β-Glucuronidase triggers extracellular MMAE release from an integrin-targeted conjugate

Paula López Rivas; Christoph Müller; Christian Breunig; Torsten Hechler; Andreas Pahl; Daniela Arosio; Laura Belvisi; Luca Pignataro; Alberto Dal Corso; Cesare Gennari

doi:10.1039/C9OB00617F

β-Glucuronidase triggers extracellular MMAE release from an integrin-targeted conjugate†

Paula López Rivas,^a Christoph Müller,^b Christian Breunig,^b Torsten Hechler,^b Andreas Pahl,^b Daniela Arosio,

^c Laura Belvisi,

^ac Luca Pignataro,

^a Alberto Dal Corso

^a and Cesare Gennari

*^ac

Author affiliations

* Corresponding authors

^a Università degli Studi di Milano, Dipartimento di Chimica, Via C. Golgi, Milan, Italy
E-mail: cesare.gennari@unimi.it

^b Heidelberg Pharma Research GmbH, Schriesheimer Strasse 101, Ladenburg, Germany

^c CNR, Istituto di Scienze e Tecnologie Molecolari (ISTM), Via C. Golgi, Milan, Italy

Abstract

A non-internalizing α_vβ₃ integrin ligand was conjugated to the anticancer drug MMAE through a β-glucuronidase-responsive linker. In the presence of β-glucuronidase, only the conjugate bearing a PEG4 spacer inhibited the proliferation of integrin-expressing cancer cells at low nanomolar concentrations, indicating important structural requirements for the efficacy of these therapeutics.

This article is part of the themed collection: Chemical Biology in OBC

Organic & Biomolecular Chemistry

β-Glucuronidase triggers extracellular MMAE release from an integrin-targeted conjugate†

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β-Glucuronidase triggers extracellular MMAE release from an integrin-targeted conjugate

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