From netrin‐1‐targeted SPECT/CT to internal radiotherapy for management of advanced solid tumors

Author:

Kryza David12ORCID,Wischhusen Jennifer3,Richaud Mathieu34ORCID,Hervieu Maëva34,Sidi Boumedine Jacqueline14,Delcros Jean‐Guy5ORCID,Besse Sophie6,Baudier Thomas7ORCID,Laval Pierre‐Alexandre3,Breusa Silvia134ORCID,Boutault Erwan6,Clermidy Hugo3ORCID,Rama Nicolas3ORCID,Ducarouge Benjamin8ORCID,Devouassoux‐Shisheboran Mojgan9,Chezal Jean‐Michel6ORCID,Giraudet Anne‐Laure2,Walter Thomas3410,Mehlen Patrick3ORCID,Sarrut David7ORCID,Gibert Benjamin34ORCID

Affiliation:

1. Imthernat, LAGEPP, CNRS UMR 5007 Université de Lyon, Hospices Civils de Lyon Lyon France

2. Lumen Nuclear Medicine group, Hospices Civils de Lyon et Centre Léon Bérard Lyon France

3. Apoptosis, Cancer and Development Laboratory‐ Equipe labellisée ‘La Ligue’, LabEx DEVweCAN Institut Convergence PLAsCAN, Centre de Recherche en Cancérologie de Lyon, INSERM U1052‐CNRS 5286, Université de Lyon1 Lyon France

4. Gastroenterology and technologies for health, Centre de Recherche en Cancérologie de Lyon, INSERM U1052‐CNRS5286 Université Lyon 1 Lyon France

5. Small molecules for biological targets, Centre de Recherche en Cancérologie de Lyon. UMR INSERM 1052 – CNRS 5286 ISPB Rockefeller Lyon France

6. Université Clermont Auvergne, Inserm, Imagerie Moléculaire et Stratégies Théranostiques Clermont‐Ferrand France

7. CREATIS, INSA Lyon, INSERM U1206 – CNRS UMR 5220 Université de Lyon Lyon France

8. Netris Pharma Lyon France

9. Hospices Civils de Lyon, Department of Pathology Lyon France

10. Hospices Civils de Lyon, Hôpital Edouard Herriot, Service de Gastroentérologie et d'Oncologie Digestive Lyon Cedex 03 France

Abstract

AbstractTargeted radionuclide therapy is a revolutionary tool for the treatment of highly spread metastatic cancers. Most current approaches rely on the use of vectors to deliver radionuclides to tumor cells, targeting membrane‐bound cancer‐specific moieties. Here, we report the embryonic navigation cue netrin‐1 as an unanticipated target for vectorized radiotherapy. While netrin‐1, known to be re‐expressed in tumoral cells to promote cancer progression, is usually characterized as a diffusible ligand, we demonstrate here that netrin‐1 is actually poorly diffusible and bound to the extracellular matrix. A therapeutic anti‐netrin‐1 monoclonal antibody (NP137) has been preclinically developed and was tested in various clinical trials showing an excellent safety profile. In order to provide a companion test detecting netrin‐1 in solid tumors and allowing the selection of therapy‐eligible patients, we used the clinical‐grade NP137 agent and developed an indium‐111‐NODAGA‐NP137 single photon emission computed tomography (SPECT) contrast agent. NP137‐111In provided specific detection of netrin‐1‐positive tumors with an excellent signal‐to‐noise ratio using SPECT/CT imaging in different mouse models. The high specificity and strong affinity of NP137 paved the way for the generation of lutetium‐177‐DOTA‐NP137, a novel vectorized radiotherapy, which specifically accumulated in netrin‐1‐positive tumors. We demonstrate here, using tumor cell‐engrafted mouse models and a genetically engineered mouse model, that a single systemic injection of NP137‐177Lu provides important antitumor effects and prolonged mouse survival. Together, these data support the view that NP137‐111In and NP137‐177Lu may represent original and unexplored imaging and therapeutic tools against advanced solid cancers.

Funder

Agence Nationale de la Recherche

CNIB

Publisher

Springer Science and Business Media LLC

Subject

Molecular Medicine

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