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《天津医科大学学报》[ISSN:1006-8147/CN:12-1259/R]

卷:

28卷

期数:

2022年01期

页码:

40-46

栏目:

基础研究

出版日期:

2022-01-20

文章信息/Info

Title:

The effect of selumetinib on cell proliferation and apoptosis of malignant peripheral nerve sheath tumor

文章编号:

1006-8147（2022）01-0040-07

作者:

高雅¹; 赵洋¹; 朱香熹²; 赵玉龙¹; 李光明¹; 杨吉龙³; 叶帅⁴; 朱泽¹

（1.天津医科大学基础医学院病原生物学系，天津300070；2.遵义医科大学珠海校区临床医学系，珠海519090；3.天津医科大学肿瘤医院骨与软组织肿瘤科，天津300060；4.天津医科大学总医院护理部，天津300050）

Author(s):

GAO Ya¹; ZHAO Yang¹; ZHU Xiang-xi²; ZHAO Yu-long¹; LI Guang-ming¹; YANG Ji-long³; YE Shuai⁴; ZHU Ze¹

（1.Department of Pathogen Biology，School of Basic Medical Sciences，Tianjin Medical University，Tianjin 300070，China；2.Department of Clinical Medicine，Zhuhai Campus of Zunyi Medical University，Zhuhai 519090，China; 3.Department of Bone and Soft Tissue Oncology，Cancer Institute and Hospital，Tianjin Medical University，Tianjin 300060，China; 4. Department of nursing，General Hospital of Tianjin Medical University，Tianjin 300050，China）

关键词:

司美替尼; 恶性周围神经鞘瘤; H3K27me3; 增殖; 细胞凋亡

Keywords:

selumetinib; MPNST; H3K27me3; proliferation; apoptosis

分类号:

R739.43

DOI:

-

文献标志码:

A

摘要:

目的：探讨MEK1/2抑制剂司美替尼（selumetinib）对恶性周围神经鞘瘤（MPNST）细胞增殖和凋亡的影响及其机制。方法：用不同浓度的司美替尼处理细胞株ST88-14和STS26T，通过CCK-8、克隆形成、Transwell、细胞划痕、流式细胞术检测司美替尼对细胞增殖、凋亡、迁移和侵袭的影响。实时荧光定量PCR检测多梳抑制复合物2（PRC2）核心组分的mRNA表达水平。免疫印迹试验检测组蛋白3上的第27位赖氨酸的三甲基化（H3K27me3）的表达。结果：司美替尼抑制ST88-14、STS26T细胞增殖（t=16.44，P<0.05；t=16.21，P<0.05）、侵袭（t=10.51，P<0.05；t=8.44，P<0.05）、迁移（t=4.02，P<0.05；t=2.21，P<0.05）；与对照组相比，10 μmol/L和20 μmol/L司美替尼可使ST88-14、STS26T细胞凋亡率显著升高（t=14.64、10.10，均P<0.05；t=3.06、13.10，均P<0.05）；与对照组相比，司美替尼作用于ST88-14、STS26T细胞48 h，PRC2核心组分SUZ12和EZH2的mRNA水平显著升高（t=13.39、16.84，均P<0.05；t=6.10、12.93，均P<0.05）；与对照组相比，20 μmol/L司美替尼可显著增加ST88-14，STS26T细胞H3K27me3的表达（t=12.82，P<0.05；t=18.78，P<0.05）。结论：司美替尼通过促进H3K27me3表达抑制MPNST细胞的增殖，促进细胞凋亡。

Abstract:

Objective：To investigate the effects of selumetinib，a MEK1/2 inhibitor，on cell proliferation and apoptosis of malignant peripheral nerve sheath tumor（MPNST） and its mechanism. Methods: Cell lines ST88-14 and STS26T were treated with selumetinib at different concentrations，and the effects of selumetinib on cell proliferation，apoptosis，migration and invasion were detected by CCK-8 assay，colony formation assay，Transwell assay，cell scratch assay and flow cytometry.The mRNA expression level of each core component of PRC2 was detected by real-time fluorescence quantitative PCR. Western blotting assay was used to detect the expression of trimethylation of lysine 27 on histone 3（H3K27me3）. Results: Selumetinib inhibited the proliferation（t=16.44，P<0.05；t=16.21，P<0.05），invasion（t=10.51，P<0.05；t=8.44，P<0.05） and migration（t=4.02，P<0.05；t=2.21，P<0.05） of ST88-14，STS26T cells. Compared with the control group，the apoptosis rates of ST88-14 and STS26T cells were significantly increased when drug concentrations were 10 μmol/L and 20 μmol/L（t=14.64，10.10，both P<0.05; t=3.06，13.10，both P<0.05）. Compared with the control group，the mRNA levels of SUZ12 and EZH2，the core components of PRC2，were significantly increased by selumetinib for 48 h after treatment with ST88-14 and STS26T cells（t=13.39，16.84，both P<0.05；t=6.10，12.93，both P<0.05）. Compared with the control group，20 μmol/L selumetinib significantly increased the expression of H3K27me3 in ST88-14 and STS26T cells（t=12.82，P<0.05；t =18.78，P<0.05）. Conclusion: Selumetinib can inhibit the proliferation of MPNST cell lines and promote apoptosis by promoting the expression of H3K27me3.

参考文献/References:

[1] 廖智超，张超，刘新月，等.恶性周围神经鞘瘤靶向治疗的研究进展[J].中华肿瘤杂志，2019，41（9）：648-653.
[2] KORFHAGE J，LOMBARD D B. Malignantperipheral nerve sheath tumors：from epigenome to bedside[J]. Mol Cancer Res，2019，17（7）：1417-1428.
[3] WOJCIK J B，MARCHIONE D M，SIDOLI S，et al. Epigenomic reordering induced by polycomb loss drives oncogenesis but leads to therapeutic vulnerabilities in malignant peripheral nerve sheath tumors[J]. Cancer Res，2019，79（13）：3205-3219.
[4] CONWAY E，HEALY E，BRACKEN AP. PRC2 mediated H3K27 methylations in cellular identity and cancer[J]. Curr Opin Cell Biol，2015，37：42-48 .
[5] DU X，YANG J，YLIPAA A，et al. Genomic amplification and high expression of EGFR are key targetable oncogenic events in malignant peripheral nerve sheath tumor[J]. J Hematol Oncol，2013，6（1）：503-505.
[6] De RAEDT T，BEERT E，PASMANT E，et al. PRC2 loss amplifies ras-driven transcription and confers sensitivity to BRD4-based therapies[J]. Nature，2014 ，514（7521）：247-251.
[7] WACHTER S，WUNDERLICH A，GREENE BH，et al. Selumetinib activity in thyroid cancer cells： modulation of sodium iodide symporter and associated miRNAs[J]. Int J Mol Sci，2018，19（7）：2077.
[8] MOORE A R，ROSENBERG SC，MCCORMICK F，et al. Ras-targeted therapies：is the undruggable drugged？[J]. Nat Rev Drug Discov，2020，19（8）：533-552.
[9] XIA M，LI X，DIAO Y，et al. Targeted inhibition of glutamine metabolism enhances the antitumor effect of selumetinib in Kras-mutant NSCLC[J].Transl Oncol，2021，14（1）：100920.
[10] DAVIES B R，LOGIE A，MCKAY J S，et al. AZD6244 （ARRY-142886），a potent inhibitor of mitogen-activated protein kinase/extracellular signal-regulated kinase kinase 1/2 kinases：mechanism of action in vivo，pharmacokinetic/pharmacodynamic relationship，and potential for combination in preclinical models[J]. Mol Cancer Ther，2007，6（8）：2209-2219.
[11] FARLEY J，BRADY W E，VATHIPADIEKAL V，et al. Selumetinib in women with recurrent low-grade serous carcinoma of the ovary or peritoneum：an open-label，single-arm，phase 2 study[J]. Lancet Oncol，2013，14（2）：134-140.
[12] 夏训明.美国FDA批准Koselugo（selumetinib/司美替尼单抗）用于儿童治疗神经纤维瘤病1型[J].广东药科大学学报，2020， 36（3）：416.
[13] GROSS A M，WOLTER P L，DOMBI E，et al. Selumetinib in children with inoperable plexiform neurofibromas[J]. N Engl J Med，2020，382（15）：1430-1442.
[14] 软组织和骨肿瘤分子病理学检测专家共识（2019年版）[J].中华病理学杂志，2019，48（7）：505-509.
[15] BATES S E. Epigenetic therapies for cancer[J]. N Engl J Med，2020， 383（7）：650-663
[16] ZHANG M，WANG Y，JONES S，et al. Somatic mutations of SUZ12 in malignant peripheral nerve sheath tumors[J]. Nat Genet，2014， 46（11）：1170-1172.
[17] LEE W，TECKIE S，WIESNER T，et al. PRC2 is recurrently inactivated through EED or SUZ12 loss in malignant peripheral nerve sheath tumors[J]. Nat Genet，2014，46（11）：1227-1232.
[18] 宋紫暄，李光明，张静，等.H3K27三甲基化蛋白可作为MPNST的重要诊断标记物[J].天津医科大学学报，2018，24（4）：353-356.

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　SONG Zi-xuan,LI Guang-ming,ZHANG Jing,et al.H3K27me3 is a highly sensitive diagnostic marker for MPNST[J].Journal of Tianjin Medical University,2018,24(01):353.
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备注/Memo

备注/Memo:

基金项目 国家自然科学基金（81672650）
作者简介 高雅（1995-），女，硕士在读，研究方向：病原生物学；通信作者：朱泽，E-mail: zhuze@tmu.edu.cn。

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更新日期/Last Update: 2022-01-20