Evaluation and optimization of the efficacy of anticancer conjugates targeting folate receptors

En dépit des progrès réalisés ces dernières décennies, le cancer demeure un problème majeur de santé publique. La plupart des chimiothérapies conventionnelles exploitent les propriétés cytotoxiques d'agents non sélectifs qui affectent les cellules à division rapide, qu'elles soient cancéreuses ou non, ce qui peut aboutir à une toxicité importante et de sévères effets secondaires. Pour pallier à ce problème, l'utilisation de ligands de ciblage pour délivrer spécifiquement l'agent cytotoxique aux cellules malignes tout en épargnant les tissus sains est une approche prometteuse. Parmi les différents ligands exploités, l'acide folique fait l'objet d'une attention particulière due à la surexpression préférentielle de son récepteur par de nombreux types de cellules cancéreuses. Cependant, les essais cliniques menés sur des molécules reposant sur cette stratégie indiquent que leur efficacité dépend surtout du niveau d'expression du récepteur ciblé. Dans ce contexte, j'ai développé deux approches permettant d'augmenter l'efficacité du ciblage des récepteurs à l'acide folique. D'une part, j'ai réalisé la validation biologique de nouveaux conjugués conçus pour délivrer conjointement deux agents anticancéreux. D'autre part, j'ai mis au point un traitement capable d'augmenter, in vitro et in vivo, l'expression des récepteurs à l'acide folique à la surface des cellules tumorales. Cela aboutit à l'internalisation d'une plus grande quantité de vecteur, qui se traduit in vivo, par une inhibition plus importante de la croissance tumorale, sans toxicité sur les cellules saines.Despite significant advances obtained during the last decades, cancer is still lack of effective treatments. Indeed, most conventional chemotherapies relies on non-selective agents that kill indifferently healthy and tumor cells with high rate of division. This can lead to elevated toxicity and severe side effects. In this context, therapeutic approaches that exploit targeting ligands to selectively deliver cytotoxic drugs to malignant cells are currently promising. Among these different ligands, folate conjugates are subject to special attention due to the preferential overexpression of the folate receptor on several human cancer cell types that can mediate specific attachment and internalization of folate-derived imaging and therapeutic agents. However, clinical trials carried on such molecules revealed that their efficiency is mainly governed by folate receptor expression level on tumor cells. In this respect, I developed two approaches to increase efficacy of folate receptor targeting. On one hand, I realized biological validation of new targeting devices designed for the simultaneous delivery of two therapeutic agents. On the other hand, I developed a treatment to enhance in vitro and in vivo folate receptor expression at the surface of malignant cells. This treatment allows the internalization of a larger amount of a folic acid conjugate, previously synthesized and validated in our laboratory. That results in a drastically improvement of the in vivo tumor growth inhibition, without toxicity toward healthy cells

A β-glucuronidase-responsive albumin-binding prodrug for potential selective kinase inhibitor-based cancer chemotherapy

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A dendritic β-galactosidase-responsive folate-monomethylauristatin E conjugate.

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In vivo synthesis of triple-loaded albumin conjugate for efficient targeted cancer chemotherapy

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Combination of Targeted Therapies for Colorectal Cancer Treatment

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Controlled Release of a Micelle Payload via Sequential Enzymatic and Bioorthogonal Reactions in Living Systems

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A β-Cyclodextrin-Albumin Conjugate for Enhancing Therapeutic Efficacy of Cytotoxic Drugs

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Cx43 Present at the Leading Edge Membrane Governs Promigratory Effects of Osteoblast-Conditioned Medium on Human Prostate Cancer Cells in the Context of Bone Metastasis

International audienceAmong the different interacting molecules implicated in bone metastases, connexin43 (Cx43) may increase sensitivity of prostate cancer (PCa) cells to bone microenvironment, as suggested by our in silico and human tissue samples analyses that revealed increased level of Cx43 expression with PCa progression and a Cx43 specific expression in bone secondary sites. The goal of the present study was to understand how Cx43 influences PCa cells sensitivity and aggressiveness to bone microenvironment. By means of Cx43-overexpressing PCa cell lines, we revealed a Cx43-dependent promigratory effect of osteoblastic conditioned media (ObCM). This effect on directional migration relied on the presence of Cx43 at the plasma membrane and not on gap junctional intercellular communication and hemichannel functions. ObCM stimulation induced Rac1 activation and Cx43 interaction with cortactin in protrusions of migrating PCa cells. Finally, by transfecting two different truncated forms of Cx43 in LNCaP cells, we determined that the carboxy terminal (CT) part of Cx43 is crucial for the responsiveness of PCa cells to ObCM. Our study demonstrates that Cx43 level and its membrane localization modulate the phenotypic response of PCa cells to osteoblastic microenvironment and that its CT domain plays a pivotal role

A mechanically interlocked molecular system programmed for the delivery of an anticancer drug

The development of mechanically interlocked molecular systems programmed to operate autonomously in biological environments is an emerging field of research with potential medicinal applications. Within this framework, functional rotaxane- and pseudorotaxane-based architectures are starting to attract interest for the delivery of anticancer drugs, with the ultimate goal to improve the efficiency of cancer chemotherapy. Here, we report an enzyme-sensitive [2]-rotaxane designed to release a potent anticancer drug within tumor cells. The molecular device includes a protective ring that prevents the premature liberation of the drug in plasma. However, once located inside cancer cells the [2]-rotaxane leads to the release of the drug through the controlled disassembly of the mechanically interlocked components, in response to a determined sequence of two distinct enzymatic activations. Furthermore, in vitro biological evaluations reveal that this biocompatible functional system exhibits a noticeable level of selectivity for cancer cells overexpressing β-galactosidas

A galactosidase-responsive doxorubicin-folate conjugate for selective targeting of acute myelogenous leukemia blasts

International audienceCytarabine combined with an anthracycline or an anthracenedione represents the usual intensive induction therapy for the treatment of AML. However, this protocol induces severe side effects and treatment-related mortality due to the lack of selectivity of these cytotoxic agents. In this paper, we present the study of the first galactosidase-responsive molecular "Trojan Horse" programmed for the delivery of doxorubicin exclusively inside AML blasts over-expressing the folate receptor (FR). This targeting system allows the selective killing of AML blasts without affecting normal endothelial, cardiac or hematologic cells from healthy donors suggesting that FDC could reduce adverse events usually recorded with anthracyclines