9- Paediatric Endocrinology 1/2)

Question 1

normal blood glucose

Answer 1

Ideal blood glucose : 4.4 and 6.1 mmol/l

Question 2

T1DM background

Answer 2

• Pancreas doesn’t produce enough insulin
• Lack of insulin causes high blood glucose

Question 3

Pathophysiology T1DM

Answer 3

• Insulin is produced by beta cells in the islets of Langerhans in the pancreas
• Insulin reduces blood sugar in two ways
  1) Allows cells to absorb glucose to use as fuel
  2) Causes muscle and liver cells to absorb glucose and convert it glycogen for storage
• Ketogenesis occurs when there is insufficient glucose and glycogen stores are exhausted e.g. prolonged fasting
  1) Involves converting fatty acids into ketones
  2) Ketones can be used as fuel (characteristic acetone breath)

Question 4

Risk factors T1DM

Answer 4

• Genetic
• Viral triggers e.g. coxsackie and enterovirus

Question 5

presentation of T1DM

Answer 5

• In Diabetic ketoacidosis
• Triad of symptoms of hyperglycaemia
  o Polyuria
  o Polydipsia
  o Weight loss
• Recurrent infections

Question 6

investigations for T1DM

Answer 6

• Baseline bloods including FBC, renal profile (U&E) and a formal laboratory glucose
• Blood cultures should be performed in patients with suspected infection (i.e. with fever)
• HbA1c can be used to get a picture of the blood sugar over the previous 3 months. This gives an idea of how long they have been diabetic prior to presenting.
• Thyroid function tests and thyroid peroxidase antibodies (TPO) to test for associated autoimmune thyroid disease
• Tissue transglutaminase (anti-TTG) antibodies for associated coeliac disease
• Insulin antibodies, anti-GAD antibodies and islet cell antibodies to test for antibodies associated with destruction of the pancreas and the development of type 1 diabetes

Question 7

diagnostic criteria for T1DM

Answer 7

Normal range- 3.3- 7 mmol/l

• Symptoms (polyuria, polydipsia, fatigue) retinopathy, neuropathy etc) plus one abnormal result or
• Two abnormal results at different times (at least week)
• Glucose levels
  o Fasting >7.0 mmol/l and/or
  o 2 hours after 75g glucose >11.1 mmol/l
  o Hba1c >6.5%

Question 8

fasting blood glucose above

Answer 8

> 7.0 mmol/l suggests diabetes mellitus

Question 9

oral glucose tolerance test

Answer 9

2h after 75g of glucose >11.1 mmol

Question 10

Hba1C above

Answer 10

> 6.5% or 48mmol

Question 11

management of T1DM

Answer 11

• Education
  o Exercise
  o Diet
  o Carbohydrate and Glucose monitoring with BM
• Subcutaneous insulin regimes
• Monitoring and management of both short and long term complications

Question 12

short term complications

Answer 12

• hypoglycaemia
• nocturnal hypoglycaemia
• hyperglycaemia and DKA

Question 13

hypoglycaemia

Answer 13

Presentation: hunger, tremor, sweating, irritability, dizziness and pallor
- Severe: unconsciousness, coma and death

Management
- Rapid acting glucose e.g. Lucozade and slower acting carbs e.g. biscuits
- If severe: IV dextrose and IM glucagon

Question 14

nocturnal hypoglycaemia

Answer 14

• Presentation: sweaty at night
• Management: altering bolus insulin regimes

Question 15

Hyperglycaemia and DKA

Answer 15

• Management of hyperglycaemia: will need insulin dose increased
• Management of DKA: inpatient management (see later)

Question 16

long term complications of T1DM

Answer 16

Damage to endothelial cells of blood vessels and suppression of the immune system.
- macrovascular
- microvascular
- ingection related complications

Question 17

macrovascular complications

Answer 17

o CAD
o Peripheral ischaemia e.g. diabetic foot
o Stroke
o Hypertension

Question 18

microvascular complications

Answer 18

o Peripheral neuropathy
o Retinopathy
o Nephropathy e.g. glomerulosclerosis

Question 19

Infection related complications

Answer 19

UTI, pneumonia, skin and soft tissue infections, candidiasis

Question 20

normal insulin prescription in children invovles

Answer 20

• Long acting given once a day
• Short acting given 30 mins before meals

Question 21

Basal bolus regimes

Answer 21

1) Basal: long acting insulin e.g. Lantus
- Typically given in evening

2) Bolus: short acting e.g. Actrapid
- 3 times a day before meals or when carbohydrates consumed

Question 22

what are replacing basal bolus regimes in children

Answer 22

insulin pumps

Question 23

insulin pumps

Answer 23

Devices which continuously infuse insulin at different rates to control blood sugar

Procedure: pump with cannula inserted in skin which pushes insulin under the skin. Cannula replaced every 2-3 days and insertion site rotates
- Child >12

Advantages
- Better glucose control

Disadvantages
- Difficulties learning to use
- Having it attached at all times
- Infection

2 types
o Tethered
o Patch

Question 24

complications of insulin

Answer 24

Lipodystrophy
- Patients should rotate site of injection
- Tissues can harden and prevents normal absorption of insulin

Hypoglycaemia

Question 25

monitoring blood glucose in T1DM involves

Answer 25

HbA1C
capillary blood glcuose
flash glucose monitoring e.g. FreeStyle libre

Question 26

HbA1c

Answer 26

• Measures glycated haemoglobin
• Reflects average BG over past 3 months since they have a lifespan of 120 (3 months) days
• Measured every 3-6 months to track

Question 27

Capillary blood glucose

Answer 27

o Measured using glucose meter
o Immediate result
o Used to self-test before insulin admin

Question 28

Flash glucose monitoring e.g. FreeStyle Libre

Answer 28

• Sensor on the skin which measures glucose in interstitial fluid and subcut tissue
• 5 min lag behind blood glucose (still require FGM), but measures at intervals to give a good impression of what glucose is doing over time
• Reader and sensor system (sensor replaced every 2) weeks
• Expensive

Question 29

Diabetic ketoacidosis

Answer 29

Background
A life threatening, medical emergency. It is the most common way that children with a new diagnosis of type 1 diabetes present.

Question 30

Pathophysiology

Answer 30

• T1DM- not enough insulin and therefore cant use glucose
• Ketoacidosis, dehydration and potassium imbalance is what kills patients

Question 31

Ketoacidosis

Answer 31

• Due to starvation picture, ketones produced by the liver to use as fuel
• Overtime glucose and ketones rise
• Ketones are acidic, therefore the kidneys produce bicarbonate to buffer the ketone acids in the blood and maintain normal pH
• Overtime ketone acids use up bicarbonate and blood becomes acidic

Question 32

Dehydration

Answer 32

• Hyperglycaemia overwhelms kidneys and glucose starts being filtered into the urine
• Glucose in urine draw water out due to osmotic diuresis – polyuria – severe hydration - polydipsia

Question 33

potassium imbalance

Answer 33

• Insulin drives potassium into cells
• Without insulin potassium is not stored in cells
• Causes high potassium, however this is then excreted in the urine – meaning total body potassium is low due to no storage
• When insulin is started- > hypokalaemia -> arrhythmia

Question 34

Presentation of DKA

Answer 34

• Polyuria
• Polydipsia
• Nausea and vomiting
• Weight loss
• Acetone smell to their breath
• Dehydration and subsequent hypotension
• Altered consciousness
• Symptoms of an underlying trigger (i.e. sepsis)

Question 35

Investigations for DKA

Answer 35

• Hyperglycaemia (i.e. blood glucose > 11 mmol/l)
• Ketosis (i.e. blood ketones > 3 mmol/l)
• Acidosis (i.e. pH < 7.3)

Question 36

ketogenesis

Answer 36

normally occurs when there is an insufficient supply of glucose and glycogens stores are exhausted.
- This may happen during prolonged fasting or very low carbohydrate diets

Question 37

process of ketogenesis

Answer 37

The liver takes fatty acids and converts them to ketones.

• Ketones are water soluble fatty acids that can be used as fuel.
• They can cross the blood brain barrier and be used by the brain.
• Producing ketones is normal and not harmful in healthy patients when under fasting conditions or on a very low carbohydrate, high fat diet.
• Ketone levels can be measured in the urine using a urine dipstick and in the blood using a ketone meter.
• People in ketosis have a characteristic acetone smell to their breath.

Question 38

why does ketogenesis cause metabolic acidosis in DKA

Answer 38

• Ketone acids (ketones) are buffered in normal patients so the blood does not become acidotic. When underlying pathology (i.e. type 1 diabetes) causes extreme hyperglycaemic ketosis, this results in a metabolic acidosis that is life threatening. This is called diabetic ketoacidosis.

Question 39

Management of DKA

Answer 39

1. Correct dehydration evenly over 48 hours. This will correct the dehydration and dilute the hyperglycaemia and the ketones. Correcting it faster increases the risk of cerebral oedema.
2. Give a fixed rate insulin infusion This allows cells to start using glucose again. This in turn switches off the production of ketones.

Other important principles:

• Avoid fluid boluses to minimise the risk of cerebral oedema, unless required for resuscitation.
• Treat underlying triggers, for example with antibiotics for septic patients.
• Prevent hypoglycaemia with IV dextrose once blood glucose falls below 14mmol/l.
• Add potassium to IV fluids and monitor serum potassium closely.
• Monitor for signs of cerebral oedema.
• Monitor glucose, ketones and pH to assess their progress and determine when to switch to subcutaneous insulin.

Question 40

why can cerebral oedema occur when treatment DKA

Answer 40

o Dehydration and high blood sugar concentration cause water to move from the intracellular space in the brain to the extracellular space.
o This causes the brain cells to shrink and become dehydrated.
o Rapid correction of dehydration and hyperglycaemia (with fluids and insulin) causes a rapid shift in water from the extracellular space to the intracellular space in the brain cells.
o This causes the brain to swell and become oedematous, which can lead to brain cell destruction and death.

Question 41

cerebral oedema management

Answer 41

- Neurological observations (i.e. GCS) should be monitored very closely (e.g. hourly) to look for signs of cerebral oedema. Be concerned when patients being treated for diabetic ketoacidosis develop headaches, altered behaviour, bradycardia or changes to consciousness.

Management options for cerebral oedema are
- slowing IV fluids
- IV mannitol
- IV hypertonic saline.

Question 42

Type 2 diabetes mellitus background

Answer 42

T2DM is a multifactorial and heterogeneous condition in which the balance between insulin sensitivity and insulin secretion is impaired. The condition is characterized by hyperinsulinemia; however, there is relative insulin insufficiency to overcome underlying concomitant tissue insulin resistance.
- Increasing incidence in developed countries
- Parallels upward trend in childhood obesity
- In US 45% of new diabetes cases in children are T2DM

Question 43

pathophysiology of T2DM

Answer 43

Not autoimmune
- No association with HLA-linked genes

RF
- Obesity
- Family history of T2DM
- Ethnic origin
 Asian
 African-American
 Afro-Caribbean
 Pacific islander
- PCOS
- Small for gestational age

Question 44

presentation of T2DM

Answer 44

• Hyperglycaemia
• Typical manifestation of insulin deficiency e.g.
  o Polydipsia
  o Polyuria
• Presentations of DKA may occasionally be seen

Question 45

investigations for T2DM

Answer 45

• presence of T2DM risk factors
• lack of absolute/persistent insulin deficiency;
• absence of pancreatic autoantibodies.

Question 46

first line management of T2DM

Answer 46

• Educational support
  o diet
  o exercise
• Manage obesity and comorbiditiesa
• Screening and management of T2DM comorbidities such as hyperlipidaemia and hypertension

Question 47

second line management of t2DM

Answer 47

when lfiestyle interventions have failed
METFORMIN (like adults)

MOA- works by decreasing glucoseneogenesis and increasing sensivity to insulin

Question 48

third line management of T2DM

Answer 48

Insulin therapy

Question 49

Diabetes insipidus
Background

Answer 49

Posterior pituitary gland secretes two hormones
1) Oxytocin
2) Antidiuretic hormone (ADH)

DI caused by deficiency in ADH (cranial) or resistance to its actions in the kidney (nephrogenic)
- Cranial more common
- Can be acquired or inherited

Question 50

Pathophysiology Cranial DI

Answer 50

Damage to hypothalamus or pit gland
- Brain injury e.g. tumour, surgery, infection
- Genetic causes e.g. neurohypophysis diabetes insipidus

Question 51

pathophysiology nephrogenic DI

Answer 51

• Kidney failure
• Sickle cell
• Polycystic kidney disease
• Lithium
• Genetic causes

Question 52

RF DI

Answer 52

• Brain tumour
• Head injury

Question 53

presentation of DI

Answer 53

• Large volumes of dilute urine (<300mOsm/L)- polyuria
• Polydipsia
• Nocturia
• Colourless urine
• Weak muscles
• Hypernatremia
• Dehydration
• Death
• Infant specific (hereditary)
  o Failure to thrive
  o Fever
  o Constipation

Question 54

Investigations for DI

Answer 54

• 24 hour urinary volume and osmolality
  o >3l
  o High serum osmolality (>300 mOsm) and
  low urine osmolality (<300 mOsm)
• DM and renal failure should also be excluded
• Water deprivation test

Question 55

water deprivation test

Answer 55

A water deprivation test involves not drinking any liquid for several hours to see how your body responds. If you have diabetes insipidus, you’ll continue to pee large amounts of dilute urine when normally you’d only pee a small amount of concentrated urine
* high plasma osmolality, low urine osmolality
* a urine osmolality of >700 mOsm/kg excludes diabetes insipidus
* water deprivation test
* cranial: urine osmolality will increase after desmopressin
* nephrogenic: urine osmolality will not change

Question 56

management of cranial DI

Answer 56

• Synthetic analogues of ADH- desmopressin (intranasal or oral)
• Dose titrated to patient
• Patient education about hazards of excessive water intake

Question 57

managment of nephrogenic DI

Answer 57

• Underlying cause should be reversed, if symptoms persist patient should drink according to thirst and keep with water loss
• Low salt, low protein diet, thiazide diuretics and NSAIDS