首页> 外文期刊>The Journal of Nuclear Medicine >Applying PET to Broaden the Diagnostic Utility of the Clinically Validated CA19.9 Serum Biomarker for Oncology.
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Applying PET to Broaden the Diagnostic Utility of the Clinically Validated CA19.9 Serum Biomarker for Oncology.

机译:应用宠物扩大临床验证的CA19.9血清生物标志物进行肿瘤学的诊断效用。

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Despite their considerable advantages, many circulating biomarkers have well-documented limitations. One prominent shortcoming in oncology is a high frequency of false-positive indications for malignant disease in upfront diagnosis. Because one common cause of false positivism is biomarker production from benign disorders in unrelated host tissues, we hypothesized that probing the sites of biomarker secretion with an imaging tool could be a broadly useful strategy to deconvolute the meaning of foreboding but inconclusive circulating biomarker levels.In preparation to address this hypothesis clinically, we developed (89)Zr-5B1, a fully human, antibody-based radiotracer targeting tumor-associated CA19.9 in the preclinical setting.(89)Zr-5B1 localized to multiple tumor models representing diseases with undetectable and supraphysiologic serum CA19.9 levels. Among these, (89)Zr-5B1 detected orthotopic models of pancreatic ductal adenocarcinoma, an elusive cancer for which the serum assay is measured in humans but with limited specificity in part because of the frequency of CA19.9 secretion from benign hepatic pathologies.In this report, a general strategy to supplement some of the shortcomings of otherwise highly useful circulating biomarkers with immunoPET is described. To expedite the clinical validation of this model, a human monoclonal antibody to CA19.9 (a highly visible but partially flawed serum biomarker for several cancers) was radiolabeled and evaluated, and the compelling preclinical evidence suggests that the radiotracer may enhance the fidelity of diagnosis and staging of pancreatic ductal adenocarcinoma, a notoriously occult cancer.
机译:尽管有相当大的优势,但许多循环的生物标志物具有良好的局限性。肿瘤学中的一个突出缺点是前期诊断中恶性疾病的伪阳性适应性的高频率。因为假实心主义的一个常见原因是从无关宿主组织中的良性疾病产生的生物标志物生产,我们假设探测与成像工具的生物标志物分泌位点可能是一种广泛的策略,以解构预测预测的含义但不确定的循环生物标志物水平。准备在临床上解决这一假设,我们开发了(89)ZR-5B1,一种靶向肿瘤相关的CA19.9的全人,抗体的基于r脱氨酸酯在临床前设置。(89)ZR-5B1本地化为代表疾病的多种肿瘤模型无法察觉和超级学血清CA19.9水平。其中,(89)ZR-5B1检测到胰腺导管腺癌的原位模型,血清测定在人类中测量血清测定的难以捉摸的癌症,而是由于来自良性肝病理学的Ca19.9分泌物的频率是有限的特异性。本报告称,描述了一种补充其他具有免疫迁徙的一些缺点的一些缺点的一般策略。为了加快该模型的临床验证,对Ca19.9的人单克隆抗体(高度可见但部分缺陷的几种癌症的血清生物标志物)是放射性标记和评价的,并且令人尖锐的临床前证据表明放射性机构可以增强诊断的保真度和胰腺导管腺癌的分期,令人惊奇地隐匿性癌症。

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