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肽受体作为癌症诊断与治疗的分子靶点。

Peptide receptors as molecular targets for cancer diagnosis and therapy.

作者信息

Reubi Jean Claude

机构信息

Division of Cell Biology and Experimental Cancer Research, Institute of Pathology, University of Berne, CH-3010 Berne, Switzerland.

出版信息

Endocr Rev. 2003 Aug;24(4):389-427. doi: 10.1210/er.2002-0007.

Abstract

During the past decade, proof of the principle that peptide receptors can be used successfully for in vivo targeting of human cancers has been provided. The molecular basis for targeting rests on the in vitro observation that peptide receptors can be expressed in large quantities in certain tumors. The clinical impact is at the diagnostic level: in vivo receptor scintigraphy uses radiolabeled peptides for the localization of tumors and their metastases. It is also at the therapeutic level: peptide receptor radiotherapy of tumors emerges as a serious treatment option. Peptides linked to cytotoxic agents are also considered for therapeutic applications. The use of nonradiolabeled, noncytotoxic peptide analogs for long-term antiproliferative treatment of tumors appears promising for only a few tumor types, whereas the symptomatic treatment of neuroendocrine tumors by somatostatin analogs is clearly successful. The present review summarizes and critically evaluates the in vitro data on peptide and peptide receptor expression in human cancers. These data are considered to be the molecular basis for peptide receptor targeting of tumors. The paradigmatic peptide somatostatin and its receptors are extensively reviewed in the light of in vivo targeting of neuroendocrine tumors. The role of the more recently described targeting peptides vasoactive intestinal peptide, gastrin-releasing peptide, and cholecystokinin/gastrin is discussed. Other emerging and promising peptides and their respective receptors, including neurotensin, substance P, and neuropeptide Y, are introduced. This information relates to established and potential clinical applications in oncology.

摘要

在过去十年中,已证实肽受体可成功用于人类癌症的体内靶向治疗这一原理。靶向治疗的分子基础基于体外观察结果,即肽受体可在某些肿瘤中大量表达。其临床影响体现在诊断层面:体内受体闪烁显像利用放射性标记的肽来定位肿瘤及其转移灶。在治疗层面也有体现:肿瘤的肽受体放射治疗成为一种重要的治疗选择。与细胞毒性药物相连的肽也被考虑用于治疗应用。使用未标记放射性、无细胞毒性的肽类似物对肿瘤进行长期抗增殖治疗,仅对少数几种肿瘤类型显示出前景,而生长抑素类似物对神经内分泌肿瘤的对症治疗显然是成功的。本综述总结并批判性地评估了关于人类癌症中肽和肽受体表达的体外数据。这些数据被认为是肿瘤肽受体靶向治疗的分子基础。鉴于神经内分泌肿瘤的体内靶向治疗,对典型的肽生长抑素及其受体进行了广泛综述。讨论了最近描述的靶向肽血管活性肠肽、胃泌素释放肽和胆囊收缩素/胃泌素的作用。还介绍了其他新出现且有前景的肽及其各自的受体,包括神经降压素、P物质和神经肽Y。这些信息与肿瘤学中已确立的和潜在的临床应用相关。

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