Clinical Biochemistry 2

Question 1

Total proteins in diagnostics.

Answer 1

Comprises albumin and globulin fractions.
Measure globulins by subtracting albumin from total protein.
Ratio between albumin and globulin can narrow down the differentials list.
Estimated by ‘total solids’ (TS) on refractometer.
- TS also incorporates other solids – cholesterol, glucose, urea, (but not electrolytes – hence raised baseline). (Rough estimate).

Question 2

Specific other proteins to consider.

Answer 2

Acute phase proteins – that increase and decrease in inflammation. E.g. CRP.
Can be used as worry-metres.
Clotting factors.

Question 3

1. Albumin size, charge and activity.
2. Where is albumin synthesised?
3. Albumin protein type?
4. Albumin function?
5. What analytes are albumin-bound?
6. Why does relative hyperalbuminemia occur?

Answer 3

1. Large (65kDa), negatively charged (Repelled from glomerular surface so does not cross glomerulus very well), osmotically-active.
2. Liver.
3. Negative acute phase protein.
4. Maintaining colloid oncotic pressure – so a decrease in inflammatory state will cause a loss of water from the blood.
5. Calcium – changes in albumin affect total calcium readings (as ~1/2 circulating calcium stuck to albumin).
   Thyroid hormones.
   Steroids and fatty acids.
6. Haemoconcentration often as a result of dehydration (also increased total protein).

Question 4

What can cause hypoalbuminemia?

Answer 4

Reduced absorption so malnutrition; GI disease.
Reduced production
- Hepatic dysfunction
- APP (acute phase protein) response
Increased loss
- Protein losing enteropathy (PLE). E.g. parvo. (albumin and globulins lost at same time so + and - charge).
- Protein losing nephropathy (PLN). Albumin-selective.
- Haemorrhage. E.g. RTA, fleas, ticks, GI, renal.
- Severe exudative disease incl. third-spacing e.g. ascites (+/- losses via drainage). E.g. burns.

Question 5

Hypoproteinaemia differentials.

Answer 5

Hypoproteinaemia.
Distinguish whether pan-hypoproteinaemia or isolated hypoalbuminemia.
If pan-hypoproteinaemia, consider:
- haemorrhage.
- Severe exudative disease.
- protein losing enteropathy.
- third spacing.
If isolated hypoalbuminemia, consider:
- mild-moderate.
- mild-marked.
If mild-moderate:
- (negative) APP response.
If moderate-marked:
- liver failure.
- protein losing nephropathy.
- protein losing enteropathy (w/ inflammatory component).

Question 6

How can the differentials for hypoproteinaemia be worked through?

Answer 6

With haematology, serum biochemistry, liver function testing, urinalysis, advanced imaging.

Question 7

1. What are globulins?
2. What type of globulin contributes most to globulin fraction? – Where are these synthesised?
3. Causes of hypoglobulinaemia?

Answer 7

1. Every other protein other than albumin in serum/plasma. They are mostly very large proteins.
   There are alpha, beta and gamma globulins.
2. Gamma globulins, which are antibodies (aka immunoglobulins) – synthesised by B-lymphoid (plasma) cells.
3. Immunological incompetency e.g. failure of passive transfer (colostrum ingestion).
   Protein loss (w/ concurrent hypoalbuminemia).
   – Caused by haemorrhage, exudative disease, and PLE (NB. not in PLN or liver disease).

Question 8

1. What causes hyperglobulinaemia?
2. Differentiation between types?

Answer 8

1. Mild-moderate commonly accompanies inflammatory / infectious diseases.
   - APP response.
   - Polyclonal gammopathy (diverse antigen stimulation).
   Marked (less commonly mild-moderate) secondary to B-cell neoplasia (e.g. multiple myeloma; lymphoma).
2. Serum protein electrophoresis (SPE).

Question 9

Hyperglobulinaemia investigative pathway.

Answer 9

Distinguish if mild-moderate or moderate-marked.
If mild-moderate, consider whether:
- Other features of inflammation present and evaluate for inflammatory / infectious disease e.g. immune-mediated, severe skin / dental disease.
- No other evidence of inflammation so consider moderate-marked differentials.
If moderate-marked:
- Run serum protein electrophoresis:
– If monoclonal, evaluate for B-cell neoplasia (most likely). Very rarely chronic inflammatory disease causes monoclonal (or restricted oligoclonal) gammopathies.
– If polyclonal, review for inflammatory / infectious disease e.g. leishmaniosis, ehrlichiosis, FIP.

Question 10

1. What happens to negative APPs in inflammation?
2. Give examples of negative APPs.
3. What happens to positive APPs in inflammation?
4. Give examples of positive APPs.

Answer 10

1. Decrease.
2. Albumin and transferrin (iron sequestered –> inhibits RBC production).
3. Increase.
4. C-RP (dogs)
   serum amyloid A (SAA) in horses (pre-racing inflammation).
   a1-acid glycoprotein (A1-AGP) – cats.
   Haptoglobin – ruminants.

Question 11

1. How is glucose acquired?
2. What if inadequately supplied?
3. Use?
4. Normal glucose range for dogs and cats?
5. How glucose glucose controlled in the body?
6. What happens when glucose levels drop too low?
7. ” “ increase to too high?

Answer 11

1. Ingestion in diet and end product of carbohydrate breakdown.
2. Synthesised in the liver.
3. Utilised by all cells (incl. bacteria) for energy.
4. 3.5-5.0 mmol/L.
5. Under hormone control.
   Insulin is released in response to hyperglycaemia.
   Various hormones (importantly glucagon and catecholamines e.g. adrenaline) released in response to hypoglycaemia or rapidly decreasing glucose concentrations.
6. Ultimately coma, seizure, death.
7. Osmotic impact on blood.
   Cuts and abrasions more likely to become infected with bacteria.

Question 12

1. Glucose measurement.
2. Mild postprandial hyperglycaemia.

Answer 12

1. Point of care (in-house) glucometers.
   Lab via biochemistry machine (external).
   Where there is a delay between sampling and testing, ideally use OxF tubes. So the cells in the sample do not get a chance to use up the glucose that is in that sample.
2. Fasted samples from cats and dogs.
   Consider stress as well e.g. urine samples to be taken from felines days after vet appts and not straight away.
   Avoid fasting equine spp.
   Fasted samples not possible in ruminants.
   – in lactating cows, mammary vein glucose lower than jugular vein glucose.

Question 13

1. In what breeds is hypoglycaemia commonly seen? – Why?
2. Hypoglycaemia differentials?

Answer 13

1. Toy breeds – Low fat (and therefore glycogen) reserves so if stop eating for reasons such as GI disease, likely to become hypoglycaemic, often to the point of loss of consciousness.
2. Inadequate synthesis due to:
   - hepatic dysfunction / portosystemic shunting.
   - hypoadrenocorticism (Addisons).
   Excessive consumption e.g. sepsis.
   Excess hypoglycaemic agents.
   - insulin (syringes, persons).
   - Xylitol (toxicity). – sweet taste kick starts insulin where it is not needed.
   - Oral hypoglycaemics e.g. w/ diabetic owner or newer diabetic drugs.
   Paraneoplastic e.g. insulinoma, hepatomas, IGF-2 producing tumours. OR massive cancer using up a lot of glucose for energy.

Question 14

Investigating hypoglycaemia.

Answer 14

Consider signalment.
Liver dysfunction / portovascular anomaly e.g. shunt.
- Routine blood analysis –> ammonia, BAST –> advanced imaging.
Hypoadrenocorticism.
- Basal cortisol (screen) –> ACTH stim (diagnostic).
Sepsis
- T-FAST / A-FAST / other imaging.
Neoplasia
- imaging – hepatoma; IGF-2 producing tumours (typically smooth muscle); insulinoma (pancreas and metastasis).
- glucose WITH insulin (NB: during hypoglycaemia as insulin release may be episodic). –> insulin conc. appropriate?

Question 15

Hyperglycaemia causes?

Answer 15

Transient (i.e. physiological)
- Stress-associated hyperglycaemia common in cats.
- Post-prandial (monogastrics).
Persistent (i.e. pathological)
- Diabetes mellitus = insulin insufficiency.
– glucosuria; =/- ketonaemia / ketonuria; usually increase serum fructosamine.
- Pre-diabetes mellitus (w/ potential to progress).
– obesity
– steroids –> exogenous vs endogenous (hyperadrenocorticism; pars pituitary intermedia dysfunction).
– Hypersomatotropism (i.e. acromegaly) – overproduction of GH due to brain tumour.

Question 16

Investigating hyperglycaemia

Answer 16

Consider signalment.
Interpret in conjunction:
- urine glucose
– in conjunction w/ hyperglycaemia, indicates persistent hyperglycaemia above renal threshold (10mmol/L in dogs, 14-17mmol/L in cats).
– NB: If stress hyperglycaemia suspected, measure at home >24 hours after event.
- Fructosamine
– irreversibly glycated albumin.
– reflects glycaemic status over the preceding 2-3 weeks (may be normal in very recent onset diabetes mellitus).
– Increased turnover w/ hyperthyroid / hypoalbuminaemic / azotaemic.

Question 17

Ketones – cause.

Answer 17

Negative energy balance (inadequate carb provision) –> lipolysis –> ketone bodies.
- Starvation / prolonged anorexia.
- Diabetes mellitus (glucose provision, cannot use in absence of insulin).
- Ruminant ketosis – cattle e.g. lactation demands, displaced abomasum.
- Pregnancy toxaemia – sheep.
Beta-hydroxybutyric acid.
- Most common ketone body in cats / dogs / cattle / sheep.
- BHB not measured by urine ‘Diastix’ as human optimised.
- Other ketone bodies (acetone, acetoacetate) produced in lower concentrations.

Question 18

Non-esterified fatty acids (NEFAs).

Answer 18

Marker of lipolysis – mostly used in assessment of energy balance in ruminants (alongside ketones).
Can be seen increased due to pre-prandial sample taken, stress, or due to delayed sample analysis.
Can be seen increased due to negative energy balance – food deprivation, excess demands (lactation, pregnancy), hepatic lipidosis.
Interpret with ketones (BHB) and glucose.

Question 19

What 2 types of fats are in the body?

Answer 19

Cholesterol and triglycerides.

Question 20

1. What is cholesterol used for in the body?
2. What are serum cholesterol levels dependent on?

Answer 20

1. Cell membrane formation.
   Steroid / sex hormone pathways.
   Vit D metabolism.
   Bile acid metabolism.
2. Dietary intake.
   Hepatic synthesis.
   Excretion in bile.

Question 21

1. Composition of triglycerides.
2. Main sites of triglyceride synthesis.
3. Reason for triglyceride increase?
4. Reason for triglyceride reduction?

Answer 21

1. 3 long fatty acids and a glycerol.
2. Enterocytes (from diet).
   Adipocytes (from fat).
   Hepatocytes.
3. Post-prandial.
   Increased hormone sensitive lipase.
4. Lipoprotein lipase.

Question 22

Hyperlipidaemia – increased triglycerides and cholesterol.

Answer 22

Increased supply through diet so occurs post-prandially or through high fat diet.
Altered metabolism or increased production.
- exogenous steroids can increase cholesterol.
- endocrinopathy can increase cholesterol e.g. hypothyroidism; DM; hyperadrenocorticism.
- nephrotic syndrome increases cholesterol.
- negative energy balance (esp horses, camelids) can increase triglycerides.
- hepatic lipidosis can increase triglycerides.
Decreased excretion
- cholestasis.
Hereditary dyslipidaemias – e.g. hypertriglyceridaemia of miniature schnauzers.

Question 23

Hyperlipidaemia investigative pathway

Answer 23

Fed or not?
Fast 24 hrs.
If hyperlipidaemia resolved by fasting, then is post-prandial.
If persists, consider:
- obesity.
- cholestasis. (imaging)
- endocrinopathy.
- PLN. urinalysis helpful.
*if all these excluded, consider:
- pars pituitary intermedia dysfunction (horses).
- hyperadrenocorticism / exogenous steroids.
- DM.
- hypothyroidism (dogs).

Question 24

Hypocholesterolaemia causes.

Answer 24

Artefact (severe icterus).
Decreased supply
- fat-restricted diet.
- malabsorption
– intestinal diseased (esp w/ PLE).
– exocrine pancreatic insufficiency.
Reduced production
- liver dysfunction e.g. portovascular anomaly.
Increased losses / utilisation.
- blood loss.
- cancer – haemophagocytic disease; histiocytic sarcoma; multiple myeloma; lymphoma.
Hypoadrenocorticism (Addisons) – mechs unclear.