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Evaluation of a novel 177Lu-labelled therapeutic Affibody molecule with a deimmunized ABD domain and improved biodistribution profile
Uppsala University, Disciplinary Domain of Medicine and Pharmacy, Faculty of Medicine, Department of Immunology, Genetics and Pathology, Cancer precision medicine.ORCID iD: 0000-0001-5871-5779
Uppsala University, Disciplinary Domain of Medicine and Pharmacy, Faculty of Medicine, Department of Immunology, Genetics and Pathology, Cancer precision medicine. Affibody AB, Solna, 171 65, Sweden.ORCID iD: 0000-0003-2660-9837
Uppsala University, Disciplinary Domain of Medicine and Pharmacy, Faculty of Medicine, Department of Immunology, Genetics and Pathology.ORCID iD: 0000-0001-6038-8295
Uppsala University, Disciplinary Domain of Medicine and Pharmacy, Faculty of Medicine, Department of Immunology, Genetics and Pathology, Cancer precision medicine.ORCID iD: 0000-0002-4778-3909
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2024 (English)In: European Journal of Nuclear Medicine and Molecular Imaging, ISSN 1619-7070, E-ISSN 1619-7089, Vol. 51, no 13, p. 4038-4048Article in journal (Refereed) Published
Abstract [en]

Purpose

Fusion of Affibody molecules with an albumin-binding domain (ABD) provides targeting agents, which are suitable for radionuclide therapy. To facilitate clinical translation, the low immunogenic potential of such constructs with targeting properties conserved is required.

Methods

The HER2-targeting Affibody molecule ZHER2:2891 was fused with a deimmunized ABD variant and DOTA was conjugated to a unique C-terminal cysteine. The novel construct, PEP49989, was labelled with 177Lu. Affinity, specificity, and in vivo targeting properties of [177Lu]Lu-PEP49989 were characterised. Experimental therapy in mice with human HER2-expressing xenografts was evaluated.

Results

The maximum molar activity of 52 GBq/µmol [177Lu]Lu-PEP49989 was obtained. [177Lu]Lu-PEP49989 bound specifically to HER2-expressing cells in vitro and in vivo. The HER2 binding affinity of [177Lu]Lu-PEP49989 was similar to the affinity of [177Lu]Lu-ABY-027 containing the parental ABD035 variant. The renal uptake of [177Lu]Lu-PEP49989 was 1.4-fold higher, but hepatic and splenic uptake was 1.7-2-fold lower than the uptake of [177Lu]Lu-ABY-027. The median survival of xenograft-bearing mice treated with 21 MBq [177Lu]Lu-PEP49989 (> 90 days) was significantly longer than the survival of mice treated with vehicle (38 days) or trastuzumab (45 days). Treatment using a combination of [177Lu]Lu-PEP49989 and trastuzumab increased the number of complete tumour remissions. The renal and hepatic toxicity was minimal to mild.

Conclusion

In preclinical studies, [177Lu]Lu-PEP49989 demonstrated favourable biodistribution and a strong antitumour effect, which was further enhanced by co-treatment with trastuzumab.
Place, publisher, year, edition, pages
Springer, 2024. Vol. 51, no 13, p. 4038-4048
Keywords [en]
Affibody molecules, Albumin binding domain, Lutetium-177, Therapy
National Category
Pharmaceutical and Medical Biotechnology Medicinal Chemistry Radiology, Nuclear Medicine and Medical Imaging
Identifiers
URN: urn:nbn:se:uu:diva-546436DOI: 10.1007/s00259-024-06840-5ISI: 001281644700005PubMedID: 39008065Scopus ID: 2-s2.0-85198617744OAI: oai:DiVA.org:uu-546436DiVA, id: diva2:1925662
Funder
Uppsala University, UFV-PA 2022/3323Swedish Cancer Society, 211485PjSwedish Cancer Society, 232645PjF01HSwedish Cancer Society, 230650JIASwedish Research Council, 2022-00556Swedish Research Council, 2022-01519Available from: 2025-01-09 Created: 2025-01-09 Last updated: 2025-12-08Bibliographically approved
In thesis
1. Affibody Molecule-mediated Radionuclide Therapy of HER2-expressing Cancers
Open this publication in new window or tab >>Affibody Molecule-mediated Radionuclide Therapy of HER2-expressing Cancers
2026 (English)Doctoral thesis, comprehensive summary (Other academic)
Abstract [en]

Human Epidermal Growth Factor Receptor 2 (HER2) is over-expressed in several cancers, including breast, gastric, ovarian, and lung cancers. Although HER2-targeted monoclonal antibodies have improved clinical outcomes, resistance remains a major challenge. Their large molecular size also limits tumor penetration and leads to prolonged circulation, increasing off-target toxicity. Affibody molecules offer an attractive alternative due to their small size (~7 kDa), high stability, and strong, specific HER2 binding. Their rapid tumor penetration and fast blood clearance make them suitable for imaging and Targeted Radionuclide Therapy (TRT). Therapeutic radionuclides like lutetium-177 and rhenium-188 can be site specifically labeled with Affibody molecules via conjugated chelators, enabling selective delivery of cytotoxic radiation to HER2-expressing tumors. A major limitation of Affibody-based TRT is high renal uptake. Strategies such as non-residualizing labels and fusion with albumin-binding domains (ABD) aim to improve biodistribution. Non-residualiz-ing labels utilize the slow internalization of HER2-bound Affibody molecules in tumors while allowing rapid renal clearance, resulting in higher tumor-to-kidney ratios. ABD fusion prolongs circulation by binding to serum albumin, reducing renal filtration and enhancing tumor accumulation. These approaches form the basis of the work summarized in this thesis.

Paper I showed that the non-residualizing label, [188Re]Re-ZHER2:41071 pro-vided favorable tumor-to-kidney ratios and improved survival in mice without organ toxicity. Paper II evaluated chelator positioning in ABD-fused constructs and demonstrated that placing DOTA to helix 1 of ABD did not reduce renal uptake. Paper III showed that chemo-enzymatic peptide synthesis enables production of ABD-fused Affibody molecules with preserved structure, HER2 affinity, albumin binding, and in vivo targeting. Paper IV demonstrated that [177Lu]Lu-ABY-027, alone or combined with trastuzumab, significantly prolonged survival in xenografted mice, with combination therapy providing better outcome. Paper V introduced a variant with deimmunized ABD, PEP49989, which improved biodistribution profile and provided potent therapeutic efficacy, further enhanced by trastuzumab, with minimal renal and hepatic toxicity.

In conclusion, strategies such as non-residualizing label and ABD fusion enable effective tumor targeting and therapeutic effects. These advances validate Affibody-based TRT as a promising complement to existing HER2-directed therapies and provide important design principles for next-generation radio-pharmaceuticals with improved safety, efficacy, and translational potential. 
Place, publisher, year, edition, pages
Uppsala: Acta Universitatis Upsaliensis, 2026. p. 77
Series
Digital Comprehensive Summaries of Uppsala Dissertations from the Faculty of Medicine, ISSN 1651-6206 ; 2224
Keywords
Affibody molecule, HER2, targeted radionuclide therapy, tumor targeting, lutetium-177, rhenium-188, non-residualizing label, albumin-bind-ing domain (ABD)
National Category
Cancer and Oncology
Research subject
Medical Science
Identifiers
urn:nbn:se:uu:diva-572728 (URN)978-91-513-2704-4 (ISBN)
Public defence
2026-02-06, Rudbecksalen, Rudbeck laboratory, Dag Hammarskjölds Väg 20, Uppsala, 09:00 (English)
Opponent
Supervisors
Available from: 2026-01-15 Created: 2025-12-08 Last updated: 2026-01-15

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Liu, YongshengOroujeni, MaryamLiao, YunqiVorobyeva, AnzhelikaOrlova, AnnaFrejd, Fredrik Y.Tolmachev, Vladimir

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Liu, YongshengOroujeni, MaryamLiao, YunqiVorobyeva, AnzhelikaOrlova, AnnaFrejd, Fredrik Y.Tolmachev, Vladimir
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Cancer precision medicineDepartment of Immunology, Genetics and PathologyTheranostics
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