在一个快速进展性痴呆的病例中,CJD的诊断有什么承诺?

Sana Aslam, Mason A Fritz, Laura Cordes, Marwan N Sabbagh
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引用次数: 3

摘要

背景:开发准确诊断朊病毒疾病的方法一直是寻找成功诊断和治疗快速进展性痴呆的挑战。朊病毒疾病很少见。然而,在鉴别诊断时应考虑这些因素。尽管罕见,但其他几种疾病经常被误诊为朊病毒疾病。大多数阿尔茨海默病(AD)和路易体病(LBD)患者也符合克雅氏病(CJD)标准。这两组患者在症状和病理上的相似之处使诊断复杂化,并可能危及患者护理。目前流行的CJD诊断方法缺乏对CJD最终诊断的高度敏感性。在目前所有可用的方法中,实时地震诱发转换(RT-QuIC)分析提供了最高的灵敏度,可以实现准确诊断,并产生早期定量结果。临床病例:一名75岁的妇女患有快速发展的痴呆症,不能排除患有克雅氏病,在神经学中心接受治疗。实验室测试结果、磁共振成像(MRI)、脑脊液(CSF)研究、正电子发射断层扫描(PET)和脑电图(EEG)证明不足以确诊CJD。除了AD、LBD或CJD之外,其他潜在的、但不太可能的病理也可能导致了患者的症状。最终诊断为LBD或朊病毒病。脑部活检证实为海绵状脑病,进一步检查证实为散发性克雅氏病。结论:RT-QuIC诊断CJD的灵敏度高于目前流行的诊断方法,具有较好的应用前景。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

What Promises the CJD Diagnosis in a Case of Rapidly Progressive Dementia?

What Promises the CJD Diagnosis in a Case of Rapidly Progressive Dementia?

What Promises the CJD Diagnosis in a Case of Rapidly Progressive Dementia?

Background: Developing methods for accurately diagnosing prion diseases has been a challenge in the search for successful diagnosis and treatment of rapidly progressive dementia. prion diseases are rare. However, they should be considered in the differential diagnosis. Despite their rarity, several other conditions are often misdiagnosed as prion diseases. Most Alzheimer's (AD) and Lewy Body Disease (LBD) patients also meet Creutzfeldt-Jakob Disease (CJD) criteria. The similarities in symptomology and pathology between these two patient groups complicates diagnosis and can compromise patient care. Prevalent methods for the diagnosis of CJD lack the heightened sensitivity to conclusively detect CJD. Of all currently available methods, real-time quaking induced conversion (RT-QuIC) analysis provides the highest sensitivity necessary to allow for an accurate diagnosis and yields early, quantitative results.

Clinical case: A 75-year-old woman with rapidly progressing dementia, for which CJD could not be ruled out, appeared for care at a neurological center. Laboratory test results, Magnetic Resonance Imaging (MRI), Cerebrospinal Fluid (CSF) studies, Positron Emission Tomography (PET), and an Electroencephalogram (EEG) proved inadequate to confirm CJD. In addition to AD, LBD, or CJD, other potential, yet improbable, pathologies could have caused the patient's symptoms. The patient's diagnosis ultimately was limited to either LBD or prion disease. Spongiform encephalogy was confirmed by a brain biopsy, and further testing confirmed sporadic CJD.

Conclusion: RT-QuIC offers higher sensitivity than currently prevalent diagnostic methods and appears most promising for CJD diagnosis.

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