新辅助治疗对直肠癌近红外肿瘤成像中靶点表达的影响。

Impact of Neoadjuvant Treatment on Target Expression in Rectal Cancer for Near-Infrared Tumor Imaging.

作者信息

Zonoobi Elham, Neijenhuis Lisanne K A, Lemij Annelieke A, Linders Daan G J, Nazemalhosseini-Mojarad Ehsan, Bhairosingh Shadhvi S, Dekker-Ensink N Geeske, van Vlierberghe Ronald L P, Peeters Koen C M J, Holman Fabian A, Tollenaar Rob A E M, Hilling Denise E, Crobach A Stijn L P, Vahrmeijer Alexander L, Kuppen Peter J K

机构信息

Department of Surgery, Leiden University Medical Center, P.O. Box 9600, 2300 RC Leiden, The Netherlands.

Division of Gastroenterology and Hepatology, Department of Medicine, School of Medicine, Stanford University, Stanford, CA 94305, USA.

出版信息

Cancers (Basel). 2025 Jun 12;17(12):1958. doi: 10.3390/cancers17121958.

DOI:10.3390/cancers17121958

PMID:40563608

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12190537/

Abstract

BACKGROUND

Rectal cancer (RC) patients with a clinical complete response (cCR) after neoadjuvant chemoradiotherapy (nCRT) may qualify for a watch-and-wait (W&W) approach. However, a 20-30% local tumor regrowth rate highlights challenges in identifying true responders. This study explores markers for future near-infrared fluorescence tumor imaging by endoscopy to differentiate responders and the effect of nCRT on their expression.

METHODS

RC samples ( = 51) were collected from both pre-treatment biopsies and corresponding post-treatment surgical specimens. Samples were categorized by treatment response and determined using tumor regression grade (TRG) scoring. Immunohistochemistry assessed the expression of CEA, EpCAM, EGFR, and c-MET in tumors and adjacent normal tissues. Expression levels were quantified using H-scores (0-3), combining the percentage and intensity of stained cells. Pre- and post-treatment H-scores were compared to evaluate the impact of nCRT.

RESULTS

CEA, EpCAM, and c-MET were overexpressed in tumor tissue as compared to adjacent healthy mucosa in 100% (51/51), 98.4% (50/51), and 92% (47/51) of tumor biopsies, respectively, while EGFR showed no overexpression. A tumor-to-normal (T/N) ratio ≥ 2 was considered sufficient for differentiation in molecular fluorescence imaging. In pre-treatment biopsy samples, c-MET showed the highest T/N expression ratio (53% of the samples ≥ 2), followed by CEA (26.3%) and EpCAM (16%). Following nCRT treatment, CEA and c-MET maintained a ≥ 2 differential expression in 45% of all samples, whereas EpCAM exhibited this difference in only 9.2% of cases. Neoadjuvant therapy even significantly improved the T/N expression ratio for CEA and c-MET ( < 0.01) and EpCAM ( < 0.05), while EGFR expression remained lower than adjacent normal tissue. Significant increases in all marker expressions were observed in minimal responders (TRG4/5, < 0.01-0.001), while near-complete responders (TRG2) exhibited non-significant changes in CEA, c-MET, and EGFR expression.

CONCLUSIONS

c-MET and CEA emerged as optimal tumor imaging targets, showing sustained differential expression after nCRT. In vivo fluorescence-guided endoscopy using probes against these markers could play a role in future clinical decision-making.

摘要

背景

新辅助放化疗（nCRT）后达到临床完全缓解（cCR）的直肠癌（RC）患者可能适合采用观察等待（W&W）策略。然而，20%-30%的局部肿瘤复发率凸显了识别真正缓解者的挑战。本研究探索用于未来内镜近红外荧光肿瘤成像的标志物，以区分缓解者以及nCRT对其表达的影响。

方法

收集51例RC患者治疗前活检组织及相应治疗后手术标本。样本按治疗反应分类，并采用肿瘤退缩分级（TRG）评分确定。免疫组织化学评估肿瘤及相邻正常组织中CEA、EpCAM、EGFR和c-MET的表达。使用H评分（0-3）对表达水平进行量化，综合染色细胞的百分比和强度。比较治疗前后的H评分以评估nCRT的影响。

结果

与相邻健康黏膜相比，肿瘤组织中CEA、EpCAM和c-MET在100%（51/51）、98.4%（50/51）和92%（47/51）的肿瘤活检组织中分别过度表达，而EGFR未过度表达。肿瘤与正常组织（T/N）比值≥2被认为足以用于分子荧光成像鉴别。在治疗前活检样本中，c-MET显示最高的T/N表达比值（53%的样本≥2），其次是CEA（26.3%）和EpCAM（16%）。nCRT治疗后，CEA和c-MET在所有样本的45%中维持≥2的差异表达，而EpCAM仅在9.2%的病例中呈现这种差异。新辅助治疗甚至显著提高了CEA、c-MET和EpCAM的T/N表达比值（P<0.01），而EGFR表达仍低于相邻正常组织。在微小缓解者（TRG4/5，P<0.01-0.001）中观察到所有标志物表达显著增加，而接近完全缓解者（TRG2）中CEA、c-MET和EGFR表达无显著变化。