FACT inhibitor CBL0137, administered in an optimized schedule, potentiates radiation therapy for glioblastoma by suppressing DNA damage repair

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-09-09 DOI:10.1007/s11060-024-04819-8
Tara A. Barone, Denisha L. Robinson, Jingxin Qiu, Katerina V. Gurova, Andrei A. Purmal, Andrei V. Gudkov, Robert J. Plunkett
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Abstract

Purpose

Standard-of-care for glioblastoma remains surgical debulking followed by temozolomide and radiation. However, many tumors become radio-resistant while radiation damages surrounding brain tissue. Novel therapies are needed to increase the effectiveness of radiation and reduce the required radiation dose. Drug candidate CBL0137 is efficacious against glioblastoma by inhibiting histone chaperone FACT, known to be involved in DNA damage repair. We investigated the combination of CBL0137 and radiation on glioblastoma.

Methods

In vitro, we combined CBL0137 with radiation on U87MG and A1207 glioblastoma cells using the clonogenic assay to evaluate the response to several treatment regimens, and the Fast Halo Assay to examine DNA repair. In vivo, we used the optimum combination treatment regimen to evaluate the response of orthotopic tumors in nude mice.

Results

In vitro, the combination of CBL0137 and radiation is superior to either alone and administering CBL0137 two hours prior to radiation, having the drug present during and for a prolonged period post-radiation, is an optimal schedule. CBL0137 inhibits DNA damage repair following radiation and affects the subcellular distribution of histone chaperone ATRX, a molecule involved in DNA repair. In vivo, one dose of CBL0137 is efficacious and the combination of CBL0137 with radiation increases median survival over either monotherapy.

Conclusions

CBL0137 is most effective with radiation for glioblastoma when present at the time of radiation, immediately after and for a prolonged period post-radiation, by inhibiting DNA repair caused by radiation. The combination leads to increased survival making it attractive as a dual therapy.

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FACT抑制剂CBL0137通过抑制DNA损伤修复,以优化的时间表给药,增强了胶质母细胞瘤放射治疗的效果
目的 治疗胶质母细胞瘤的标准仍然是手术切除,然后使用替莫唑胺和放射治疗。然而,许多肿瘤会对放射线产生抗药性,而放射线会损害周围的脑组织。我们需要新的疗法来提高放射治疗的有效性并减少所需的放射剂量。候选药物CBL0137通过抑制已知参与DNA损伤修复的组蛋白伴侣FACT对胶质母细胞瘤有疗效。我们研究了 CBL0137 和放射线对胶质母细胞瘤的联合作用。方法在体外,我们将 CBL0137 和放射线联合作用于 U87MG 和 A1207 胶质母细胞瘤细胞,使用克隆形成试验评估对几种治疗方案的反应,并使用快速光晕试验检测 DNA 修复。结果在体外,CBL0137 和放射线的组合优于单独使用其中一种。在放射线照射前两小时服用 CBL0137,并在照射期间和照射后长时间服用该药物,是一种最佳的治疗方案。CBL0137 可抑制辐射后的 DNA 损伤修复,并影响组蛋白伴侣 ATRX(一种参与 DNA 修复的分子)的亚细胞分布。结论CBL0137通过抑制辐射引起的DNA修复,在放射治疗胶质母细胞瘤时与放射治疗同时使用、放射治疗后立即使用和放射治疗后长期使用效果最佳。联合用药可提高生存率,因此作为一种双重疗法很有吸引力。
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CiteScore
7.20
自引率
4.30%
发文量
567
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