A biparatopic anti‐EGFR nanobody efficiently inhibits solid tumour growth

Roovers, Rob C.; Vosjan, Maria J. W. D.; Laeremans, Toon; Khoulati, Rachid el; Bruin, Renée C.G. de; Ferguson, Kathryn M.; Verkleij, Arie J.; Dongen, Guus A.M.S. van; Henegouwen, Paul M.P. van Bergen en

doi:10.1002/ijc.26145

Cited by 217 publications

(199 citation statements)

References 45 publications

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“…17 The heavy-chain only antibody-derived variable domain (VHH) has attracted much interest because of its stability, size (15 kDa), and cavity binding, as well as the ease with which it is engineered into manifold constructs with improved potency or broadened cross-reactivity profiles. 18,19 Due to the overwhelming attention that VHHs received over the last 2 decades, camelid conventional antibodies were overlooked.…”

Section: Introductionsupporting

confidence: 44%

Camelid Ig V genes reveal significant human homology not seen in therapeutic target genes, providing for a powerful therapeutic antibody platform

Klarenbeek

Mazouari²,

Desmyter

et al. 2015

mAbs

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de Haard & Ikbel Achour (2015) Camelid Ig V genes reveal significant human homology not seen in therapeutic target genes, providing for a powerful therapeutic antibody platform, mAbs, 7:4, 693-706, DOI: 10.1080/19420862.2015 To link to this article: https://doi.org/10. 1080/19420862.2015 Camelid immunoglobulin variable (IGV) regions were found homologous to their human counterparts; however, the germline V repertoires of camelid heavy and light chains are still incomplete and their therapeutic potential is only beginning to be appreciated. We therefore leveraged the publicly available HTG and WGS databases of Lama pacos and Camelus ferus to retrieve the germline repertoire of V genes using human IGV genes as reference. In addition, we amplified IGKV and IGLV genes to uncover the V germline repertoire of Lama glama and sequenced BAC clones covering part of the Lama pacos IGK and IGL loci. Our in silico analysis showed that camelid counterparts of all human IGKV and IGLV families and most IGHV families could be identified, based on canonical structure and sequence homology. Interestingly, this sequence homology seemed largely restricted to the Ig V genes and was far less apparent in other genes: 6 therapeutically relevant target genes differed significantly from their human orthologs. This contributed to efficient immunization of llamas with the human proteins CD70, MET, interleukin (IL)-1b and IL-6, resulting in large panels of functional antibodies. The in silico predicted human-homologous canonical folds of camelidderived antibodies were confirmed by X-ray crystallography solving the structure of 2 selected camelid anti-CD70 and anti-MET antibodies. These antibodies showed identical fold combinations as found in the corresponding human germline V families, yielding binding site structures closely similar to those occurring in human antibodies. In conclusion, our results indicate that active immunization of camelids can be a powerful therapeutic antibody platform.

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Section: Introductionsupporting

confidence: 44%

Camelid Ig V genes reveal significant human homology not seen in therapeutic target genes, providing for a powerful therapeutic antibody platform

Klarenbeek

Mazouari²,

Desmyter

et al. 2015

mAbs

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“…12, 13), and bispecific (Nanobodies binding to 2 different antigens; refs. 13,14) molecules. These formats are easy to construct and the modular proteins can often be expressed at high levels in bacteria or yeast.…”

Section: Introductionsupporting

confidence: 40%

“…What is more, biodistribution of aEGFRaEGFR-aAlb (50 kDa) was comparable with cetuximab (150 kDa), while it showed faster and deeper tumor penetration. The therapeutic potential of aEGFR-Nanobodies in comparison with conventional aEGFR mAbs was shown by Roovers and colleagues (13).…”

Section: Introductionmentioning

confidence: 45%

Nanobodies Targeting the Hepatocyte Growth Factor: Potential New Drugs for Molecular Cancer Therapy

Vosjan

Vercammen

Kolkman

et al. 2012

Molecular Cancer Therapeutics

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114

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Hepatocyte growth factor (HGF) and its receptor c-Met are associated with increased aggressiveness of tumors and poor prognostic outcome of patients with cancer. Here, we report the development and characterization of therapeutic anti-HGF (aHGF)-Nanobodies and their potential for positron emission tomographic (PET) imaging to assess HGF expression in vivo. Two aHGF-Nanobodies designated 1E2 and 6E10 were identified, characterized, and molecularly fused to an albumin-binding Nanobody unit (Alb8) to obtain serum half-life extension. The resulting Nanobody formats were radiolabeled with the positron emitter zirconium-89 ( 89 Zr, t1/ 2 ¼ 78 hours), administered to nude mice bearing U87 MG glioblastoma xenografts, and their biodistribution was assessed. In addition, their therapeutic effect was evaluated in the same animal model at doses of 10, 30, or 100 mg per mouse. The 89 Zr-Nanobodies showed similar biodistribution with selective tumor targeting. For example, 1E2-Alb8 showed decreased blood levels of 12.6%ID/g AE 0.6%ID/g, 7.2%ID/g AE 1.0%ID/g, 3.4%ID/g AE 0.3%ID/g, and 0.3%ID/g AE 0.1%ID/g at 1, 2, 3, and 7 days after injection, whereas tumor uptake levels remained relatively stable at these time points: 7.8%ID/g AE 1.1%ID/g, 8.9%ID/g AE 1.0%ID/g, 8.7%ID/g AE 1.5%ID/g, and 7.2%ID/g AE1.6%ID/g. Uptake in normal tissues was lower than in tumor, except for kidneys. In a therapy study, all Nanobody-treated mice showed tumor growth delay compared with the control saline group. In the 100-mg group, four of six mice were cured after treatment with 1E2-Alb8 and 73 days follow-up, and three of six mice when treated with 6E10-Alb8. These results provide evidence that Nanobodies 1E2-Alb8 and 6E10-Alb8 have potential for therapy and PET imaging of HGFexpressing tumors.

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“…They consist of heavy chains only and have desirable features such as small size, decreased immunogenicity, and high binding affinities. 56 Nanobodies have been designed for use in cancer therapy, 57,58 antivenoms, 59 inflammatory conditions, 60 and immunoimaging. [60][61][62][63][64] Nanobodies can detect vascular and parenchymal amyloid beta (A␤) deposits in vivo to differentiate cerebral ␤-amyloid indicative of Alzheimer disease and vascular A␤ plaques associated with cerebral amyloid angiopathy.…”

Section: Nanobodiesmentioning

confidence: 41%

New Applications of Nanotechnology for Neuroimaging

Suffredini

East

Levy

2013

AJNR Am J Neuroradiol

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SUMMARY:Advances in nanotechnology have the potential to dramatically enhance the detection of neurologic diseases with targeted contrast agents and to facilitate the delivery of focused therapies to the central nervous system. We present the physicochemical rationale for their use, applications in animal models, and ongoing clinical trials using these approaches. We highlight advances in the use of nanoparticles applied to brain tumor imaging, tumor angiogenesis, neurodegeneration, grafted stem cells, and neuroprogenitor cells.ABBREVIATIONS: amyloid beta ϭ A␤; NO ϭ nitric oxide; NOS ϭ nitric oxide synthase; PBCA ϭ poly(n-butyl cyanoacrylate); QDots ϭ quantum dots; SPIO ϭ

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A biparatopic anti‐EGFR nanobody efficiently inhibits solid tumour growth

Cited by 217 publications

References 45 publications

Camelid Ig V genes reveal significant human homology not seen in therapeutic target genes, providing for a powerful therapeutic antibody platform

Camelid Ig V genes reveal significant human homology not seen in therapeutic target genes, providing for a powerful therapeutic antibody platform

Nanobodies Targeting the Hepatocyte Growth Factor: Potential New Drugs for Molecular Cancer Therapy

New Applications of Nanotechnology for Neuroimaging

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