February 2025
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30 Reads
Cell Communication and Signaling
Animal models are crucial for elucidating the pathological mechanisms underlying Parkinson’s disease (PD). Unfortunately, most of transgenic mouse models fail to manifest pathological changes observed in PD patients, pending the advancement of PD research. However, the mechanism underlying this discrepancy remains elusive. Here, we provide compelling evidence that the compensatory expression of synaptotagmin-11 (Syt11) plays a key role in concealing PD-associated phenotypes in parkin knockout (KO) mouse models. Unlike the normal dopamine (DA) release and motor behaviors observed in parkin KO mice, parkin knockdown (KD) in the substantia nigra pars compacta (SNpc) in adult mice led to both the impaired DA release and the pronounced motor deficits. Interestingly, Syt11, a well-established parkin substrate involved in PD, was specifically upregulated in parkin KD mice and in parkin KO mice during the suckling stage, but not in adult parkin KO mice. Importantly, the overexpression of Syt11 alone is capable of inducing PD-like motor and non-motor impairments, as well as the impaired DA release and reuptake, which is essential for parkin-associated pathogenesis of PD. Therefore, this work not only elucidate a compensatory mechanism that accounts for the absence of overt PD phenotypes in parkin KO mice, but also contribute to the comprehensive understanding of the progression of PD, opening new avenues for the therapeutic treatment of PD. Supplementary Information The online version contains supplementary material available at 10.1186/s12964-025-02037-x.
![SNI mouse model shows pain and anxiodepression-like behaviors
a, Statistics of thermal pain response of Sham and SNI mice (Sham, n = 7; SNI, n = 8 mice). b, Representative tracking maps in the OFT (upper) and EPM (lower) tests of Sham and SNI mice. c, Statistics of locomotion of Sham and SNI mice (Sham, n = 8; SNI, n = 8 mice). d-f, Statistics of the dark-light box (DLB, d), sucrose preference test (SPT, e), and forced swimming test (FST, f) of Sham (n = 7) and SNI (n = 8 for DLB, n = 7 for SPT and FST) mice. g, Sample traces (left) and statistics (right) of current injection-evoked APs of lateral VTADA neurons of TH-GFP mice 6 weeks after SNI (Sham, n = 8; SNI, n = 10 cells from 3 pairs of mice). h, Schematic of the CFE recordings of DA release in the NAc and the mPFC. Left, schematic of the CFE recording of DA release in the NAc. Right, schematic of the injection of Cre-dependent chemogenetic activation virus (DIO-hM3Dq) in the VTA of TH-Cre mice and CFE recording of DA release in the mPFC in response to CNO. i, Sample traces (Iamp and current integration) and statistics of DA release in response to CNO application (100 μ\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$${\rm{\mu }}$$\end{document}M, 7 s) in the mPFC 6 weeks after SNI (Sham, n = 5; SNI, n = 6 slices from 3 pairs of mice). j, Statistics of OFT behavior of SNI (n = 7) versus Sham (n = 7) mice 7 days after SNI surgery. k, Statistics of VTADA neuron firing rate of SNI versus Sham mice 7 days after SNI surgery (Sham, n = 12 neurons from 3 mice; SNI, n = 11 neurons from 3 mice). The data are presented as the mean ± s.e.m. Unpaired Student’s t-test, *P < 0.05, **P < 0.01, ***P < 0.001. Detailed statistics information can be found in the Source Data.
Source data](https://www.researchgate.net/profile/Changhe-Wang/publication/377114612/figure/fig1/AS:11431281259968821@1720753310470/SNI-mouse-model-shows-pain-and-anxiodepression-like-behaviors-a-Statistics-of-thermal_Q320.jpg)
