Drugs for BPH 3.1.1 Flashcards

1
Q

What are examples of selective alpha-1 adrenoreceptor blockers?

A
  • Alfuzosin
  • Prazosin
  • Silodosin
  • Tamsulosin
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2
Q

What are examples of 5a reductase inhibitors?

A

Finasteride = inhibits type 1 5a-reductase

Dutasteride = inhibits type 1 and type 2 5a reductase

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3
Q

Bladder neck and prostate gland are innervated by ANS, what does alpha-1 stimulation do?

A

Increases smooth muscle contraction therefore it inhibits the outflow of urine

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4
Q

Following on from the previous question, what is the MOA of alpha-1 blockers (APST)?

A

α1-blockers relax smooth muscle in the prostate and bladder neck –> facilitate micturition (urinating) in patients with benign prostatic hyperplasia / hypertrophy (BPH).

Blockade of postsynaptic a1-adrenoceptors

  • Block alpha receptors in non-vascular smooth muscle
  • Relaxes smooth muscle in bladder neck and prostate
  • Reduces resistance to urine flow
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5
Q

For alpha-1 blockers, which are more specific for bladder and prostate?

A

Silodosin and tamsulosin – more specific – affects bladder and prostate act on D$-adrenoceptors

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6
Q

For alpha-1 blockers, which one is less specific and thus causes vasodilation in ateries and veins?

A

Prazosin

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7
Q

True or false, a-1 blockers have very little effect on presynaptic D-adrenoceptors therefore much less reflex tachycardia than non-selective a blockers.

A

V true

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8
Q

What are the AE of a-1 blockers (APST)?

A

AE similar to phentolamine

  • Orthostatic hypotension (feeling faint on standing up), dizziness, headache, weakness, fatigue, drowsiness, diarrhoea, fatigue
  • Nasal congestion, urinary urgency, First dose hypotension
  • Tachycardia (less than phentolamine), palpitations, blurred vision
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9
Q

Where is testosterone synthesised? What is it converted to?

A

Testosterone is synthesized in the testes by the same pathways as in the ovaries.

Testosterone is converted to dihydrotestosterone (DHT) by 5α-reductase in the prostate, hair follicles, and skin.

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10
Q

What are the main androgens responsible for development and progression of BPH?

A

Testosterone and DHT are main androgens responsible for this

> DHT more potent than testosterone

> DHT more than testosterone in androgenic stimulation

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11
Q

If DHT formulation inhibited, what happens to the prostate?

A

If DHT formation is inhibited, there will be significant decreased androgenic stimulation in prostate –> decrease prostate growth.

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12
Q

MOA of 5a-reductase inhibitors?

A

5α-reductase inhibitors downregulate prostate growth by blocking the conversion of testosterone to DHT which is the more potent stimulator of prostate enlargement

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13
Q

Where are type 1 and type 2 5a reductases found?

A

Type 1 found in liver, skin. and hair

Type 2 is predominant in genital tissue and prostate

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14
Q

What are the therapeutic effects of 5a-reductase inhibitors?

A
  • Downregulate prostate growth
  • Reduce prostate volume
  • Can retard progression of BPH
  • Improve urinary flow and decrease the risk of urinary retentuon
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15
Q

CIR AE of 5a-reductase inhibitors

A

Common

  • impotence, decreased libido, ejaculation disorder (including decreased ejaculate volume)

Infrequent

  • breast tenderness or enlargement

Rare

  • allergic reaction, poor semen quality, infertility, depression
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