Diabetes mellitus

Diabetes mellitus

Objective

•       At the end of this lecture, student will be able to explain

•       Explain the biochemical aspects of DM

•       Distinguish type 1 from type 2 DM

•       Interpret blood glucose levels in fasting states

Overview

•       DM is a heterogeneous group of syndromes characterized by  an elevation of fasting blood glucose caused by absolute or relative deficiency of insulin

•       Two types of DM:

     Type 1 (insulin-dependent DM)

     Type 2 (noninsulin dependent DM)

•       Prevalence of type 2  increasing with:

     Aging (increase in rate of life-age of population)

     Increasing prevalence of obesity

Comparison between type 1 & type 2 DM

Type 1 Diabetes Mellitus

About 10% having DM

•       Onset: usually during childhood

•       Caused by absolute deficiency of insulin :

•       may be caused by autoimmune attack of b-cells of the pancreas, viral infection or toxin

•       Destruction is enhanced by environmental factors as viral infection & a genetic 

•       Rapid symptoms appear when 80-90% of the b-cells have been destroyed

•       Insulin is the only treatment

Onset of type 1 DM

Metabolic changes of type 1 DM

1- Hyperglycemia

2- Diabetic Ketoacidosis (DKA)

3- Hypertriacylglyceridemia & hypercholestrolemia

1- Hyperglycemia:

Increased glucose in blood

Due to:

Decreased glucose uptake by muscles & adipose tissues (by GLUT-4) & Increased hepatic gluconeogenesis (& glycogenlysis)

2- DiabeticKetoacidosis (DKA):

   Increased ketone bodies in blood (ketonemia) leads to metabolic acidosis

DKA occurs in untreated or uncontrolled cases of DM

  - In 25 – 40% of newly diagnosed type 1 DM (untreated & uncontrolled yet)

  - In stress states demanding more insulin (as during infection, illness or during surgery    Uncontrolled DM)

   - No comply with therapy (intake of meals with no insulin medication i.e. Uncontrolled DM)

Diagnosis of DKA

1- History(for a cause of DKA)

2- Clinical Examination

3- Lab Investigations: (to confirm the diagnosis & follow up of treatment)

                - Urine by dipstick: Glucose & Ketones +++ (RAPID TEST)

                - Blood Chemistry Analysis:

                     * Blood Glucose: High

                               * Blood Urea:  High (due to dehydration)

                               * Electrolytes: Low (or normal) sodium

                                                         High (or normal) potassium

                               * Assessment of acid-base status: (metabolic acidosis)

                                     - Blood Bicarbonate: Low (usually below 5 mmol/L)

                                     - pCO2: Low (compensatory)

Biochemical Basis of Treatment of DKA

AIM: (EMERGENCY TREATMENT)

1- Correction of dehydration(Hypovolemia): by IV fluids & Sodium

2- Correction of acidosis: by IV bicarbonate

3- Correction of metabolic abnormality: by insulin IV infusion

4- Potassiumis given with insulin treatment as insulin induces K+ entry into cells

5- IV GLUCOSESHOULD BE STARTED IN CASE GLUCOSE IN BLOOD FALLS BELOW 10 mmol/L (AVOID HYPOGLYCEMIA INDUCED BY INSULIN)

6- FOLLOW UP is QUITE IMPORTANT to monitor

                  *Blood glucose level

                  *Electrolytes (Na+ & K+)

                  *Acid-base status (blood bicarbonatelevel)

3- Hypertriacylglyceridemia & hypercholestrolemia:

• Released fatty acids from adipose tissues are converted to triacylglycerol & cholesterol in the liver.

        Triacylglycerol is secreted from the liver in VLDL to blood (with liver cholesterol)

• Chylomicrons (from diet fat) accumulates (due to low lipoprotein lipase activity as a result of low or absent insulin)

       Chylomicrons contain Triacyglycerols (mainly) & Cholesterol

         Increased VLDL & chylomicrons in blood results in hypertriacylglyceridemia & hypercholesterolemia

Diagnosis of type 1 DM

•       Clinically:

         Age: during childhood or puberty (< 20 years of age)

         With Abrupt (Sudden) appearance of:

         Polyuria, Polydepsia, Polyphagia, Fatigue, Weight loss

         Complicationas ketoacidosis (common, may be the cause of diagnosis)

•       Laboratory diagnosis:

        Fasting blood glucose: > or equal 126 mg/dl

        100 – 125 mg/dl is called impaired fasting blood glucose

        HBA1c: High (more than 6% of normal hemoglobin)     

        Insulin level in blood: low

        Circulating islet-cell antibodies detection

Biochemical Aspects for Treatment & Control of Type 1 DM

AIM

Exogenous insulin by subcutaneous injection is given to:

1- Control Hyperglycemia (long run complications)   

2- Prevent occurrence of Ketoacidosis (emergency case!!)

 Strategies of Treatment

1- Standard Treatment

2- Intensive Treatment (Tight Control)

1- Standard Treatment:

       By one or two injections of insulin/day

AIM: Mean blood glucose level   225-275 mg/dl (normal: 110 mg/dl)

            HbA1c level:  8-9 % of total Hb (normal: 6% of total hemoglobin)

HbA1c:

     HbA1c is proportional to average blood concentration over the previous several months

      So, it provides a measure of how proper treatment normalized blood glucose in diabetic over several months

2- Intensive Treatment: (Tight control)

     By more frequent monitoring & subsequent injection of insulin 

      (i.e. 3 or more times / day)

      It will more closely normalize blood glucose to prevent chronic complications of existence of hyperglycemia for a long period.

AIM:  Mean blood glucose levels of 150 mg/dl

           HbA1c: approximately 7% of total hemoglobin

Advantage: Reduction in chances of occurrence of chronic complications of DM: e.g. retinopathy, nephropathy & neuropathy by about 60%

Complications of Treatment by Insulin

Hypoglycemia is a common complication of insulin treatment (in more than 90% of patients on insulin medication)

More Common with intensive treatment strategy

Causes of hypoglycemia due to insulin treatment

Diabetics cannot depend on glucagon or epinephrine to avoid hypoglycemia as:

No glucagon (early in the disease)

No epinephrine (with progression of the disease diabetic autonomic neuropathy with inability to secrete epinephrine in response to hypoglycemia)

So, patients with long-standing type 1 DM are particularly vulnerable to hypoglycemia

Contraindications of Intensive Treatment

•       Children: risk of episodes of hypoglycemia may affect the brain development

•       Elderly people: as hypoglycemia can cause strokes & heart attacks in older people

Type 2 Diabetes Mellitus

Type 2 DM

•       90% of diabetics (in USA)

•       Develops gradually

•       may be without obvious symptoms

•       may be detected by routine screening tests

•       BUT: many type 2 diabetics have symptoms of polyuria & polydepsia

•       In type 2 DM: a combination of insulin resistance & dysfunctional b-cells

•       Metabolic changes in type 2: are milderthan type 1, as insulin secretion, although not adequate, restrains ketoacidosis

Causes of Type 2 DM
Insulin Resistance & Dysfunctional b-cell                                                       

Insulin resistance is the decreased ability of target tissues, such as liver, adipose tissue & muscle to respond properly to normal circulating insulin

Obesity is the most common cause of insulin resistance

Obesity causes insulin resistance as:

    -  Substances produced by fat cells as leptin and resistin may contribute to development of insulin resistance

     - Free fatty acids elevated in obesity is involved in insulin resistance

Obesity, Insulin Resistance & DM

• Obesity is the most common cause for insulin resistance.

      HOWEVER, Most people with obesity & insulin resistance do notdevelop DM!!

• How insulin resistance leads to DM??

      1- In the absence of defect in b-cell function, nondiabetic, obese individuals can compensate for insulin resistance by secreting high amounts of insulin from b-cell (i.e. Hyperinsulinemia)

      So, glucose levels in blood remain within normal range

      2- In late cases, b-cell dysfunction with low insulin secretion occurs due to increased amounts of free fatty acids & other factors secreted by fat cells (as leptin & resistin) may end in development of type 2 DM (hyperglycemia).

In Type 2 DM

Initially (In early stages: with Insulin resistance) the pancreas retains b-cell capacity

â

Insulin is secreted (may be higher than normal i.e. hyperinsulinemia)

â

Normal blood glucose levels

_______________________________________________

With time (late stages)

b-cells become dysfunctional (low function)  (due to  harmful effects of  FFAs & substances released by increased fat cells)

â

b-cells failto secrete enough insulin (low insulin)

â

Increased blood glucose levels (hyperglycemia)

 

Metabolic changes in Type 2 DM

 Metabolic abnormalities of type 2 DM are the results of insulin resistance (in liver, muscle & adipose tissue)

1- Hyperglycemia

2- Hypertriacylglyceridemia

3- Nonketotic hyperglycemic coma

In cases with severe hyperglycemia especially in older age diabetics type 2

Hyperglycemia induces osmotic diuresis with loss of ECF

The osmotic diuresis causes loss of water in excess of sodium leading to very high plasma osmolality (with hypernatremia) & marked dehydration

No ketgenesis due to presence of sufficient insulin to prevent DKA (or sometimes there is minimal ketogenesis with minimal metabolic acidosis i.e. Bicarbonate is not much lowered as in DKA)

Treatment:

Fluid replacement + Insulin IV infusion + follow up (Emergency Case!!)

Chronic Effects of DM

The long-standing hyperglycemia causes the chronic complications of DM

 1- Atherosclerosis: DiabeticRetinopathy

                                           Diabetic Nephropathy: glomerular proteinuria

                                           Diabetic Neuropathy: peripheral neuritis

                                           Cardiovascular Diseases (as MI) & strokes (as cereb. hge)

   2- Sorbitolaccumulation in certain cells with its complications

   3- Glycated proteins formation with microvascular complications

For avoiding these complications, long-term control of hyperglycemia is recommended for all types of DM

In cells where entry of glucose is notdependent on insulin (eye lens, retina, kidney, neurones)

â

á Intracellular Levels of Glucose

â

á SORBITOL accumulation in these cells

â

Cataract

Diabetic Retinopathy

Diabetic Nephropathy

Diabetic Neuropathy

Treatment of Type 2 DM

•       AIM: 

      1- To maintain blood glucose concentrations within normal limits

      2- To prevent the development of long-term complications occurring due to prolonged hyperglycemia

•       Lines of treatment:

       1- Weight reduction (to control insulin resistance)

       2- Exercise

       3- Dietary modification

       4- Hypoglycemic agents

       5- Insulin (required in somecases)

Case Study

Parents of a 15 years old boy was reported by his school that he was found drowsy & they have got to take him to hospital according to the advice of his school doctor. 

In the hospital, his mother told the doctor that her son seemed unusually thirsty for the last 3 months & she thought that he had lost weight. She admitted also that on the morning before leaving for school, he was complaining of abdominal pain & discomfort.

On examination:

• Semiconscious 
• Deep & rapid respiration 
• Pulse rate 120 beats/minute
• BP: 90/50
• Cold extremities

What investigations were recommended for him??

What is the diagnosis of this case??

What is the treatment??

Clinical Biochemistry Lab Investigations

Blood Chemistry

Random Blood Glucose:  550 mg/dl

Urea: 160 mg/dl      (N: 20 -40)

Na+:   127 mmol/L (N: 135 – 145)

K+:  6.9 mmol/L       (N: 3.5 – 4.5)

pCO2:  2.9  kPa        (N: 4.4 – 6.1)

HCO3- :  7 mmol/L  (N: 21 – 27.5)

pO2:  14 kPa             (N: 12 – 17)

Urine Analysis:

Urine Dipstick Test:

        - Glucose +++ 

        - Ketone +++

        - Albumin ++

Summary

•       Type 1 is insulin depended

•       Type 2 is insuling independent

•       Complications are more dangerous

•       Lab abnormalities

–      Altered sugar values

–      Proteinuria

–      HbA₁C