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Journal of Peking University(Health Sciences) ›› 2019, Vol. 51 ›› Issue (4): 769-774. doi: 10.19723/j.issn.1671-167X.2019.04.031

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Superficial siderosis of the central nervous system caused by myxopapillary ependymoma of conus medullaris and cauda equine: a case report and literature review

Li XU1,Ming-jie HU2,Yu-yu LI1,Hong-dang QU1,Wei-dong QIAN1,Xiao-lin LIU1,()   

  1. 1. Department of Neurology, The First Affiliated Hospital of Bengbu Medical College, Bengbu 233004, Anhui, China
    2. School of Life Sciences, Bengbu Medical College, Bengbu 233020, Anhui, China
  • Received:2018-08-24 Online:2019-08-18 Published:2019-09-03
  • Contact: Xiao-lin LIU E-mail:xuli197292@126.com
  • Supported by:
    Supported by the Humanities and Social Science Research Program of Anhui University(SK2018A0181)

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Abstract:

Superficial siderosis of the central nervous system (SSCNS) is a rare disorder caused by hemosiderin deposits in the subpial layers of the brain and spinal cord due to prolonged or recurrent low-grade bleeding into the cerebrospinal fluid (CSF). Central nervous system tumor could be one of the sources of bleeding. Some problems exist at present regarding the diagnosis and treatment of SSCNS in China. On account of fewer cases, the insufficient awareness of the condition, and the lack of long-term follow-up data, enough attention has not been paid to etiological diagnosis. The speculative high rate of missed diagnoses of SSCNS indicates a great disparity in the treatment from the world’s advanced level. Related data of clinical and basic research need to accumulate as soon as possible to promote the clinical diagnosis and treatment of the disease. The progressive neurological deficits are involved in the typical clinical manifestations of SSCNS with a triad of bilateral symmetrical sensorineural hearing loss, cerebellar ataxia and signs of corticospinal tract dysfunction. Nevertheless, there are few patients with the triad signs at the same time, which lead to a delayed diagnosis or misdiagnosis. Detection of this disease was commonly post-mortem until the advent of MRI with signal and location characteristics, which made diagnosis easier. Siderosis appears as a hypointense rim covering the surface of the cerebellum, the brain stem, the spinal cord, similar to a black pencil line, thin on SE-T2-weighted images, thick and cons-picuous on GE-T2-weighted images or on susceptibility-weighted imaging (SWI). The only effective way of treating the disorder is to identify the source of bleeding and remove it. MR examination is useful for seeking a source of bleeding too. Therefore, once superficial siderosis is considered, lesions of the central nervous system must be searched using MRI of the brain and spine. We report here a 37-year-old male diagnosed of SSCNS with the classical clinical symptoms of cerebellar ataxia, sensorineural hearing loss and myelopathy. T2-weighed MRI showed characteristic marginal hypo-intensity around the central nervous system. Etiological explorations revealed a large conus medullaris / cauda equina ependymoma filling the lumbosacral spinal canal, a myxopapillary ependymoma (MPE) confirmed by surgical resection and histopathological examination. The related literature was reviewed to ascertain the mechanism of SSCNS secondary to MPE, and to discuss the pathogenesis, clinical features, diagnosis and treatment of SSCNS. This paper aims to improve the awareness of SSCNS and diagnostic level, and to lay stress on the etiological explorations that is beneficial to the development of exact treatment plan.

Key words: Superficial siderosis of central nervous system, Myxopapillary ependymoma, Magnetic resonance imaging

CLC Number: 

  • R739.4

Figure 1

T2-weighted brain MR images showed that the linear hypointensity was seen along the cerebellar folia, vermis, interhemispheric fissure,the cord surface and around the midbrain, pons (A-C, arrowheads); Susceptibility weighted imaging demonstrated the low outline clearly along the cerebellar vermis, interhemispheric fissure and around the medulla, pons more and midbrain prominently (D-G, arrows)"

Figure 2

The lobulated intradural mass in the T12-S1 spinal canal: A and B: Sagittal T1-weighted MR image showed a lobulated predominantly isointense intradural mass filling the spinal canal (arrows); Hyperintensity was seen at the margins of the tumor lobulations (arrowheads);The conus was indistinct. C: Sagittal T2-weighted MR image showed a lobulated predominantly hyperintense intradural mass filling the spinal canal (arrows); Hypointense hemorrhage was seen in the region of the conus mcdullaris (arrowheads).D: Sagittal contrast-enhanced T1-weighted MR image showed heterogeneous enhancement of the mass (arrows)"

Figure 3

Tumor cells distributed as individual or in small groups.Cell nucleus tend to be round or overall in shape and part of them structured in adenoid or papillary, with a mount of mucus around the cells and in the glandular cavity(HE ×400)"

Table 1

Characteristics of patients with SSCNS caused by myxopapillary ependymoma"

Characteristic Patient no.
1 2 3 4 5 6 7 8
Reference (Pikis et al,
2014)		 (Grech et al,
2013)		 (Spengos
et al, 2007)		 (Vibert et al,
2004)		 (Messori
et al, 2004)		 (Lemmerling
et al, 1998)		 (Friedman
et al, 1998)		 Current
report
Age at diagnosis/years 33 64 63 55 65 50 21 37
Gender Male Female Male Female Male Male Male Male
Duration of symptoms before diagnosis 1.5 years 5 years 10 years 20 years 5 years 6 weeks 3 years
Primary tumor L1-L2 L2 L2-L3 L1-S1 L2-L4 L2-L3 L1-S1 L1-S1
Clinical features
Primary symptom Back pain Back pain Gait instability Hearing loss Hearing loss Hearing loss Urinary/fecal
incontinence		 Hearing
loss
Back pain + + N N N N + +
Sensorineural hearing loss Sudden/left Progressive/
bilateral		 Progressive/
bilateral		 Sudden/right,
Progressive/
left		 Bilateral Progressive/
bilateral		 Cranial nerves
were normal		 Progressive/
bilateral
Gait ataxia - ++ ++ ++ ++ ++ - +
Limb ataxia - + ++ N ++ ++ N +
Nystagmus N N N + ++ N N +
Pyramidal tract signs N N ++ N ++ N + +
Sensation impairment of legs N N ++ N ++ N + +
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