Literature DB >> 24435448

Enhancement of the tumor penetration of monoclonal antibody by fusion of a neuropilin-targeting peptide improves the antitumor efficacy.

Tae-Hwan Shin1, Eun-Sil Sung, Ye-Jin Kim, Ki-Su Kim, Se-Ho Kim, Seok-Ki Kim, Young-Don Lee, Yong-Sung Kim.   

Abstract

The limited localization and penetration of monoclonal antibodies (mAb) into solid tumors restricts their antitumor efficacy. Here, we describe a solid tumor-targeting antibody with enhanced tumor penetration activity. We designed a 22-residue peptide (A22p), which was extracted from the C-terminal basic region of semaphorin 3A (Sema3A) but modified to have higher affinity with neuropilin receptors (NRP), and genetically fused it to the C-terminus of Fc of human immunoglobulin G1 via a 15-residue (G4S)3 linker, generating Fc-A22p, for the bivalent binding to NRPs. In contrast to Fc or the monovalent A22p peptide alone, Fc-A22p homed to tumor vessels and induced vascular permeability through VE-cadherin downregulation and penetrated tumor tissues by interacting with NRPs in mice bearing human tumor xenografts. We extended the Fc-A22p platform by generating mAb-A22p antibodies of two clinically approved solid tumor-targeting mAbs, the anti-EGF receptor mAb cetuximab (erbitux), and the anti-Her2 mAb trastuzumab (herceptin). The mAb-A22p antibodies retained the intrinsic antigen binding, natural Fc-like biophysical properties, and productivity in mammalian cell cultures, comparable with those of the parent mAbs. In mouse xenograft tumor models, the mAb-A22p antibodies more efficiently homed to tumor vessels and spread into the extravascular tumor parenchyma, which significantly enhanced antitumor efficacy compared with the parent mAbs. Our results suggest that mAb-A22p is a superior format for solid tumor-targeting antibodies due to its enhanced tumor tissue penetration and greater antitumor efficacy compared with conventional mAbs. ©2014 AACR.

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Year:  2014        PMID: 24435448     DOI: 10.1158/1535-7163.MCT-13-0748

Source DB:  PubMed          Journal:  Mol Cancer Ther        ISSN: 1535-7163            Impact factor:   6.261


  25 in total

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5.  A general strategy for generating intact, full-length IgG antibodies that penetrate into the cytosol of living cells.

Authors:  Dong-Ki Choi; Jeomil Bae; Seung-Min Shin; Ju-Yeon Shin; Sunghoon Kim; Yong-Sung Kim
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Journal:  Adv Drug Deliv Rev       Date:  2016-04-01       Impact factor: 15.470

8.  Quantification of recombinant immunotoxin delivery to solid tumors allows for direct comparison of in vivo and in vitro results.

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9.  Transient Competitive Inhibition Bypasses the Binding Site Barrier to Improve Tumor Penetration of Trastuzumab and Enhance T-DM1 Efficacy.

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10.  Tumor-penetrating iRGD peptide inhibits metastasis.

Authors:  Kazuki N Sugahara; Gary B Braun; Tatiana Hurtado de Mendoza; Venkata Ramana Kotamraju; Randall P French; Andrew M Lowy; Tambet Teesalu; Erkki Ruoslahti
Journal:  Mol Cancer Ther       Date:  2014-11-12       Impact factor: 6.261

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