Diagnosis of Progressive Multiple Sclerosis From the Imaging Perspective

多发性硬化 医学 磁共振成像 神经影像学 白质 神经退行性变 脊髓 高强度 疾病 进行性疾病 病理 放射科 免疫学 精神科
作者
Massimo Filippi,Paolo Preziosa,Frederik Barkhof,Declan Chard,Nicola De Stefano,Robert J. Fox,Claudio Gasperini,Ludwig Kappos,Xavier Montalbán,Bastiaan Moraal,Daniel S. Reich,Àlex Rovira,Ahmed Toosy,Anthony Traboulsee,Brian G. Weinshenker,Burcu Zeydan,Brenda Banwell,Maria Rocca
出处
期刊:JAMA Neurology [American Medical Association]
卷期号:78 (3): 351-351 被引量:27
标识
DOI:10.1001/jamaneurol.2020.4689
摘要

Although magnetic resonance imaging (MRI) is useful for monitoring disease dissemination in space and over time and excluding multiple sclerosis (MS) mimics, there has been less application of MRI to progressive MS, including diagnosing primary progressive (PP) MS and identifying patients with relapsing-remitting (RR) MS who are at risk of developing secondary progressive (SP) MS. This review addresses clinical application of MRI for both diagnosis and prognosis of progressive MS.Although nonspecific, some spinal cord imaging features (diffuse abnormalities and lesions involving gray matter [GM] and ≥2 white matter columns) are typical of PPMS. In patients with PPMS and those with relapse-onset MS, location of lesions in critical central nervous system regions (spinal cord, infratentorial regions, and GM) and MRI-detected high inflammatory activity in the first years after diagnosis are risk factors for long-term disability and future progressive disease course. These measures are evaluable in clinical practice. In patients with established MS, GM involvement and neurodegeneration are associated with accelerated clinical worsening. Subpial demyelination and slowly expanding lesions are novel indicators of progressive MS.Diagnosis of PPMS is more challenging than diagnosis of RRMS. No qualitative clinical, immunological, histopathological, or neuroimaging features differentiate PPMS and SPMS; both are characterized by imaging findings reflecting neurodegeneration and are also impacted by aging and comorbidities. Unmet diagnostic needs include identification of MRI markers capable of distinguishing PPMS from RRMS and predicting the evolution of RRMS to SPMS. Integration of multiple parameters will likely be essential to achieve these aims.
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