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Spreading ɑ-synuclein pathology initiated from the sublaterodorsal tegmental nucleus models RBD followed by Parkinsonian phenotypes in mice

Y. Shen, W.B Yu, B. Shen, H. Dong, J. Zhao, Y. Fan, Y.F Yang, Y.M Sun, Y.L Tang, F.T Liu, JJ. Wu, B.G Xiao, H. Yu, J. Koprich, Z.L Huang, J. Wang (Shanghai, China)

Meeting: MDS Virtual Congress 2020

Abstract Number: 829

Keywords: Alpha-synuclein, Parkinsonism, Rapid eye movement(REM)

Category: Parkinson's Disease: Pathophysiology

Objective:
To recapitulate ɑ-synucleinopathy based RBD-like behaviors in mice which could further proceed to develop Parkinsonian behavioral and histopathological phenotypes.

Background:
Idiopathic REM sleep behavior disorder (RBD), characterized by skeletal muscle atonia loss and dream-enactment behaviors during REM sleep, is proven to be a prodromal biomarker of ɑ-synucleinopathies such as Parkinson’s disease (PD), multiple system atrophy (MSA) and dementia with Lewy body (DLB) [1]. Accumulating clinical and experimental evidence suggests that degeneration or incapacitation of the sublaterodorsal tegmental nucleus (SLD) can lead to RBD phenotypes in human and animals [2-5]. Nevertheless, despite the fact that manipulative incapacitation of the SLD nucleus induces typical RBD-like behaviors in animals, it cannot reflect the synucleinopathy essence of idiopathic RBD and fails to mimic the conversion process of RBD to PD [6, 7].

Method: The study methods were divided into three parts: Part I~III. Firstly, in Part I, we established the preparation protocol of preformed a-syn fibrils (PFFs) and characterized the morphology and beta-sheet structure of PFFs. Then, in Part II, we injected PFFs into mouse SLD nucleus and performed video-polysomnography (PSG) recordings. After the PSG recording, we sacrificed the mice and determined the neuron survival status and a-syn pathology in SLD. At last, in Part III, we performed a battery of Parkinsonian behavioral tests and histopathological studies on the mice that receiving PFFs injection.

Results:
In this study, we demonstrated that the mice receiving PFFs injection displayed typical RBD-like behaviors, accompanying progressive neuron entity loss and pathological ɑ-synuclein aggregation in the SLD. Moreover, the RBD mice gradually proceeded to exhibit Parkinsonian motor & non-motor deficits, concomitant with worsening nigrostriatal degeneration and spreading ɑ-synuclein pathology across the whole brain. Apart from these, we also revealed typical Lewy pathology in the subcoeruleus nucleus of an RBD/PD patient, which provided human tissue-based neuropathological evidence for animal study findings of this study.

Conclusion:
In conclusion, we introduced a synucleinopathy-based RBD modeling strategy, which could not only help to explore the neuropathogenic mechanism of RBD but also be used to develop disease-modifying therapeutics for PD.

References: 1. Högl B, Stefani A, Videnovic A. Idiopathic REM sleep behaviour disorder and neurodegeneration—an update[J]. Nature Reviews Neurology, 2018, 14(1): 40. 2. García-Lorenzo D, Longo-Dos Santos C, Ewenczyk C, et al. The coeruleus/subcoeruleus complex in rapid eye movement sleep behaviour disorders in Parkinson’s disease. Brain, 2013, 136(7): 2120-2129. 3. Valencia Garcia S, Libourel P A, Lazarus M, et al. Genetic inactivation of glutamate neurons in the rat sublaterodorsal tegmental nucleus recapitulates REM sleep behaviour disorder[J]. Brain, 2017, 140(2): 414-428. 4. Lu J, Sherman D, Devor M, et al. A putative flip–flop switch for control of REM sleep[J]. Nature, 2006, 441(7093): 589-594. 5. Krenzer M, Anaclet C, Vetrivelan R, et al. Brainstem and spinal cord circuitry regulating REM sleep and muscle atonia[J]. PloS one, 2011, 6(10): e24998. 6. Peever J, Luppi P H, Montplaisir J. Breakdown in REM sleep circuitry underlies REM sleep behavior disorder[J]. Trends in neurosciences, 2014, 37(5): 279-288. 7. McKenna D, Peever J. Degeneration of rapid eye movement sleep circuitry underlies rapid eye movement sleep behavior disorder[J]. Movement Disorders, 2017, 32(5): 636-644.

To cite this abstract in AMA style:

Y. Shen, W.B Yu, B. Shen, H. Dong, J. Zhao, Y. Fan, Y.F Yang, Y.M Sun, Y.L Tang, F.T Liu, JJ. Wu, B.G Xiao, H. Yu, J. Koprich, Z.L Huang, J. Wang. Spreading ɑ-synuclein pathology initiated from the sublaterodorsal tegmental nucleus models RBD followed by Parkinsonian phenotypes in mice [abstract]. Mov Disord. 2020; 35 (suppl 1). https://www.mdsabstracts.org/abstract/spreading-a-synuclein-pathology-initiated-from-the-sublaterodorsal-tegmental-nucleus-models-rbd-followed-by-parkinsonian-phenotypes-in-mice/. Accessed May 17, 2025.
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