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首页> 外文期刊>Neurology: Official Journal of the American Academy of Neurology >AlphaB-crystallin immunolocalization yields new insights into inclusion body myositis (see comments)
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AlphaB-crystallin immunolocalization yields new insights into inclusion body myositis (see comments)

机译:AlphaB-crystallin immunolocalization收益率新洞察包涵体肌炎(见注释)

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OBJECTIVE: To study the expression of the small heat shock protein, alphaB-crystallin (alphaBC), in inclusion body myositis (IBM). BACKGROUND: In humans, alphaBC is constitutively expressed in the eye lens, muscle, and heart, but not in lymphoid tissues. Induced expression of alphaBC occurs under metabolic stress, in virus-infected lymphocytes, and in degenerative brain lesions, including neurofibrillary tangles and senile plaques in AD. The previously reported pathologic similarities between AD and IBM prompted us to study alphaBC expression in IBM. METHODS: Immunolocalization of alphaBC in muscle of 11 patients with IBM, 50 patients with other muscle diseases, and 4 controls; and quantitative analysis of the frequency of fibers with 1) increased alphaBC expression in IBM and polymyositis and 2) structural abnormality (vacuolated, non-necrotic and invaded by mononuclear cells, Congo red-positive, SMI-31 positive, and ubiquitin positive) in IBM. RESULTS: We detected enhanced expression of alphaBC not only in all structurally abnormal IBM fibers, but also, and with severalfold higher frequency, in IBM fibers without significant structural abnormality (X fibers) (p values in paired t-tests < 0.001). We also found enhanced alphaBC in abnormal fibers in other diseases; X fibers, however, were extremely sparse or absent, except in two atypical cases of polymyositis refractory to immunotherapy. CONCLUSION: That the X fibers are much more frequent than the structurally abnormal fibers in IBM points to a pathogenic stressor acting upstream to the development of structural abnormalities. The identification of this stressor is now of paramount importance for deciphering the enigma of IBM.
机译:目的:研究小的表达热休克蛋白,alphaB-crystallin (alphaBC),包涵体肌炎(IBM)。人类,alphaBC持续表达目镜、肌肉和心脏,但不是淋巴组织。在代谢压力下,发生在病毒感染淋巴细胞,在退行性脑损伤,包括神经原纤维缠结和老年斑块在广告。广告和IBM促使我们之间的相似之处在IBM研究alphaBC表达式。Immunolocalization肌肉的alphaBC 11IBM,患者50例其他肌肉疾病,4控制;分析纤维的频率与1)在IBM和alphaBC表达增加多肌炎和2)结构异常(有液泡的、非坏死性和入侵单核细胞,刚果red-positive SMI-31积极、IBM和泛素阳性)。结果:我们发现增强的表现IBM alphaBC不仅在所有结构异常纤维,而且,高几倍频率,在IBM纤维不显著纤维结构异常(X) (p值配对t < 0.001)。alphaBC异常纤维在其他疾病;然而,纤维非常稀疏或缺席,除了两个典型多肌炎的病例耐火材料免疫疗法。X纤维更频繁在IBM指向一个结构异常纤维致病性上游的压力作用结构异常的发展。这个压力是现在的的识别至关重要的破译谜IBM的。

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