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施万细胞合成α7β1整合素,其对于外周神经发育和髓鞘形成并非必需。

Schwann cells synthesize alpha7beta1 integrin which is dispensable for peripheral nerve development and myelination.

作者信息

Previtali S C, Dina G, Nodari A, Fasolini M, Wrabetz L, Mayer U, Feltri M L, Quattrini A

机构信息

Neuropathology Unit, San Raffaele Scientific Institute, Milan, Italy.

出版信息

Mol Cell Neurosci. 2003 Jun;23(2):210-8. doi: 10.1016/s1044-7431(03)00014-9.

Abstract

Defects in laminins or laminin receptors are responsible for various neuromuscular disorders, including peripheral neuropathies. Interactions between Schwann cells and their basal lamina are fundamental to peripheral nerve development and successful myelination. Selected laminins are expressed in the endoneurium, and their receptors are developmentally regulated during peripheral nerve formation. Loss-of-function mutations have confirmed the importance and the role of some of these molecules. Here we show for the first time that another laminin receptor, alpha7beta1 integrin, previously described only in neurons, is also expressed in Schwann cells. The expression of alpha7 appears postnatally, such that alpha7beta1 is the last laminin receptor expressed by differentiating Schwann cells. Genetic inactivation of the alpha7 subunit in mice does not affect peripheral nerve formation or the expression of other laminin receptors. Of note, alpha7beta1 is not necessary for basal lamina formation and myelination. Nonetheless, these data taken together with the previous demonstration of impaired axonal regrowth in alpha7-null mice suggest a possible Schwann cell-autonomous role for alpha7 in nerve regeneration.

摘要

层粘连蛋白或层粘连蛋白受体的缺陷是包括周围神经病变在内的各种神经肌肉疾病的病因。雪旺细胞与其基膜之间的相互作用对于周围神经发育和成功髓鞘形成至关重要。特定的层粘连蛋白在内皮中表达,并且它们的受体在周围神经形成过程中受到发育调控。功能丧失突变证实了其中一些分子的重要性和作用。在这里,我们首次表明另一种层粘连蛋白受体α7β1整合素,以前仅在神经元中描述过,也在雪旺细胞中表达。α7的表达在出生后出现,因此α7β1是分化中的雪旺细胞表达的最后一种层粘连蛋白受体。小鼠中α7亚基的基因失活不影响周围神经形成或其他层粘连蛋白受体的表达。值得注意的是,α7β1对于基膜形成和髓鞘形成不是必需的。尽管如此,这些数据与先前在α7基因敲除小鼠中轴突再生受损的证明一起表明α7在神经再生中可能具有雪旺细胞自主作用。

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