MAGE-A9对人乳腺癌MDA-MB-231细胞中P53转录活性及功能的影响

Effect of melanoma-associated antigen-A9 on transcriptional activity and function of P53 in human breast cancer MDA-MB-231 cells

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摘要目的:探讨黑素瘤相关抗原-A9(melanoma-associated antigen,MAGE-A9)对人乳腺癌细胞中P53转录活性及功能的影响。方法:通过LipofectamineTM2000体外转染质粒pcDNA3.0、pcDNA3.0-p53、pCMV6-MAGE-A9和pcDNA3.0-p53/MAGE-A9至人乳腺癌MDA-MB-231细胞,RT-PCR和Western blotting检测细胞中p21WAF1mRNA和蛋白的表达,荧光素酶报告基因分析检测细胞中p21WAF1启动子介导的荧光素酶表达活性,MTT法检测转染不同质粒对MDA-MB-231细胞增殖的影响。结果:转染pcDNA3.0-p53/MAGE-A9组MDA-MB-231细胞中p21WAF1mRNA和蛋白表达水平均明显低于pcDNA3.0-p53组[(0.15±0.01)vs(0.18±0.02),(0.03±0.00)vs(0.06±0.01);均P<0.05]。转染pcDNA3.0-p53质粒可以增强MDAMB-231细胞中p21WAF1启动子介导的荧光素酶的表达[(58.56±3.47)vs(1.00±0.12),P<0.01],转染pcDNA3.0-p53/MAGE-A9后,MDA-MB-231细胞中p21WAF1启动子介导的荧光素酶的表达较转染pcDNA3.0-p53组明显降低[(22.02±4.91)vs(58.56±3.47),P<0.05]。与pcDNA3.0组相比,pcDNA3.0-p53组MDA-MB-231细胞增殖率明显明显降低[(228.89±22.39)%vs(337.23±23.67)%,P<0.05];而pcDNA3.0-p53/MAGE-A9组MDA-MB-231细胞增殖率明显高于pcDNA3.0-p53组[(291.51±5.91)%vs(228.89±22.39)%,P<0.05]。结论:MAGE-A9可抑制MDA-MB-231细胞中P53的转录活性及细胞增殖。 Objective ： To explore the effect of melanoma-associated antigen （MAGE）-A9 on the transcriptional activity and the function of P53. Methods： Plasmids pcDNA3.0, pcDNA3.0-p53 and pCMV6-MAGE-A9 were transfeced in vitro into human breast cancer MDA-MB-231 cells using LipofectamineTM2000. The expressions of p21WAF1 mRNA and protein in MDA-MB-231 cells were analyzed by RT-PCR and Western blotting. Luciferase reporter assay was performed to determine the luciferase activity induced by p21WAF1 promoter in MDA-MB-231 cells. MTT assay were adopted to explore the effect of different plasmids on the cell proliferation. Results： The expression of p21WAF1 both in mRNA and protein levels was decreased in pcDNA3.0-p53/MAGE-A9 group, compared with pcDNA3.0-p53 group （／[0.15±0.01／] vs ／[0.18±002／], ／[0.03±0.00／] vs ／[0.06±0.01／], P〈0.05）. The luciferase activity induced by p21WAF1 promoter was remarkably increased in MDA-MB-231 cells transfected with plasmid pcDNA3.0-p53 （／[58.56±3.47／] vs ／[1.00±012／], P〈001）. After transfected with pcDNA3.0-p53/MAGE-A9, the luciferase activity induced by p21WAF1 promoter in MDA-MB-231 cells was significantly reduced compared with that in pcDNA3.0-p53 group （／[22.02±4.91／] vs ／[58.56±3.47／], P〈005）. Compared with pcDNA3.0 group, the proliferation rate were significantly decreased in pcDNA3.0-p53 group （／[228.89±22.39／]% vs ／[337.23±23.67／]%, P〈0.05）, while in pcDNA3.0-p53/MAGE-A9 group, it was significantly higher than that in pcDNA3.0-p53 group （／[291.51±5.91／]% vs ／[228.89±22.39／]%, P〈0.05）. Conclusion： MAGE-A9 can inhibit the transcriptional activity of P53 and proliferation of MDA-MB-231 cells.

作者吕伟华桑梅香王彬于凡单保恩

机构地区河北医科大学第四医院科研中心河北医科大学第四医院肿瘤研究所

出处《中国肿瘤生物治疗杂志》 CAS CSCD 北大核心 2013年第5期535-539,共5页 Chinese Journal of Cancer Biotherapy

基金河北省卫生厅科研基金资助项目(No.20100120) 河北省自然科学基金资助项目(No.H2012206077)~~

关键词黑素瘤相关抗原-A9 P53 乳腺癌转录活性 MDA-MB-231细胞荧光素酶报告基因分析 melanoma-associated antigen-A9 （MAGE-A9） P53 breast cancer transcriptional activity MDA-MB-231 cell luciferase reporter gene assay

分类号 R737.9 [医药卫生—肿瘤] R730.2 [医药卫生—临床医学]

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参考文献21

1Meek DW, Marcar L. MAGE-A antigens as targets in tumour ther- apy [J]. Cancer Lett, 2012, 324(2):126-132. 被引量：1
2Ozaki T, Nakagawara A. P53 : The attractive tumor suppressor in the cancer research field [J]. J Biomed Biotechnol, 2011,2011 : 603925. 被引量：1
3Yang B, Herrin SM, Wu J, et al. MAGE-A, mMage-b, and MAGE-C proteins form complexes with KAP1 and suppress P53- dependent apoptosis in MAGE-positive cell lines [ J ]. Cancer Res, 2007, 67(20): 9954-9962. 被引量：1
4Monte M, Simonatto M, Peche LY, et al. MAGE-A tumor anti- gens target P53 transactivation function through histone deacetylase recruitment and confer resistance to chemotherapeutic agents [ J]. Proc Natl Acad Sci U S A, 2006, 103(30) : 11160-11165. 被引量：1
5桑梅香,单保恩,耿翠芝,高威.人黑素瘤抗原MAGE-A4对p53转录活性的影响[J].肿瘤,2009,29(5):428-432. 被引量：7
6丁春艳..肿瘤抗原MAGE-A9、-A10、-A12在乳腺癌组织中的表达及对乳腺癌细胞增殖的影响[D].河北医科大学,2011:
7Sang M, Wang L, Ding C, et al. Melanoma-associated antigen genes--an update [J]. Cancer Lett, 2011, 302(2) : 85-90. 被引量：1
8Meixiang S, Yishui L, Xinliang Z, et al. MAGE-A family: At- tractive targets for cancer immunotherapy [ J ]. Vaccine, 2011,29 (47) : 8496-8500. 被引量：1
9吕伟华,桑梅香,单保恩.MAGE－A基因亚家族及其在肿瘤临床上的应用前景[J].中国肿瘤生物治疗杂志,2013,20(2):242-246. 被引量：7
10Curigliano G, Viale G, Ghioni M, et al. Cancer-testis antigen ex- pression in triple-negative breast cancer [ J]. Ann Oncol, 2011, 22(1) : 98-103. 被引量：1

二级参考文献61

1吉晓滨,苏娟,陈敬贤,谢景华.黑色素瘤抗原在喉癌中的表达及临床评价[J].中华临床医师杂志（电子版）,2011,5(24):7271-7276. 被引量：7
2OHMAN FORSLUND K,NORDQVIST K.The melanoma antigen genes--any clues to their functions in normal tissues[J].Exp Cell Res,2001,265(2):185-194. 被引量：1
3BARKER PA,SALEHI A.The MAGE proteins:emerging roles in cell cycle progression,apoptosis,and neurogenetic disease[J].J Neurosci Res,2002,67(6):705- 712. 被引量：1
4MONTE M,SIMONATTO M,PECHE LY,et al.MAGE-A tumor antigens target p53 transactivation function through histone deacetylase recruitment and confer resistance to chemotherapeutic agents[J].Proc Natl Acad Sci USA,2006,103(30):11160-11165. 被引量：1
5NAGAO T,HIGASHITSUJI H,NONOGUCHI K,et al.MAGE-A4 interacts with the liver oncoprotein gankyrin and suppresses its tumorigenic activity[J].J Bio Chem,2003,278(12):10668-10674. 被引量：1
6SAKURAI T,ITOH K,HIGASHITSUJI H,et al.A cleaved form of MAGE-A4 binds to Miz-1 and induces apoptosis in human cells[J].J Biol Chem,2004,279(15):15505-15514. 被引量：1
7PEIKERT T,SPECKS U,FARVER C,et al.Melanoma antigen A4 is expressed in non-small cell lung cancers and promotes apoptosis[J].Cancer Res,2006,66(9):4693-4700. 被引量：1
8KAGHAD M,BONNET H,YANG A,et al.Monoallelically expressed gene related to p53 at 1p36,a region frequently deleted in neuroblastoma and other human cancers[J].Cell,1997,90(4):809-819. 被引量：1
9KOIDA N,OZAKI T,YAMAMOTO H,et al.Inhibitory role of Plk1 in the regulation of p73-dependent apoptosis through physical interaction and phosphorylation[J].J Biol Chem,2008,283(13):8555-8563. 被引量：1
10NAKANISHI M,OZAKI T,YAMAMOTO H,et al.NFBD1/MDC1 associates with p53 and regulates its function at the crossroad between cell survival and death in response to DNA damage[J].J Boil Chem,2007,282(31):22993-23004. 被引量：1

共引文献11

1吕伟华,桑梅香,单保恩.MAGE－A基因亚家族及其在肿瘤临床上的应用前景[J].中国肿瘤生物治疗杂志,2013,20(2):242-246. 被引量：7
2李广旭,宋平平,张百江.黑色素瘤相关抗原(MAGE)基因在肺癌中的表达及意义[J].中国肺癌杂志,2013,16(6):308-313. 被引量：4
3谢其美,陈军,桑红.恶性黑素瘤1例[J].中国麻风皮肤病杂志,2013,29(8):534-536.
4杨小岗,桑梅香,范晓杰,周欣亮,丁春艳,陈平,何翠颖,单保恩.乳腺癌组织中MAGE-A4和P73蛋白的表达及其临床意义[J].中国肿瘤生物治疗杂志,2013,20(5):597-602. 被引量：2
5李英彬,吕飞飞.外周血黑色素瘤抗原基因表达与胃癌转移及预后的关系[J].中国基层医药,2014,21(8):1134-1137.
6李宁,吉晓滨,谢景华,刘启才.葡萄球菌肠毒素A与黑色素瘤抗原A3共表达真核质粒致敏小鼠淋巴细胞对喉癌细胞模型的影响[J].中国耳鼻咽喉颅底外科杂志,2015,21(2):119-123. 被引量：1
7董丹宁,王多明,刘凯,胡云辉,王若峥.鼻咽癌MAGE-A1、MAGE-A3特异性CTL免疫应答差异与临床相关性[J].新疆医学,2016,46(11):1368-1372. 被引量：5
8张玉琴,陆云飞.TrKB及MAGE-A4在三阴性乳腺癌组织中的表达及其临床意义[J].广西医科大学学报,2018,35(5):668-671. 被引量：2
9赵英玲,黄望香,罗玲,叶春桃.重组人p53腺病毒转染急性早幼粒细胞白血病源性树突状细胞的免疫效应研究[J].黑龙江中医药,2018,47(4):57-60.
10李俊,孙继程,杜国新.脑胶质瘤患者血清黑色素瘤相关抗原-A3特异性细胞毒性T淋巴细胞免疫反应水平及临床意义[J].癌症进展,2020,18(22):2295-2299. 被引量：1

1彭延延,施秋萍,杨大朋,王海啸,马长艳.冬凌草甲素对人乳腺癌细胞侵袭的抑制作用及机制[J].苏州大学学报（医学版）,2012,32(3):318-321. 被引量：5
2徐莹莹,桑梅香,单保恩.肿瘤抗原MAGE与p53关系的研究进展[J].癌变．畸变．突变,2013,25(2):152-154. 被引量：2
3尚超,洪杨,郭艳,薛一雪.脑胶质瘤中miR-143对MACC1表达的调控作用[J].中国医科大学学报,2014,43(2):106-109. 被引量：3
4杨大朋,郭琼,郭依丹,彭延延,马长艳.Osterix在转移性乳腺癌细胞中的表达及对MMP-2、MMP-9和VEGF启动子活性的影响[J].苏州大学学报（医学版）,2010,30(3):466-469.
5魏付桥,申清香,刘昌化,罗康宁,谢文彪,胡军.PEITC通过抑制结肠癌细胞PI3K/NF-κB活性而抑制MMP-9表达[J].中南医学科学杂志,2014,42(4):351-354. 被引量：2
6方勇,魏付桥.白藜芦醇对乳腺癌患者基质金属蛋白酶9活性的影响[J].当代医学,2014,20(2):27-28. 被引量：1
7高海东,余之刚,江立玉,马榕,孙靖中.原癌基因gankyrin在乳腺浸润性导管癌中的表达研究[J].中华普通外科杂志,2007,22(9):683-686. 被引量：2
8朱娟娟,付汉江,朱捷,张胜权,郑晓飞.非编码基因MEG3稳定表达细胞株建立及其对p53转录活性的影响[J].军事医学,2011,35(6):424-427. 被引量：4
9刘海,秦学玲,鲜均明,周光耀,梁传余.纳米脂质体介导p53治疗鼻咽癌的实验研究[J].中国耳鼻咽喉颅底外科杂志,2008,14(1):21-24. 被引量：9
10刘玉斌,曹爱国,李之茂,谢静.白藜芦醇下调NF-κB介导的MMP-9表达抑制人NCI-H446细胞的侵袭迁移[J].实用预防医学,2013,20(9):1141-1144. 被引量：2

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MAGE-A9对人乳腺癌MDA-MB-231细胞中P53转录活性及功能的影响

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