Literature DB >> 28662334

Protease-Cleavable Linkers Modulate the Anticancer Activity of Noninternalizing Antibody-Drug Conjugates.

Alberto Dal Corso1, Samuele Cazzamalli1, Rémy Gébleux1, Martin Mattarella2, Dario Neri1.   

Abstract

Antibody-drug conjugates (ADCs) represent an attractive class of biopharmaceutical agents, with the potential to selectively deliver potent cytotoxic agents to tumors. It is generally assumed that ADC products should preferably bind and internalize into cancer cells in order to liberate their toxic payload, but a growing body of evidence indicates that also ADCs based on noninternalizing antibodies may be potently active. In this Communication, we investigated dipeptide-based linkers (frequently used for internalizing ADC products) in the context of the noninternalizing F16 antibody, specific to a splice isoform of tenascin-C. Using monomethyl auristatin E (MMAE) as potent cytotoxic drug, we observed that a single amino acid substitution of the Val-Cit dipeptide linker can substantially modulate the in vivo stability of the corresponding ADC products, as well as the anticancer activity in mice bearing the human epidermoid A431 carcinoma. In these settings, the linker based on the Val-Ala dipeptide exhibited better performances, compared to Val-Cit, Val-Lys, and Val-Arg analogues. Mass spectrometric analysis revealed that the four linkers displayed not only different stability in vivo but also differences in cleavage sites. Moreover, the absence of anticancer activity for a F16-MMAE conjugate featuring a noncleavable linker indicated that drug release modalities, based on proteolytic degradation of the immunoglobulin moiety, cannot be exploited with noninternalizing antibodies. ADC products based on the noninternalizing F16 antibody may be useful for the treatment of several human malignancies, as the cognate antigen is abundantly expressed in the extracellular matrix of several tumors, while being virtually undetectable in most normal adult tissues.

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Year:  2017        PMID: 28662334      PMCID: PMC5521252          DOI: 10.1021/acs.bioconjchem.7b00304

Source DB:  PubMed          Journal:  Bioconjug Chem        ISSN: 1043-1802            Impact factor:   4.774


  41 in total

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3.  Investigation of Hydrophilic Auristatin Derivatives for Use in Antibody Drug Conjugates.

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Journal:  Curr Opin Immunol       Date:  2016-03-07       Impact factor: 7.486

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Review 2.  Antibody drug conjugates and bystander killing: is antigen-dependent internalisation required?

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Journal:  Br J Cancer       Date:  2017-10-24       Impact factor: 7.640

3.  Multivalency Increases the Binding Strength of RGD Peptidomimetic-Paclitaxel Conjugates to Integrin αV β3.

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5.  Chemically Defined Antibody- and Small Molecule-Drug Conjugates for in Vivo Tumor Targeting Applications: A Comparative Analysis.

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6.  Enhanced Therapeutic Activity of Non-Internalizing Small-Molecule-Drug Conjugates Targeting Carbonic Anhydrase IX in Combination with Targeted Interleukin-2.

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7.  A non-internalizing antibody-drug conjugate based on an anthracycline payload displays potent therapeutic activity in vivo.

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8.  Simultaneous targeting of primary tumor, draining lymph node, and distant metastases through high endothelial venule-targeted delivery.

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Review 9.  The Chemistry Behind ADCs.

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Journal:  Pharmaceuticals (Basel)       Date:  2021-05-07

10.  Antibody drug conjugates (ADCs) charged with HDAC inhibitor for targeted epigenetic modulation.

Authors:  Elena Cini; Valentina Faltoni; Elena Petricci; Maurizio Taddei; Laura Salvini; Giuseppe Giannini; Loredana Vesci; Ferdinando Maria Milazzo; Anna Maria Anastasi; Gianfranco Battistuzzi; Rita De Santis
Journal:  Chem Sci       Date:  2018-07-03       Impact factor: 9.825

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