Tamoxifen in Duchenne Muscular Dystrophy

Inclusion Criteria: Group A (ambulant patients) * Documented diagnosis of DMD by mutation analysis in the dystrophin gene or by substantially reduced levels of dystrophin protein (i.e. absent or \<5% of normal) on Western blot or immunostaining * Stable treatment with glucocorticoids \>6 months (no significant change in dosage (\>0.2mg/kg)) at screening; dosing adaptations according to weight change are allowed * Male gender * 6.5 to 12 years of age at time of screening * weight \>20kg * ambulant patients * able to walk at least 350 meters in 6 minute walking distance test without assistance at screening * MFM D1 subdomain of the MFM scale \>40% at screening * Ability to provide informed consent and to comply with study requirements * Patients harbouring a nonsense mutation treatable with the approved drug ataluren should be under stable ataluren treatment for at least 3 months or in case of nontolerance being off ataluren treatment for at least 3 months before screening Group B (non-ambulant patients) * Documented diagnosis of DMD by mutation analysis in the dystrophin gene or by substantially reduced levels of dystrophin protein (i.e. absent or \<5% of normal) on Western blot or immunostaining * Not using glucocorticoids for \>6 months * Male gender * Non-ambulant patients (walking distance less than 10 meters) * 10 to 16 years of age at time of screening * Ability to provide informed consent and to comply with study requirements Open label extension \- Recent participation and completion of TAMDMD study Exclusion Criteria: * Known individual hypersensitivity or allergy to tamoxifen or other ingredients/excipients of IMP * Female gender * Use of tamoxifen or testosterone within the last 3 months * Known or suspected malignancy * Other chronic disease or clinically relevant limitation of renal, liver or heart function * Known or suspected non-compliance * Any injury which may impact functional testing, e.g. upper or lower limb fracture * Planned or expected spinal fusion surgery during the study period (as judged by the Investigator; i.e. due to rapid progressing scoliosis), previous spinal fusion surgery is allowed if it took place more than 6 months prior to screening. * Inability to follow the procedures of the study, e.g. due to language problems, psychological disorders of the participant/parents (as judged by the investigator) * Concomitant participation in any other interventional trial (and up to 3 months prior to screening) * Use of CYP2D6 inhibitors or of CYP3A4 inducers (apart from glucocorticoids), platelet aggregation inhibitors and coumarin-type anti-coagulants * Use of drugs metabolized by CYP2C9, such as phenprocoumon, phenytoin, warfarin, celecoxib, fluvastatin, ginko biloba, St. John's wort and sulfamethoxazol * Galactosemia (lack of galactose-1-phosphat-uridylyltransferase or UDP-galactose-4-epimerase or galactokinase; Fanconi-Bickel-syndrome); congenital lack of lactase; glucose-galactose malabsorption * Presence of one or more of the following eye disorders: cataract, retinopathia, optic neuropathy, alteration of the cornea * Presence of one or more of the following laboratory abnormalities: anaemia, thrombocytopenia, leukopenia, neutropenia or agranulocytosis Group A: * Glucocorticoid naïve patients * Start of glucocorticoid treatment or change in dosage \<6 month prior to screening (dosing adaptations according to weight change are allowed) Group B: * Glucocorticoid treated patients or patients that stopped glucocorticoid treatment \<6 month prior to screening * Assisted ventilation of any kind necessary