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人结肠癌细胞系中转化生长因子α和β的表达:对自分泌模型的启示

Transforming growth factor alpha and beta expression in human colon cancer lines: implications for an autocrine model.

作者信息

Coffey R J, Goustin A S, Soderquist A M, Shipley G D, Wolfshohl J, Carpenter G, Moses H L

出版信息

Cancer Res. 1987 Sep 1;47(17):4590-4.

PMID:2887281
Abstract

Three human colon cancer lines (SW480, SW620, WIDR) secrete different levels of transforming growth factor beta (TGF beta)-like and transforming growth factor alpha (TGF alpha)/epidermal growth factor (EGF)-like molecules into serum-free conditioned media as measured by competing activity in TGF beta and EGF radioreceptor assays. SW480 cells, the highest producers of TGF beta-like activity, lack detectable TGF beta receptors while SW620 cells, the highest producers of TGF alpha/EGF-like activity, lack EGF receptors. This study investigated the production of these growth factors at the mRNA level and examined the mechanism of loss of detectable receptors. Using complementary DNA probes for TGF beta and TGF alpha, it was demonstrated that mRNA levels correlated with the amounts of TGF beta and TGF alpha produced; TGF beta gene expression was highest in SW480 cells and TGF alpha gene expression was highest in SW620 cells. Acid washing of the SW480 cells prior to performing the TGF beta binding assay resulted in the unmasking of substantial levels of TGF beta receptors. Neither acid washing nor preincubation with suramin uncovered EGF receptors in SW620 cells. Also, and in contrast to the other two lines, EGF receptor expression could not be detected in SW620 cells by Northern gel analysis of receptor messenger RNA or by immunological analysis of receptor protein. Thus two distinct mechanisms (occupation of TGF beta receptor in SW480 cells, or absence of EGF receptor in SW620 cells) explain the lack of detectable TGF beta and EGF receptors in the binding assays. The autocrine hypothesis remains viable for TGF beta in SW480 cells but not for TGF alpha in SW620 cells; this would not discount a paracrine role in this latter case.

摘要

三种人结肠癌细胞系(SW480、SW620、WIDR)在无血清条件培养基中分泌不同水平的转化生长因子β(TGFβ)样和转化生长因子α(TGFα)/表皮生长因子(EGF)样分子,这通过TGFβ和EGF放射受体分析中的竞争活性来测定。SW480细胞是TGFβ样活性的最高产生者,缺乏可检测到的TGFβ受体,而SW620细胞是TGFα/EGF样活性的最高产生者,缺乏EGF受体。本研究在mRNA水平上研究了这些生长因子的产生,并检查了可检测受体缺失的机制。使用针对TGFβ和TGFα的互补DNA探针,证明mRNA水平与产生的TGFβ和TGFα量相关;TGFβ基因表达在SW480细胞中最高,TGFα基因表达在SW620细胞中最高。在进行TGFβ结合测定之前对SW480细胞进行酸洗,导致大量水平的TGFβ受体被暴露。酸洗或与苏拉明预孵育均未在SW620细胞中发现EGF受体。此外,与其他两个细胞系相反,通过受体信使RNA的Northern凝胶分析或受体蛋白的免疫分析,在SW620细胞中未检测到EGF受体表达。因此,两种不同的机制(SW480细胞中TGFβ受体的占据,或SW620细胞中EGF受体的缺失)解释了结合测定中缺乏可检测的TGFβ和EGF受体。自分泌假说对于SW480细胞中的TGFβ仍然可行,但对于SW620细胞中的TGFα则不然;在后一种情况下,这并不排除旁分泌作用。

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