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University Hospital Galway

Dr Verena Gounden

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diabetes mellitus diabetic ketoacidosis medical notes

Summary

These notes cover monitoring diabetes mellitus, including complications like diabetic ketoacidosis and chronic complications. The presentation also discusses normal fasting ketosis, ketosis in diabetes, ketoacidosis, and different lab investigations. It also touches on volume status and potassium disturbances.

Full Transcript

# Monitoring Diabetes Mellitus ## Dr Verena Gounden Consultant Chemical Pathologist Galway University Hospitals ## Overview - Monitoring related to complications - Acute: Diabetic Ketoacidosis - Chronic: Renal, Atherosclerotic/dyslipidaemia - Lab investigations used for monitoring - Self...

# Monitoring Diabetes Mellitus ## Dr Verena Gounden Consultant Chemical Pathologist Galway University Hospitals ## Overview - Monitoring related to complications - Acute: Diabetic Ketoacidosis - Chronic: Renal, Atherosclerotic/dyslipidaemia - Lab investigations used for monitoring - Self monitoring ## Diabetic Ketoacidosis - In about 25% of T1DM patients, their ability to compensate for their insulin deficiency has failed at presentation due to: - delayed presentation - inability to respond to thirst - intercurrent illness - These patients present with a more severe metabolic disturbance known as diabetic ketoacidosis - This is life-threatening condition in which severe insulin deficiency leads to: - Hyperglycaemia (usually >25 mmol/L) - Ketosis (usually > 3 mmol/L) - Metabolic Acidosis - Volume Depletion & Shock - Electrolyte disturbances - Additional symptoms to those described earlier include: - Abdominal pain, nausea, vomiting - Variable effects on mental status from drowsiness with profound lethargy to coma ## Normal Fasting Ketosis - In the fasting state, as plasma glucose levels drop, the pancreas stops producing insulin - Lack of insulin increases lipolysis in adipose tissue with the release of fatty acids into the bloodstream - Fatty acids can be metabolised as an energy source by most tissues (fatty acid β-oxidation) - However, free fatty acids cannot cross the blood brain barrier - Therefore, in the fasting state fatty acids are also oxidised in the liver to 'ketone bodies', acetoacetate & β-hydroxybutyrate, which can be used as an energy source by the brain & other tissues. After 3-4 day fast, ketone bodies provide 30-40% of the body's energy requirements - Acetoacetate can undergo spontaneous decarboxylation to acetone which gives rise to a characteristic fruity odour from breath associated with fasting ## Ketosis in Diabetes - In untreated T1DM, the hormonal milieu is similar to fasting: - severe insulin deficiency can give rise to a ketosis similar to fasting - excessive ketone production can be detected in urine (ketonuria) & blood (ketonemia) - As in fasting, acetone gives rise to a characteristic fruity odour from breath ## Ketoacidosis in Diabetes - Markedly elevated levels of acetoacetate & β-hydroxybutyrate (ketoacids) induce a metabolic acidosis - pH will be low, in severe cases dropping below 7.0 (RR 7.35-7.45) - H+ increasing from 40 to 100nmol/L! - Acidosis is largely buffered by converting: - HCO3¯ + H+→ H2CO3 → H2O + CO2 - HCO3 usually falls less than 10 mmol/L at presentation (RI 22-29 mmol/L) - Characteristic compensatory hyperventilation with slow deep breaths (Kussmaul's respirations) in an effort to remove CO2 ## Raised anion gap metabolic acidosis - If unsure of cause of metabolic acidosis, the anion gap is a simple diagnostic tool - Anion gap = Na+ - (CI¯ + HCO3¯) - In DKA, the anion gap may be 20-40 mmol/L (RI <15 mmol/L) - due to the unmeasured anions (β-hydroxybuyrate & acetacetate) - Other causes of raised anion gap metabolic acidosis include: - Lactic acidosis (secondary to severe dehydration & shock) - Starvation ketosis - Alcoholic ketoacidosis - Uremic acidosis in renal failure - Toxic ingestions (salicylate, methanol, ethylene glycol) ## Volume Status - Volume contraction is a hallmark of diabetic ketoacidosis - Driven by hyperosmolality secondary to hyperglycaemia - Mild diabetic ketoacidosis - Osmotic diuresis - Movement of H2O from the intracellular to extracellular space - Partially counterbalanced by polydipsia - Severe diabetic ketoacidosis - Inability to maintain fluid balance (babies, elderly, sick) - Fluid deficits of 5-10 L are common - Hypovolaemic shock - Lactic acidosis, uraemic acidosis - Hypotension - Rapid, weak, thready pulse - Thirst & dry mouth - Cold & mottled skin ## Potassium disturbance - Factors ↑ extracellular fluid (ECF) K+ - Shift of K+ to extracellular space due to acidosis (H + exchanged for K+ in ECF) - Insulin required to stimulate Na+/K+ ATPase - Factors ↓ ECF K + - Increased K+ excretion due to raised plasma K + - secondary hyperaldosteronism - occasionally vomiting - Commonly N/↑ plasma K+ masking a total body K+ deficiency - Both hyper- & hypokalaemia can result in cardiac arrhythmias ## Pathogenesis of DKA and HHS; Triggers include stress, infection, and insufficient insulin. FFA: free fatty acid; HHS: hyperosmolar hyperglycemic state From: Kitabchi AE, Umpierrez GE, Miles JM, et al. Diabetes Care. 2009, 32:1335-43; used with permission | | | | | | :-------------------- | :------------------------------- | :---------------------------------- | :-------------------- | | **Absolute Insulin Deficiency** | **Counterregulatory Hormones** | **Relative Insulin Deficiency** | | | ↑ Lipolysis | Protein synthesis | Absent or minimal ketogenesis | | | ++ | ↑Proteolysis | | | | ↑ FFA to liver | ↑Gluconeogenic substrates | | | | ↑ Ketogenesis | ↑Gluconeogenesis | ↑Glycogenolysis | | | Alkali reserve | | | | | ↑ Ketoacidosis | | | | | Triacylglycerol | | | | | Hyperlipidemia | | | Hyperosmolarity | | | Hyperglycaemia | | | | | Glycosuria (osmotic diuresis) | | | | | Loss of water and electrolytes | | | | | ↓ | | | | | Dehydration | | | | | Decreased fluid intake | | | | | Impaired renal function | | | | | | | **DKA** | | | | | **HHS** | Ref Diabetic ketoacidosis - Etiology | BMJ Best Practice US ## Chronic Complications - The long term management of diabetes is to minimise the risk of the patient developing chronic complications - All the main complications of diabetes seem to stem from effects on the vasculature - **Microvascular disease** - Retinopathy (leading cause of blindness) - Nephropathy (leading cause of end stage renal disease) - Neuropathy - **Atherosclerosis** - Coronary artery disease - Cerebrovascular accidents - Peripheral vascular disease - There are a variety of modifications that patient's need to make to minimise these risks - Good glucose control - Smoking cessation - Healthy lifestyle habits (nutrition, exercise) - Controlling hypertension - Managing dyslipidaemia ## DCCT: A1C and Microvascular Complications - A chart shows a graph of relative risk versus HbA1c (mmol/l) for Retinopathy, Nephropathy, Neuropathy, Microalbumin. The values on the x axis (HbA1c, mmol/l) go from 42 to 108, split into increments of 11. - The y axis (Relative Risk) goes from 1 to 15. For HbA1c values of 42-75, the Relative Risk value for the four conditions is mostly negligible. For HbA1c values of 75-108, the Relative Risk value increases with increasing HbA1c values. - **Skyler JS. Endocrinol Metab Clin North Am. 1996;25:243-254.** ## Kidney Disease ## Diabetic Kidney Disease - DM is the most common predisposing factor for developing chronic kidney disease and requiring dialysis - **Urinary Albumin Excretion Rate (AER, ACR a.k.a. microalbuminuria)** - This is a marker of dysfunction of the renal glomeruli as it indicates that albumin is leaking through the damaged glomeruli - It may present intermittently in T1DM 3-5 years after first diagnosis and over time in some patients becomes persistent. - Its presence and quantity are risk factors for chronic kidney disease - risk marker for other microvascular & atherosclerotic diseases - **Glomerular Filtration Rate** - While a reduction in glomerular filtration rate can have multiple causes, a reduction of GFR over time in diabetes usually indicates a loss of functioning nephrons - While there are methods available to directly measure GFR, in clinical practice this is usually estimated based on the serum creatinine of the patient - The calculation used in our laboratory takes into account the gender and age of the patient. No factors for the race are utilised (in keeping with current guidelines) - **Other** - Kidney Failure Risk Equation (KFRE) risk prediction tool for a kidney replacement therapy in the next two or five years in individuals with chronic kidney disease (CKD) stages 3a-5 ## CKD Classification CKD is classified based on: - Cause (C) - GFR (G) - Albuminuria (A) | GFR categories (ml/min/1.73m²) Description and range | GFR | Albuminuria categories Description and range | A1 | A2 | A3 | | :-------------------------------------------------- | :-- | :------------------------------------------- | :------------- | :------------- | :------------- | | G1 Normal or high | ≥90 | | 1 if CKD | Treat | Refer** | | G2 Mildly decreased | 60-89 | | 1 if CKD | Treat | Refer** | | G3a Mildly to moderately decreased | 45-59 | | Treat | Treat | Refer | | G3b Moderately to severely decreased | 30-44 | | Treat | Treat | Refer | | G4 Severely decreased | 15-29 | | Refer* | Refer* | Refer | | G5 Kidney failure | <15 | | Refer | Refer | Refer | ## Atherosclerotic Disease - Similar to atherosclerosis in non-diabetic subjects, but more rapidly progressive and extensive - Insulin resistance and hyperglycaemia both accelerate atherosclerosis by instigating endothelial cell dysfunction and dyslipidaemia ## Diabetic Dyslipidaemia - Insulin resistance results in: - Increasing free fatty acid (FFA) release from adipose tissue - FFA are are converted to triglycerides in liver and repackaged as Very Low Density Lipoprotein (VLDL) - Metabolism of the excess VLDL results in low levels of HDL and increased numbers of small dense LDL particles which predispose diabetics to atherosclerosis - This risk can be managed through good diabetic control and the use of lipid modifying drugs such as statins - Diabetic dyslipidaemia is usually monitored using routine lipid profile parameters - Total & LDL cholesterol often normal & falsely reassuring as routine tests don't clearly identify patients with an increased number of proatherogenic small dense LDL particles that contain little cholesterol - However this can usually be inferred as these patients generally have low HDL cholesterol levels and raised triglyceride levels ## Monitoring ### Lab Investigations - **HbA1c** - used to: - Monitor long-term glycaemic control - Evaluate and adjust therapy - Measure risk for the development of microvascular complications - Screen for and diagnose diabetes - Assess quality of diabetes care - Evaluate new medications for diabetes - Available formal lab and point of care testing (POCT not for diagnosis) - **Alternatives to HbA1c** - Role when the use of HbA1c is limited due to clinical reasons eg Hgb variants - These are not standardised, not widely available - No evidence based – clinical decision/limits of cut-points currently - Examples Fructosamine, glycated albumin ### Self monitoring: Glucose Monitoring - There are several self-monitoring devices shown. - **ONETOUCH VeriolQ** - **CONTOUR** - **ACCU-CHEK Aviva** - **FreeStyle Lite** - **ACCU-CHEK Mobile** ### Continuous Glucose Monitoring - An image shows: - A device which is attached to the skin - A smartphone with a graph showing a glucose reading of 110 mg/dL - An Apple Watch with graph showing a glucose reading of 110 mg/dL - **NUM System with Share and the ollow apps are available in the US only** ### Graphing Glycaemic Control - Two graphs show glucose (mmol/L) versus Time (00:00 - 22:00) - The graphs shows the curves of Glucose readings throughout the day. - The graph indicates the 10th to 90th percentile, and the 25th to 75th percentile. - The median value has been plotted on the graph and has been indicated. - The target range for glucose reading has also been indicated on the graph. ### Ketone Meters - There are three Ketone Meters shown in the image. - **CareTouch Gen** - **Nova Max** - **Precision Xtra** ## Case Scenarios

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