| Literature DB >> 35308554 |
Xinhui Wu1, Jingxi Wang2, Zhen Ye3, Jin Wang3, Xibei Liao3, Mengsi Liv3, Zhen Svn3.
Abstract
Background and Aims: Evidence on the association between irritable bowel syndrome (IBS) and colorectal cancer (CRC) risk is inconsistent. Therefore, we aimed to examine whether IBS leads to an increased risk for CRC using a systematic review and meta-analysis approach.Entities:
Keywords: CRC screening; colorectal cancer; epidemiology; irritable bowel syndrome; meta-analysis; risk factor
Year: 2022 PMID: 35308554 PMCID: PMC8924657 DOI: 10.3389/fmed.2022.819122
Source DB: PubMed Journal: Front Med (Lausanne) ISSN: 2296-858X
The PICOS criteria for the definition of research question.
| Populations | Non-specific |
| Intervention | Patients diagnosed with irritable bowel syndrome |
| Comparator | Patients without a diagnosis of irritable bowel syndrome, general population |
| Outcome | Risk ratio or standardized incidence ratio for colorectal cancer |
| Study design | Cohort study, case-control study |
Figure 1Flowchart of study selection.
Main characteristics of the eligible studies.
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| Chang et al. | Taiwan, China | 1999–2009 | Prospective cohort | Mean 55.9 | 23,847/15,537 | Community | 9,160 | 30,224 | ICD code | Colonoscopy and national cancer registry data | Adjusted for age, gender, BMI, CRC family history, alcohol drinking, education, diabetes, and hypertension | Mean 7.78 |
| Canavan et al. ( | UK | Since 1987 | Prospective cohort | IBS: mean 42.9; non-IBS: mean 42.8 | 476,900/182,857 | UK CPRD | 112,854 | 546,903 | Read code | CRC Read term code or ICD code | Matched by sex and age | IBS: mean 6.5; non-IBS: mean 3.6 |
| García Rodriguez et al. ( | UK | 1994–1998 | Prospective cohort | 20–79 | NP | England and Wales GPRD | 2,956 | 20,000 | Read code | Read code | Adjusted for age and gender | Mean 3 |
| Nørgaard et al. ( | Denmark | 1977–2008 | Retrospective cohort | Median 47 | 39,998/17,853 | DNRP | 57,851 | Expected incidence rate | ICD code | ICD code | Standardized on period of follow-up, age, gender, and time of diagnosis | Mean 8.8 |
| Hsiao et al. | Taiwan, China | 2000–2010 | Retrospective cohort | IBS: mean 44.6; non-IBS: mean 44.4 | 148,878/126,360 | LHID | 91,746 | 183,492 | ICD code | ICD code | Matched by age, gender, and time of diagnosis; adjusted for age, gender, urbanization, hypertension, diabetes, and hyperlipidemia | 1–11 |
| Hu et al. ( | Taiwan, China | 2000–2010 | Retrospective cohort | Median 50.9 | 13,727/16,111 | NHIRD | 29,838 | Expected incidence rate | ICD code (≥3 visits and diagnosis was not altered within 3 months) | Registry for Catastrophic Illness (histologic confirmation is required) | Standardized on age, gender, and duration of IBS | Median 4.56 |
IBS, irritable bowel syndrome; CRC, colorectal cancer; ICD, International Classification of Diseases; F/M, female/male; NP, not provided; CRPD, Clinical Practice Research Datalink; GRPD, General Practice Research Database; DNRK, Danish National Registry of Patients; LHID, Longitudinal Health Insurance Database; NHIRD, Taiwan National Health Insurance Research Database.
The quality assessment of included studies.
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| Chang et al. ( | ⋆ | ⋆ | ⋆ | ✰ | ⋆⋆ | ⋆ | ⋆ | ⋆ | 8 |
| Canavan et al. ( | ⋆ | ⋆ | ⋆ | ✰ | ⋆✰ | ⋆ | ⋆ | ⋆ | 7 |
| García Rodriguez et al. ( | ⋆ | ⋆ | ⋆ | ✰ | ⋆⋆ | ⋆ | ✰ | ⋆ | 7 |
| Nørgaard et al. ( | ⋆ | ⋆ | ⋆ | ✰ | ⋆✰ | ⋆ | ⋆ | ⋆ | 7 |
| Hiso et al. ( | ⋆ | ⋆ | ⋆ | ✰ | ⋆⋆ | ⋆ | ⋆ | ⋆ | 8 |
| Hu et al. ( | ⋆ | ⋆ | ⋆ | ✰ | ⋆✰ | ⋆ | ⋆ | ⋆ | 7 |
A median/mean follow-up of more than 3 years or a maximum follow-up of more than 10 years was considered adequate.
Figure 2Overall association between irritable bowel syndrome and subsequent colorectal cancer risk.
Subgroup analysis of the association between IBS and subsequent CRC risk.
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| 5 | 1.52 | 1.04–2.22 | 0.032 | 98.2% | <0.001 |
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| ≤ 1 year | 3 | 6.84 | 3.70–12.65 | <0.001 | 95.6% | <0.001 |
| >1 year | 4 | 1.02 | 0.88–1.18 | 0.813 | 77.1% | <0.001 |
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| <50 years | 3 | 2.03 | 1.17–3.53 | 0.012 | 89.8% | <0.001 |
| ≥ 50 years | 3 | 1.28 | 0.94–1.75 | 0.118 | 95.6% | <0.001 |
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| Female | 3 | 1.30 | 0.81–2.08 | 0.280 | 96.8% | <0.001 |
| Male | 3 | 1.32 | 0.71–2.46 | 0.376 | 97.6% | <0.001 |
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| Prospective | 2 | 1.43 | 1.06–1.94 | 0.020 | 81.8% | 0.019 |
| Retrospective | 3 | 1.59 | 0.84–3.00 | 0.154 | 99.1% | <0.001 |
Figure 3Sensitivity analysis of the colorectal cancer risk in patients with irritable bowel syndrome.
Comparison of the use of random-effects vs. fixed-effects models.
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| Overall | 1.52 (1.04–2.22) | 1.52 (1.45–1.60) |
| Followed-up ≤ 1 year | 6.84 (3.70–12.65) | 6.26 (5.60–7.01) |
| Followed-up >1 year | 1.02 (0.88–1.18) | 0.98 (0.92–1.04) |
| Age <50 years | 2.03 (1.17–3.53) | 1.75 (1.48–2.06) |
| Age ≥ 50 years | 1.28 (0.94–1.75) | 1.50 (1.41–1.60) |
| Female | 1.30 (0.81–2.08) | 1.41 (1.30–1.52) |
| Male | 1.32 (0.71–2.46) | 1.72 (1.57–1.89) |
| Prospective | 1.43 (1.06–1.94) | 1.57 (1.44–1.72) |
| Retrospective | 1.59 (0.84–3.00) | 1.50 (1.41–1.59) |