Induction of animal model of Graves' disease in BALB/c mice

Induction of animal model of Graves' disease in BALB/c mice

下载PDF

导出

摘要 Objective To construct an animal model of Graves’ disease(GD)by immunizing BALB/c mice with hM12 cells co-expressing major histocompatibility complex(MHC)class II molecules and human thyrotropin receptor(TSHR)molecules.Methods BALB/c mice in experimental group(H-2d)were immunized with hM12 cells intraperitoneally every 2 weeks for six times,while mice in control group were immunized with M12 cells.Five weeks later,the thyroids were histologically examined,and serum samples were tested for thyroid-stimulating antibodies(TSAb)and thyroid hormone levels.Results One BALB/c mouse in experimental group developed Graves’-like disease.Total T4 and T3 levels in this mouse were above the upper limit of normal,TSAb activity was displayed in its serum.The thyroid histologically showed the features of thyroid hyperactivity including thyrocyte hypercellularity and colloid ABSorption.None of control mice developed Graves’-like disease.Conclusion An animal model with some characteristics of human Graves’ disease was successfully induced and the model will facilitate studies aimed directly at understanding the pathogenesis of autoimmunity in Graves’ disease. Objective To construct an animal model of Graves' disease(GD)by immunizing BALB/c mice with hM12 cells co-expressing major histocompatibility complex(MHC)class II molecules and human thyrotropin receptor(TSHR)molecules.Methods BALB/c mice in experimental group(H-2d)were immunized with hM12 cells intraperitoneally every 2 weeks for six times,while mice in control group were immunized with M12 cells.Five weeks later,the thyroids were histologically examined,and serum samples were tested for thyroid-stimulating antibodies(TSAb)and thyroid hormone levels.Results One BALB/c mouse in experimental group developed Graves'-like disease.Total T4 and T3 levels in this mouse were above the upper limit of normal,TSAb activity was displayed in its serum.The thyroid histologically showed the features of thyroid hyperactivity including thyrocyte hypercellularity and colloid ABSorption.None of control mice developed Graves'-like disease.Conclusion An animal model with some characteristics of human Graves' disease was successfully induced and the model will facilitate studies aimed directly at understanding the pathogenesis of autoimmunity in Graves' disease.

作者 Zhu-fang Tian1,2,Bing-yin Shi1,Xiao-yan Wu1,Li Xu1 1.Department of Endocrinology,the First Affiliated Hospital,Medical School of Xi’an Jiaotong University,Xi’an 710061 2.Department of Endocrinology,Xi’an Central Hospital,Xi’an 710003,China

出处《Journal of Pharmaceutical Analysis》 SCIE CAS 2009年第4期211-214,221,共5页 药物分析学报（英文版）

基金 supported by the National Natural Science Foundation of China(No.30371335)

关键词 major histocompatibility complex Ⅱ thyrotropin receptor M12 cell Graves' disease major histocompatibility complex Ⅱ thyrotropin receptor M12 cell Graves' disease

分类号 R581.1 [医药卫生—内分泌]

引文网络
相关文献

参考文献22

1伍丽萍,施秉银,郭丽英,徐利,兰玲,刘娟,张进安,旬利茹.在雌性小鼠制备Graves病动物模型[J].中华内分泌代谢杂志,2006,22(4):388-391. 被引量：15
2田竹芳,雒文田,吴晓燕,朱本章.MHC-Ⅱ类分子与hTSH受体共表达系统的建立[J].实用医技杂志,2004,11(10A):1949-1952. 被引量：2
3Nagayama Y.Animal models of Graves hyperthyroidis mThyroid,2007.
4Latrofa F,Chazenbalk GD,Pichurin P,et al.Affinity-en-richment of thyrotropin receptor autoantibodies from Graves patients and nor mal individuals provides insight into their properties and possible origin from natural antibodiesThe Journal of Clinical Endocrinology,2004.
5Hollowell JG,Staehling NW,Flanders WD,et al.Serum TSH, T(4), and thyroid antibodies in the United States population (1988 to 1994): National Health and Nutrition Examination Survey (NHANES III)Journal of Clinical Endocrinology and Metabolism,2002.
6Barrett K,Liakata E,Rao PV,et al.Induction of hyperthyroidism in mice by intradermal immunization with DNA encoding the thyrotropin receptorClinical and Experimental Immunology,2004.
7Vanderpump MP,Tunbridge WM,French JM,et al.The incidence of thyroid disorders in the community: a twenty-year follow-up of the Whick ham SurveyClinical Endocrinology,1995.
8Sandra M McLachlan,Yuji Nagayama,and Basil Rapoport.Insight into Graves‘ Hyperthyroidism from Animal ModelsEndocrine Reviews,2005.
9Shimojo N,Kohno Y,Yamaguchi KI,et al.Induction of Graves-like disease in mice by immunization with fibroblasts transfected with the thyrotropin receptor and a class Ⅱ moleculeProceedings of the National Academy of Sciences of the United States of America,1996.
10Kaithamana S,Fan J,Osuga Y,et al.Induction of Experimental Autoimmune Graves’ Disease in BALB/c MiceJ Immunol,1999.

二级参考文献13

1武敏,施秉银.Graves病动物模型研究进展[J].陕西医学杂志,2006,35(3):321-323. 被引量：1
2施秉银．甲状腺功能亢进症．见：施秉银，马秀萍，主编．现代甲状腺诊断与治疗．西安：陕西科学技术出版社，1998,3-24．
3Vanderpump MPJ, Tunbridge WMG, French JM, et al. The incidence of thyroid disorders in the community: a twenty-year follow-up of the Whickham survey. Clin Endocrinol, 1995,43:55-68.
4Ludgate M. Animal models of Graves' disease. Eur J Endcrinol, 2000,142:1-8.
5Loosfelt H, Pichon C, Jolivet A, et al. Two-subunit structure of the human thyrotropin receptor. Proc Natl Acad Sci USA, 1992,89:3765-3769.
6Chazenbalk GD, Pichurin P, Chen CR, et al. Thyroid-stimulating autoantibodies in Graves disease preferentially recognize the free A subunit, not the thyrotropin holoreceptor. J Clin Invest, 2002,110:209-217.
7Shimojo N, Kohno Y, Yamaguchi KI, et al. Induction of Graves-like disease in mice by immunization with fibroblasts transfected with the thyrotropin repector and a class Ⅱ molecule. Proc Natl Acad Sci USA,1996,93 : 11074-11079.
8Kaithamana S, Fan J, Osuga Y, ct al. Induction of experimental autoimmunc Graves' disease in BALB/c mice. J Immunol, 1999,163:5157-5164.
9Costagliola S, Rodien P, Many MC, et al. Genetic immunization against the human thyrotropin receptor causes thyroiditis and allows production of monoclonal antibodies recognizing the native receptor. J Immunol, 1998,160 : 1458-1465.
10Costagliola S, Many MC, Denef .IF, et al. Genetic immunization of outbred mice with thyrotropin receptor cDNA provides a model of Graves' disease. J Clin Invest, 2000,105:803-811.

共引文献15

1余毅恺,张木勋,胡蜀红,林梅,帅红霞.基因枪注射BALB/c小鼠制备Graves病模型[J].中国免疫学杂志,2008,24(8):737-741. 被引量：5
2施秉银.甲状腺功能亢进症的治疗现状与展望[J].西安交通大学学报（医学版）,2008,29(4):361-364. 被引量：11
3蒲丹,郭辉,马爱群,施秉银.胎儿微嵌合体对Graves病动物模型制备的影响[J].西安交通大学学报（医学版）,2009,30(3):331-334. 被引量：3
4蒲丹,郭辉,施秉银,马爱群.胎儿微嵌合体对Graves病动物模型甲状腺内树突状细胞的影响[J].第四军医大学学报,2009,30(18):1665-1668.
5田竹芳,雒文田,吴晓燕,徐利.主要组织相容性复合物Ⅱ对Graves病发病影响的研究[J].中国现代医药杂志,2009,11(11):1-4.
6王素莉,赵禹,陈祖培,田恩江,陈昆明,郭琳,潘红艳,李强,高海林,张晓光.拮抗甲状腺刺激性抗体单链抗体的制备及鉴定[J].国际内分泌代谢杂志,2010,30(6):368-370.
7董全文,战淑彩.药物治疗甲状腺功能亢进症的应用及分析[J].中国实用医药,2010,5(35):34-35. 被引量：22
8伍丽萍,施秉银,杨婧,旬利茹,徐利,田竹芳,高珊,张煜.性别差异对Graves病动物模型建立的影响[J].中华内分泌代谢杂志,2011,27(6):505-508. 被引量：6
9王悦,伍丽萍,施秉银.Graves病动物模型研究进展[J].医学综述,2012,18(10):1455-1458. 被引量：4
10余月,王曙,石星,朱子阳,王旭,郭梅,刘倩琦.Graves病母鼠分娩后甲状腺自身抗体水平的观察[J].南京医科大学学报（自然科学版）,2012,32(7):928-932.

1Xiao-lei Zou Zeng-yu Zhao Yun-yang Wang Zhi-qiang Su Ming Xiang.DIABETOGENIC T CELLS INDUCE AUTOIMMUNE DIABETES IN BALB/c MICE[J].Chinese Medical Sciences Journal,2008,23(2):88-94. 被引量：1
2李万森.GD肝病26例临床分析[J].中国实用医药,2006,1(5):15-15.
3文芳,刘好,马志敏,秦建平,曹仁贤.他巴唑对Graves病患者sICAM—1的影响[J].医学临床研究,2002,19(6):434-435.
4毛永华,吴文迅,谢亚争,高美华,任晓燕.Graves病合并全血细胞减少2例及文献复习[J].郑州大学学报（医学版）,2015,50(5):730-732. 被引量：1
5张卉,阎胜利,王娈,綦玉琴.CTLA-4基因启动子-318位点C/T多态性与抗甲状腺药物导致白细胞减少的相关性[J].免疫学杂志,2010,26(12):1070-1073. 被引量：3
6王瑛,周宁,唐哲,何美琼,高辉,常李荣.细胞因子在Graves病发病机理中的作用[J].中国综合临床,2003,19(2):103-104. 被引量：9
7李异白.突眼性甲状腺肿误诊为消化系统疾病30例临床分析[J].黑龙江医学,2003,27(1):74-75. 被引量：1
8武红梅,刘新宇,吴艳君.左旋甲状腺素治疗Graves病疗效观察[J].医师进修杂志,2005,28(8):48-49.
9李异白.毒性弥漫性甲状腺肿误诊为消化系统疾病[J].现代实用医学,2003,15(1):38-38. 被引量：2
10帕尔哈提,李岚,赵勤英,姜述斌,张宝简,毛拉提,马俊.使用替罗非班时泮托拉唑对非ST段抬高型急性冠脉综合征患者消化道保护作用的评价[J].心脏杂志,2012,24(3):366-369. 被引量：2

Journal of Pharmaceutical Analysis

2009年第4期

浏览历史

内容加载中请稍等...

Induction of animal model of Graves' disease in BALB/c mice

参考文献22

二级参考文献13

共引文献15

相关作者

相关机构

相关主题

浏览历史