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Fanconi syndrome consists of multiple defects in renal proximal tubular reabsorption, causing glucosuria, phosphaturia, generalized aminoaciduria, and HCO3 wasting. Symptoms in children are failure to thrive, growth retardation, and rickets. Symptoms in adults are osteomalacia and muscle weakness. Diagnosis is by showing glucosuria, phosphaturia, and aminoaciduria. Treatment is HCO3 replacement and measures directed at renal failure.
Etiology
Fanconi syndrome can be
Hereditary Fanconi syndrome:
This disorder usually accompanies another genetic disorder, particularly cystinosis. Cystinosis is an inherited (autosomal recessive) metabolic disorder in which cystine accumulates within cells and tissues (and is not excreted to excess in the urine as occurs in cystinuria—see Congenital Renal Transport Abnormalities: Cystinuria). Besides renal tubular dysfunction, other complications of cystinosis include eye disorders, hepatomegaly, hypothyroidism, and other manifestations.
Fanconi syndrome may also accompany Wilson disease, hereditary fructose intolerance, galactosemia, glycogen storage disease, oculocerebrorenal syndrome (Lowe syndrome), mitochondrial cytopathies, and tyrosinemia. Inheritance patterns vary with the associated disorder.
Acquired Fanconi syndrome:
This disorder may be caused by various drugs, including certain cancer chemotherapy drugs (eg, ifosfamide, streptozocin), antiretrovirals (eg, didanosine, cidofovir), and outdated tetracycline. All of these drugs are nephrotoxic. Acquired Fanconi syndrome also may occur after renal transplantation and in patients with multiple myeloma, amyloidosis, intoxication with heavy metals or other chemicals, or vitamin D deficiency.
Pathophysiology
Various defects of proximal tubular transport function occur, including impaired resorption of glucose, phosphate, amino acids, HCO3, uric acid, water, K, and Na. The aminoaciduria is generalized, and, unlike that in cystinuria, increased cystine excretion is a minor component. The basic pathophysiologic abnormality is unknown but may involve a mitochondrial disturbance. Low levels of serum phosphate cause rickets, which is worsened by decreased proximal tubular conversion of vitamin D to its active form.
Symptoms and Signs
In hereditary Fanconi syndrome, the chief clinical features—proximal tubular acidosis, hypophosphatemic rickets, hypokalemia, polyuria, and polydipsia—usually appear in infancy.
When Fanconi syndrome occurs because of cystinosis, failure to thrive and growth retardation are common. The retinas show patchy depigmentation. Interstitial nephritis develops, leading to progressive renal failure that may be fatal before adolescence.
In acquired Fanconi syndrome, adults present with the laboratory abnormalities of renal tubular acidosis (proximal type 2), hypophosphatemia, and hypokalemia. They may present with symptoms of bone disease (osteomalacia) and muscle weakness.
Diagnosis
Diagnosis is made by showing the abnormalities of renal function, particularly glucosuria (in the presence of normal serum glucose), phosphaturia, and aminoaciduria. In cystinosis, slit-lamp examination may show cystine crystals in the cornea.
Treatment
Other than removing the offending nephrotoxin, there is no specific treatment. Acidosis may be lessened by giving tablets or solutions of Na or K HCO3 or citrate, eg, Shohl's solution (Na citrate and citric acid; 1 mL is equivalent to 1 mmol of HCO3) given 1 mEq/kg bid to tid or 5 to 15 mL after meals and at bedtime. K depletion may require replacement therapy with a K-containing salt. Hypophosphatemic rickets can be treated (see Congenital Renal Transport Abnormalities: Hypophosphatemic Rickets). Renal transplantation has been successful in treating renal failure. However, when cystinosis is the underlying disease, progressive damage may continue in other organs and eventually result in death.
Key Points
Last full review/revision April 2013 by James I. McMillan, MD
Content last modified April 2013
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