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siRNA干预树突状细胞CD40表达对大鼠炎症性肠病的治疗作用

Therapentic effect of siRNA inhibiting CD40 expression in dendritic cells on inflammatory bowel disease in rats

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摘要目的:应用小干扰RNA(siRNA)沉默树突状细胞(DCs)CD40分子的表达,观察其对大鼠炎症性肠病(IBD)的影响。方法:设计并合成高效的siRNA载体及真核表达载体pcDNA3-CD40,分别转染入大鼠DCs细胞。采用PCR和Western blotting法检测DCs中CD40mRNA及蛋白表达水平。18只Wistar大鼠采用2,4,6-三硝基苯磺酸(TNBS)建立IBD大鼠模型,分为对照组、干预组及过表达组。对照组大鼠给予生理盐水腹腔注射;干预组大鼠给予含有干涉表达载体pSilencer 4.1-CMV neo-CD40的DCs腹腔注射;过表达组大鼠给予含有pcDNA3-CD40的DCs腹腔注射。15d后观察各组大鼠的腹泻、黏液脓血便等临床症状。结果:成功构建RNA干涉载体并转染DCs,PCR及Western blotting法检测DCs中CD40mRNA及蛋白表达水平均下调。转染后的DCs作用于各组大鼠,与对照组比较,干预组大鼠的腹泻、黏液脓血便症状得到明显改善;过表达组大鼠腹泻、黏液脓血便情况加重,并有2只大鼠死亡。结论:siRNA干预DCs中CD40分子的表达对大鼠IBD具有治疗作用。 Objective To use small interfering RNA（siRNA）to silence the expression of CD40 molecule in dendritic cells（DCs）,and to observe its effect on inflammatory bowel disease（IBD）in the rats.Methods A highly efficient siRNA carrier and eukaryotic expression vector pcDNA3-CD40 were designed and synthesized,and they were transfected into DCs of the rats respectively to build the inflammatory bowel disease（IBD）models in the rats.18 Wistar rats were divided into control group,intervention group and overexpression group.All rats models were built using trinitro-benzene-sulfonic acid（TNBS）.After successful construction,the rats in control group were injected intraperitoneally with normal saline,the rats in intervention group were injected intraperitoneally with interference expression vector,and the rats in overexpression group were injected intraperitoneally with pcDNA3-CD40.The clinical symptoms such as diarrhea and mucopurulent bloody stool were observed after 15 d.Results The interference expression vector was constructed successfully.The expression levels of CD40 mRNA and protein in DCs were both reduced detected by PCR and Western blotting method.The transfected DCs were successfully acted on model rats.The clinical symptoms such as diarrhea,mucus purulent blood in intervention group were improved significantly compared with control group.The symptoms such as diarrhea and mucopurulent bloody stool were deteriorated in overexpression group,of which two rats were dead.Conclusion The intervened expression of CD40 in DCs with siRNA has a therapeutic effect on IBD in rats.

作者王丽英杨勇李占东李东复刘力宾王敏

机构地区吉林大学第二医院消化内科解放军第吉林工程技术师范学院食品工程学院生物工程教研室

出处《吉林大学学报（医学版）》 CAS CSCD 北大核心 2015年第1期54-59,共6页 Journal of Jilin University：Medicine Edition

基金吉林省科技厅自然科学基金资助课题(201115086)

关键词炎症性肠病树突状细胞小干扰RNA CD40 inflammatory bowel disease dendritic cells small interfering RNA CD40

分类号 R332 [医药卫生—人体生理学] R574.62 [医药卫生—消化系统]

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参考文献12

1Xavier RJ, Podolsky DK. Unravelling the pathogenesis of inflammatory bowel disease [J]. Nature, 2007, 448 (7152): 427-434.
2Leung RK, Whittaker PA. RNA interference: From gene silencing to gene-speeific therapeutics [J]. Pharmacol Ther, 2005, 107 (2): 222-239.
3Zhang B, Wu T, Chen M, et al. The CD40/CD40L system: a new therapeutic target for disease [J]. Immunol Lett, 2013, 153 (1/2): 58-61.
4Danese S, Scaldaferri F, Vetrano S, et al. Critical role of the CD40-CD40-1igand pathway in regulating mucosal inflammation-driven angiogenesis in inflammatory bowel disease [J]. Gut, 2007, 56 (9): 1248-1256.
5LI ZY, Mao H, Kallick DA, et al. The effects of thiophosphate substitutions on native siRNA gene silencing [J]. Biochem Bioph Res Commun, 2005, 329 (3): 1026-1030.
6Jurjus AR, Khoury NN, Reimund JM. Animal models of inflammatory bowel disease [ J ]. J Pharmacol Toxicol Methods, 2004, 50 (2): 81-92.
7Globig AM, Hennecke N, Martin B, et al. Comprehensive intestinal T helper cell profiling reveals specific accumulation of IFN-7+ IL-17+ coproducing CD4+ T cells in active inflammatory bowel disease [J]. Inflamm Bowel Dis, 2014, 20 (12): 2321-2329.
8Wilson MS, Ramalingam TR, Rivollier A, et al. Colitis and intestinal inflammation in 1L-10-/ mice results fromIL=13Rα2-mediated attenuation of IL-13 activity [ J ]. Gstroenterology, 2011, 140 (1): 254-264.
9Sawada-HaseN, Kiyohara T, Miyagawa J, et al. An increased number of CD40-high monocytes in patients with CrohrC s disease [J]. Am J Gastroenterol, 2000, 95 (6): 1516-1523.
10Daness S, Sans M, Fiocchi C. The CI)40/CEMOL costim ulatory pathway in inflammatory bowel disease [ J ]. Gut, 2004, 53 (7): 1035-1043.

二级参考文献27

1Chinese Society of Hepatology and Chinese Society of Infectious Diseases,Chinese Medical Association. 42 Dongsi Xidajie,Beijing 100710,China.慢性乙型肝炎防治指南[J].中华肝脏病杂志,2005,13(12):881-891. 被引量：1927
2卢高峰,唐芙爱,郑鹏远,马军,白经修.恩替卡韦对慢性乙型肝炎患者树突状细胞功能的体外影响[J].世界华人消化杂志,2007,15(11):1292-1296. 被引量：13
3谢谆怡,陈永文,付晓岚,杨承英,吴玉章.慢性乙型肝炎患者外周血淋巴及单核细胞表面B7-H1表达研究[J].南方医科大学学报,2007,27(11):1635-1637. 被引量：3
4SHEN L, EVEL-KABLER K, STRUBE R, et al. Silencing of SOCS1 enhances antigen presentation by dendritic cells and antigen - specific anti - tumor immunity[ J ]. Nat Biotechnol, 2004, 22 ( 12 ) : 1546 - 1553.
5HONG B, REN W, SONG XT, et al. Human suppressor of cytokine signaling 1 controls immunostimulatory activity of monocyte - derived dendritic cells [ J ]. Cancer Res, 2009, 69(20): 8076 -8084.
6UDAGAWA M, KUDO -SAITO C, HASEGAWA G, et al. En- hancement of immunologic tumor regression by intratumoral administration of dendritic cells in combination withcryoabla- tive tumor pretreatment and Bacillus Calmette - Guerin cell wall skeleton stimulation[J]. Clin Cancer Res, 2006, 12 (24):7465 -7475.
7CURIEL T J, COUKOS G, ZOU L, et al. Specific recruitment of regulatory T cells in ovarian carcinoma fosters immune privilege and predicts reduced survival[ J]. Nat Med, 2004, 10(9) : 942 -949.
8PALUCKAL AK, UENO H, FAY J, et al. Dendritic cells: a critical player in cancer therapy? [ J ]. J Immunother, 2008, 31 (9) : 793 -805.
9PARK HY, JIN JO, SONG MG, et al. Expression of dendritic cell markers on cultured neutrophils and its modulation by an- ti -apoptotic and pro - apoptotic compounds [ J ]. Exp Mol Med, 2007, 39(4): 439 -449.
10TATSUMI T, TAKEHARA T, YAMAGUCHI S, et al. Intrahe- patic delivery of alpha -galactosylceramide -pulsed dendritic cells suppresses liver tumor[J]. Hepatology, 2007, 45( 1 ):22 -30.

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1王辉,张文.RNA干预—免疫学研究的新领域[J].医学与哲学,2002,23(10):28-29.
2袁成福.RNA干扰及其实验方法[J].湖北民族学院学报（医学版）,2005,22(4):44-47. 被引量：2
3黎曼,柴华旗.系统性红斑狼疮患者外周血单核细胞CD40表达及临床意义[J].中国血液流变学杂志,2010(3):392-394. 被引量：1
4陶颖.RNA干预——一种古老而神奇的免疫方式[J].科学画报,2003,0(1):12-13.
5戴兰,王兆钺,张日,朱明清,沈文红,何杨,阮长耿.CD40L在特发性血小板减少性紫癜患者中的表达及其意义[J].苏州大学学报（医学版）,2010,30(6):1224-1225. 被引量：2
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7王珂,黄瑾,李淑芳.结核性胸膜炎病变局部B淋巴细胞CD23、CD40表达及其影响因素的探讨[J].中国防痨杂志,1998,20(3):143-145. 被引量：1
8张坤,余佩武,高朋芬,汪灏,刘伟,饶云.胃癌患者外周血DCs细胞表型变化研究[J].第三军医大学学报,2004,26(13):1207-1209. 被引量：5
9刘绍霞,张立英,赵国强,张国俊.腺病毒siRNA沉默TGF-β1对肺间质纤维化大鼠TGF-β1的表达及Ⅰ、Ⅲ型胶原含量的影响[J].郑州大学学报（医学版）,2012,47(6):785-790. 被引量：1
10杨旻,戴先文,陶惠人,闫铭,胡蕴玉,李明全.RNA干预法特异性抑制核激活因子受体配体诱导破骨细胞的形成[J].中国组织工程研究与临床康复,2007,11(19):3661-3664. 被引量：1

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