Inflammatory bowel disease

Question 1

What are the two major forms of IBD?

Answer 1

Ulcerative colitis (UC)
Crohn's disease (CD)

Question 2

In what percentage of patients is the distinction between UC and CD incomplete?

Answer 2

10%

Question 3

How many people in the UK currently have IBD?

Answer 3

300,000

Question 4

Why is CD more extensively studied?

Answer 4

It is more serious and difficult to treat

Question 5

What are the risk factors for IBD?

Answer 5

Genetic predispositions

Environmental factors which could include smoking and diet/obesity (it’s a disease of affluence)

Question 6

What is obesity a risk factor for?

Answer 6

CD but not UC

Question 7

What is the simple point of the disease’s pathogenesis?

Answer 7

Defective interaction between mucosal immune system and gut flora

Question 8

Explain the basic development of IBD?

Answer 8

Complex interplay between host and microbes
Disrupted innate immunity
Uncontrolled inflammation
Physical damage to epithelium and leakiness of tight junctions

Question 9

What mediates UC?

Answer 9

TH2

Question 10

What is UC dependent on?

Answer 10

Cytokines such as IL-5 and IL-13

Question 11

What does UC tend to affect?

Answer 11

Just mucosa and submucosa

Question 12

Where does UC always start?

Answer 12

It always starts in the rectum and spreads proximally- it’s always continuous

Question 13

How can you cure UC in worst case scenario?

Answer 13

Surgery- remove affected piece of bowel and it doesn’t reoccur

Question 14

What is CD mediated by?

Answer 14

TH1

Question 15

What is the main cytokine in CD?

Answer 15

TNF-alpha

Question 16

What is the effect of CD being TH1 mediated?

Answer 16

It causes a more severe inflammatory response

Question 17

What does CD affect?

Answer 17

It can penetrate all the way through the gut and can affect any point of GI tract from mouth to anus

Question 18

What is the main problem with CD?

Answer 18

It causes patchy inflammation which means you can’t remove affected area as easily as UC

Question 19

What happens if you cut out affected area in CD?

Answer 19

It is likely to reoccur

Question 20

What are you more likely to develop in CD than UC?

Answer 20

Abscesses, fissures and fistulae

Question 21

What is chrohn’s physically characterised by in terms of appearance?

Answer 21

Cobblestone appearance

Question 22

What is a fistula?

Answer 22

Abnormal or surgically made passage between a hollow tubular organ and body surface or between two hollow or tubular organs

Question 23

What are the clinical features of IBD?

Answer 23

Diarrhoea, blood, mucus
Weight loss
Skin rash
Right iliac fossa mass/pain
Primary sclerosing cholangitis
Aphthous ulcers
Anaemia, uveitis, fevers, sweats and jaundice
Abdominal pain
Arthritis arthralgia

Question 24

What does someone need if they have very bloody diarrhoea?

Answer 24

Fluid/electrolyte replacement
Blood transfusion/oral iron
Nutritional support

Question 25

How is IBD treated?

Answer 25

Symptomatically:
Glucocorticoids e.g. prednisolone
Aminosalicylates e.g. mesalazine
Immunosuppressives e.g. azathioprine

Question 26

What potentially curative therapies are there?

Answer 26

Manipulation of gut microbiome
Biological therapies:
Anti-TNF alpha e.g. infliximab
Anti alpha-4-integrin e.g. natalizumab

Question 27

How effective are aminosalicylates in UC and CD?

Answer 27

In UC:
First line inducing and maintaining remission
Good evidence base
Crohn’s disease:
Unsure effectiveness in active disease
May help maintain surgically induced remission
Less clear cut than utility in UC

Question 28

What is mesalazine?

Answer 28

5-aminosalicylic acid (5-ASA)

Question 29

What is olsalazine?

Answer 29

Slightly more complex molecules- consists of 2 linked 5-ASA molecules (no benefit compared to mesalazine)
Anti-inflammatory

Question 30

What is the mechanism of anti-inflammatory action?

Answer 30

Inhibition of:
-IL-1
-TNF-alpha
-Platelet activating factor (PAF)
Decreased antibody secretion
Non-specific cytokine inhibition
Reduced cell migration (macrophages)
Localised inhibition of immune responses

Question 31

What is anti-inflammatory action more effective in?

Answer 31

UC than CD which is weird as it seems to be targeting Th1 and UC is mainly governed by Th2 system

Question 32

What is the pharmacokinetics of 5-ASA derivatives? (mesalazine and olsalazine)

Answer 32

Mesalazine doesn’t need to be metabolised so is absorbed in small bowel and colon
Olsalazine is more complex and needs to be activated by colonic flora so is only absorbed in colon

Question 33

What is better between topical 5-ASA and topical steroids at inducing remission in UC?

Answer 33

Topical-5-ASA

Combined with steroids is even better

Question 34

Why is the use of glucocorticoids for UC in decline?

Answer 34

It has been shown that aminosalicylates are better than glucocorticoids ar doing the job

Question 35

How can glucocorticoids be used?

Answer 35

Topically (enema) or IV if severe

Question 36

What are the drugs of choice for inducing remission in Crohn’s?

Answer 36

Glucocorticoids but you’re likely to get side effects if they’re used to maintain remission

Question 37

Give some examples of glucocorticoids?

Answer 37

Prednisolone, fluticasone and budesonide

Question 38

What are glucocorticoids?

Answer 38

Powerful anti-inflammatory and immunosuppressive drugs derived from cortisol that activate intracellular glucocorticoid receptors which then act as positive or negative transcription factors

Question 39

What strategies are there for minimising side effects of glucocorticoids?

Answer 39

Topical administration- fluid or foam enemas
Low dose in combination with another drug
Oral or topically administered drug with high hepatic first pass metabolism e.g. budesonide- so relatively little active glucocorticoid escapes into systemic circulation

Question 40

How does budesonide compare to standard glucocorticoids?

Answer 40

Budesonide has fewer side effects but standard oral glucocorticoids are better at inducing remission in active Crohn’s disease and budesonide is a little better than placebo at preventing CD relapse

Question 41

How effective have immunosuppressive agents been at inducing remission in UC and CD?

Answer 41

A number of drugs have been tried but have not been successful

Question 42

Which immunosuppressive drugs have been tried ad how effective have they been?

Answer 42

Azathioprine has shown significant degree of success in UC and CD
Methotrexate has demonstrable efficacy in some IBD patients
Cyclosporin is useful only in severe UC

Question 43

What is azathioprine mainly used for?

Answer 43

Maintain remission in CD

Question 44

What is the onset of azathioprine like?

Answer 44

Slow- 3-4 months of treat required before clinical benefits seen which can be problematic as patients may relapse between starting treatment and seeing benefits

Question 45

How is azathioprine activated?

Answer 45

It is a pro-drug that is activated in vivo by gut flora to 6-mercaptopurine

Question 46

What is 6-mercaptopurine?

Answer 46

Purine antagonist so it interferes with DNA synthesis and cell remplication

Question 47

What does 6-mercaptopurine impair and enhance?

Answer 47

It impairs:
Cell and antibody mediated immune responses
Lymphocyte proliferation
Mononuclear cell infiltration
Synthesis of antibodies
It enhances:
T cell apoptosis

Question 48

What percentage of patients on azathioprine have to stop treatment because of side effects?

Answer 48

10%

Question 49

What unwanted effects is azathioprine associated with?

Answer 49

Pancreatitis
Bone marrow suppression
Hepatotoxicity
Increased risk (4 fold) of lymphoma and skin cancer

Question 50

How many routes of metabolism are there for azathioprine?

Answer 50

3

Question 51

Why don’t you want too much use of the metabolism of azathioprine pathway that involves HRPT?

Answer 51

It produces active metabolites that are beneficial but cause myelosuppression

Question 52

Why don’t you want too much use of the metabolism of azathioprine pathway that involves TPMT?

Answer 52

It will produce metabolites that aren’t beneficial and hepatotoxic

Question 53

Which pathway is preferred for azathioprine metabolism?

Answer 53

Xanthine oxidase- its metabolites are inert so won’t cause any problems

Question 54

What does allopurinol inhibit?

Answer 54

Xanthine oxidase

Question 55

What is allopurinol used to treat?

Answer 55

Gout

Question 56

What happens if the xanthine oxidase is inhibited?

Answer 56

You will shunt azathioprine through other pathways so patients need to be monitored to make sure they aren’t making too many toxic metabolites

Question 57

How effective is azathioprine at maintaining remission in CD?

Answer 57

Clear benefit over placebo

Question 58

How effective is methotrexate at maintaining remission in CD?

Answer 58

It has a demonstrable effect

Question 59

What does methotrexate do?

Answer 59

It is a folate antagonist which reduces the synthesis of thymidine and other purines

Question 60

Why is methotrexate not widely used?

Answer 60

There are significant unwanted side effects

Question 61

How effective are nutrition based therapies/probiotics at obtaining and maintaining remission in UC and CD?

Answer 61

No evidence for probiotics in CD

Evidence for probiotics in UC

Question 62

What is the rationale for Faecal microbiota replacement therapies (FMT)?

Answer 62

There is insufficient evidence for it but rational is gut flora is out of control and there are organisms that you don’t want there causing harm so wipe them out and replace them with good normal microbiota

Question 63

How does antibiotic treatment (rifaximin) have an effect on CD and UC?

Answer 63

It induces and sustains remission in moderate CD
It may be beneficial in UC
It interferes with bacterial transcription by binding to RNA polymerase and it reduces the amount of mRNA coding for inflammatory mediators in UC

Question 64

What biological therapies have been approved for use in IBD?

Answer 64

Anti-TNF-alpha antibodies:

• Infliximab (IV)
• Adalimumab (SC)

Question 65

How effective are anti-TNF alpha antibodies in treating CD?

Answer 65

They are used very effectively

Question 66

What percentage of patients will respond within 6 weeks to anti-TNF-alpha antibodies?

Answer 66

60% (potentially curative

Question 67

What does refractory disease mean?

Answer 67

It describes disease that doesn’t respond to attempted forms of treatment

Question 68

How effective are anti-TNF alpha antibodies in treating UC?

Answer 68

Some evidence of effectiveness which is surprising because TNF-alpha is a Th1 cytokine

Question 69

What is the mechanism of action of anti-TNF-alpha antibodies?

Answer 69

Anti-TNF alpha reduces activation of TNF-alpha receptors in the gut, TNF-alpha is right at the top of inflammatory cascade so you get general down regulation of other cytokines as well
It also reduces infiltration and activation of leukocytes
Also bind to membrane associated TNF-alpha
Induces cytolysis of cells expressing TNF-alpha
Promotes apoptosis of activated T cells

Question 70

What is the half life of infliximab like?

Answer 70

It has a very long half life of 9.5 days which means benefits can last for 30 weeks after a single infusion (most patients relapse after 8-12 weeks so there is a repeat infusion every 8 weeks)

Question 71

What is a big problem with anti-TNF-alpha antibodies?

Answer 71

There is emerging evidence showing that upto 50% of responders lose response within 3 years due to production of anti-drug antibodies and increased drug clearance

Question 72

What adverse effects of anti-TNF-alpha antibodies are there and what causes this?

Answer 72

All of these are consequences of knocking out the key cytokine in the inflammatory cascade:
4-5x increase in incidence of tuberculosis and other infections
Risk of reactivating dormant TB
Increased risk of septicaemia
Worsening of heart failure
Increased risk of demyelinating disease
Increased risk of malignancy
Immunogenic- azathioprine reduces risk but raises risk of TB/malignancy

Question 73

What was the SONIC study and what did it show?

Answer 73

It was a study on infliximab- 500 patients with CD were monitored for 30 weeks- it showed that early use of infliximab in patients with refractory disease is better than last resort. CRP levels and endoscopy might allow identification of patients that are most likely to benefit