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©The Author(s) 2022.
World J Gastrointest Oncol. Mar 15, 2022; 14(3): 547-567
Published online Mar 15, 2022. doi: 10.4251/wjgo.v14.i3.547
Published online Mar 15, 2022. doi: 10.4251/wjgo.v14.i3.547
Epidemiology | CRC in ulcerative colitis | CRC in indeterminate colitis | CRC in Crohn's disease | |
Annual incidence | Past | Stewénius et al[111], 1995, 1.4/1000 PYD; Eaden et al[2], 2001, 2/1000 PYD-after 10 yr of initial onset; 7/1000 PY (patients with extensive colitis 90%) 30 yr of initial onset; Castaño-Milla et al[112], 2012, 1.01/1000 PYD - after 10 yr of initial onset; 3.75/1000 PYD - after 20 yr of initial onset; 5.85/1000 PYD - after 30 yr of initial onset | Stewénius et al[111], 1995, 2.4/1000 PYD | Olén et al[113], 2020, a Scandinavian population-based cohort study 0.31 per 1000 PY(1968); Laukoetter et al[114], 2011, 0.5/1000 PYD |
Present | Fumery et al[115], 2017, the annual incidence of CRC was 0.8% (95%CI: 0.4-1.3) | Olén et al[113], 2020, a Scandinavian population-based cohort study 0.47 per 1000 person-years (2017) | ||
Risk | Past | Eaden et al[2], 2001, 0.3% after 30 yr of initial onset | Canavan et al[3], 2006, 2.9% after 10 yr of initial onset; 5.6% after 20 yr; 8.3% after 30 yr. Friedman et al[116], 2008, 7% by 10th surveillance (patients with extensive colitis 90%). Basseri et al[117], 2012, 5.6% by 10th surveillance (patients with extensive colitis 55%) | |
Present | Fumery et al[115], 2017, the risk of CRC was higher when LGD was diagnosed by an expert gastrointestinal pathologist (1.5%) than by community pathologists (0.2%). Factors significantly associated with dysplasia progression were concomitant: PSC (OR, 3.4; 95% CI: 1.5-7.8); Invisible dysplasia (vs visible dysplasia; OR, 1.9; 95% CI: 1.0-3.4), distal location (vs proximal location; OR, 2.0; 95% CI: 1.1-3.7); Multifocal dysplasia (vs unifocal dysplasia; OR, 3.5; 95% CI: 1.5-8.5) | Keller et al[118], 2019, IBD-CRC is responsible for approximately 2% of the annual mortality from CRC overall, but 10%-15% of the annual deaths in IBD patients | Olén et al[113], a Scandinavian population-based cohort study. Patients with Crohn's disease who were diagnosed with CRC were at increased risk of CRC mortality compared with reference individuals also diagnosed with CRC [HR 1.42 (1.16-1.75) when adjusted for tumour stage] |
Cytokines | The mechanism | Potential target of therapy? | Ref. |
TNF-α | Triggers systemic inflammation and is one of the cytokines that make up the acute phase reaction in IBD and other chronic inflammatory diseases TNF-α regulates the induction MACC1 via the NF-κB subunit p65 and the transcription factor c-Jun in CRC cells | Yes: Anti TNF used to control inflammation in IBD; hence may reduce incidence of CRC but this is debatable | Pache et al[119], Kobelt et al[120] |
IL-6 family | In the chronic phase of inflammation, IL-6 is able to activate almost all the cells of the body: trans-signalling-Increased formations of IL-6-sIL-6R complexes interact with gp130 on the membrane of CD4+T-cells and leads to an increased expression and nuclear translocation of STAT3, which causes the induction of anti-apoptotic genes, e.g., Bcl-xl. This leads to resistance of lamina propria T-cells to apoptosis. T-cell expansion contributes to chronic intestinal inflammation | No: Anti IL-6 antibodies not successfully used in IBD. Unlikely to be useful in reducing risk of IBD-CRC | Atreya and Neurath[121], Allocca et al[122], Coskun et al[123], Danese et al[124] |
IL-11 | IL-11 belongs to the IL-6 family of cytokines. IL-11 has pro-tumorigenic activities such as proliferation, self-renewal, invasion and angiogenesis | No: No evidence to suggest it could be used as therapeutic agent. Could be useful as a diagnostic and prognostic biomarker | Murakami et al[125], Johnstone et al[126], Ren et al[127], Unver and McAllister[128], Pastor et al[129], Putoczki et al[130] |
IL-17 | IL-7 is a cytokine that helps the long-term survival of Th17 cells and innate lymphoid cells that express the transcription factor RORγt. It is suspected to be important for maintaining populations of T cells that induce and induce mucosal inflammation in IBD. IL-7 also maintains NKT cells that produce IL-17, using the PI3K/AKT/mTOR pathway | No: Anti-IL-17 medications are associated with IBD exacerbation | Hohenberger et al[131], Moschen et al[132] |
IL-21 | IL21 plays a dual role: IL-21 deficiency as a novel cause of early-onset IBD in human subjects accompanied by defects in B-cell development. Reduced numbers of circulating CD19 (+) B cells, including IgM (+) naive and class-switched IgG memory B cells, with a concomitant increase in transitional B-cell numbers. IL-21 Overproduction: IL-21 plays an important role in sustaining tissue-damaging immune responses | Yes: Could be used as a potential new therapeutic target in CD but unclear if it will influence IBD-CRC | Di Fusco et al[133], Salzer et al[134] |
IL-23 | IL-23R signalling affects disease susceptibility increased production of IL-23 by macrophages, dendritic cells or granulocytes has been observed in various mouse models of colitis, colitis-associated cancer and IBD patients | Yes: Currently in clinical trials for CD but too early to comment on effect on IBD-CRC | Moschen et al[132], Neurath[135] |
Ref. | Number of patients and cohort | Results | Conclusions benefit-yes/no |
Rosenstock et al[136], 1985, Retrospective Review | 248 chronic UC patients | In this cohort of patients: Overall incidence of HGD was 6%; HGD or carcinoma found in 24 procedures in 16 patients, mean disease duration of 16 yr, 15 patients had HGD; DALM most consistent indicator of carcinoma. > 95% of cancers 6 recognized at colonoscopy | The presence/absence of dysplasia a reliable histological marker that correlates with the presence/absence of cancer in UC. DALM with HGD had the strongest indication for surgery. Benefit- yes |
Lashner et al[137], 1990, Prospective surveillance programme | 99 patients with pancolitis | In this cohort of patients: Both groups comparable in terms of age at onset, disease duration and gender; Total 8 fewer deaths in the surveillance group (P < 0.05); Colectomy was less common and was performed 4 yr later in the surveillance group (P < 0.05) | Screening in UC associated with improved survival and delayed colectomy. Findings did not show improvement in cancer-related survival. Benefit-equivocal |
Löfberg et al[138], 1990, 15-yr Prospective surveillance programme | 72 UC, 12 patients developed definite dysplasia | In this cohort of patients: LGD detected in 7 patients; HGD in 4 and 1 Dukes' Stage-A cancer at operation; The cumulative risk of developing at least LGD was 14% after 25 yr of disease; Abnormal, aneuploid DNA content detected in biopsies of 12/59 patients (20.3%) this correlated significantly with LGD and HGD | Long-term use of surveillance in UC is reliable in detecting dysplasia and identify patients for prophylactic surgery. Benefit-yes; Earlier detection of neoplasia |
Nugent et al[139], 1991, 13-yr Prospective surveillance programme | 213 UC patients | In this cohort of patients: A total of 15 patients underwent colectomy; A total of 7 patients had unsuspected carcinoma at various stages; Dysplasia detected among 11 patients; No difference in the prevalence of dysplasia between left-sided v/s extensive disease; No carcinoma detected among 175 patients without dysplasia on initial biopsies | Surveillance programme effective aid in reducing the risk of carcinoma in UC. Short term risk of CRC low if biopsy negative. Colectomy deferred in this group. Benefit-yes |
Lynch et al[140], 1993, Prospective surveillance(between 1978 and 1990) | 160 UC patients | In this cohort of patients: A total of 739 colonoscopies carried out (4.6 colonoscopies/per patient); A 709 patient-years follow-up was carried out; In 1 patient Dukes's A cancer was detected; IBD-CRC caused the death of 1 patient; Overall, 9 IBD-CRC cases were diagnosed during the study period but only 1 case was detected by way of the surveillance programme | Results of this large study with long follow-up cast doubts on the effectiveness of the surveillance programmes in detecting CRC in patients with UC. Benefit-no |
Jonsson et al[141], 1994, Prospective, longitudinal study between 1977 and 1991 | 131 patients with UC | In this cohort of patients: A total of 632 colonoscopies performed, dysplasia was diagnosed in 24 (4 HGD), other than those with cancer; CRC diagnosed in 4 patients, of whom 2 included in the programme with a diagnosis of cancer; CRC and dysplasia are seen mainly in the left colon and in pancolitis patients | The surveillance programme was resource consuming and the cost-benefit must be questioned. Benefit-no. No cost-benefit as per authors |
Karlén et al[142], 1998, Prospective case-control study | 4664 patients with UC, 142 patients with definite UC | In this cohort of patients: In 2 out of 40 patients with UC and 18/102 controls had at least one-surveillance colonoscopy (RR 0.29, 95% CI: 0.06-1.31); Out of 12 controls, only one patient with UC had two or more surveillance colonoscopies (RR 0.22, 95%CI: 0.03-1.74), indicating a protective dose-response relation | Surveillance may be associated with decreased risk of death from CRC in patients with long-standing UC. Benefit-yes. May improve survival |
Friedman et al[143], 2001, Prospective Longitudinal study | 259 patients with chronic Crohn's colitis | In this cohort of patients: A total of 663 examinations were performed on 259 patients; The median interval between examinations was 24 mo; More frequent examinations were carried out(1-6 mo) in patients with dysplasia; Dysplasia or cancer was detected in 16% (10 indefinite, 23 LGD, 4 HGD and 5 cancers); Definite dysplasia or cancer was associated with age > 45 yr and had increased symptoms | Colonoscopic surveillance should be strongly considered in chronic extensive Crohn's colitis. Benefit-yes. May improve survival |
Biasco et al[144], 2002, Prospective Longitudinal study (20 yr duration) | 65 patients with UC > 7 yr | In this cohort of patients: A total of 23 (35.3%) patients had surgery; A total of 29 (44.66%) patients discontinued the programme; Only 11 (16.9%) patients have remained in the programme | Results cast some doubts on the significance of such a programme and on its long-term feasibility. Benefit-no. Long-term feasibility doubtful |
Hata et al[145] 2003, Retrospective January 1979 and December 2001 | 217 UC patients | In this cohort of patients: A total of 15 patients were detected to have definite dysplasia; Among 5/15 proved to have invasive cancer in resected specimens; cumulative risk for development of definite dysplasia at 10, 20 and 30 yr was 3.1%, 10.0%, and 15.6% respectively; A cumulative risk for the development of invasive cancer at 10, 20, and 30 yr was 0.5%, 4.1%, and 6.1%, respectively | The surveillance programme is useful for detecting IBD-CRC and survival may be improved by surveillance colonoscopy. Benefit-yes. May improve survival |
- Citation: Majumder S, Shivaji UN, Kasturi R, Sigamani A, Ghosh S, Iacucci M. Inflammatory bowel disease-related colorectal cancer: Past, present and future perspectives. World J Gastrointest Oncol 2022; 14(3): 547-567
- URL: https://www.wjgnet.com/1948-5204/full/v14/i3/547.htm
- DOI: https://dx.doi.org/10.4251/wjgo.v14.i3.547