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本文引用的文献

1
The biological underpinnings of radiation therapy for vestibular schwannomas: Review of the literature.前庭神经鞘瘤放射治疗的生物学基础:文献综述
Laryngoscope Investig Otolaryngol. 2021 Mar 30;6(3):458-468. doi: 10.1002/lio2.553. eCollection 2021 Jun.
2
The natural history of vestibular schwannoma growth-prospective 40-year data from an unselected national cohort.前庭神经鞘瘤生长的自然史——来自一个未选择的全国队列的40年前瞻性数据。
Neuro Oncol. 2021 May 5;23(5):827-836. doi: 10.1093/neuonc/noaa230.
3
Effects of Neurod1 Expression on Mouse and Human Schwannoma Cells.神经调节蛋白 1 表达对小鼠和人许旺细胞瘤细胞的影响。
Laryngoscope. 2021 Jan;131(1):E259-E270. doi: 10.1002/lary.28671. Epub 2020 May 21.
4
The JNK inhibitor AS602801 Synergizes with Enzalutamide to Kill Prostate Cancer Cells In Vitro and In Vivo and Inhibit Androgen Receptor Expression.JNK抑制剂AS602801与恩杂鲁胺协同作用,在体外和体内杀死前列腺癌细胞并抑制雄激素受体表达。
Transl Oncol. 2020 Apr;13(4):100751. doi: 10.1016/j.tranon.2020.100751. Epub 2020 Mar 18.
5
Combination therapy with mTOR kinase inhibitor and dasatinib as a novel therapeutic strategy for vestibular schwannoma.mTOR 激酶抑制剂联合 dasatinib 作为一种治疗前庭神经鞘瘤的新策略。
Sci Rep. 2020 Mar 6;10(1):4211. doi: 10.1038/s41598-020-60156-6.
6
Natural History of Sporadic Vestibular Schwannoma: A Volumetric Study of Tumor Growth.散发型前庭神经鞘瘤自然史:肿瘤生长的容积学研究。
Otolaryngol Head Neck Surg. 2018 Sep;159(3):535-542. doi: 10.1177/0194599818770413. Epub 2018 Apr 24.
7
Combination Therapy with c-Met and Src Inhibitors Induces Caspase-Dependent Apoptosis of Merlin-Deficient Schwann Cells and Suppresses Growth of Schwannoma Cells.c-Met 和Src 抑制剂联合治疗诱导 Merlin 缺陷雪旺细胞的 caspase 依赖性凋亡并抑制神经鞘瘤细胞的生长。
Mol Cancer Ther. 2017 Nov;16(11):2387-2398. doi: 10.1158/1535-7163.MCT-17-0417. Epub 2017 Aug 3.
8
Calculating the Tumor Volumes in Vestibular Schwannomas: Are the ABC/2 and Volumetric Methods Comparable?计算前庭神经鞘瘤的肿瘤体积:ABC/2法和容积法是否具有可比性?
Otol Neurotol. 2017 Jul;38(6):889-894. doi: 10.1097/MAO.0000000000001423.
9
The importance of nerve microenvironment for schwannoma development.神经微环境对神经鞘瘤发展的重要性。
Acta Neuropathol. 2016 Aug;132(2):289-307. doi: 10.1007/s00401-016-1583-8. Epub 2016 May 28.
10
Bentamapimod (JNK Inhibitor AS602801) Induces Regression of Endometriotic Lesions in Animal Models.苯达莫德(JNK抑制剂AS602801)在动物模型中可诱导子宫内膜异位症病灶消退。
Reprod Sci. 2016 Jan;23(1):11-23. doi: 10.1177/1933719115600553. Epub 2015 Sep 2.

应用 c-Jun N-末端激酶抑制剂 AS602801 治疗后体外和体内散发性和神经纤维瘤病 2 型相关前庭神经鞘瘤生长减少。

Reduction of sporadic and neurofibromatosis type 2-associated vestibular schwannoma growth in vitro and in vivo after treatment with the c-Jun N-terminal kinase inhibitor AS602801.

机构信息

1Department of Neurosurgery, University of Iowa, Iowa City.

2Department of Otolaryngology-Head and Neck Surgery, University of Iowa, Iowa City, Iowa; and.

出版信息

J Neurosurg. 2022 Sep 9;138(4):962-971. doi: 10.3171/2022.7.JNS22934. Print 2023 Apr 1.

DOI:10.3171/2022.7.JNS22934
PMID:36087315
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10193498/
Abstract

OBJECTIVE

Vestibular schwannomas (VSs) are benign nerve sheath tumors that result from mutation in the tumor suppressor gene NF2, with functional loss of the protein merlin. The authors have previously shown that c-Jun N-terminal kinase (JNK) is constitutively active in human VS cells and plays a central role in their survival by suppressing accumulation of mitochondrial superoxides, implicating JNK inhibitors as a potential systemic treatment for VS. Thus, the authors hypothesized that the adenosine 5'-triphosphate-competitive JNK inhibitor AS602801 would demonstrate antitumor activity in multiple VS models.

METHODS

Treatment with AS602801 was tested in primary human VS cultures, human VS xenografts, and a genetic mouse model of schwannoma (Postn-Cre;Nf2flox/flox). Primary human VS cell cultures were established from freshly obtained surgical tumor specimens; treatment group media was enriched with AS602801. VS xenograft tumors were established in male athymic nude mice from freshly collected human tumor. Four weeks postimplantation, a pretreatment MRI scan was obtained, followed by 65 days of AS602801 (n = 18) or vehicle control (n = 19) treatment. Posttreatment MRI scans were used to measure final tumor volume. Tumors were then harvested. Finally, Postn-Cre;Nf2flox/flox mice were treated with AS602801 (n = 10) or a vehicle (n = 13) for 65 days. Posttreatment auditory brainstem responses were obtained. Dorsal root ganglia from Postn-Cre;Nf2flox/flox mice were then harvested. In all models, schwannoma identity was confirmed with anti-S100 staining, cell proliferation was measured with the EdU assay, and cell death was measured with terminal deoxynucleotidyl transferase-mediated dUTP nick-end labeling staining. All protocols were approved by the local institutional review board and Institutional Animal Care and Use Committees.

RESULTS

Treatment with AS602801 decreased cell proliferation and increased apoptosis in primary human VS cultures. The systemic administration of AS602801 in mice with human VS xenografts reduced tumor volume and cell proliferation. Last, the AS602801-treated Postn-Cre;Nf2flox/flox mice demonstrated decreased cell proliferation in glial cells in the dorsal root ganglia. However, AS602801 did not significantly delay hearing loss in Postn-Cre;Nf2flox/flox mice up to 3 months posttreatment.

CONCLUSIONS

The data suggest that JNK inhibition with AS602801 suppresses growth of sporadic and neurofibromatosis type 2-associated VSs. As such, AS602801 is a potential systemic therapy for VS and warrants further investigation.

摘要

目的

前庭神经鞘瘤(VSs)是良性神经鞘瘤,由肿瘤抑制基因 NF2 突变引起, Merlin 蛋白功能丧失。作者先前表明,c-Jun N 末端激酶(JNK)在人 VS 细胞中持续激活,通过抑制线粒体超氧化物的积累来发挥其存活的核心作用,这暗示 JNK 抑制剂可能是 VS 的一种潜在全身性治疗方法。因此,作者假设,三磷酸腺苷竞争性 JNK 抑制剂 AS602801 将在多种 VS 模型中显示出抗肿瘤活性。

方法

在原代人 VS 培养物、人 VS 异种移植物和施万细胞瘤的遗传小鼠模型(Postn-Cre;Nf2flox/flox)中测试 AS602801 的治疗效果。从新获得的手术肿瘤标本中建立原代人 VS 细胞培养物;治疗组培养基中富含 AS602801。从新收集的人类肿瘤中,在雄性无胸腺裸鼠中建立 VS 异种移植物肿瘤。植入后 4 周,进行预处理 MRI 扫描,然后进行 65 天的 AS602801(n=18)或载体对照(n=19)治疗。治疗后进行 MRI 扫描,以测量最终肿瘤体积。然后收获肿瘤。最后,用 AS602801(n=10)或载体(n=13)治疗 Postn-Cre;Nf2flox/flox 小鼠 65 天。治疗后获得听觉脑干反应。然后从 Postn-Cre;Nf2flox/flox 小鼠中收获背根神经节。在所有模型中,用抗 S100 染色确认施万细胞瘤的身份,用 EdU 测定法测量细胞增殖,用末端脱氧核苷酸转移酶介导的 dUTP 缺口末端标记染色法测量细胞死亡。所有方案均获得当地机构审查委员会和机构动物护理和使用委员会的批准。

结果

AS602801 治疗降低了原代人 VS 培养物中的细胞增殖并增加了细胞凋亡。在携带人 VS 异种移植物的小鼠中,AS602801 的全身给药减少了肿瘤体积和细胞增殖。最后,用 AS602801 治疗的 Postn-Cre;Nf2flox/flox 小鼠在背根神经节中的神经胶质细胞中表现出细胞增殖减少。然而,AS602801 并没有显著延迟 Postn-Cre;Nf2flox/flox 小鼠在治疗后 3 个月内的听力损失。

结论

数据表明,用 AS602801 抑制 JNK 可抑制散发性和神经纤维瘤病 2 型相关 VSs 的生长。因此,AS602801 可能是 VS 的一种潜在全身性治疗方法,值得进一步研究。