Human Cell Surface Receptors as Molecular Imaging Candidates for Metastatic Prostate Cancer.

Isis C Sroka, Gerald D Pond, Raymond B Nagle, Frank Porreca, Tamara King, Gary Pestano, Bernard W Futscher, Jaime M Gard, Janice Riley, Anne E Cress
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引用次数: 8

Abstract

Existing clinical imaging procedures lack sensitivity and specificity in detecting early prostate cancer bone metastatic lesions. In this study, we developed a highly reproducible bone metastasis xenograft model and identified possible molecular imaging candidates for detecting early bone metastatic lesions. Bone trophic human prostate cells (PC-3B1) were isolated and characterized for their ability to reach bone after intracardiac injection into SCID mice. The appearances of skeletal metastases were evaluated using digital radiographic imaging and confirmed by necropsy and histology. The PC-3B1 cells retain a bone homing phenotype after long term propagation in tissue culture and exhibit progressive bone lesions within 3 weeks following intracardiac injection. Comparative transcription signatures of PC-3 and PC-3B1 cells were determined using a cancer specific microarray and confirmed by RT-PCR analysis. The analysis identified increased expression of four cell surface molecules in PC-3B1 cells that may be suitable as molecular imaging candidates to detect bone micro metastases.

人细胞表面受体作为转移性前列腺癌的分子成像候选者。
现有的临床影像学方法在检测早期前列腺癌骨转移病变方面缺乏敏感性和特异性。在这项研究中,我们建立了一个高度可重复的骨转移异种移植模型,并确定了可能用于检测早期骨转移病变的分子成像候选物。骨营养性人前列腺细胞(PC-3B1)被分离出来,并在SCID小鼠心内注射后被鉴定为能够到达骨。骨骼转移灶的表现采用数字放射成像评估,并经尸检和组织学证实。PC-3B1细胞在组织培养中长期繁殖后仍保持骨归巢表型,并在心脏内注射后3周内表现出进行性骨病变。使用肿瘤特异性芯片检测PC-3和PC-3B1细胞的比较转录特征,并通过RT-PCR分析证实。分析发现PC-3B1细胞中四个细胞表面分子的表达增加,可能适合作为检测骨微转移的分子成像候选物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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