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Dr. Ashwini
7th term
 It is a metabolic disorder of multiple etiology
characterized by chronic Hyperglycaemia with
disturbances of Carbohydrates, Fats and Protein
metabolism resulting from defects in Insulin secretion,
Insulin action or Both.
Clinical Features
 Easy Fatigability
 Polyuria
 Polydipsia
 Wasting
 Weight loss
 Air hunger
 Blurred vision
 Poor wound healing
Complications
Acute :- Diabetic ketoacidosis.
Hyperglycemic Hyperosmolar state.
Chronic :-
A. Microvascular
B. Macrovascular
C. Others
A. Microvascular complications :- Retinopathy,
Macular edema, Sensory & motor neuropathy,
Autonomic neuropathy.
B. Macrovascular complications :- Coronary
heart disease, Peripheral arterial disease,
Cerebrovascular disease.
C. Others :- Cataract, Glaucoma, Periodontal disease,
Hearing loss, Gastroparesis, Diarrhea, Uropathy,
Sexual dysfunction, Acanthosis nigricans,
Necrobiosis lipoidica, Vitiligo etc….
Retinopathy Macular edema
Glaucoma Cataract
Acanthosis nigricans
Necrobiosis lipoidica
Vitiligo Neuropathic foot ulcer
Lipohypertrophy
Types
 Type 1 :- IDDM also called Juvenile Diabetes
 Type2 :- NIDDM
 Type3 :- Gestational Diabetes
 Type4 :- Other Specific Types
Type 1
 Insulin Dependent Diabetes Mellitus.
 Also called Juvenile Diabetes
 Common among 10-14 yrs of age group.
 Accounts for 5%-10% of all diagnosed cases of Diabetes
Mellitus.
 90% is Autoimmune mediated.
10% is Idiopathic.
Type 2
 Non Insulin Dependent Diabetes Mellitus.
 Common among adults and elderly people.
 Accounts for about 90-95% of all the diagnosed cases
of Diabetes.
 Begins as Insulin resistance, as the need for insulin
rises, the pancreas gradually loses it’s ability to
produce insulin.
Type 3
 Gestational Diabetes.
 It is a condition of Glucose Intolerance diagnosed in
some women during pregnancy.
 Common in African americans, Latino americans,
American Indians, Obese and women with family
history of Diabetes.
 After pregnancy, 5-10% of women with Gestational
Diabetes are found to develop Type 2 Diabetes.
Other Specific Types
 Genetic defects of Beta-cell function.
 Genetic defect in insulin action.
 Pancreatic diseases.
 Excess endogenous production of hormonal
antagonist to Insulin.
 Drug- Induced.
 Viral infections.
 Latent Autoimmune Diabetes in Adults (LADA).
 Modified Onset of Diabetes in Young (MODY).
Burden of Diabetes
 Iceberg Disease.
 Currently (2010) 285 million people are affected worldwide
of which 20% is contributed by SEAR (China & India).
 International Diabetic Federation (IDF) data indicate that
the number reaches 333 million by 2025, of which 90% is
Type 2.
 Increased prevalence in newly Industrialized & Developing
countries.
 Disease is acquired in the most Productive period of Life.
 Accounts for 6-12% of all Health care expenditure annually.
Globally, the Diabetic cases crosses 300 millions by 2025.
Rising Diabetic burden on INDIA.
Risk Factors
Host Factors
 Age
 Sex
 Genetic Factors
 Genetic Markers:- HLA-B8, HLA-B15, HLA-DR3 and HLA-
DR4
 Immune mechanism
 Maternal Diabetes
 Obesity
World-wide estimated number of adults with diabetes
by age group and year.
Environmental Factors
 Sedentary life style
 Diet rich in Saturated Fatty acids
 Decreased consumption of Diatary Fibers
 Malnutrition
 Alcohol
 Chemical agents
 Stress
 Other factors
Screening
Urine examination:- LAck of Sensitivity
Gives too many “False Negatives”
Blood Sugar Testing:-
RBS - >200mg/dl with symptoms & signs of diabetes.
FBS - >126mg/dl
PPBS - >200mg/dl
Glycated Haemoglobin - >6.5%
Target Population:-
More than 40yrs
Family history of Diabetes
Obese
HDL <35mg/dl and Triglycerides >250mg/dl
Women who had baby weighing >4.0kg
Women who show excess weight gain during pregnancy
Patients with Premature Atherosclerosis
Prevention
PRIMARY PREVENTION
 Population Strategy
 High-Risk Strategy
SECONDARY PREVENTION
TERTIARY PREVENTION
Primary Prevention
POPULATION STRATEGY
 The scope for primary prevention of IDDM is limited.
 Based on Elimination of environmental risk factors ,
development of prevention programmes for NIDDM is
possible.
HIGH-RISK STRATEGY
 Effectively directed at TARGET POPULATION groups.
 No special high risk strategy for IDDM.
 Risk of Diabetes in NIDDM can be reduced by correcting
sedentary lifestyle, over nutrition, obesity, and avoiding
alcohol, smoking & OCPs.
Secondary Prevention
Aims :-
To maintain blood glucose levels as close within
normal limits.
To maintain ideal body weight.
Treatment :-
Diet alone – small balanced meals more frequently.
Diet and Oral Antidiabetic drugs.
Diet and Insulin.
Combination of Oral Antidiabetic drugs and Insulin.
Oral Hypoglycaemic Medications
Self-Care
 Patients should be educated to practice self-care. This
allows the patient to assume responsibility and control of
his / her own diabetes management. Self-care should
include:
◦ Blood glucose monitoring
◦ Body weight monitoring
◦ Foot-care
◦ Personal hygiene
◦ Healthy lifestyle/diet or physical activity
◦ Identify targets for control
◦ Stopping smoking
◦ Carrying Diabetic Identity card
Diabetes Identity Card
Tertiary Prevention
Aim:- Prevention of complications from occurring.
The main objective at the tertiary level is to organize
specialized clinics and units capable of providing
diagnostic and management skills at high order.
Also to be involved in Epidemiological research.
Diabetes mallitus
Diabetes mallitus

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Diabetes mallitus

  • 2.  It is a metabolic disorder of multiple etiology characterized by chronic Hyperglycaemia with disturbances of Carbohydrates, Fats and Protein metabolism resulting from defects in Insulin secretion, Insulin action or Both.
  • 3. Clinical Features  Easy Fatigability  Polyuria  Polydipsia  Wasting  Weight loss  Air hunger  Blurred vision  Poor wound healing
  • 4. Complications Acute :- Diabetic ketoacidosis. Hyperglycemic Hyperosmolar state. Chronic :- A. Microvascular B. Macrovascular C. Others
  • 5. A. Microvascular complications :- Retinopathy, Macular edema, Sensory & motor neuropathy, Autonomic neuropathy. B. Macrovascular complications :- Coronary heart disease, Peripheral arterial disease, Cerebrovascular disease. C. Others :- Cataract, Glaucoma, Periodontal disease, Hearing loss, Gastroparesis, Diarrhea, Uropathy, Sexual dysfunction, Acanthosis nigricans, Necrobiosis lipoidica, Vitiligo etc….
  • 7. Acanthosis nigricans Necrobiosis lipoidica Vitiligo Neuropathic foot ulcer Lipohypertrophy
  • 8. Types  Type 1 :- IDDM also called Juvenile Diabetes  Type2 :- NIDDM  Type3 :- Gestational Diabetes  Type4 :- Other Specific Types
  • 9. Type 1  Insulin Dependent Diabetes Mellitus.  Also called Juvenile Diabetes  Common among 10-14 yrs of age group.  Accounts for 5%-10% of all diagnosed cases of Diabetes Mellitus.  90% is Autoimmune mediated. 10% is Idiopathic.
  • 10. Type 2  Non Insulin Dependent Diabetes Mellitus.  Common among adults and elderly people.  Accounts for about 90-95% of all the diagnosed cases of Diabetes.  Begins as Insulin resistance, as the need for insulin rises, the pancreas gradually loses it’s ability to produce insulin.
  • 11. Type 3  Gestational Diabetes.  It is a condition of Glucose Intolerance diagnosed in some women during pregnancy.  Common in African americans, Latino americans, American Indians, Obese and women with family history of Diabetes.  After pregnancy, 5-10% of women with Gestational Diabetes are found to develop Type 2 Diabetes.
  • 12. Other Specific Types  Genetic defects of Beta-cell function.  Genetic defect in insulin action.  Pancreatic diseases.  Excess endogenous production of hormonal antagonist to Insulin.  Drug- Induced.  Viral infections.  Latent Autoimmune Diabetes in Adults (LADA).  Modified Onset of Diabetes in Young (MODY).
  • 13. Burden of Diabetes  Iceberg Disease.  Currently (2010) 285 million people are affected worldwide of which 20% is contributed by SEAR (China & India).  International Diabetic Federation (IDF) data indicate that the number reaches 333 million by 2025, of which 90% is Type 2.  Increased prevalence in newly Industrialized & Developing countries.  Disease is acquired in the most Productive period of Life.  Accounts for 6-12% of all Health care expenditure annually.
  • 14. Globally, the Diabetic cases crosses 300 millions by 2025.
  • 16. Risk Factors Host Factors  Age  Sex  Genetic Factors  Genetic Markers:- HLA-B8, HLA-B15, HLA-DR3 and HLA- DR4  Immune mechanism  Maternal Diabetes  Obesity
  • 17. World-wide estimated number of adults with diabetes by age group and year.
  • 18. Environmental Factors  Sedentary life style  Diet rich in Saturated Fatty acids  Decreased consumption of Diatary Fibers  Malnutrition  Alcohol  Chemical agents  Stress  Other factors
  • 19. Screening Urine examination:- LAck of Sensitivity Gives too many “False Negatives” Blood Sugar Testing:- RBS - >200mg/dl with symptoms & signs of diabetes. FBS - >126mg/dl PPBS - >200mg/dl Glycated Haemoglobin - >6.5%
  • 20. Target Population:- More than 40yrs Family history of Diabetes Obese HDL <35mg/dl and Triglycerides >250mg/dl Women who had baby weighing >4.0kg Women who show excess weight gain during pregnancy Patients with Premature Atherosclerosis
  • 21. Prevention PRIMARY PREVENTION  Population Strategy  High-Risk Strategy SECONDARY PREVENTION TERTIARY PREVENTION
  • 22. Primary Prevention POPULATION STRATEGY  The scope for primary prevention of IDDM is limited.  Based on Elimination of environmental risk factors , development of prevention programmes for NIDDM is possible. HIGH-RISK STRATEGY  Effectively directed at TARGET POPULATION groups.  No special high risk strategy for IDDM.  Risk of Diabetes in NIDDM can be reduced by correcting sedentary lifestyle, over nutrition, obesity, and avoiding alcohol, smoking & OCPs.
  • 23. Secondary Prevention Aims :- To maintain blood glucose levels as close within normal limits. To maintain ideal body weight. Treatment :- Diet alone – small balanced meals more frequently. Diet and Oral Antidiabetic drugs. Diet and Insulin. Combination of Oral Antidiabetic drugs and Insulin.
  • 25. Self-Care  Patients should be educated to practice self-care. This allows the patient to assume responsibility and control of his / her own diabetes management. Self-care should include: ◦ Blood glucose monitoring ◦ Body weight monitoring ◦ Foot-care ◦ Personal hygiene ◦ Healthy lifestyle/diet or physical activity ◦ Identify targets for control ◦ Stopping smoking ◦ Carrying Diabetic Identity card
  • 27.
  • 28. Tertiary Prevention Aim:- Prevention of complications from occurring. The main objective at the tertiary level is to organize specialized clinics and units capable of providing diagnostic and management skills at high order. Also to be involved in Epidemiological research.