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在细胞培养和犬科癌症患者中,评估一种与羟基脲或替莫唑胺联合应用的前胱冬酶-3 激活剂对高级别脑膜瘤的作用。

Evaluation of a procaspase-3 activator with hydroxyurea or temozolomide against high-grade meningioma in cell culture and canine cancer patients.

机构信息

Department of Chemistry, University of Illinois at Urbana-Champaign, Urbana, Illinois, USA.

Carl R. Woese Institute for Genomic Biology, University of Illinois at Urbana-Champaign, Urbana, Illinois, USA.

出版信息

Neuro Oncol. 2021 Oct 1;23(10):1723-1735. doi: 10.1093/neuonc/noab161.

Abstract

BACKGROUND

High-grade meningioma is an aggressive type of brain cancer that is often recalcitrant to surgery and radiotherapy, leading to poor overall survival. Currently, there are no FDA-approved drugs for meningioma, highlighting the need for new therapeutic options, but development is challenging due to the lack of predictive preclinical models.

METHODS

To leverage the known overexpression of procaspase-3 in meningioma, PAC-1, a blood-brain barrier penetrant procaspase-3 activator, was evaluated for its ability to induce apoptosis in meningioma cells. To enhance the effects of PAC-1, combinations with either hydroxyurea or temozolomide were explored in cell culture. Both combinations were further investigated in small groups of canine meningioma patients and assessed by MRI, and the novel apoptosis tracer, [18F]C-SNAT4, was evaluated in patients treated with PAC-1 + HU.

RESULTS

In meningioma cell lines in culture, PAC-1 + HU are synergistic while PAC-1 + TMZ show additive-to-synergistic effects. In canine meningioma patients, PAC-1 + HU led to stabilization of disease and no change in apoptosis within the tumor, whereas PAC-1 + TMZ reduced tumor burden in all three canine patients treated.

CONCLUSIONS

Our results suggest PAC-1 + TMZ as a potentially efficacious combination for the treatment of human meningioma, and also demonstrate the utility of including pet dogs with meningioma as a means to assess anticancer strategies for this common brain tumor.

摘要

背景

高级别脑膜瘤是一种侵袭性脑癌,通常对手术和放疗具有抗性,导致整体生存率较差。目前,尚无 FDA 批准用于脑膜瘤的药物,这凸显了对新治疗选择的需求,但由于缺乏预测性临床前模型,开发具有挑战性。

方法

利用已知的脑膜瘤中 procaspase-3 的过表达,评估了穿透血脑屏障的 procaspase-3 激活剂 PAC-1 诱导脑膜瘤细胞凋亡的能力。为了增强 PAC-1 的效果,在细胞培养中探索了与羟基脲或替莫唑胺联合用药的方法。这两种组合在一小部分犬脑膜瘤患者中进一步进行了研究,并通过 MRI 进行评估,并在接受 PAC-1 + HU 治疗的患者中评估了新型凋亡示踪剂[18F]C-SNAT4。

结果

在脑膜瘤细胞系中,PAC-1 + HU 具有协同作用,而 PAC-1 + TMZ 则表现出相加至协同作用。在犬脑膜瘤患者中,PAC-1 + HU 导致疾病稳定,肿瘤内凋亡无变化,而 PAC-1 + TMZ 使所有 3 名接受治疗的犬患者的肿瘤负担减少。

结论

我们的结果表明 PAC-1 + TMZ 可能是治疗人类脑膜瘤的有效联合用药,并且还证明了将患有脑膜瘤的宠物狗纳入评估这种常见脑肿瘤的抗癌策略的一种手段的实用性。

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