Synthesis and antiviral activity of an imidazo[1,2-a]pyrrolo[2,3-c]pypridine series against the bovine viral diarrhea virus

A series of imidazo[1,2-a]pyrrolo[2,3-c]pyridines has been prepared and evaluated for their anti-BVDV activities in MDBK cells. From the synthesized analogues bearing modifications of the substituents at positions 2, 3, 7 and 8, compounds 10a, b, 16, 24, 25 and 26 exhibited significant anti-BVDV activities.status: publishe

Is tetraspanin 8 a target for radioimmunotherapy in syngeneic APC/min colorectal cancer model ?

International audienc

Conception et validation préclinique de nanobodies radiomarqués dirigés contre HER3 dans le cancer du sein triple négatif

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Synthesis and preliminary biological evaluations of PSMA-targeted NIR upconverting nanoparticles for optical/scintigraphic imaging of prostate cancer.

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Preliminary evaluations of PSMA-targeted NIR upconverting nanoparticles for dual scintigraphic/fluorescence-guided surgery in prostate cancer.

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Proteoglycans as Target for an Innovative Therapeutic Approach in Chondrosarcoma: Preclinical Proof of Concept

International audienceTo date, surgery remains the only option for the treatment of chondrosarcoma, which is radio-and chemoresistant due in part to its large extracellular matrix (ECM) and poor vascularity. In case of unresectable locally advanced or metastatic diseases with a poor prognosis, improving the management of chon-drosarcoma still remains a challenge. Our team developed an attractive approach of improvement of the therapeutic index of chemotherapy by targeting proteoglycan (PG)-rich tissues using a quaternary ammonium (QA) function conjugated to mel-phalan (Mel). First of all, we demonstrated the crucial role of the QA carrier for binding to aggrecan by surface plasmon resonance. In the orthotopic model of Swarm rat chondrosar-coma, an in vivo biodistribution study of Mel and its QA derivative (Mel-QA), radiolabeled with tritium, showed rapid radioactivity accumulation in healthy cartilaginous tissues and tumor after [ 3 H]-Mel-QA injection. The higher T/M ratio of the QA derivative suggests some advantage of QA-active targeting of chondrosarcoma. The antitumoral effects were characterized by tumor volume assessment, in vivo 99m Tc-NTP 15-5 scinti-graphic imaging of PGs, 1 H-HRMAS NMR spectroscopy, and histology. The conjugation of a QA function to Mel did not hamper its in vivo efficiency and strongly improved the toler-ability of Mel leading to a significant decrease of side effects (hematologic analyses and body weight monitoring). Thus, QA conjugation leads to a significant improvement of the therapeutic index, which is essential in oncology and enable repeated cycles of chemotherapy in patients with chondrosarcoma