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Diabetes and the Eye
Dr Shahjada Selim
Associate Professor
Department of Endocrinology
Bangabandhu Sheikh Mujib Medical University, Dhaka
Email: selimshahjada@gmail.com,
info@shahjadaselim.com
Diabetes and the Eye
Diabetic Retinopathy
Diabetic retinopathy is the leading cause of new blindness in persons aged
25-74
Diabetic Macula Oedema
Glaucoma
Iris Neovascularisation
Neuropathies
Corneal Anomalies
Hyperopic /Myopic Prescription Changes
Extra-ocular Muscle Palsy
Dry Eye Disease (50%) (reduced corneal sensitivity)
DIABETIC RETINOPATHY
DIABETIC RETINOPATHY
1. Epidemiology and risk factors
2. Classification and features of Diabetic
retinopathy (DR)
3. Complications of DR and their prevention
4. Screening protocol for DR and referral to Ophthalmologist
5. Direct ophthalmoscopy and identification of fundus
findings
Epidemiology of DR
RISK of developing DR:
• Type 1 DM – 70%
• Type 2 - 39%
• Type 2 on insulin – 70%
Prevalence of the type of Diabetes
 Type 2 – in 90% of diabetic patients
Diabetic retinopathy - most common
cause of legal blindness between
ages 20 and 70 years.
All people with Type 1 or Type 2 diabetes
are at risk of developing diabetic
retinopathy.
• Over the same duration, type 1 may
result in worse diabetic retinopathy
• The longer a person has diabetes,
the greater the risk. (25% for 15
years)
• Poor control of blood sugar levels
can increase the risk
Access Economics Pty Ltd. Clear Insight – The Economic Impact and Cost of Vision Loss in Australia, 1.2 Diabetic Retinopathy, August 2004,
Who is at risk?
• Systemic Hypertension
• Hyperlipidaemia
• Renal disease
• Pregnancy (with prior Type 1 or Type 2
diabetes)
• Family History of DR
• Smoking
Other Risk Factors
Intensive glucose therapy
Reduces the onset of new DR by 75%
Reduces the progression of DR by 50%
HbA1c 6-7%
1% decrease in HbA1c associated with lowering
the
◦risk of retinopathy 40%
◦progression to sight threatening DR 25%
◦risk for laser 24%
◦risk for blindness 5%
Controlling Diabetic Retinopathy Risk
Tight BP control associated with lower risk
of
Retinopathy progression 35%
Need for laser 35%
Risk for vision loss 50%
 Others: Hyperlipidemia(lipidil) / Smoking and
Alcohol consumption / Pregnancy / Body Mass
Index / Inflammation
Controlling Diabetic Retinopathy Risk
• It is estimated only ½ the Australians with diabetes have a
regular eye exam and 1/3rd have never been checked.
• Often there are no symptoms of diabetic retinopathy until
serious damage has occurred.
• Early diagnosis and treatment can prevent severe vision
loss
• Eye examination every Year is recommended for people
with diabetes.
Evidence indicates that early detection of Diabetic
Retinopathy by regular eye examination, is key to
reducing vision loss and blindness from diabetes.
Pathogenesis
Microangiopathy which has features of
both microvascular leakage and occlusion
Larger vessels may also be involved
Microvascular leakage
Loss of pericytes results in distention of
weak capillary wall producing
microaneurysms which leak.
Blood-retinal barrier breaks down causing
plasma constituents to leak into the retina
– retinal oedema, hard exudates
Microvascular occlusion
Basement membrane thickening,
endothelial cell damage, deformed RBCs,
platelet stickiness and aggregation
Vascular Endothelial Growth Factor
(VEGF) is produced by hypoxic retina
VEGF stimulates the growth of shunt and
new vessels
Classification of DR
I. Non-proliferative DR (NPDR)
• Mild
• Moderate
• Severe
• Very severe
II. Proliferative DR (PDR)
III. Clinically significant macular oedema
(CSME)
- May exist by itself or along with NPDR and PDR
• At least one microaneurysm - earliest clinically detectable
lesion
 Retinal hemorrhages
 Hard or soft exudates
Mild NPDR
Moderate NPDR
• Microaneurysms
and/or dot and blot
hemorrhages in at
least 1 quadrant
• Soft exudates
(Cotton wool spots)
• Venous beading or
IRMA (intraretinal
microvascular
abnormalities)
IRMA
Mild and Moderate Non- proliferative DR
was previously known as Background DR
Severe NPDR
Any one of the following 3 features is present
• Microaneurysms and intraretinal
hemorrhages in all 4 quadrants
• Venous beading in 2 or more quadrants
• Moderate IRMA in at least 1 quadrant
Known as the 4-2-1 rule
Very severe NPDR
Any two of the features of the 4-2-1
rule is present
Severe and Very severe Non-proliferative
DR was known as the Pre-proliferative DR
Clinically significant Macular
Oedema
• Retinal oedema close to fovea
• Hard exudates close to fovea
• Presents with dimness of vision
• By itself or along with NPDR or PDR
CSME – Hard exudates close to fovea and
associated retinal thickening
Proliferative DR
(PDR)
Characterized by
Proliferation of
new vessels from
retinal veins
• New vessels on
the optic disc
• New vessels
elsewhere on the
retina
Proliferative DR
NVD
COMPLICATIONS OF DIABETIC
RETINOPATHY
• Vitreous hemorrhage
• Tractional retinal detachment
• Rubeosis Iridis
• Glaucoma
• Blindness
Vitreous Hemorrhage
SUBHYALOID HEMORRHAGE
Tractional retinal detachment
Rubeosis Iridis
Neovascular Glaucoma
• Complication of rubeosis iridis
• New vessels cause angle closure
• Mechanical obstruction to aqueous outflow
• Intra ocular pressure rises
• Pupil gets distorted as iris gets pulled
• Eye becomes painful and red
• Loss of vision
Blindness
• Non-clearing vitreous hemorrhage
• Neovascular glaucoma
• Tractional retinal detachment
• Macular ischemia
PREVENTION OF COMPLICATIONS
• By early institution of appropriate treatment
• This requires early detection of DR in its
asymptomatic treatable condition
• By routine fundus examination of all
Diabetics (cost effective screening)
• And appropriate referral to ophthalmologist
Mild and Moderate NPDR
- No specific treatment for retinopathy
- Good metabolic control to delay
progression
- Control of associated Hypertension,
Anemia and Renal failure
Severe and very severe NPDR
– Close follow up by Ophthalmologist
Clinically significant macular oedema
- Laser photocoagulation to minimise risk of
visual loss
─ Retinal laser photocoagulation as per the
judgment of ophthalmologist (in high risk eyes)
─ It converts hypoxic retina (which produces
ANGIOGENIC factors) into anoxic retina (which
can’t)
Proliferative DR
Screening protocol for Diabetic
retinopathy
1. Screening once in a 1 year
• Diabetics with normal fundus
• Mild NPDR
2. Screening once in 6 months
• Moderate NPDR
Referral to Ophthalmologist
• Visual Symptoms
– Diminished visual acuity
– Seeing floaters
– Painful eye
• Fundus findings
- Macular oedema/hard exudates close to fovea
- Proliferative DR
- Vitreous hemorrhage
- Moderate to severe and very severe NPDR
- Retinal detachment
- Cataract obscuring fundus view
Referral to Ophthalmologist
• Presence of Risk Factors
- Pregnancy
- Nephropathy
Simulation of defective vision as experienced by a
Diabetic whose vision has been affected by Diabetic
retinopathy
Normal Defective
DIRECT OPHTHALMOSCOPY
• Examination of the fundus of the eye
• To screen for Diabetic Retinopathy
• After dilatation of both eyes with 0.5%
tropicamide
View of the retina through an
ophthalmoscope
Normal fundus views of Right
and left eye
Mild NPDR – Microaneurysms, Dot and
Blot hemorrhages
Moderate NPDR
Moderate NPDR with CSME
Circinate retinopathy – Hard exudates in a
ring around leaking aneurysms
DRUSEN
Age related Macular degeneration: Note the
drusen. Not to be confused with Hard exudates. There
are no microaneurysms or dot/blot hemorrhages.
Severe NPDR
• Cotton wool patches
• Hemorrhages - 4 quadrants
With CSME
Very severe NPDR
-Venous beading
- scars of laser spots
- Absorbing hemorrhages
Cotton-wool patches,
venous segmentation
CSME –
in
Different
Stages of
NPDR
Proliferative DR – New vessels elsewhere on
the retina along the supero-temporal vessels
PDR – New vessels on disc
PDR – New vessels on disc and new vessels
elsewhere on retina
PDR – with vitreous hemorrhage
Vitreous bleed
Vitreous Hemorrhage
Tractional retinal
detachment Fibro-vascular
proliferation
Thank you!
Any doubts?

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Diabetes and the Eye- DR Selim

  • 1. Diabetes and the Eye Dr Shahjada Selim Associate Professor Department of Endocrinology Bangabandhu Sheikh Mujib Medical University, Dhaka Email: selimshahjada@gmail.com, info@shahjadaselim.com
  • 2. Diabetes and the Eye Diabetic Retinopathy Diabetic retinopathy is the leading cause of new blindness in persons aged 25-74 Diabetic Macula Oedema Glaucoma Iris Neovascularisation Neuropathies Corneal Anomalies Hyperopic /Myopic Prescription Changes Extra-ocular Muscle Palsy Dry Eye Disease (50%) (reduced corneal sensitivity)
  • 4. DIABETIC RETINOPATHY 1. Epidemiology and risk factors 2. Classification and features of Diabetic retinopathy (DR) 3. Complications of DR and their prevention 4. Screening protocol for DR and referral to Ophthalmologist 5. Direct ophthalmoscopy and identification of fundus findings
  • 5. Epidemiology of DR RISK of developing DR: • Type 1 DM – 70% • Type 2 - 39% • Type 2 on insulin – 70%
  • 6. Prevalence of the type of Diabetes  Type 2 – in 90% of diabetic patients Diabetic retinopathy - most common cause of legal blindness between ages 20 and 70 years.
  • 7. All people with Type 1 or Type 2 diabetes are at risk of developing diabetic retinopathy. • Over the same duration, type 1 may result in worse diabetic retinopathy • The longer a person has diabetes, the greater the risk. (25% for 15 years) • Poor control of blood sugar levels can increase the risk Access Economics Pty Ltd. Clear Insight – The Economic Impact and Cost of Vision Loss in Australia, 1.2 Diabetic Retinopathy, August 2004, Who is at risk?
  • 8. • Systemic Hypertension • Hyperlipidaemia • Renal disease • Pregnancy (with prior Type 1 or Type 2 diabetes) • Family History of DR • Smoking Other Risk Factors
  • 9. Intensive glucose therapy Reduces the onset of new DR by 75% Reduces the progression of DR by 50% HbA1c 6-7% 1% decrease in HbA1c associated with lowering the ◦risk of retinopathy 40% ◦progression to sight threatening DR 25% ◦risk for laser 24% ◦risk for blindness 5% Controlling Diabetic Retinopathy Risk
  • 10. Tight BP control associated with lower risk of Retinopathy progression 35% Need for laser 35% Risk for vision loss 50%  Others: Hyperlipidemia(lipidil) / Smoking and Alcohol consumption / Pregnancy / Body Mass Index / Inflammation Controlling Diabetic Retinopathy Risk
  • 11. • It is estimated only ½ the Australians with diabetes have a regular eye exam and 1/3rd have never been checked. • Often there are no symptoms of diabetic retinopathy until serious damage has occurred. • Early diagnosis and treatment can prevent severe vision loss • Eye examination every Year is recommended for people with diabetes. Evidence indicates that early detection of Diabetic Retinopathy by regular eye examination, is key to reducing vision loss and blindness from diabetes.
  • 12. Pathogenesis Microangiopathy which has features of both microvascular leakage and occlusion Larger vessels may also be involved
  • 13. Microvascular leakage Loss of pericytes results in distention of weak capillary wall producing microaneurysms which leak. Blood-retinal barrier breaks down causing plasma constituents to leak into the retina – retinal oedema, hard exudates
  • 14. Microvascular occlusion Basement membrane thickening, endothelial cell damage, deformed RBCs, platelet stickiness and aggregation Vascular Endothelial Growth Factor (VEGF) is produced by hypoxic retina VEGF stimulates the growth of shunt and new vessels
  • 15. Classification of DR I. Non-proliferative DR (NPDR) • Mild • Moderate • Severe • Very severe II. Proliferative DR (PDR) III. Clinically significant macular oedema (CSME) - May exist by itself or along with NPDR and PDR
  • 16. • At least one microaneurysm - earliest clinically detectable lesion  Retinal hemorrhages  Hard or soft exudates Mild NPDR
  • 17. Moderate NPDR • Microaneurysms and/or dot and blot hemorrhages in at least 1 quadrant • Soft exudates (Cotton wool spots) • Venous beading or IRMA (intraretinal microvascular abnormalities) IRMA
  • 18. Mild and Moderate Non- proliferative DR was previously known as Background DR
  • 19. Severe NPDR Any one of the following 3 features is present • Microaneurysms and intraretinal hemorrhages in all 4 quadrants • Venous beading in 2 or more quadrants • Moderate IRMA in at least 1 quadrant Known as the 4-2-1 rule
  • 20. Very severe NPDR Any two of the features of the 4-2-1 rule is present
  • 21. Severe and Very severe Non-proliferative DR was known as the Pre-proliferative DR
  • 22. Clinically significant Macular Oedema • Retinal oedema close to fovea • Hard exudates close to fovea • Presents with dimness of vision • By itself or along with NPDR or PDR
  • 23. CSME – Hard exudates close to fovea and associated retinal thickening
  • 24. Proliferative DR (PDR) Characterized by Proliferation of new vessels from retinal veins • New vessels on the optic disc • New vessels elsewhere on the retina
  • 26. COMPLICATIONS OF DIABETIC RETINOPATHY • Vitreous hemorrhage • Tractional retinal detachment • Rubeosis Iridis • Glaucoma • Blindness
  • 30. Neovascular Glaucoma • Complication of rubeosis iridis • New vessels cause angle closure • Mechanical obstruction to aqueous outflow • Intra ocular pressure rises • Pupil gets distorted as iris gets pulled • Eye becomes painful and red • Loss of vision
  • 31. Blindness • Non-clearing vitreous hemorrhage • Neovascular glaucoma • Tractional retinal detachment • Macular ischemia
  • 32. PREVENTION OF COMPLICATIONS • By early institution of appropriate treatment • This requires early detection of DR in its asymptomatic treatable condition • By routine fundus examination of all Diabetics (cost effective screening) • And appropriate referral to ophthalmologist
  • 33. Mild and Moderate NPDR - No specific treatment for retinopathy - Good metabolic control to delay progression - Control of associated Hypertension, Anemia and Renal failure Severe and very severe NPDR – Close follow up by Ophthalmologist
  • 34. Clinically significant macular oedema - Laser photocoagulation to minimise risk of visual loss ─ Retinal laser photocoagulation as per the judgment of ophthalmologist (in high risk eyes) ─ It converts hypoxic retina (which produces ANGIOGENIC factors) into anoxic retina (which can’t) Proliferative DR
  • 35. Screening protocol for Diabetic retinopathy 1. Screening once in a 1 year • Diabetics with normal fundus • Mild NPDR 2. Screening once in 6 months • Moderate NPDR
  • 36. Referral to Ophthalmologist • Visual Symptoms – Diminished visual acuity – Seeing floaters – Painful eye • Fundus findings - Macular oedema/hard exudates close to fovea - Proliferative DR - Vitreous hemorrhage - Moderate to severe and very severe NPDR - Retinal detachment - Cataract obscuring fundus view
  • 37. Referral to Ophthalmologist • Presence of Risk Factors - Pregnancy - Nephropathy
  • 38. Simulation of defective vision as experienced by a Diabetic whose vision has been affected by Diabetic retinopathy Normal Defective
  • 39. DIRECT OPHTHALMOSCOPY • Examination of the fundus of the eye • To screen for Diabetic Retinopathy • After dilatation of both eyes with 0.5% tropicamide
  • 40. View of the retina through an ophthalmoscope
  • 41. Normal fundus views of Right and left eye
  • 42. Mild NPDR – Microaneurysms, Dot and Blot hemorrhages
  • 45. Circinate retinopathy – Hard exudates in a ring around leaking aneurysms
  • 46. DRUSEN Age related Macular degeneration: Note the drusen. Not to be confused with Hard exudates. There are no microaneurysms or dot/blot hemorrhages.
  • 47. Severe NPDR • Cotton wool patches • Hemorrhages - 4 quadrants With CSME
  • 48. Very severe NPDR -Venous beading - scars of laser spots - Absorbing hemorrhages Cotton-wool patches, venous segmentation
  • 50. Proliferative DR – New vessels elsewhere on the retina along the supero-temporal vessels
  • 51. PDR – New vessels on disc
  • 52. PDR – New vessels on disc and new vessels elsewhere on retina
  • 53. PDR – with vitreous hemorrhage Vitreous bleed