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在Balb/c 3T3成纤维细胞中,CD44蛋白水平及其生物学活性受血清因子调控,也受ras基因转化的影响,但不受sis癌基因转化的影响。

CD44 protein levels and its biological activity are regulated in Balb/c 3T3 fibroblasts by serum factors and by transformation with the ras but not with the sis oncogene.

作者信息

Kogerman P, Sy M S, Culp L A

机构信息

Department of Molecular Biology and Microbiology, Case Western Reserve University School of Medicine, Cleveland, Ohio 44106, USA.

出版信息

J Cell Physiol. 1996 Nov;169(2):341-9. doi: 10.1002/(SICI)1097-4652(199611)169:2<341::AID-JCP13>3.0.CO;2-C.

DOI:10.1002/(SICI)1097-4652(199611)169:2<341::AID-JCP13>3.0.CO;2-C
PMID:8908201
Abstract

CD44s (standard isoform) levels and hyaluronan-binding activity were investigated in Balb/c 3T3 cells and their derivatives transformed with ras or sis oncogenes as a function of serum concentration in the medium. 3T3 cells contained low levels of CD44 and did not bind hyaluronan when grown in medium containing 0.5 or 10% serum. In 5% serum, however, the cells had much higher levels of CD44 and were able to bind hyaluronan. CD44 levels also increased in 3T3 cells restimulated with either 5 or 10% serum after prior maintenance in low serum. In cells restimulated with 5% serum, high levels of CD44 were sustained for at least 72 hr. In cells restimulated with 10% serum, however, the increase in CD44 levels reverted by 48 hr. Transformation of 3T3 cells with ras (but not with sis) oncogene rendered CD44 levels insensitive to serum modulation: ras-transformed cells contained high levels of CD44 and bound hyaluronan at all serum concentrations and at all time points tested. Sis-transformed cells behaved like 3T3 cells in these modulatory changes. Platelet-derived growth factor (PDGF), when supplementing 0.5% serum, mimicked the effects of serum on the levels and hyaluronan-binding capacity of CD44 in 3T3 cells and the CD44-upregulating activity of serum was neutralized by incubation with anti-PDGF antibodies. These data demonstrate that serum factors, specifically PDGF, mediate regulation of CD44 levels in BAlb/c 3T3 cells and that transformation of 3T3 cells by ras renders CD44 expression insensitive to the modulating effects of serum in vitro. These results correlate with the metastatic capacity of these cells in vivo.

摘要

研究了Balb/c 3T3细胞及其用ras或sis癌基因转化的衍生物中CD44s(标准异构体)水平和透明质酸结合活性与培养基中血清浓度的关系。3T3细胞在含0.5%或10%血清的培养基中生长时,CD44水平较低且不结合透明质酸。然而,在5%血清中,细胞的CD44水平要高得多且能够结合透明质酸。在低血清中预先培养后再用5%或10%血清重新刺激的3T3细胞中,CD44水平也会升高。在用5%血清重新刺激的细胞中,高水平的CD44至少维持72小时。然而,在用10%血清重新刺激的细胞中,CD44水平的升高在48小时后恢复。用ras(而非sis)癌基因转化3T3细胞使CD44水平对血清调节不敏感:ras转化的细胞在所有测试的血清浓度和所有时间点都含有高水平的CD44并结合透明质酸。在这些调节变化中,sis转化的细胞表现得与3T3细胞相似。当补充0.5%血清时,血小板衍生生长因子(PDGF)模拟了血清对3T3细胞中CD44水平和透明质酸结合能力的影响,并且血清的CD44上调活性通过与抗PDGF抗体孵育而被中和。这些数据表明,血清因子,特别是PDGF,介导了Balb/c 3T3细胞中CD44水平的调节,并且ras对3T3细胞的转化使CD44表达在体外对血清的调节作用不敏感。这些结果与这些细胞在体内的转移能力相关。

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