Diffusion Kurtosis Imaging Detects Microstructural Changes in a Methamphetamine-Induced Mouse Model of Parkinson's Disease

Arab, A.; Rudá-Kučerová, J.; Minsterová, A.; Dražanová, Eva; Szabó, N.; Starčuk jr., Zenon; Rektorová, I.; Khairnar, A.

doi:https://dx.doi.org/10.1007/s12640-019-00068-0

Number of the records: 1

Diffusion Kurtosis Imaging Detects Microstructural Changes in a Methamphetamine-Induced Mouse Model of Parkinson's Disease

To the basket
RIV
DOI
WOS
SCOPUS
PUBMED
Bookmark
1.
0511376 - ÚPT 2020 RIV US eng J - Journal Article
Arab, A. - Rudá-Kučerová, J. - Minsterová, A. - Dražanová, Eva - Szabó, N. - Starčuk jr., Zenon - Rektorová, I. - Khairnar, A.
Diffusion Kurtosis Imaging Detects Microstructural Changes in a Methamphetamine-Induced Mouse Model of Parkinson's Disease.
Neurotoxicity Research. Roč. 36, č. 4 (2019), s. 724-735. ISSN 1029-8428. E-ISSN 1476-3524
R&D Projects: GA MŠMT(CZ) EF16_013/0001775; GA MŠMT(CZ) LM2015062; GA MŠMT ED0017/01/01
Institutional support: RVO:68081731
Keywords : behaviour * diffusion kurtosis imaging * methamphetamine * mice * MRI * Parkinson's disease * tract-based spatial statistics
OECD category: Neurosciences (including psychophysiology
Impact factor: 2.992, year: 2019
Method of publishing: Limited access
https://link.springer.com/article/10.1007%2Fs12640-019-00068-0

Methamphetamine (METH) abuse is known to increase the risk of Parkinson's disease (PD) due to its dopaminergic neurotoxicity. This is the rationale for the METH model of PD developed by toxic METH dosing (10 mg/kg four times every 2 h) which features robust neurodegeneration and typical motor impairment in mice. In this study, we used diffusion kurtosis imaging to reveal microstructural brain changes caused by METH-induced neurodegeneration. The METH-treated mice and saline-treated controls underwent diffusion kurtosis imaging scanning using the Bruker Avance 9.4 Tesla MRI system at two time-points: 5 days and 1 month to capture both early and late changes induced by METH. At 5 days, we found a decrease in kurtosis in substantia nigra, striatum and sensorimotor cortex, which is likely to indicate loss of DAergic neurons. At 1 month, we found an increase of kurtosis in striatum and sensorimotor cortex and hippocampus, which may reflect certain recovery processes. Furthermore, we performed tract-based spatial statistics analysis in the white matter and at 1 month, we observed increased kurtosis in ventral nucleus of the lateral lemniscus and some of the lateral thalamic nuclei. No changes were present at the early stage. This study confirms the ability of diffusion kurtosis imaging to detect microstructural pathological processes in both grey and white matter in the METH model of PD. The exact mechanisms underlying the kurtosis changes remain to be elucidated but kurtosis seems to be a valuable biomarker for tracking microstructural brain changes in PD and potentially other neurodegenerative disorders.
Permanent Link: http://hdl.handle.net/11104/0301656

Number of the records: 1