Determinanten der Plazebowirkung beim Reizdarm-Syndrom

P. Enck; S. Klosterhalfen; W. Kruis

doi:10.1055/s-2005-872605

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Dtsch Med Wochenschr 2005; 130(34/35): 1934-1937
DOI: 10.1055/s-2005-872605

Originalien

Gastroenterologie
© Georg Thieme Verlag Stuttgart · New York

Determinanten der Plazebowirkung beim Reizdarm-Syndrom[1]

Determination of placebo effect in irritable bowel syndromeP. Enck¹ , S. Klosterhalfen² , W. Kruis³

¹Medizinische Klinik VI: Psychosomatische Medizin und Psychotherapie, Universitätsklinikum Tübingen;
²Institut für Medizinische Psychologie, Universitätsklinikum Düsseldorf;
³Klinik für Innere Medizin/Gastroenterologie, Evangelisches Krankenhaus Köln-Kalk

Further Information

Publication History

eingereicht: 7.3.2005

akzeptiert: 6.6.2005

Publication Date:
25 August 2005 (online)

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Abstract
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Zusammenfassung

Hintergrund und Fragestellung: Welche Faktoren die Plazebowirkungen bestimmen, ist weitgehend unklar. Ziel der Untersuchung war die Exploration möglicher prädiktiver Faktoren in einem bereits publizierten Datensatz.

Methoden: Wir haben die Daten einer Studie bei 120 Patienten mit Reizdarmsyndrom (RDS) im Hinblick auf Faktoren re-analysiert, die die Plazebowirkung beeinflussen. Die Patienten waren randomisiert einem von drei Armen zugewiesen worden: sie erhielten doppelblind Mebeverin (n = 40) oder Plazebo (n = 40) oder, in einem offenen Design, Ballaststoffe (n = 40) für 16 Wochen. Die Behandlung wurde von drei verschiedenen Ärzten durchgeführt (A, B und C mit 44, 27 bzw. 18 Patienten), eine vierte Gruppe (n = 31) hatte wechselnde behandelnde Ärzte. Die Symptome wurden alle 4 Wochen überprüft; die Compliance der Patienten, die Schwere der Symptome (Kruis-Score), Alter und Geschlecht der Patienten und die behandelnden Ärzte wurden in die Analyse einbezogen.

Ergebnisse: Unter Plazebo/Medikation betrug die Rate der Studienabbrecher je 30 %, unter der Diättherapie war sie niedriger. Die Compliance war mit 75 % für die Plazebogruppe am niedrigsten, und mit 89 bzw. 82 % für das Medikament und die Ballaststoffe deutlich höher. Symptombesserung trat bei 39 % in der Plazebogruppe auf, bei 20 % in der Verumgruppe und in 43 % unter Diät. Für Medikament und Plazebo war die Besserung zwischen den Ärzten sehr unterschiedlich: 32 % für A (43 Jahre, weiblich), 19 % für B und C (beide männlich, 32 und 40 Jahre) zusammen; dieser Effekt war nicht signifikant. Plazebo-Responder waren häufiger Frauen (47 %) als Männer (28 %), während das Alter nur Einfluss auf die diätetische Behandlung hatte: Responder waren in der Regel jünger. Plazebo-Responder hatten einen niedrigeren Kruis-Score (45 vs 52 Punkte), aber dies traf auch auf die Medikamentengruppe (52 vs 62 Punkte) und Ernährungstherapie zu (56 vs 68 Punkte).

Folgerungen: Vor allem der behandelnde Arzt (Geschlecht, Ausbildung), aber auch das Geschlecht der Patienten beeinflussen die Plazebowirkung, Patienten mit niedrigem Kruis-Score (geringerer Wahrscheinlichkeit für eine funktionelle Erkrankung) scheinen eher eine Plazebowirkung zu zeigen.

Summary

Background and objective: The determinants of the placebo effect are not well established. Goal of this study was to explore likely predictive factors in an already published data set.

Methods: We re-analysed data from a study in 120 patients with the irritable bowel syndrome (IBS) that were randomly assigned to three arms of the study to receive (double-blind) either a drug (mebeverin) (n = 40) or placebo (n = 40), or (in an open trial) dietary treatment (fibre) (n = 40) for up to 16 week. Treatment was conducted by 3 different doctors (A, B, C) with 44, 27, and 18 patients, resp. A fourth group (n = 31) was treated by different varying physicians. Symptoms were assessed every 4 weeks, and the degree of patient compliance and the number of drop-outs, the number of patients improved/not improved (in %), symptom severity (Kruis Score) at enrolment, and age and gender as covariates were included into the analysis.

Results: Drop-out rate was 30 % for placebo, 30 % for mebeverin, and 15 % for the diet. For the patients remaining in the study, average compliance was 75 % with placebo, but 89 % for the drug and 82 % for the diet. Response rates were 39 % for placebo, but 20 % for the drug; response rate for the diet (open trial) was 43 % under all doctors. Response rates for drug and placebo combined were 32 % for doctor A (female,43 years), but 19 % for doctors B and C together (both males, 32 and 40 years)); this effect was not significant. Placebo responders were more often women (47 %) than men (28 %), while age effects were only found with dietary treatment: responders were younger. Placebo responders had an overall lower Kruis Score than non-responders (45 vs 52 points), but this was also true for drug (52 vs. 62 points) and diet responders (56 vs 68 points).

Conclusion: The major factors contributing to the placebo response are the treating physician (gender, training), and the patientsŽ gender (female). Patients with lower Kruis score (more likely non-functionally disordered) may be prone to higher (placebo) response rates.

1 Unterstützt mit Mitteln der Deutschen Forschungsgemeinschaft (EN 50/18, KL 811/2)

Literatur

1 Allescher H D, Bockenhoff A, Knapp G, Wienbeck M, Hartung J. Treatment of non-ulcer dyspepsia: a meta-analysis of placebo-controlled prospective studies. Scand J Gastroenterol. 2001; 36 934-941

MissingFormLabel

Search in Google Scholar
2 Chey W D, Chey W Y, Heath A T, Dukes G E, Carter E G, Northcutt A, Ameen V Z. Long-term safety and efficacy of alosetron in women with severe diarrhea-predominant irritable bowel syndrome. Am J Gastroenterol. 2004; 99 2185-2203

MissingFormLabel

Search in Google Scholar
3 Cremonini F, Delgado-Aros S, Camilleri M. Efficacy of alosetron in irritable bowel syndrome: a meta-analysis of randomized controlled trials. Neurogastroenterol Motil. 2003; 15 79-86

MissingFormLabel

Search in Google Scholar
4 de Craen A J, Moerman D E, Heisterkamp S H, Tytgat G N, Tijssen J G, Kleijnen J. Placebo effect in the treatment of duodenal ulcer. Br J Clin Pharmacol. 1999; 48 853-860

MissingFormLabel

Search in Google Scholar
5 De Pascalis V, Chiaradia C, Carotenuto E. The contribution of suggestibility and expectation to placebo analgesia phenomenon in an experimental setting. Pain. 2002; 96 393-402

MissingFormLabel

Search in Google Scholar
6 Enck P, Klosterhalfen S. The placebo response in functional bowel disorders: Perspectives and putative mechanisms. Neurogastroenterol Mot. 2005; 17 325-330

MissingFormLabel

Search in Google Scholar
7 Evans K R, Sills T, Wunderlich G R, McDonald H P. Worsening of depressive symptoms prior to randomization in clinical trials: a possible screen for placebo responders?. J Psychiatr Res. 2004; 38 437-444

MissingFormLabel

Search in Google Scholar
8 Ilnyckyj A, Shanahan F, Anton P A, Cheang M, Bernstein C N. Quantification of the placebo response in ulcerative colitis. Gastroenterology. 1997; 112 1854-1858

MissingFormLabel

Search in Google Scholar
9 Jackson J L, O’Malley P G, Tomkins G, Balden E, Santoro J, Kroenke K. Treatment of functional gastrointestinal disorders with antidepressant medications: a meta-analysis. Am J Med. 2000; 108 65-72

MissingFormLabel

Search in Google Scholar
10 Klein K B. Controlled treatment trials in the irritable bowel syndrome: a critique. Gastroenterology. 1988; 95 232-241

MissingFormLabel

Search in Google Scholar
11 Klosterhalfen S, Enck P. Psychobiology of the placebo response. J Auton Neurosci. 2005; , im Druck

MissingFormLabel

Search in Google Scholar
12 Kruis W, Thieme C, Weinzierl M, Schussler P, Holl J, Paulus W. A diagnostic score for the irritable bowel syndrome. Its value in the exclusion of organic disease. Gastroenterology. 1984; 87 1-7

MissingFormLabel

Search in Google Scholar
13 Kruis W, Weinzierl M, Schussler P, Holl J. Comparison of the therapeutic effect of wheat bran, mebeverine and placebo in patients with the irritable bowel syndrome. Digestion. 1986; 34 196-201

MissingFormLabel

Search in Google Scholar
14 Mearin F, Balboa A, Zarate N, Cucala M, Malagelada J R. Placebo in functional dyspepsia: symptomatic, gastrointestinal motor, and gastric sensorial responses. Am J Gastroenterol. 1999; 94 116-125

MissingFormLabel

Search in Google Scholar
15 Moayyedi P. Meta-analysis: Can we mix apples with oranges?. Am J Gastroenterol. 2004; 99 2297-2301

MissingFormLabel

Search in Google Scholar
16 Moerman D E. Cultural variations in the placebo effect: ulcers, anxiety, and blood pressure. Med Anthropol Q. 2000; 14 51-72

MissingFormLabel

Search in Google Scholar
17 Moerman D E, Jonas W B. Deconstructing the placebo effect and finding the meaning response. Ann Intern Med. 2002; 136 471-476

MissingFormLabel

Search in Google Scholar
18 Patel S M, Stason W B, Legedza A. et al . The placebo effects i irritable bowel syndrome (IBS) trials - A meta-analysis. Neurogastroenterol Motil. 2005; 17 1-9

MissingFormLabel

Search in Google Scholar
19 Poynard T, Regimbeau C, Benhamou Y. Meta-analysis of smooth muscle elaxants in the treatment of irritable bowel syndrome. Aliment Pharmacol Ther. 2001; 15 355-361

MissingFormLabel

Search in Google Scholar
20 Reynaert C, Janne P, Vause M, Zdanowicz N, Lejeune D. Clinical trials of antidepressants: the hidden face: where locus of control appears to play a key role in depression outcome. Psychopharmacology (Berl). 1995; 119 449-454

MissingFormLabel

Search in Google Scholar
21 Robertson C, Idris N R, Boyle P. Beyond classical meta-analysis: can inadequately reported studies be included?. Drug Discov Today. 2004; 9 924-931

MissingFormLabel

Search in Google Scholar
22 Schneider A, Enck P, Streitberger K. et al . Acupuncture treatment in the irritable bowel syndrome (IBS). Gut. 2005; , (zur Publikation eingereicht)

MissingFormLabel

Search in Google Scholar
23 Spanier J A, Howden C W, Jones M P. A systematic review of alternative therapies in the irritable bowel syndrome. Arch Intern Med. 2003; 163 265-274

MissingFormLabel

Search in Google Scholar
24 Spiller R C. Problems and challenges in the design of irritable bowel syndrome clinical trials: experience from published trials. Am J Med. 1999; 107 91S-97S (Suppl)

MissingFormLabel

Search in Google Scholar
25 Streitberger K, Kleinhenz J. Introducing a placebo needle into acupuncture research. Lancet. 1998; 352 364-365

MissingFormLabel

Search in Google Scholar
26 Su C, Lichtenstein G R, Krok K, Brensinger C M, Lewis J D. A meta-analysis of the placebo response rates of remission and response in clinical trials of active CrohnŽs disease. Gastroenterology. 2004; 126 1257-1269

MissingFormLabel

Search in Google Scholar
27 Weihrauch T R, Gauler T C. Placebo - efficacy and adverse effects in controlled clinical trials. Arzneimittelforschung. 1999; 49 385-393

MissingFormLabel

Search in Google Scholar
28 Welge J A, Keck P E. Moderators of placebo response to antipsychotic treatment in patients with schizophrenia: a meta-regression. Psychopharmacology (Berl). 2003; 166 1-10

MissingFormLabel

Search in Google Scholar
29 White P J. Methodological concerns when designing trials for the efficacy of acupuncture for the treatment of pain. Adv Exp Med Biol. 2004; 546 217-227

MissingFormLabel

Search in Google Scholar

1 Unterstützt mit Mitteln der Deutschen Forschungsgemeinschaft (EN 50/18, KL 811/2)

Prof. Dr. Paul Enck

Med. Klinik VI: Psychosomatische, Medizin und Psychotherapie, Forschungsbereich

Schaffhausenstraße 113

72072 Tübingen

Phone: 07071/9387374

Fax: 07071/9387379

Email: paul.enck@uni-tuebingen.de