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BDF1小鼠支持细胞细胞骨架成分的年龄相关变化。

Age-related changes in cytoskeletal components of the BDF1 mouse Sertoli cell.

作者信息

Tanemura K, Kurohmaru M, Kuramoto K, Matsumoto M, Hayashi Y

机构信息

Department of Veterinary Anatomy, Faculty of Agriculture, University of Tokyo.

出版信息

Tissue Cell. 1994 Jun;26(3):447-55. doi: 10.1016/0040-8166(94)90028-0.

Abstract

Age-related changes in mouse Sertoli cell cytoskeletal components (F-actin, vimentin and cytokeratin) were investigated by light and transmission electron microscopy and immunofluorescence using BDF1 mice from 3-33 months of age. In old mice (30 and 33 months of age), the testicular seminiferous epithelia were extremely thin, containing scarce round spermatids and spermatocytes with no elongated spermatids. In these epithelia, the Sertoli cells had lost their polarity and had become flattened. F-actin was detectable at the junction between adjoining Sertoli cells and around the spermatid head in young mice. In old mice, F-actin was distributed at the junction between adjacent Sertoli cells, around the spermatid head, and at the luminal side of the Sertoli cell cytoplasm. Vimentin was detected around the Sertoli cell nucleus and extended into the Sertoli cell trunk towards the tubular lumen in young mice. In old mice testes, however, vimentin was recognized around the Sertoli cell nucleus, but not in the Sertoli cell trunk. Additionally, sheet-like reactions of vimentin, running parallel to the basement membrane, were detected near the luminal surface. Although cytokeratin was not detected in the Sertoli cells of mice until 27 months of age, it was obvious in the extremely thin seminiferous epithelia of older mice. Cytokeratin was randomly distributed within the Sertoli cell cytoplasm. In these Sertoli cells, the expression of vimentin was concurrently detected. Detection of cytokeratin in the extremely thin seminiferous epithelia is one of the most characteristic phenomena of age-related testicular changes in Sertoli cells of older mice.

摘要

利用3至33月龄的BDF1小鼠,通过光学显微镜、透射电子显微镜以及免疫荧光技术,研究了小鼠支持细胞细胞骨架成分(F-肌动蛋白、波形蛋白和细胞角蛋白)随年龄的变化。在老年小鼠(30和33月龄)中,睾丸生精上皮极其薄,含有稀少的圆形精子细胞和精母细胞,没有长形精子细胞。在这些上皮中,支持细胞失去了极性并变得扁平。F-肌动蛋白在年轻小鼠相邻支持细胞之间的连接处以及精子细胞头部周围可检测到。在老年小鼠中,F-肌动蛋白分布在相邻支持细胞之间的连接处、精子细胞头部周围以及支持细胞胞质的管腔侧。波形蛋白在年轻小鼠支持细胞核周围被检测到,并朝着管腔延伸到支持细胞的主干中。然而,在老年小鼠睾丸中,波形蛋白在支持细胞核周围被识别,但在支持细胞主干中未被识别。此外,在管腔表面附近检测到与基底膜平行的波形蛋白片状反应。虽然直到27月龄小鼠的支持细胞中才检测到细胞角蛋白,但在老年小鼠极其薄的生精上皮中很明显。细胞角蛋白随机分布在支持细胞胞质内。在这些支持细胞中,同时检测到波形蛋白的表达。在极其薄的生精上皮中检测到细胞角蛋白是老年小鼠支持细胞与年龄相关的睾丸变化最具特征性的现象之一。

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