DIS - Glaucoma Medications I - Week 5

Question 1

Must glaucoma patients whose treatment is initiated by an optometrist be referred to an ophthalmologist? Explain.

Answer 1

Yes, within 4 months of initiating treatment, for chronic glaucoma to consider surgical options

Question 2

List the four types of aqueous suppressants. Note which isnt yet available in Australia.

Answer 2

Adrenergic alpha agonist
Adrenergic beta blocker
Carbonic anhydrase inhibitor
Rho-kinase inhibitor (NA)

Question 3

List two types of outflow modulators for the uveoscleral route.

Answer 3

Prostaglandin Analogues (PGAs)
Adrenergic alpha agonists

Question 4

List three types of outflow modulators for the trabecular meshwork. Note which isnt yet available in Australia.

Answer 4

Muscarinic
Rho-kinase inhibitor (NA)
Nitric oxide (NA)

Question 5

List two alpha agonist aqueous suppressant drugs and concentrations used.

Answer 5

Iopidine (0.5%)
Brimonidine (0.15%, 0.2%)

Question 6

List two rho-kinase inhibitor aqueous suppressant drugs and concentrations used.

Answer 6

Rhopressa (0.02%)
Netarsudil (0.02%)

Question 7

List three beta blocker aqueous suppressant drugs and concentrations used.

Answer 7

Betaxolol (0.25%, 0.5%)
Timolol (0.25%, 0.5%)
Nyogel (0.1%)

Question 8

List three carbonic anhydrase inhibitor aqueous suppressant drugs and concentrations used.

Answer 8

Brinzolamide (1%)
Dorzolamide (2%)
Diamox (azetazomalide 250mg PO)

Question 9

List five prostaglandin analogue uveoscleral outflow modulator drugs and concentrations used.

Answer 9

Latanoprost (0.005%)
Tafluprost (0.0015%)
Travoprost (0.004%)
Bimatoprost (0.03%)
Latanoprostene bunod (0.024%)

Question 10

List an alpha agonist uveoscleral outflow modulator drug and the concentration used.

Answer 10

Brimonidine (0.15%, 0.2%)

Question 11

List a muscarinic trabecular meshwork outflow modulator drug and the concentration used.

Answer 11

Pilocarpine (1%, 2%, 4%)

Question 12

List two rho-kinase inhibitor trabecular meshwork outflow modulator drugs and concentrations used.

Answer 12

Rhopressa (0.02%)
Netarsudil (0.02%)

Question 13

List a nitric oxide trabecular meshwork outflow modulator drug and the concentrations used.

Answer 13

Latanoprostene bunod (0.024%)

Question 14

What enzyme sustains ionic flux within the ciliary body and how does water diffuse passively?

Answer 14

Carbonic anhydrase
Water diffuses via aquaporins

Question 15

What does the inhibition of carbonic anhydrase do to aqueous production and how (3)?

Answer 15

Decreases aqueous production
By blocking carbonic anhydrase, you block the conversion of CO2 and H2O into HCO3- and H+
This prevents the exchange of these two molecules with Cl- and Na+ into the cell and out into the posterior chamber (these ions stay put), disrupting ionic flux

Question 16

Where are alpha and beta receptors located (3)?

Answer 16

Ciliary epithelium
Veins of schlemms canal
Veins of the ciliary body

Question 17

Describe how a beta-blocker reduces aqueous production by explaining what a beta agonist does (5).

Answer 17

Stimulates a g-protein cascade resulting in an increase to adenyl cyclase, increasing levels of cAMP
This activates a kinase which increases aqueous production
A beta-blocker would stop this from happening

Question 18

Describe how an alpha-agonist results in a decrease in aqueous production. Note whether this is a1 or a2. Describe where receptors of the other alpha are found and two things an agonist results in.

Answer 18

An a2 agonist stimulates a g-protein cascade (different to a beta g-protein cascade) resulting in an inhibition of adenyl cyclase, decreasing levels of cAMP
This inactivates a kinase which results in decreased aqueous production
Veins have a1 receptors, agonists reult in increased TM outflow and uveoscleral outflow

Question 19

Compare the onset and duration of the effects of beta blockers and alpha agonists (both a1 and a2) on aqueous production.

Answer 19

Alpha a2 and beta blockers have a slow onset and are long lasting
Alpha a1 agonists have a fast onset, short duration

Question 20

Are diamox tablets (oral) available for optomtrists? Explain (2).

Answer 20

No, do it via a GP or pharmacist

Question 21

Can diamox tablets and drops be used concurrently?

Answer 21

No, avoid concurrent use

Question 22

What percentage rise in IOP is seen if you swap from oral diamox to topical?

Answer 22

25%

Question 23

What percentage drop in IOP is seen with oral diamox? What about topical use?

Answer 23

Oral - up to 50%
Topical - up to 20%

Question 24

What is oral diamox often taken with? How long does IOP take to decrease with this combo? what about if diamox is injected?

Answer 24

500mg KCl
120 mins for IOP decrease if oral
15 mins if injected

Question 25

List two contraindications for diamox. Explain why if applicable (3). Also mention a certain diuretic in this context.

Answer 25

Allergy if sensitive to sulpha drugs
Kidney disease - risk for acidosis and potassium depletion - especially if with thiazide diuretic (+500mg K po)

Question 26

What are the systemic effects of carbonic anhydrase inhibitor drops? Explain why.

Answer 26

Few to no systemic effects because they bind to red blood cells

Question 27

How often are carbonic anhydrase inhibitor drops taken? What is the half life and what is this due to?

Answer 27

bid
Half life ~4h due to corneal reservoir

Question 28

Do carbonic anhydrase inhibitor drops decrease IOP more, the same, or less than most other drugs?

Answer 28

Less

Question 29

How do carbonic anhydrase inhibitor drops affect IOP diurnal fluctuation? Is this good or bad?

Answer 29

Reduces it - a good thing

Question 30

Do carbonic anhydrase inhibitor drops have a good or poor vascular and nocturnal profile?

Answer 30

Good

Question 31

Are the effects of carbonic anhydrase inhibitor drops fast or slow?

Answer 31

Fast (1h)

Question 32

With what other IOP lowering drug are carbonic anhydrase inhibitor drops a good adjunct (and how many drops per day).?

Answer 32

Prostaglandins
-carbonic anhydrase inhibitor drops bid for adjunct therapy

Question 33

List two primary therapies for which carbonic anhydrase inhibitor drops are used (and how many drops per day).

Answer 33

For large diurnal IOP fluctuation (tid)
For patients with low tension glaucoma (tid)
-to promote vasobenefits

Question 34

Are there any allergic responses to carbonic anhydrase inhibitor drops?

Answer 34

No

Question 35

In which case should carbonic anhydrase inhibitor drops be avoided? Explain why.

Answer 35

Avoid in corneal grafts
-cornea needs carbonic anhydrase to pump

Question 36

What kind of formulary are brinzolamide (Azopt) generally made, are different drugs in this class similar, and what kind of release does this formulary have?

Answer 36

All have similar formularies
Azopt - buffered suspension - shake before use
Suspensions give slower release

Question 37

Does Azopt sting more or less on instillation? Compare the IOP reduction it has to dorzolamide (Trusopt).

Answer 37

Less stinging
Same IOP effect as Trusopt

Question 38

How should Azopt be stored?

Answer 38

Upside down as its a suspension

Question 39

Is Azopt ok for use in pregnancy and lactation?

Answer 39

Yesd

Question 40

What advice is given to patients who need to use Azopt (3)?

Answer 40

Shake before use
Store upside down
May feel discomfort for a while, if vision blurs avoid driving and operating machinery

Question 41

Do beta blockers have a small or large effect on IOP?

Answer 41

Large

Question 42

Do beta blockers have many side effects/contraindications or few?

Answer 42

Many

Question 43

Can the effects of a beta blocker wear off?

Answer 43

Yes

Question 44

Are beta blockers effective at night?

Answer 44

No

Question 45

Using IOP and blood pressure, describe how beta blockers are not helpful in low tension glaucoma, especially at night.

Answer 45

Beta blockers do not work
at night
Blood pressure decrease coupled with high IOP means decreased perfusion pressure - must avoid in low tension glaucoma

Question 46

Describe why beta blockers do not work at night.

Answer 46

They are aqueous suppressants. Aqueous flow decreases at night on its own, these drugs cant decrease it any further

Question 47

What happens to ~50% of beta blocker patients after 1-2 years?

Answer 47

Tachyphylaxis

Question 48

List 5 ocular side effects of beta blockers.

Answer 48

Blurred vision
Corneal hypoaesthesia
SPK
Macular oedema
Conjunctivitis

Question 49

List four side effects beta blockers can have on the lungs (1), heart (2), and endocrine system (1).

Answer 49

Bronchospasm
Bradycardia
Reduced blood pressure
Increased HDLs

Question 50

What effect do beta blockers have on myasthenia gravis?

Answer 50

Worsens it

Question 51

What effect do beta blockers have on hyperthyroidism and diabetes?

Answer 51

Masks their signs

Question 52

What effect do beta blockers have on libido and sleep disorders? Explain why if applicable and what it can lead to.

Answer 52

Decreases libido
Increases sleep disorders
-depresses melatonin (can lead to depression)

Question 53

What ocular condition is a contraindication for beta blockers?

Answer 53

Low tension glaucoma

Question 54

When prescribing beta blockers, for what 5 conditions should a patient be worked up for by their GP?

Answer 54

Bradycardia
Athsma
Myasthenia gravis
Diabetes
Depression

Question 55

Is there an additive effect of topical + systemic beta blocker? Should it be used in this manner with caution? Explain (1).

Answer 55

There is an additive effect
Use with caution and monitor for bradycardia
Effect most on blood pressure and pulse

Question 56

Must a patients Gp be informed in long term beta blocker therapy?

Answer 56

Yes

Question 57

Do oral beta blockers have an effect on IOP?

Answer 57

Yes, 1mmHg

Question 58

Is timolol (nyogel) a selective or non-selective beta blocker?

Answer 58

Non-selective

Question 59

How is timolol best used?

Answer 59

As an adjunct with an alpha agonist or PGA for night time benefit

Question 60

Is betaxolol a selective or non-selective beta blocker?

Answer 60

Selective b1 blocker

Question 61

What is the safest beta blocker for asthmatics?

Answer 61

Betaxolol

Question 62

Does betaxolol have more, the same, or less effects on cardiac/blood pressure as timolol?

Answer 62

The same

Question 63

Does betaxolol have more, the same, or less effects on IOP as timolol?

Answer 63

Less

Question 64

What does recent evidence suggest of the effect non-selective beta blockers have on blood vessels and why is this significant?

Answer 64

Suggests they (timolol) can cause vasoconstriction, offsetting IOP benefit

Question 65

In what disease is betaxolol contraindicated?

Answer 65

Cardiac disease

Question 66

Where are a1 receptors found, and what is the mechanism of action for alpha 1 agonists?

Answer 66

Found on the veins
They increase the uveoscleral outflow and increase TM outflow (major)

Question 67

Explain how alpha agonists have a neuroprotective effect.

Answer 67

Increased blood flow to the optic nerve

Question 68

What effect can alpha agonists have in kids? what about adults (2)?

Answer 68

Kids - can make them drowsy
Adults - systemic hypotension and lethargy in some

Question 69

List three contraindications for alpha agonists.

Answer 69

Tricyclic antidepressants
MAO inhibitors
Severe cardiovascular disease

Question 70

Is there an IOP effect at night with a1 agonists? What about blood flow?

Answer 70

No IOP effect at night
But increased blood flow

Question 71

Is the effect of a1 immediate?

Answer 71

Yes

Question 72

What drug is recommended for use in glaucoma and what kind of drug is it (including selectivity). Why does it have short term applications? Explain why IOP control wears off (and after how long).

Answer 72

Apraclonidine
-a1 selective agonist
Short term application due to tachyphylaxis
Its a1 selectivity means IOP control wears off in 30% of people after 3-4 months

Question 73

List three ocular effects apraclonidine can have.

Answer 73

Mydriasis
Lid retraction
Conjunctival vasoconstriction

Question 74

What selectivity does brimonidine have? Does it cause tachyphylaxis? How quickly does it act and what kind of IOP response does it elicit?

Answer 74

Selective a2 agonist
Doesnt cause tachyphylaxis
Fast response (<2h)
Moderate IOP response (4-5mmHg)

Question 75

Is brimonidine good for short or long term application?

Answer 75

Long term

Question 76

Is brimonidine good to use for low tension glaucoma or should it be avoided?

Answer 76

Good for low tension glaucoma

Question 77

What line drug is brimonidine considered?

Answer 77

Acceptable as 2nd line drug

Question 78

How many drops per day is brimonidine used? What gives better compliance? How should it be used if as an adjunct?

Answer 78

tid for max effect
bid gives better compliance
bid as an adjunct

Question 79

Does brimonidine have neuroprotective effects like some other alpha agonists?

Answer 79

Yes

Question 80

What is combigan and why is it used?

Answer 80

IOP benefits of timolol and blood flow benefits of alphagan (brimonidine) as well as night time alpha benefits (IOP not reduced)

Question 81

Compare IOP control and night time effect in beta blocker vs alpha agonists. Describe an advantage of alpha agonist over beta blockers. Are a combination of the two good or avoided?

Answer 81

Beta blocker - good IOP control excpet at night
Alpha agonist - good IOP control except at night
-good pOBF effect
Combination of the two is good overall

Question 82

Describe the direct (3) and indirect (3) pathways of how muscarinic drugs act on aqueous flow.

Answer 82

Direct
-M3 receptors on ciliary body activates muscles
-cells pull on the scleral spur
-decreases IOP

Indirect
-muscarinic receptors on trabecular cells activate actin fibres
-trabecular pores close
-IOP increases

Question 83

Do cholinergic agonists activate muscarinic/nicotinic receptors?

Answer 83

Yes

Question 84

What kind of agonist is pilocarpine (2)?

Answer 84

Muscarinic and nicotinic

Question 85

Does pilocarpine have a fast or slow onset? How long does the response last?

Answer 85

Fast onset (1h) and short lasting response

Question 86

How many drops for pilocarpine per day? What effect does having brown eyes have and why? What should be done in these cases?

Answer 86

tid
Reduced effect in brown eyes due to non-specific pigment binding (use 2%)

Question 87

What is the major applicaiton of pilocarpine and why (2)? Is it used for modern glaucoma? Explain.

Answer 87

Low doese (0.016%) useful in PDS/PDG where miosis and reduced iris movement is desired
Not used much for glaucoma due to adverse effects

Question 88

List 5 contraindications for pilocarpine.

Answer 88

History of peripheral retinal detachment
High myopia
Central media opacity
Young patients
Uveitis

Question 89

Why does cholinergic toxicity happen mostly due to?

Answer 89

Systemic absoprtion
Reduce with digital occlusion and closed eyes

Question 90

Does latanoprost have a quick or delayed onset? what is done with dosing as a result?

Answer 90

Delayed - dose at night

Question 91

What happens to IOP early with latanoprost? What about with chronic application? What is this mainly due to?

Answer 91

IOP spike early on
Chronic application - no spike
-mainly MMP3 related

Question 92

Describe the dual action of latanoprost (2 each). Note which is the main effect.

Answer 92

Inhibition of MMPs (main effect)
-reduces IOP
-small initially, large effect chronically

Inhibition of TNFα
-decreased inflammatory response, increased venous outflow
-increased endothelial vacuoles/veins
-fast IOP effect

Question 93

Do PGAs tend to be very individual dependent in terms of response or do most poeple respond the same way?

Answer 93

Very individual dependent

Question 94

Are PGAs safe?

Answer 94

Yesd

Question 95

What are 5 ocular side effects of PGAs?

Answer 95

Iris darkening
Skin discolouration
Reduced adipocyte activity (sunken eyes)
Thicker lashes
Promotes ocular inflammation

Question 96

What can PGAs predispose you to?

Answer 96

Recurrent HSV keratitis

Question 97

List two contraindications for PGAs.

Answer 97

Pregnancy
Ocular inflammatory disease

Question 98

What is the safest PGA for glaucoma PGF2a activation?

Answer 98

Latanoprost (xalatan)

Question 99

Does xalatan have an increased or decreased response in low tension glaucoma compared to other glaucomas?

Answer 99

Reduced

Question 100

What is the major benefit of xalatan compared to other PGAs?

Answer 100

Additive to all other drugs, including pilocarpine

Question 101

List three side effects of xalatan.

Answer 101

Iris darkening
Lash growth
Loss of orbital fat (sunken eyes)

Question 102

List two reasons why xalatan can cause red eye. Note which is short term and long term.

Answer 102

Short term (up to 30 days) - due to altered outflow in veins
Long term - due to MMP3 related cell swelling

Question 103

What benefit does travoprost (travatan) have over latanoprost (xalatan)? List a consequence of this.

Answer 103

Better receptor binding
-more adverse effects

Question 104

Which PGA causes greater eyelash growth and can cause significantly more conjunctival hyperaemia?

Answer 104

Bimatoprost (lumigan)

Question 105

How does the IOP reduction of latanoprost compare after 1 month and what is typically done?

Answer 105

It has poor IOP reduction after 1 month - switching to bimatoprosy may control IOP

Question 106

Which of the gluacoma eyedrops should be avoided for 2 months after eye surgery and why? What can its effect be blocked by?

Answer 106

Avoid PGs for 2 months after eye surgery
-increased PGs in the eye after surgery promotes cystoid macular oedema
PG effect can be blocked with NSAID treatment
Can cotreat with NSAID to suppress inflammation