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伯基特淋巴瘤无血清细胞系sfRamos产生生长激素的免疫反应形式。

Production of immunoreactive forms of growth hormone by the Burkitt tumor serum-free cell line sfRamos.

作者信息

Baglia L A, Cruz D, Shaw J E

机构信息

Department of Medical Microbiology and Immunology, Ohio State University College of Medicine, Columbus.

出版信息

Endocrinology. 1992 May;130(5):2446-54. doi: 10.1210/endo.130.5.1572277.

Abstract

Tumor B-cell mitogenesis may be regulated by autocrine secretions that cross-react immunologically with neuroendocrine peptides. This hypothesis is supported by our recent report that immunoreactive human PRL (ir-hPRL) is produced by and required for the continuous growth of sfRamos, a Burkitt tumor serum-free cell line. Further support for the hypothesis is provided in this study. The data illustrate that antiserum immunoglobulin fraction G (IgG) to synthetic human GH (NIDDK anti-synth hGH IC-4), but not nonimmune serum IgG, completely inhibited sfRamos proliferation. In addition, anti-synth hGH, but not nonimmune serum, identified several polypeptides in sfRamos spent medium that were not in serum-free control medium, as determined by sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE) under reducing conditions and the Western immunoblot procedure. The ir-hGH polypeptides were in the 35- to more than 300-kilodalton (kDa) range, with a 48-kDa polypeptide as a major component. A polypeptide with electrophoretic properties identical to those of the hGH monomer (22 kDa) was not detected, even with prior incubation of spent medium with N-ethylmaleimide and dithiothreitol. Pituitary preparations of hPRL and hGH, each with the monomer form as the major component, were neither mitogenic for growth-arrested cells nor did they synergize with spent medium to enhance growth, either alone or in combination, whereas spent medium with immunoreactive polypeptides larger than the monomer form markedly stimulated proliferation of growth-arrested cells. These findings demonstrate that sfRamos mitogenesis is potentially regulated by autocrine secretions with cross-immunoreactivity to two anterior pituitary hormones.

摘要

肿瘤B细胞的有丝分裂可能受自分泌分泌物调节,这些分泌物与神经内分泌肽发生免疫交叉反应。我们最近的报告支持了这一假说,即免疫反应性人催乳素(ir-hPRL)由伯基特肿瘤无血清细胞系sfRamos产生,且是其持续生长所必需的。本研究为该假说提供了进一步支持。数据表明,抗合成人生长激素的抗血清免疫球蛋白G(IgG)组分(NIDDK抗合成hGH IC-4),而非非免疫血清IgG,完全抑制了sfRamos的增殖。此外,抗合成hGH而非非免疫血清,在sfRamos的消耗培养基中鉴定出了几种无血清对照培养基中不存在的多肽,这是通过还原条件下的十二烷基硫酸钠-聚丙烯酰胺凝胶电泳(SDS-PAGE)和蛋白质免疫印迹法确定的。ir-hGH多肽在35至超过300千道尔顿(kDa)范围内,其中以48-kDa多肽为主要成分。即使在用N-乙基马来酰亚胺和二硫苏糖醇预先孵育消耗培养基后,也未检测到电泳性质与hGH单体(22 kDa)相同的多肽。以单体形式为主要成分的垂体来源的hPRL和hGH制剂,对生长停滞细胞均无促有丝分裂作用,单独或联合使用时也不会与消耗培养基协同增强生长,而含有大于单体形式的免疫反应性多肽的消耗培养基则显著刺激生长停滞细胞的增殖。这些发现表明,sfRamos的有丝分裂可能受与两种垂体前叶激素具有交叉免疫反应性的自分泌分泌物调节。

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