酪氨酸羟化酶
内科学
内分泌学
内侧前脑束
多巴胺
纹状体
帕金森病
病变
医学
黑质纹状体通路
胶质纤维酸性蛋白
心理学
病理
黑质
多巴胺能
疾病
免疫组织化学
作者
Ella A. Kasanga,Isabel Soto,Ashley Centner,Robert McManus,Marla K. Shifflet,Walter Navarrete,Yoonhee Han,Jerome Lisk,Toni Ehrhardt,Kate Wheeler,Isha Mhatre-Winters,Jason R. Richardson,Christopher Bishop,Vicki A. Nejtek,Michael F. Salvatore
标识
DOI:10.1016/j.expneurol.2024.114875
摘要
Alleviation of motor impairment by aerobic exercise (AE) in Parkinson's disease (PD) patients points to activation of neurobiological mechanisms that may be targetable by therapeutic approaches. However, evidence for AE-related recovery of striatal dopamine (DA) signaling or tyrosine hydroxylase (TH) loss has been inconsistent in rodent studies. This ambiguity may be related to the timing of AE intervention in relation to the status of nigrostriatal neuron loss. Here, we replicated human PD at diagnosis by establishing motor impairment with >80% striatal DA and TH loss prior to initiating AE, and assessed its potential to alleviate motor decline and restore DA and TH loss. We also evaluated if serum levels of neurofilament light (NfL) and glial fibrillary acidic protein (GFAP), biomarkers of human PD severity, changed in response to AE. 6-hydroxydopamine (6-OHDA) was infused unilaterally into rat medial forebrain bundle to induce progressive nigrostriatal neuron loss over 28 days. Moderate intensity AE (3× per week, 40 min/session), began 8–10 days post-lesion following establishment of impaired forelimb use. Striatal tissue DA, TH protein and mRNA, and serum levels of NfL/GFAP were determined 3-wks after AE began. Despite severe striatal DA depletion at AE initiation, forelimb use deficits and hypokinesia onset were alleviated by AE, without recovery of striatal DA or TH protein loss, but reduced NfL and GFAP serum levels. This proof-of-concept study shows AE alleviates motor impairment when initiated with >80% striatal DA loss without obligate recovery of striatal DA or TH protein. Moreover, the AE-related reduction of NfL and GFAP serum levels may serve as objective blood-based biomarkers of AE efficacy.
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