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对癌症患者循环抗体库进行指纹识别。

Fingerprinting the circulating repertoire of antibodies from cancer patients.

作者信息

Mintz Paul J, Kim Jeri, Do Kim-Anh, Wang Xuemei, Zinner Ralph G, Cristofanilli Massimo, Arap Marco A, Hong Waun Ki, Troncoso Patricia, Logothetis Christopher J, Pasqualini Renata, Arap Wadih

机构信息

Department of Genitourinary Medical Oncology, The University of Texas M. D. Anderson Cancer Center, 1515 Holcombe Boulevard, Houston, TX 77030, USA.

出版信息

Nat Biotechnol. 2003 Jan;21(1):57-63. doi: 10.1038/nbt774. Epub 2002 Dec 23.

Abstract

Recognition of molecular diversity in disease is required for the development of targeted therapies. We have developed a screening method based on phage display to select peptides recognized by the repertoire of circulating tumor-associated antibodies. Here we isolated peptides recognized by antibodies purified from the serum of prostate cancer patients. We identified a consensus motif, NX(S/T)DK(S/T), that bound selectively to circulating antibodies from cancer patients over control antibodies from blood donors. We validated this motif by showing that positive serum reactivity to the peptide was specifically linked to disease progression and to shorter survival in a large patient population. Moreover, we identified the corresponding protein eliciting the immune response. Finally, we showed a strong and specific positive correlation between serum reactivity to the tumor antigen, development of metastatic androgen-independent disease, and shorter overall survival. Exploiting the differential humoral response to cancer through such an approach may identify molecular markers and targets for diagnostic and therapeutic intervention.

摘要

开发靶向治疗需要识别疾病中的分子多样性。我们基于噬菌体展示开发了一种筛选方法,以选择被循环肿瘤相关抗体库识别的肽段。在此,我们从前列腺癌患者血清中分离出被抗体识别的肽段。我们鉴定出一个共有基序NX(S/T)DK(S/T),该基序与癌症患者的循环抗体选择性结合,而不与献血者的对照抗体结合。我们通过证明肽段的阳性血清反应性与疾病进展以及大量患者群体中较短的生存期特异性相关,验证了该基序。此外,我们鉴定出引发免疫反应的相应蛋白质。最后,我们显示血清对肿瘤抗原的反应性、转移性雄激素非依赖性疾病的发展与较短的总生存期之间存在强烈且特异性的正相关。通过这种方法利用对癌症的差异性体液反应,可能会识别出用于诊断和治疗干预的分子标志物和靶点。

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