less invasive prophylactic and therapeutic treatment against SARS-CoV-2 Omicron variants. VHH-IgA1.1 recognizes a conserved epitope of SARS-CoV-2 spike protein Receptor Binding Domain (RBD) and potently neutralizes major global SARS-CoV-2 variants of concern (VOC) including the Omicron variant and its sub lineages BA.1.1, BA.2 and BA.2.12.1. VHH-IgA1.1 is also much more potent against Omicron variants as compared to an IgG Fc fusion construct, demonstrating the importance of IgA mediated mucosal protection for Omicron infection. Intranasal administration of VHH-IgA1.1 prior to or after challenge conferred significant protection from severe respiratory disease in K18-ACE2 transgenic mice infected with SARS-CoV-2 VOC. More importantly, for cost-effective production, VHH-IgA1.1 produced in Pichia pastoris had comparable potency to mammalian produced antibodies. Our study demonstrates that intranasal administration of affordably produced VHH-IgA fusion protein provides effective mucosal immunity against infection of SARS-CoV-2 including emerging variants.

Published

2022

20. Ciltacabtagene autoleucel: The second anti-BCMA CAR T-cell therapeutic armamentarium of relapsed or refractory multiple myeloma

Author

Endeshaw Chekol Abebe, Mestet Yibeltal Shiferaw, Fitalew Tadele Admasu, and Tadesse Asmamaw Dejenie

Subjects

Epitopes, Clinical Trials, Phase II as Topic, Receptors, Chimeric Antigen, Clinical Trials, Phase I as Topic, T-Lymphocytes, Immunology, Immunology and Allergy, Humans, B-Cell Maturation Antigen, Single-Domain Antibodies, Multiple Myeloma, Single-Chain Antibodies

Abstract

Ciltacabtagene autoleucel (also known as cilta-cel) is a chimeric antigen receptor (CAR) T-cell therapy that targets B-cell maturation antigen (BCMA) on the surface of cancer cells in B cell malignancies, such as multiple myeloma (MM). It is a second-generation CAR that is outfitted with an ectodomain comprising two BCMA-binding single chain variable fragment (ScFv) domains, a transmembrane domain, and an endodomain possessing CD3ζ and 4-1BB. Cilta-cel is an autologous, gene-edited CAR T-cell that is prepared by collecting and modifying the recipient’s T-cells to create a patient personalized treatment in the laboratory to be infused back. This CAR T-cell product exceptionally entails CARs with two BCMA-targeting single-domain antibodies that detect two epitopes of BCMA expressed on the malignant cells of MM. Cilta-cel is the current addition to the treatment armamentarium of relapsed or refractory (r/r) MM after its approval by the FDA on February 28, 2022, based on the results of the Phase 1b/2 CARTITUDE-1 study. It was the second approved anti-BCMA CAR T-cell product after idecabtagene vicleucel (ide-cel) to treat myeloma patients. It induces early, deep, and long-lasting responses with a tolerable safety profile in r/r MM. Cilta-cel-treated myeloma patients may potentially experience adverse effects ranging from mild to life-threatening, but they are mostly manageable toxicities. Besides, it has a consistent safety profile upon a longer follow-up of patients. Cilta-cel generally outperforms ide cel in terms of efficacy in MM, but shows comparable adverse events. This review highlights the current updates on cilta-cel efficacy, adverse events, comparison with ide-cel, and its future direction in the treatment of MM.

Published

2022

21. Neutralizing epitopes on

Author

Baohua, Chen, Kay, Perry, and Rongsheng, Jin

Subjects

Epitopes, Clostridioides difficile, Bacterial Toxins, Animals, Single-Domain Antibodies

Abstract

Toxin A (TcdA) and toxin B (TcdB) are two key virulence factors secreted by

Published

2022

22. Nucleocapsid Specific Diagnostics for the Detection of Divergent SARS-CoV-2 Variants

Author

Ariel Isaacs, Alberto A. Amarilla, Julio Aguado, Naphak Modhiran, Eduardo A. Albornoz, Alireza A. Baradar, Christopher L. D. McMillan, Jovin J. Y. Choo, Adi Idris, Aroon Supramaniam, Nigel A. J. McMillan, David A. Muller, Paul R. Young, Trent M. Woodruff, Ernst J. Wolvetang, Keith J. Chappell, and Daniel Watterson

Subjects

SARS-CoV-2, Immunology, Antibodies, Monoclonal, COVID-19, Humans, Immunology and Allergy, Nucleocapsid Proteins, Single-Domain Antibodies, Nucleocapsid, Antibodies, Neutralizing, Pandemics

Abstract

Since the start of the COVID-19 pandemic, multiple waves of SARS-CoV-2 variants have emerged. Of particular concern is the omicron variant, which harbors 28 mutations in the spike glycoprotein receptor binding and N-terminal domains relative to the ancestral strain. The high mutability of SARS-CoV-2 therefore poses significant hurdles for development of universal assays that rely on spike-specific immune detection. To address this, more conserved viral antigens need to be targeted. In this work, we comprehensively demonstrate the use of nucleocapsid (N)-specific detection across several assays using previously described nanobodies C2 and E2. We show that these nanobodies are highly sensitive and can detect divergent SARS-CoV-2 ancestral, delta and omicron variants across several assays. By comparison, spike-specific antibodies S309 and CR3022 only disparately detect SARS-CoV-2 variant targets. As such, we conclude that N-specific detection could provide a standardized universal target for detection of current and emerging SARS-CoV-2 variants of concern.

Published

2022

23. Anti-HIV-1 Nanobody-IgG1 Constructs With Improved Neutralization Potency and the Ability to Mediate Fc Effector Functions

Author

Schriek, Angela I, van Haaren, Marlies M, Poniman, Meliawati, Dekkers, Gillian, Bentlage, Arthur E H, Grobben, Marloes, Vidarsson, Gestur, Sanders, Rogier W, Verrips, Theo, Geijtenbeek, Teunis B H, Heukers, Raimond, Kootstra, Neeltje A, de Taeye, Steven W, van Gils, Marit J, Afd Biomol.Mass Spect. and Proteomics, Sub Cell Biology, Biomolecular Mass Spectrometry and Proteomics, Afd Biomol.Mass Spect. and Proteomics, Sub Cell Biology, Biomolecular Mass Spectrometry and Proteomics, Experimental Immunology, Graduate School, Medical Microbiology and Infection Prevention, AII - Infectious diseases, Infectious diseases, APH - Aging & Later Life, and Molecular cell biology and Immunology

Subjects

Fc fusion, Fc-mediated effector functions, Immunology, Single-Domain Antibodies, neutralization, HIV Antibodies, Antibodies, Neutralizing/pharmacology, Antibodies, Neutralizing, Antibodies, nanobodies, Immunoglobulin G, HIV Seropositivity, HIV-1, Humans, Immunology and Allergy, Neutralizing/pharmacology, Broadly Neutralizing Antibodies, Single-Domain Antibodies/pharmacology

Abstract

The most effective treatment for HIV-1, antiretroviral therapy, suppresses viral replication and averts the disease from progression. Nonetheless, there is a need for alternative treatments as it requires daily administration with the possibility of side effects and occurrence of drug resistance. Broadly neutralizing antibodies or nanobodies targeting the HIV-1 envelope glycoprotein are explored as alternative treatment, since they mediate viral suppression and contribute to the elimination of virus-infected cells. Besides neutralization potency and breadth, Fc-mediated effector functions of bNAbs also contribute to thein vivoefficacy. In this study multivalent J3, 2E7 and 1F10 anti-HIV-1 broadly neutralizing nanobodies were generated to improve neutralization potency and IgG1 Fc fusion was utilized to gain Fc-mediated effector functions. Bivalent and trivalent nanobodies, coupled using long glycine-serine linkers, showed increased binding to the HIV-1 Env and enhanced neutralization potency compared to the monovalent variant. Fusion of an IgG1 Fc domain to J3 improved neutralization potency compared to the J3-bihead and restored Fc-mediated effector functions such as antibody-dependent cellular phagocytosis and trogocytosis, and natural killer cell activation. Due to their neutralization breadth and potency and their ability to induce effector functions these nanobody-IgG1 constructs may prove to be valuable towards alternative HIV-1 therapies.

Published

2022

24. Antibody or Antibody Fragments: Implications for Molecular Imaging and Targeted Therapy of Solid Tumors.

Author

Xenaki, Katerina T., Oliveira, Sabrina, and van Bergen en Henegouwen, Paul M. P.

Subjects

CANCER immunotherapy, THERAPEUTIC use of immunoglobulins, TUMOR prevention

Abstract

The use of antibody-based therapeutics has proven very promising for clinical applications in cancer patients, with multiple examples of antibodies and antibody-drug conjugates successfully applied for the treatment of solid tumors and lymphomas. Given reported recurrence rates, improvements are clearly still necessary. A major factor limiting the efficacy of antibody-targeted cancer therapies may be the incomplete penetration of the antibody or antibody-drug conjugate into the tumor. Incomplete tumor penetration also affects the outcome of molecular imaging, when using such targeting agents. From the injection site until they arrive inside the tumor, targeting molecules are faced with several barriers that impact intratumoral distribution. The primary means of antibody transport inside tumors is based on diffusion. The diffusive penetration inside the tumor is influenced by both antibody properties, such as size and binding affinity, as well as tumor properties, such as microenvironment, vascularization, and targeted antigen availability. Engineering smaller antibody fragments has shown to improve the rate of tumor uptake and intratumoral distribution. However, it is often accompanied by more rapid clearance from the body and in several cases also by inherent destabilization and reduction of the binding affinity of the antibody. In this perspective, we discuss different cancer targeting approaches based on antibodies or their fragments. We carefully consider how their size and binding properties influence their intratumoral uptake and distribution, and how this may affect cancer imaging and therapy of solid tumors. [ABSTRACT FROM AUTHOR]

Published

2017

25. Intracellular Crosslinking of Filoviral Nucleoproteins with Xintrabodies Restricts Viral Packaging.

Author

Darling, Tamarand Lee, Sherwood, Laura Jo, and Hayhurst, Andrew

Subjects

IMMUNOGLOBULINS, EBOLA virus, MARBURG virus

Abstract

Viruses assemble large macromolecular repeat structures that become part of the infectious particles or virions. Ribonucleocapsids (RNCs) of negative strand RNA viruses are a prime example where repetition of nucleoprotein (NP) along the genome creates a core polymeric helical scaffold that accommodates other nucleocapsid proteins including viral polymerase. The RNCs are transported through the cytosol for packaging into virions through association with viral matrix proteins at cell membranes. We hypothesized that RNC would be ideal targets for crosslinkers engineered to promote aberrant protein--protein interactions, thereby blocking their orderly transport and packaging. Previously, we had generated single-domain antibodies (sdAbs) against Filoviruses that have all targeted highly conserved C-terminal regions of NP known to be repetitively exposed along the length of the RNCs of Marburgvirus (MARV) and Ebolavirus (EBOV). Our crosslinker design consisted of dimeric sdAb expressed intracellularly, which we call Xintrabodies (X-for crosslinking). Electron microscopy of purified NP polymers incubated with purified sdAb constructs showed NP aggregation occurred in a genus-specific manner with dimeric and not monomeric sdAb. A virus-like particle (VLP) assay was used for initial evaluation where we found that dimeric sdAb inhibited NP incorporation into VP40-based VLPs whereas monomeric sdAb did not. Inhibition of NP packaging was genus specific. Confocal microscopy revealed dimeric sdAb was diffuse when expressed alone but focused on pools of NP when the two were coexpressed, while monomeric sdAb showed ambivalent partition. Infection of stable Vero cell lines expressing dimeric sdAb specific for either MARV or EBOV NP resulted in smaller plaques and reduced progeny of cognate virus relative to wild-type Vero cells. Though the impact was marginal at later time-points, the collective data suggest that viral replication can be reduced by crosslinking intracellular NP using relatively small amounts of dimeric sdAb to restrict NP packaging. The stoichiometry and ease of application of the approach would likely benefit from transitioning away from intracellular expression of crosslinking sdAb to exogenous delivery of antibody. By retuning sdAb specificity, the approach of crosslinking highly conserved regions of assembly critical proteins may well be applicable to inhibiting replication processes of a broad spectrum of viruses. [ABSTRACT FROM AUTHOR]

Published

2017

26. Quantitative flow cytometric selection of tau conformational nanobodies specific for pathological aggregates.

Author

Zupancic JM, Smith MD, Trzeciakiewicz H, Skinner ME, Ferris SP, Makowski EK, Lucas MJ, McArthur N, Kane RS, Paulson HL, and Tessier PM

Subjects

Humans, Animals, Mice, tau Proteins, Amyloidogenic Proteins, Mice, Transgenic, Single-Domain Antibodies, Alzheimer Disease

Abstract

Single-domain antibodies, also known as nanobodies, are broadly important for studying the structure and conformational states of several classes of proteins, including membrane proteins, enzymes, and amyloidogenic proteins. Conformational nanobodies specific for aggregated conformations of amyloidogenic proteins are particularly needed to better target and study aggregates associated with a growing class of associated diseases, especially neurodegenerative disorders such as Alzheimer's and Parkinson's diseases. However, there are few reported nanobodies with both conformational and sequence specificity for amyloid aggregates, especially for large and complex proteins such as the tau protein associated with Alzheimer's disease, due to difficulties in selecting nanobodies that bind to complex aggregated proteins. Here, we report the selection of conformational nanobodies that selectively recognize aggregated (fibrillar) tau relative to soluble (monomeric) tau. Notably, we demonstrate that these nanobodies can be directly isolated from immune libraries using quantitative flow cytometric sorting of yeast-displayed libraries against tau aggregates conjugated to quantum dots, and this process eliminates the need for secondary nanobody screening. The isolated nanobodies demonstrate conformational specificity for tau aggregates in brain samples from both a transgenic mouse model and human tauopathies. We expect that our facile approach will be broadly useful for isolating conformational nanobodies against diverse amyloid aggregates and other complex antigens., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Zupancic, Smith, Trzeciakiewicz, Skinner, Ferris, Makowski, Lucas, McArthur, Kane, Paulson and Tessier.)

Published

2023

27. A comparison of the binding sites of antibodies and single-domain antibodies.

Author

Gordon GL, Capel HL, Guloglu B, Richardson E, Stafford RL, and Deane CM

Subjects

Antibodies, Binding Sites, Epitopes, Antigens, Single-Domain Antibodies

Abstract

Antibodies are the largest class of biotherapeutics. However, in recent years, single-domain antibodies have gained traction due to their smaller size and comparable binding affinity. Antibodies (Abs) and single-domain antibodies (sdAbs) differ in the structures of their binding sites: most significantly, single-domain antibodies lack a light chain and so have just three CDR loops. Given this inherent structural difference, it is important to understand whether Abs and sdAbs are distinguishable in how they engage a binding partner and thus, whether they are suited to different types of epitopes. In this study, we use non-redundant sequence and structural datasets to compare the paratopes, epitopes and antigen interactions of Abs and sdAbs. We demonstrate that even though sdAbs have smaller paratopes, they target epitopes of equal size to those targeted by Abs. To achieve this, the paratopes of sdAbs contribute more interactions per residue than the paratopes of Abs. Additionally, we find that conserved framework residues are of increased importance in the paratopes of sdAbs, suggesting that they include non-specific interactions to achieve comparable affinity. Furthermore, the epitopes of sdAbs are only marginally less accessible than those of Abs: we posit that this may be explained by differences in the orientation and compaction of sdAb and Ab CDR-H3 loops. Overall, our results have important implications for the engineering and humanization of sdAbs, as well as the selection of the best modality for targeting a particular epitope., Competing Interests: Author RS was employed by company Twist Bioscience. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Gordon, Capel, Guloglu, Richardson, Stafford and Deane.)

Published

2023

28. Identification and characterisation of anti-IL-13 inhibitory single domain antibodies provides new insights into receptor selectivity and attractive opportunities for drug discovery.

Author

Walker K, Baravalle R, Holyfield R, Kalms J, Wright H, Seewooruthun C, Muskett FW, Scott-Tucker A, Merritt A, Henry A, Lawson ADG, Hall G, Prosser C, and Carr MD

Subjects

Interleukin-4 metabolism, Interleukin-13 Receptor alpha1 Subunit metabolism, Cytokines, Interleukin-13 metabolism, Single-Domain Antibodies

Abstract

Interleukin-13 (IL-13) is a cytokine involved in T-cell immune responses and is a well validated therapeutic target for the treatment of asthma, along with other allergic and inflammatory diseases. IL-13 signals through a ternary signalling complex formed with the receptors IL-13Rα1 and IL-4Rα. This complex is assembled by IL-13 initially binding IL-13Rα1, followed by association of the binary IL-13:IL-13Rα1 complex with IL-4Rα. The receptors are shared with IL-4, but IL-4 initially binds IL-4Rα. Here we report the identification and characterisation of a diverse panel of single-domain antibodies (VHHs) that bind to IL-13 (K D 40 nM-5.5 μM) and inhibit downstream IL-13 signalling (IC 50 0.2-53.8 μM). NMR mapping showed that the VHHs recognise a number of epitopes on IL-13, including previously unknown allosteric sites. Further NMR investigation of VHH204 bound to IL-13 revealed a novel allosteric mechanism of inhibition, with the antibody stabilising IL-13 in a conformation incompatible with receptor binding. This also led to the identification of a conformational equilibrium for free IL-13, providing insights into differing receptor signalling complex assembly seen for IL-13 compared to IL-4, with formation of the IL-13:IL-13Rα1 complex required to stabilise IL-13 in a conformation with high affinity for IL-4Rα. These findings highlight new opportunities for therapeutic targeting of IL-13 and we report a successful 19 F fragment screen of the IL-13:VHH204 complex, including binding sites identified for several hits. To our knowledge, these 19 F containing fragments represent the first small-molecules shown to bind to IL-13 and could provide starting points for a small-molecule drug discovery programme., Competing Interests: Authors JK, AS-T, AH, AL and CP are employees of UCB. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest. The author's declare that this study received funding from the Antibody-Assisted Drug Discovery Consortium, which is a research partnership between the University of Leicester, LifeArc and UCB Biopharma. The funder was involved in the study design, collection, analysis, interpretation of data, the writing of this article, as well as the decision to submit it for publication., (Copyright © 2023 Walker, Baravalle, Holyfield, Kalms, Wright, Seewooruthun, Muskett, Scott-Tucker, Merritt, Henry, Lawson, Hall, Prosser and Carr.)

Published

2023

29. Neutralizing Dromedary-Derived Nanobodies Against BotI-Like Toxin From the Most Hazardous Scorpion Venom in the Middle East and North Africa Region

Author

Rahma Ben Abderrazek, Ayoub Ksouri, Faten Idoudi, Sayda Dhaouadi, Emna Hamdi, Cécile Vincke, Azer Farah, Zakaria Benlasfar, Hafedh Majdoub, Mohamed El Ayeb, Serge Muyldermans, Balkiss Bouhaouala-Zahar, and Cellular and Molecular Immunology

Subjects

Scorpions, Mice, Camelus, Scorpion Stings, Immunology, Immunology and Allergy, Animals, Scorpion Venoms, Scorpion Stings/therapy, Single-Domain Antibodies/therapeutic use, Single-Domain Antibodies, complex mixtures

Abstract

Scorpion envenoming is a severe health problem in many regions causing significant clinical toxic effects and fatalities. In the Middle East/North Africa (MENA) region, Buthidae scorpion stings are responsible for devastating toxic outcomes in human. The only available specific immunotherapeutic treatment is based on IgG fragments of animal origin. To overcome the limitations of classical immunotherapy, we have demonstrated the in vivo efficacy of NbF12-10 bispecific nanobody at preclinical level. Nanobodies were developed against BotI analogues belonging to a distinct structural and antigenic group of scorpion toxins, occurring in the MENA region. From Buthus occitanus tunetanus venom, BotI-like toxin was purified. The 41 N-terminal amino acid residues were sequenced, and the LD50 was estimated at 40 ng/mouse. The BotI-like toxin was used for dromedary immunization. An immune VHH library was constructed, and after screening, two nanobodies were selected with nanomolar and sub-nanomolar affinity and recognizing an overlapping epitope. NbBotI-01 was able to neutralize 50% of the lethal effect of 13 LD50 BotI-like toxins in mice when injected by i.c.v route, whereas NbBotI-17 neutralized 50% of the lethal effect of 7 LD50. Interestingly, NbBotI-01 completely reduced the lethal effect of the 2 LD50 of BotG50 when injected at 1:4 molar ratio excess. More interestingly, an equimolar mixture of NbBotI-01 with NbF12-10 neutralized completely the lethal effect of 7 and 5 LD50 of BotG50 or AahG50, at 1:4 and 1:2 molar ratio, respectively. Hence, NbBotI-01 and NbF12-10 display synergic effects, leading to a novel therapeutic candidate for treating Buthus occitanus scorpion stings in the MENA region.

Published

2022

30. Generation of a High-Affinity Nanobody Against CD147 for Tumor Targeting and Therapeutic Efficacy Through Conjugating Doxorubicin

Author

Li, Rifei, Zhu, Xinjie, Zhou, Peng, Qiao, Yuehua, Li, Yinqian, Xu, Yice, and Shi, Xi

Subjects

Mice, Doxorubicin, Neoplasms, Immunology, Immunology and Allergy, Animals, Mice, Nude, Single-Domain Antibodies, Xenograft Model Antitumor Assays

Abstract

CD147, a glycosylated transmembrane protein in the immunoglobulin superfamily, is overexpressed on the surfaces of various tumor cells and promotes cancer cell proliferation, invasion, and metastasis. Nanobodies, characterized by small sizes, high affinities and specificities, and low immunogenicities, are promising diagnostic and therapeutic tools. However, there are few reports on nanobodies that specifically target CD147. In this work, a specific anti-CD147 nanobody has been successfully identified using phage display technology. The tumor target and antitumor effects have also been detected in different CD147-positive tumors in in vitro and in vivo assays, respectively. Meanwhile, it has a synergistic effect for inhibiting 4T1-bearing mice through conjugating doxorubicin. It may afford new strategies for cancer therapies.

Published

2022

31. Discovery of Anti-PD-L1 Human Domain Antibodies for Cancer Immunotherapy

Author

Hao Liu, Yanli Liu, Zhen Zhao, Yuanke Li, Bahaa Mustafa, Zhijin Chen, Ashutosh Barve, Akshay Jain, Xiaolan Yao, Guangfu Li, and Kun Cheng

Subjects

Mice, Antineoplastic Agents, Immunological, Immunology, Colonic Neoplasms, Programmed Cell Death 1 Receptor, Immunology and Allergy, Animals, Antibodies, Monoclonal, Humans, Immunotherapy, Single-Domain Antibodies, B7-H1 Antigen

Abstract

Immunotherapy using monoclonal antibodies targeting the PD-1/PD-L1 interaction has shown enormous success for various cancers. Despite their encouraging results in clinics, antibody-based checkpoint inhibitors have several limitations, such as poor tumor penetration. To address these limitations of monoclonal antibodies, there is a growing interest in developing low-molecular-weight checkpoint inhibitors, such as antibody fragments. Several antibody fragments targeting PD-1/PD-L1 were recently discovered using phage libraries from camel or alpaca. However, animal-derived antibody fragments may elicit unwanted immune responses, which limit their therapeutic applications. For the first time, we used a human domain antibody phage library and discovered anti-human PD-L1 human single-domain antibodies (dAbs) that block the PD-1/PD-L1 interaction. Among them, the CLV3 dAb shows the highest affinity to PD-L1. The CLV3 dAb also exhibits the highest blocking efficacy of the PD-1/PD-L1 interaction. Moreover, the CLV3 dAb significantly inhibits tumor growth in mice implanted with CT26 colon carcinoma cells. These results suggest that CLV3 dAb can be potentially used as an anti-PD-L1 inhibitor for cancer immunotherapy.

Published

2021

32. Half-Life Extended Nanobody-Based CD38-Specific Bispecific Killercell Engagers Induce Killing of Multiple Myeloma Cells

Author

Julia Hambach, William Fumey, Tobias Stähler, Anna Josephine Gebhardt, Gerhard Adam, Katja Weisel, Friedrich Koch-Nolte, and Peter Bannas

Subjects

Albumins, Cell Line, Tumor, Immunology, Immunology and Allergy, Humans, Single-Domain Antibodies, Multiple Myeloma, ADP-ribosyl Cyclase 1, Half-Life

Abstract

CD38 is a target for immunotherapy of multiple myeloma. Llama-derived CD38-specific nanobodies allow easy reformatting into mono-, bi- and multispecific proteins. To evaluate the utility of nanobodies for constructing CD38-specific nanobody-based killer cell engagers (nano-BiKEs), we generated half-life extended nano-BiKEs (HLE-nano-BiKEs) by fusing a CD38-specific nanobody to a CD16-specific nanobody for binding to the Fc-receptor on NK cells and further to an albumin-specific nanobody to extend the half-life in vivo. HLE-nano-BiKEs targeting three different epitopes (E1, E2, E3) of CD38 were expressed in transiently transfected HEK-6E cells. We verified specific and simultaneous binding to CD38 on myeloma cells, CD16 on NK cells, and to albumin. We tested the capacity of these HLE-nano-BiKEs to mediate cytotoxicity against CD38-expressing multiple myeloma cell lines and primary myeloma cells from human bone marrow biopsies in bioluminescence and flowcytometry assays with NK92 cells as effector cells. The results revealed specific time- and dose-dependent cytolysis of CD38+ myeloma cell lines and effective depletion of CD38-expressing multiple myeloma cells from primary human bone marrow samples. Our results demonstrate the efficacy of CD38-specific HLE-nano-BiKEs in vitro and ex vivo, warranting further preclinical evaluation in vivo of their therapeutic potential for the treatment of multiple myeloma.

Published

2021

33. Single-Domain Antibodies for Targeting, Detection, and In Vivo Imaging of Human CD4+ Cells

Author

Traenkle, Bjoern, Kaiser, Philipp D., Pezzana, Stefania, Richardson, Jennifer, Gramlich, Marius, Wagner, Teresa R., Seyfried, Dominik, Weldle, Melissa, Holz, Stefanie, Parfyonova, Yana, Nueske, Stefan, Scholz, Armin M., Zeck, Anne, Jakobi, Meike, Schneiderhan-Marra, Nicole, Schaller, Martin, Maurer, Andreas, Gouttefangeas, Cécile, Kneilling, Manfred, Pichler, Bernd J., Sonanini, Dominik, and Rothbauer, Ulrich

Subjects

CD4-Positive T-Lymphocytes, Immunology, Optical Imaging, PET imaging, immunotherapies, Single-Domain Antibodies, CD4, Molecular Imaging, nanobody, Mice, magnetic resonance imaging, Animals, Heterografts, Humans, immune tracer, Original Research

Abstract

The advancement of new immunotherapies necessitates appropriate probes to monitor the presence and distribution of distinct immune cell populations. Considering the key role of CD4+ cells in regulating immunological processes, we generated novel single-domain antibodies [nanobodies (Nbs)] that specifically recognize human CD4. After in-depth analysis of their binding properties, recognized epitopes, and effects on T-cell proliferation, activation, and cytokine release, we selected CD4-specific Nbs that did not interfere with crucial T-cell processes in vitro and converted them into immune tracers for noninvasive molecular imaging. By optical imaging, we demonstrated the ability of a high-affinity CD4-Nb to specifically visualize CD4+ cells in vivo using a xenograft model. Furthermore, quantitative high-resolution immune positron emission tomography (immunoPET)/MR of a human CD4 knock-in mouse model showed rapid accumulation of 64Cu-radiolabeled CD4-Nb1 in CD4+ T cell-rich tissues. We propose that the CD4-Nbs presented here could serve as versatile probes for stratifying patients and monitoring individual immune responses during personalized immunotherapy in both cancer and inflammatory diseases.

Published

2021

34. Imaging of Glioblastoma Tumor-Associated Myeloid Cells Using Nanobodies Targeting Signal Regulatory Protein Alpha

Author

Karen De Vlaminck, Ema Romão, Janik Puttemans, Ana Rita Pombo Antunes, Daliya Kancheva, Isabelle Scheyltjens, Jo A. Van Ginderachter, Serge Muyldermans, Nick Devoogdt, Kiavash Movahedi, Geert Raes, Laboratory of Molecullar and Cellular Therapy, Cellular and Molecular Immunology, Faculty of Sciences and Bioengineering Sciences, Clinical sciences, Supporting clinical sciences, Medical Imaging, Faculty of Medicine and Pharmacy, Department of Bio-engineering Sciences, Vriendenkring VUB, and Basic (bio-) Medical Sciences

Subjects

Stromal cell, Antibodies, Neoplasm, Immunology, Brain tumor, Gene Expression, Spleen, CD47 Antigen, Enzyme-Linked Immunosorbent Assay, Host Specificity, Mice, Immunology and Microbiology(all), Cell Line, Tumor, medicine, Signal-regulatory protein alpha, Biomarkers, Tumor, Immunology and Allergy, Animals, Humans, myeloid cell, Myeloid Cells, Receptors, Immunologic, Receptor, SIRP alpha, Original Research, biology, Microglia, Chemistry, Brain Neoplasms, CD47, glioblastoma, imaging, RC581-607, Single-Domain Antibodies, medicine.disease, Flow Cytometry, Antigens, Differentiation, Immunohistochemistry, Molecular Imaging, Disease Models, Animal, medicine.anatomical_structure, nanobodies (VHH), Radiology Nuclear Medicine and imaging, signal regulatory protein alpha, oncology, Cancer research, biology.protein, Immunologic diseases. Allergy, Antibody

Abstract

Glioblastoma (GBM) is the most common malignant primary brain tumor. Glioblastomas contain a large non-cancerous stromal compartment including various populations of tumor-associated macrophages and other myeloid cells, of which the presence was documented to correlate with malignancy and reduced survival. Via single-cell RNA sequencing of human GBM samples, only very low expression of PD-1, PD-L1 or PD-L2 could be detected, whereas the tumor micro-environment featured a marked expression of signal regulatory protein alpha (SIRPα), an inhibitory receptor present on myeloid cells, as well as its widely distributed counter-receptor CD47. CITE-Seq revealed that both SIRPα RNA and protein are prominently expressed on various populations of myeloid cells in GBM tumors, including both microglia- and monocyte-derived tumor-associated macrophages (TAMs). Similar findings were obtained in the mouse orthotopic GL261 GBM model, indicating that SIRPα is a potential target on GBM TAMs in mouse and human. A set of nanobodies, single-domain antibody fragments derived from camelid heavy chain-only antibodies, was generated against recombinant SIRPα and characterized in terms of affinity for the recombinant antigen and binding specificity on cells. Three selected nanobodies binding to mouse SIRPα were radiolabeled with 99mTc, injected in GL261 tumor-bearing mice and their biodistribution was evaluated using SPECT/CT imaging and radioactivity detection in dissected organs. Among these, Nb15 showed clear accumulation in peripheral organs such as spleen and liver, as well as a clear tumor uptake in comparison to a control non-targeting nanobody. A bivalent construct of Nb15 exhibited an increased accumulation in highly vascularized organs that express the target, such as spleen and liver, as compared to the monovalent format. However, penetration into the GL261 brain tumor fell back to levels detected with a non-targeting control nanobody. These results highlight the tumor penetration advantages of the small monovalent nanobody format and provide a qualitative proof-of-concept for using SIRPα-targeting nanobodies to noninvasively image myeloid cells in intracranial GBM tumors with high signal-to-noise ratios, even without blood-brain barrier permeabilization.

Published

2021

35. Editorial: Nanobody-based cancer immunotherapy and immunoimaging.

Author

Jafari M, Maali A, Shokrgozar MA, and Sharifzadeh Z

Subjects

Humans, Antibodies, Monoclonal, Immunotherapy, Single-Domain Antibodies, Neoplasms therapy

Abstract

Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Published

2023

36. Engineering an Antibody V Gene-Selective Vaccine

Author

David S. Peabody, Alemu Tekewe Mogus, Daniel K. Rohrer, Daniel Lingwood, Larance Ronsard, Bryce Chackerian, Ralston M. Barnes, Nils Lonberg, Ashraf S. Yousif, Vintus Okonkwo, Julianne Peabody, and Pascal Devant

Subjects

Male, Immunology, B-cell receptor, Receptors, Antigen, B-Cell, Mice, Transgenic, RNA Phages, Complementarity determining region, Ligands, Protein Engineering, Proof of Concept Study, Virus, Antibody Repertoire, Antigen, Antibody Specificity, antibody, VLP, Animals, Humans, Immunology and Allergy, Vaccines, Virus-Like Particle, prime, Gene, Gene Library, Original Research, B-Lymphocytes, B cell receptor, biology, Vaccination, breakpoint cluster region, Single-Domain Antibodies, RC581-607, Adoptive Transfer, Virology, biology.protein, Female, Immunologic diseases. Allergy, Antibody, lineage

Abstract

The ligand-binding surface of the B cell receptor (BCR) is formed by encoded and non-encoded antigen complementarity determining regions (CDRs). Genetically reproducible or ‘public’ antibodies can arise when the encoded CDRs play deterministic roles in antigen recognition, notably within human broadly neutralizing antibodies against HIV and influenza virus. We sought to exploit this by engineering virus-like-particle (VLP) vaccines that harbor multivalent affinity against gene-encoded moieties of the BCR antigen binding site. As proof of concept, we deployed a library of RNA bacteriophage VLPs displaying random peptides to identify a multivalent antigen that selectively triggered germline BCRs using the human VH gene IGVH1-2*02. This VLP selectively primed IGHV1-2*02 BCRs that were present within a highly diversified germline antibody repertoire within humanized mice. Our approach thus provides methodology to generate antigens that engage specific BCR configurations of interest, in the absence of structure-based information.

Published

2021

37. Prospects of Neutralizing Nanobodies Against SARS-CoV-2

Author

Zhihong Liu, Fangfang Chen, and Fan Jiang

Subjects

0301 basic medicine, 2019-20 coronavirus outbreak, Coronavirus disease 2019 (COVID-19), Mini Review, viruses, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, Antibody Affinity, Antibodies, Viral, Virus, Epitopes, 03 medical and health sciences, 0302 clinical medicine, Neutralization Tests, Peptide Library, Animals, Humans, Immunology and Allergy, Medicine, skin and connective tissue diseases, Patient compliance, receptor binding domain, Binding Sites, SARS-CoV-2, business.industry, fungi, COVID-19, food and beverages, RC581-607, Single-Domain Antibodies, Fast onset, Antibodies, Neutralizing, Virology, neutralizing, nanobodies (VHH), 030104 developmental biology, Drug concentration, Immunization, Immunologic diseases. Allergy, phage display, business, 030217 neurology & neurosurgery, Protein Binding

Abstract

Since December 2019, the SARS-CoV-2 has erupted on a large scale worldwide and spread rapidly. Passive immunization of antibody-related molecules provides opportunities for prevention and treatment of high-risk patients and children. Nanobodies (Nbs) have many strong physical and chemical properties. They can be atomized, administered by inhalation, and can be directly applied to the infected site, with fast onset, high local drug concentration/high bioavailability, and high patient compliance (no needles). It has very attractive potential in the treatment of respiratory viruses. Rapid and low-cost development of Nbs targeting SARS-CoV-2 can quickly be achieved. Nbs against SARS-CoV-2 mutant strains also can be utilized quickly to prevent the virus from escaping. It provides important technical supports for the treatment of the SARS-CoV-2 and has the potential to become an essential medicine in the toolbox against the SARS-CoV-2.

Published

2021

38. A novel shark single-domain antibody targeting OGT as a tool for detection and intracellular localization.

Author

Xi X, Xiao G, An G, Liu L, Liu X, Hao P, Wang JY, Song D, Yu W, and Gu Y

Subjects

Antibodies, Acetylglucosaminidase, Amino Acids, Single-Domain Antibodies

Abstract

Introduction: O-GlcNAcylation is a type of reversible post-translational modification on Ser/Thr residues of intracellular proteins in eukaryotic cells, which is generated by the sole O-GlcNAc transferase (OGT) and removed by O-GlcNAcase (OGA). Thousands of proteins, that are involved in various physiological and pathological processes, have been found to be O-GlcNAcylated. However, due to the lack of favorable tools, studies of the O-GlcNAcylation and OGT were impeded. Immunoglobulin new antigen receptor (IgNAR) derived from shark is attractive to research tools, diagnosis and therapeutics. The variable domain of IgNARs (VNARs) have several advantages, such as small size, good stability, low-cost manufacture, and peculiar paratope structure., Methods: We obtained shark single domain antibodies targeting OGT by shark immunization, phage display library construction and panning. ELISA and BIACORE were used to assess the affinity of the antibodies to the antigen and three shark single-domain antibodies with high affinity were successfully screened. The three antibodies were assessed for intracellular function by flow cytometry and immunofluorescence co-localization., Results: In this study, three anti-OGT VNARs (2D9, 3F7 and 4G2) were obtained by phage display panning. The affinity values were measured using surface plasmon resonance (SPR) that 2D9, 3F7 and 4G2 bound to OGT with KD values of 35.5 nM, 53.4 nM and 89.7 nM, respectively. Then, the VNARs were biotinylated and used for the detection and localization of OGT by ELISA, flow cytometry and immunofluorescence. 2D9, 3F7 and 4G2 were exhibited the EC50 values of 102.1 nM, 40.75 nM and 120.7 nM respectively. VNAR 3F7 was predicted to bind the amino acid residues of Ser375, Phe377, Cys379 and Tyr 380 on OGT., Discussion: Our results show that shark single-domain antibodies targeting OGT can be used for in vitro detection and intracellular co-localization of OGT, providing a powerful tool for the study of OGT and O-GlcNAcylation., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Xi, Xiao, An, Liu, Liu, Hao, Wang, Song, Yu and Gu.)

Published

2023

39. Novel Human Tenascin-C Function-Blocking Camel Single Domain Nanobodies

Author

Sayda Dhaouadi, Rahma Ben Abderrazek, Thomas Loustau, Chérine Abou-Faycal, Ayoub Ksouri, William Erne, Devadarssen Murdamoothoo, Matthias Mörgelin, Andreas Kungl, Alain Jung, Sonia Ledrappier, Zakaria Benlasfar, Sandrine Bichet, Ruth Chiquet-Ehrismann, Ismaïl Hendaoui, Gertraud Orend, and Balkiss Bouhaouala-Zahar

Subjects

0301 basic medicine, Extracellular matrix, 0302 clinical medicine, Antibody Specificity, tumor biomarker, Immunology and Allergy, Original Research, biology, medicine.diagnostic_test, Chemistry, Tenascin C, Liver Neoplasms, Tenascin, musculoskeletal system, Immunohistochemistry, Cell biology, 030220 oncology & carcinogenesis, diagnostic tool, fibronectin type III repeat, Protein Binding, lcsh:Immunologic diseases. Allergy, Camelus, Colon, extracellular matrix, Immunology, CD11c, Enzyme-Linked Immunosorbent Assay, 03 medical and health sciences, Western blot, Cell Line, Tumor, medicine, Cell Adhesion, Animals, Humans, tenascin-c, therapeutic tool, Cell adhesion, Tumor microenvironment, Single-Domain Antibodies, Antibodies, Neutralizing, Fibronectin, nanobody, 030104 developmental biology, HEK293 Cells, Tumor progression, biology.protein, Colitis, Ulcerative, Binding Sites, Antibody, interaction modeling, lcsh:RC581-607

Abstract

The extracellular matrix (ECM) molecule Tenascin-C (TNC) is well-known to promote tumor progression by multiple mechanisms. However, reliable TNC detection in tissues of tumor banks remains limited. Therefore, we generated dromedary single-domain nanobodies Nb3 and Nb4 highly specific for human TNC (hTNC) and characterized the interaction with TNC by several approaches including ELISA, western blot, isothermal fluorescence titration and negative electron microscopic imaging. Our results revealed binding of both nanobodies to distinct sequences within fibronectin type III repeats of hTNC. By immunofluroescence and immunohistochemical imaging we observed that both nanobodies detected TNC expression in PFA and paraffin embedded human tissue from ulcerative colitis, solid tumors and liver metastasis. As TNC impairs cell adhesion to fibronectin we determined whether the nanobodies abolished this TNC function. Indeed, Nb3 and Nb4 restored adhesion of tumor and mesangial cells on a fibronectin/TNC substratum. We recently showed that TNC orchestrates the immune-suppressive tumor microenvironment involving chemoretention, causing tethering of CD11c+ myeloid/dendritic cells in the stroma. Here, we document that immobilization of DC2.4 dendritic cells by a CCL21 adsorbed TNC substratum was blocked by both nanobodies. Altogether, our novel TNC specific nanobodies could offer valuable tools for detection of TNC in the clinical practice and may be useful to inhibit the immune-suppressive and other functions of TNC in cancer and other diseases.

Published

2021

40. Nanobodies—Useful Tools for Allergy Treatment?

Author

Sergei Tillib, Ines Zettl, and Sabine Flicker

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, 2019-20 coronavirus outbreak, Mini Review, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, Type i allergy, VHH, Computational biology, Passive Treatment, Epitope, Epitopes, 03 medical and health sciences, Broad spectrum, 0302 clinical medicine, allergy treatment, Hypersensitivity, Humans, Immunology and Allergy, Medicine, Antigens, Antibodies, Blocking, business.industry, Immunogenicity, blocking antibody, Immunoglobulin E, Single-Domain Antibodies, allergy, nanobody, 030104 developmental biology, Immunotherapy, Immune reaction, business, lcsh:RC581-607, 030215 immunology, allergen

Abstract

In the last decade single domain antibodies (nanobodies, VHH) qualified through their unique characteristics have emerged as accepted and even advantageous alternative to conventional antibodies and have shown great potential as diagnostic and therapeutic tools. Currently nanobodies find their main medical application area in the fields of oncology and neurodegenerative diseases. According to late-breaking information, nanobodies specific for coronavirus spikes have been generated these days to test their suitability as useful therapeutics for future outbreaks. Their superior properties such as chemical stability, high affinity to a broad spectrum of epitopes, low immunogenicity, ease of their generation, selection and production proved nanobodies also to be remarkable to investigate their efficacy for passive treatment of type I allergy, an exaggerated immune reaction to foreign antigens with increasing global prevalence.

Published

2020

41. Nanobodies: Prospects of Expanding the Gamut of Neutralizing Antibodies Against the Novel Coronavirus, SARS-CoV-2

Author

Rocktotpal Konwarh

Subjects

lcsh:Immunologic diseases. Allergy, Opinion, 2019-20 coronavirus outbreak, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Pneumonia, Viral, Immunology, Cross Reactions, Peptidyl-Dipeptidase A, Antibodies, Viral, spike protein, Pichia, Betacoronavirus, Epitopes, Animals, Coronavirus Nucleocapsid Proteins, Humans, Immunology and Allergy, Neutralizing antibody, Pandemics, biology, SARS-CoV-2, Vaccination, Antibodies, Monoclonal, COVID-19, neutralizing antibody, Spike Protein, Viral Vaccines, Nucleocapsid Proteins, Single-Domain Antibodies, Phosphoproteins, biology.organism_classification, Antibodies, Neutralizing, Virology, nanobodies, Spike Glycoprotein, Coronavirus, biology.protein, Angiotensin-Converting Enzyme 2, Severe acute respiratory syndrome coronavirus, Antibody, Coronavirus Infections, lcsh:RC581-607, Camelids, New World

Published

2020

42. Protection From Influenza by Intramuscular Gene Vector Delivery of a Broadly Neutralizing Nanobody Does Not Depend on Antibody Dependent Cellular Cytotoxicity

Author

Joanne Marie M. Del Rosario, Matthew Smith, Kam Zaki, Paul Risley, Nigel Temperton, Othmar G. Engelhardt, Mary Collins, Yasuhiro Takeuchi, and Simon E. Hufton

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, medicine.drug_class, Immunology, Genetic Vectors, Hemagglutinin (influenza), Cross Reactions, Monoclonal antibody, medicine.disease_cause, Antibodies, Viral, Injections, Intramuscular, Epitope, Neutralization, Adenoviridae, 03 medical and health sciences, 0302 clinical medicine, Orthomyxoviridae Infections, vaccine, Influenza, Human, medicine, Immunology and Allergy, Animals, Humans, Original Research, Antibody-dependent cell-mediated cytotoxicity, QR355, biology, antibody dependent cellular cytotoxicity, adeno associated viral vectors, Antibody-Dependent Cell Cytotoxicity, virus diseases, immunoprophylaxis, Single-Domain Antibodies, Virology, Antibodies, Neutralizing, Influenza A virus subtype H5N1, nanobody, 030104 developmental biology, Single-domain antibody, monoclonal antibody, Influenza A virus, biology.protein, Immunotherapy, Antibody, lcsh:RC581-607, influenza, Camelids, New World, 030215 immunology

Abstract

Cross-subtype neutralizing single domain antibodies against influenza present new opportunities for immunoprophylaxis and pandemic preparedness. Their simple modular structure and single open reading frame format are highly amenable to gene therapy-mediated delivery. We have previously described R1a-B6, an alpaca-derived single domain antibody (nanobody), that is capable of potent cross-subtype neutralization in vitro of H1N1, H5N1, H2N2, and H9N2 influenza viruses, through binding to a highly conserved epitope in the influenza hemagglutinin stem region. To evaluate the potential of R1a-B6 for immunoprophylaxis, we have reformatted it as an Fc fusion for adeno-associated viral (AAV) vector delivery. Our findings demonstrate that a single intramuscular injection in mice of AAV encoding R1a-B6 fused to Fc fragments of different isotypes equipped either, with or without antibody dependent cellular cytotoxicity (ADCC) activity, was able to drive sustained high-level expression (0.5–1.1 mg/mL) in sera with no evidence of reduction for up to 6 months. R1a-B6-Fc fusions of both isotypes gave complete protection against lethal challenge with both pandemic A/California/07/2009 (H1N1)pdm09 and avian influenza A/Vietnam/1194/2004 (H5N1). This data suggests that R1a-B6 is capable of cross-subtype protection and ADCC was not essential for R1a-B6 efficacy. Our findings demonstrate AAV delivery of cross-subtype neutralizing nanobodies may be an effective strategy to prevent influenza infection and provide long-term protection independent of a host induced immune response.

Published

2020

43. Fluorescently tagged nanobodies and NanoBRET to study ligand-binding and agonist-induced conformational changes of full-length EGFR expressed in living cells.

Author

Comez D, Glenn J, Anbuhl SM, Heukers R, Smit MJ, Hill SJ, and Kilpatrick LE

Subjects

Humans, Transforming Growth Factor alpha, Ligands, Epidermal Growth Factor, HEK293 Cells, ErbB Receptors, Coloring Agents, Immunoglobulin Heavy Chains, Single-Domain Antibodies

Abstract

Introduction: The Epidermal Growth Factor Receptor is a member of the Erb receptor tyrosine kinase family. It binds several ligands including EGF, betacellulin (BTC) and TGF-α, controls cellular proliferation and invasion and is overexpressed in various cancer types. Nanobodies (VHHs) are the antigen binding fragments of heavy chain only camelid antibodies. In this paper we used NanoBRET to compare the binding characteristics of fluorescent EGF or two distinct fluorescently labelled EGFR directed nanobodies (Q44c and Q86c) to full length EGFR., Methods: Living HEK293T cells were stably transfected with N terminal NLuc tagged EGFR. NanoBRET saturation, displacement or kinetics experiments were then performed using fluorescently labelled EGF ligands (EGF-AF488 or EGF-AF647) or fluorescently labelled EGFR targeting nanobodies (Q44c-HL488 and Q86c-HL488)., Results: These data revealed that the EGFR nanobody Q44c was able to inhibit EGF binding to full length EGFR, while Q86c was able to recognise agonist bound EGFR and act as a conformational sensor. The specific binding of fluorescent Q44c-HL488 and EGF-AF488 was inhibited by a range of EGFR ligands (EGF> BTC>TGF-α)., Discussion: EGFR targeting nanobodies are powerful tools for studying the role of the EGFR in health and disease and allow real time quantification of ligand binding and distinct ligand induced conformational changes., Competing Interests: RH is CSO of QVQ Holding B.V. and SA is affiliated to QVQ Holdings. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Comez, Glenn, Anbuhl, Heukers, Smit, Hill and Kilpatrick.)

Published

2022

44. Research progress on unique paratope structure, antigen binding modes, and systematic mutagenesis strategies of single-domain antibodies.

Author

Liu C, Lin H, Cao L, Wang K, and Sui J

Subjects

Molecular Biology, Immunoglobulin G, Single-Domain Antibodies

Abstract

Single-domain antibodies (sdAbs) showed the incredible advantages of small molecular weight, excellent affinity, specificity, and stability compared with traditional IgG antibodies, so their potential in binding hidden antigen epitopes and hazard detection in food, agricultural and veterinary fields were gradually explored. Moreover, its low immunogenicity, easy-to-carry target drugs, and penetration of the blood-brain barrier have made sdAbs remarkable achievements in medical treatment, toxin neutralization, and medical imaging. With the continuous development and maturity of modern molecular biology, protein analysis software and database with different algorithms, and next-generation sequencing technology, the unique paratope structure and different antigen binding modes of sdAbs compared with traditional IgG antibodies have aroused the broad interests of researchers with the increased related studies. However, the corresponding related summaries are lacking and needed. Different antigens, especially hapten antigens, show distinct binding modes with sdAbs. So, in this paper, the unique paratope structure of sdAbs, different antigen binding cases, and the current maturation strategy of sdAbs were classified and summarized. We hope this review lays a theoretical foundation to elucidate the antigen-binding mechanism of sdAbs and broaden the further application of sdAbs., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Liu, Lin, Cao, Wang and Sui.)

Published

2022

45. Neutralizing epitopes on Clostridioides difficile toxin A revealed by the structures of two camelid VHH antibodies.

Author

Chen B, Perry K, and Jin R

Subjects

Animals, Epitopes, Bacterial Toxins, Clostridioides difficile, Single-Domain Antibodies

Abstract

Toxin A (TcdA) and toxin B (TcdB) are two key virulence factors secreted by Clostridioides difficile , which is listed as an urgent threat by the CDC. These two large homologous exotoxins are mainly responsible for diseases associated with C. difficile infection (CDI) with symptoms ranging from diarrhea to life threatening pseudomembranous colitis. Single-domain camelid antibodies (VHHs) AH3 and AA6 are two potent antitoxins against TcdA, which when combined with two TcdB-targeting VHHs showed effective protection against both primary and recurrent CDI in animal models. Here, we report the co-crystal structures of AH3 and AA6 when they form complexes with the glucosyltransferase domain (GTD) and a fragment of the delivery and receptor-binding domain (DRBD) of TcdA, respectively. Based on these structures, we find that AH3 binding enhances the overall stability of the GTD and interferes with its unfolding at acidic pH, and AA6 may inhibit the pH-dependent conformational changes in the DRBD that is necessary for pore formation of TcdA. These studies reveal two functionally critical epitopes on TcdA and shed new insights into neutralizing mechanisms and potential development of epitope-focused vaccines against TcdA., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Chen, Perry and Jin.)

Published

2022

46. Generation of high affinity ICAM-1-specific nanobodies and evaluation of their suitability for allergy treatment.

Author

Zettl I, Ivanova T, Zghaebi M, Rutovskaya MV, Ellinger I, Goryainova O, Kollárová J, Villazala-Merino S, Lupinek C, Weichwald C, Drescher A, Eckl-Dorna J, Tillib SV, and Flicker S

Subjects

Animals, Humans, Intercellular Adhesion Molecule-1, Allergens, Camelus, Single-Domain Antibodies, Rhinitis, Allergic, Seasonal, Hypersensitivity therapy

Abstract

The nasal cavity is an important site of allergen entry. Hence, it represents an organ where trans-epithelial allergen penetration and subsequent IgE-mediated allergic inflammation can potentially be inhibited. Intercellular adhesion molecule 1 (ICAM-1) is highly expressed on the surface of respiratory epithelial cells in allergic patients. It was identified as a promising target to immobilize antibody conjugates bispecific for ICAM-1 and allergens and thereby block allergen entry. We have previously characterized a nanobody specific for the major birch pollen allergen Bet v 1 and here we report the generation and characterization of ICAM-1-specific nanobodies. Nanobodies were obtained from a camel immunized with ICAM-1 and a high affinity binder was selected after phage display (Nb44). Nb44 was expressed as recombinant protein containing HA- and His-tags in Escherichia coli (E.coli) and purified via affinity chromatography. SDS-PAGE and Western blot revealed a single band at approximately 20 kDa. Nb44 bound to recombinant ICAM-1 in ELISA, and to ICAM-1 expressed on the human bronchial epithelial cell line 16HBE14o- as determined by flow cytometry. Experiments conducted at 4°C and at 37°C, to mimic physiological conditions, yielded similar percentages (97.2 ± 1.2% and 96.7 ± 1.5% out of total live cells). To confirm and visualize binding, we performed immunofluorescence microscopy. While Texas Red Dextran was rapidly internalized Nb44 remained localized on the cell surface. Additionally, we determined the strength of Nb44 and ICAM-1 interaction using surface plasmon resonance (SPR). Nb44 bound ICAM-1 with high affinity (10 -10 M) and had slow off-rates (10 -4 s -1 ). In conclusion, our results showed that the selected ICAM-1-specific nanobody bound ICAM-1 with high affinity and was not internalized. Thus, it could be further used to engineer heterodimers with allergen-specific nanobodies in order to develop topical treatments of pollen allergy., Competing Interests: AD is employed by Cytiva GmbH. CL reports personal fees from Thermofisher, outside the submitted work. JE-D reports grants and personal fees from Astrazeneca, personal fees from Sanofi and GSK, outside the submitted work. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as potential conflict of interest., (Copyright © 2022 Zettl, Ivanova, Zghaebi, Rutovskaya, Ellinger, Goryainova, Kollárová, Villazala-Merino, Lupinek, Weichwald, Drescher, Eckl-Dorna, Tillib and Flicker.)

Published

2022

47. Applications of nanobodies in brain diseases.

Author

Zheng F, Pang Y, Li L, Pang Y, Zhang J, Wang X, and Raes G

Subjects

Humans, Blood-Brain Barrier, Brain, Genetic Vectors, Single-Domain Antibodies, Alzheimer Disease drug therapy

Abstract

Nanobodies are antibody fragments derived from camelids, naturally endowed with properties like low molecular weight, high affinity and low immunogenicity, which contribute to their effective use as research tools, but also as diagnostic and therapeutic agents in a wide range of diseases, including brain diseases. Also, with the success of Caplacizumab, the first approved nanobody drug which was established as a first-in-class medication to treat acquired thrombotic thrombocytopenic purpura, nanobody-based therapy has received increasing attention. In the current review, we first briefly introduce the characterization and manufacturing of nanobodies. Then, we discuss the issue of crossing of the brain-blood-barrier (BBB) by nanobodies, making use of natural methods of BBB penetration, including passive diffusion, active efflux carriers (ATP-binding cassette transporters), carrier-mediated influx via solute carriers and transcytosis (including receptor-mediated transport, and adsorptive mediated transport) as well as various physical and chemical methods or even more complicated methods such as genetic methods via viral vectors to deliver nanobodies to the brain. Next, we give an extensive overview of research, diagnostic and therapeutic applications of nanobodies in brain-related diseases, with emphasis on Alzheimer's disease, Parkinson's disease, and brain tumors. Thanks to the advance of nanobody engineering and modification technologies, nanobodies can be linked to toxins or conjugated with radionuclides, photosensitizers and nanoparticles, according to different requirements. Finally, we provide several perspectives that may facilitate future studies and whereby the versatile nanobodies offer promising perspectives for advancing our knowledge about brain disorders, as well as hopefully yielding diagnostic and therapeutic solutions., Competing Interests: GR is shareholder of Precirix and Abscint and is inventor on various patent applications covering diagnostic and/or therapeutic use of Nbs. FZ is shareholder of Shaanxi Shaanxi Haisinuowei Technology Co. LTD and is inventor on various patent applications covering diagnostic and/or therapeutic use of Nbs. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Zheng, Pang, Li, Pang, Zhang, Wang and Raes.)

Published

2022

48. Targeting multiple myeloma with nanobody-based heavy chain antibodies, bispecific killer cell engagers, chimeric antigen receptors, and nanobody-displaying AAV vectors.

Author

Hambach J, Mann AM, Bannas P, and Koch-Nolte F

Subjects

Humans, ADP-ribosyl Cyclase 1, Immunoglobulin Heavy Chains therapeutic use, Killer Cells, Natural, Receptors, Chimeric Antigen genetics, Receptors, Chimeric Antigen therapeutic use, Multiple Myeloma drug therapy, Antibodies, Bispecific therapeutic use, Single-Domain Antibodies

Abstract

Nanobodies are well suited for constructing biologics due to their high solubility. We generated nanobodies directed against CD38, a tumor marker that is overexpressed by multiple myeloma and other hematological malignancies. We then used these CD38-specific nanobodies to construct heavy chain antibodies, bispecific killer cell engagers (BiKEs), chimeric antigen receptor (CAR)-NK cells, and nanobody-displaying AAV vectors. Here we review the utility of these nanobody-based constructs to specifically and effectively target CD38-expressing myeloma cells. The promising results of our preclinical studies warrant further clinical studies to evaluate the potential of these CD38-specific nanobody-based constructs for treatment of multiple myeloma., Competing Interests: PB and FK-N are co-inventors on a patent application on CD38-specific nanobodies. AM and FK-N are co-inventors on a patent application on nanobody-displaying AAV vectors. FK-N receives a share of antibody and protein sales via MediGate GmbH, a wholly owned subsidiary of the University Medical Center Hamburg-Eppendorf. The remaining author declares that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest. MediGate GmbH was not involved in the study design, collection, analysis, interpretation of data, the writing of this article, or the decision to submit it for publication., (Copyright © 2022 Hambach, Mann, Bannas and Koch-Nolte.)

Published

2022

49. CD38-specific nanobodies allow in vivo imaging of multiple myeloma under daratumumab therapy.

Author

Pape LJ, Hambach J, Gebhardt AJ, Rissiek B, Stähler T, Tode N, Khan C, Weisel K, Adam G, Koch-Nolte F, and Bannas P

Subjects

Humans, Animals, Mice, ADP-ribosyl Cyclase 1 metabolism, Fluorescent Dyes, Epitopes, Multiple Myeloma diagnostic imaging, Multiple Myeloma drug therapy, Single-Domain Antibodies

Abstract

Rationale: Recent studies have demonstrated the feasibility of CD38-specific antibody constructs for in vivo imaging of multiple myeloma. However, detecting multiple myeloma in daratumumab-pretreated patients remains difficult due to overlapping binding epitopes of the CD38-specific imaging antibody constructs and daratumumab. Therefore, the development of an alternative antibody construct targeting an epitope of CD38 distinct from that of daratumumab is needed. We report the generation of a fluorochrome-conjugated nanobody recognizing such an epitope of CD38 to detect myeloma cells under daratumumab therapy in vitro , ex vivo , and in vivo ., Methods: We conjugated the CD38-specific nanobody JK36 to the near-infrared fluorescent dye Alexa Fluor 680. The capacity of JK36 AF680 to bind and detect CD38-expressing cells pretreated with daratumumab was evaluated on CD38-expressing tumor cell lines in vitro , on primary myeloma cells from human bone marrow biopsies ex vivo , and in a mouse tumor model in vivo ., Results: Fluorochrome-labeled nanobody JK36 AF680 showed specific binding to CD38-expressing myeloma cells pretreated with daratumumab in vitro and ex vivo and allowed for specific imaging of CD38-expressing xenografts in daratumumab-pretreated mice in vivo ., Conclusions: Our study demonstrates that a nanobody recognizing a distinct, non-overlapping epitope of CD38 allows the specific detection of myeloma cells under daratumumab therapy in vitro , ex vivo , and in vivo., Competing Interests: FK-N receives a share of antibody sales via MediGate GmbH, a wholly-owned subsidiary of the University Medical Center Hamburg-Eppendorf. PB and FK-N are co-inventors on a patent application on CD38-specific nanobodies. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Pape, Hambach, Gebhardt, Rissiek, Stähler, Tode, Khan, Weisel, Adam, Koch-Nolte and Bannas.)

Published

2022

50. Development of Nanobodies Against Hemorrhagic and Myotoxic Components of

Author

Henri, Bailon Calderon, Verónica Olga, Yaniro Coronel, Omar Alberto, Cáceres Rey, Elizabeth Gaby, Colque Alave, Walter Jhon, Leiva Duran, Carlos, Padilla Rojas, Harrison, Montejo Arevalo, David, García Neyra, Marco, Galarza Pérez, César, Bonilla, Benigno, Tintaya, Giulia, Ricciardi, Natalia, Smiejkowska, Ema, Romão, Cécile, Vincke, Juan, Lévano, Mary, Celys, Bruno, Lomonte, and Serge, Muyldermans

Subjects

Male, snake, Bothrops atrox, Antivenins, viperidae, Immunology, Snake Bites, venom, Hemorrhage, Myotoxicity, Single-Domain Antibodies, neutralization, complex mixtures, nanobodies, Mice, Treatment Outcome, hemorrhagic, Crotalid Venoms, Animals, Immunologic Factors, Bothrops, Immunization, myotoxic, Camelids, New World, Original Research

Abstract

Snake envenoming is a globally neglected public health problem. Antivenoms produced using animal hyperimmune plasma remain the standard therapy for snakebites. Although effective against systemic effects, conventional antivenoms have limited efficacy against local tissue damage. In addition, potential hypersensitivity reactions, high costs for animal maintenance, and difficulties in obtaining batch-to-batch homogeneity are some of the factors that have motivated the search for innovative and improved therapeutic products against such envenoming. In this study, we have developed a set of nanobodies (recombinant single-domain antigen-binding fragments from camelid heavy chain-only antibodies) against Bothrops atrox snake venom hemorrhagic and myotoxic components. An immune library was constructed after immunizing a Lama glama with whole venom of B. atrox, from which nanobodies were selected by phage display using partially purified hemorrhagic and myotoxic proteins. Biopanning selections retrieved 18 and eight different nanobodies against the hemorrhagic and the myotoxic proteins, respectively. In vivo assays in mice showed that five nanobodies inhibited the hemorrhagic activity of the proteins; three neutralized the hemorrhagic activity of whole B. atrox venom, while four nanobodies inhibited the myotoxic protein. A mixture of the anti-hemorrhagic and anti-myotoxic nanobodies neutralized the local tissue hemorrhage and myonecrosis induced by the whole venom, although the nanobody mixture failed to prevent the venom lethality. Nevertheless, our results demonstrate the efficacy and usefulness of these nanobodies to neutralize important pathologies of the venom, highlighting their potential as innovative therapeutic agents against envenoming by B. atrox, a viperid species causing many casualties in South America.

Published

2019