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Supervised clustering for TSPO PET imaging

Journal

Publisher

SPRINGER
DOI: 10.1007/s00259-021-05309-z

Keywords

TSPO; PET; Supervised clustering; Pseudo-reference region

Funding

  1. King's College London
  2. National Institute for Health Research (NIHR) Biomedical Research Centre at South London and Maudsley NHS Foundation Trust and King's College London
  3. Intramural Research Program of the National Institute of Mental Health, National Institutes of Health [ZIAMH002852]

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This technical note serves as a practical guide for implementing a supervised clustering algorithm (SVCA) reference region approach in the context of TSPO PET studies, highlighting its strengths and limitations in studying neuroinflammation. The SVCA method offers a non-invasive quantification of TSPO expression by identifying voxels with minimal specific binding in PET images, overcoming limitations of arterial sampling and TSPO contamination in anatomically-defined reference regions. The standardized implementation of SVCA methodology in TSPO PET analysis aims to improve replicability and comparability across study sites.
Purpose This technical note seeks to act as a practical guide for implementing a supervised clustering algorithm (SVCA) reference region approach and to explain the main strengths and limitations of the technique in the context of 18-kilodalton translocator protein (TSPO) positron emission tomography (PET) studies in experimental medicine. Background TSPO PET is the most widely used imaging technique for studying neuroinflammation in vivo in humans. Quantifying neuroinflammation with PET can be a challenging and invasive procedure, especially in frail patients, because it often requires blood sampling from an arterial catheter. A widely used alternative to arterial sampling is SVCA, which identifies the voxels with minimal specific binding in the PET images, thus extracting a pseudo-reference region for non-invasive quantification. Unlike other reference region approaches, SVCA does not require specification of an anatomical reference region a priori, which alleviates the limitation of TSPO contamination in anatomically-defined reference regions in individuals with underlying inflammatory processes. Furthermore, SVCA can be applied to any TSPO PET tracer across different neurological and neuropsychiatric conditions, providing noninvasivequantification of TSPO expression. Methods We provide an overview of the development of SVCA as well as step-by-step instructions for implementing SVCA with suggestions for specific settings. We review the literature on SVCAapplications using first- and second- generation TSPO PET tracers and discuss potential clinically relevant limitations and applications. Conclusions The correct implementation of SVCA can provide robust and reproducible estimates of brain TSPO expression. This review encourages the standardisation of SVCA methodology in TSPO PET analysis, ultimately aiming to improve replicability and comparability across study sites.

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