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白细胞介素13对人乳腺癌细胞增殖和克隆生长的抑制作用

Inhibition of proliferation and clonal growth of human breast cancer cells by interleukin 13.

作者信息

Serve H, Oelmann E, Herweg A, Oberberg D, Serve S, Reufi B, Mücke C, Minty A, Thiel E, Berdel W E

机构信息

Department of Hematology and Oncology, Universitaetsklinikum Benjamin Franklin, Freie Universitaet, Hindenburgdamm, Berlin, Germany.

出版信息

Cancer Res. 1996 Aug 1;56(15):3583-8.

PMID:8758930
Abstract

We tested the influence of recombinant human interleukin (rhIL)-l3 and rhIL-4 on clonal growth of human breast cancer cell lines. rhIL-13 and rhIL-4 inhibited clonal growth of three of nine lines to approximately 50% of controls (ED50, 0.5 ng/ml). rhIl-13 reduced [3H]thymidine incorporation in all three cell lines: two showing a minor (84% and 83% of controls) and one showing a major response (25% of control). Both cytokines markedly reduced serum-induced G(0/1) exit (approximately 25% versus 60%). 125I-labeled interleukin (IL) 13 binding assays revealed high-affinity binding sites for IL-13 on two of the three responding cell lines (KD approximately 60 pM). (Y124D)IL-4 effectively antagonized all effects of rhIl-13 and rhIL-4, arguing for shared receptor components between them. However, neither rhIl-4 nor (Y124D) IL-4 could displace 125I-labeled IL-13 from binding, although unlabeled rhIL-13 effectively did so. Using reverse transcription-PCR, we studied the expression of the common gamma chain (gammac) in responding cell lines, putatively being shared between IL-4 receptor and IL-13 receptor; none of the three cell lines express gammac. In conclusion, we demonstrate antiproliferative effects of IL-4 and IL-13 on carcinoma cells which express IL-13 binding sites without participation of gammac.

摘要

我们测试了重组人白细胞介素(rhIL)-13和rhIL-4对人乳腺癌细胞系克隆生长的影响。rhIL-13和rhIL-4抑制了九条细胞系中三条的克隆生长,使其降至对照组的约50%(半数有效剂量,0.5 ng/ml)。rhIL-13降低了所有三条细胞系中[3H]胸苷的掺入:两条显示出轻微反应(分别为对照组的84%和83%),一条显示出主要反应(为对照组的25%)。两种细胞因子均显著降低了血清诱导的G(0/1)期退出(约25%对60%)。125I标记的白细胞介素(IL)13结合试验显示,在三条有反应的细胞系中的两条上存在IL-13的高亲和力结合位点(解离常数约为60 pM)。(Y124D)IL-4有效拮抗了rhIL-13和rhIL-4的所有作用,表明它们之间存在共同的受体成分。然而,rhIL-4和(Y124D)IL-4均不能从结合中置换125I标记的IL-13,尽管未标记的rhIL-13可以有效置换。利用逆转录-聚合酶链反应,我们研究了有反应的细胞系中共同γ链(γc)的表达,推测其在IL-4受体和IL-13受体之间共享;三条细胞系均未表达γc。总之,我们证明了IL-4和IL-13对表达IL-13结合位点的癌细胞具有抗增殖作用,且该作用不依赖γc的参与。

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