Abstract:The placebo response is the efficacy attributable to a treatment that is thought to have no specific pharmacologic effect on the condition being treated. Although potentially helpful in clinical practice, high and unpredictable placebo response rates present a major impediment to the success of clinical trials in inflammatory bowel disease (IBD) and irritable bowel syndrome (IBS). Diverse factors contribute to the placebo response rates observed in clinical trials. These include patient characteristics, physic… Show more
“…Human IBD drug trials, particularly those in Crohn's disease, are complicated by both uncertainty about current disease activity and also by the relapsing and remitting clinical course. These variables are believed to be significant contributors to high placebo rates, which can obscure therapeutic benefits of drug candidates (Su et al 2004;Sands et al 2005;Sands 2009;D'Haens et al 2012). The need to reduce placebo risk in IBD trials has led to increasing use of expensive and sometimes invasive imaging modalities to compensate for the lack of highly reliable indicators of disease activity (Solem et al 2008;Loftus et al 2007;Buisson et al 2013), so development of reliable and noninvasive disease activity biomarkers is an ongoing area of interest.…”
Section: Utilization Of Animal Models In Ibd Researchmentioning
Animal models of human disease are a critical tool in both basic research and drug development. The results of preclinical efficacy studies often inform progression of therapeutic candidates through the drug development pipeline; however, the extent to which results in inflammatory bowel disease (IBD) models predict human drug response is an ongoing concern. This review discusses how murine models are currently being used in IBD research. We focus on the considerations and caveats for commonly used models in preclinical efficacy studies and discuss the value of models that utilize specific pathogenic pathways of interest rather than model all aspects of human disease.
“…Human IBD drug trials, particularly those in Crohn's disease, are complicated by both uncertainty about current disease activity and also by the relapsing and remitting clinical course. These variables are believed to be significant contributors to high placebo rates, which can obscure therapeutic benefits of drug candidates (Su et al 2004;Sands et al 2005;Sands 2009;D'Haens et al 2012). The need to reduce placebo risk in IBD trials has led to increasing use of expensive and sometimes invasive imaging modalities to compensate for the lack of highly reliable indicators of disease activity (Solem et al 2008;Loftus et al 2007;Buisson et al 2013), so development of reliable and noninvasive disease activity biomarkers is an ongoing area of interest.…”
Section: Utilization Of Animal Models In Ibd Researchmentioning
Animal models of human disease are a critical tool in both basic research and drug development. The results of preclinical efficacy studies often inform progression of therapeutic candidates through the drug development pipeline; however, the extent to which results in inflammatory bowel disease (IBD) models predict human drug response is an ongoing concern. This review discusses how murine models are currently being used in IBD research. We focus on the considerations and caveats for commonly used models in preclinical efficacy studies and discuss the value of models that utilize specific pathogenic pathways of interest rather than model all aspects of human disease.
“…IBS type symptoms may account for the high placebo responses sometimes seen with CDAI use in trials. (10, 11) These high placebo rates lead to difficulty in demonstrating treatment efficacy, as evidenced by a recent trial of certolizumab in CD, where the use of biomarkers as objective measures of disease activity may have enhanced the ability to reach statistical significance. (12) In UC, mucosal healing can be assessed by flexible sigmoidoscopy; however, this test is invasive and adds significant cost to care.…”
Section: Historical Measurement Tools Of Ibd Activitymentioning
Crohn’s disease and ulcerative colitis represent the two main forms of the idiopathic chronic inflammatory bowel diseases (IBD). Currently available blood and stool based biomarkers provide reproducible, quantitative tools which can complement clinical assessment to aid clinicians in IBD diagnosis and management. C-reactive protein and fecal based leukocyte markers can help the clinician distinguish IBD from non-inflammatory diarrhea and assess disease activity. The ability to differentiate between forms of IBD and predict risk for disease complications is specific to serologic tests including antibodies against Saccharomyces cerevisiae and perinuclear antineutrophil cytoplasmic proteins. Advances in genomic, proteomic and metabolomic array based technologies are facilitating the development of new biomarkers for IBD. The discovery of novel biomarkers which can correlate with mucosal healing or predict long term disease course has the potential to significantly improve patient care. This article reviews the uses and limitations of currently available biomarkers and highlights recent advances in IBD biomarker discovery.
“…Comparison of different definitions of success is complex, as a patient could be considered in remission by one trial but in a state of active disease by another. In addition, clinical trials of treatments of UC are known to have a diverse and unpredictable placebo response rate [206]. A 2007 meta-analysis of 40 clinical trials found that placebo induced remission rates ranged from 0-40% while placebo response was as high as 67% [207].…”
Section: Safety and Toxicology Of Probioticsmentioning
confidence: 99%
“…Shorter trials with fewer study visits lessen the cost of the study and reduce placebo values [206]. Long term trials may document a decrease in clinical effectiveness as relapses occur, the treatment ceases working and symptoms return.…”
Section: Safety and Toxicology Of Probioticsmentioning
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