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新型放射增敏剂组合增强微束放射治疗在脑癌治疗中的生物剂量测定

Microbeam Radiation Therapy Bio-Dosimetry Enhanced by Novel Radiosensitiser Combinations in the Treatment of Brain Cancer.

作者信息

Valceski Michael, Engels Elette, Vogel Sarah, Paino Jason, Potter Dylan, Hollis Carolyn, Khochaiche Abass, Barnes Micah, O'Keefe Alice, Cameron Matthew, Roughley Kiarn, Rosenfeld Anatoly, Lerch Michael, Corde Stéphanie, Tehei Moeava

机构信息

Centre for Medical Radiation Physics, University of Wollongong, Wollongong, NSW 2522, Australia.

Molecular Horizons, University of Wollongong, Wollongong, NSW 2522, Australia.

出版信息

Cancers (Basel). 2024 Dec 19;16(24):4231. doi: 10.3390/cancers16244231.

Abstract

: Brain cancer is notoriously resistant to traditional treatments, including radiotherapy. Microbeam radiation therapy (MRT), arrays of ultra-fast synchrotron X-ray beams tens of micrometres wide (called peaks) and spaced hundreds of micrometres apart (valleys), is an effective alternative to conventional treatments. MRT's advantage is that normal tissues can be spared from harm whilst maintaining tumour control. Combining MRT with targeted radiosensitisers, such as nanoparticles, chemotherapeutic drugs, and halogenated pyrimidine drugs, can further improve radiotherapy by enhancing radiation damage. However, the underlying mechanisms of MRT are still being understood, which is essential to ensuring the reliable and successful use of MRT. : An in vitro study was performed using γH2AX imaging, and quantification was performed via confocal microscopy and a clonogenic cell survival assay. : We show that methotrexate chemotherapeutics and iododeoxyuridine enhance MRT cell-killing and thulium oxide nanoparticles (TmNPs) broaden MRT peaks, and using γH2AX immunofluorescent confocal microscopy to quantify DNA damage, we further our knowledge of MRT mechanisms. γH2AX images verify the biological responses of cells aligning with the physical collimation of MRT, and we can accurately measure MRT microbeam characteristics bio-dosimetrically. The peak-to-valley dose ratio (PVDR), the ratio of the peak dose to the valley dose that characterises an MRT field, was accurately measured biologically using γH2AX imaging, despite studies previously finding this challenging. : The measurement of biological PVDR has been performed for the first time with high-Z radiosensitisers, including nanoparticles, and several novel radiosensitiser-enhanced MRT mechanisms were discovered. Our results deepen our understanding of MRT with radiosensitisers, and can contribute to its accurate and future successful use in treating cancer.

摘要

脑癌对包括放疗在内的传统治疗方法具有 notoriously 的抗性。微束放射治疗(MRT)是由宽度为数十微米(称为峰)且间隔数百微米(谷)的超快同步加速器 X 射线束阵列组成,是传统治疗方法的一种有效替代方案。MRT 的优势在于可以在控制肿瘤的同时使正常组织免受伤害。将 MRT 与靶向放射增敏剂(如纳米颗粒、化疗药物和卤代嘧啶药物)相结合,可以通过增强辐射损伤进一步改善放疗效果。然而,MRT 的潜在机制仍在研究中,这对于确保 MRT 的可靠和成功应用至关重要。:使用γH2AX 成像进行了一项体外研究,并通过共聚焦显微镜和克隆形成细胞存活测定进行了定量分析。:我们表明,甲氨蝶呤化疗药物和碘脱氧尿苷可增强 MRT 的细胞杀伤作用,氧化铥纳米颗粒(TmNPs)可拓宽 MRT 峰,并且使用γH2AX 免疫荧光共聚焦显微镜对 DNA 损伤进行定量分析,我们进一步了解了 MRT 机制。γH2AX 图像验证了细胞的生物学反应与 MRT 的物理准直一致,并且我们可以通过生物剂量学准确测量 MRT 微束特征。尽管此前的研究发现测量表征 MRT 场的峰剂量与谷剂量之比(PVDR)具有挑战性,但使用γH2AX 成像在生物学上准确测量了该比值。:首次使用包括纳米颗粒在内的高 Z 放射增敏剂进行了生物 PVDR 的测量,并发现了几种新型放射增敏剂增强 MRT 的机制。我们的结果加深了我们对 MRT 与放射增敏剂的理解,并有助于其在未来准确且成功地用于癌症治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/98c3/11674565/456eebb64d36/cancers-16-04231-g0A1.jpg

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