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生长激素在Chang肝癌细胞GERL中的结合与内化的免疫细胞化学证明。

Immunocytochemical demonstration of the binding and internalization of growth hormone in GERL of Chang hepatoma cells.

作者信息

Wang J J, Chang J P, Teng C S

机构信息

Department of Biology and Anatomy, National Defense Medical Center, Taipei, Taiwan, Republic of China.

出版信息

Cell Tissue Res. 1990 Nov;262(2):273-81. doi: 10.1007/BF00309882.

Abstract

The binding and internalization of endogenous growth hormone in Chang hepatoma cells were localized on the cell surface and in the Golgi-endoplasmic reticulum-lysosome (GERL) area by various indirect immunocytochemical labeling techniques, namely, peroxidase or colloidal gold conjugated to secondary antibody, and avidin-biotin complex methods. Rabbit antiserum and monoclonal antibodies raised against HPLC-purified porcine growth hormone were used in this study. In fixed material, antigen-antibody complexes were found to be homogeneously distributed along the cell membrane. Control groups showed negative binding on the cell surface. Trypsin treatment before immunolabeling removed antibody binding completely, but hyaluronidase was ineffective. Pretreatment of lectins did not block the recognition of primary antibody to antigen molecules on cell surface. Internalization of the antigen-antibody peroxidase or gold complexes was demonstrated in the cells, which were immunolabeled at 4 degrees C, and then reincubated for 0-30 min at 37 degrees C before fixation. After reincubation, the internalized ligand complexes were found in vesicles near the cell surface or in the GERL area near the Golgi apparatus which, however, did not label for peroxidase. These findings suggest that the trypsin-sensitive growth hormone, specifically bound and internalized into Chang hepatoma cells, is localized in the GERL instead of the Golgi apparatus and might be involved in the mechanism of tumor cell growth.

摘要

通过各种间接免疫细胞化学标记技术,即与二抗偶联的过氧化物酶或胶体金以及抗生物素蛋白-生物素复合物方法,在内源性生长激素与Chang肝癌细胞的结合和内化过程中,发现其定位于细胞表面以及高尔基体-内质网-溶酶体(GERL)区域。本研究使用了针对高效液相色谱纯化的猪生长激素产生的兔抗血清和单克隆抗体。在固定材料中,抗原-抗体复合物沿细胞膜呈均匀分布。对照组在细胞表面显示阴性结合。免疫标记前用胰蛋白酶处理可完全消除抗体结合,但透明质酸酶无效。凝集素预处理并未阻断一抗对细胞表面抗原分子的识别。在4℃进行免疫标记,然后在37℃再孵育0 - 30分钟后固定的细胞中,证明了抗原-抗体过氧化物酶或金复合物的内化。再孵育后,在内化的配体复合物存在于细胞表面附近的囊泡中或高尔基体附近的GERL区域中,然而,这些区域并未标记上过氧化物酶。这些发现表明,对胰蛋白酶敏感的生长激素特异性结合并内化进入Chang肝癌细胞,定位于GERL而非高尔基体,可能参与肿瘤细胞生长机制。

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