J Neurogastroenterol Motil 2025; 31(1): 28-37  https://doi.org/10.5056/jnm24084
Efficacy of Amitriptyline in Irritable Bowel Syndrome: A Systematic Review and Meta-analysis
Minahil Iqbal,1 Sara Hira,2 Humza Saeed,3 Sufyan Shahid,4 Suha T Butt,3 Kamran Rashid,3 Mohammad Ahmad,5 Hammad Hussain,6 Anzalna Mughal,6 Gabriel P A Costa,7 Fernanda Gushken,8 Neil Nero,9 Shreya Sengupta,10 and Akhil Anand11,12*
1Allama Iqbal Medical College, Lahore, Pakistan; 2Fatima Memorial Hospital, Lahore, Pakistan; 3Rawalpindi Medical University, Rawalpindi, Pakistan; 4Khawaja Muhammad Safdar Medical College, Sialkot, Pakistan; 5King Edward Medical University, Lahore, Pakistan; 6Islamic International Medical College, Rawalpindi, Pakistan; 7Faculty of Medicine, University of Ribeirão Preto, Ribeirão Preto, SP, Brazil; 8Faculdade Israelita de Ciências da Saúde Albert Einstein, São Paulo, SP, Brazil; 9Floyd D. Loop Alumni Library, Cleveland Clinic, Cleveland, OH, USA; 10Department of Gastroenterology and Hepatology, Cleveland Clinic, Cleveland, OH, USA; 11Department of Psychiatry and Psychology, Cleveland Clinic, Cleveland, OH, USA; and 12Department of Psychiatry, University Hospitals Medical Center, Cleveland, OH, USA
Correspondence to: *Akhil Anand, MD
Cleveland Clinic Center for Behavioral Health, 1730 West 25th Street/2A, Cleveland, OH 44113, USA
Tel: +1-216-363-2309, E-mail: Ananda3@ccf.org
Received: June 1, 2024; Revised: September 20, 2024; Accepted: September 22, 2024; Published online: January 31, 2025
© The Korean Society of Neurogastroenterology and Motility. All rights reserved.

cc This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
Abstract
Background/Aims
Amitriptyline is prescribed off-label for irritable bowel syndrome (IBS). We conducted a meta-analysis to assess its efficacy.
Methods
A systematic literature review was conducted until November 10, 2023, using MEDLINE, Embase, Cochrane Library, and Web of Science to study the efficacy of amitriptyline in patients with IBS. We included all randomized controlled trials that compared amitriptyline to placebo. Revised Cochrane risk-of-bias tool was used to assess the quality of studies. Meta-analyses were performed using a bivariate random-effects model. Statistical analyses were performed using R Software 4.2.3 and heterogeneity was assessed with I2 statistics.
Results
Seven trials were included with 796 patients (61% female). Amitriptyline was associated with better treatment response (OR, 5.30; 95% CI, 2.47 to 11.39; P < 0.001), reduced Irritable Bowel Syndrome Symptom Severity Scores (MD, –50.72; 95% CI, –94.23 to –7.20; P = 0.020) and improved diarrhea (OR, 10.55; 95% CI, 2.90 to 38.41; P < 0.001). No significant difference between the 2 groups regarding the adverse effects was observed. Three trials showed an overall low risk of bias, 2 trials showed an overall high risk of bias due to randomization and missing data, and 2 trials had some concerns regarding missing data.
Conclusions
Amitriptyline was found to be well-tolerated and effective in treating IBS compared to placebo. These findings support the use of amitriptyline for the management of IBS, particularly among patients with the IBS diarrhea subtype. Future research should focus on the dose-dependent effects of amitriptyline in IBS to better guide clinicians in personalized titration regimens.
Keywords: Abdominal pain; Amitriptyline; Antidepressants, tricyclic; Diarrhea; Irritable bowel syndrome
Introduction

Irritable bowel syndrome (IBS) is a chronic disorder of gut-brain interaction characterised by abdominal pain or discomfort along with altered bowel habits.1 Worldwide, approximately 11% of the population suffers from IBS, leading to an estimated annual healthcare cost of US$ 1.5-10 billion.2,3 According to the Rome IV criteria, IBS is defined as recurrent abdominal pain occurring at least once a week for a minimum of 3 months, accompanied by 2 or more of the following characteristics: (1) pain related to defecation, (2) changes in stool frequency, or (3) changes in stool consistency. To meet the criteria, these symptoms must have been present for at least 3 months, with an onset of at least 6 months prior to diagnosis.4 IBS is a chronic condition with an unpredictable pattern, which can significantly impact one’s quality of life.5 While there is no definitive treatment or cure for IBS, therapeutic options can address specific symptoms.6

The current treatment options recommended for IBS by the American College of Gastroenterology include dietary changes, soluble fiber supplementation, peppermint, chloride channel activators, guanylate cyclase activators, alosetron, mixed opioid agonists/antagonists, gut-directed psychotherapies, antibiotics (rifaximin), antidiarrheal medication (loperamide) and laxatives (linaclotide). Selective serotonin reuptake inhibitors (SSRIs) such as citalopram, fluoxetine, paroxetine, and tricyclic antidepressants (TCAs) like amitriptyline, nortriptyline, and imipramine, are also prescribed.7

TCAs have been prescribed off-label to treat IBS-related diarrhea for nearly 4 decades.8 Among all TCAs, amitriptyline stands out for its potent anticholinergic and sedative effects.9 It is believed that low-dose amitriptyline (25 mg to 50 mg) can alleviate IBS symptoms by reducing subjective pain or stress-related exacerbations.10 Despite their effectiveness, TCAs are underutilized in treating IBS. A web-based questionnaire sent to 275 primary care physicians revealed that less than 10% of respondents often prescribed TCAs for IBS.11 Moreover, there are no head-to-head trials done to establish safety of individual TCAs for the treatment of IBS.

Several meta-analyses have evaluated the efficacy of TCAs for IBS.12-15 However, only 1 meta-analysis has focused solely on amitriptyline.12 This meta-analysis included 4 studies with a total of 130 participants, and found amitriptyline to be beneficial for IBS adult patients (OR, 4.18; 95% CI, 2.00 to 8.77, Z = 3.79, P < 0.001). However, the analysis was limited by the small sample size. Since then, 2 large-scale trials have been conducted to investigate the efficacy of amitriptyline for IBS.16,17 Both studies had larger sample sizes than previous studies.

The purpose of this systematic review and meta-analysis is to assess the effectiveness of amitriptyline in treating IBS. This review provides an expanded and updated synthesis of all available randomized controlled trials (RCTs) that have investigated the efficacy of amitriptyline in treating IBS in comparison to a placebo. We hypothesize that amitriptyline has superior efficacy and comparable safety profile in managing symptoms of IBS when compared to placebo.

Materials and Methods

This systematic review and meta-analysis was carried out in accordance with the guidelines given by the Preferred Reporting Items for Systematic Reviews and Meta-Analysis (PRISMA) and the Cochrane Handbook for Systematic Reviews of Interventions.18,19 The study protocol is available at the International Prospective Register of Systematic Reviews (PROSPERO) under the identifier CRD42023479361.

Search Strategy

A comprehensive search strategy was developed with a medical librarian to identify potentially relevant articles. Indexing terms and keywords with truncation were combined using Boolean and proximity operators. No language restriction was imposed on the search. The following databases were searched from inception until November 10, 2023: Medline/PubMed (Ovid), Embase (Ovid), Cochrane Central Register of Controlled Trial, and Web of Science. Covidence software was used to manage, screen, de-duplicate, and extract this systematic review. Complete search strategies for each database are in Supplementary Material.

Eligibility Criteria

Inclusion in this meta-analysis was limited to RCTs comparing the effectiveness of amitriptyline with placebo for IBS treatment and reporting at least 1 outcome of interest. The outcomes of interest were response to treatment, Irritable Bowel Syndrome Symptom Severity Scores (IBS-SSS), decrease in abdominal pain, and improvement in diarrhea. Secondary outcomes assessed were adverse events, including dry mouth, constipation, and tachycardia. Exclusion criteria included studies lacking a control group, had a different comparator or had overlapping patient populations in multiple studies.

The efficacy outcomes were reported and described in the included studies as follows:

IBS-SSS: a 5-item rating system for IBS that assesses the severity and frequency of abdominal pain, bloating or distention, satisfaction with bowel habits, and overall impact of IBS on quality of life. Each factor is rated on a scale from 0 to 100, where 100 indicates increased severity. The final score ranges from 0 to 500.

Response to treatment: a reduction of > 50% of symptoms reported by patients at the end of the study or at least 15% improvement from baseline in overall quality of life score.

Decrease in abdominal pain: this measure was reported either as a decreased number of pain symptoms or a decrease in the mean visual analog scale score for pain.

Improvement in diarrhea: improvement in diarrhea was reported as a decrease in diarrhea frequency or an improvement in at least 1 level on the Bristol Stool Chart with respect to the shape or hardness of the stool.

Data Extraction

Titles and abstracts identified from the search were independently screened and assessed based on eligibility by 2 reviewers. After screening, the same reviewers then assessed the full-text articles for eligibility. From the articles retrieved from this search, additional references were identified by a manual search among the eligible articles. Any disagreements were resolved by consensus. Data from the eligible studies were extracted and catalogued independently by 2 reviewers using electronic spreadsheets specifically designed for this meta-analysis. The data collected included the first author’s name, the year of publication, number of participants, study design, follow-up duration, criteria used for diagnosis of IBS, IBS subtypes, amitriptyline dose, age, and sex of participants. For crossover trials, data were collected for treatment and control periods separately. In cases where data were not available or were insufficient within the published reports, e-mail attempts to contact authors were made.

Statistical and Sensitivity Analysis

Statistical analysis was performed on Review Manager 5.4. Treatment effects for binary outcomes were compared using pooled odds ratio (OR) with 95% confidence intervals (CI). To pool continuous outcomes, weighted mean differences were employed. The Cochran Q test and I2 statistics were used to assess heterogeneity; P-values < 0.10 and I² > 25% were considered significant for heterogeneity. The DerSimonian and Laird Random effects model was used for all of the outcomes.20 R software version 4.3.2 was used to perform leave-one-out sensitivity analysis and meta-regression to assess heterogeneity.21

Quality Assessment

Study quality was independently assessed by 2 authors using the Revised Cochrane risk of bias (RoB-2) tool for randomized and crossover trials.22 Studies were scored as low risk of bias, high risk of bias or some concerns depending on their biases in selection, performance, detection, attrition, and reporting.23 Any disagreements were resolved by consensus. Due to the limited number of studies (< 10), it was not possible to evaluate publication bias.24

Results

The systematic literature review yielded 832 studies after removing duplicates. After excluding 794 studies based on title and abstract screening, 38 full-text articles were reviewed for eligibility. Full-text screening identified 5 RCTs16,17,25-27 and 2 crossover trials.28,29 All 7 trials were included in the final analysis. No studies were captured from the manual search. See Figure 1 for the PRISMA Flow Diagram.

Figure 1. Preferred Reporting Items for Systematic Reviews and Meta-Analysis (PRISMA) flow diagram of the included studies.

Study Characteristics

Table provides a comprehensive overview of the 7 studies. We excluded a study30 from Chao and Zhang12 previous meta-analysis because that study included participants with functional dyspepsia as well as IBS. Although functional dyspepsia has overlapping symptoms with IBS, it is a distinct condition.31 Among patients in the included trials (n = 796), the mean ages ranged from 14.2 years to 49.2 years with 61% (486 of 796) identified as females. Among the 5 trials that specified patients according to IBS subtypes, 56% (414 of 742) of patients had IBS-diarrhea (IBS-D) subtype. Among the 2 trials reporting the IBS-SSS scores, the mean scores ranged from 253.38 to 273.4 in the amitriptyline arm and 264.64 to 272.1 in the placebo arm. Across the trials, the amitriptyline dose varied from 10 mg to 75 mg, and the study durations ranged from 8 weeks to 52 weeks. Three IBS-D studies (Bahar et al,27 Li et al,17 and Vahedi et al26) reported improvement in diarrhea symptoms, but used different metrics: Bahar et al27 used percentage change, while Vahedi et al26 and Li et al17 used dichotomous outcomes.

Table. Baseline Characteristics of the Included Studies

AuthorYearCountryStudy designTreatment period (wk)Criteria for diagnosisAmitriptyline doses (mg)ParticipantsAge (yr)Sex (M/F)Mean DOS (mo)IBS-SSSIBS-subtype
I/CAMIPlaceboAMIPlaceboIBS-CIBS-DIBS-MIBS-U
ATLANTIS2023EnglandRCT52Rome IV10-3046349.2/47.8148/31510a,b273.4272.17718119114
Li2019ChinaRCT52Rome III2517041.3/42.588/8214.13 ± 10.1515.78 ± 9.7253.38264.64013900
Vahedi2008IranRCT8Rome II105439/3329/2143 ± 5236 ± 3705000
Bahar2008USARCT13Rome II10/20/303315.3/14.29/2403300
Morgan2005USAC-RCT11Rome II25, 5022390/227114
Rajagopalan1998AustraliaRCT12Rome25, 50, 754035.1/34.511/1159.4 ± 28.748 ± 23.2
Steinhart1982USAC-RCT11ARS5014413/115.07a

aIn years.

bMedian.

DOS, duration of symptoms; M/F, male/female; IBS-SSS, irritable bowel syndrome symptom severity score; IBS, irritable bowel syndrome; I/C, intervention/control; AMI, amitriptyline; IBS-C, constipation predominant IBS; IBS-D, diarrhea predominant IBS; IBS-M, mixed bowel habits IBS; IBS-U, unclassified IBS; USA, United States of America; RCT, randomized controlled trial; C-RCT, crossover randomized controlled trial; ARS, arbitrary rating scale.



Outcome Measures

Patients who were treated with amitriptyline showed a statistically significant higher response to treatment compared to placebo (OR, 5.30; 95% CI, 2.47 to 11.39; P < 0.001). Upon conducting a sensitivity analysis of treatment response in studies that included only IBS-D patients, the treatment response was still statistically significant for amitriptyline (OR, 7.46; 95% CI, 3.74 to 14.88; P < 0.001). Additionally, we found a significant decrease in IBS-SSS (MD, –50.72; 95% CI, –94.23 to –7.20; P = 0.020) and improvement in diarrhea (OR, 10.55; 95% CI, 2.90 to 38.41; P < 0.001). In patients treated with amitriptyline relative to placebo. A decrease in abdominal pain (OR, 5.23; 95% CI, 0.87 to 31.68; P = 0.070) was found to be marginally significant. See Figure 2 for the forest plots of all outcome measures.

Figure 2. Forests plots for efficacy outcomes. (A) Forest plot of studies comparing amitriptyline with placebo in terms of “Treatment response” outcome. (B) Sensitivity analysis of Treatment response including trials with IBS-diarrhea patients only. (C) Forest plot of studies comparing Irritable Bowel Syndrome Symptom Severity Scores. (D) Forest plot of studies comparing Decrease in Abdominal Pain. (E) Forest plot of studies comparing Improvement in Diarrhea. M-H, Mantel-Haenszel.

Adverse Events

Overall, there were no statistically significant differences in adverse effects between the placebo and amitriptyline groups. The adverse events included tachycardia (OR, 1.04; 95% CI, 0.64 to 1.69; P = 0.870), dry mouth (OR, 2.50; 95% CI, 0.51 to 12.22; P = 0.260), and constipation (OR, 1.52; 95% CI, 0.51 to 4.49; P = 0.450). See Supplementary Figures 1-3 for forest plots of tachycardia, dry mouth, and constipation. Across all studies, adverse events were mainly self-reported and assessed in a binary manner.

The ATLANTIS trial used the Antidepressant Side-Effect Checklist, a validated self-reporting instrument that measures 21 adverse reactions to antidepressants. Participants rated the severity of each item on a 4-point scale (0 = absent; 1 = mild; 2 = moderate; and 3 = severe) and indicated whether a symptom, if present, was likely a side effect of the antidepressant drug (yes or no).32 The trial found that less than 5 percent of participants treated with amitriptyline experience severed symptoms, other than constipation and diarrhea. Additionally, the trial reported a higher attrition rate in the amitriptyline group compared to the placebo group, with rates of 13% and 9% respectively.

Leave-one-out Sensitivity Analysis and Meta-regression

Leave-one-out sensitivity analysis33 decreased the heterogeneity I2 from 66% to 0% by eliminating the ATLANTIS trial for response to treatment (Fig. 3). However, moderate to severe heterogeneity persisted for the rest of the outcomes and adverse effects. Meta-regression showed that at the 3-month follow-up, there was no significant association between follow-up duration and odds ratio. However, at the 6-month follow-up, the odds ratio decreased as the follow-up duration increased (Supplementary Fig. 7 and 8). To validate our findings, we conducted a sensitivity analyses: one excluding studies with a high risk of bias (Supplementary Fig. 9), and another excluding the crossover trials (Supplementary Fig. 10). The results across all these analyses confirmed the reliability of our findings. For further details, refer to Supplementary Figures 4-6 for leave-one-out sensitivity analysis for outcomes and adverse effects, sensitivity analysis and meta-regression plots.

Figure 3. Leave-one-out sensitivity analysis for treatment response.

Quality Assessment

According to our assessment using the RoB-2, 3 trials16,26,28 showed a low risk of bias. However, 2 trials25,27 exhibited a high risk of bias due to problems with randomization and missing data. The studies by Bahar et al27 and Rajagopalan et al25 had a high risk of bias due to inadequate reporting of key methodological details. Specifically, Bahar et al27 failed to describe random sequence generation, allocation concealment, blinding, and handling of incomplete outcome data, with 2 dropouts lacking explanation. Similarly, Rajagopalan et al25 lacked clarity on random sequence generation and allocation concealment, with unreported reasons for equal numbers of dropouts in each group. Additionally, 2 other trials17,29 raised some concerns due to missing outcome data due to loss of patient follow-up. See Supplementary Table for the risk of bias assessment.

Discussion

This systematic review and meta-analysis found that amitriptyline, compared to placebo, improved treatment response rates, reduced severity of irritable bowel syndrome symptoms, and improved diarrhea while maintaining a similar safety profile. However, for abdominal pain, amitriptyline showed only a marginally significant improvement compared to placebo (Fig. 2). Our findings are consistent with previous meta-analyses by Chao and Zhang,12 Ford et al,13 and Ruepert et al,15 all of which reported statistically significant improvements in IBS symptoms with TCAs compared to placebo. The exact mechanism by which amitriptyline alleviates IBS symptoms is unclear. It is hypothesized that amitriptyline’s potent anticholinergic properties may reduce visceral hypersensitivity and gastrointestinal motility.34,35 Our analysis revealed a marginally significant reduction in abdominal pain, consistent with preclinical findings suggesting that TCAs may also decrease pain fibers responses in the pelvic nerve, leading to decreased sensitivity to painful colorectal distension.36

According to our analysis, amitriptyline had a similar safety profile to placebo. This finding contrasts with a previous meta-analysis by Ford et al13 2019 which suggested that TCAs had a higher risk of adverse effects to placebo, such as drowsiness and dry mouth. However, it is worth noting that the previous analysis compared both TCAs and SSRIs to placebo.13 Similarly, the most common side effects reported in our analysis were constipation, tachycardia, and dry mouth. In fact, the ATLANTIS trial reported a wide range of additional adverse effects captured by an Antidepressant Side Effect Checklist Questionnaire, but none of the reported adverse events were statistically significant for the amitriptyline arm.16 In the ATLANTIS trial, 2 Serious Adverse Events occurred in the amitriptyline arm compared to 3 in the placebo arm. Details regarding these events were not reported due to the small number of occurrences and to preserve patient anonymity. The reduced side effects in our analysis, compared to previous studies, may be attributed to the ATLANTIS trial's large sample size and relatively low dose (10-30 mg) of amitriptyline. This dose was further titrated based on side effects and symptom response, which may have reduced the incidence of adverse events. Additionally, the ATLANTIS trial used a comprehensive Antidepressant Side-Effect Checklist, potentially capturing a wider range of effects. We acknowledge that this large trial likely had a substantial influence on our overall results. None of the other studies reported Serious Adverse Events. These results could impact future IBS management, as few general practitioners currently prescribe amitriptyline for IBS.11

The American College of Gastroenterology strongly recommends using TCAs to alleviate global symptoms of IBS.1 For amitriptyline, the recommendation is to start with an initial 10 mg dose, with gradual dose adjustment based on response and tolerability. Slow up-titration may minimize side effects and improve adherence.37 However, slow titration may delay therapeutic effects. In the ATLANTIS trial, titration started at 10 mg daily, and increased to a maximum of 30 mg over 3 weeks based on treatment response and tolerability. In the Rajagopalan et al25’s trial, amitriptyline titration was fixed. Patients were prescribed 25 mg every night for the first week, followed by 50 mg every night for the second week, and then 75 mg every night until the end of the treatment period.25 The Morgan et al29 trial was also a forced titration study, but prescribed 25 mg of amitriptyline for the first week and 50 mg for the following weeks. The remaining trials did not perform titration regimens. Overall, no study reported the effects of amitriptyline dose titration in IBS. Future research should evaluate optimal dosage ranges and titration schedules. A fixed-dose RCTs would provide valuable insights into the efficacy, safety and tolerability of amitriptyline in the treatment of IBS. Additionally, studies should investigate the impact of dose titration on symptom improvement, time to clinical response, and patient adherence. By conducting such studies, researchers can develop evidence-based recommendations for personalized amitriptyline treatment plans that maximize therapeutic benefits while minimizing adverse effects in patients with IBS.

Amitriptyline is typically administered at low doses in IBS. A study by Halpert et al38 found that increasing the dosage or blood levels of desipramine did not improve IBS symptoms. This suggests that lower doses may be sufficient in managing IBS symptoms with minimal side effects.38 Conversely, Drossman et al39 have suggested that if no side effects are present, doses may be increased to 100-150 mg. All trials analyzed in our study used sub-therapeutic doses compared to those used for treating depression. It is hypothesized that the observed benefits may be attributed to amitriptyline's high anti-cholinergic property, which reduces visceral hypersensitivity and gastrointestinal motility, particularly relevant for IBS-D. Future research should investigate the dose-dependent effects of amitriptyline in IBS, explore physician and patient perceptions of amitriptyline for IBS treatment, as well as design robust phase III trials, building on the methodology of the ATLANTIS trial, with a focus on IBS-D. Despite the American College of Gastroenterology and the American Gastroenterological Association’s recommendations, there remains a need for more clinical trials to determine the efficacy of TCAs in treating IBS.1,40

The analyzed studies lacked participant homogeneity. For example, Morgan et al29 included only adult females, and Bahar et al27 included both sexes but only adolescents, while all other studies included both sexes but only adults. Sex differences play a significant role in IBS, but limitations in this study prevented a meta-analysis by sex. This underscores the need for future studies to prioritize sex-based analysis to ensure a comprehensive understanding of the disease. Also, only 2 trials ATLANTIS trial and Morgan et al29 included patients other than the IBS-D population. Another example of clinical heterogeneity, in the Li et al17 study the mean duration of IBS symptoms was 14 months, while in ATLANTIS the mean duration was 120 months. The studies also lacked methodological homogeneity, such as the use of IBS-SSS in the ATLANTIS trial and Li et al,17 versus self-reporting in other studies, and differing thresholds for clinically significant improvements, like the 35-point minimum in the ATLANTIS trial. Recently, several new assessment tools have been introduced, including the IBS Quality of Life Questionnaire,41 the Digestive Health Status Instrument,42 and the Patient Health Questionnaire-12 Somatic Symptom Scale,43 which may improve clinical homogeneity in future meta-analyses. All trials were similar in certain aspects. It is important to note that they were all double-blind, randomized, and placebo-controlled. Additionally, they consistently excluded patients with severe mental illness and those already taking psychiatric medications. Finally, except for the study by Morgan et al,29 all studies were conducted in an outpatient setting.

The sensitivity analysis reported a decrease in heterogeneity largely attributed to the ATLANTIS study’s large sample size. The meta-regression showed that the ATLANTIS trial, specifically its 6-month follow-up data, is a significant contributor to the meta-analysis’s heterogeneity. Meta-regression results offer a possible explanation for this variability, suggesting that treatment efficacy may decrease over time due to factors like waning treatment adherence, resistance development, or natural disease progression. However, the 3-month follow-up data from the ATLANTIS trial did not show a significant association between follow-up duration and treatment response, potentially due to the shorter time frame. Future studies should include longer follow-up periods, similar to the ATLANTIS trial, and also consider the potential impact of varying outcome assessment methods on heterogeneity.

Limitations

Our meta-analysis has several limitations. Firstly, the inclusion of 2 crossover trials introduces the potential for a unit-of-analysis error.44 Secondly, all trials with the exception of Steinhart et al28 relied on the Rome criteria to recruit patients, but these criteria have changed significantly since their initial version in 1992. This evolution has led to inconsistencies in how patients are selected for the studies.45 There was variability in the treatment period, assessment tools, outcome measures used, and amitriptyline dosages, which further impacts the heterogeneity of the analysis. For studies that included patients with different IBS subtypes, data on specific outcomes for each subtype were not reported, limiting our ability to perform a subgroup analysis, particularly for constipation predominant IBS patients. Finally, it is also important to interpret the findings cautiously because of the clinical and methodological differences between the studies.

In conclusion, IBS is a common chronic gut-brain disease which significantly impacts quality of life for patients. Our analysis suggests that amitriptyline may improve response to treatment, IBS-SSS score, and diarrhea while having a similar safety profile to placebo. Amitriptyline should be considered as a treatment option in IBS-D patients. Future research should investigate dose-dependent effects of amitriptyline, employ standardized outcome measures, extend treatment periods, and encompass diverse patient populations across various age groups and all IBS subtypes to enhance the generalizability of findings.

Financial support

None.

Conflicts of interest

None.

Author contributions

Minahil Iqbal: conceptualization, methodology, data collection, formal analysis, writing manuscript, and editing manuscript; Sara Hira: conceptualization, methodology, data collection, formal analysis, and supervision; Humza Saeed: conceptualization, methodology, data collection, and formal analysis; Sufyan Shahid: conceptualization, methodology, data collection, and formal analysis; Suha T Butt, Kamran Rashid, Mohammad Ahmad, Hammad Hussain, and Anzalna Mughal: conceptualization, methodology, data collection, formal analysis; Gabriel P A Costa and Fernanda Gushken: conceptualization, methodology, formal analysis, and editing manuscript; Neil Nero: methodology, data collection, and resources; Shreya Sengupta: conceptualization, methodology, resources, writing manuscript, editing manuscript, visualization, and supervision; and Akhil Anand: conceptualization, methodology, data collection, resources, writing manuscript, editing manuscript, visualization, and supervision.

Supplementary Materials

Note: To access the supplementary material, table, and figures mentioned in this article, visit the online version of Journal of Neurogastroenterology and Motility at http://www.jnmjournal.org/, and at https://doi.org/10.5056/jnm24084.

References
  1. Lacy BE, Pimentel M, Brenner DM, et al. ACG clinical guideline: management of irritable bowel syndrome. Am J Gastroenterol 2021;116:17-44.
    Pubmed CrossRef
  2. Canavan C, West J, Card T. The epidemiology of irritable bowel syndrome. Clin Epidemiol 2014;6:71-80.
    Pubmed KoreaMed CrossRef
  3. Peery AF, Crockett SD, Murphy CC, et al. Burden and cost of gastrointestinal, liver, and pancreatic diseases in the United States: update 2018. Gastroenterology 2019;156:254-272.e11.
    Pubmed KoreaMed CrossRef
  4. Lacy BE, Mearin F, Chang L, et al. Bowel disorders. Gastroenterology 2016;150:1393-1407, e5.
    Pubmed CrossRef
  5. BouSaba J, Sannaa W, Camilleri M. Pain in irritable bowel syndrome: does anything really help?. Neurogastroenterol Motil 2022;34:e14305.
    Pubmed KoreaMed CrossRef
  6. Vasant DH, Paine PA, Black CJ, et al. British society of gastroenterology guidelines on the management of irritable bowel syndrome. Gut 2021;70:1214-1240.
    Pubmed CrossRef
  7. Trinkley KE, Nahata MC. Treatment of irritable bowel syndrome. J Clin Pharm Ther 2011;36:275-282.
    Pubmed CrossRef
  8. Lancaster-Smith MJ, Prout BJ, Pinto T, Anderson JA, Schiff AA. Influence of drug treatment on the irritable bowel syndrome and its interaction with psychoneurotic morbidity. Acta Psychiatr Scand 1982;66:33-41.
    Pubmed CrossRef
  9. Thour A, Marwaha R. Amitriptyline. In: StatPearls. Treasure Island (FL): StatPearls Publishing 2023:1-6.
    CrossRef
  10. Thoua NM, Murray CD, Winchester WJ, et al. Amitriptyline modifies the visceral hypersensitivity response to acute stress in the irritable bowel syndrome. Aliment Pharmacol Ther 2009;29:552-560.
    Pubmed CrossRef
  11. Shivaji UN, Ford AC. Beliefs about management of irritable bowel syndrome in primary care: cross-sectional survey in one locality. Prim Health Care Res Dev 2015;16:263-269.
    Pubmed CrossRef
  12. Chao GQ, Zhang S. A meta-analysis of the therapeutic effects of amitriptyline for treating irritable bowel syndrome. Intern Med 2013;52:419-424.
    Pubmed CrossRef
  13. Ford AC, Lacy BE, Harris LA, Quigley EMM, Moayyedi P. Effect of antidepressants and psychological therapies in irritable bowel syndrome: an updated systematic review and meta-analysis. Am J Gastroenterol 2019;114:21-39.
    Pubmed CrossRef
  14. Rahimi R, Nikfar S, Rezaie A, Abdollahi M. Efficacy of tricyclic antidepressants in irritable bowel syndrome: a meta-analysis. World J Gastroenterol 2009;15:1548-1553.
    Pubmed KoreaMed CrossRef
  15. Ruepert L, Quartero AO, de Wit NJ, van der Heijden GJ, Rubin G, Muris JW. Bulking agents, antispasmodics and antidepressants for the treatment of irritable bowel syndrome. Cochrane database Syst Rev 2011;2011:CD003460.
    Pubmed KoreaMed CrossRef
  16. Ford AC, Wright-Hughes A, Alderson SL, et al. amitriptyline at low-dose and titrated for irritable bowel syndrome as second-line treatment in primary care (ATLANTIS): a randomised, double-blind, placebo-controlled, phase 3 trial. Lancet 2023;402:1773-1785.
    Pubmed CrossRef
  17. Li WD, Jia L, Jiang SM, Ping L, Xu M. The therapeutic effect of low-dose amitriptyline on patients with refractory diarrhea-predominant irritable bowel syndrome and its 1-year follow-up study. Int J Clin Exp Med 2019;12:891-898.
  18. Page MJ, McKenzie JE, Bossuyt PM, et al. The PRISMA 2020 statement: an updated guideline for reporting systematic reviews. BMJ 2021;372:n71.
    Pubmed KoreaMed CrossRef
  19. Higgins JPT, Thomas J, Chandler J, et al. Cochrane handbook for systematic reviews of interventions. 2nd ed. Chichester: John Wiley & Sons 2019.
    CrossRef
  20. Langan D, Higgins JPT, Jackson D, et al. A comparison of heterogeneity variance estimators in simulated random-effects meta-analyses. Res Synth Methods 2019;10:83-98.
    Pubmed CrossRef
  21. Balduzzi S, Rücker G, Schwarzer G. How to perform a meta-analysis with R: a practical tutorial. Evid Based Ment Health 2019;22:153-160.
    Pubmed KoreaMed CrossRef
  22. Sterne JAC, Savović J, Page MJ, et al. RoB 2: a revised tool for assessing risk of bias in randomized trials. BMJ 2019;366:I4898.
  23. Higgins JP, Altman DG, Gøtzsche PC, et al. The Cochrane collaboration's tool for assessing risk of bias in randomised trials. BMJ 2011;343:d5928.
    Pubmed KoreaMed CrossRef
  24. Egger M, Davey Smith G, Schneider M, Minder C. Bias in meta-analysis detected by a simple, graphical test. BMJ 1997;315:629-634.
    Pubmed KoreaMed CrossRef
  25. Rajagopalan M, Kurian G, John J. Symptom relief with amitriptyline in the irritable bowel syndrome. J Gastroenterol Hepatol 1998;13:738-741.
    Pubmed CrossRef
  26. Vahedi H, Merat S, Momtahen S, et al. Clinical trial: the effect of amitriptyline in patients with diarrhoea-predominant irritable bowel syndrome. Aliment Pharmacol Ther 2008;27:678-684.
    Pubmed CrossRef
  27. Bahar RJ, Collins BS, Steinmetz B, Ament ME. Double-blind placebo-controlled trial of amitriptyline for the treatment of irritable bowel syndrome in adolescents. J Pediatr 2008;152:685-689.
    Pubmed CrossRef
  28. Steinhart MJ, Wong PY, Zarr ML. Therapeutic usefulness of amitriptyline in spastic colon syndrome. Int J Psychiatry Med 1981;11:45-57.
    Pubmed CrossRef
  29. Morgan V, Pickens D, Gautam S, Kessler R, Mertz H. Amitriptyline reduces rectal pain related activation of the anterior cingulate cortex in patients with irritable bowel syndrome. Gut 2005;54:601-607.
    Pubmed KoreaMed CrossRef
  30. Mertz H, Fass R, Kodner A, Yan-Go F, Fullerton S, Mayer EA. Effect of amitriptyline on symptoms, sleep, and visceral perception in patients with functional dyspepsia. Am J Gastroenterol 1998;93:160-165.
    Pubmed CrossRef
  31. Gwee KA, Chua AS. Functional dyspepsia and irritable bowel syndrome, are they different entities and does it matter?. World J Gastroenterol 2006;12:2708-2712.
    Pubmed KoreaMed CrossRef
  32. Uher R, Farmer A, Henigsberg N, et al. Adverse reactions to antidepressants. Br J Psychiatry 2009;195:202-210.
    Pubmed CrossRef
  33. Penn State Eberly College of Science. 16.8 - Random Effects/Sensitivity Analysis | STAT 509. Available from URL: http://handbook.cochrane.org/. Available from URL: https://online.stat.psu.edu/stat509/lesson/16/16.5 (accessed 21 Apr 2016)
  34. McQuay HJ, Carroll D, Glynn CJ. Low dose amitriptyline in the treatment of chronic pain. Anaesthesia 1992;47:646-6512.
    Pubmed CrossRef
  35. Gorard DA, Libby GW, Farthing MJ. Effect of a tricyclic antidepressant on small intestinal motility in health and diarrhea-predominant irritable bowel syndrome. Dig Dis Sci 1995;40:86-95.
    Pubmed CrossRef
  36. Su X, Gebhart GF. Effects of tricyclic antidepressants on mechanosensitive pelvic nerve afferent fibers innervating the rat colon. Pain 1998;76:105-114.
    Pubmed CrossRef
  37. Torta RG. Antidepressant up-titration: pharmacological and psychological considerations. Expert Opin Drug Saf 2012;11:685-688.
    Pubmed CrossRef
  38. Halpert A, Dalton CB, Diamant NE, et al. Clinical response to tricyclic antidepressants in functional bowel disorders is not related to dosage. Am J Gastroenterol 2005;100:664-671.
    Pubmed CrossRef
  39. Drossman DA, Tack J, Ford AC, Szigethy E, Törnblom H, Van Oudenhove L. Neuromodulators for functional gastrointestinal disorders (Disorders of Gut−Brain Interaction): a rome foundation working team report. Gastroenterology 2018;154:1140-117, e1.
    Pubmed CrossRef
  40. Lembo A, Sultan S, Chang L, Heidelbaugh JJ, Smalley W, Verne GN. AGA clinical practice guideline on the pharmacological management of irritable bowel syndrome with diarrhea. Gastroenterology 2022;163:137-151.
    Pubmed CrossRef
  41. Patrick DL, Drossman DA, Frederick IO, DiCesare J, Puder KL. Quality of life in persons with irritable bowel syndrome: development and validation of a new measure. Dig Dis Sci 1998;43:400-411.
    Pubmed CrossRef
  42. Shaw M, Talley NJ, Adlis S, Beebe T, Tomshine P, Healey M. Development of a digestive health status instrument: tests of scaling assumptions, structure and reliability in a primary care population. Aliment Pharmacol Ther 1998;12:1067-1078.
    Pubmed CrossRef
  43. Spiller RC, Humes DJ, Campbell E, et al. The patient health questionnaire 12 somatic symptom scale as a predictor of symptom severity and consulting behaviour in patients with irritable bowel syndrome and symptomatic diverticular disease. Aliment Pharmacol Ther 2010;32:811-820.
    Pubmed CrossRef
  44. Elbourne DR, Altman DG, Higgins JP, Curtin F, Worthington HV, Vail A. Meta-analyses involving cross-over trials: methodological issues. Int J Epidemiol 2002;31:140-149.
    Pubmed CrossRef
  45. Lacy BE, Patel NK. Rome criteria and a diagnostic approach to irritable bowel syndrome. J Clin Med 2017;6:99.
    Pubmed KoreaMed CrossRef


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