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人类恶性积液中转化生长因子的多样性。

Multiplicity of transforming growth factors in human malignant effusions.

作者信息

Seo M K, Lynch K E, Podolsky D K

机构信息

Department of Medicine, Harvard Medical School, Boston, Massachusetts.

出版信息

Cancer Res. 1988 Apr 1;48(7):1792-7.

PMID:2894891
Abstract

Human malignant effusions were found to contain transforming growth factor (TGF) activity capable of stimulating anchorage independent growth of nontransformed rodent fibroblasts. Bio-Gel P-60 chromatography of acid-ethanol extracts demonstrated the presence of three populations of TGF activities in 57% of malignant effusions. Two activities were similar to those of TGF alpha and TGF beta as judged by their size (Mr approximately equal to 6,000 and approximately equal to 25,000, respectively), biological activity (ability to stimulate anchorage independent growth of NRK fibroblasts in the absence or presence of epidermal growth factor, respectively), and capacity to competitively inhibit binding of 125I-labeled epidermal growth factor to A-431 membranes and 125I-TGF beta to baby hamster kidney fibroblasts, respectively. In addition a third factor which stimulated anchorage independent growth of nontransformed rodent fibroblast and human colonic epithelial cells was also recovered following Bio-Gel P-60 chromatography of extracts from several cytology positive human malignant effusions of patients with colonic and breast carcinoma as well as other malignancies. The latter malignant effusion related transforming growth factor was not present in benign or cytology negative effusions. Malignant effusion related TGF factor was inactivated by sulfhydryl reducing agents, heat, and trypsin treatment but was stable in 1% acetic acid and ethanol. Partial purification was accomplished by chromatography of an acid-ethanol extract on Bio-Gel P-60 followed by high performance liquid chromatography with C18-mu Bondapak to yield a nearly pure protein with apparent molecular weights of 64,000 by sodium dodecyl sulfate-polacrylamide gel electrophoresis when run in nonreducing conditions and 32,000 when run in reducing conditions. Malignant effusion related TGF was able to stimulate anchorage independent growth of nontransformed fibroblasts in the absence of other growth factors. It did not competitively inhibit binding of 125I-labeled epidermal growth factor, 125I-TGF beta, or 125I-labeled platelet derived growth factor. Therefore, this factor isolated from human malignant effusions may be distinct from previously described transforming growth factors. Collectively these observations indicate that human malignant effusions contain a multiplicity of transforming growth factors. It is possible that the malignant effusion related transforming growth factors play a role or reflect the metastatic growth properties of various tumors.

摘要

研究发现,人类恶性积液中含有能够刺激未转化的啮齿动物成纤维细胞进行不依赖贴壁生长的转化生长因子(TGF)活性。对酸 - 乙醇提取物进行Bio - Gel P - 60层析分析表明,57%的恶性积液中存在三种TGF活性成分。从大小(分别约为6000和25000)、生物学活性(分别在有无表皮生长因子存在时刺激NRK成纤维细胞进行不依赖贴壁生长的能力)以及竞争抑制125I标记的表皮生长因子与A - 431细胞膜结合和125I - TGFβ与幼仓鼠肾成纤维细胞结合的能力判断,其中两种活性分别与TGFα和TGFβ相似。此外,在对来自结肠癌、乳腺癌及其他恶性肿瘤患者的数例细胞学检查呈阳性的人类恶性积液提取物进行Bio - Gel P - 60层析后,还发现了第三种因子,它能刺激未转化的啮齿动物成纤维细胞和人类结肠上皮细胞进行不依赖贴壁生长。后一种与恶性积液相关的转化生长因子在良性或细胞学检查呈阴性的积液中不存在。与恶性积液相关的TGF因子经巯基还原剂、加热及胰蛋白酶处理后失活,但在1%乙酸和乙醇中稳定。通过对酸 - 乙醇提取物先进行Bio - Gel P - 60层析,然后用C18 - μ Bondapak进行高效液相色谱,实现了部分纯化,得到一种近乎纯的蛋白质,在非还原条件下经十二烷基硫酸钠 - 聚丙烯酰胺凝胶电泳测定其表观分子量为64000,在还原条件下为32000。与恶性积液相关的TGF在无其他生长因子存在时能够刺激未转化的成纤维细胞进行不依赖贴壁生长。它不能竞争抑制125I标记的表皮生长因子、125I - TGFβ或125I标记的血小板衍生生长因子的结合。因此,从人类恶性积液中分离出的这种因子可能与先前描述的转化生长因子不同。总体而言,这些观察结果表明人类恶性积液中含有多种转化生长因子。与恶性积液相关的转化生长因子有可能发挥作用,或反映各种肿瘤的转移生长特性。

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