Camacho-Hubner C, McCusker R H, Clemmons D R
Department of Medicine, University of North Carolina, Chapel Hill 27599.
J Cell Physiol. 1991 Aug;148(2):281-9. doi: 10.1002/jcp.1041480214.
The insulin-like growth factors (IGFs) I and II are present in extracellular fluids associated with specific binding proteins (IGFBPs) that can modify their biologic actions. These studies were undertaken to determine which forms of IGFBP are secreted by endometrial carcinoma (HEC-1B) and breast carcinoma (MDA-231) cells, to characterize variables that control IGFBP secretion, and to study the effect of IGFBP-1 and IGFBP-2 on IGF-I stimulated cell proliferation. Secreted IGFBPs were identified by ligand blotting and IGFBP-1 was quantified using a specific radioimmunoassay (RIA). MDA-231 cell conditioned media (CM) contained four (43,000, 39,000, 30,000 and 24,000 Mr) forms of IGFBP, and HEC-1B cell CM contained three forms (39,000, 34,000 and 30,000 Mr). Immunoblotting showed that the 30,000 Mr form secreted by both cell types was IGFBP-1. Likewise the 34,000 Mr band in HEC-1B media reacted with IGFBP-2 antiserum and the 39,000 and 43,000 Mr bands reacted with IGFBP-3 antiserum. IGF-I stimulated the secretion of IGFBP-3 from both cell types and IGFBP-2 from HEC-1B cells but either decreased or caused no change in secretion of IGFBP-1 and a 24,000 Mr form. In contrast, insulin inhibited the secretion of IGFBP-1 but increased the secretion of the 24,000 Mr form. Compounds that elevate intracellular cAMP levels increased the secretion of IGFBP-3, IGFBP-1, and the 24,000 Mr form from both MDA-231 and HEC-1B cells. When sparse cultures of MDA-231 cells were used, addition of IGF-I caused a 24% increase in cell number after 48 hr. This mitogenic response was enhanced by the presence of recombinant human IGFBP-1 (45% increase in cell number, P less than 0.001). Bovine IGFBP-2 did not potentiate IGF-I stimulated cell proliferation. These findings show that two tumor cell lines secrete distinct forms of IGFBPs and that there is differential regulation of IGFBP secretion. At least one form secreted by both tumors may act as a positive autocrine modulator of IGF-I's growth stimulating actions.
胰岛素样生长因子(IGFs)I和II存在于细胞外液中,与特定的结合蛋白(IGFBPs)相关,这些结合蛋白可以改变它们的生物学作用。进行这些研究是为了确定子宫内膜癌(HEC-1B)和乳腺癌(MDA-231)细胞分泌哪些形式的IGFBP,表征控制IGFBP分泌的变量,并研究IGFBP-1和IGFBP-2对IGF-I刺激的细胞增殖的影响。通过配体印迹法鉴定分泌的IGFBPs,并使用特异性放射免疫测定法(RIA)对IGFBP-1进行定量。MDA-231细胞条件培养基(CM)含有四种(43,000、39,000、30,000和24,000 Mr)形式的IGFBP,而HEC-1B细胞CM含有三种形式(39,000、34,000和30,000 Mr)。免疫印迹显示,两种细胞类型分泌的30,000 Mr形式是IGFBP-1。同样,HEC-1B培养基中的34,000 Mr条带与IGFBP-2抗血清反应,39,000和43,000 Mr条带与IGFBP-3抗血清反应。IGF-I刺激两种细胞类型分泌IGFBP-3以及HEC-1B细胞分泌IGFBP-2,但IGFBP-1和一种24,000 Mr形式的分泌则减少或没有变化。相反,胰岛素抑制IGFBP-1的分泌,但增加24,000 Mr形式的分泌。提高细胞内cAMP水平的化合物增加了MDA-231和HEC-1B细胞中IGFBP-3、IGFBP-1和24,000 Mr形式的分泌。当使用MDA-231细胞的稀疏培养物时,添加IGF-I在48小时后使细胞数量增加24%。这种促有丝分裂反应因重组人IGFBP-1的存在而增强(细胞数量增加45%,P小于0.001)。牛IGFBP-2不能增强IGF-I刺激的细胞增殖。这些发现表明,两种肿瘤细胞系分泌不同形式的IGFBPs,并且IGFBP分泌存在差异调节。两种肿瘤分泌的至少一种形式可能作为IGF-I生长刺激作用的阳性自分泌调节剂。
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