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雄性金皮小鼠和雌性携带者神经胶质细胞死亡水平的差异。

Differences in levels of neuroglial cell death in jimpy male mice and carrier females.

作者信息

Knapp P E, Dutta S, Skoff R P

机构信息

Department of Anatomy and Cell Biology, Wayne State University, Detroit, Mich.

出版信息

Dev Neurosci. 1990;12(3):145-52. doi: 10.1159/000111844.

Abstract

Jimpy (jp) is an X-linked disorder which results in a variety of glial cell abnormalities and the virtual absence of myelin in the central nervous system (CNS) of affected males. Female heterozygote carriers of the jp gene are mosaics. The wild-type genome will be expressed in roughly half of their cells, while in the other half the jp genome will be expressed. We have exploited this characteristic in order to determine whether the premature oligodendroglial death previously described in jp males is a primary effect of the mutation. Mosaic spinal cords were examined at the light-microscopic level for the presence of pyknotic cells at ages when oligodendroglial death is quite pronounced in jp males. The percentage of pyknotic glial cells (less than 0.6%) is not statistically different in normal and mosaic females at 5 and 30 days. At 14-15 days there is a slight increase in mosaic cords (1.2 vs. 0.75%) but there are still 10 times more dying glia in jp male cords of the same age. The low level of oligodendroglial death in mosaic spinal cords suggests that it is secondary to some other jp abnormality. Small increases in glial death over a protracted period of time could result in lower numbers of oligodendrocytes in older mosaics. Even if this occurs, the data still support the idea that the phenotype of genetically jp cells can be favorably altered by the mosaic environment.

摘要

Jimpy(jp)是一种X连锁疾病,会导致多种神经胶质细胞异常,并且患病男性的中枢神经系统(CNS)中几乎没有髓磷脂。jp基因的女性杂合子携带者是嵌合体。野生型基因组将在其大约一半的细胞中表达,而在另一半细胞中jp基因组将被表达。我们利用这一特性来确定先前在jp雄性中描述的少突胶质细胞过早死亡是否是突变的主要影响。在少突胶质细胞死亡在jp雄性中非常明显的年龄,在光镜水平检查嵌合脊髓中是否存在固缩细胞。在5天和30天时,正常和嵌合雌性中固缩神经胶质细胞的百分比(小于0.6%)在统计学上没有差异。在14 - 15天时,嵌合脊髓中有轻微增加(1.2%对0.75%),但在相同年龄的jp雄性脊髓中,正在死亡的胶质细胞仍然多10倍。嵌合脊髓中少突胶质细胞死亡水平较低表明它是继发于jp的其他一些异常。在较长一段时间内胶质细胞死亡的小幅增加可能导致老年嵌合体中少突胶质细胞数量减少。即使发生这种情况,数据仍然支持这样的观点,即基因上jp细胞的表型可以被嵌合环境有利地改变。

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