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乳腺囊肿中乳腺肿瘤标志物蛋白GCDFP - 15及其外分泌上皮对应物的差异抗体反应性和CD4结合

Differential antibody reactivity and CD4 binding of the mammary tumor marker protein GCDFP-15 from breast cyst and its counterparts from exocrine epithelia.

作者信息

Caputo E, Autiero M, Mani J C, Basmaciogullari S, Piatier-Tonneau D, Guardiola J

机构信息

International Institute of Genetics and Biophysics, CNR, Naples, Italy.

出版信息

Int J Cancer. 1998 Sep 25;78(1):76-85. doi: 10.1002/(sici)1097-0215(19980925)78:1<76::aid-ijc13>3.0.co;2-3.

DOI:10.1002/(sici)1097-0215(19980925)78:1<76::aid-ijc13>3.0.co;2-3
PMID:9724097
Abstract

Analysis of biopsies from breast cancer patients demonstrated that GCDFP-15 (gross cystic disease fluid protein-15) is a specific immunocytochemical marker of primary and secondary apocrine breast tumors. The protein has an amino acid sequence identical to SABP (secretory actin-binding protein), to PIP (prolactin-inducible protein) and to gp17, a protein isolated from human seminal plasma. The latter was found to bind to CD4, a T-cell co-receptor involved in antigen recognition, thereby inhibiting the ability of the receptor to interact with the HIV-1 envelope protein gp120. We compare here the ability of independently purified GCDFP-15, SABP and gp17 and of recombinant PIP both to cross-react with a panel of monoclonal antibodies (MAbs) raised against GCDFP-15 or gp17, respectively, and to bind to CD4. We show that, although the various factors share the ability to bind to the panel of antibodies used, differences in the pattern of MAb recognition can be demonstrated. By comparing the kinetic constants for binding of GCDFP-5 and gp17 to CD4 by biosensor technology, significant differences in binding affinities were observed between the 2 factors, thus reflecting structural differences. Surface plasmon resonance analysis also showed that anti-GCDFP-15 and anti-gp17 antibodies inhibit the binding of CD4 to GCDFP-15 and gp17, respectively, to different extents. Our data thus indicate that, while the various forms of the protein are encoded by the same cDNA, tissue specificities due to post-translational modifications exist. This information may be relevant for developing more sensitive and accurate tests for the use of GCDFP-15 as a diagnostic mammary tumor marker and, most importantly, raises the possibility that GCDFP-15 may constitute a breast tumor-specific antigen.

摘要

对乳腺癌患者活检样本的分析表明,GCDFP - 15(大汗腺囊肿病液体蛋白 - 15)是原发性和继发性顶泌乳腺肿瘤的一种特异性免疫细胞化学标志物。该蛋白的氨基酸序列与SABP(分泌型肌动蛋白结合蛋白)、PIP(催乳素诱导蛋白)以及从人精浆中分离出的蛋白gp17相同。已发现后者可与CD4结合,CD4是一种参与抗原识别的T细胞共受体,从而抑制该受体与HIV - 1包膜蛋白gp120相互作用的能力。我们在此比较了独立纯化的GCDFP - 15、SABP和gp17以及重组PIP分别与一组针对GCDFP - 15或gp17产生的单克隆抗体(MAb)发生交叉反应并与CD4结合的能力。我们表明,尽管各种因子都具有与所用抗体组结合的能力,但单克隆抗体识别模式存在差异。通过生物传感器技术比较GCDFP - 5和gp17与CD4结合的动力学常数,观察到这两种因子之间结合亲和力存在显著差异,从而反映出结构差异。表面等离子体共振分析还表明,抗GCDFP - 15和抗gp17抗体分别不同程度地抑制CD4与GCDFP - 15和gp17的结合。因此,我们的数据表明,虽然该蛋白的各种形式由相同的cDNA编码,但由于翻译后修饰存在组织特异性。这一信息可能与开发更灵敏、准确的检测方法有关,以便将GCDFP - 15用作诊断乳腺肿瘤标志物,最重要的是,增加了GCDFP - 15可能构成乳腺肿瘤特异性抗原的可能性。

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