Abstract
Opioid peptides are involved in various pathophysiological processes, including algesia, epilepsy, and drug dependence. A strong association between l-DOPA-induced dyskinesia (LID) and elevated prodynorphin mRNA levels has been established in both patients and in animal models of Parkinson's disease, but to date the endogenous prodynorphin peptide products have not been determined. Here, matrix-assisted laser desorption ionization (MALDI) imaging mass spectrometry (IMS) was used for characterization, localization, and relative quantification of striatal neuropeptides in a rat model of LID in Parkinson's disease. MALDI IMS has the unique advantage of high sensitivity and high molecular specificity, allowing comprehensive detection of multiple molecular species in a single tissue section. Indeed, several dynorphins and enkephalins could be detected in the present study, including dynorphin A(1–8), dynorphin B, α-neoendorphin, MetEnkRF, MetEnkRGL, PEnk (198–209, 219–229). IMS analysis revealed elevated levels of dynorphin B, α-neoendorphin, substance P, and PEnk (220–229) in the dorsolateral striatum of high-dyskinetic animals compared with low-dyskinetic and lesion-only control rats. Furthermore, the peak-intensities of the prodynorphin derived peptides, dynorphin B and α-neoendorphin, were strongly and positively correlated with LID severity. Interestingly, these LID associated dynorphin peptides are not those with high affinity to κ opioid receptors, but are known to bind and activate also μ- and Δ-opioid receptors. In addition, the peak intensities of a novel endogenous metabolite of α-neoendorphin lacking the N-terminal tyrosine correlated positively with dyskinesia severity. MALDI IMS of striatal sections from Pdyn knockout mice verified the identity of fully processed dynorphin peptides and the presence of endogenous des-tyrosine α-neoendorphin. Des-tyrosine dynorphins display reduced opioid receptor binding and this points to possible novel nonopioid receptor mediated changes in the striatum of dyskinetic rats. Because des-tyrosine dynorphins can only be detected by mass spectrometry, as no antibodies are available, these findings highlight the importance of MALDI IMS analysis for the study of molecular dynamics in neurological diseases.
Highlights
The abbreviations used areL-DOPA, L-3,4-dihydroxy-phenylalanine; dihydroxy benzoic acid (DHB), 2,5-dihydroxybenzoic acid; 6-OHDA, 6-hydroxydopamine; AIM, Abnormal involuntary movements; aNeo, Alpha-neoendorphin; caudate putamen (CPu), Caudate putamen; DA, Dopamine; dynorphin B (DynB), Dynorphin B; imaging mass spectrometry (IMS), Imaging mass spectrometry; KOPr, MOPr, DOPr, kappa -, mu -, delta-opioid receptor; LID, L-DOPA-induced dyskinesia; LC-ESI FTICR mass tolerance (MS), Liquid chromatography-electrospray Fourier transform mass spectrometry; matrix-assisted laser desorption ionization (MALDI), Matrix-assisted laser desorption/ionization; PD, Parkinson’s disease; PPE, Preproenkephalin; PDyn, Prodynorphin; PEnk, Proenkephalin; RIA, Radioimmunoassay; regions of interest (ROI), Regions of interest; Statistical Analysis of Microarray data” (SAM), Statistical analysis of microarray data; SP, Substance P
L-DOPA-induced Dyskinesia is Associated with Regional Increase of Striatal Dynorphin Peptides as Elucidated by Imaging Mass Spectrometry*□S
Evidence point to a fundamental disturbance of the basal ganglia function induced by the loss of dopamine (DA) and that leads to the facilitation of dyskinogenesis in Parkinson’s disease (PD) [1]
Summary
L-DOPA, L-3,4-dihydroxy-phenylalanine; DHB, 2,5-dihydroxybenzoic acid; 6-OHDA, 6-hydroxydopamine; AIM, Abnormal involuntary movements; aNeo, Alpha-neoendorphin; CPu, Caudate putamen; DA, Dopamine; DynB, Dynorphin B; IMS, Imaging mass spectrometry; KOPr, MOPr, DOPr, kappa -, mu -, delta-opioid receptor; LID, L-DOPA-induced dyskinesia; LC-ESI FTICR MS, Liquid chromatography-electrospray Fourier transform mass spectrometry; MALDI, Matrix-assisted laser desorption/ionization; PD, Parkinson’s disease; PPE, Preproenkephalin; PDyn, Prodynorphin; PEnk, Proenkephalin; RIA, Radioimmunoassay; ROI, Regions of interest; SAM, Statistical analysis of microarray data; SP, Substance P. Prodynorphin mRNA and FosB-related protein levels were both elevated in the medial striatum in animals exhibiting rotational locomotive activity [21]. Because of this distinct regional protein and peptide expression patterns related to behavior it is important to study molecular correlates of LID using advanced imaging techniques that offer high molecular specificity. In the present study we investigated region-specific expression of striatal neuropeptides in the rat model of LID and PD using matrixassisted laser desorption and ionization (MALDI) imaging mass spectrometry (IMS; Fig. 1A). This is the first report of a MALDI IMS-based statistical interrogation of pathophysiological changes in endogenous neuropeptide levels in the mammalian brain
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