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通过优化声动力疗法和辐射增敏剂对长链非编码RNA PVT1和miR-1204表达的影响来克服乳腺癌细胞的治疗耐药性。

Overcoming breast cancer cell treatment resistance by optimizing sonodynamic therapy and radiation sensitizers on lncRNA PVT1 and miR-1204 expression.

作者信息

Neshastehriz Ali, Hormozi-Moghaddam Zeinab, Kichi Zahra Abedi, Taheri Seyedeh Mona, Amini Seyed Mohammad, Aghaei Amir

机构信息

Radiation Biology Research center, Iran University of Medical Sciences (IUMS), Tehran, Iran; Department of Radiation Sciences, Allied Medicine Faculty, Iran University of Medical Sciences, Tehran, Iran.

Department of Genetics, Faculty of biological Sciences, Tarbiat Modares University, Tehran, Iran.

出版信息

Photodiagnosis Photodyn Ther. 2025 Feb;51:104433. doi: 10.1016/j.pdpdt.2024.104433. Epub 2024 Dec 5.

Abstract

BACKGROUND

Acoustic cavitation is a foundational mechanism in ultrasound therapy, primarily through inertial cavitation resulting from microbubble collapse. Sonodynamic therapy, with inertial acoustic cavitation threshold and low-dose radiation in the presence of sensitizers, may provide significant effects for cancer treatment, potentially overcoming resistance encountered with single therapies.

METHODS

MCF7 breast cancer cells were subjected to sonodynamic therapy either alone or combined with ionizing radiation, gold nanoparticles coated with apigenin, and methylene blue. Several parameters were evaluated, including reactive oxygen species (ROS) generation and colonization. Additionally, the investigation included assessing the long non-coding RNA (lncRNA) PTV1 with miRNA1204 and related genes using Real-Time PCR.

RESULTS

Sonodynamic therapy at a mechanical index of 0.31 as acoustic cavitation threshold increased intracellular ROS. Combining sonodynamic therapy and 2 Gy X-ray radiation with methylene blue and gold nanoparticles coated with apigenin significantly decreased plating efficiency (4.44±1.69), and survival fraction (2.75±1.98) compared with control (Ctrl.) (98.77±4.49) and (97.59± 2.94), respectively. This was associated with a marked increase in ROS with a mean fluorescence intensity of 20,576.2 ± 4.6 (>4.5 times). The combined treatment also increased p53 expression and decreased the expression of PVT1, miR-1204, and related genes.

CONCLUSION

Sonodynamic therapy in inertial acoustic cavitation threshold, combined with ionizing radiation in the presence of biocompatible nanoparticles, could enhance the therapeutic effects on the miR-1204, derived from lncRNA PVT1, that functions as an oncogenic microRNA in breast cancer. This approach has the potential to overcome treatment resistance encountered with single therapies.

摘要

背景

声空化是超声治疗的一种基本机制,主要通过微泡破裂产生的惯性空化实现。在存在敏化剂的情况下,具有惯性声空化阈值和低剂量辐射的声动力疗法可能对癌症治疗产生显著效果,有可能克服单一疗法所遇到的耐药性。

方法

MCF7乳腺癌细胞单独接受声动力疗法,或与电离辐射、载有芹菜素的金纳米颗粒及亚甲蓝联合使用。评估了几个参数,包括活性氧(ROS)生成和集落形成。此外,研究还包括使用实时聚合酶链反应评估长链非编码RNA(lncRNA)PTV1与miRNA1204及相关基因。

结果

以0.31的机械指数作为声空化阈值进行声动力疗法可增加细胞内ROS。与对照组(分别为98.77±4.49和97.59±2.94)相比,声动力疗法与2 Gy X射线辐射联合亚甲蓝和载有芹菜素的金纳米颗粒显著降低了接种效率(4.44±1.69)和存活分数(2.75±1.98)。这与ROS显著增加相关,平均荧光强度为20,576.2±4.6(>4.5倍)。联合治疗还增加了p53表达,并降低了PVT1、miR-1204及相关基因的表达。

结论

在惯性声空化阈值下的声动力疗法,与生物相容性纳米颗粒存在下的电离辐射联合使用,可增强对源自lncRNA PVT1的miR-1204的治疗效果,miR-1204在乳腺癌中起致癌微小RNA的作用。这种方法有可能克服单一疗法所遇到的治疗耐药性。

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