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通过免疫PCR检测非小细胞肺癌患者细胞外囊泡上的肿瘤相关膜受体

Detection of Tumor-Associated Membrane Receptors on Extracellular Vesicles from Non-Small Cell Lung Cancer Patients via Immuno-PCR.

作者信息

Stiller Christiane, Viktorsson Kristina, Paz Gomero Elizabeth, Hååg Petra, Arapi Vasiliki, Kaminskyy Vitaliy O, Kamali Caroline, De Petris Luigi, Ekman Simon, Lewensohn Rolf, Karlström Amelie Eriksson

机构信息

Department of Protein Science, School of Engineering Sciences in Chemistry, Biotechnology and Health, KTH Royal Institute of Technology, AlbaNova University Center, SE-10691 Stockholm, Sweden.

Biomedical Centre, Department of Pharmaceutical Biosciences, Uppsala University, SE-75123 Uppsala, Sweden.

出版信息

Cancers (Basel). 2021 Feb 22;13(4):922. doi: 10.3390/cancers13040922.

Abstract

Precision cancer medicine for non-small-cell lung cancer (NSCLC) has increased patient survival. Nevertheless, targeted agents towards tumor-associated membrane receptors only result in partial remission for a limited time, calling for approaches which allow longitudinal treatment monitoring. Rebiopsy of tumors in the lung is challenging, and metastatic lesions may have heterogeneous signaling. One way ahead is to use liquid biopsies such as circulating tumor DNA or small extracellular vesicles (sEVs) secreted by the tumor into blood or other body fluids. Herein, an immuno-PCR-based detection of the tumor-associated membrane receptors EGFR, HER2, and IGF-1R on CD9-positive sEVs from NSCLC cells and pleural effusion fluid (PE) of NSCLC patients is developed utilizing DNA conjugates of antibody mimetics and affibodies, as detection agents. Results on sEVs purified from culture media of NSCLC cells treated with anti-EGFR siRNA, showed that the reduction of EGFR expression can be detected via immuno-PCR. Protein profiling of sEVs from NSCLC patient PE samples revealed the capacity to monitor EGFR, HER2, and IGF-1R with the immuno-PCR method. We detected a significantly higher EGFR level in sEVs derived from a PE sample of a patient with an -driven NSCLC adenocarcinoma than in sEVs from PE samples of non- driven adenocarcinoma patients or in samples from patients with benign lung disease. In summary, we have developed a diagnostic method for sEVs in liquid biopsies of cancer patients which may be used for longitudinal treatment monitoring to detect emerging bypassing resistance mechanisms in a noninvasive way.

摘要

非小细胞肺癌(NSCLC)的精准癌症医学提高了患者生存率。然而,针对肿瘤相关膜受体的靶向药物仅能在有限时间内导致部分缓解,这就需要能够进行纵向治疗监测的方法。对肺部肿瘤进行再次活检具有挑战性,而且转移病灶可能具有异质性信号。一种可行的方法是使用液体活检,例如循环肿瘤DNA或肿瘤分泌到血液或其他体液中的小细胞外囊泡(sEVs)。在此,利用抗体模拟物和亲和体的DNA偶联物作为检测试剂,开发了一种基于免疫PCR的方法,用于检测NSCLC细胞和NSCLC患者胸腔积液(PE)中CD9阳性sEVs上的肿瘤相关膜受体EGFR、HER2和IGF-1R。从用抗EGFR siRNA处理的NSCLC细胞培养基中纯化的sEVs的检测结果表明,通过免疫PCR可以检测到EGFR表达的降低。对NSCLC患者PE样本中sEVs的蛋白质分析揭示了用免疫PCR方法监测EGFR、HER2和IGF-1R的能力。我们检测到,一名由驱动的NSCLC腺癌患者的PE样本来源的sEVs中的EGFR水平显著高于非驱动腺癌患者的PE样本来源的sEVs或良性肺病患者的样本中的EGFR水平。总之,我们开发了一种用于癌症患者液体活检中sEVs的诊断方法,可以用于纵向治疗监测,以无创方式检测新出现的旁路耐药机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9052/7926549/b361818081e0/cancers-13-00922-g001.jpg

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