SOAP. – Ulcerative Colitis – SỔ TAY LÂM SÀNG

Ulcerative Colitis

Jill C. Cash and Cheryl A. Glass

Definition

A.Ulcerative colitis (UC) is one of the two inflammatory bowel diseases (IBDs), along with Crohn’s disease (CD). UC is limited to the colon; it extends proximally from the anal verge in an uninterrupted pattern to a part of or the entire colon. Extracolonic manifestations also include uveitis, pyoderma gangrenosum, pleuritis erythema nodosum, ankylosing spondylitis, and spondyloarthropathies. Refer to Table 14.27 for the definition of severity of UC.

B.Neither UC nor CD should be confused with irritable bowel Disease (IBD) , which affects the motility of the colon. Smoking is negatively associated with UC; the relationship is reversed in CD. The general course of UC is intermittent exacerbations and remissions. In severe cases, surgery may be required. The choice of treatment depends on disease activity and extent of pathology, patient acceptability, and mode of drug delivery.

TABLE 14.27 Definition of Severity of Ulcerative Colitis

Mild UC	•≤4 bloody stools/d with or without blood •No systemic toxicity •Normal ESR •Mild abdominal pain or cramping
Moderate UC	•> 4 bloody stools/d •No signs of systemic toxicity •Pulse < 90 beats/min •Temperature < 37.5° C (99.5° F) •Hemoglobin > 10.5 g/dL •ESR < 30 mm/hr •Moderate abdominal pain
Acute Severe UCa	•≥6 bloody stools/d or observable massive and significant blood BM AND •1 or more symptoms of systemic toxicity •Tachycardia > 90 beats/min •Temperature > 37.8° C (100.4° F) •Hemoglobin < 10.5 g/dL •Increased ESR (>30 mm/hr)
Fulminant UC	•>10 stools/d •Continuous rectal bleeding •Systemic toxicity •Tachycardia > 90 beats/min •Fever > 37.8°C (100.4°F) •Anemia requiring blood transfusions •Abdominal tenderness and distension •Colonic dilation on radiography •May lead to toxic megacolon or colonic perforation

a Acute severe colitis is defined by Truelove and Witts Criteria (1955).

ESR, erythrocytic sedimentation rate; UC, Ulcerative colitis.

Source: Adapted from Truelove, S. C. & Witts, L. J. (1955). Cortisone in ulcerative colitis; final report on a therapeutic trial. British Medical Journal 2(4947), 1041–1048.

C.Histologically, most of the pathology of UC is limited to the mucosa and submucosa. The severity of UC is defined by the following:

1.Pan-ulcerative (total colitis): Extensive disease with evidence of UC proximal to the splenic flexure. Massive dilation of the colon (toxic megacolon) may lead to bowel perforation.

2.Left-sided disease: Continuous UC that is present from the rectum, the descending colon up to, but not proximal to, the splenic flexure

3.Proctosigmoiditis: Disease is limited to the rectum and sigmoid colon involvement.

4.Ulcerative proctitis: Disease is limited to the rectum—usually less than the full rectum.

D.In 2015, the Toronto Consensus Clinical Practice Guidelines for the Management of Nonhospitalized UC published 34 recommendations, including statements on 5-aminosalicylates (5-ASA) corticosteroids, immunosuppressants, anti-tumor necrosis factor (TNF) therapy, and other agents, including probiotics. The guidelines are available at www.gastrojournal.org/article/S0016-5085(15)00303-0/abstract.

E.The 2015 Toronto Consensus guideline defined remission and response with UC as:

1.Complete remission: Both symptomatic remission and endoscopic healing defined as follows:

a.Endoscopic healing: Normal mucosa, vascular blurring, or chronic changes (e.g., inflammatory polyps, scarring) without friability.

b.Symptomatic remission: Normal stool frequency (≤3/d) and no blood in the stool.

2.Symptomatic response: Meaningful improvement in symptoms as judged by both the patient and physician in the absence of remission; response should not be considered a desirable final outcome but is useful to assess early response to treatment.

Incidence

A.The annual incidence of UC is 10.4 to 12 per 100,000, depending on the country.

B.UC is three times more common than CD.

C.The most common cause of death in patients with UC is toxic megacolon.

D.Adenocarcinoma of the colon develops in 3% to 5 % of patients with UC; the risk increases with the duration of the disease.

E.Approximately 6.2% of patients with IBD have a major extraintestinal manifestation..

1.Uveitis is the most common—3.8%.

2.Primary sclerosing cholangitis—3%.

3.Ankylosing spondylitis—2.7%.

4.Erythema nodosum—1.9%.

5.Pyoderma gangrenosum—1.2%.

Pathogenesis

A.Exact etiology is unknown.

B.UC may be considered an autoimmune disease. Persons with UC often have p-antineutrophil cytoplasmic antibodies (p-ANCAs). Abnormalities of humoral and cell-mediated immunity and/or generalized enhanced reactivity against intestinal bacterial antigen may also be causes of UC.

Predisposing Factors

A.Caucasian.

B.Jewish descent.

C.30% more females than males.

D.Genetic susceptibility (chromosomes 12 and 16).

Common Complaints

A.Frequent small-volume diarrhea.

B.Bloody diarrhea with or without mucus.

C.Severe bowel urgency.

D.Abdominal cramps and pain with bowel movement (BM).

E.Constipation.

F.Anorexia.

G.Anemia.

H.Nocturnal BMs.

Other Signs and Symptoms

A.Tenesmus (rectal urgency/constant feeling of need to pass stool).

B.Abdominal tenderness.

C.Arthralgias.

D.Fatigue secondary to anemia.

E.Severe UC:

1.Fever.

2.Tachycardia.

3.Significant abdominal tenderness.

4.Signs of volume depletion.

Subjective Data

A.Review the onset, duration, signs, and symptoms (number of stools, presence/absence of blood in the stool, fever, and abdominal pain).

B.Review the patient’s recent travel history or camping for the presence of intestinal infection.

C.Review the patient’s medication history, including antiboitics and nonsteroidal anti-inflammatory drugs (NSAIDs). One third of patients with exacerbation of UC report recent NSAID use.

D.Review family history for IBD, celiac disease, and colorectal cancer.

E.Review the patient’s smoking status.

F.Review the patient’s history or contact related to tuberculosis (TB; testing required prior to biologic therapy).

G.Evaluate if the patient has symptoms of uveitis including light sensitivity, floaters, blurry vision, or pain/tenderness to touch.

Physical Examination

A.Check temperature (if indicated), pulse, and blood pressure. Measure height and weight to calculate body mass index (BMI). Follow serial weights.

B.Inspection:

1.Observe the general overall appearance for nutritional status, cachexia, and pallor.

2.Observe the perianal region for the presence of tags, fissures, fistulas, and abscess.

3.Observe the abdomen for distension and presence of surgical scars.

4.Eye examination for redness, irritation, and ocular complications (episcleritis, scleritis, and uveitis).

5.Evaluate for the presence of dermatological findings, including erythema nodosum and pyoderma gangrenosum.

C.Auscultation:

1.Auscultate the heart and lungs.

2.Auscultate all four quadrants of the abdomen.

D.Palpation:

1.Palpate all four quadrants of the abdomen, observing for tenderness, rebound, and guarding.

2.Evaluate the presence of hepatomegaly.

3.Evaluate the joints for tenderness, warmth, swelling, and effusion.

4.Perform digital rectal examination to assess for anal strictures and rectal masses.

Diagnostic Tests

A.Diagnosis is best made with endoscopy and biopsy.

B.Laboratory tests:

1.Complete blood count (CBC) with electrolytes.

2.Platelet count.

3.Erythrocyte sedimentation rate (ESR).

4.C-reactive protein (CRP).

5.Cytomegalovirus (CMV): chronic immunosuppressive steroids.

6.HIV.

C.Stool testing:

1.Evaluate bacterial, viral, or parasitic causes of diarrhea.

2.Occult blood.

3.Fecal leukocytes.

D.Plain abdominal radiograph.

E.CT scan.

F.MRI.

G.Ultrasound.

H.Double-contrast barium enema.

I.Celiac antibody testing should be considered.

J.Intestinal TB testing should be considered.

Differential Diagnoses

A.UC.

B.Ischemic colitis (especially in the elderly).

C.Toxic megacolon.

D.Colon cancer.

E.Adenocarcinoma.

F.Rectal cancer.

G.Radiation colitis.

H.Intestinal infections.

I.Intestinal lymphoma.

J.Chronic diverticulitis.

K.Amebiasis.

Plan

A.General interventions:

1.Severe UC should be managed jointly by a gastroenterologist in conjunction with a colorectal surgeon.

2.Stress reduction and stress management may improve symptoms.

3.Pretreatment screening for TB, using Mantoux (a PPD) skin testing, is needed before initiation of immunomodulators and thiopurines.

4.Immunization status:

a.Immunizations with inactivated vaccine should be brought up to date and rigorously maintained during treatment, including influenza, meningococcus, and pneumococcus.

b.Check varicella titers prior to treatment with immunomodulators and reimmunize if titers are low.

c.The risk of administering live vaccines (polio, rubella, and yellow fever) to patients on immunomodulators has not been established; however, most experts avoid live vaccines during treatment.

B. See Section III: Patient Teaching Guide Crohn’s Disease and Ulcerative Colitis.

C.Dietary management:

1.Adequate nutrition is critical to promotion of healing. Sufficient protein and calories limit the stress on an inflamed bowel.

2.Many patients with UC have concurrent lactose intolerance (see Appendix B for lactose-intolerance dietary recommendations).

3.Decrease dietary fiber during increased disease activity.

4.Low-residue diet may decrease the frequency of BMs.

5.High-residue diet may be helpful in ulcerative proctitis when constipation is the dominant symptom.

6.Vitamin and nutritional supplements may be recommended.

D.See Section III: Patient Teaching Guide Nicotine Dependence.

E.Pharmacologic treatment. Refer to the American College of Gastroenterology Practice Guidelines for full treatment algorithms at http://s3.gi.org/physicians/guidelines/UlcerativeColitis.pdf or the 2015 Toronto Consensus Guidelines for the Management of UC algorithms:

1.The choice of topical agents is guided by the proximal distribution of UC into the bowel, as well as patient preference (see Table 14.28).

2.Refer to Table 14.6 for a stepwise medication approach for both of the inflammatory bowel diseases (IBDs).

The aminosalicylates (5-ASA) class of anti-inflammatory drugs is the most common treatment for patients with mild (<4 bloody stools per day) or moderate active disease (>4 bloody stools a day without systemic toxicity).

a.Sulfasalazine (azulfidine) for mild to moderate UC and remission maintenance:

i.Pediatrics: 50 to 75 mg/kg each 24 hours, divided into three to four doses.

ii.Reduced absorption of folic acid and digoxin has been reported when administered with sulfasalazine.

b.Balsalazide (Colazal) for mild to moderate UC and remission maintenance:

i.Induction: 6.75 g/d, given three times daily dosing.

TABLE 14.28 Management of Mild to Moderate Distal Ulcerative Colitis With Topical Agents

Topical agent	Proximal extent/distribution of agent
Suppository	10 cm
Hydrocortisone foam	15–20 cm
Enema	As far as the splenic flexure

Source: Adapted from the AGA Ulcerative Colitis in Adults Practice Guidelines (2010).

ii.Maintenance: 2 to 6.75 g/d, given twice a day dosing.

3.Mesalamine for mild to moderate UC and remission maintenance.

Asacol:

c.i.Two Asacol 400 mg tablets are not interchangeable or substitutable with one mesalamine delayed-release 800 mg tablet.

d.Apriso: 1.5 mg/d orally in the morning.

Salofalk: 1 to 4 g/d in one or two divided doses:

e.i.Also available as a suppository, rectal suspension, and enema.

f.Pentasa: 1 g/d orally four times a day dosing for up to 8 weeks:

i.Also available in a suppository.

g.Multi-Matrix System (MMX) marketed as Lialda: Active to moderate UC:

i.Induction: 2.4 to 4.8 g/d for up to 8 weeks.

ii.Maintenance: 2.4 g/d.

h.Rowasa enema: 4 g/60 mL rectally at bedtime; retain for approximately 8 hours.

i.Mesalamine (Canasa) suppository 1 g/d at bed-time; retain in the rectum for at least 1 to 3 hours. Treat active proctitis for 3 to 6 weeks.

4.Corticosteroids suppress the immune system and are used for moderate to severe UC:

Prednisone (Deltasone, Orasone):

a.i.Induction: 40 to 60 mg/d by mouth for 7 to 14 days followed by gradual taper by 5 mg/wk.

ii.Maintenance: 2.5 to 5 mg/wk.

5.Immune modifiers are used to decrease corticosteroid dosage:

aAzathioprine (AZA; Imuran) 2 to 3 mg/kg/d orally:

i.Monitoring includes: CBC, including platelet counts weekly during the first month, twice monthly for the second and third months of therapy, then monthly or more frequently if dosage alteration is necessary.

ii.Thiopurine methyltransferase (TPMT) testing: Testing is recommended for consideration to be given to either genotype or phenotype patients for TPMT.

b.6-Mercaptopurine (6-MP; Purinethol) 1 to 1.5 mg/kg/d orally

i.Patients with little or no inherited TPMT activity are at increased risk for severe Purinethol toxicity and generally require substantial dose reduction.

Antibiotics

6.1.Cyclosporine (Neoral, Sandimmune)

a.Intravenous (IV) infusion: 2 to 4 mg/kg/d

b.Can be switched to a doubled oral dose for out-patient therapy

2.Ciprofloxacin (Cipro) 500 mg orally twice a day

3.Metronidazole (Flagyl)

7.Biologic therapy (anti-tumor necrosis factor [TNF] agents) for moderate to severe UC: A tuberculin skin test is recommended prior to therapy. Patients started on Infliximab should also be screened for hepatitis B before initiating therapy:

1.Infliximab (Remicade) infusion therapy has a half-life of approximately 10 days.

2.Adalimumab (Humira) for the treatment of moderate to severe UC.

3.Golimumab (Simponi):

a.Initial dosage is 200 mg subcutaneously at week 0.

b.Second dose (week 2): 100 mg.

c.Maintenance dose: 100 mg every 4 weeks.

4.Vedolizumab (ENTYVIO):

a.Initial dose: 300 mg IV at weeks 0, 2, and 6.

b.Maintenance dose: 300 mg IV every 8 weeks of therapy.

c.Discontinue if no evidence of therapeutic benefit by week 14.

F.Indications for consideration of a total colectomy:

1.Failed medical therapy: Refractory UC.

2.Severe hemorrhage.

3.Fulminate colitis not responsive to treatment.

4.Toxic megacolon.

5.Obstruction or stricture.

G.Indications for consideration for elective surgery:

1.Long-term steroid dependence.

2.Dysplasia or adenocarcinoma found on screening biopsy.

3.Disease present 7 to 10 years.

Follow-Up

A.Screening colonoscopy are recommended for all patients with UC for 8 to 10 years after the onset of symptoms due to the increase in colonic neoplasia.

B.Patients with extensive UC or left-sided colitis with negative findings on the screening colonoscopy should begin surveillance colonoscopy in 1 to 2 years.

C.Steroids should not be used as maintenance therapy. Patients who require long-term steroids are at increased risk of osteoporosis.

D.Subsequent laboratory monitoring tests are dependent on the prescribed therapy.

E.Anxiety and depression are higher in patients with IBD. Screen for depression at each visit.

Emergent Issues/Instructions

Patients with ocular complications require an urgent consultation.

Consultation/Referral

A.Gastroenterologist for confirmatory diagnosis with a colonoscopy.

B.Consultation with a surgeon for severe or fulminant colitis. Toxic megacolon is a life-threatening complication and requires urgent surgical intervention.

C.Patients who have had UC for 8 to 10 years are at risk for colon cancer; therefore, colonoscopy for surveillance is recommended.

Individual Considerations

A.Adults:

1.Live vaccinations should not be administered to immunocompromised patients. If required, vaccines should be administered at the time of UC diagnosis:

a.The flu and pneumonia should be routinely administered.

b.Consider administering the human papillomavirus vaccine.

2.Women with IBD have been reported to have a high incidence of abnormal Pap smears. Adherence to Pap smear guidelines (refer Chapter 2).

3.Abnormal sperm counts, motility, and morphology are seen with sulfasalazine.

B.Geriatrics

1.Due to polypharmacy a full review of medications, herbals, and over-the-counter (OTC) drugs should be undertaken to identify mediations that should be avoided in the geriatric population, duplicate medications, and medications that are able to be to be decreased or deprescribed (refer Chapter 3 Section Deprescribing).

2.For the older adult with existing UC, nurse practitioner (NPs) should practice special consideration of the following geriatric syndromes:

a.Delirium is a common early sign of acute illness or infection in the elderly. It is more common in patients with existing cognitive impairment. At a minimum, patients and family should be asked if the patient has experienced episodes of altered mental status:

i.The Brief Confusion Assessment Method (bCAM) is a well-documented assessment for delirium. The bCAM is available at www.mnhospitals.org/Portals/0/Documents/ptsafety/LEAPT%20Delirium/HELP%20Program%20CAM%20Flowsheet.pdf.

b.Pain-Poorly relieved pain is an important cause of functional impairment at any age group:

i.The elderly patients have a diminished sensorium, allowing pathology to advance to a dangerous point prior to symptom development.

ii.The elderly with abdominal pain may present with altered mental status. Cognitive impairment can make assessment and diagnosis of pain more difficult.

For dementia or noncommunicative patients: The American Medical Directors Association has endorsed the Pain Assessment in Advanced Dementia (PAINAD) scores the following items:

•Breathing: Examples include normal, labored, hyperventilation.

•Negative vocalization: Examples include moaning, negative language, crying.

•Facial expression: Examples include smiling, frowning, grimacing.

•Body language: Examples include relaxed, tense, rigid, or striking out.

•Consolability: Examples include extent to which a caregiver is able to console, distract, or reassure.

c.Weight loss/appetite suppression-Weight loss is a predictor of mortality. Clinically significant weight loss is considered to be 5% loss of usual body weight in 3 months or 10% in 6 months.

3.Monitor weight patterns/BMI (Caution: BMI is not used to identify loss of muscle mass).

4.Monitoring both serum albumin and anemia: hypoalbuminemia and anemia is not necessarily associated with low bodyweight. It can be caused by decreases in liver protein synthesis:

i.Serum albumin concentration is commonly recommended.

ii.Hemoglobin, prealbumin, and transferrin.

iii.Cholesterol.

iv.Depression-anxiety and depression are common in IBD and are factors that lead to decreased health-related quality of life. A depression screen should be done at each office visit:

a.An on-line Patient Health Questionnaire-9 (PHQ-9) is available at https://www.mdcalc.com/phq-9-patient-health-questionnaire-9.

b.The Geriatric depression scale, short form, a 15-item questionnaire that can be quickly applied in the clinical setting is available at https://web.stanford.edu/yesavage/GDS.english.short.html.

Resources

American College of Gastroenterology (ACG): http://gi.org

Crohn’s and Colitis Foundation of America (CCFA): www.ccfa.org