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非典型帕金森病的普通神经科医生实用诊断算法:一项共识声明。

A General Neurologist's Practical Diagnostic Algorithm for Atypical Parkinsonian Disorders: A Consensus Statement.

作者信息

Bruno Michiko K, Dhall Rohit, Duquette Antoine, Haq Ihtsham U, Honig Lawrence S, Lamotte Guillaume, Mari Zoltan, McFarland Nikolaus R, Montaser-Kouhsari Leila, Rodriguez-Porcel Federico, Shurer Jessica, Siddiqui Junaid, Spears Christopher C, Wills Anne-Marie A, Diaz Kristophe, Golbe Lawrence I

机构信息

Neuroscience Institute (MKB), The Queen's Medical Center; Medicine (MKB), University of Hawaii, John A Burns School of Medicine, Honolulu; Neurology (RD), University of Arkansas for Medical Sciences, Little Rock; Service de Neurologie (AD), Département de Médecine, Centre Hospitalier de l'Université de Montréal (CHUM), Montreal, Quebec, Canada; Neurology (IUH), University of Miami, FL; Neurology (LSH), Columbia University Irving Medical Center, New York; Neurology (GL), The University of Utah; Neurology (GL), George E. Wahlen Department of Veterans Affairs Medical Center, Salt Lake City, UT; Neurology (NRM), University of Florida, Gainesville; Neurology (LM-K), Brigham and Women Hospital and Harvard Medical School, Boston, MA; Neurology (ZM), Johns Hopkins University, Baltimore, MD; Cleveland Clinic Lou Ruvo Center for Brain Health (ZM), Las Vegas, NV; Neurology (FR-P), Medical University of South Carolina, Charleston; CurePSP (J. Shurer, KD, LIG), New York; Neurological Institute (J. Siddiqui), Cleveland Clinic, OH; Neurology (CCS), University of Michigan, Ann Arbor; Neurology (AMW), Massachusetts General Hospital and Harvard Medical School, Boston; and Neurology (LIG), Rutgers Robert Wood Johnson Medical School, New Brunswick, NJ.

出版信息

Neurol Clin Pract. 2024 Dec;14(6):e200345. doi: 10.1212/CPJ.0000000000200345. Epub 2024 Aug 16.

Abstract

PURPOSE OF REVIEW

The most common four neurodegenerative atypical parkinsonian disorders (APDs) are progressive supranuclear palsy (PSP), multiple system atrophy (MSA), corticobasal syndrome (CBS), and dementia with Lewy bodies (DLB). Their formal diagnostic criteria often require subspecialty experience to implement as designed and all require excluding competing diagnoses without clearly specifying how to do that. Validated diagnostic criteria are not available at all for many of the other common APDs, including normal pressure hydrocephalus (NPH), vascular parkinsonism (VP), or drug-induced parkinsonism (DIP). APDs also include conditions of structural, genetic, vascular, toxic/metabolic, infectious, and autoimmune origin. Their differential diagnosis can be challenging early in the course, if the presentation is atypical, or if a rare or non-neurodegenerative condition is present. This review equips community general neurologists to make an early provisional diagnosis before, or in place of, referral to a tertiary center. Early diagnosis would allay diagnostic uncertainty, allow prompt symptomatic management, provide disease-specific information and support resources, avoid further pointless testing and treatments, and create the possibility of trial referral.

RECENT FINDINGS

We address 64 APDs using one over-arching flow diagram and a series of detailed tables. Most instances of APDs can be diagnosed with a careful history and neurological exam, along with a non-contrast brain MRI. Additional diagnostic tests are rarely needed but are delineated where applicable. Our diagnostic algorithm encourages referral to a tertiary center whenever the general neurologist feels it would be in the patient's best interest. Our algorithm emphasizes that the diagnosis of APDs is an iterative process, refined with the appearance of new diagnostic features, availability of new technology, and advances in scientific understanding of the disorders. Clinicians' proposals for all diagnostic tests for the APDs, including repeat visits, should be discussed with patients and their families to ensure that the potential information to be gained aligns with their larger clinical goals.

SUMMARY

We designed this differential diagnostic algorithm for the APDs to enhance general neurologists' diagnostic skills and confidence and to help them address the less common or more ambiguous cases.

摘要

综述目的

最常见的四种神经退行性非典型帕金森综合征(APD)为进行性核上性麻痹(PSP)、多系统萎缩(MSA)、皮质基底节综合征(CBS)和路易体痴呆(DLB)。其正式诊断标准按设计往往需要专科经验才能实施,且都要求排除其他竞争性诊断,但未明确说明如何进行。许多其他常见的APD,包括正常压力脑积水(NPH)、血管性帕金森综合征(VP)或药物性帕金森综合征(DIP),根本没有经过验证的诊断标准。APD还包括结构、遗传、血管、毒性/代谢、感染和自身免疫性病因引起的疾病。如果临床表现不典型、存在罕见或非神经退行性疾病,或者在病程早期,其鉴别诊断可能具有挑战性。本综述旨在使社区普通神经科医生能够在转诊至三级中心之前或替代转诊进行早期初步诊断。早期诊断可减轻诊断不确定性,实现及时的症状管理,提供疾病特异性信息和支持资源,避免进一步无意义的检查和治疗,并创造试验性转诊的可能性。

最新发现

我们使用一个总体流程图和一系列详细表格来分析64种APD。大多数APD病例通过仔细的病史、神经系统检查以及非增强脑MRI即可诊断。很少需要额外的诊断测试,但在适用的情况下会进行说明。我们的诊断算法鼓励普通神经科医生在认为转诊符合患者最佳利益时将患者转诊至三级中心。我们的算法强调,APD的诊断是一个迭代过程,会随着新诊断特征的出现、新技术的可用性以及对这些疾病科学认识的进步而不断完善。临床医生针对APD的所有诊断测试(包括复诊)的建议都应与患者及其家属讨论,以确保获得的潜在信息与他们更大的临床目标一致。

总结

我们设计了这种APD鉴别诊断算法,以提高普通神经科医生的诊断技能和信心,并帮助他们处理不太常见或更模糊的病例。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7366/11341009/ef44527b958e/CPJ-2023-000602f1.jpg

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