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Selective tumor uptake of a boronated porphyrin in an animal model of cerebral glioma.

机译:脑胶质瘤动物模型中硼化卟啉的选择性肿瘤吸收。

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摘要

The prognosis for patients with high-grade cerebral glioma is poor. Most treatment failures are due to local recurrence of tumor, indicating that a more aggressive local therapy could be beneficial. Adjuvant treatments such as porphyrin-sensitized photodynamic therapy (PDT) or boron neutron capture therapy (BNCT) have the potential to control local recurrence. The selective tumor uptake of a boronated porphyrin was studied in CBA mice bearing an implanted intracerebral glioma. Biopsy samples of tumor, normal brain, and blood were analyzed by a fluorometric assay following intraperitoneal and intravenous administration of boronated protoporphyrin (BOPP). This compound was selectively localized to tumor at ratios as high as 400:1 relative to normal brain. Confocal laser scanning microscopy of glioma cells in vitro and in vivo showed that BOPP was localized within mitochondria and excluded from the nucleus of these cells. This discrete subcellular localization was confirmed by density gradient ultracentrifugation after homogenization of mouse tumor biopsies. The selective discrete localization of these compounds within the tumor suggests that this compound may be used as a dual PDT/BNCT sensitizer.
机译:高度脑胶质瘤患者的预后较差。大多数治疗失败是由于肿瘤的局部复发所致,这表明更积极的局部治疗可能是有益的。诸如卟啉敏化光动力疗法(PDT)或硼中子俘获疗法(BNCT)的辅助治疗具有控制局部复发的潜力。在携带植入的脑内神经胶质瘤的CBA小鼠中研究了硼化卟啉的选择性肿瘤吸收。在腹膜内和静脉内施用硼原卟啉(BOPP)后,通过荧光测定法分析了肿瘤,正常大脑和血液的活检样品。相对于正常大脑,该化合物以高达400:1的比例选择性地定位于肿瘤。胶质瘤细胞在体外和体内的共聚焦激光扫描显微镜观察表明,BOPP位于线粒体内,并从这些细胞的核中排除。小鼠肿瘤活检组织匀浆后,通过密度梯度超速离心证实了这种离散的亚细胞定位。这些化合物在肿瘤中的选择性离散定位表明该化合物可用作双重PDT / BNCT敏化剂。

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