Glaucoma For The “ Regular”...
Transcript of Glaucoma For The “ Regular”...
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Glaucoma For The “ Regular” Optometrist
Eric E. Schmidt, O.D.Omni Eye Specialists
Wilmington, [email protected]
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Glaucoma Risk Factors
• FINDACAR
• The more risk factors one has, the more likely one is to develop glaucoma
• The more risk factors one has, the lower the IOP target should be
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A Review Of Risk Factors
• FINDACAR– Family history– IOP– Nearsightedness– Diabetes/Vascular disease– Age– Corneal thickness– Asymmetry– Race
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A risk factor analysis is critical
• For the diagnosis• To increase your level of suspicion• For initiating therapy• For changing therapy
• BUT…are any of these more important than others?
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Reviewing The Glaucoma Studies
What do they all mean?
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EMGT Conclusions
1) Reducing IOP (by 25%) prevents or slows VF defect and progression
2) For each 1mm of IOP reduction there is a 10% lower risk of VF loss
3) Study design and outcome show that these results are only due to IOP reduction (non IOP related factors showed difference between the 2 groups)
4) Tx effect was equal across age and glaucoma categories
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Eric’s spin on the EMGT
• 1-2 extra mm Hg may indeed be important-especially in advanced cases.
• For those pxs who need treatment, aggressive therapy is warranted
• It is probably better to treat early than late• You do not necessarily need to wait until the VF
defects arise before therapy is initiated• The benefit of treatment does last throughout the
lifetime of the px – just remember the risk/benefit
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AGIS Results
• Pxs who achieved IOP < 18mm on 100% of f/up visits showed no VF progression (avg IOP 12.3mm)
• Pxs w/ IOP < 18mm on<50% of f/up visits showed VF progression (mean IOP 20.2mm)
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Low IOP Slows or Halts Vision Loss in Open-Angle Glaucoma
0%
20%
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80%
100%
Mean IOP (mm Hg)
Perc
enta
ge o
f Pat
ient
s
Stable Progressed
stable
Mao et al, AJO, 1991
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Aggressive IOP Lowering Needed In Advanced POAG
IOP <15 mm Hg
0%
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40%
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11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28Mean IOP Over 15 Years (mm Hg)
Perc
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f Eye
s
Stable Progressed
Shirakashi et al, Ophthalmologica, 1993
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Diurnal IOP Fluctuations Speed Glaucomatous Progression
Asrani et al, J Glauc, 2000
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Patients With Diurnal IOPRange >11.8 mm Hg
Patients With Diurnal IOPRange <7.7 mm Hg
Pat
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s (%
)
Stable Visual Field
Visual Field Loss
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AGIS Results
• Diurnal Curve Is Real Important– Avg IOP of 15mm with a curve btwn 13mm –
17mm progresses less than if curve is btwn 11mm – 19mm
• The peak IOP is important• Which tx best affect the diurnal curve?
• Also remember risk/benefit ratio
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Consistently Low IOP Reduces Vision Loss
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0 20 40 60 80 100Follow-up Visit (Months)
Mea
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core
All visits <1875 to 100% of visits <1850 to 75% of visits <180 to 50% of visits <18
Mean IOP
20.2 mm Hg
16.9 mm Hg14.7 mm Hg
12.3 mm Hg
AGIS 7, AJO, 2000
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OHTS
• Goal of tx – 20% drop in IOP- 24mm target IOP
RESULTS: At 5 years4.4% of tx group developed POAG9.5% of no tx group developed POAG
So - lowering IOP in Oc Hx reduced the likelihood of glaucoma by 50% - RIGHT?
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OHTS – A Closer Look
• 90% of untreated group did not progress• 95.6% of tx group did not progress
• It proved that in those individuals who are going to progress to POAG lowering IOP by 22.4% will delay the onset by at least 5 yrs.
• Who are “ those individuals at risk”?
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OHTS – The Nitty Gritty
• The most predictive factors for conversion:– Older age
• 22% increase/ decade– Larger horizontal and vertical C/D
• 32% increase/0.1 larger– Higher baseline IOP
• 10% increase/ mm Hg– Thinner corneas
• 71% increase in risk/ 40 microns thinner
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Risk Factors For Conversion
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The pachymetry issue
• Juicy Data– 36% of pxs w/ IOP >25.75 AND K thickness < 555
microns developed POAG– 6% of pxs w/ same IOP but K thickness > 588
converted toPOAG• Juicy Data II
– 15% pxs w/ C/D .3/.3 and K thickness < 555 microns converted but
– 4% of pxs w/ same disk parameters and K thickness> 588 microns converted
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More Pachymetry Chatter
• African-Americans have thinner corneas• Perhaps thin corneas translate to poor
connective tissue at the disk as well• Is there a fudge-factor for K thickness?
– Baseline of 545 microns– Add or subtract 2.5mm Hg for every 50
microns deviation (Doughty and Zaman, Surv Ophthalmol, 2000).
• How should you use this data?
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Corneal Thickness And Glaucoma The Latest Scoop
• CCT and VF loss –– CCT is a strong predictor for field loss in both
NTG and POAG
– CCT-adjusted IOP does not predict VF loss
• Sullivan-Mee, Halverson, et.al. Optometry 2005;76:228-38.
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Corneal Thickness and Glaucoma
• CCT and Visual Function In OHT pxs– OHT pxs with abnormal SWAP results had
significantly thinner CCT than normals or OHT pxs with no VF defects
– Abnormal VF – 545microns– OHT w/ normal VF – 572 microns– Normals – 557 microns
• Medeiros, Sample, Weinreb – AJO Feb, 2003 135,No.2
• So????
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CCT And Glaucoma-More latest scoop
• RNFL thickness and CCT in OHT pxs– RNFL in OHT pxs with CCT < 555 was
significantly thinner than in those with CCT >555.
– RNFL of normals and OHT pxs with CCT >555 were similar
– Points to an inherent structural predispositon to glaucomatous damage?
– Kaushik,S, et.al, AJO May 2006, 884-890.
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CCT and Treatment Response• OHTS group –AJO, November, 2004• Pxs with thinner corneas responded better to
PGA and beta-blockers– 1mm difference for beta-blockers– 1.5-2.5 mm difference for PGAs– 550 microns was tipping point
• Fan and Camras reported similar results with brimonidine (ARVO, 2004)
• Why??? And what clinical implications are there?
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Predictive Factors For Progressing POAG
• Older age• Advanced VF damage• Smaller neuroretinal im• Larger zone Beta
– Martus, Jonas, et.al. AJO, June 2005• Baseline IOP, but not Mean IOP
• Martinez-Bello, et al, AJO March 2000.
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Risk factors for progression • Predictive Factors for Progressive Optic Nerve Damage
in Various Types of Chronic Open-Angle Glaucoma -– Martus, Budde, Jonas, et.al. – AJO 6/05
• POAG-– Older age– Advanced perimetric damage– Smaller neuroretinal rim– Larger Beta zone
• NTG-– Baseline disk hemorrhage
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When deciding to treat …
• Identify…– Risk factors for conversion– Risk factors for progression– Risk factors for rate of progression
• Initial peak IOP• Age• C/D ratio• Systemic/vascular status
– Noscitur a sociis!
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IOP and Glaucoma
• Which IOP is most important?– Mean IOP– Peak IOP– Trough IOP– IOP range
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• For pxs who showed progression of glaucoma despite IOP at acceptable range – 3% showed a peak IOP >21mm– 35% showed a range of IOP >5mm
– Collaer, Caprioli, et.al, J Glaucoma 2005;14(3): 196-200
• Underscores the importance of serial tonometry even in well controlled pxs
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When Is The Peak IOP?
• 3,025 IOP readings on 1,072 eyes• NTG, POAG, Pre-perimetric G, OHT• Results:
– Peak IOP – 7AM – 20.4%– Noon – 17.8%– 5PM - 13.9%– 9PM – 26.7%
– Jonas, Budde, et al. AJO, June 2005;139:136-137
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Jonas study conclusion
• “Any single IOP measurement taken between 7AM and 9PM has a higher than 75% chance to miss the highest point of the diurnal curve.”
• Stresses the need for serial tonometry.
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“New” Goal of treatment in Glaucoma
• Low and Stable IOP
• Minimize the diurnal curve
• Prevent IOP peaks
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Treatment Goals of Glaucoma• Maximum IOP reduction—achieve lower IOP
to help preserve sight; historically physicians tried to achieve pressures below 20 mm Hg
• Maintaining low IOP over 24 hours—avoid pressure spikes associated with visual field progression
• Ease of use—patient compliance is best with simple, easy-to-use medication regimen (typical glaucoma patient uses at least 3 other systemic medicines); monotherapy is preferred
• Safety—minimize systemic safety issues
Gottfredsdottir et al. J Glaucoma. 1997.
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Recommendations
• Minimum initial target IOP reduction of 25% recommended for glaucoma patients
• More aggressive initial target IOP reductions of 30% or 35% recommended for most patients: especially those at higher risk
• Target IOP must be DYNAMIC, re-evaluated periodically, and lowered if patient progresses despite meeting the initial target IOP– Re-evaluate and adjust patient’s target IOP
at least every 5 years, and in light of newest information
The Delphi Panel. PDR. 2003.
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General Rule #1
• 30% decrease as an initial target
• Target decrease from highest untreated IOP
• CNTGS, OHTS
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General Rule #2
• Mild glaucoma – decrease IOP 30%
• Moderate glaucoma – decrease IOP 40%
• Severe glaucoma – decrease IOP 50% (at least)
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When should the target IOP be changed?
• VF progression (even at target IOP)• Neuroretinal rim recession (even at target
IOP)• Parametric changes• Long term stability – even if on multiple
meds
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Importance of IOP Stability
• IOP variation is a risk factor for VF loss in glaucoma
• VF protected best when pressures are consistently kept under 18 mm Hg
• Wide swings in IOP during the day or from visit to visit should be avoided
• Stabilizing IOP is vital
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Treatment Paradigm Summary• Mean IOP in study populations
– Early treatment to lower IOP reduces and delays progression– NEI trials show better outcomes at lowest IOP
• IOP in individual patient– To preserve vision, every mm Hg matters– Individualized, low target IOP recommended
• New predictors of progression– Diurnal fluctuation and long-term variation in IOP within
individual patients can cause glaucomatous damage• Treatment goal: get IOP low, and keep it low
Heijl et al. Arch Ophthalmol. 2002; Kass et al. Arch Ophthalmol. 2002; Lichter et al. Ophthalmology. 2001; AGIS Investigators: 7. Am J Ophthalmol. 2000.
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Primary Medical Therapy
• Building block approach
• Start with the STRONGEST FOUNDATION
• Efficacy Goals of Primary Therapy– Achieve lowest IOP on single agent– High response rate – every mm Hg matters – Maintain consistent long term and diurnal
pressure lowering
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Eric’s 7 Simple Rules For Treatment
1. Choose 30% IOP decrease as initial target
2. Squash the diurnal curve (Keep IOP peak <18mm)
3. Assess risk factors for progression and rate of progression(CT<555, IOP >26,C/D 0.5)
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Eric’s Rules cont.
4. If you are going to treat; treat aggressively
5. KISS
6. Be mindful of perfusion issues
7. Above all, do no harm
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The Glaucoma Treatment Universe 2008
• Prostaglandins• Alpha –agonist• CAI• Combo drugs• Ginkgo , etc
• Beta-blockers• Cardioselective beta-
blockers• ALT/SLT• Trabeculectomy• Nutrition issues
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Prostaglandins
• All decrease IOP by increasing uveoscleral outflow
• All are effective at squashing the diurnal curve
• They have either no effect or a positive effect on retinal perfusion
• But does 1 work better than the others?
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Why Are so Many Patients on Multiple Medications?
• Target IOPs set lower than in the past• As disease progresses, patients need
even lower IOP• Even the most effective IOP-lowering
medications, the lipids, do not get all patients to low target IOPs
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Choosing Therapy: Switch or Add?
• Target IOP should be reached with minimal number of medications
• Build strongest foundation prior to adjunctive therapy• Switching to a more effective medication may be best
course of action• Differences within medication classes exist• Potential benefits of monotherapy
– Improved patient compliance– Decreased cost– Reduced cumulative exposure to benzalkonium chloride
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What If:
• A patient failed on Xalatan?
• If switched to Lumigan, 57% achieved target IOP
• If switched to Travatan, 45.5% achieved target IOP
• SO?
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Latanoprost Non-Responders: Switch to Bimatoprost
Gandolfi, Cimino. Ophthalmology. 2003.
24.7 24.8 24.1
18.1
12
14
16
18
20
22
24
26
Baseline(Untreated)
After 30 DaysWashoutBetween
Treatments
After 30 Dayson
Latanoprost
After 30 Dayson
Bimatoprost
*P <.001 vs baseline, washout, and latanoprost
*
n = 15
Mea
n 16
-Hou
r Diu
rnal
IOP
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Regarding Prostaglandins:
• Generally the 1st line of treatment• There are interindividual differences in
efficacy• Are there racial differences?• If at first one fails; try, try , try again (with
another prostaglandin)
• Why wouldn’t you use a prostaglandin 1st?
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Prostaglandin Side Effects
• Conjunctival hyperemia: Severe hyperemia– Lumigan 3.5%– Travatan 1.5%– Xalatan <1%– Rescula 1%
• Is this a transient phenomenon?• Is it an allergic conjunctivitis?• Is it worth stopping the drop?
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Prostaglandin Side Effects• Iris pigmentation
– Is it reversible?– Is it pre-cancerous?
• Xalatan – 6.7% @ 6mths16% @ 12mths
• Travatan – 3% @ 12 mths• Lumigan – 1.9% @ 12mths• Rescula – 1 patient
• SO?
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Other Prostaglandin side effects
• CME• Uveitis• Reactivation of HSK• Hypertrichosis
• One must take into consideration the benefits of low IOP with the risks of the side effects
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Final prostaglandin thoughts
• They are additive to other G drugs but not with each other
• Travatan and Lumigan maintain target IOP 36hrs after instillation and significant IOP drop up to 84 hrs after instillation
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What if Target Pressure Is Not Reached With Even the Most
Powerful Monotherapy?
• Add a second medication!
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Primary Considerations in Choosing Adjunctive Therapy
• Efficacy when used with the first-line medication– IOP should be reduced by at least an additional
15% to a level as low as possible– A medication that is effective monotherapy, or when
added to one medication, may not be effective when added to a different medication!
• Safety– Safety concerns increase with each additional
medication: add the safest medication possible
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Brimonidine vs Dorzolamide Added to Topical Beta-Blocker
• Only patients who met target 15% IOP reduction were continued beyond 1 month
0
20
40
60
80
100*
* * P < .007
Patie
nts
Ach
ievi
ng T
arge
t≥
15%
IOP
Red
uctio
n (%
)
Month 1 Month 3
86%
62%
78%
44%
Brimonidine BID Dorzolamide TID
Simmons, Alphagan/Trusopt Study Group. Clin Ther. 2001.
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Treatment paradigm – Step 2
• Prostaglandins 1st
• If not successful – try another agent by itself: Brimonidine bid or timolol QAM or CAI BID
• If neither of these get IOP to desired level then add
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Treatment Paradigm, Part III
1.Prostaglandins alone2. Brimonidine or beta-blocker alone3. Prostaglandin + beta-blocker or
brimonidine (unless 1 of these absolutely sucked!)
4. Consider CAI or combo drop if (3) is not successful
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Treatment paradigm, part IV
• If on 2 meds and target IOP not met…– 1. Consider 3rd drop (Betoptic S or CAI)– 2. Substitute Cosopt or Combigan for least successful
drop– 3. Consider ALT or SLT
• What is maximum medical therapy nowadays?• SLT/ALT and trabeculectomy should not be
considered weapons of last choice or last chance
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Remember The Diurnal Curve!!!
• PGAs• Trabeculectomy• Brimonidine -TID• CAI – TID• What about beta-blockers?
– BID vs QAM– ½% vs ¼%– Effect on diurnal curve
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Visual Fields and Glaucoma
• Are they still cool?
• Are they considered the standard of care?
• How often?
• Do they better measure early detection or progression?
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Are certain VF parameters more predictive for progression?
• Johnson, Sample et al. – AJO 8/2002 177-185
• Highest predictors of conversion– GHT “outside normal limits”– 2 hemifield clusters worse than 5% level– 4 abnormal (P<.05) locations on pattern
deviation probability plot– Specificity increased with 2nd confirmatory VF
test
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Which VF instrument is best?
• SAP, SWAP or FDT– FDT and SWAP similar in flagging abnormal
locations– FDT defects were more extensive in 62%
• SWAP more specific and accurate than SAP but harder to administer
• FDT questionable in end stage glaucoma• Use 10-2 strategy in advanced glaucoma
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What About Imaging Units?
• Are they essential?
• What do they do ?
• What do they don’t do?
• Are they the standard of care?
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3 Questions For The Audience:
• 1. What is your definition of glaucoma?
• 2. What is the pathology of glaucoma?
• 3. Is retinal imaging the standard of care for treating glaucoma?
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RNFL and Glaucoma
• Axons of retinal ganglion cells form the retinal nerve fiber layer (RNFL)
• Glaucoma is characterized by loss of ganglion cells leading to loss of retinal nerve fibers
Glaucoma is a disease of the RNFL
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RNFL and Glaucoma
• RNFL changes are early to occur in glaucoma• Up to 50% of the retinal nerve fibers may be lost
before a visual field defect is detectable• Early detection of glaucoma by RNFL imaging
and analysis leads to early treatment, improving the chance to delay or halt the disease progression
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It’s Like An Alphabet Soup!!!
• GDx• HRT• OCT• RTA
• Are they all the same?• Are they all different?• Are there clinical studies to prove their claims?
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DIAGNOSE: Early is Better
Disc change precedes VF loss in most cases