Pharmacological neuromodulation by intracerebroventricular administration of anaerobic dopamine in the treatment of advanced Parkinson's disease

Author:

Devos David1ORCID,Moreau Caroline2,Odou Pascal2,Labreuche Julien3,Demailly Alexandre4,Touzet Gustavo3,Reyns Nicolas2,Gouges Bastien3ORCID,Duhamel Alain3,Barthelemy Christine2,Lannoy Damien2,Carta Natacha2,Palas Benjamin3,Vasseur Michèle3,Marchand Felix2,Ollivier Thomas5,Leclercq Celine3,Potey Camille3,Ouk Thavarak3,Baigne Simon6,Dujardin Kathy7,Carton Louise2,Rolland Anne-Sophie3,Devedjian Jean Christophe8,Foutel Véronique6,Deplanque Dominique5,Fisichella Matthieu6

Affiliation:

1. CHU of Lille, Univ. Lille, Inserm UMRS_1171, Licend, Department of Medical Pharmacology, F-59000 Lille

2. University of Lille

3. CHU of Lille

4. Captech

5. Univeristy of Lille

6. InBrain Pharma

7. Univ. Lille, Inserm, CHU Lille

8. Faculte de Medecine Lille Nord de France University, CHU Lille

Abstract

Abstract

Continuous compensation of cerebral dopamine deficiency represents an ideal treatment for Parkinson's disease. However, dopamine does not cross the digestive and blood-brain barriers, and is rapidly oxidised. The new concept is continuous intra-cerebroventricular administration of anaerobic dopamine (A-dopamine) using a telemetry-controlled subcutaneous abdominal pump connected to a subcutaneous catheter implanted in the third ventricle, near the striatum. A phase I study was conducted showing no serious A-dopamine-induced adverse events in 12 patients, followed by a randomised, controlled, open-label, cross-over, phase II study of 1 month of A-dopamine vs. 1 month of optimised oral antiparkinsonian therapy. The primary endpoint, a blinded assessment of the percentage over the total target (i.e. time with dyskinesia or bradykinesia), recorded by actimetry at home using a wristwatch, was significantly reduced. All expected secondary clinical outcomes were significantly improved, providing the first promising data on the feasibility, safety and efficacy of this new device aided therapy for advanced stage patients. ClinicalTrials.gov identifier:NCT04332276

Publisher

Springer Science and Business Media LLC

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4. Carbidopa-based modulation of the functional effect of the AAV2-hAADC gene therapy in 6-OHDA lesioned rats;Ciesielska A;PLoS One,2015

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