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儿童溶血尿毒综合征伴中枢神经系统受累的早期弥散加权 MRI 模式。

Patterns in early diffusion-weighted MRI in children with haemolytic uraemic syndrome and CNS involvement.

机构信息

Institute of Diagnostic and Therapeutic Neuroradiology, Hannover Medical School, 30623 Hannover, Germany.

出版信息

Eur Radiol. 2012 Mar;22(3):506-13. doi: 10.1007/s00330-011-2286-0. Epub 2011 Oct 8.

DOI:10.1007/s00330-011-2286-0
PMID:21979865
Abstract

OBJECTIVES

Diffusion-weighted imaging (DWI) in children with diarrhoea associated haemolytic uraemic syndrome (D+HUS) and cerebral involvement was evaluated retrospectively.

METHODS

DWI within 24 h of onset of neurological symptoms. The apparent diffusion coefficient (ADC) was measured in grey/white matter and correlated with clinical and laboratory findings.

RESULTS

DWI was abnormal in all. Abnormal ADC was detected in the supratentorial white matter (6/12) and cortex (1/12), the basal ganglia (5/12), the thalami (4/12), and the cerebellum (1/12). ADC was reduced in 5/12, increased in 4/12, and both in 3/12. Mean serum sodium was lower in patients with DWI abnormalities affecting the white matter (6/12), than in those with basal ganglia/thalamic involvement (6/12). Neurological outcome was normal in 4/11 and abnormal in 7/11, and 1 patient died, outcome did not correlate to either localisation or type of DWI abnormality.

CONCLUSIONS

In D+HUS with neurological symptoms, early DWI may reveal abnormal ADC not only in the basal ganglia/thalami, but also in the white matter/cortex. Besides thrombotic microangiopathy, toxic effects of shiga toxin, azotaemia and hyponatraemia / hypoosmolality may be involved in cerebral involvement in children with D+HUS. Findings on early MRI seem not to predict clinical course or outcome.

KEY POINTS

• DWI MR imaging may detect early CNS involvement in haemolytic uraemic syndrome • Different pathogenetical mechanisms may contribute to the CNS disease in HUS • Early MRI findings do not seem to allow prediction of clinical outcome.

摘要

目的

回顾性评估腹泻相关溶血尿毒症综合征(D+HUS)伴脑受累患儿的弥散加权成像(DWI)。

方法

在出现神经症状后 24 小时内进行 DWI。测量灰质/白质的表观扩散系数(ADC),并与临床和实验室发现相关联。

结果

所有患儿的 DWI 均异常。在 12 例患儿中,6 例出现幕上白质(6/12)和皮质(1/12)、5 例基底节(5/12)、4 例丘脑(4/12)和 1 例小脑(1/12)的异常 ADC。ADC 降低见于 5/12 例,升高见于 4/12 例,降低和升高均见于 3/12 例。6 例 DWI 异常影响白质的患儿的血清钠均值低于 6 例基底节/丘脑受累的患儿。11 例患儿中,4 例神经结局正常,7 例异常,1 例死亡,局部化或 DWI 异常类型与结局均无相关性。

结论

在伴神经症状的 D+HUS 中,早期 DWI 不仅可显示基底节/丘脑异常 ADC,还可显示白质/皮质异常 ADC。除血栓性微血管病外,志贺毒素的毒性作用、氮质血症和低钠血症/低渗透压血症可能与 D+HUS 患儿的脑受累有关。早期 MRI 发现似乎无法预测临床病程或结局。

关键点

• DWI MRI 可能可检测到溶血尿毒症综合征的中枢神经系统早期受累。

• 不同的发病机制可能导致 HUS 中的中枢神经系统疾病。

• 早期 MRI 发现似乎不能预测临床结局。

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