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Journal club of Sulaimania
General Teaching Hospital
         Prepared by
    Dr. Mohamed Shekhani.
Introduction
• It is the metabolic abnormality of type 1 diabetes.
• Near patient testing for the ketones is now readily available for
  monitoring allowing for a shift away from using glucose levels to
  drive treatment decisions in the management of DKA.
• National UK guidelines have been developed to reflect the
  development in technology.
• They are evidence based where possible but are also drawn from
  accumulated multiprofessional knowledge & consensus agreement.
Pathophysiology & diagnosis
• Usually occurs as a consequence of insulin deficiency.
• This enhances hepatic glucose production.
• Enhanced fat breakdown increases serum free fatty acids that are then
  metabolised producing large quantities of ketones & metabolic acidosis.
• Fluid depletion is a serious problem caused by osmotic diuresis.
• Electrolyte shifts & depletion are, in part, related to the osmotic
  diuresis.
• Hyper & hypokalaemia are particular dangers.
• Absolute diagnostic criteria do not exist, but the following are proposed:
• Ketonaemia =>3 mmol/l by ketone meter, or significant ketonuria (> 2+
  on standard urine sticks)
• BS >11 mmol/l or known DM
• Venous bicarbonate (HCO3)< 15 mmol/l &or venous pH <7.3.
Developments in management
• Recent developments now allow us to focus on:
• The underlying abnormality (ketonaemia), which simplifies the treat-
  ment of those who present with modest elevation of blood glucose but
  with acidosis secondary to ketonaemia ‘euglycaemic diabetic
  ketoacidosis’.
• Blood glucose is routinely checked at the bedside, but portable ketone
  meters now also allow bedside measurement of 3-beta-hydroxybutyrate.
• The resolution of DKA depends upon the suppression of ketonaemia,
  therefore the measurement of blood ketones now represents best
  practice in monitoring the response to treatment.
• Access to blood gas& blood electrolyte measurements is now usually
  available within a few minutes of blood being taken.
• Glucose, ketones and electrolytes,including bicarbonate&venous pH,
  should be assessed at, or near, the bedside.
DM specialist teams:
• (DST) involvement shortens patient stay and improves outcomes.
• All patients should be reviewed by a member of the DST prior to
  discharge, not undertaking this is a governance issue.
General management issues:
• The most important initial therapeutic intervention is appropriate
  fluid replacement followed by insulin administration.
• The main aims of fluid replacement are to:
• Restore circulatory volume.
• Clear ketones.
• Correct electrolyte imbalance.
• The aim of the first few litres of fluid is to correct any
  hypotension, replenish the intravascular deficit &counteract the
  effects of the osmotic diuresis with rectification of electrolyte
  disturbance.
• In RF or HF, elderly& adolescents, the rate / volume of fluid
  replacement may need to be modified.
Severity assessment:
• The presence of one or more of the following may indicate severe
  DKA &admission to a level 2/high dependency unit environment;
  insertion of CVL& immediate senior review should be considered:
• Blood ketones>6 mmol/l
• Bicarbonate level < 5 mmol/l
• Venous/arterial pH < 7.1
• Hypokalaemia on admission (< 3.5 mmol/l)
• Glasgow Coma Scale <12 or abnormal AVPU (Alert,Voice, Pain,
  Unresponsive) scale
• Oxygen saturation < 92% on air (assuming normal baseline
  respiratory function)
• Systolic BP<90 mmHg
• PR>100 or <60 bpm.
Insulin therapy& metabolic treatment targets:
• A fixed rate IV insulin infusion (FRIVII) calculated on 0.1
  units/kg infusion is recommended.
• Patient demographics are changing&patients with DKA are now
  more likely to be obese or suffering with other insulin-resistant
  states, including pregnancy leading to the re-emergence of FRIVII
  in adults.
• The FRIVII may need to be adjusted; the recommended targets
  are:
• Reduction of the blood ketone concentration by 0.5 mmol/l/hour
• If ketone meter not available, the venous bicarbonate should rise
  by 3 mmol/l/hour& capillary blood glucose fall by 3 mmol/l/hour
• Potassium should be maintained between 4.0 -5.0 mmol/l.
IV glucose concentration:
• The management should be focused on clearing ketones as well as
  normalising blood glucose.
• It is often necessary to administer an (iv) infusion of 10% glucose
  via an iv pump in order to avoid hypoglycaemia&permit the
  continuation of a FRIVII to suppress ketogenesis.
• Introduction of 10% glucose is recommended when the blood
  glucose falls below 14 mmol/l.
• It is important to continue 0.9% sodium chloride solution concur-
  rently via an iv pump.
Continuation of long-acting insulin analogues:
• Continuation of long-acting analogues (insulin detemir –
  Levemir®, insulin glargine – Lantus®) during the initial
  management of DKA provides background insulin when the iv
  insulin is discontinued&avoids rebound hyperglycaemia when iv
  insulin is stopped &avoids excess length of stay.
Serious complications:
• Hypokalaemia&hyperkalaemia are potentially life-threatening
  conditions during the management of DKA.
• There is a risk of ARF associated with severe dehydration therefore no
  potassium be prescribed with the initial fluid resuscitation or if the
  serum potassium level remains above 5.5 mmol/l.
• Potassium will almost always fall as the DKA is treated with insulin,
  thus it is recommended that 0.9% sodium chloride solution with
  potassium 40 mmol/l (ready-mixed) is prescribed as long as the serum
  potassium <5.5 mmol/l & the patient is passing urine.
• If the serum potassium falls below 3.5 mmol/l the potassium regimen
  needs review.
• All aspects of potassium use must comply with local & national
  guidance.
• Other serious complications include cerebral &pulmonary.
• Close attention to fluid balance&slower fluid replacement is recom-
  mended for younger adults; for children <18 years of age.
Conclusion & summary:
• DKA is a medical emergency with a significant morbidity&mortality.
• It is now recommended that FRIVII be used with bedside measurement
  of metabolic parameters.
• The DST should always be involved as soon as possible and ideally
  within 24 hours because this has been demonstrated to be associated
  with a better patient experience &reduced length of stay.
• In the management of diabetic ketoacidosis the following guidance
  should therefore be followed:
• Measure blood ketones, venous (not arterial) pH & bicarbonate & use
  results as treatment markers
• Monitor ketones &glucose using bedside meters, when available &
  operating within their quality assurance range
• Monitor electrolytes on blood gas analysers with intermittent laboratory
  confirmation
• Replace ‘sliding scale’ insulin with weight-based FRIVII
• Involve the DST as soon as possible
• Continue long-acting insulin analogues as normal.

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Med j club dka.

  • 1. Journal club of Sulaimania General Teaching Hospital Prepared by Dr. Mohamed Shekhani.
  • 2. Introduction • It is the metabolic abnormality of type 1 diabetes. • Near patient testing for the ketones is now readily available for monitoring allowing for a shift away from using glucose levels to drive treatment decisions in the management of DKA. • National UK guidelines have been developed to reflect the development in technology. • They are evidence based where possible but are also drawn from accumulated multiprofessional knowledge & consensus agreement.
  • 3. Pathophysiology & diagnosis • Usually occurs as a consequence of insulin deficiency. • This enhances hepatic glucose production. • Enhanced fat breakdown increases serum free fatty acids that are then metabolised producing large quantities of ketones & metabolic acidosis. • Fluid depletion is a serious problem caused by osmotic diuresis. • Electrolyte shifts & depletion are, in part, related to the osmotic diuresis. • Hyper & hypokalaemia are particular dangers. • Absolute diagnostic criteria do not exist, but the following are proposed: • Ketonaemia =>3 mmol/l by ketone meter, or significant ketonuria (> 2+ on standard urine sticks) • BS >11 mmol/l or known DM • Venous bicarbonate (HCO3)< 15 mmol/l &or venous pH <7.3.
  • 4. Developments in management • Recent developments now allow us to focus on: • The underlying abnormality (ketonaemia), which simplifies the treat- ment of those who present with modest elevation of blood glucose but with acidosis secondary to ketonaemia ‘euglycaemic diabetic ketoacidosis’. • Blood glucose is routinely checked at the bedside, but portable ketone meters now also allow bedside measurement of 3-beta-hydroxybutyrate. • The resolution of DKA depends upon the suppression of ketonaemia, therefore the measurement of blood ketones now represents best practice in monitoring the response to treatment. • Access to blood gas& blood electrolyte measurements is now usually available within a few minutes of blood being taken. • Glucose, ketones and electrolytes,including bicarbonate&venous pH, should be assessed at, or near, the bedside.
  • 5. DM specialist teams: • (DST) involvement shortens patient stay and improves outcomes. • All patients should be reviewed by a member of the DST prior to discharge, not undertaking this is a governance issue.
  • 6. General management issues: • The most important initial therapeutic intervention is appropriate fluid replacement followed by insulin administration. • The main aims of fluid replacement are to: • Restore circulatory volume. • Clear ketones. • Correct electrolyte imbalance. • The aim of the first few litres of fluid is to correct any hypotension, replenish the intravascular deficit &counteract the effects of the osmotic diuresis with rectification of electrolyte disturbance. • In RF or HF, elderly& adolescents, the rate / volume of fluid replacement may need to be modified.
  • 7. Severity assessment: • The presence of one or more of the following may indicate severe DKA &admission to a level 2/high dependency unit environment; insertion of CVL& immediate senior review should be considered: • Blood ketones>6 mmol/l • Bicarbonate level < 5 mmol/l • Venous/arterial pH < 7.1 • Hypokalaemia on admission (< 3.5 mmol/l) • Glasgow Coma Scale <12 or abnormal AVPU (Alert,Voice, Pain, Unresponsive) scale • Oxygen saturation < 92% on air (assuming normal baseline respiratory function) • Systolic BP<90 mmHg • PR>100 or <60 bpm.
  • 8. Insulin therapy& metabolic treatment targets: • A fixed rate IV insulin infusion (FRIVII) calculated on 0.1 units/kg infusion is recommended. • Patient demographics are changing&patients with DKA are now more likely to be obese or suffering with other insulin-resistant states, including pregnancy leading to the re-emergence of FRIVII in adults. • The FRIVII may need to be adjusted; the recommended targets are: • Reduction of the blood ketone concentration by 0.5 mmol/l/hour • If ketone meter not available, the venous bicarbonate should rise by 3 mmol/l/hour& capillary blood glucose fall by 3 mmol/l/hour • Potassium should be maintained between 4.0 -5.0 mmol/l.
  • 9. IV glucose concentration: • The management should be focused on clearing ketones as well as normalising blood glucose. • It is often necessary to administer an (iv) infusion of 10% glucose via an iv pump in order to avoid hypoglycaemia&permit the continuation of a FRIVII to suppress ketogenesis. • Introduction of 10% glucose is recommended when the blood glucose falls below 14 mmol/l. • It is important to continue 0.9% sodium chloride solution concur- rently via an iv pump.
  • 10. Continuation of long-acting insulin analogues: • Continuation of long-acting analogues (insulin detemir – Levemir®, insulin glargine – Lantus®) during the initial management of DKA provides background insulin when the iv insulin is discontinued&avoids rebound hyperglycaemia when iv insulin is stopped &avoids excess length of stay.
  • 11. Serious complications: • Hypokalaemia&hyperkalaemia are potentially life-threatening conditions during the management of DKA. • There is a risk of ARF associated with severe dehydration therefore no potassium be prescribed with the initial fluid resuscitation or if the serum potassium level remains above 5.5 mmol/l. • Potassium will almost always fall as the DKA is treated with insulin, thus it is recommended that 0.9% sodium chloride solution with potassium 40 mmol/l (ready-mixed) is prescribed as long as the serum potassium <5.5 mmol/l & the patient is passing urine. • If the serum potassium falls below 3.5 mmol/l the potassium regimen needs review. • All aspects of potassium use must comply with local & national guidance. • Other serious complications include cerebral &pulmonary. • Close attention to fluid balance&slower fluid replacement is recom- mended for younger adults; for children <18 years of age.
  • 12. Conclusion & summary: • DKA is a medical emergency with a significant morbidity&mortality. • It is now recommended that FRIVII be used with bedside measurement of metabolic parameters. • The DST should always be involved as soon as possible and ideally within 24 hours because this has been demonstrated to be associated with a better patient experience &reduced length of stay. • In the management of diabetic ketoacidosis the following guidance should therefore be followed: • Measure blood ketones, venous (not arterial) pH & bicarbonate & use results as treatment markers • Monitor ketones &glucose using bedside meters, when available & operating within their quality assurance range • Monitor electrolytes on blood gas analysers with intermittent laboratory confirmation • Replace ‘sliding scale’ insulin with weight-based FRIVII • Involve the DST as soon as possible • Continue long-acting insulin analogues as normal.