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分子 MRI 可实现脑转移瘤的早期和敏感检测。

Molecular MRI enables early and sensitive detection of brain metastases.

机构信息

CR-UK/MRC Gray Institute for Radiation Oncology and Biology, Department of Oncology, University of Oxford, Oxford OX3 7LJ, United Kingdom.

出版信息

Proc Natl Acad Sci U S A. 2012 Apr 24;109(17):6674-9. doi: 10.1073/pnas.1117412109. Epub 2012 Mar 26.

Abstract

Metastasis to the brain is a leading cause of cancer mortality. The current diagnostic method of gadolinium-enhanced MRI is sensitive only to larger tumors, when therapeutic options are limited. Earlier detection of brain metastases is critical for improved treatment. We have developed a targeted MRI contrast agent based on microparticles of iron oxide that enables imaging of endothelial vascular cell adhesion molecule-1 (VCAM-1). Our objectives here were to determine whether VCAM-1 is up-regulated on vessels associated with brain metastases, and if so, whether VCAM-1-targeted MRI enables early detection of these tumors. Early up-regulation of cerebrovascular VCAM-1 expression was evident on tumor-associated vessels in two separate murine models of brain metastasis. Metastases were detectable in vivo using VCAM-1-targeted MRI 5 d after induction (<1,000 cells). At clinical imaging resolutions, this finding is likely to translate to detection at tumor volumes two to three orders of magnitude smaller (0.3-3 × 10(5) cells) than those volumes detectable clinically (10(7)-10(8) cells). VCAM-1 expression detected by MRI increased significantly (P < 0.0001) with tumor progression, and tumors showed no gadolinium enhancement. Importantly, expression of VCAM-1 was shown in human brain tissue containing both established metastases and micrometastases. Translation of this approach to the clinic could increase therapeutic options and change clinical management in a substantial number of cancer patients.

摘要

脑转移是癌症死亡的主要原因。目前的诊断方法是增强 MRI 检测钆,这种方法仅对较大的肿瘤敏感,而此时治疗选择有限。因此,早期发现脑转移对改善治疗至关重要。我们开发了一种基于氧化铁微粒的靶向 MRI 造影剂,可对血管内皮细胞黏附分子-1(VCAM-1)进行成像。我们的目标是确定 VCAM-1 是否在与脑转移相关的血管上上调,如果是,那么 VCAM-1 靶向 MRI 是否能够早期检测到这些肿瘤。在两种不同的脑转移小鼠模型中,肿瘤相关血管上 VCAM-1 的早期上调是明显的。使用 VCAM-1 靶向 MRI 可以在诱导后 5 天(<1000 个细胞)检测到转移灶。在临床成像分辨率下,这一发现可能转化为检测体积小两个数量级的肿瘤(0.3-3×10^5 个细胞),比临床可检测的肿瘤体积(10^7-10^8 个细胞)小。MRI 检测到的 VCAM-1 表达随着肿瘤的进展而显著增加(P<0.0001),并且肿瘤没有增强。重要的是,在包含已建立转移灶和微转移灶的人类脑组织中也检测到了 VCAM-1 的表达。这种方法在临床上的应用可能会增加治疗选择,并改变大量癌症患者的临床管理。

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