Genetic heterogeneity of early onset Parkinson disease: The dilemma of clinico-genetic correlation.

IF 3.1 3区 医学 Q2 CLINICAL NEUROLOGY Parkinsonism & related disorders Pub Date : 2024-09-16 DOI:10.1016/j.parkreldis.2024.107146
Roopa Rajan, Vikram V Holla, Nitish Kamble, Ravi Yadav, Pramod Kumar Pal
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Abstract

With advances in genetic testing increasing proportion of early onset Parkinson disease (EOPD) are being identified to have an underlying genetic aetiology. This is can be in the form of either highly penetrant genes associated with phenotypes with monogenic or mendelian inheritance patterns or those genes known as risk factor genes which confer an increased risk of PD in an individual. Both of them can modify the phenotypic manifestation in a patient with PD. This improved knowledge has helped in deciphering the intricate role of various cellular pathways in the pathophysiology of PD including both early and late and even sporadic PD. However, the phenotypic and genotypic heterogeneity is a major challenge. Different deleterious alterations in a same gene can result in a spectrum of presentation spanning from juvenile to late onset and typical to atypical parkinsonism manifestation. Similarly, a single phenotype can occur due to abnormality in two or more different genes. This conundrum poses a dilemma in the clinical approach and in understanding the clinico-genetic correlation. Understanding the clinico-genetic correlation carries even more importance especially when genetic testing is either not accessible or affordable or in many regions both. In this narrative review, we aim to discuss briefly the approach to various PARK gene related EOPD and describe in detail the clinico-genetic correlation of individual type of PARK gene related genetic EOPD with respect to their classical clinical presentation, pathophysiology, investigation findings and treatment response to medication and surgery.

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早发帕金森病的遗传异质性:临床与遗传相关性的困境。
随着基因检测技术的进步,越来越多的早发性帕金森病(EOPD)被发现有潜在的遗传病因。其形式可以是与单基因遗传或孟德尔遗传模式的表型相关的高渗透基因,也可以是那些被称为风险因子基因的基因,这些基因会增加个体患帕金森病的风险。这两种基因都能改变帕金森病患者的表型表现。这些知识的提高有助于破译各种细胞通路在帕金森病病理生理学中的复杂作用,包括早期和晚期帕金森病,甚至散发性帕金森病。然而,表型和基因型的异质性是一大挑战。同一基因的不同有害改变可导致从幼年到晚期发病、从典型到不典型的帕金森病表现谱。同样,两种或多种不同基因的异常也可能导致单一表型的出现。这一难题给临床方法和理解临床-遗传相关性带来了困境。尤其是当基因检测无法获得或负担不起,或在许多地区两者兼而有之时,理解临床-基因相关性就显得更为重要。在这篇叙述性综述中,我们旨在简要讨论各种 PARK 基因相关 EOPD 的治疗方法,并详细描述与 PARK 基因相关的各种遗传性 EOPD 在经典临床表现、病理生理学、检查结果以及药物和手术治疗反应方面的临床-遗传相关性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Parkinsonism & related disorders
Parkinsonism & related disorders 医学-临床神经学
CiteScore
6.20
自引率
4.90%
发文量
292
审稿时长
39 days
期刊介绍: Parkinsonism & Related Disorders publishes the results of basic and clinical research contributing to the understanding, diagnosis and treatment of all neurodegenerative syndromes in which Parkinsonism, Essential Tremor or related movement disorders may be a feature. Regular features will include: Review Articles, Point of View articles, Full-length Articles, Short Communications, Case Reports and Letter to the Editor.
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