Enhancing precision in colorectal cancer surgery: development of an LGR5-targeting RSPO1 peptide mimetic as a contrast agent for intraoperative fluorescence molecular imaging.

IF 3.4 3区 生物学 Q3 CELL BIOLOGY
Erika Parasido, Patricia Ribeiro, Ramesh M Chingle, Thomas Rohwetter, Nikita Gupta, George Avetian, Elisa Bladelli, Mariaelena Pierobon, Yu Chen, Qinggong Tang, Martin Schnermann, Olga Rodriguez, David Robbins, Terrence R Burke, Chris Albanese, Chukwuemeka Ihemelandu
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引用次数: 0

Abstract

Colorectal cancer (CRC) is the third most common cancer worldwide. In the United States alone, CRC was responsible for approximately 52,550 deaths in 2023, with an estimated 153,020 new cases. CRC presents with synchronous peritoneal spread in 5-10% of patients, and up to 20-50% of patients with recurrent disease will develop metachronous colorectal cancer peritoneal metastatic (CRC-PM) disease. Eradication of the tumor, tumor margins and microscopic residual disease is paramount, as microscopic residual disease is associated with local recurrences, with 5-year survival rates of less than 35%. The success of resection and reduction of residual disease depends on the accuracy with which cancer cells and normal tissue can be intra-operatively distinguished. Fluorescence Molecular Imaging (IFMI) and tumor-targeted contrast agents represent a promising approach for intraoperative detection and surgical intervention. Proper target selection, the development of scalable imaging agents and enhanced real-time tumor and tumor microenvironment imaging are critical to enabling enhanced surgical resection. LGR5 (leucine-rich repeat-containing G-protein-coupled receptor 5), a colonic crypt stem cell marker and the receptor for the R-spondins (RSPO) in the Wnt signaling pathway, is also expressed on colorectal cancer stem cells (CSC) and on CRC tumors and metastases, suggesting it could be a useful target for imaging of CRC. However, there are numerous diverging reports on the role of LGR5 in CRC therapy and outcomes. Herein, we report on the synthesis and validation of a 37 amino acid RSPO1-mimetic peptide, termed RC18, that was specifically designed to access the R-spondin binding site of LGR5 to potentially be used for interoperative imaging of CRC-PM. The receptor-binding capabilities of the RC18 indicate that direct interactions with LGR5 neither significantly increased LGR5 signaling nor blocked RSPO1 binding and signal transduction, suggesting that the RSPO1-mimetic is functionally inert, making it an attractive contrast agent for intraoperative CRC-PM imaging.

提高结直肠癌手术的精确性:开发一种 LGR5 靶向 RSPO1 肽模拟物,作为术中荧光分子成像的造影剂。
结肠直肠癌(CRC)是全球第三大常见癌症。2023 年,仅在美国就有约 52,550 人死于 CRC,新增病例约 153,020 例。5%-10%的 CRC 患者会出现同步腹膜扩散,高达 20%-50%的复发患者会发展为转移性结直肠癌腹膜转移(CRC-PM)疾病。根除肿瘤、肿瘤边缘和显微镜下残留疾病至关重要,因为显微镜下残留疾病与局部复发有关,5 年生存率低于 35%。切除和减少残留疾病的成功与否取决于术中区分癌细胞和正常组织的准确性。荧光分子成像(IFMI)和肿瘤靶向造影剂是一种很有前景的术中检测和手术干预方法。正确的靶点选择、可扩展成像剂的开发以及增强的肿瘤和肿瘤微环境实时成像对于提高手术切除效果至关重要。LGR5(富亮氨酸重复含G蛋白偶联受体5)是结肠隐窝干细胞标志物,也是Wnt信号通路中的R-spondins(RSPO)受体,在结直肠癌干细胞(CSC)、CRC肿瘤和转移灶上也有表达,这表明它可能是CRC成像的一个有用靶点。然而,关于 LGR5 在 CRC 治疗和预后中的作用的报道众说纷纭。在此,我们报告了一种 37 个氨基酸的 RSPO1 拟态肽(称为 RC18)的合成和验证过程,该肽专门设计用于进入 LGR5 的 R-spondin 结合位点,可能用于 CRC-PM 的术间成像。RC18 的受体结合能力表明,它与 LGR5 的直接相互作用既不会显著增加 LGR5 的信号转导,也不会阻断 RSPO1 的结合和信号转导,这表明 RSPO1 拟态肽在功能上是惰性的,使其成为一种有吸引力的用于术中 CRC-PM 成像的造影剂。
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来源期刊
Cell Cycle
Cell Cycle 生物-细胞生物学
CiteScore
7.70
自引率
2.30%
发文量
281
审稿时长
1 months
期刊介绍: Cell Cycle is a bi-weekly peer-reviewed journal of high priority research from all areas of cell biology. Cell Cycle covers all topics from yeast to man, from DNA to function, from development to aging, from stem cells to cell senescence, from metabolism to cell death, from cancer to neurobiology, from molecular biology to therapeutics. Our goal is fast publication of outstanding research.
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