The Reconfiguration Pattern of Individual Brain Metabolic Connectome for Parkinson's Disease Identification

Background: Positron Emission Tomography (PET) with 18F-fluorodeoxyglucose (18F-FDG) reveals metabolic abnormalities in Parkinson's disease (PD) at a systemic level. Previous metabolic connectome studies derived from groups of patients have failed to identify the individual neurophysiological details. We aim to establish an individual metabolic connectome method to characterize the aberrant connectivity patterns and topological alterations of the individual-level brain metabolic connectome and their diagnostic value in PD. Methods: The 18F-FDG PET data of 49 PD patients and 49 healthy controls (HCs) were recruited. Each individual's metabolic brain network was ascertained using the proposed Jensen-Shannon Divergence Similarity Estimation (JSSE) method. The intergroup difference of the individual's metabolic brain network and its global and local graph metrics were analyzed to investigate the metabolic connectome's alterations. The identification of the PD from HC individuals was used by the multiple kernel support vector machine (MK-SVM) to combine the information from connection and topological metrics. The validation was conducted using the nest leave-one-out cross-validation strategy to confirm the performance of the methods. Results: The proposed JSSE metabolic connectome method showed the most involved metabolic motor networks were PUT-PCG, THA-PCG, and SMA pathways in PD, which was similar to the typical group-level method, and yielded another detailed individual pathological connectivity in ACG-PCL, DCG-PHG and ACG pathways. These aberrant functional network measures exhibited an ideal classification performance in the identifying of PD individuals from HC individuals at an accuracy of up to 91.84%.
Comment: 9 figures