1. Unexplained Rhabdomyolysis: �A Step Too Far? Sarah Hatch
Senior Clinical Biochemist
Royal Liverpool Hospital
2. The Patient 25 year old female student
Non-smoker, no alcohol
Originally from Zimbabwe (2002)
No recent travel (3 years)
3. Presentation A&E Assessment:
Loss of appetite
Persistent nausea
Vomiting 10x daily
Weakness and lethargy
Lower back pain
Mild fever
Previously well
4. Initial Examination Temperature 36.7 oC
Heart rate 95 beats/min
Respiratory rate 14 breaths/min
Blood pressure 114/78 mmHg
Glasgow coma scale 15/15
Sterno-subcostel pain
Radiating to the back
Related to standing and walking
5. Previous Medical History Heavy fall down stairs two weeks earlier
No loss of consciousness
Mild bruising and lower back pain
Attended A&E
Analgesia
Co-codamol
30 mg codeine phosphate
500 mg paracetamol
x2 QDS
Celecoxib
NSAID, COX-2 inhibitor
200 mg OD
6. Biochemistry
7. Acute Renal Failure ? Pre-renal:
Secondary to hypovolaemia
Persistent vomiting
Co-codamol
Hepatorenal syndrome
? Intrinsic:
Secondary to NSAIDs
Celecoxib
Sepsis
Mild febrile illness
Sickle cell anaemia
Glomerulonephritis
Rhabdomyolysis
Injury 2/52 ago, no significant bruising
8. Urinalysis Patient stated no haematuria
Output 30 - 50 mL/hour
Darkly coloured
pH 6.0
Strongly positive for protein (3+)
> 3 g/L
Strongly positive for blood (3+)
Colorimetric detection of peroxidase activity
Equally sensitive to haemoglobin and myoglobin
Detects red cells
9. Renal ultrasound: echobright kidneys consistent with diffuse parenchymal disease, no obstruction
10. “Add-On” Investigation Acute renal failure
secondary to rhabdomyolysis
11. Creatine Kinase 82 kDa dimeric enzyme
2500 U/g protein in skeletal muscle
97 - 99% CK-3 (MM)
1 - 3 % CK-2 (MB)
< 1% CK-1 (BB)
Non-cardiac source
12. Damage to skeletal muscle may take various forms. Crush injuries damage muscle cells directly, as well as impairing the blood supply; other causes may damage muscle cells by interfering with their metabolism. The muscle tissue rapidly fills with fluid from the bloodstream, as well as sodium and chloride. The swelling itself may lead to destruction of muscle cells, but those cells that survive react by pumping sodium out of the cells in exchange for calcium (through the sodium-calcium exchanger). The accumulation of calcium in the sarcoplasmic reticulum leads to continuous muscle contraction and depletion of ATP (the main source of energy); calcium also stimulates phospholipase A2, and the production of free radicals. In addition, neutrophil granulocytes (the most abundant white blood cells) enter the muscle tissue, perpetuating an inflammatory reaction and releasing further free radicals. A phospholipase is an enzyme that converts phospholipids into fatty acids and other lipophilic substances. Phospholipase A2 - cleaves the SN-2 acyl chain Damage to skeletal muscle may take various forms. Crush injuries damage muscle cells directly, as well as impairing the blood supply; other causes may damage muscle cells by interfering with their metabolism. The muscle tissue rapidly fills with fluid from the bloodstream, as well as sodium and chloride. The swelling itself may lead to destruction of muscle cells, but those cells that survive react by pumping sodium out of the cells in exchange for calcium (through the sodium-calcium exchanger). The accumulation of calcium in the sarcoplasmic reticulum leads to continuous muscle contraction and depletion of ATP (the main source of energy); calcium also stimulates phospholipase A2, and the production of free radicals. In addition, neutrophil granulocytes (the most abundant white blood cells) enter the muscle tissue, perpetuating an inflammatory reaction and releasing further free radicals. A phospholipase is an enzyme that converts phospholipids into fatty acids and other lipophilic substances. Phospholipase A2 - cleaves the SN-2 acyl chain
13. The swollen and inflamed muscle may directly compress structures in the same fascial compartment, causing compartment syndrome. The swelling may also further compromise blood supply into the area. Finally, destroyed muscle cells release potassium, phosphate, myoglobin (a heme and therefore iron-containing protein), creatine kinase (an enzyme) and uric acid (a breakdown product of purines from DNA) into the blood. Activation of the coagulation system may precipitate diffuse intravascular coagulation. High potassium levels (hyperkalemia) may lead to potentially fatal disruptions in heart rhythm. Phosphate precipitates with calcium from the circulation, leading to hypocalcemia (low calcium levels). Compartment syndrome is an acute medical problem following injury or surgery in which increased pressure (usually caused by inflammation) within a confined space (fascial compartment) in the body impairs blood supply,without prompt treatment, leading to nerve damage and muscle death The swollen and inflamed muscle may directly compress structures in the same fascial compartment, causing compartment syndrome. The swelling may also further compromise blood supply into the area. Finally, destroyed muscle cells release potassium, phosphate, myoglobin (a heme and therefore iron-containing protein), creatine kinase (an enzyme) and uric acid (a breakdown product of purines from DNA) into the blood. Activation of the coagulation system may precipitate diffuse intravascular coagulation. High potassium levels (hyperkalemia) may lead to potentially fatal disruptions in heart rhythm. Phosphate precipitates with calcium from the circulation, leading to hypocalcemia (low calcium levels). Compartment syndrome is an acute medical problem following injury or surgery in which increased pressure (usually caused by inflammation) within a confined space (fascial compartment) in the body impairs blood supply,without prompt treatment, leading to nerve damage and muscle death
14. Myoglobin 17.8 kDa haem protein
Renal clearance
Freely filtered
Endocytosis and proteolysis in proximal tubule
0.01 - 5.0 % filtered load in urine
Rhabdomyolysis
Reabsorption saturated
Red-brown discoloured urine
Renal damage
Obstructive casts formed in acidic conditions
Haem toxic to renal tubules
Acute tubular necrosis and renal failure The pathophysiology of myoglobinuric ARF has been extensively studied in an animal model of glycerol-induced ARF. The main mechanisms involved are renal vasoconstriction, intraluminal cast formation and direct heme protein-induced cytotoxicity. Renal vasoconstriction is favored by muscle necrosis, which leads to hypovolemia and the activation of cytokines. This increases capillary permeability and the binding of heme protein to nitric oxide: the endothelium relaxing factor. Casts are produced after the filtration of myoglobin through the glomerular basement membrane, which causes water reabsorption and a rise in myoglobin concentration. Following this, in the presence of acidic urine, myoglobin precipitation takes place and causes obstructive cast formation. Dehydration and renal vasoconstriction favor this process, through increased tubule reabsorption of sodium and water, which consequently increases myoglobin concentration in the tubules.The pathophysiology of myoglobinuric ARF has been extensively studied in an animal model of glycerol-induced ARF. The main mechanisms involved are renal vasoconstriction, intraluminal cast formation and direct heme protein-induced cytotoxicity. Renal vasoconstriction is favored by muscle necrosis, which leads to hypovolemia and the activation of cytokines. This increases capillary permeability and the binding of heme protein to nitric oxide: the endothelium relaxing factor. Casts are produced after the filtration of myoglobin through the glomerular basement membrane, which causes water reabsorption and a rise in myoglobin concentration. Following this, in the presence of acidic urine, myoglobin precipitation takes place and causes obstructive cast formation. Dehydration and renal vasoconstriction favor this process, through increased tubule reabsorption of sodium and water, which consequently increases myoglobin concentration in the tubules.
15. Clinical Sequelae Of Rhabdomyolysis Acute renal failure
Renal vasoconstriction, acute tubular necrosis
Rapid deterioration, slow recovery
Falling creatine kinase suggests single acute muscle insult
16. Hyperkalaemia
Release of cellular potassium
Impaired renal excretion
Dialysis withheld
18. Principles Of Management Fluid resuscitation
Catherisation
Oral and 1.4 % intravenous sodium bicarbonate
Maintain urine > pH 7 to prevent
tubular precipitation of myoglobin
Renal replacement therapy
Dialysis
Haemofiltration
19. Causes Of Rhabdomyolysis: �Differential Diagnosis Physical
Direct muscle damage
Impaired blood supply
Prolonged immobilisation
Seizures
Electric shock
Burns
Ischemia or necrosis
Extreme exertion
Inflammatory
Infections
Polymyositis
Dermatomyositis
20. Final Diagnosis: Inconclusive Minor bruising on buttocks
Autoimmune disease negative
ANCA and anti-GBM
Sickle cell disease negative
Haemoglobin electrophoresis
Not medication
21. Awaiting Neurological Referral Investigation for underlying metabolic myopathy
Glycogen storage disease
Type V (McArdles, glycogen phosphorylase)
Fatty acid oxidation defect
Carnitine-palmitoyl transferase deficiency
Mitochondrial defect
No background history
Exercise intolerance
Muscle cramps
Discoloured urine
22. Outcome Further investigations
Muscle biopsy
Electromyography
Acyl carnitines
Enzyme analysis
Possible long-term renal impairment
12 weeks post admission:
Creatinine = 58, Urea = 4.3, CK = 124
24. Biochemical Response Relatively slow improvement in plasma glucose.
Became hypokalaemic despite K+ supplements.
Rehydration slowly decreased Na+, urea, creatinine…
Bicarbonate low indicating persistence of underlying acidosis.Relatively slow improvement in plasma glucose.
Became hypokalaemic despite K+ supplements.
Rehydration slowly decreased Na+, urea, creatinine…
Bicarbonate low indicating persistence of underlying acidosis.
