Are we giving biologics too much time? When should we stop treatment? 被引量：1

Are we giving biologics too much time? When should we stop treatment?

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摘要 The optimal duration of biological treatment, particularly anti-TNF, in inflammatory bowel disease （IBD） is a very important question both for patients and physicians. There is no published evidence to clearly and definitely answer this question. However data on natural history of IBD, long term safety of biologics, immunosuppressors （IS） cessation and some preliminary studies on biologics cessation may help us to discuss this topic. The decision to stop a biological treatment is currently based on a compromise between the benefits and risks associated with the prolongation of this treatment. IBD, more particularly CD, are characterized by the development of complications and the need for recurrent hospitalizations and surgeries in approximately 2/3 of cases. In these patients potentially in need of biological treatments, it is probable that, as it has been demonstrated for IS, the longer a stable remission has be achieved under treatment, the lower the risk of relapse is alter treatment cessation. Further prospective studies should now aim at disclosing patient characteristics associated with a low risk of relapse to imple- ment this strategy. The optimal duration of biological treatment, particu- larly anti-TNF, in inflammatory bowel disease (IBD) is a very important question both for patients and physicians. There is no published evidence to clearly and definitely answer this question. However data on natural history of IBD, long term safety of biologics, immunosuppressors (IS) cessation and some preliminary studies on biologics cessation may help us to discuss this topic. The decision to stop a biological treatment is currently based on a compromise between the benefits and risks associated with the prolongation of this treat- ment. IBD, more particularly CD, are characterized by the development of complications and the need for recurrent hospitalizations and surgeries in approximately 2/3 of cases. In these patients potentially in need of biological treatments, it is probable that, as it has been demonstrated for IS, the longer a stable remission has be achieved under treatment, the lower the risk of relapse is after treatment cessation. Further prospective studies should now aim at disclosing patient characteristics associated with a low risk of relapse to implement this strategy.

作者 Edouard Louis J Belaiche C Reenaers

机构地区 Department of Gastroenterology CHU Liège

出处《World Journal of Gastroenterology》 SCIE CAS CSCD 2008年第36期5528-5531,共4页 世界胃肠病学杂志（英文版）

关键词 Inflammatory bowel disease Immunosuppressors Biological treatment 肠炎生物制剂免疫抑制剂生物疗法

分类号 R574 [医药卫生—消化系统]

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1[1]Hanauer SB,Feagan BG,Lichtenstein GR,Mayer LF,Schreiber S,Colombel JF,Rachmilewitz D,Wolf DC,Olson A,Bao W,Rutgeerts P.Maintenance infliximab for Crohn's disease:the ACCENT I randomised trial.Lancet 2002; 359:1541-1549
2[2]Colombel JF,Sandborn WJ,Rutgeerts P,Enns R,Hanauer SB,Panaccione R,Schreiber S,Byczkowski D,Li J,Kent JD,Pollack PF.Adalimumab for maintenance of clinical response and remission in patients with Crohn's disease:the CHARM trial.Gastroenterology 2007; 132:52-65
3[3]Schreiber S,Khaliq-Kareemi M,Lawrance IC,Thomsen OO,Hanauer SB,McColm J,Bloomfield R,Sandborn WJ.Maintenance therapy with certolizumab pegol for Crohn's disease.N Engl J Med 2007; 357:239-250
4[4]Munkholm P,Langholz E,Davidsen M,Binder V.Disease activity courses in a regional cohort of Crohn's disease patients.Scand J Gastroentero11995; 30:699-706
5[5]Wolters FL,Russel MG,Sijbrandij J,Ambergen T,Odes S,Riis L,Langholz E,Politi P,Qasim A,Koutroubakis I,Tsianos E,Vermeire S,Freitas J,van Zeijl G,Hoie O,Bernklev T,Beltrami M,Rodriguez D,Stockbrugger RW,Moum B.Phenotype at diagnosis predicts recurrence rates in Crohn's disease.Gut 2006; 55:1124-1130
6[6]Beaugerie L,Seksik P,Nion-Larmurier I,Gendre JP,Cosnes J.Predictors of Crohn's disease.Gastroenterology 2006; 130:650-656
7[7]Loly C,Belaiche J,Louis E.Predictors of severe Crohn's disease.Scand J Gastroenterol 2008; 1-8
8[8]Louis E,Collard A,Oger AF,Degroote E,Aboul Nasr E1 Yafi FA,Belaiche J.Behaviour of Crohn's disease according to the Vienna classification:changing pattern over the course of the disease.Gut 2001; 49:777-782
9[9]Cosnes J,Cattan S,Blain A,Beaugerie L,Carbonnel F,Parc R,Gendre JP.Long-term evolution of disease behavior of Crohn's disease.Inflamm Bowel Dis 2002; 8:244-250
10[10]Kugathasan S,Saubermann LJ,Smith L,Kou D,Itoh J,Binion DG,Levine AD,Blumberg RS,Fiocchi C.Mucosal T-cell immunoregulation varies in early and late inflammatory bowel disease.Gut 2007; 56:1696-1705

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1Elena Ricart,Orlando García-Bosch,Ingrid Ordás,Julián Panés.Are we giving biologics too late? The case for early versus late use[J].World Journal of Gastroenterology,2008,14(36):5523-5527. 被引量：4
2孟潞英.慢性乙型病毒性肝炎的生物治疗[J].中西医结合肝病杂志,1995,5(S1):92-94.
3陈爱国,张天民.生物疗法与结核病[J].冶金防痨,1996,6(3):265-267.
4刘新垣.肝病生物治疗策略[J].中西医结合肝病杂志,1999,9(6):1-3.
5Groopman JE,崔衍贞.血液病生物疗法的新动向[J].国外医学（输血及血液学分册）,1990,13(3):150-152.
6董怡.对治疗类风湿关节炎生物制剂的认识和看法[J].风湿病学杂志,2000,4(3):133-134. 被引量：17
7刘宗印.风湿病的生物治疗[J].山东医药,1997,37(4):36-37.
8江秀富,张军.细胞因子及其抑制剂对急性胰腺炎的作用[J].国外医药（合成药．生化药．制剂分册）,1998,19(4):217-219. 被引量：1
9刘继华,刘秋莹.类风湿关节炎治疗研究若干新进展[J].医师进修杂志,2001,24(7):58-60.
10闫敏,李晓萍,尹寒麒.类风湿关节炎的诊断与治疗若干进展[J].西藏医药,2002,23(2):28-29.

World Journal of Gastroenterology

2008年第36期

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Are we giving biologics too much time? When should we stop treatment? 被引量：1

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