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正常、突变和转基因中枢神经系统的形态计量分析:髓鞘碱性蛋白表达与髓鞘形成的相关性。

Morphometric analysis of normal, mutant, and transgenic CNS: correlation of myelin basic protein expression to myelinogenesis.

作者信息

Shine H D, Readhead C, Popko B, Hood L, Sidman R L

机构信息

Center for Biotechnology, Baylor College of Medicine, Houston, Texas 77030.

出版信息

J Neurochem. 1992 Jan;58(1):342-9. doi: 10.1111/j.1471-4159.1992.tb09316.x.

Abstract

The neurological mutant mice shiverer (shi) and myelin deficient (shimld) lack a functional gene for the myelin basic proteins (MBP), have virtually no myelin in their CNS, shiver, seize, and die early. Mutant mice homozygous for an MBP transgene have MBP mRNA and MBP in net amounts approximately 25% of normal, have compact myelin, do not shiver or seize, and live normal life spans. We bred mice with various combinations of the normal, transgenic, shi, and shimld genes to produce mice that expressed MBP mRNA at levels of 0, 5, 12.5, 17.5, 50, 62.5, and 100% of normal. The CNS of these mice were analyzed for MBP content, tissue localization of MBP, degree of myelination, axon size, and myelin thickness. MBP protein content correlated with predicted MBP gene expression. Immunocytochemical staining localized MBP to white matter in normal and transgenic shi mice with an intensity of staining comparable to the degree of MBP gene expression. An increase in the percentage of myelinated axons and the thickness of myelin correlated with increased gene expression up to 50% of normal. The percentage of myelinated axons and myelin thickness remained constant at expression levels greater than 50%. The presence of axons loosely wrapped with oligodendrocytic membrane in mice expressing lower amounts of MBP mRNA and protein suggested that the oligodendroglia produced sufficient MBP to elicit axon wrapping but not enough to form compact myelin. Mean axon circumference of myelinated axons was greater than axon circumference of unmyelinated axons at each level of gene expression, further evidence that oligodendroglial cells preferentially myelinate axons of larger caliber.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

神经学突变小鼠颤抖鼠(shi)和髓磷脂缺乏鼠(shimld)缺乏髓磷脂碱性蛋白(MBP)的功能基因,其中枢神经系统(CNS)几乎没有髓磷脂,会颤抖、惊厥,并早亡。纯合MBP转基因的突变小鼠,其MBP信使核糖核酸(mRNA)和MBP的净含量约为正常水平的25%,有紧密的髓磷脂,不颤抖也不惊厥,寿命正常。我们将具有正常、转基因、shi和shimld基因的各种组合的小鼠进行杂交,以培育出MBP mRNA表达水平为正常水平0%、5%、12.5%、17.5%、50%、62.5%和100%的小鼠。对这些小鼠的中枢神经系统进行分析,检测MBP含量、MBP的组织定位、髓鞘形成程度、轴突大小和髓磷脂厚度。MBP蛋白含量与预测的MBP基因表达相关。免疫细胞化学染色将MBP定位到正常和转基因shi小鼠的白质中,染色强度与MBP基因表达程度相当。有髓轴突百分比和髓磷脂厚度的增加与基因表达增加相关,直至达到正常水平的50%。在表达水平大于50%时,有髓轴突百分比和髓磷脂厚度保持恒定。在表达较低水平的MBP mRNA和蛋白的小鼠中,存在被少突胶质细胞膜松散包裹的轴突,这表明少突胶质细胞产生了足够的MBP来引发轴突包裹,但不足以形成紧密的髓磷脂。在每个基因表达水平上,有髓轴突的平均轴突周长大于无髓轴突的轴突周长,这进一步证明少突胶质细胞优先使较大口径的轴突形成髓鞘。(摘要截选至250词)

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