Impact of cathepsin B-sensitive triggers and hydrophilic linkers on<i>in vitro</i>efficacy of novel site-specific antibody–drug conjugates

Bryden, Francesca; Martin, Camille; Letast, Stéphanie; Llès, Eva; Viéitez-Villemin, Inmaculada; Rousseau, Anaïs; Colas, Cyril; Brachet-Botineau, Marie; Allard-Vannier, Émilie; Larbouret, Christel; Viaud‐Massuard, Marie‐Claude; Joubert, Nicolas

doi:10.1039/c7ob02780j

Cited by 40 publications

(51 citation statements)

References 24 publications

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“…As shown in Figure 1, all tested AFCs had an average FAR of 1.5 calculated from the FAR distribution (Figure 1). As expected, for the same average FAR, the distribution of SGM-based AFCs 7a, 7b, 8a, and 8b was more homogeneous (2 species, FAR 1 and 2) compared to their lysine-conjugated counterparts 9a, 9b, 10a, and 10b (5 or 6 species, ranging from FAR 0 to FAR 5) [16,26,27].…”

Section: Mass Spectrometrysupporting

confidence: 80%

“…In this context, our team [16][17][18] and several others [8,19] developed second-generation maleimides or SGM (dibromomaleimide or dithiophenylmaleimide) [16,20] to produce ADCs or AFCs. After mild reduction of the mAb, these SGMs are able to undergo bioconjugation onto mAb through interchain cysteine cross-linking (Scheme 2b) to afford stable AFCs with a controlled FAR.…”

Section: Introductionmentioning

confidence: 99%

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In Vitro Characterization and Stability Profiles of Antibody–Fluorophore Conjugates Derived from Interchain Cysteine Cross-Linking or Lysine Bioconjugation

et al. 2019

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Fluorescent labelling of monoclonal antibodies (mAbs) is classically performed by chemical bioconjugation methods. The most frequent labelling technique to generate antibody–fluorophore conjugates (AFCs) involves the bioconjugation onto the mAb lysines of a dye bearing an N-hydroxysuccinimide ester or an isothiocyanate group. However, discrepancies between labelling experiments or kits can be observed, related to reproducibility issues, alteration of antigen binding, or mAb properties. The lack of information on labelling kits and the incomplete characterization of the obtained labelled mAbs largely contribute to these issues. In this work, we generated eight AFCs through either lysine or interchain cysteine cross-linking bioconjugation of green-emitting fluorophores (fluorescein or BODIPY) onto either trastuzumab or rituximab. This strategy allowed us to study the influence of fluorophore solubility, bioconjugation technology, and antibody nature on two known labelling procedures. The structures of these AFCs were thoroughly analyzed by mass spectroscopy, and their antigen binding properties were studied. We then compared these AFCs in vitro by studying their respective spectral properties and stabilities. The shelf stability profiles and sensibility to pH variation of these AFCs prove to be dye-, antibody- and labelling-technology-dependent. Fluorescence emission in AFCs was higher when lysine labelling was used, but cross-linked AFCs were revealed to be more stable. This must be taken into account for the design of any biological study involving antibody labelling.

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Section: Mass Spectrometrysupporting

confidence: 80%

Section: Introductionmentioning

confidence: 99%

In Vitro Characterization and Stability Profiles of Antibody–Fluorophore Conjugates Derived from Interchain Cysteine Cross-Linking or Lysine Bioconjugation

et al. 2019

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“…Bryden et al showed that Val-Ala and Val-Cit dipeptides could be incorporated into NGM linkers. 134 In the first instance, the hydrophobic nature of the Val-Ala motif was reported to cause a significant reduction in reactivity and only the Val-Cit-NGM linker was able to yield 450% of the desired DAR 4 ADC. However, later incorporation of PEG chains off-set the hydrophobicity issue and allowed for the generation of viable ADCs with either dipeptide motif.…”

Section: Disulfide Rebridgingmentioning

confidence: 99%

Site-selective modification strategies in antibody–drug conjugates

et al. 2021

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“…No effect was observed on HER2-negative MCF-7 cells. Although SDCs with a DAR of 1 are not yet as powerful as the corresponding ADCs with a DAR of 4 [79], this work represents the first step towards the design of more efficient small conjugates with higher DARs, opening up the path to further in vivo or even (pre)clinical studies in order to assess their promising potential against solid tumors [80]. Current ADCs targeting HER2 are ineffective in removing cancer cells expressing relatively low HER2 levels of expression.…”

Section: Alternative Adc Formatsmentioning

confidence: 99%

Antibody–Drug Conjugates: The Last Decade

et al. 2020

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An armed antibody (antibody–drug conjugate or ADC) is a vectorized chemotherapy, which results from the grafting of a cytotoxic agent onto a monoclonal antibody via a judiciously constructed spacer arm. ADCs have made considerable progress in 10 years. While in 2009 only gemtuzumab ozogamicin (Mylotarg®) was used clinically, in 2020, 9 Food and Drug Administration (FDA)-approved ADCs are available, and more than 80 others are in active clinical studies. This review will focus on FDA-approved and late-stage ADCs, their limitations including their toxicity and associated resistance mechanisms, as well as new emerging strategies to address these issues and attempt to widen their therapeutic window. Finally, we will discuss their combination with conventional chemotherapy or checkpoint inhibitors, and their design for applications beyond oncology, to make ADCs the magic bullet that Paul Ehrlich dreamed of.

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Impact of cathepsin B-sensitive triggers and hydrophilic linkers onin vitroefficacy of novel site-specific antibody–drug conjugates

Cited by 40 publications

References 24 publications

In Vitro Characterization and Stability Profiles of Antibody–Fluorophore Conjugates Derived from Interchain Cysteine Cross-Linking or Lysine Bioconjugation

In Vitro Characterization and Stability Profiles of Antibody–Fluorophore Conjugates Derived from Interchain Cysteine Cross-Linking or Lysine Bioconjugation

Site-selective modification strategies in antibody–drug conjugates

Antibody–Drug Conjugates: The Last Decade

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