4.7 Article

Substantia Nigra Integrity Correlates with Sequential Working Memory in Parkinson's Disease

Journal

JOURNAL OF NEUROSCIENCE
Volume 41, Issue 29, Pages 6304-6313

Publisher

SOC NEUROSCIENCE
DOI: 10.1523/JNEUROSCI.0242-21.2021

Keywords

basal ganglia; functional MRI; neuromelanin-sensitive MRI; Parkinson's disease; sequential working memory; substantia nigra

Categories

Funding

  1. National Natural Science Foundation of China [31961133025, 31771216]
  2. Shanghai Municipal Science and Technology Major Project [2018SHZDZX05]
  3. Shanghai Municipal Science and Technology Commission [2018ZR1406500]

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In Parkinson's disease, damage to the substantia nigra may lead to deficits in sequential working memory, mediated by dysfunction in the basal ganglia. Patients showed poorer performance in a digitordering task and smaller SNs compared to healthy controls. The study suggests that SN integrity is crucial for sequencing performance in PD patients.
Maintaining and manipulating sequences online is essential for daily activities such as scheduling a day. In Parkinson's disease (PD), sequential working memory deficits have been associated with altered regional activation and functional connectivity in the basal ganglia. This study demonstrates that the substantia nigra (SN) integrity correlated with basal ganglia function and sequencing perform-ance in 29 patients with PD (17 women) and 29 healthy controls (HCs; 18 women). In neuromelanin-sensitive structural magnetic resonance imaging (MRI), PD patients showed smaller SNs than HCs. In a digitordering task with functional MRI (fMRI), partici-pants either recalled sequential digits in the original order (pure recall) or rearranged the digits and recalled the new sequence (reorder and recall). PD patients performed less accurately than HCs, accompanied by the caudate and pallidal hypoactivation, subthalamic hyperactivation, and weakened functional connectivity between the bilateral SN and all three basal ganglia regions. PD patients with larger SNs tended to exhibit smaller ordering-related accuracy costs (reorder and recall vs pure recall). This effect was fully mediated by the ordering-related caudate activation. Unlike HCs, the ordering-related accuracy cost correlated with the ordering-related caudate activation but not subthalamic activation in PD patients. Moreover, the ordering-related caudate activation correlated with the SN area but not with the daily dose of D-2/3 receptor agonists. In PD patients, the daily dose of D-2/3 receptor agonists correlated with the ordering-related subthalamic activation, which was not related to the accuracy cost. The findings suggest that damage to the SN may lead to sequential working memory deficits in PD patients, mediated by basal ganglia dysfunction.

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