Article Text
Statistics from Altmetric.com
Description
A 27-year-old woman presents with vomiting and abdominal pain for 2 days. She had been diagnosed with ulcerative colitis (UC) 2 weeks prior and was started on oral sulfasalazine and prednisolone. Currently, she is afebrile and not tachycardic. On examination, the abdomen was distended and tender centrally. Serial abdominal radiographs showed persistently dilated transverse colon with loss of haustra (figure 1). CT abdomen revealed diffuse bowel thickening involving the ascending colon, caecum and terminal ileum with multiple pseudopolyps at the ascending colon (figure 2). The transverse colon is dilated up to 6.8 cm (figure 3). There are also multiple enlarged right-sided mesenteric nodes. A diagnosis of toxic megacolon (TM) was made. She deteriorated during admission due to acute pulmonary embolism. Blood investigations showed marked leucocytosis (32×109/L) and raised C-reactive proteins (98.7 mg/L). Subtotal colectomy involving the caecum until splenic flexure was performed followed by ileostomy and mucous fistula. Her clinical symptoms improved remarkably following surgery and she was discharged well within a week.
TM is a potentially fatal complication of severe colitis. It is defined as a segmental or total colonic distension of >6 cm in the presence of acute colitis and signs of systemic toxicity. Although any cause of colitis increases the risk of TM, UC is the most associated predisposing factor. TM is present in up to 10% of all UC admission. In earlier reviews, mortality rates vary from 19% to 27% with up to fivefold increase in mortality rate in case of perforation.1 2 In 2018, however, Doshi et al found that all-cause in-hospital mortality was 7.9%.2 Up to 57% of those who undergo medical therapy will eventually require colectomy.1 3 Clostridium difficile is the most commonly associated infectious pathogen (76%) and its presence can further complicate TM.2 Unfortunately, stool culture and toxin assays were not performed for our patient.
Clinical features of TM are often preceded by signs and symptoms of colitis. Patients may experience bloatedness, abdominal distension and constipation—as such, antimotility medications are contraindicated. Blood results may show elevated leucocytosis and anaemia. Radiographically, the transverse colon is often dilated due to its anterosuperior position and a diameter of >6 cm is highly suspicious.1 ‘Thumbprinting sign’ may be present. CT findings will highlight the extent of involvement (colonic submucosal oedema, pseudopolyps, ahaustral pattern, dilatation), adjacent inflammation (mesenteric fat stranding) and other associated features (ascites, abscesses, small bowel involvement). Although CT findings facilitate further management, there are no specific features to suggest the underlying cause or clinical outcome of TM.3
Management is divided into supportive, medical and surgical therapy. Supportive care includes optimising fluid regime, bowel rest or decompression and discontinuation of aggravating drugs. Medical therapy is targeted at the underlying cause of TM—corticosteroids in UC, antibiotics in treating organism-induced TM to reduce mortality if perforation occurs. Absolute indications for surgery include perforations, uncontrollable bleeding and progressive dilatation. Surgical resections result in rapid clinical improvement, and as such is recommended by some experts to be performed as soon as diagnosis is made. Nevertheless, trial of medical therapy can be initiated first.1
Learning points
Diagnosis of toxic megacolon (TM) is made based on constellation of clinical, laboratory and imaging findings.
Any cause of colitis can lead to TM, but ulcerative colitis is often the culprit.
Medical therapy can be initiated but surgical resection must be performed if the patient is deteriorating or not showing signs of improvement.
Footnotes
Contributors SCLO and NM have contributed sufficiently to the project and have met all criteria to be included as authors.
Funding The authors have not declared a specific grant for this research from any funding agency in the public, commercial or not-for-profit sectors.
Competing interests None declared.
Patient consent Obtained.
Provenance and peer review Not commissioned; externally peer reviewed.