Intro to IBS - Stein Flashcards

1
Q

Describe and contrast the epidemiologies of Ulcerative Colitis and Crohn’s disease.

A

Both are “western” diseases with high prevalence in North America and Western Europe.

About 1mil cases in the US; half UC, half CD.

Note: Most cases are sporadic.

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2
Q

Between UC and CD, which feature:

Mouth-to-anus involvement?

Superficial inflammation?

Patchy areas of involvement?

A

Mouth-to-anus: Crohn’s disease.

Superficial: Ulcerative colitis

Patchy involvement: Crohn’s disease.

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3
Q

Compare and contrast the clinical presentations of UC and CD.

A

Both feature: Abdominal pain, weight loss (and growth stunting), fever, fatigue, urgency, and bloody diarrhea.

Ulcerative colitis often features tenesmus (eg passing of mucus)

Crohn’s may feature vomiting.

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4
Q

Describe the appearance of ulcerative colitis on endoscopy

A

Erythema, edema, and loss of the usual vascular pattern.

Granularity & friability of the mucosa.

Erosions, ulcers, and bleeding.

Pseudopolyps, cecal patch, and backwash ileitis (pan-colitis only)

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5
Q

What is the most severe variant of ulcerative colitis?

How common is it?

A

Fulminant UC; features systemic signs (fever, elevated WBC) and high risk of perforation.

About 9% of patients feature this on initial rpesentation. Can develop at any course of the disease…

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6
Q

Which parts of the GI tract are (USUALLY) affected by Crohn’s disease?

A

Usually both the small and large intestine are affected by CD. However, it can affect anywhere “mouth to anus”

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7
Q

What are the three “major” endoscopic findings in Crohn’s disease?

A

Aphthous ulcers, cobblestoning, discontinuous (“skip”) lesions.

(also seen: strictures, fistulae)

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8
Q

Do each of the following features hint at Crohn’s or UC more?

Rectal sparing

Loss of normal vasculature

Involvement of terminal ileum but not cecum

Granulomas on biopsy

A

Rectal sparing: CD

Loss of normal vasculature: UC

Involvement of terminal ileum but not cecum: CD

Granulomas on biopsy: CD

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9
Q

Try to recall 6-7 extra-intestinal manifestations of IBDs.

A

Acute arthropathy

Erythema Nodosum (and pyoderma gangrenosum)

Choledocholithiasis and nephrolithiasis

Ocular complications (scleritis, uveitis)

Sacroillitis and ankylosing spondylitis

Primary sclerosing cholangitis

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10
Q

Describe the pathogenesis of inflammatory bowel diseases. Broad strokes.

A

Defects at the GI lining (NOD2, Th17, tight junctions) as well as microbiota disturbances facilitate an exaggerated immune response.

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11
Q

What is the desired outcome of IBS?

What is the worst outcome?

A

Remission of symptoms (“patient feels fine”)

Development of penetrating fistulas.

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12
Q

What treatment options are available for IBD (categories, not specifics)

A

Steroids

Immunomodulators

“Biologics” (eg mAbs)

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13
Q

Name four biologic treatments of IBS and their mechanism of action.

A

Infliximab: Anti-TNF mAb

Certolizumab pegol: Anti-TNF Fab fragment

Adalimumab: Anti-TNF mAb

Natalizumab: Anti-a4 integrin mAb

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14
Q

Which of the four biologics is no longer indicated due to increased incidence of brain infections?

Why are biologics the best choice of treatment for those with IBS?

A

Natalizumab

Good efficacy (high rate of remissions and mucosal repair) and allows weaning of glucocorticoids.

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15
Q

(low-yield slide) What were the findings of each of the following Anti-TNF trials?

CHARM

PRECiSE

SONIC

A

CHARM: Adalimumab (anti-TNF antibody) improves remissions in IBD.

PRECiSE: Certolizumab pegol improves remissions in IBD.

SONIC: Infliximab (and azathioprine) improve remission & mucosal healing and work better if given early in the disease course.

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16
Q

Name two potential side effects of a standard IBS treament regimen.

A

Increased infections (mostly due to steroid effect)

Incrased risk of lymphoma (anti-TNF effect)

17
Q

What treatment exists for IBS patients refractory to anti-TNF therapy?

A

Surgical removal of the affected bowel. Generally a last resort…