Petrini Iacopo, Sollini Martina, Bartoli Francesco, Barachini Serena, Montali Marina, Pardini Eleonora, Burzi Irene Sofia, Erba Paola Anna
General Pathology, Department of Translational Research & New Technologies in Surgery and Medicine, University of Pisa and Azienda Ospedaliero Universitaria Pisana, 56100 Pisa, Italy.
Department of Biomedical Sciences, Humanitas University, Pieve Emanuele, 20090 Milan, Italy.
Cancers (Basel). 2022 May 24;14(11):2592. doi: 10.3390/cancers14112592.
to exploit tissue-specific interactions among thymic epithelial tumor (TETs) cells and extra-domain B fibronectin (ED-B FN).
The stromal pattern of ED-B FN expression was investigated through tumor specimen collection and molecular profiling in 11 patients with recurrent TETs enrolled in prospective theragnostic phase I/II trials with Radretumab, an ED-B FN specific recombinant human antibody. Radretumab radioimmunotherapy (R-RIT) was offered to patients who exhibited the target expression. Experiments included immunochemical analysis (ICH), cell cultures, immunophenotypic analysis, Western blot, slot-blot assay, and quantitative RT-PCR of two primary thymoma cultures we obtained from patients' samples and in the Ty82 cell line.
The in vivo scintigraphic demonstration of ED-B FN expression resulted in R-RIT eligibility in 8/11 patients, of which seven were treated. The best observed response was disease stabilization ( 5/7) with a duration of 4.3 months (range 3-5 months). IHC data confirmed high ED-B FN expression in the peripherical microenvironment rather than in the center of the tumor, which was more abundant in B3 thymomas. Further, there was a predominant expression of ED-B FN by the stromal cells of the thymoma microenvironment rather than the epithelial cells.
Our data support the hypothesis that thymomas induce stromal cells to shift FN production to the ED-B subtype, likely representing a favorable hallmark for tumor progression and metastasis. Collectively, results derived from clinical experience and molecular insights of the in vitro experiments suggested that R-RIT inefficacy is unlikely related to low target expression in TET, being the mechanism of R-RIT resistance eventually related to patients' susceptibility (i.e., inherent characteristics), the pattern expression of the target (i.e., at periphery), the biological characteristics of the tumor (i.e., aggressive and resistant phenotypes), and/or to format of the target agent (i.e., 131I-L19-SIP).
探索胸腺上皮肿瘤(TETs)细胞与域外B纤连蛋白(ED-B FN)之间的组织特异性相互作用。
通过收集肿瘤标本并进行分子分析,对11例复发性TETs患者的ED-B FN表达的基质模式进行了研究,这些患者参加了使用ED-B FN特异性重组人抗体Radretumab的前瞻性治疗诊断I/II期试验。对表现出靶标表达的患者提供Radretumab放射免疫疗法(R-RIT)。实验包括免疫化学分析(ICH)、细胞培养、免疫表型分析、蛋白质免疫印迹、狭缝印迹分析以及对我们从患者样本和Ty82细胞系中获得的两种原发性胸腺瘤培养物进行定量逆转录聚合酶链反应。
ED-B FN表达的体内闪烁显像显示8/11例患者符合R-RIT治疗条件,其中7例接受了治疗。观察到的最佳反应是疾病稳定(5/7),持续时间为4.3个月(范围3 - 5个月)。免疫组化数据证实,ED-B FN在肿瘤外周微环境中高表达,而非肿瘤中心,在B3胸腺瘤中更为丰富。此外,胸腺瘤微环境的基质细胞而非上皮细胞中ED-B FN表达占主导。
我们的数据支持以下假设,即胸腺瘤诱导基质细胞将纤连蛋白的产生转变为ED-B亚型,这可能是肿瘤进展和转移的有利标志。总体而言,临床经验和体外实验的分子见解结果表明,R-RIT无效不太可能与TET中低靶标表达有关,R-RIT耐药机制最终与患者易感性(即固有特征)、靶标的表达模式(即在周边)、肿瘤的生物学特征(即侵袭性和耐药表型)和/或靶标药物形式(即131I-L19-SIP)有关。
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