Pharmacology of IBD

Question 1

what are the two major forms of IBD?

Answer 1

o Ulcerative colitis.
o Crohn’s disease
– most studied of the two as it is the worse one

when there is a fine boundary–> intermediate colitis

Question 2

what are the risk factors of IBD?

Answer 2

o Genetic predisposition
 – in 163 loci.
o Environmental factors 
– smoking (CD especially), diet/obesity, gut microbiome.
o Obesity
 – ONLY for CD and not for UC.

Question 3

what is the main pathogenesis of IBD?

Answer 3

defective interactions between the mucosal immune system and the gut flora.
disrupted innate immunity
uncontrolled inflammation and therefore physical damage

Question 4

how is the CD autoimmune disease mediated?

Answer 4

Th1 giving a worse inflammatory response
Dependant on TNF-a cytokine.

UC is Th2 mediated

Question 5

what mediates the UC autoimmune disease?

Answer 5

Th2

Dependant on IL-5 & IL-13 cytokines.

Question 6

how does CD and UC differ in layers of the gut they affect?

Answer 6

CD affects all layers of the gut

UC affects the mucosa/submucosa

Question 7

how does the inflamed area differ in CD and UC?

are abscesses found in them?

Answer 7

CD consists of patchy areas of inflammation with abscesses being common. This makes surgical removal very difficult (can then reoccur)

UC consists of continuous areas of inflammation where abscesses are not common and therefore easier to cure by surgery

Question 8

what are the clinical features of IBD? how are they categorised?

Answer 8

systemic and local

	Right iliac fossa pain.
	Skin rash.
	Diarrhoea, blood, mucus.
	Weight loss.
	Arthritis, arthralgia.
	Abdominal pain.
	Anaemia.

Question 9

what are the different therapies available for different stages of IBD?

Answer 9

1- supportive (acute cases)
2- classic symptomatic treatments (not curing the disease; at active state and prevention of remission)
3- (potentially) curative

Question 10

what are the 3 groups of drugs involved in classic symptomatic treatment?

Answer 10

o Glucocorticoids – e.g. prednisolone.
o Aminosalicylates – e.g. mesalazine.
o Immunosuppressives – e.g. azathioprine.

Question 11

what is provided in supportive therapy in acute cases?

Answer 11

o Fluid/electrolyte replacement.
o Blood transfusion or oral iron.
o Nutritional support – as malnutrition is common.

Question 12

what are the treatment options in the potentially curative treatment?

Answer 12

o	Manipulation of the microbiome.
o	Drugs
 - Anti-TNF-alpha  
(e.g. infliximab).
- Anti-a-4-integrins 
(e.g. natalizumab)

Question 13

what IBD is aminosalicylates preferred in?

Answer 13

Ulcerative colitis – first line in inducing and maintaining remission with a good evidence base. Given oraly and/or rectally (disease at rectum)

Crohn’s disease – non-effective in active disease but may help maintain surgically-induced remission.

Question 14

what is mesalazine?

Answer 14

5-aminosalicyclic acid / 5-ASA

e.g. Olsalazine (2 linked 5-ASA molecules)

an anti-inflammatory drug

Question 15

what is the mechanism of action of mesalazine?

Answer 15

o Inhibition of IL-1, TNF-a and PAF (Platelet Activating Factor).
o Decrease antibody secretion.
o Non-specific cytokine inhibition.
o Reduce cell migration – macrophages.
o Localised inhibition of immune responses.

nb PAF is for platelet aggregation, inflammatory and allergy

Question 16

where is mesalazine absorbed?

Answer 16

does not need to be metabolised and is absorbed by small bowel and colon

Question 17

what effect does mesalazine have in UC?

which form of mesalazine is ideal for this function ?

Answer 17

• maintaining remission in UC
• Topical 5-ASA is better than topical steroids in
• Combined topical 5-ASA and oral steroids better at inducing remission than oral 5-ASA alone

Question 18

where is olsalazine absorbed?

Answer 18

metabolised by gut flora and absorbed by the colon

Question 19

what are the glucocorticoids that can be used in symptomatic treatment?

Answer 19

Prednisolone
Fluticasone
Budesonide

Question 20

which IBD is glucocorticoid use preferred in?

Answer 20

Crohn’s disease
– drug of choice for inducing remission, SEs likely if used to maintain
remission.

Ulcerative colitis (not recommended)
– use is in decline, can be used topically or via IV.
5-ASA seems to be superior.

Question 21

what action do glucocorticoids have in treatment?

Answer 21

Powerful anti-inflammatory drug and immunosuppressives

Activate intra-cellular GC receptors to regulate transcription factors.

Question 22

what is the problem with long term use of glucocorticoids?

Answer 22

long-term use side effects: Cushing-like symptoms

• osteoporosis (fragile bones),
• hypertension (high blood pressure),
• diabetes,
• weight gain,
• increased vulnerability to infection,
• cataracts and glaucoma (eye disorders),
• thinning of the skin,
• bruising easily

Question 23

how should glucocorticoids be administered to limit its negative effects?

Answer 23

• Administer topically.
• Use a low-dose in combination with another drug (steroid-sparing agent)
• Use an oral/topical drug with HIGH first-pass metabolism so little can escape systemically

Question 24

which glucocorticoid option has high first pass metabolism and therefore a preferable glucocorticoid to use?

Answer 24

Budesonide (for mild cases)

has fewer SEs than Prednisolone as it stays in the gut and does not escape systemically

Question 25

which form of glucocorticoid are better than Budesonide at inducing remission in active Crohn’s disease?

Answer 25

oral GCs

Question 26

what are the immunosuppressives used in symptomatic treatment of IBD?

Answer 26

Azathioprine
Methotrexate
Cyclosporine

Question 27

how do CD and UC differ in the regions of the GIT they affect?

Answer 27

CD affects any part of the GIT

UC affects the rectum spreading proximally

Question 28

in which IBD can azathioprine be used?

Answer 28

in both CD and UC

o CD
- used to maintain remission
- superior to placebo & budesonide in CD.
o UC
- useful for maintaining remission in SOME patients.

Question 29

what type of drug is azathioprine? when can its effects be seen?

Answer 29

Immunosuppressive “steroid sparing” agent

Slow onset of action therefore 3-4 months’ treatment is required before clinical benefits are seen.

Question 30

how is azathioprine activated and what action does it have?

Answer 30

prodrug activated by gut flora into 6-mercaptopurine (6-MP)
[6-MP could be given directly]

this is a purine antagonist that interferes with DNA synthesis and cell replication

Question 31

what is methotrexate? why is it not used as much any more?

Answer 31

immunosuppressive

• folate antagonist
• reduces synthesis of thymidine and other purines
• efficacy in some IBD patients
• not widely used due to significant side effects

Question 32

in what IBD is cyclosporine used in?

Answer 32

UC

Question 33

what are the effects of azathioprine?

Answer 33

Impairs:

• humoral and innate immune responses
• lymphocyte proliferation
• mononuclear cell infiltration - synthesis of antibodies

promotes:
- T cell apoptosis

Question 34

what are the unwanted effects of azathioprine?

Answer 34

some metabolites have unwanted effects:

• Bone marrow suppression (6-TGN is myelosuppressive)
• Hepatotoxicity (6-MeMP)
• x4 risk increase of lymphoma and skin cancer
• Pancreatitis

Question 35

what are the 3 metabolism routes of 6-MP?

Answer 35

o HPRT – beneficial but causes myelosuppression.

o TPMT – hepatotoxic metabolites.

o XO – inert metabolites (IDEAL and MAIN pathway)
–> allopurinol (treats gout) inhibits XO and so blocks this pathway therefore don’t coadminister

Question 36

what is the preferred route of 6-MP metabolite metabolism?

Answer 36

Xanthine Oxidase

produces inert metabolites

Question 37

what are the 3 options that induce microbiome manipulation?

Answer 37

 Nutrition-based therapies i.e. probiotics

 Faecal microbiota replacement (FMT)
- insufficient evidence for FMT, it is not known whether change in microbiota is an effect or cause

 Antibiotic treatment (Rifaximin)

Question 38

which IBD is nutritional based therapy preferred in?

Answer 38

o UC
– evidence for probiotics in the induction and maintenance of remission, people respond differently

o CD
– no evidence for probiotics

Question 39

which IBD is antibiotic treatment preferred in?

Answer 39

o CD
– induces and sustains remission in moderate cases

o UC
– may be beneficial

Question 40

what effect do antibiotics have?

mechanism of action

Answer 40

e.g. rifixamin
Interferes with bacterial transcription by binding to RNA polymerase
– reduces mRNA coding by inflammatory mediators.

Question 41

how can delivery of a drug be altered?

Answer 41

• pH dependent
• time dependent polymer
• osmotic pressure control using push layer that sweeps and pushes drug out
• prodrug based conjugate

Question 42

what is nutritional therapy?

Answer 42

a liquid diet that rests the mucosa so the flora can recover

hard to maintain in adults (unpalatable)

Question 43

what are the Anti-TNF alpha drugs that can be used?

Answer 43

Infliximab (IV)
Adalimumab (SC).

these are monoclonal antibodies
these have fewer side effects

Question 44

which IBD are anti-TNF-alpha antibodies preferred in?

Answer 44

o CD
– used successfully, 60% responsive within 6 weeks, potentially curative.

o UC – some evidence of effectiveness
(but UC is not TNF-a mediated, it is mainly IL mediated)

Question 45

how does Infliximab affect TNF Alpha?

Answer 45

• binds to soluble TNF-a and receptor bound TNF-a
• it can strip away TNF-a bound onto cells
• reduces activation of TNF-a receptors in the gut

Question 46

why is anti TNF alpha not every effective in UC?

Answer 46

UC is not mediated by TNF alpha but rather by interleukins

UC is Th2 mediated i.e used IL
CD is Th1 mediated i.e. TNF a

Question 47

what is the effect of TNF-alpha inactivation? what overall effects does this have?

Answer 47

As TNF-a activates other cytokines, TNF-a inactivation downregulates other cytokines, and infiltration and activation of leukocytes.

• Induces cytolysis of cells expressing TNF-a.
• Promotes apoptosis of activated T-cells.

Question 48

what are the pharmacokinetic details of the anti-TNF-a drugs?

Answer 48

o Very long T1/2 – 9.5 days.
o Benefits last for 30 weeks after infusion.
o Patients relapse after 8-12 weeks (repeat infusion every 8 weeks).

Question 49

what is the problem with use of anti-TNF-a drugs over time?

Answer 49

patients lose response to drugs after 3 years due to increased metabolism & anti-drug ABs that have been created

Question 50

what is the root to all the adverse effects of biological therapies?

what are the adverse effects?

Answer 50

due to consequences of knocking out the key cytokine inflammatory cascades:

o 4-5x increase incidence of TB and other infections
– and risk of reactivating dormant TB.
o Increased risk of septicaemia
– downregulates inflammation.
o Worsening of heart failure.
o Increased risk of demyelinating disease and malignancy.
o Can be immunogenic
– Azathioprine reduces risk but raises TB/malignancy risk.

Question 51

when should infliximab be used?

Answer 51

Early use of infliximab in refractory disease is better than using it as a last resort

These patients at high risk should be identified with endoscopy and CRP levels

Question 52

what are some other targets that potential drugs can target?

Answer 52

 Alpha-4 Integrin
– cell adhesion molecule.

 IL-13
– particularly in UC as its Th2 mediated

 Janus kinases 1, 2, 3 
– block signalling by IL-2, 4, 9, 15, 21 
(lymphocyte activation and function) 
- block signalling by IL-6 and INF-gamma
(pro-inflammatory) 
– good in UC as its Th2 mediated

Question 53

what therapies can be used for CD?

Answer 53

• glucocorticoids
• azathioprine
• antibiotics
• Anti-TNF-a drugs

NOT
- aminosalicyclates etc

Question 54

what therapies can be used in UC?

Answer 54

• aminosalicylates
• azathioprine
• nutritional based therapies