• KSBNS 2024


Original Article

Exp Neurobiol 2021; 30(5): 365-373

Published online October 31, 2021

© The Korean Society for Brain and Neural Sciences

Diffusion Measure Changes of Substantia Nigra Subregions and the Ventral Tegmental Area in Newly Diagnosed Parkinson’s Disease

Jae-Hyuk Shim and Hyeon-Man Baek*

Department of Health Sciences and Technology, GAIHST, Gachon University, Incheon 21999, Korea

Correspondence to: *To whom correspondence should be addressed.
TEL: 82-32-899-6678, FAX: 82-32-899-6677

Received: July 26, 2021; Revised: September 13, 2021; Accepted: September 22, 2021

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License ( which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

Historically, studies have extensively examined the basal ganglia in Parkinson’s disease for specific characteristics that can be observed with medical imaging. One particular methodology used for detecting changes that occur in Parkinson’s disease brains is diffusion tensor imaging, which yields diffusion indices such as fractional anisotropy and radial diffusivity that have been shown to correlate with axonal damage. In this study, we compare the diffusion measures of basal ganglia structures (with substantia nigra divided into subregions, pars compacta, and pars reticula), as well as the diffusion measures of the diffusion tracts that pass through each pair of basal ganglia structures to see if significant differences in diffusion measures can be observed in structures or tracts in newly diagnosed Parkinson’s disease patients. Additionally, we include the ventral tegmental area, a structure connected to various basal ganglia structures affected by dopaminergic neuronal loss and have historically shown significant alterations in Parkinson’s disease, in our analysis. We found significant fractional anisotropy differences in the putamen, and in the diffusion tracts that pass through pairs of both substantia nigra subregions, subthalamic nucleus, parabrachial pigmental nucleus, ventral tegmental area. Additionally, we found significant radial diffusivity differences in diffusion tracts that pass through the parabrachial nucleus, putamen, both substantia nigra subregions, and globus pallidus externa. We were able to find significant diffusion measure differences in structures and diffusion tracts, potentially due to compensatory mechanisms in response to dopaminergic neuronal loss that occurs in newly diagnosed Parkinson’s disease patients.

Keywords: Parkinson’s disease, Basal ganglia, MRI, Diffusion tractography

Basal ganglia structures such as the subthalamic nucleus (STN) and substantia nigra (SN) have been crucial targets for studying Parkinson’s disease (PD). It has been well established that the death of dopaminergic neurons commonly occurs in the substantia nigra of clinical PD patients [1], which in turn contributes to the dysfunction of downstream nigrostriatal pathways (putamen, GPe, STN, GPi/SNr, thalamus, motor cortex) related to movement disorders [2]. However, most reviews reported axonal degeneration starting from 50% of SN dopamine neurons to 70% before motor signs appear, making it vital to detect neuronal loss in the SN before PD diagnosis. Additionally, there are various diseases with similar motor symptoms that are found in PD such as multiple system atrophy and tremor, making it desirable to distinguish PD from other motor diseases by observing biomarkers visible in SN [3, 4]. Examining how SN biomarkers change under treatments such as L-DOPA and deep brain stimulation can help explain the results of experiments regarding the effectiveness of treatments or conflicting results that arise due to side effects of treatments [5, 6].

Diffusion tensor imaging (DTI) has been used as a common MRI sequence to measure diffusion indices such as fractional anisotropy (FA), axial diffusivity (AD), radial diffusivity (RD), and mean diffusivity (MD), which describe random Brownian motion of water molecules. Various studies have shown correlations between significantly low levels of diffusion measures and alterations in white matter microstructural integrity. Increases in RD have been shown to indicate fibers with significant demyelination while healthy, myelinated fibers were shown to have high FA and low RD [7, 8]. Additionally, studies showed that decreased AD can indicate axonal injury, and increased MD can describe microstructural damages that occur in necrosis [9, 10]. As such, many studies have compared diffusion measures between PD patients and healthy controls (HC) to observe whether the death of dopaminergic neurons in SN can be traced to significant changes in diffusion measures [11, 12].

While the focus of diffusion weighted results are generally on white matter tract integrity, diffusion indices have also been used to indicate significant changes in deep gray matter structures in various neurodegenerative disorders. As breakdown of microstructures in grey matter structures occur, certain diffusion indices such as MD can indicate increase in net diffusion due to fewer obstacles impeding diffusion, as opposed to diffusion in a particular direction [13]. Meta-analyses and review articles of PD DTI studies showed that studies were able to find significant changes in diffusion measures of various grey matter structures, particularly in the putamen and the thalamus. While many studies of DTI measures in PD SN, where dopaminergic neuronal loss occurs, were able to find significant differences in DTI measures of PD and HC SN, there were also conflicting results that suggest the use of DTI measures as PD biomarkers may be inconsistent [14].

In order to clarify whether DTI measures can be used for identifying abnormalities of the SN normally found in PD, various studies have attempted to replicate significant differences of DTI measures between PD and HC SN [15]. However, inconsistent results between several studies shifted the scope of finding potential significant DTI differences between SN down to SN subregions particularly in the pars compacta SN subregion (SNc) where the loss of dopaminergic neurons occurs [15, 16]. Most studies showed conflicting results regardless of the comparison between SN subregions, but such issues may have been attributed to inconsistencies in delineating SN into SNc and SNr due to their small size and lack of defining borders [11].

In this study, we compare the fractional anisotropy (FA), quantitative anisotropy (QA), mean diffusivity (MD), axial diffusivity (AD), radial diffusivity (RD), of regions defined by the CIT168 atlas where it is either rich in dopaminergic neurons or is the target of dopaminergic innervation between PD and HC. We delineate structures from the CIT168 atlas such as putamen, caudate, nucleus accumbens (NA), globus pallidus externa (GPe), globus pallidus interna (GPi), substantia nigra pars compacta (SNc), substantia nigra pars reticula (SNr), and subthalamic nucleus (STN) [17]. Additionally, as part of the CIT168 atlas, we delineate parabrachial pigmented nucleus (PBP) and ventral tegmental area (VTA), two structures part of the mesocorticolimbic pathway responsible for reward and motivation. While not directly affected by dopaminergic neuronal loss in the SNc, VTA, and PBP are inspected for significant differences in diffusion measures due to the associated neuronal and morphological changes that can occur in PD VTA and PBP. In addition, we generate diffusion tractography between each segmented structure for comparing DTI measures of white matter tracts that pass through each structure. Assessing diffusion measures of tracts representing pathways affected by PD may show more conclusive evidence of disrupted dopaminergic connectivity.


65 HC and 65 PD subjects used in the preparation of this article were recruited from the Parkinson’s Progression Markers Initiative (PPMI) database ( [18]. For up-to-date information on the study, visit Each PD subject was assessed for PD using Part III of Movement Disorder Society-sponsored revision of the Unified Parkinson’s Disease Rating Scale (MDS-UPDRS III), observation of dopaminergic neurons through dopamine transporter SPECT scans, and displaying motor symptoms such as resting tremor or bradykinesia. Assessment of PD was done before any subjects were administered PD medication that can interfere with PD symptom testing. All subjects involved in this research were tested negative for neurological disorders apart from PD. Group demographics and clinical characteristics are shown in Table 1. All subjects provided written informed consent to share each subject’s unidentified clinical data with investigators.

MRI data acquisition

MRI data of HC and PD subjects used in this study was obtained from the PPMI database ( Diffusion MRI images were acquired using standard protocols on 3T scanners at approximately 11 blinded PPMI imaging sites. T1-weighted images were acquired using 3D T1-weighted MPRAGE sequence (echo time (TE)=90 ms, repetition time (TR)=2,300 ms, 1 mm3 resolution) and DTI images were acquired using 2D single-shot echo-planar DTI sequence (TE=88 ms, TR=900 ms, 2 mm3 resolution, 72 slices, flip angle=90°, 64 gradient directions, b-value=1,000 s/mm2). More details regarding MRI sequence information can be found in the PPMI MRI technical operations manual (

Image processing

Prior to segmentation and diffusion fiber reconstruction, a series of preprocessing steps were performed on each subject’s DTI image to correct for errors such as eddy currents and head motion. Through various programs provided by MRtrix3, DTI images went through denoising (dwidenoise), Gibbs ringing removal (dwidenoise), motion and distortion correction (dwifslreproc), bias field correction (dwibiascorrect), and resampled to 1 mm3 isotropic resolution (mrgrid) [19, 20].

Atlas segmentation of CIT168 structures, putamen, caudate, nucleus accumbens (NA), globus pallidus external (GPe), globus pallidus internal (GPi), substantia nigra pars compacta (SNc), substantia nigra pars reticula (SNr), subthalamic nucleus (STN), parabrachial pigmented nucleus (PBP), ventral tegmental area (VTA), was done through the default Lead-DBS Lead Connectome pathway [21]. First, each subject’s b0 image extracted from DTI images is co-registered to the T1w image using SPM12 ( Following the co-registration, the co-registered T1w images are normalized using a modified version of advanced normalization tools (ANTs) to the MNI ICBM 2009b template space in which the CIT168 atlas is preregistered to. Inverse warps generated from normalization and co-registration are applied on the CIT168 atlas to warp the atlas to the subject’s diffusion space. The quality of each co-registration and normalization were visually inspected using edge detection-based wireframes and atlas segmentations overlaid on top of co-registered images generated by Lead-DBS.

Diffusion processing

Lead Connectome, a MATLAB-based structural connectomic analysis pipeline that utilizes DSI studio for generalized Q-ball imaging (GQI) for reconstruction and deterministic fiber tracking, was used to generate a structural connectome for each subject [22]. 400,000 tracts were generated using a step size of 0.5 mm, an angular threshold of 75°, minimum length of 10 mm, and maximum length of 300 mm. DSI studio’s statistics tool was used to obtain values of diffusion network measures (FA, QA, MD, AD, RD) in segmented CIT168 structures, and the DSI studio’s connectivity matrix tool was used to obtain diffusion network measures of fiber tracts that connect each pair of segmented structures.

Statistical analysis

Group characteristics, age, education years, and MoCA test scores were tested for significant differences using student’s t-test to ensure that group differences of diffusion measures were not influenced by differences of group characteristics. Volumes and diffusion measures of segmented CIT168 structures were compared between all HC and PD using student’s t-test. The Benjamini-Hochberg false discovery rate (FDR) procedure was done on volumetric and diffusion measure comparisons with significance set to p<0.05 to correct for false positives when conducting multiple comparisons. The same methodology using student’s t-test and FDR was done to find significant differences (significance at p<0.05) in diffusion measures of PD and HC diffusion fiber tracts between each segmentation pair.

CIT168 structures that were segmented using PPMI HC and PD diffusion images with Lead-DBS are shown in Fig. 1. Demographics and clinical characteristics of HC and PD subjects were compared for significant differences using student’s t-test. MDS-UPDRS III scores showed significant differences (p<0.001) between HC and PD, as shown in Table 1.

The student’s t-test was used to compare each volume and diffusion measure (FA, QA, MD, AD, RD) of segmented CIT168 structures between HC and PD as shown in Table 2 and Table 3. The Benjamini-Hochberg procedure was used to control for false discovery rate (FDR) with significance set to p<0.05. Structures showed no significant group differences in volume of HC and PD segmentations as shown in Table 2. Structures with significant diffusion measure differences were putamen (FA, MD, AD, RD) and GPi (MD, RD) but post FDR correction showed significant differences were limited to MD and RD of the putamen.

The student’s t-test was also used to compare the diffusion measures (FA, QA, MD, AD, RD) and fiber tract counts of connectivity between each CIT168 structure pair segmented with Lead-DBS. The Benjamini-Hochberg procedure was used to control for false discovery rate (FDR) with significance set to p<0.05. No connectivity pair showed significant differences in fiber tract counts, MD, AD, and QA post FDR correction. Only right hemisphere connectivity pairs showed significant difference between HC and PD diffusion measures. 8 connectivity pairs showed significant differences in FA and 4 connectivity pairs showed significant differences in RD as shown in Table 4.

For our study, we utilized diffusion MRI images to compare diffusion measures of CIT168 structures influenced by the death of dopaminergic neurons. We mainly focused on the significant differences of diffusion measures in SN substructures, SNc and SNr, based on reports of DTI alterations being localized to SNc where the loss of dopaminergic neurons occurs. Additionally, we investigated the diffusion measures of diffusion fiber tracts that passed through pairs of CIT168 structures to observe how diffusion fibers change under PD. Our results revealed that after correcting for false discovery rate, the only structure that showed significant differences in diffusion measures was Putamen. SN substructures with significant diffusion measure differences in diffusion tracts paired with PBP, GPe, GPi, VTA, and putamen.

A significant number of studies on group differences of brain structure diffusion measures have been done to observe DTI changes in PD [14, 15]. Effects of dopamine loss due to death of dopaminergic neurons in SN causing imbalance of several other neurotransmitters in downstream motor systems and other structures have been illustrated through diffusion measure changes [23, 24]. A review paper that compiled multiple different non-hypothesis-driven, diffusion assessments of PD and controls showed multiple instances where studies found correlations between motor symptoms and diffusion measure changes [14]. While the majority of such studies found FA decreases and MD increases in regions that were analyzed, many studies showed that PD subjects had FA increases in the putamen, results which are in line with our significant FA increases in PD right putamen (HC=0.260, PD=0.280, p=0.020) [25, 26]. The putamen is a key structure in the motor system affected by Parkinson’s, as it is directly connected to the SNc through dopaminergic neurons [27]. Additionally, as a result of dopaminergic neuronal loss, projections from the putamen to other basal ganglia structures such as GPe, STN, GPi, and SNr are abnormally altered, causing increased inhibition of downstream signals to structures such as centromedian (CM) and the motor cortex [27]. This in turn reduces the excitatory signals from the CM and the motor cortex to the putamen, which effectively creates a loop of increased motor cortex inhibition signals as putamen is less able to suppress inhibition signals to the motor cortex [28].

While there were significant differences in diffusion measures of the putamen, there were no significant differences in diffusion measures of both SNc and SNr after FDR correction. As the focal point of numerous PD studies, the SN has been a frequent region of interest for finding correlations between dopaminergic neuronal death and change in diffusion measures [14]. Various meta-analyses and reviews reported 2 studies with increased FA in SN, 11 with no significant FA changes, and 19 with significant FA decreases [14, 15]. Therefore, conflicting diffusion measure results have led to further investigation towards the substructures of SN, which consists of the posterior part of SN where dopaminergic neurons are located, referred to as SNc, and the lateral part of SN referred to as SNr [29]. Due to dopaminergic neuronal death being localized to SNc and excitatory signals to SNr being less inhibited by loss of dopamine, it is possible that observing SN as a whole can lead to inconsistencies in significant diffusion measure differences [29]. Despite our results showing significant FA differences in both of the SN subregions, none of the results survived FDR correction. Our results were similar to other previous studies that reported no significant diffusion measure differences in either subregion of SN, but multiple conflicting studies were also able to find significant FA differences in SN subregions [30, 31]. Inconsistencies between results of studies observing SN can be due to multiple factors regarding the type of PD subjects involved in studies and the consistencies between SN segmentations. PPMI subjects involved in the study consist of early diagnosed cases, averaging at 6.4 months of disease duration and consisting of mixed young-onset subjects (age≤50) and standard onset subjects (age>50). A longitudinal study comparing FA of brain structures between types of PPMI subjects involving young onset, young controls, old onset, and old controls showed that young-onset subjects had significantly higher FA in multiple brain structures than young controls while older onset subjects had significantly lower FA in SN than old controls [14]. As such, the mixture of subject ages, duration of disease, and diagnosis could have influenced how significant the FA differences were in the subregions of SN.

In our analysis of diffusion measures of basal ganglia diffusion tractography, we found several diffusion tracts that pass through pairs of basal ganglia structures with significant differences in FA and RD. Tractography that passed through pair combinations of basal ganglia structures, SNc, SNr, PBP, and VTA showed FA increases in PD subjects, and tractography that passed through PBP and either putamen, GPe, or SNc showed RD decreases in PD subjects (SNc, SNr, p=0.035; SNc, STN, p=0.021; SNc, PBP, p=0.021; SNc, VTA, p=0.035; SNr, PBP, p=0.021; SNr, VTA, p=0.021; STN, PBP, p=0.037; PBP, VTA, p=0.037). Diffusion tractography has been used prominently for detecting connectivity between regions of interest by simulating a rough estimate of white matter tracts through the diffusion of water [32]. As such, PD studies have utilized diffusion tractography to identify significant changes in tractography that might reflect the disruption of dopaminergic connectivity and its effects on the basal ganglia [33, 34]. Reports of significant decreases in FA of diffusion tractography have been consistent throughout various studies, particularly in the nigrostriatal tract that connects the SN to the putamen via dopaminergic neurons [14, 33, 34]. However, our results showed no significant FA differences in tracts with any basal ganglia structure that pairs with the putamen, and the pairs of basal ganglia structures (SNc, SNr, PBP, VTA) that did show significant FA differences were FA increases rather than the commonly reported FA decreases. There are several possible explanations for significant FA increases, including inflammation from dopaminergic neuronal loss and compensatory responses to structural connectivity changes [35]. VTA and PBP are part of the mesocorticolimbic reward and motivation system, which involves the A10 group of dopaminergic neurons situated laterally to the A9 group of dopaminergic neurons stemming from SNc [36]. Neurons passing through VTA have been shown to be connected to structures that are also connected to SNc, and albeit at a slower rate, degenerate in PD similarly to SNc dopaminergic neurons [37]. Due to its close location from SNc, diffusion tracts that are shown to pass through VTA, PBP with SNc may show increased FA due to elevated levels of oxidative stress and neuroinflammation from dopamine degradation [38-40]. Another potential explanation for the FA increase in VTA, PBP connectivity is enhanced activation of bidirectional neurons from the striatum to the VTA due to a disrupted regulatory system reliant on dopamine signaling [41].

RD, which measures the diffusivity perpendicular to the tract, has been historically used for detecting demyelination and inflammation. An increase in RD has been correlated with demyelinated axons, as well as increased motor and memory dysfunctions [42, 43]. However, our results using the PPMI dataset showed significantly decreased PD RD in tracts passing through the PBP, SNr, SNc, Putamen, and GPe (putamen, SNr, p=0.041; putamen, PBP, p=0.034; GPe, PBP, p=0.040; SNc, PBP, p=0.034). Similar to our seemingly conflicting results regarding FA increases in PD diffusion tracts, the decrease in RD can be attributed to neural compensatory mechanisms observed in PD patients at the early stages of diagnosis. A study comparing diffusion measures of diffusion tracts in PD patients with early and progressive stages of PD showed that the lower RD observed in early PD patient white matter tracts became more comparable to that of HC white matter tracts at later stages of the disease [44]. The study suggests that the initial decreases of RD in PD were from compensations from dopaminergic deficiency which slowly phases out due to worsened symptoms and expended neural resources as the disease progresses, resulting in increased RD of white matter tracts [44].

There are various limitations of the methods used in the study that could have significantly affected the results. First, the PPMI data used in this study were acquired from 11 different sites, with their locations blinded for subject confidentiality, and potentially with different MRI vendors. While quality check from PPMI and preprocessing steps for diffusion images were done to correct for possible inhomogeneities that can arise due to different scanners, it is possible that our results were significantly affected regardless. Second, the normalization and coregistration methods used for atlas-based segmentations in the Lead-DBS pipeline while utilizes algorithms shown to have high dice-coefficient when segmenting the STN and GPi, may have minor inaccuracies in segmenting other regions of the basal ganglia. While all segmentations through this method were checked visually, it is possible that certain regions had minor inaccuracies, which could significantly affect DTI metrics due to the small size of the segmentations. Third, certain regions, such as VTA, PBP, and the inner boundaries of the two SN substructures, SNc and SNr do not express boundaries in T1w and diffusion weighted images. As such, visual inspection of such structures are limited to their general location given by the CIT168 atlas.

In this study, we were able to utilize the Lead-DBS segmentation pipeline and DSI studio diffusion tractography pipeline to compare diffusion measures of basal ganglia structures and the tracts that pass through the structures. We were able to find significant FA differences in the putamen, then find significant FA differences in tracts covering basal ganglia structures involved in PD, such as VTA, PBP, SNc, SNr, and STN. Our findings showed that similar to other studies on PD patients at earlier stages of the disease, the tracts passing through basal ganglia had significant diffusion measure differences that were contradictory to studies with PD at more advanced stages of the disease, likely due to compensatory mechanisms that slowly get weaker as the disease progresses. Future longitudinal studies on PD patients will be necessary to verify whether the pattern of diffusion measure changes in diffusion tracts as the disease progresses also occur in VTA and PBP diffusion tracts.

This research was supported by Brain Research Program through the National Research Foundation of Korea (NRF) funded by the Ministry of Science and ICT (NRF-2017M3C7A1044367).

Fig. 1. Basal ganglia segmentation involved in Parkinson’s disease. Left represents segmentations overlaid on top of MNI template, right represents an example segmentation of a PD subject used in this study (Patient 3127), overlaid on the same subject’s T1w image. Structures segmented are left and right putamen, caudate, nucleus accumbens (NA), globus pallidus externus (GPe), globus pallidus internus (GPi), substantia nigra pars compacta (SNc), substantia nigra pars reticula (SNr), subthalamic nucleus (STN), parabrachial pigmented nucleus (PBP), ventral tegmental area (VTA).
Table. 1.

Group characteristics of PD and HC

GroupHC (n=65)PD (n=65)p-value
Age (mean±SD)58.7±11.160.5±9.60.316
Sex (male/female)44/2143/22
Dominant side (left/right)27/38
Education years (mean±SD)15.5±3.015.2±3.10.186
Age onset (years)58.4±10.2
Duration of disease (months)6.4±6.9
Total levodopa equivalent daily dose547.0±264.0
MoCA (mean±SD)28.3±1.227.7±1.80.509
MDS-UPDRS III Score (mean±SD)0.7±1.719.5±8.9<0.001

HC, healthy controls; PD, parkinson’s disease; SD, standard deviation; MoCA, Montreal Cognitive Assessment Test Scoring; MDS-UPDRS III, Movement Disorder Society-sponsored revision of the Unified Parkinson’s Disease Rating Scale.

Table. 2.

Volumetric differences of HC and PD basal ganglia, PBP, VTA segmentations

HC volumeL4,697.144,475.98412.98781.88436.6348.28475.05265.08221.18122.38
PD volumeL4,857.184,689.72429.86801.26452.1849.22497.63274.35233.11127.18

Comparison of average volume (in mm3) between ROIs segmented using HC (healthy control) images and PD (Parkinson’s disease) images. Each comparison was done through a t-test, and corrected for false positives through FDR correction. p-values shown in this table are p-values adjusted from FDR correction. No significant differences (p<0.05) were found between control volumes and patient volumes.

Table. 3.

Diffusion measure differences of the PD and HC basal ganglia, VTA, PBP


Nucleus accumbensL0.0530.0590.2070.2180.7980.8080.9560.9800.7180.722
Globus pallidus externalL0.0320.0350.3330.3510.7130.7270.9590.9920.5900.594
Globus pallidus internalL0.0480.0480.4250.4290.6870.6991.0061.0290.5270.534
Substantia Nigra pars compactaL0.0610.0600.4350.4500.7780.7781.1501.1630.5920.586
Substantia Nigra pars reticularL0.0670.0660.5560.5680.7560.7561.2411.2570.5150.506
Subthalamic nucleusL0.0560.0550.5200.5210.7060.6881.1051.0830.5070.491
Parabrachial pigmented nucleusL0.0590.0550.4450.4410.7120.7121.0481.0390.5440.549
Ventral tegmental areaL0.0770.0720.4700.4750.7330.7061.0861.0540.5560.532

Average diffusion measures of left and right basal ganglia structures. Significant differences and p-values were calculated using student t-tests, with p-values adjusted for multiple corrections using FDR correction. Bolded values represent diffusion measures with significant difference (p<0.05), values with asterisk represent measures with significant difference after FDR correction. FA, Fractional Anisotropy; QA, Quantitative Anisotropy; MD, Mean Diffusivity; AD, Axial Diffusivity; RD, Radial Diffusivity.

Table. 4.

Diffusion measures of diffusion connectivity between segmented structures with significant differences

RegionsHC averagesPD averagesp





All regions in this table are right hemisphere structures. HC and PD averages represent averages of diffusion measures FA and RD. p-values in this table are FDR corrected.

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