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Antiphospholipid antibodies and cerebellar ataxia: A clinical analysis and literature review

机译:抗磷脂抗体与小脑性共济失调的临床分析及文献复习

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摘要

Background: Although it has been established that antiphospholipid antibodies (APAbs) bind to and modulate the signaling of cerebellar neurons in vitro, the clinical correlation between increased APAbs and cerebellar ataxia has rarely been investigated. Methods: We reviewed 10 patients presenting with cerebellar ataxia with increased blood APAbs from our database along with 3 APAb-associated cerebellar ataxia patients in the literature. Results: Of these 10 patients, 4 exhibited a subacute onset of progressive ataxia, and there were no significant structural changes in their brains that appeared to be responsible for the symptoms. Another 6 showed a chronic course of ataxia, and shared similar morphological changes that included symmetrical lesions in bilateral hemispheres, periventricular lucency and central and temporal atrophy of varying severity; the cerebellum was spared. The predominant APAbs for subacute and chronic ataxia were the anti-beta2-glycoprotein I antibody and anticardiolipin antibody, respectively. Cancer was found in 1 patient with subacute ataxia and in 4 with chronic ataxia. The removal of the cancer, the plasmapheresis and immunosuppressive therapy successfully abolished the ataxia and increased APAb levels in all 5 patients. Conclusions: The relation between APAbs and nonvascular neurological disorders, such as cerebellar ataxia, should be further studied. APAbs may mediate neurological deficits via different mechanisms such as structural damage or functional neurotoxicity. Clinically, the examination of blood APAb levels is recommended for patients with cerebellar ataxia without a determined cause, and the further survey of systemic cancers in the case of APAb positivity is also recommended. Finally, plasmapheresis is a reasonable and effective treatment for APAb-associated cerebellar ataxia.
机译:背景:尽管已经确定抗磷脂抗体(APAbs)可以在体外结合并调节小脑神经元的信号传导,但很少研究增加的APAbs与小脑性共济失调之间的临床相关性。方法:我们从文献中回顾了10例伴有血液APAb增加的小脑性共济失调患者以及3例与APAb相关的小脑性共济失调患者。结果:在这10例患者中,有4例表现为亚急性进行性共济失调,大脑中没有明显的结构变化,似乎与症状有关。另外6例表现出慢性共济失调,并具有相似的形态变化,包括双侧半球对称性病变,脑室透明性和严重程度不同的中央和颞部萎缩。小脑得以幸免。亚急性和慢性共济失调的主要APAb分别是抗β2-糖蛋白I抗体和抗心磷脂抗体。亚急性共济失调患者1例,慢性共济失调患者4例。癌症的清除,血浆置换和免疫抑制疗法成功地消除了共济失调,所有5例患者的APAb水平均升高。结论:APAbs与非血管性神经系统疾病如小脑性共济失调之间的关系应进一步研究。 APAb可能通过不同的机制(例如结构性损伤或功能性神经毒性)介导神经功能缺损。临床上,建议对无确定原因的小脑共济失调患者进行血液APAb水平检查,并建议对APAb阳性的全身性癌症进行进一步检查。最后,血浆置换术是治疗APAb相关性小脑共济失调的一种合理有效的方法。

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