4.7 Article

Identifying a whole-brain connectome-based model in drug-naive Parkinson's disease for predicting motor impairment

期刊

HUMAN BRAIN MAPPING
卷 43, 期 6, 页码 1984-1996

出版社

WILEY
DOI: 10.1002/hbm.25768

关键词

brain connectome; motor impairment; Parkinson's disease; predictions; resting-state fMRI

资金

  1. National Natural Science Foundation of China [81971577, 87171888, 82001767, 81771820]
  2. 13th Five-year Plan for National Key Research and Development Program of China [2016YFC1306600]
  3. Natural Science Foundation of Zhejiang Province [LQ21H180008, LQ20H180012]
  4. China Postdoctoral Science Foundation [2021T140599, 2019M662082]
  5. National Natural Science Foundation of China's Major Regional International Cooperation Project [81520108010]
  6. Key Research and Development Program of Zhejiang Province [2020C03020]

向作者/读者索取更多资源

Identifying a whole-brain connectome-based predictive model in drug-naive patients with Parkinson's disease and validating its predictions on drug-managed patients provides insights into the functional underpinnings of motor impairment and brain-behavior associations. The model was effective in predicting individual motor impairment severity in drug-naive patients and demonstrated generalizability in Parkinson's disease patients under long-term drug influence.
Identifying a whole-brain connectome-based predictive model in drug-naive patients with Parkinson's disease and verifying its predictions on drug-managed patients would be useful in determining the intrinsic functional underpinnings of motor impairment and establishing general brain-behavior associations. In this study, we constructed a predictive model from the resting-state functional data of 47 drug-naive patients by using a connectome-based approach. This model was subsequently validated in 115 drug-managed patients. The severity of motor impairment was assessed by calculating Unified Parkinson's Disease Rating Scale Part III scores. The predictive performance of model was evaluated using the correlation coefficient (r(true)) between predicted and observed scores. As a result, a connectome-based model for predicting individual motor impairment in drug-naive patients was identified with significant performance (r(true) = .845, p < .001, p(permu) = .002). Two patterns of connection were identified according to correlations between connection strength and the severity of motor impairment. The negative motor-impairment-related network contained more within-network connections in the motor, visual-related, and default mode networks, whereas the positive motor-impairment-related network was constructed mostly with between-network connections coupling the motor-visual, motor-limbic, and motor-basal ganglia networks. Finally, this predictive model constructed around drug-naive patients was confirmed with significant predictive efficacy on drug-managed patients (r = .209, p = .025), suggesting a generalizability in Parkinson's disease patients under long-term drug influence. In conclusion, this study identified a whole-brain connectome-based model that could predict the severity of motor impairment in Parkinson's patients and furthers our understanding of the functional underpinnings of the disease.

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