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Neuregulin and erbB receptor expression in normal and diseased human white matter.

机译:在正常和患病的人白质中神经调节蛋白和erbB受体的表达。

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摘要

Human white matter from non-neurologic cases, multiple sclerosis (MS) and other neurologic diseases (OND, inflammatory and non-inflammatory), was subjected to immunocytochemistry and Western blotting for expression of the neuregulin, glial growth factor-2 (GGF2), and its receptors, erbB2, erbB3 and erbB4. GGF2 has previously been shown to have mitogenic effects upon oligodendrocytes in vitro and an enhancing effect upon remyelination in animals with autoimmune demyelination. In all types of human white matter examined, expression of the ligand GGF2 and its three receptors was consistently found on oligodendrocytes, with higher levels being seen in cases of MS. Expression was also seen, albeit at lower levels, on astrocytes and microglial cells, the latter most commonly in MS and OND. In human lymph node tissue, some lymphocytes were positive for erbB2, erbB3 and erbB4. Western blots confirmed the presence of all three receptors in normal, MS and OND white matter. GGF2 and erbB receptor expression did not correlate with areas of remyelination and reactivity occurred throughout the tissue, with some increase in intensity at the edge of MS lesions. Examination of precursor oligodendrocyte immunoreactivity (with anti-PDGF-Ralpha and NG2), revealed widespread expression throughout both normal and diseased white matter. The presence of GGF2 and its receptors on oligodendrocytes and lymphocytes render this cell type a candidate for functional signaling via this pathway, perhaps in relationship to myelinating activity.
机译:对来自非神经系统疾病,多发性硬化症(MS)和其他神经系统疾病(OND,炎症性和非炎性疾病)的人类白质进行免疫细胞化学和蛋白质印迹分析,以表达神经调节蛋白,神经胶质生长因子2(GGF2),及其受体erbB2,erbB3和erbB4。先前已证明,GGF2在体外对少突胶质细胞具有促有丝分裂作用,并在具有自身免疫性脱髓鞘作用的动物中对重新髓鞘化具有增强作用。在检查的所有类型的人类白质中,在少突胶质细胞上始终都能发现配体GGF2及其三个受体的表达,在MS病例中水平更高。在星形胶质细胞和小胶质细胞上也可以看到表达,尽管水平较低,后者在MS和OND中最常见。在人淋巴结组织中,一些淋巴细胞对erbB2,erbB3和erbB4呈阳性。 Western印迹证实了正常,MS和OND白质中所有三种受体的存在。 GGF2和erbB受体的表达与髓鞘再生的区域不相关,并且在整个组织中都发生反应,在MS病变边缘的强度有所增加。检查前体少突胶质细胞免疫反应性(与抗PDGF-Ralpha和NG2),发现在正常和患病白质中均广泛表达。少突胶质细胞和淋巴细胞上GGF2及其受体的存在使该细胞类型成为通过该途径进行功能性信号传导的候选者,可能与髓鞘形成有关。

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