Clinical Signs and Symptoms of Refeeding Syndrome
References
Pathogenesis of refeeding syndrome
How does refeeding syndrome develop?
Prolonged fasting:
During prolonged fasting, hormonal and metabolic changes are aimed at preventing protein and muscle breakdown.
Muscle and other tissues decrease their use of ketone bodies and use fatty acids as the main energy source. This results in an increase in blood levels of ketone bodies, stimulating the brain to switch from glucose to ketone bodies as its main energy source.
The liver decreases its rate of gluconeogenesis, thus preserving muscle protein. During the period of prolonged starvation, several intracellular minerals become severely depleted. However, serum concentrations of these minerals (including phosphate) may remain normal. This is because these minerals are mainly in the intracellular compartment, which contracts during starvation. In addition, there is a reduction in renal excretion.
Refeeding:
During refeeding, glycaemia leads to increased insulin and decreased secretion of glucagon. Insulin stimulates glycogen, fat, and protein synthesis. This process requires minerals such as phosphate and magnesium and cofactors such as thiamine. Insulin stimulates the absorption of potassium into the cells through the sodium-potassium ATPase symporter, which also transports glucose into the cells. Magnesium and phosphate are also taken up into the cells. Water follows by osmosis. These processes result in a decrease in the serum levels of phosphate, potassium, and magnesium, all of which are already depleted.
The clinical features of the refeeding syndrome occur as a result of the functional deficits of these electrolytes and the rapid change in basal metabolic rate.
Patients at high risk of refeeding syndrome
Patient populations at risk for refeeding syndrome include those with:
· anorexia nervosa and other restrictive eating disorders,
· chronic conditions causing malnutrition (cancer, congenital heart disease),
· malabsorptive syndromes (inflammatory bowel disease, cystic fibrosis),
· High stress patient unfed for >7 days.
· cerebral palsy
· bariatric surgery
· bowel resections
· Patients with uncontrolled diabetes mellitus (electrolyte depletion, diuresis).
· Long term users of antacids (magnesium and aluminum salts bind phosphate)
· Long term users of diuretics (loss of electrolytes).
Early identification of high-risk patients is crucial. The NICE guidelines provide a useful tool in this regard:
Results from a deletion of a region of chromosome 7q11.23, containing the elastin gene.
Manifestations and picture:
· Affected individuals often present with poor feeding and hypercalcaemia as a neonate (resolve in 2nd year).
· Elfin facies (full cheeks, full lower lip (fish-shaped), long philtrum) sometimes a stellate iris.
· Medial eyebrow flare, Depressed nasal bridge, Epicanthic folds
· Cardiac: The elastin deletion causes arteriopathy, which can affect any artery, but the characteristic lesion is supravalvular aortic stenosis, peripheral Pulmonary artery stenosis.
· Child: outgoing (cocktail party speech, Friendly manner), adult: withdrawn
· Mild-to-moderate learning difficulties
· Short stature
· Hypoplastic nails
· Skeletal: Scoliosis, kyphosis, Joint limitations
· Renal: renal artery stenosis, Nephrocalcinosis, Pelvic kidney, Urethral stenosis
