Literature DB >> 19628871

Biodistribution of a bispecific single-chain diabody and its half-life extended derivatives.

Roland Stork1, Emmanuelle Campigna, Bruno Robert, Dafne Müller, Roland E Kontermann.   

Abstract

Small recombinant antibody molecules such as bispecific single-chain diabodies (scDb) possessing a molecular mass of approximately 55 kDa are rapidly cleared from circulation. We have recently extended the plasma half-life of scDb applying various strategies including PEGylation, N-glycosylation and fusion to an albumin-binding domain (ABD) from streptococcal protein G. Here, we further analyzed the influence of these modifications on the biodistribution of a scDb directed against carcinoembryonic antigen (CEA) and CD3 capable of retargeting T cells to CEA-expressing tumor cells. We show that a prolonged circulation time results in an increased accumulation in CEA+ tumors, which was most pronounced for scDb-ABD and PEGylated scDb. Interestingly, tumor accumulation of the scDb-ABD fusion protein was approximately 2-fold higher compared with PEGylated scDb, although both molecules exhibit similar plasma half-lives and similar affinities for CEA. Comparing half-lives in neonatal Fc receptor (FcRn) wild-type and FcRn heavy chain knock-out mice the contribution of the FcRn to the long plasma half-life of scDb-ABD was confirmed. The half-life of scDb-ABD was approximately 2-fold lower in the knock-out mice, while no differences were observed for PEGylated scDb. Binding of the scDb derivatives to target and effector cells was not or only marginally affected by the modifications, although, compared with scDb, a reduced cytotoxic activity was observed for scDb-ABD, which was further reduced in the presence of albumin. In summary, these findings demonstrate that the extended half-life of a bispecific scDb translates into improved accumulation in antigen-positive tumors but that modifications might also affect scDb-mediated cytotoxicity.

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Year:  2009        PMID: 19628871      PMCID: PMC2757963          DOI: 10.1074/jbc.M109.027078

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  35 in total

1.  Improved pharmacokinetics of recombinant bispecific antibody molecules by fusion to human serum albumin.

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3.  Engineering of a femtomolar affinity binding protein to human serum albumin.

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4.  Tumor localization of anti-CEA single-chain Fvs: improved targeting by non-covalent dimers.

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  32 in total

1.  Plasma half-life extension of small recombinant antibodies by fusion to immunoglobulin-binding domains.

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2.  Eradication of Established Tumors by Chemically Self-Assembled Nanoring Labeled T Cells.

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Review 5.  Genetically engineered humanized mouse models for preclinical antibody studies.

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7.  Extending half-life by indirect targeting of the neonatal Fc receptor (FcRn) using a minimal albumin binding domain.

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8.  Biodistribution studies with tumor-targeting bispecific antibodies reveal selective accumulation at the tumor site.

Authors:  Thomas List; Dario Neri
Journal:  MAbs       Date:  2012-10-02       Impact factor: 5.857

9.  Target-mediated exposure enhancement: a previously unexplored limit of TMDD.

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10.  Development and characterization of small bispecific albumin-binding domains with high affinity for ErbB3.

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Journal:  Cell Mol Life Sci       Date:  2013-06-02       Impact factor: 9.261

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