In Colombia, ulcerative Colitis is managed by gastroenterologists. Ulcerative colitis is a chronic immune-mediated inflammatory bowel disease that produces continuous mucosal ulceration of the colon, starting at the rectum and extending proximally without skipping segments. It affects roughly 1.2 million people in the United States and around 5 million worldwide (Ng Lancet 2017), with peak incidence in North America and Europe and rising rates across newly industrialized regions.
Ulcerative colitis (ICD-10: K51) is a chronic relapsing-remitting inflammatory bowel disease characterized by continuous mucosal and submucosal inflammation that begins in the rectum and extends proximally to a variable degree, always limited to the colon. The histologic signature is crypt distortion, crypt abscesses, basal plasmacytosis, and depleted goblet cells, with inflammation confined to the mucosa rather than penetrating the full bowel wall as in Crohn's disease. The pathogenesis is multifactorial — genetically susceptible hosts (over 200 risk loci identified, with NOD2 less prominent than in Crohn's) develop dysregulated mucosal immunity against the gut microbiome, driven by Th2 and Th9 pathways and a leaky epithelial barrier. Disease extent is described by the Montreal classification as proctitis (E1, rectum only), left-sided colitis (E2, up to the splenic flexure), or extensive colitis / pancolitis (E3, beyond the splenic flexure), and severity is graded by Mayo score, UCEIS endoscopic score, or the Truelove-Witts criteria for acute severe disease.
The key symptoms of Ulcerative Colitis are: Bloody diarrhea, often with visible red blood mixed into stool or coating it, persisting for weeks rather than days and present in roughly 90% of patients at presentation., Urgent need to defecate (urgency), with little warning between the urge and the need to reach a toilet, frequently disrupting work, travel, and sleep., Tenesmus — a painful, persistent sensation of incomplete rectal emptying with straining even after passing stool, especially prominent in proctitis., Increased stool frequency, ranging from 4-6 loose stools daily in moderate disease to more than 10 stools per day with overt blood in severe flares., Mucus or pus discharge per rectum, sometimes passed alone without stool, reflecting active rectal inflammation., Lower abdominal cramping pain that improves transiently after passing stool, typically localized to the left lower quadrant in left-sided disease., Nocturnal bowel movements that wake the patient from sleep — a useful clinical clue that separates inflammatory diarrhea from functional disorders like irritable bowel syndrome..
Diagnosis of ulcerative colitis rests on a combination of clinical history, biochemical evidence of inflammation, stool studies that exclude infection, ileocolonoscopy with segmental biopsies, and supportive imaging. The 2019 ACG guideline (Rubin et al.) recommends starting with a thorough history covering stool frequency, blood, urgency, nocturnal symptoms, extraintestinal manifestations, NSAID use, and travel or antibiotic exposure. Initial laboratory work-up includes complete blood count, C-reactive protein, ESR, albumin, ferritin, and liver function tests — looking for anemia, hypoalbuminemia, and inflammatory signal. Stool studies are mandatory before treatment: stool culture, ova and parasites, and C. difficile PCR to exclude infectious colitis that can mimic or coexist with UC. Fecal calprotectin above 150-250 µg/g supports active mucosal inflammation and helps distinguish IBD from irritable bowel syndrome with high accuracy. The definitive diagnostic test is ileocolonoscopy with biopsies from each colonic segment plus the terminal ileum. UC shows continuous mucosal inflammation starting in the rectum and extending proximally with a clear demarcation, normal terminal ileum (except for occasional backwash ileitis in pancolitis), and histology demonstrating crypt distortion, crypt abscesses, basal plasmacytosis, and goblet cell depletion confined to the mucosa. Disease activity is scored using the Mayo endoscopic subscore (0 normal, 1 mild, 2 moderate, 3 severe) or the UCEIS. CT or MR enterography are reserved for distinguishing UC from Crohn's disease when small-bowel involvement is suspected. Flexible sigmoidoscopy without bowel preparation is preferred over full colonoscopy in suspected acute severe colitis to reduce perforation risk.
With consistent treat-to-target management, modern outcomes for ulcerative colitis are markedly better than a generation ago. About 50% of patients achieve sustained steroid-free remission on first-line 5-ASA, and most of the remainder reach durable remission on a biologic, JAK inhibitor, or S1P modulator. Lifetime colectomy rates have fallen from over 30% in the pre-biologic era to roughly 10-15% in contemporary cohorts. Endoscopic and histologic healing, once achieved, predicts the longest flare-free intervals and the lowest cumulative colorectal cancer risk. Cancer risk rises after eight years of disease and accumulates by roughly 1% per year of duration after the first decade in patients with extensive disease, but is sharply reduced by adherent maintenance therapy and structured surveillance. Patients with primary sclerosing cholangitis carry the highest cancer risk and need annual colonoscopy. Overall life expectancy in well-managed UC is close to that of the general population, and most patients work, parent, and travel without significant restriction.
A gastroenterologist should lead care from the point of initial diagnostic colonoscopy onward. Specialist input is essential for confirming UC versus Crohn's, choosing between 5-ASA and advanced therapy, managing treatment failures, running inpatient care for acute severe colitis, coordinating colorectal surgery, and overseeing long-term dysplasia surveillance. Hepatology, rheumatology, dermatology, and ophthalmology are added when extraintestinal manifestations occur.
Find specialists →Mild flares typically settle over 2-4 weeks with topical or oral 5-ASA. Moderate flares treated with oral steroids show meaningful symptom improvement within 5-7 days, with steroids tapered over 6-8 weeks. Biologic and small-molecule induction works on different schedules: JAK inhibitors and S1P modulators show response within 1-2 weeks; anti-TNF and ustekinumab over 4-8 weeks; vedolizumab and IL-23 agents over 8-14 weeks. Acute severe ulcerative colitis admitted to hospital typically responds to IV steroids within 3 days; non-responders are escalated to infliximab or cyclosporine at day 3-5 with response assessed within 5-7 days. After J-pouch surgery, full pouch adaptation takes 6-12 months, during which stool frequency gradually falls from 10-15 to 4-6 per day.
Regular moderate aerobic exercise — 30 minutes most days — is safe and beneficial in stable UC, reducing fatigue and improving quality of life. During an acute flare, rest as needed and resume activity gradually as bowel symptoms settle. Resistance training helps offset steroid-related muscle loss and bone density decline. Avoid high-intensity training during severe flares due to dehydration and electrolyte risk.
Look for a board-certified gastroenterologist with experience in inflammatory bowel disease — ideally one practicing within an IBD-focused unit with infusion capacity, on-site advanced endoscopy, dedicated IBD nursing, and rapid access to a colorectal surgeon experienced in pouch surgery. Ask whether the practice uses treat-to-target follow-up with endoscopy and calprotectin, and how rapidly they can admit patients in a flare. Continuity matters — UC is a multi-decade relationship.
Medically reviewed by AIHealz Medical Editorial Board · May 12, 2026
Ranked by patient outcomes and specialized experience.
Verifying top specialists in Colombia.
Apply as specialist →Specialists who treat Ulcerative Colitis. Get expert guidance and personalized care.