Drug Effects on the Hypothalamic Pituitary Axis

Question 1

Where is growth hormone released from?

Answer 1

Anterior pituitary

Question 2

What is growth hormone released in response to?

Answer 2

GHRH and Ghrelin signals from the hypothalamus

Question 3

What does Ghrelin play a role in peripherally?

Answer 3

Appetite

Question 4

What does growth hormone stimulate?

Answer 4

Liver to synthesise and release IGF-1

Question 5

What do IGF-1 and somatostatin do in the blood?

Answer 5

Act as a negative feedback loop to the pituitary, inhibiting GH release

Question 6

Where are the 3 different places growth hormone release can go wrong?

Answer 6

1. Growth hormone insensitivity: GH doesn’t work – won’t stimulate release of IGF-1
2. Secondary deficiency: pituitary doesn’t produce GH
3. Tertiary deficiency: no release of GH because hypothalamus doesn’t release Ghrelin or GHRH

Question 7

What happens to GH levels in growth hormone insensitivity?

Answer 7

Levels are elevated because IGF-1 isn’t released, inhibiting GH release.

Question 8

What is growth hormone also known as?

Answer 8

Somatotropin

Question 9

Why can’t growth hormone supplement be administered orally?

Answer 9

Because there is zero bioavailability after oral adminstration - it is broken down and digested.

Question 10

How is growth hormone administed?

Answer 10

By injections, multiple times a day because of its short half-life.

Question 11

What is common among HRT therapies?

Answer 11

Titrating the dose until effect is seen.

Question 12

What can GH cause a reduced level of?

Answer 12

Thyroxine (T₄)

Question 13

What role does Ghrelin play in GH release?

Answer 13

Ghrelin receptor elevates Ca²⁺ and the GHRH receptor elevates cAMP, acting synergistically.

Question 14

When is IGF-1 administered?

Answer 14

In patients with GH insensitivity (e.g. Laron dwarfism) and patients with anti-GH antibodies.

Question 15

What happens if there’s not enough growth hormone?

Answer 15

Stunted growth

Question 16

What happens if there’s too much growth hormone?

Answer 16

Depending on what time in development, e.g. acromegaly (often caused by GH-releasing tumour)

Question 17

What are the treatment options for too much growth hormone?

Answer 17

• Remove tumor (if relevant)
• Reduce GH release
• Inhibit GH action

Question 18

Which therapeutics can reduce GH release?

Answer 18

Somatostatin analogues and dopamine agonists (can stimulate a reduction in GH release from pituitary)

Question 19

How can GH action be inhibited?

Answer 19

Pegvisomant - GH antagonist

Question 20

How can neuroendocrine tumours be imaged?

Answer 20

• Somatostatin receptors internalise upon activation (like many GPCRs), taking the tagged peptide ligand with them
• Tumors expressing somatostatin receptors can be imaged by in vivo receptor scintigraphy

Question 21

Do tumour cells expressing receptors for somatostatin respond to somatotatin?

Answer 21

Yes - they reduce secretion of GH

Question 22

Why does somatostatin only work for a short period of time?

Answer 22

Because it has a short half-life, undergoes enzymatic cleavage and renal elimination

Question 23

How can somatostatin be modified to extend its half-life?

Answer 23

Modify it by adding D amino acids - humans can’t cleave D amino acids, giving octreotide and lanreotide.

Question 24

How do you get Pegmisovant?

Answer 24

Turn GH into an antagonist and improve its pharmacokinetics and dynamics.

Question 25

What type of a receptor does GH bind to?

Answer 25

Tyrosine kinase receptor

Question 26

What happens when GH binds to its receptor?

Answer 26

The tyrosine kinase receptor dimerises, with the binding sites on both GH receptor monomers binding to GH.

Question 27

What is G120K-GH?

Answer 27

A GH receptor antagonist that binds one GH receptor monomer but blocks dimerisation by filling the second monomers cleft with lysine.

Question 28

Why does G120K need to be PEGylated?

Answer 28

Because it still has a short half-life, like GH.

Question 29

What is PEGylation?

Answer 29

Conjugation of the bioactive (e.g. G120K-GH) molecule with PEG polymer chains.

Question 30

What does PEGylation achieve?

Answer 30

• Increase in molecule size, reducing renal filtration.
• PEG is hydrophilic, improving solubility.
• Decreased proteolytic enzmyme accessibility

Question 31

What is one disadvantage to PEGylation?

Answer 31

Some activity is lost because the PEG polymer chains get in the way.

Question 32

Where on the bioactive molecule does PEGylation occur? Why is this a problem from G120K-GH? How is it overcome?

Answer 32

• At lysines - there are 2 lysines involved in site 1 binding, making G120K-GH completely inactive!
• Overcome by further mutations (B2036), resulting in an antagonist with good affinity by short half-life.

Question 33

What is trade off for in vivo efficacy if pegvisomant?

Answer 33

Pharmacodynamics (decreased affinity) for pharmacokinetics (increased exposure).

Question 34

How is thyroid hormone stimulated to be released from the thyroid gland?

Answer 34

Thyrotropin-releasing hormone (TRH) from hypothalamus stimulates anterior pituitary to release thyroid stimulating hormone (TSH) which then stimulates thyroid gland to release thyroid hormone to target tissues.

Question 35

What inhibits releases of thyrotropin-releasing hormone (TRH) and thyroid stimulating hormone (TSH)?

Answer 35

Thyroid hormone released from thyroid gland.

Question 36

What is Grave’s disease?

Answer 36

Hyperthyroidism: Stimulatory autoantibodies against the thyroid gland stimulate synthesis and increase release of thyroid hormone, resulting in higher levels of thyroid hormone but also decreased levels of TRH and TSH.

Question 37

What is Hashimoto’s disease?

Answer 37

Hypothyroidism: Destructive antibodies against the thyroid gland leads to decreased release of thyroid hormone and resultant increase in levels of TRH and TSH (due to lack of thyroid hormone)

Question 38

How is thyroid hormone stimulated?

Answer 38

1. Follicular cell synthesises enzymes and thyroglobulin for colloid.
2. A Na⁺-I^- symporter brings I^- into the cell. The pendrin transporter moves I^- into the colloid.
3. Enzymes add iodine to tyrosine on thyroglobulin to make T₃ and T₄
4. Thyroglobulin is taken back into the cell in vesicles.
5. Intracellular enzymes separate T₃ and T₄ from the protein.
6. Free T₃ and T₄ enter the circulation.

Question 39

What is the transient effect of iodide in hyperthyroid conditions?

Answer 39

Reduces hormone synthesis and release.

Question 40

What can be used to ablate the thyroid gland in hyperthyroidism?

Answer 40

Radioactive ¹³¹I^-.

Question 41

What protects the thyroid gland against radioactive isotopes?

Answer 41

Stable isotopes.

Question 42

Which 2 drugs are used to treat hyperthyroidism (Grave’s disease)?

Answer 42

Carbimazole and propylthiouracil.

Question 43

What is the action of carbimazole?

Answer 43

Inhibits thyroid peroxidase.

Question 44

What is the action of propylthiouracil?

Answer 44

Inhibits thyroid peroxidase and conversion T₄ and T₃

Question 45

What are the potential side effects of thioamines?

Answer 45

Goitre

Agranulocytosis

Hepatotoxicity

Question 46

Why should baseline liver function be tested if a patient is on propylthiouracil?

Answer 46

Because it causes hepatotoxicity.

Question 47

What does the amount of drug in the circulation depend on?

Answer 47

Affinity and the relative circulation of drug and protein.

Question 48

What is the general binding protein of the circulation?

Answer 48

Albumin

Question 49

What is the binding protein for thyroxine?

Answer 49

Thyroxine binding globulin

Question 50

What are the treatments for Hashimoto’s disease?

Answer 50

Thyroxine (T₄) and Liothyronine (T₃)

Question 51

When is thyroxine treatment of Hashimoto’s disease most active?

Answer 51

When thyroxine (T₄) is converted into T₃.

Question 52

What is the half-life of thyroxine?

Answer 52

7 days

Question 53

What is more active in the treatment of Hashimoto’s disease than T4?

Answer 53

T₃ - Liothyronine

Question 54

What are the disadvantages of liothyronine (T3) in the treatment of Hashimoto’s disease?

Answer 54

• Less strongly protein-bound than T₄
• Half-life of about 1 day
• Levels are less stable during the day than those of T₄ - TSH levels less easily interpreted.

Question 55

What should be used to treat most patients with Hashimoto’s disease?

Answer 55

T₄

Question 56

When should T3 be used to treat Hashimoto’s disease?

Answer 56

When there’s severe hypothyroid and myxoedoema coma.

Question 57

What is the interplay between cortisol and T3?

Answer 57

Cortisol inhibits conversion of T₄ to T₃.

T₃ inhibits cortisol production.