Mov Disord. 2012 Apr 15;27(5):651-5. doi: 10.1002/mds.25017.
Streffer JR, Grachev ID, Fitzer-Attas C, Gomez-Mancilla B, Boroojerdi B, Bronzova J, Ostrowitzki S, Victor SJ, Fontoura P, Alexander R.
Abstract
Realizing
that 60% to 80% of dopaminergic nigrostriatal neurons are nonfunctional
at the time of clinical diagnosis, there is an emerging consensus that
disease-modifying treatments should be initiated in the earliest stages
of Parkinson's disease (PD). To date, clinical trial designs and
metrics in PD have been focused on motor symptoms as the core feature
of the clinical disease. To identify earlier or "pre-motor" populations
in PD, new markers have been proposed. We address the prerequisites
needed to use these pre-motor markers in clinical trials for the
selection of subjects, definition of populations, and monitoring of
disease progression. This may require the development of new diagnostic
criteria potentially based on non-motor clinical signs, imaging
techniques, or biological features, all requiring discussion in a
regulatory framework. Questions addressed include: Which steps must be
taken to gain a broad consensus in the field from academic opinion
leaders, patient advocacy groups, regulatory bodies, and industry? How
do we prevent the selection of subgroups, which may not be
representative of the full disease spectrum? Is there a way forward in
personalized medicine? How do we balance risk and benefit in an at-risk
population? While many tools are available, a concerted effort is
required to develop integrated data sets, as well as to achieve the
necessary standardization for multicenter clinical trials. To this end,
public-private consortia (including academic centers, patient advocacy
groups, and industry) will be of crucial importance to prospectively
investigate and define the best tools and treatment paradigms. © 2012
Movement Disorder Society.
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