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婴儿皮质下囊状脑白质软化症:一种由液体处理障碍引起的独特病理实体。

Infant subcortical cystic leucomalacia: a distinct pathological entity resulting from impaired fluid handling.

机构信息

Department of Neuropathology, John Radcliffe Hospital, Oxford, United Kingdom.

出版信息

Early Hum Dev. 2011 Jun;87(6):421-6. doi: 10.1016/j.earlhumdev.2011.03.003. Epub 2011 Apr 8.

Abstract

BACKGROUND

In the first months of life the subcortical white matter appears prone to fluid accumulation and cystic change. This condition has generally been considered to be due to hypoxic-ischaemic injury (HII) and is grouped with other forms of white matter disease including periventricular leucomalacia (PVL).

AIMS

Our aim was to describe the sequential tissue changes in the formation of subcortical cystic leucomalacia in the infant brain and to delineate this from other forms of white matter disease in order to better understand its pathogenesis and aetiology.

STUDY DESIGN

Standard samples of the frontal lobe, including subcortical white matter, were stained to demonstrate the cellular processes responsible for subcortical cyst formation in infants who had died from global hypoxic-ischaemic injury (HII) and brain swelling. Cases were of infants who had survived for known periods after collapse in order to determine the time course of the pathological changes.

SUBJECTS

20 infants under 5 months of age with global HII and no other primary brain pathology, and who had survived for between 2h and 13 days after collapse.

OUTCOME MEASURES

The description of the sequential changes leading to subcortical cyst formation in infants after severe global HII.

RESULTS

With increasing time of survival after global HII the subcortical white matter became more oedematous. Subcortical cysts were seen after one day but were most common in infants surviving more than 5 days. Cysts were not associated with cellular responses and seemed to be the result of fluid accumulation. The pathology was quite distinct from PVL which is due to tissue necrosis.

CONCLUSIONS

Subcortical leucomalacia results from fluid accumulation and not necrosis. Predisposition to fluid accumulation may be age-related and due to impairment of fluid handling pathways which remain immature in this age group. Potential mechanisms are discussed.

摘要

背景

在生命的最初几个月,皮质下白质似乎容易出现液体积聚和囊性改变。这种情况通常被认为是由于缺氧缺血性损伤(HII)引起的,并与其他形式的白质疾病(包括脑室周围白质软化症[PVL])一起归类。

目的

我们的目的是描述婴儿脑皮质下囊性白质软化形成的连续组织变化,并将其与其他形式的白质疾病区分开来,以便更好地了解其发病机制和病因。

研究设计

对额叶的标准样本(包括皮质下白质)进行染色,以显示在因全球缺氧缺血性损伤(HII)和脑肿胀而死亡的婴儿中导致皮质下囊形成的细胞过程。这些病例是在崩溃后存活了已知时间的婴儿,以确定病理变化的时间过程。

研究对象

20 名年龄在 5 个月以下、无其他原发性脑病理的 HII 婴儿,在崩溃后存活 2 小时至 13 天。

研究结果

随着全球 HII 后存活时间的增加,皮质下白质变得更加水肿。皮质下囊肿在一天后可见,但在存活超过 5 天的婴儿中最常见。囊肿与细胞反应无关,似乎是液体积聚的结果。该病理与由于组织坏死引起的 PVL 完全不同。

结论

皮质下白质软化症是由于液体积聚而不是坏死引起的。液体积聚的易感性可能与年龄有关,并且由于在这个年龄段尚未成熟的液体处理途径受损所致。讨论了潜在的机制。

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