Oral immune regulation using colitis extracted proteins for treatment of Crohn's disease: Results of a phase Ⅰ clinical trial 被引量：8

Oral immune regulation using colitis extracted proteins for treatment of Crohn's disease: Results of a phase Ⅰ clinical trial

下载PDF

导出

摘要 AIM: To evaluate safety and possible efficacy of induction of oral immune regulation using colitis extracted proteins (CEP) in Crohn's disease (CD) subjects. METHODS: Ten CDs were treated orally with autologous CEP thrice weekly for 16 wk. Subjects were monitored for CDAI and IBDQ. Immune modulatory effect was assessed by T-lymphocyte FACS analysis, CEP-specific IFNγ ELISPOT assay and cytokine levels. RESULTS: Induction of oral immune regulation significantly ameliorated disease activity. All (10/10) subjects had clinical response (CDAI≤70) and 7/10 achieved clinical remission (CDAI≤150). Significant increase in mean IBDQ score was noted (134±9 vs 164±12). No treatment-related adverse events were noted. High levels of CEP-specific IFNγ spot forming colonies were detected in five subjects prior to treatment and in all five, a marked decrease was observed. The CD4+/CD8+ lymphocyte ratio and peripheral NKT cell numbers increased significantly, in 7/10 and in 5/10 subjects, respectively. Significant increase in serum IL-10 and IL-4 levels was observed in 7/10 subjects during treatment period. CONCLUSION: Immune regulation via oral administration of CEP is a safe and possibly effective treatment for subjects with moderate CD and may provide means of antigen-specific immune modulation. AIM: To evaluate safety and possible efficacy of induction of oral immune regulation using colitis extracted proteins(CEP) in Crohn's disease (CD) subjects.METHODS: Ten CDs were treated orally with autologous CEP thrice weekly for 16 wk. Subjects were monitored for CDAI and IBDQ. Immune modulatory effect was assessed by T-lymphocyte FACS analysis, CEP-specific IFNγ ELISPOT assay and cytokine levels.RESULTS: Induction of oral immune regulation significantly ameliorated disease activity. All (10/10) subjects had clinical response (CDAI≤70) and 7/10 achieved clinical remission (CDAI≤150). Significant increase in mean IBDQ score was noted (134±9vs 164±12). No treatment-related adverse events were noted. High levels of CEP-specific IFNγ spot forming colonies were detected in five subjects prior to treatment and in all five, a marked decrease was observed. The CD4+/CDS+ lymphocyte ratio and peripheral NKT cell numbers increased significantly, in 7/10 and in 5/10 subjects, respectively. Significant increase in serum IL-10 and IL-4 levels was observed in 7/10 subjects during treatment period.CONCLUSION: Immune regulation via oral administration of CEP is a safe and possibly effective treatment for subjects with moderate CD and may provide means of antigen-specific immune modulation.

作者 Eran Israeli Eran Goldin Oren Shibolet Athalia Klein Nilla Hemed Dean Engelhardt Elazar Rabbani Yaron Ilan

机构地区 Gastroenterology and Liver Units Department of Medicine Enzo Biochem New York

出处《World Journal of Gastroenterology》 SCIE CAS CSCD 2005年第20期3105-3111,共7页 世界胃肠病学杂志（英文版）

基金 Supported by the Enzo Therapeutics Inc., NY, USA

关键词 Crohn's disease Colitis extracted proteins 免疫反应大肠疾病萃取蛋白克罗恩病节段性肠炎

分类号 R574.62 [医药卫生—消化系统]

引文网络
相关文献

参考文献45

1Podolsky DK.Inflammatory bowel disease.N Engl J Med 2002; 347:417-429.
2Su C,Lichtenstein GR.Recent developments in inflammatory bowel disease.Med Clin North Am 2002;86:1497-1523.
3Rimm DL,Holland E,Tracey E,Morrow Jon S,Anderson JM.Autoantibodies specific for villin found in patients with colon cancer and other colitides.Dig Dis Sci 1995:40:389-395.
4Hibi S,Also N,Ishikawa M,Watanabe M,Yoshida T,Kobayashi K,Asakura H, Tsuru S,Tsuchiya M.Circulating antibodies to the surface antigens on colon epithelial cells inulcerative colitis.Clin Exp Immunol 1983; 54:163-168.
5Das KM,Vecchi M,Sakemaki S.A shared and unique epitope(s) on human colon,skin and biliary epithelium detected by a monoclonal antibody. Gastroenterology 1990:98:464-469.
6Strober W,Nourish MF.Immunological diseases of the gastrointestinal tract.In:RR Rich,Ed.Clinical Immunology.St.Louis: Mosey 1995:1401-1428.
7Mizoguchi A,Mizoguchi E,Chiba C,Spiekermann GM,Tonegawa S,Anderson CN,Bhan AK.Cytokine imbalance and autoantibody production in T cell receptora mutant micewith inflammatory bowel disease.J Exp Med 1996; 183:847-856.
8Strober W,Kelsall B,Fuss L,Marth T,Ludviksson B,Ehrhardt R,Neurath M.Reciprocal IFN-γ and TGF β responses regulate the occurrence of mucosal inflammation,Immunol Today 1997;18:61-64.
9Neurath MF,Kelasall BL,Presky DH,Waegell W,Strober W.Experimental granulomatous colitis in mice is abrogated by Induction of TGFβ-mediated oral tolerance.J Exp Med 1996;183:2605-2616.
10Madsen KL,Lewis Simon A,Tavernini MM,Hibbard J,Fedorak RN. Interleukin 10 prevents cytokine-induced disruption of T84 barrier integrity and limits chloride secretion.Gastroenterology 1997; 113:151-159.

同被引文献111

1徐如祥,涂艳阳.RNA干扰和肿瘤基因治疗[J].肿瘤,2004,24(5):512-513. 被引量：2
2Chang-TaiXu,Shu-YongMeng,Bo-RongPan.Drug therapy for ulcerative colitis[J].World Journal of Gastroenterology,2004,10(16):2311-2317. 被引量：21
3许昌泰,郭学刚.溃疡性结肠炎与免疫因素[J].世界感染杂志,2004,4(6):524-526. 被引量：11
4刘希双,刘思良,王光兰,戴素美,张民生,张翠萍.结肠良恶性肿瘤的关系及其发病规律[J].世界华人消化杂志,2005,13(10):1235-1238. 被引量：16
5周中银,罗和生.血脂及载脂蛋白E基因多态性与结肠腺瘤的关系[J].中华消化杂志,2005,25(11):652-654. 被引量：9
6Margalit M,Israeli E,Shibolet O.口服自体结肠蛋白质萃取物的混合物治疗克罗恩病的一项双盲临床试验:个体化治疗方法[J].中国处方药,2006,5(5):25-25. 被引量：1
7许昌泰,郭学刚.溃疡性结肠炎的药物治疗[J].天津医药,2006,34(7):508-510. 被引量：6
8许岸高,姜泊,余志金,钟旭辉,甘爱华,刘集鸿,罗秋云,熊理守.广东省社区人群大肠癌流行病学调查[J].中华医学杂志,2007,87(28):1950-1953. 被引量：24
9HARTUPEE J C, ZHANG H, BONALDO M F, et al. Isolation and characterization of a cDNA encoding a novel member of the human regenerating protein family: Reg Ⅳ [ J ]. Biochim Biophys Acta,2001,1518 ( 3 ) : 287-293.
10ZENILMAN M E, MAGNUSON T H, SWINSON K, et al. Pancreatic thread protein is mitogenic to pancreatic-derived cells in culture [ J ]. Gastroenterology, 1996, 110 ( 4 ) : 1208-1214.

引证文献8

1李陕区（综述）,吴涛（综述）,许昌泰（审校）.白细胞介素-1～4在溃疡性结肠炎发生发展中的作用[J].世界感染杂志,2007,7(1):13-15. 被引量：3
2叶月芳,厉有名.口服耐受与炎症性肠病[J].国际消化病杂志,2008,28(2):132-135. 被引量：2
3徐佳佳,郭英,黄培林.癌基因RegⅣ的研究进展[J].东南大学学报（医学版）,2009,28(1):66-69.
4钮晓音,董晨,臧敬五.IL-21及其在自身免疫病中的研究进展[J].免疫学杂志,2010,26(1):87-90. 被引量：12
5余海静,黄加权,周广海,刘阳,艾国,宁琴.IL-17在小鼠自身免疫性肝炎中的表达及其意义[J].华中科技大学学报（医学版）,2010,39(3):311-313. 被引量：7
6孙晔,刘秀梅.类风湿关节炎患者血清IL-17、IL-21水平检测及其意义的研究[J].中国医疗前沿,2011,6(9):7-9. 被引量：3
7黄玉莲,张玫.结直肠高危腺瘤的危险因素分析[J].山西医科大学学报,2011,42(8):682-684. 被引量：3
8余准,耿江,郑军华,杨斌,高其若,王光春,彭波.RNA干扰REG1A基因抑制人膀胱癌T24细胞增殖[J].肿瘤,2012,32(3):159-163. 被引量：1

二级引证文献31

1杨先旭,龚石,刘巧.IL-21与系统性红斑狼疮发病机制关系的研究进展[J].中国医学文摘（皮肤科学）,2012,29(5):278-280. 被引量：1
2郭学刚,许昌泰.T淋巴细胞在炎症性肠病发生发展中的作用[J].中国实用内科杂志,2007,27(18):1432-1436. 被引量：1
3许昌泰.T淋巴细胞与炎症性肠病[J].世界感染杂志,2007,7(5):355-358.
4朴成林,李哲浩.促炎细胞因子对阻塞性黄疸致肠黏膜损伤中的作用研究现状[J].延边大学医学学报,2008,31(1):60-62. 被引量：3
5吴银平,侯卫平,袁发焕.Col4α3NC1中多肽序列pCol(28-40)诱导抗肾小球基底膜肾炎大鼠模型的建立[J].免疫学杂志,2010,26(5):391-394.
6唐吉仙,王焱.Th17及其因子与心肌炎相关性的最新研究[J].中国保健营养（下半月）,2010(11):39-42.
7陈敏,彭克美,何敏.白细胞介素21及其免疫调节研究进展[J].动物医学进展,2012,33(3):76-79. 被引量：3
8张春江,杨平荣,马毅.自身免疫病治疗的新型靶点:Act1介导的IL-17信号通路[J].免疫学杂志,2012,28(5):441-444. 被引量：8
9雷旦生.H-ficolin与丙型肝炎发展的相关性[J].华中科技大学学报（医学版）,2012,41(3):345-347. 被引量：1
10刘志勇,赵海梅,陈瑶,程绍民,刘端勇.益生菌治疗溃疡性结肠炎的黏膜免疫耐受理论基础探析[J].中国中医基础医学杂志,2012,18(10):1142-1144. 被引量：6

1杨华,吕震.节段性肠炎误诊分析[J].临床误诊误治,1996,9(5):202-202.
2赵广峰,鲁培荣.Crohn病13例误诊分析[J].广州医学院学报,2001,29(3):56-57. 被引量：6
3节段性肠炎患者的HBV和HCV发病率高[J].传染病网络动态,2002(1):3-3.
4舒绍强.8例节段性肠炎的临床分析[J].现代医药卫生,2003,19(6):735-735.
5胡爱荣,赵艳玲.克隆病伴肝内特殊肿物心理护理1例[J].中国社区医师（医学专业）,2004,6(3):64-65. 被引量：3
6许杰.节段性肠炎行阑尾切除致肠瘘1例[J].川北医学院学报,2004,19(4):251-252.
7庄蕙,陈士葆.硫唑嘌呤治疗炎症性肠病的临床回顾[J].世界临床药物,2003,24(5):316-316.
8刘龙刚,秦孝波,宋辉.3例节段性肠炎的误诊原因分析[J].中国医药指南,2013,11(9):662-663.
9王清莲,白莲梅,李桂芬,张书评.单纯累及直肠Crohn’s病一例[J].内蒙古医学杂志,2001,33(6):569-569.
10欧阳钦,梁红亮.克罗恩病[J].继续医学教育,2006,20(3):35-39. 被引量：3

World Journal of Gastroenterology

2005年第20期

浏览历史

内容加载中请稍等...

Oral immune regulation using colitis extracted proteins for treatment of Crohn's disease: Results of a phase Ⅰ clinical trial 被引量：8

参考文献45

同被引文献111

引证文献8

二级引证文献31

相关作者

相关机构

相关主题

浏览历史