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通过生物约束微分方程系统在帕金森病动物模型中模拟联合单胺能耗竭。

Simulating combined monoaminergic depletions in a PD animal model through a bio-constrained differential equations system.

作者信息

Carli Samuele, Brugnano Luigi, Caligiore Daniele

机构信息

Computational and Translational Neuroscience Laboratory, Institute of Cognitive Sciences and Technologies, National Research Council (CTNLab-ISTC-CNR), Rome, Italy.

Entersys s.r.l., Padua, Italy.

出版信息

Front Comput Neurosci. 2024 Aug 23;18:1386841. doi: 10.3389/fncom.2024.1386841. eCollection 2024.

Abstract

INTRODUCTION

Historically, Parkinson's Disease (PD) research has focused on the dysfunction of dopamine-producing cells in the substantia nigra pars compacta, which is linked to motor regulation in the basal ganglia. Therapies have mainly aimed at restoring dopamine (DA) levels, showing effectiveness but variable outcomes and side effects. Recent evidence indicates that PD complexity implicates disruptions in DA, noradrenaline (NA), and serotonin (5-HT) systems, which may underlie the variations in therapy effects.

METHODS

We present a system-level bio-constrained computational model that comprehensively investigates the dynamic interactions between these neurotransmitter systems. The model was designed to replicate experimental data demonstrating the impact of NA and 5-HT depletion in a PD animal model, providing insights into the causal relationships between basal ganglia regions and neuromodulator release areas.

RESULTS

The model successfully replicates experimental data and generates predictions regarding changes in unexplored brain regions, suggesting avenues for further investigation. It highlights the potential efficacy of alternative treatments targeting the locus coeruleus and dorsal raphe nucleus, though these preliminary findings require further validation. Sensitivity analysis identifies critical model parameters, offering insights into key factors influencing brain area activity. A stability analysis underscores the robustness of our mathematical formulation, bolstering the model validity.

DISCUSSION

Our holistic approach emphasizes that PD is a multifactorial disorder and opens promising avenues for early diagnostic tools that harness the intricate interactions among monoaminergic systems. Investigating NA and 5-HT systems alongside the DA system may yield more effective, subtype-specific therapies. The exploration of multisystem dysregulation in PD is poised to revolutionize our understanding and management of this complex neurodegenerative disorder.

摘要

引言

从历史上看,帕金森病(PD)的研究主要集中在黑质致密部中产生多巴胺的细胞功能障碍上,这与基底神经节中的运动调节有关。治疗方法主要旨在恢复多巴胺(DA)水平,显示出有效性,但结果和副作用各不相同。最近的证据表明,PD的复杂性涉及DA、去甲肾上腺素(NA)和血清素(5-HT)系统的紊乱,这可能是治疗效果差异的潜在原因。

方法

我们提出了一个系统层面的生物约束计算模型,全面研究这些神经递质系统之间的动态相互作用。该模型旨在复制实验数据,证明NA和5-HT耗竭在PD动物模型中的影响,从而深入了解基底神经节区域与神经调质释放区域之间的因果关系。

结果

该模型成功复制了实验数据,并对未探索的脑区变化做出了预测,为进一步研究提供了途径。它突出了针对蓝斑和中缝背核的替代治疗的潜在疗效,尽管这些初步发现需要进一步验证。敏感性分析确定了关键的模型参数,为影响脑区活动的关键因素提供了见解。稳定性分析强调了我们数学公式的稳健性,增强了模型的有效性。

讨论

我们的整体方法强调PD是一种多因素疾病,并为利用单胺能系统之间复杂相互作用的早期诊断工具开辟了有前景的途径。同时研究NA和5-HT系统以及DA系统可能会产生更有效、亚型特异性的治疗方法。对PD中多系统失调的探索有望彻底改变我们对这种复杂神经退行性疾病的理解和管理。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f4fa/11378529/9499b33cce83/fncom-18-1386841-g0001.jpg

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