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颤抖-营养不良小鼠嵌合体中的周围神经:体内轴突包裹需要非施万细胞成分的证据。

Peripheral nerves in shiverer----dystrophic mouse chimeras: evidence that a non-Schwann cell component is required for axon ensheathment in vivo.

作者信息

Peterson A C

出版信息

J Neurosci. 1985 Jul;5(7):1740-54. doi: 10.1523/JNEUROSCI.05-07-01740.1985.

DOI:10.1523/JNEUROSCI.05-07-01740.1985
PMID:4020418
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6565102/
Abstract

Peripheral nerves in dystrophic mice express multiple axon ensheathment abnormalities. If an intrinsic deficiency expressed within the Schwann cells themselves were to account for this neuropathy, then such cells, existing in a chimera preparation, would be expected to express the same ensheathment abnormalities, whereas a coexisting population of non-dystrophic Schwann cells should not be similarly affected. The genotype of myelinated Schwann cells in shiverer----dystrophic chimera was established with immunocytochemical techniques. Shiverer myelin lacks the P1 component of myelin basic protein (MBP), whereas dystrophic myelin appears to contain normal levels of MBP. No correlation between the ensheathment characteristics of the chimera spinal roots and the genotype of the local Schwann cell population was found; both dystrophic Schwann cell populations expressing normalized ensheathment characteristics and shiverer Schwann cells failing to respond to the local presence of naked axons were observed. These results require that a defective extra Schwann cell component is involved in the pathogenesis of the dystrophic neuropathy. Moreover, the normal realization of that component appears to be a necessary prerequisite for shiverer Schwann cells to achieve full ensheathment competence. Although a definitive identification of the cell type(s) that expresses the dy gene locus has not been achieved in this chimera preparation, the observations are consistent with defective endoneurial fibroblast function.

摘要

营养不良小鼠的外周神经表现出多种轴突包裹异常。如果雪旺细胞自身内在的缺陷是导致这种神经病变的原因,那么在嵌合体标本中的此类细胞预计会表现出相同的包裹异常,而同时存在的非营养不良性雪旺细胞群体不应受到类似影响。采用免疫细胞化学技术确定了颤抖型 - 营养不良嵌合体中有髓雪旺细胞的基因型。颤抖型髓磷脂缺乏髓磷脂碱性蛋白(MBP)的P1成分,而营养不良性髓磷脂似乎含有正常水平的MBP。未发现嵌合体脊髓神经根的包裹特征与局部雪旺细胞群体的基因型之间存在相关性;观察到营养不良性雪旺细胞群体均表现出正常的包裹特征,而颤抖型雪旺细胞对裸露轴突的局部存在无反应。这些结果表明,雪旺细胞外的一种缺陷成分参与了营养不良性神经病变的发病机制。此外,该成分的正常实现似乎是颤抖型雪旺细胞获得完全包裹能力的必要前提。尽管在这种嵌合体标本中尚未明确鉴定出表达dy基因座的细胞类型,但这些观察结果与神经内膜成纤维细胞功能缺陷是一致的。

相似文献

1
Peripheral nerves in shiverer----dystrophic mouse chimeras: evidence that a non-Schwann cell component is required for axon ensheathment in vivo.颤抖-营养不良小鼠嵌合体中的周围神经:体内轴突包裹需要非施万细胞成分的证据。
J Neurosci. 1985 Jul;5(7):1740-54. doi: 10.1523/JNEUROSCI.05-07-01740.1985.
2
Normal basal laminas are realized on dystrophic Schwann cells in dystrophic in equilibrium shiverer chimera nerves.在营养不良性平衡型颤抖嵌合体神经中,正常的基底膜在营养不良性施万细胞上得以实现。
J Cell Biol. 1984 Nov;99(5):1831-7. doi: 10.1083/jcb.99.5.1831.
3
Hypomyelination in the peripheral nervous system of shiverer mice and in shiverer in equilibrium normal chimaera.颤抖小鼠外周神经系统以及平衡正常嵌合体中颤抖小鼠的髓鞘形成不足。
J Comp Neurol. 1984 Aug 10;227(3):348-56. doi: 10.1002/cne.902270305.
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P1 deficiency in shiverer myelin is expressed by Schwann cells in shiverer dystrophic normal mouse chimaera nerves.在颤抖性营养不良正常小鼠嵌合神经中,施万细胞表达了颤抖性髓磷脂中的P1缺乏。
Neurosci Lett. 1983 Jul 29;38(2):163-8. doi: 10.1016/0304-3940(83)90034-4.
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Quantitative studies of the abnormal axon-Schwann cell relationship in the peripheral motor and sensory nerves of the dystrophic mouse.对营养不良小鼠外周运动和感觉神经中轴突-施万细胞异常关系的定量研究。
Brain Res. 1983 Jan 10;258(2):181-96. doi: 10.1016/0006-8993(83)91141-1.
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Quantitative ultrastructural studies of the axon Schwann cell abnormality in spinal nerve roots from dystrophic mice.对营养不良小鼠脊神经根中轴突施万细胞异常的定量超微结构研究。
J Neuropathol Exp Neurol. 1975 Nov;34(6):517-30. doi: 10.1097/00005072-197511000-00006.
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Neural abnormalities in the dystrophic mouse.
J Neurol Sci. 1975 Jun;25(2):249-55. doi: 10.1016/0022-510x(75)90144-6.
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Abnormalities in Schwann cell sheaths in spinal nerve roots of dystrophic mice.营养不良小鼠脊神经根中施万细胞鞘的异常。
J Anat. 1975 Feb;119(Pt 1):169-80.
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Abnormalities expressed in long-term cultures of dorsal root ganglia from the dystrophic mouse.来自营养不良小鼠的背根神经节长期培养物中表达的异常情况。
Brain Res. 1980 Aug 4;194(2):455-70. doi: 10.1016/0006-8993(80)91225-1.
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Ongoing block of Schwann cell differentiation and deployment in dystrophic mouse spinal roots.在营养不良性小鼠脊髓神经根中持续存在施万细胞分化和分布的阻滞。
Brain Res. 1981 Apr;227(2):213-20. doi: 10.1016/0165-3806(81)90109-7.

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J Cell Biol. 1993 Dec;123(5):1223-36. doi: 10.1083/jcb.123.5.1223.