|
|
|
| Efects of Eucommia ulmoides oliver flavones on apoptotic of pediatric hemangioma endothelial cells |
| LI Yang1 LIU Guoliang2 YAO Yuan2 ZHANG Ning2▲ GUO Wei3▲ |
1.Department of Pediatric Surgery, Jinzhou Maternity and Infant Hospital, Liaoning Province, Jinzhou 121000, China;
2.College of Jiamusi, Heilongjiang University of Chinese Medicine, Heilongjiang Province, Jiamusi 154007, China;
3.The First Affiliated Hospital of Heilongjiang University of Chinese Medicine, Heilongjiang Province, Harbin 150041, China |
|
|
|
Abstract Objective To study the influence of Eucommia ulmoides oliver flavones (EUOF) on apoptosis of infantile hemangioma endothelial cell. Methods Infantile hemangioma endothelial cells were cultured in vitro. The cells was divided into blank groups (normal cultivate infantile hemangioma endothelial cells), high dose group of EUOF (50 μg/mL EUOF treatment infantile hemangioma endothelial cells), the middle dose group (5 μg/mL EUOF treatment infantile hemangioma endothelial cells), the low dose group (0.5 μg/mL EUOF treatment children hemangioma endothelial cells), then cultured for 72 hours, MTT method detected cell vitality. The TUNEL method detected apoptosis of cells; Western blot method detected expression levels of apoptosis related proteins Bax, Bcl-2 and caspase-9 in infantile hemangioma endothelial cell. Results Compared to the blank group, infantile hemangioma endothelial cell proliferation could inhibit in EUOF middle dose group, high dose group, the differences were statistically significant (P < 0.05). The rate of apoptosis in high dosages group and middle dosages group rose, the differences were statistically significant (P < 0.05); the expression of Bax in high dose group rose, differences were statistically significant (P < 0.01). The expression of caspase-9 potein in the high dose group middle dose group and low dose group rose, the differences were statistically significant (P < 0.05). The expression of bcl-2 in high dose group, middle dose group decreased, the differences were statistically significant (P < 0.05). Conclusion EUOF can inhibit the the expression of Bcl-2 protein and promote the expression of Bax and caspase-9 in infantile hemangioma endothelial cells, that is expected to be an effective therapeutic agent in the disease of hemangioma.
|
|
|
|
|
|
[1] 陈晓东,林晓曦.婴小儿血管瘤发病机制的研究进展[J].组织工程与重建外科,2010,22(3):18-19.
[2] 陈超,杨体泉.婴小儿血管瘤内皮细胞凋亡研究进展[J].中华实用儿科临床杂志,2007,22(11):869-871.
[3] 马刚,林晓曦,金云波,等.婴小儿血管瘤发生与消退的研究进展[J].中华小儿外科杂志,2007,28(5):266-268.
[4] 刘国林.婴小儿血管瘤增殖、退化机制的研究进展[J].当代医学,2010,16(1):27-29.
[5] 赵卓,张艳,张园程,等.婴小儿皮肤血管瘤的治疗现状及研究进展[J].实用皮肤病学杂志,2013,6(4):224-226.
[6] Yu H,Littlewood T,Bennett M. Forkhead transcription factor FOXO3a potently induces smooth muscle cell apoptosis and promotes extracellular matrix degradation through activation of matrix metalloproteinases [J]. Atherosclerosis,2014,235(2):e24.
[7] 丁艳霞,郭洋静,任莹璐,等.杜仲雄花中黄酮类化学成分及其抗氧化活性研究[J].中草药,2014,45(3):323-327.
[8] 冯晗,周宏灏,欧阳冬生.杜仲的化学成分及药理作用研究进展[J].中国临床药理学与治疗学,2015,20(6):713-720.
[9] 曾超珍,刘志祥.微波提取杜仲总黄酮的工艺研究[J].时珍国医国药,2009,20(5):1170-1171.
[10] 彭红梅,李小姝.杜仲的药理研究现状及应用展望[J].中医学报,2013,28(1):72-73.
[11] Radhakrishna PG,Srivastava AS,Hassanein TI,et al. Induction of apoptosis in human lung cancer cells by curcumin [J]. Cancer Lett,2004,208(2):163-170.
[12] Mat hiasen IS,Sergeev IN,Bast holm L,et al. Calcium and calpain askey mediators of apoptosis-like death induced by vitamin D compounds in breast cancer cells [J]. J Biol Chem,2002,277(34):30738-30745.
[13] 张艳.β受体阻滞剂诱导增殖期血管瘤凋亡的研究[D].天津:天津医科大学,2014.
[14] 彭威,宁慧婷,徐仙赟,等.普萘洛尔和美托洛尔体外调控小鼠血管瘤细胞增殖及凋亡作用的初步比较[J].中国小儿血液与肿瘤杂志,2016,21(2):77-80.
[15] 周晓波,赵成鹏,王鎏,等.肿瘤抑素影响婴小儿血管瘤内皮细胞增殖与凋亡的相关机制[J].中国现代医学杂志,2015,25(28):17-21.
[16] Scatena R,Bottoni P,Botta G,et al. The role of mitochondria in pharmacotoxicology:a reevaluation of an old,newly emerging topic [J]. Ajp Cell Physiol,2007,293(1):12-21.
[17] Rixe O,Fojo T. Is cell death a critical end point for anticancer therapies or is cytostasis sufficient?[J]. Clin Cancer Res,2007,13(24):7280-7287.
[18] Groenendyk J,Michalak M. Endoplasmic reticulum quality control and apoptosis [J]. Acta Biochim Pol,2005,52(6):15-20.
[19] Morishima N,Nakanishi K,Tsuchiya K,et al. Translocation of Bim to the endoplasmic reticulum (ER) mediates ER stress signaling for activation of caspase-12 during ER stress-induced apoptosis [J]. J Biol Chem,2004,279(48):50375-50385.
[20] Shang YC,Chong ZZ,Hou J,et al. The Forkhead Transcription Factor FOXO3a Controls Microglial Inflammatory Activation and Eventual Apoptotic Injury through Caspase 3 [J]. Curr Neurovasc Res,2009,6(1):20-31.
[21] Banfi C,Brioschi M,Wait R,et al. Proteome of endothelial cell-derived procoagulant microparticles [J]. Proteomics,2005,5(17):4443-4455. |
|
|
|
