Autoimmune hyperphosphatemic tumoral calcinosis

“…is a rare disorder of phosphate metabolism caused by mutations in genes related to Fibroblast Growth Factor-23 (FGF23), which include FGF23 itself, an FGF23glycosylating enzyme, N-acetylgalactosaminyltransfer ase 3 (GALNT3), and the FGF23 co-receptor α-Klotho (αKL) (1). The altered gene function decreases FGF23 synthesis or activity and causes increased renal tubular reabsorption of phosphate, thereby increasing blood calcium-phosphate product, which leads to predisposition for soft-tissue calcification (2).…”

“…The most common manifestation of HFTC is calcinosis cutis, which appears clinically as firm, otherwise asymptomatic, white, yellowish or flesh-colored papules, plaques, or nodules. The clinical course is often associated with excretion of chalky material, pain, itching, ulceration, or infection of the lesions (1).…”

“…Only about 75 patients of genetically confirmed HTFC have been reported (1). The majority (about 80%) have mutations in the GALNT3 gene followed by the FGF23 gene (about 20%) and the KL gene (1).…”

“…Therefore, the FGF23 protein is readily cleaved into biologically inactive N-terminal and C-terminal fragments (c-FGF23). The loss of FGF23 activity leads to hyperphosphatemia typical of HFTC (1). The circulating concentrations of c-FGF23 are increased whereas the intact FGF23 (i-FGF23) remains low or inappropriately normal for the level of hyperphosphatemia (1).…”

A novel homozygous variant in exon 10 of the <i>GALNT3</i> gene causing hyperphosphatemic familial tumoral calcinosis in a family from North India

“…is a rare disorder of phosphate metabolism caused by mutations in genes related to Fibroblast Growth Factor-23 (FGF23), which include FGF23 itself, an FGF23glycosylating enzyme, N-acetylgalactosaminyltransfer ase 3 (GALNT3), and the FGF23 co-receptor α-Klotho (αKL) (1). The altered gene function decreases FGF23 synthesis or activity and causes increased renal tubular reabsorption of phosphate, thereby increasing blood calcium-phosphate product, which leads to predisposition for soft-tissue calcification (2).…”

“…The most common manifestation of HFTC is calcinosis cutis, which appears clinically as firm, otherwise asymptomatic, white, yellowish or flesh-colored papules, plaques, or nodules. The clinical course is often associated with excretion of chalky material, pain, itching, ulceration, or infection of the lesions (1).…”

“…Only about 75 patients of genetically confirmed HTFC have been reported (1). The majority (about 80%) have mutations in the GALNT3 gene followed by the FGF23 gene (about 20%) and the KL gene (1).…”

“…Therefore, the FGF23 protein is readily cleaved into biologically inactive N-terminal and C-terminal fragments (c-FGF23). The loss of FGF23 activity leads to hyperphosphatemia typical of HFTC (1). The circulating concentrations of c-FGF23 are increased whereas the intact FGF23 (i-FGF23) remains low or inappropriately normal for the level of hyperphosphatemia (1).…”

A novel homozygous variant in exon 10 of the <i>GALNT3</i> gene causing hyperphosphatemic familial tumoral calcinosis in a family from North India

“…As PTH has a significant influence on promoting phosphaturia, loss of PTH caused by hypoparathyroidism or peripheral resistance to its action (pseudohypoparathyroidism) can produce elevated phosphate levels [21]. Familial tumoral calcinosis, an autosomal recessive disease caused by a mutation in the GALNT3, FGF23 or klotho gene, is characterised by resistance to FGF23, which also leads to hyperphosphataemia [40]. Increased levels of growth hormone and insulin-like growth factor 1 (Igf-1) seen in acromegaly stimulate phosphate reabsorption in the PCT.…”

Calcium, Phosphate and Magnesium Disorders

A Cross‐Sectional Cohort Study of the Effects of FGF23 Deficiency and Hyperphosphatemia on Dental Structures in Hyperphosphatemic Familial Tumoral Calcinosis