IC16 PK of male endocrine drugs

Question 1

tamsulosin drug type

Answer 1

Reversible α-1 receptor antagonist

Question 2

tamsulosin MOA

Answer 2

• Reduces vasoconstriction induced by endogenous catecholamines
• Blocking of α-adrenoreceptors on smooth muscle of prostate, prostatic urethra & bladder neck → Relaxation of SM → increases max urinary flow rate ⇒ relieving obstruction
• Improves symptoms related to bladder instability & tension of SM of lower urinary tract

Question 3

tamsulosin MOA
selectivity

Answer 3

Greater for α1A; better blockade for α1A (prostate & BV) than α1B (BV & heart) receptors
* Hence lesser effect of tamsulosin on BP & better for BPH

Question 4

tamsulosin effects

benefits; time for improvement

Answer 4

• Effects on urinary stage & voiding symptoms maintained during long term therapy
  Can hold & pass urine better ⇒ reduces pain
• Delays need for surgery/ catheterisation
• Improvement in urinary flow rate after a few hours/ days after administration

Question 5

tamsulosin PK
absorption

Answer 5

Well absorbed orally (take 0.4 mg OD)

Question 6

tamsulosin PK
distribution

Answer 6

Highly bound to plasma protein (> 90%)
Not readily distributed to tissues ⇒ Small Vd (0.2L/ kg)

Question 7

tamsulosin PK
metabolism

enzymes involved, t1/2

Answer 7

• By CYPs (ie: CYP3A4, CYP2D6)
  Take note: do not take drug with grapefruit juice → affects liver enzymes
• t1/2 ~ 20-25 hour ⇒ hence OD dosing

Question 8

tamsulosin PK
excretion

Answer 8

~10% excreted unchanged in urine
* Requires dose adjustment for renal impairment

Metabolites more soluble in urine (~90%)

Question 9

tamsulosin AE

Answer 9

Abnormal ejaculation
Back pain

Question 10

tamsulosin c/i

Answer 10

Concurrent use of another α1 adrenoceptor antagonist (CVS patients)

Question 11

finasteride drug type

Answer 11

5α-reductase inhibitor

Question 12

finasteride MOA

Answer 12

• Competitive inhibition of 5α-reductase
  No conversion of testosterone to DHT, esp in male genitalia
• Hence decreases prostate size (with higher dose, 5mg)
  Also increases hair growth (with lower dose, 1mg)

Question 13

finasteride clinical effects

Answer 13

improved urine flow, reduces frequency of acute retention of urine & the need to surgical procedures

Question 14

finasteride clinical treatment

time for effects, serum prostate-specific Ag

Answer 14

May take up to 6 months to see clinical effects after initiating treatment

Serum prostate-specific Ag levels decreases with finasteride

Question 15

finasteride PK
absorption

F

Answer 15

Well absorbed orally (5 mg OD)
F ~ 0.65

Question 16

finasteride PK
distribution

Vd

Answer 16

High plasma protein bound (~90%) ⇒ Small Vd

Question 17

finasteride PK
metabolism

t1/2

Answer 17

By liver (CYP3A4)
t1/2 ~ 6 hr

Question 18

finasteride PK
excretion

Answer 18

50% unchanged in faeces
metabolites in urine & faces

Question 19

finasteride dose adjustments

Answer 19

Not required for liver failure, renal insufficiency & elderly patients

Question 20

finasteride AE

Answer 20

Loss of libido & sexual potency
Gynaecomastia (rare)

Question 21

finasteride c/i

Answer 21

Women & children; pregnancy

Question 22

sildenafil: drug type

Answer 22

PDE5 inhibitor

Question 23

sildenafil: MOA

Answer 23

• Inhibits phosphodiesterase type-5 (PDE5) in penis
• No conversion of cGMP to 5’GMP

Outcomes
(4) Increases cGMP levels in response to NO-release by sexual stimulation
(5) causes SM relaxation
(6) increased BF to corpora cavernosa
(7) erection

Question 23

sildenafil: MOA
specificity of drug

expression of PDE5

Answer 23

PDE5 highly expressed in Corpora cavernosa of penis & vasculature; poorly in myocardium ⇒ tissue specificity to compound

Question 23

sildenafil: initiation of dose

Answer 23

Ideally lowest recommended dose possible, especially for >65 years old

Question 23

sildenafil: PK
distribution

Answer 23

Widely distributed ⇒ large Vd

Question 23

sildenafil: PK
absorption

onset, F, duration of action

Answer 23

• well absorbed orally (5mg OD)
• Onset: 30-60 mins
• F ~0.4
• Duration of action (max): ~12 hours

Question 23

sildenafil: PK
metabolism

t1/2

Answer 23

By liver: CYP3A4 (major), CYP2C9 (minor)
t1/2 ~4 hours

Question 23

sildenafil: PK
excretion

Answer 23

Metabolites largely excreted in faeces (80%) & lesser in urine (13%)
Remaining unchanged in urine

Question 24

sildenafil: dose adjustment requirments

Answer 24

Not required for liver failure, renal insufficiency & elderly patients

Question 24

sildenafil: AE

Answer 24

• Headache, dizziness, flushing, dyspepsia
• Blur vision → blue-green tinting of vision (due to blockage of retinal PDE6)
• Priapism (similar feeling to BPH)

Question 25

sildenafil: c/i

Answer 25

Cardiac patients on GTN (generates NO; accumulates cGMP)
* Potentiates vasodilation effect on GTN due to increased cGMP; due to concomitant blockade of cGMP degradation by sildenafil
* Have potential marked vasodilation & hypotension