Deborah Fanfone
University of Mons
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Publication
Featured researches published by Deborah Fanfone.
Medical Oncology | 2017
Deborah Fanfone; Nadège Despretz; Dimitri Stanicki; Jenifer Rubio-Magnieto; Mathieu Fossepre; Mathieu Surin; Sandrine Rorive; Isabelle Salmon; Luce Vander Elst; Sophie Laurent; Robert N. Muller; Sven Saussez; Carmen Burtea
The incidence of papillary thyroid cancer has increased these last decades due to a better detection. High prevalence of nodules combined with the low incidence of thyroid cancers constitutes an important diagnostic challenge. We propose to develop an alternative diagnostic method to reduce the number of useless and painful thyroidectomies using a vectorized contrast agent for magnetic resonance imaging. Galectin-1 (gal-1), a protein overexpressed in well-differentiated thyroid cancer, has been targeted with a randomized linear 12-mer peptide library using the phage display technique. Selected peptides have been conjugated to ultrasmall superparamagnetic particles of iron oxide (USPIO). Peptides and their corresponding contrast agents have been tested in vitro for their specific binding and toxicity. Two peptides (P1 and P7) were selected according to their affinity toward gal-1. Their binding has been revealed by immunohistochemistry on human thyroid cancer biopsies, and they were co-localized with gal-1 by immunofluorescence on TPC-1 cell line. Both peptides induce a decrease in TPC-1 cells’ adhesion to gal-1 immobilized on culture plates. After coupling to USPIO, the peptides preserved their affinity toward gal-1. Their specific binding has been corroborated by co-localization with gal-1 expressed by TPC-1 cells and by their ability to compete with anti-gal-1 antibody. The peptides and their USPIO derivatives produce no toxicity in HepaRG cells as determined by MTT assay. The vectorized contrast agents are potential imaging probes for thyroid cancer diagnosis. Moreover, the two gal-1-targeted peptides prevent cancer cell adhesion by interacting with the carbohydrate-recognition domain of gal-1.
Arthritis Research & Therapy | 2016
Carmen Burtea; Sophie Laurent; Tuba Sanli; Deborah Fanfone; Aude Devalckeneer; Sébastien Sauvage; Marie-Claire Beckers; Sandrine Rorive; Isabelle Salmon; Luce Vander Elst; Bernard Lauwerys; Robert N. Muller
Archive | 2017
Carmen Burtea; Sophie Laurent; Robert N. Muller; Dimitri Stanicki; Deborah Fanfone; Sven Saussez
Archive | 2017
Deborah Fanfone; Dimitri Stanicki; Mathieu Fossepre; Mathieu Surin; Sandrine Rorive; Luce Vander Elst; Sophie Laurent; Robert N. Muller; Sven Saussez; Carmen Burtea
Archive | 2017
Deborah Fanfone; Quentin Paternoster; Dimitri Stanicki; Mathieu Fossepre; Mathieu Surin; Sandrine Rorive; Luce Vander Elst; Sophie Laurent; Robert N. Muller; Sven Saussez; Carmen Burtea
Archive | 2016
Deborah Fanfone; Nadège Despretz; Dimitri Stanicki; Sophie Laurent; Robert N. Muller; Sandrine Rorive; Luce Vander Elst; Sven Saussez; Carmen Burtea
Archive | 2016
Séverine Andre; Emilie Ansciaux; Lionel Larbanoix; Deborah Fanfone; Denis Nonclercq; Luce Vander Elst; Sophie Laurent; Robert N. Muller; Carmen Burtea
Archive | 2016
Deborah Fanfone; Dimitri Stanicki; Mathieu Fossepre; Mathieu Surin; Sandrine Rorive; Luce Vander Elst; Sophie Laurent; Robert N. Muller; Sven Saussez; Carmen Burtea
Archive | 2016
Deborah Fanfone; Dimitri Stanicki; Sophie Laurent; Sandrine Rorive; Sven Saussez; Luce Vander Elst; Robert N. Muller; Carmen Burtea
Archive | 2016
Deborah Fanfone; Nadège Despretz; Dimitri Stanicki; Sophie Laurent; Robert N. Muller; Sandrine Rorive; Luce Vander Elst; Sven Saussez; Carmen Burtea