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Are delayed-start design trials to show neuroprotection in Parkinson's disease fundamentally flawed?
Movement disorders, 2008-04, Vol.23 (6), p.784-789
Clarke, Carl E.
2008
Details
Autor(en) / Beteiligte
Clarke, Carl E.
Titel
Are delayed-start design trials to show neuroprotection in Parkinson's disease fundamentally flawed?
Ist Teil von
Movement disorders, 2008-04, Vol.23 (6), p.784-789
Ort / Verlag
Hoboken: Wiley Subscription Services, Inc., A Wiley Company
Erscheinungsjahr
2008
Link zum Volltext
Quelle
Wiley Online Library Journals Frontfile Complete
Beschreibungen/Notizen
Considerable effort has gone into preclinical neuroprotection research in Parkinson's disease (PD) and several large clinical trials have been mounted, but no agent has been conclusively shown to be protective. The latest innovation in PD neuroprotection trial design is the delayed‐start design trial. If patients with early PD do better after 12 to 18 months of immediate drug therapy compared to those in whom it is delayed for 6 to 9 months, this is attributed to a neuroprotective effect. However, delayed‐start design trials may be fundamentally flawed. It has been suggested that physiological mechanisms compensating for the loss of dopaminergic neurones in early PD may be deleterious and that immediate treatment may prevent such mechanisms and thereby be neuroprotective. If this hypothesis is correct, any drug with a symptomatic effect will be neuroprotective in early PD and delayed‐start design trials will show this generic effect, not a neuroprotective effect specific to the drug. Delayed‐start design trials require patients to potentially stay untreated for 6 to 9 months. This may lead to the selection of slowly progressive types of PD, such as that in younger patients and those with tremor‐dominant disease, so the results may not be generalizable to the majority of patients. Delayed‐start design trials are powered to find small differences in total UPDRS score which may not be clinically significant; larger and longer placebo‐controlled trials are required to confirm the clinical significance of their findings. These arguments add to the growing tide of opinion for a fundamental rethink of our policy toward neuroprotection research in PD. © 2008 Movement Disorder Society
Sprache
Englisch
Identifikatoren
ISSN: 0885-3185
eISSN: 1531-8257
DOI: 10.1002/mds.21918
Titel-ID: cdi_proquest_miscellaneous_69159308
Format
–
Schlagworte
Biological and medical sciences
,
Clinical Trials as Topic
,
Degenerative and inherited degenerative diseases of the nervous system. Leukodystrophies. Prion diseases
,
delayed-start design trials
,
Disease Progression
,
Dopamine - physiology
,
Humans
,
Medical sciences
,
Models, Biological
,
Neurology
,
Neurons - physiology
,
neuroprotection
,
Neuroprotective Agents - therapeutic use
,
Parkinson Disease - drug therapy
,
Parkinson Disease - physiopathology
,
Parkinson's disease
,
Research Design - standards
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