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Alkoxyamines: toward a new family of theranostic agents against cancer.

作者信息

Moncelet Damien, Voisin Pierre, Koonjoo Neha, Bouchaud Véronique, Massot Philippe, Parzy Elodie, Audran Gérard, Franconi Jean-Michel, Thiaudière Eric, Marque Sylvain R A, Brémond Paul, Mellet Philippe

机构信息

CRMSB, CNRS-UMR-5536, Université Victor Segalen Bordeaux 2 , 146 rue Léo Saignat, Case 93, 33076 Bordeaux Cedex, France.

出版信息

Mol Pharm. 2014 Jul 7;11(7):2412-9. doi: 10.1021/mp5001394. Epub 2014 Jun 17.

DOI:10.1021/mp5001394
PMID:24936972
Abstract

Theranostics combines therapeutic and diagnostic or drug deposition monitoring abilities of suitable molecules. Here we describe the first steps of building an alkoxyamine-based theranostic agent against cancer. The labile alkoxyamine ALK-1 (t(1/2) = 50 min at 37 °C) cleaves spontaneously to generate (1) a highly reactive free alkyl radical used as therapeutic agents to induce cell damages leading to cell death and (2) a stable nitroxide used as contrast agent for Overhauser-enhanced magnetic resonance imaging (OMRI). The ALK-1 toxicity was studied extensively in vitro on the glioblastoma cell line U87-MG. Cell viability appeared to be dependent on ALK-1 concentration and on the time of the observation following alkoxyamine treatment. For instance, the LC50 at 72 h was 250 μM. Data showed that cell toxicity was specifically due to the in situ released alkyl radical. This radical induced oxidative stress, mitochondrial changes, and ultimately the U87 cell apoptosis. The nitroxide production, during the alkoxyamine homolysis, was monitored by OMRI, showing a progressive MRI signal enhancement to 6-fold concomitant to the ALK-1 homolysis. In conclusion, we have demonstrated for the first time that the alkoxyamines are promising molecules to build theranostic tools against solid tumors.

摘要

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