Kidney Stones Clinical Trial
Official title:
A Cross-Sectional Study To Investigate The Role Of FGF23, Klotho, And Sclerostin In Kidney Stone Formers
Kidney stones are very common in industrialized countries and the lifetime risk is about 10 to 15% in this population. Kidney stones are composed of inorganic and organic components. Calcium containing stones are the most common stone type accounting for more than 80% of kidney stones. Many factors predispose or contribute to the development of kidney stones, including genetic variants or mutations, diet, environmental factors, and behavior. To date, little is known on fibroblast growth factor (FGF23) levels in patients with calcium nephrolithiasis. FGF23 is crucial for phosphate homeostasis including physiological and pathophysiological conditions such as X-linked hypophosphatemic rickets and it seems that FGF23 is probably the most important regulator of serum phosphate and calcitriol (1,25(OH)2D3) levels in addition to parathyroid hormone (PTH) produced by the parathyroid gland. Novel factors such as Klotho and Sclerostin, which are involved in the bone-kidney-parathyroid endocrine axis, have been identified recently. Klotho is a putative aging suppressor gene and its deficiency results in osteopenia, hyperphosphaturia, and calcification. Klotho is mainly expressed in the kidney but also in the parathyroid gland and acts as a FGF23 specific co-receptor mediating FGF23 participation in the bone-kidney-parathyroid endocrine axis as described above. Sclerostin is a protein secreted by osteocytes that inhibits bone formation by osteoblasts. However, the potential role of FGF23, Klotho, and Sclerostin in nephrolithiasis is still poorly under-stood or even unexplored. The aim of this study is to test if levels of FGF23, Klotho, and Sclerostin are differentially regulated in kidney stone formers.
Kidney stones are very common in industrialized countries and the lifetime risk is about 10
to 15% in this population. Men are more affected than women and the mean age of the patients
is be-tween the fourth and sixth decade of life. Notably, a considerable percentage of
patients experience recurrent kidney stones with a relapse rate of 50% in 5-10 years
complicated by pain and urinary tract infections and potential loss of functional renal
parenchyma with development of chronic renal failure in the long term. Kidney stones are
composed of inorganic and organic components. Calcium containing stones are the most common
stone type accounting for more than 80% of kidney stones. Many factors predispose or
contribute to the development of kidney stones, including genetic variants or mutations,
diet, environmental factors, and behavior. Among all factors, abnormal urinary pH and
calcium excretion are predominant findings in stone formers and seem to play a major role in
the pathogenesis of stone formation (1-5). Moreover, a significant percentage of patients
with calcium nephrolithiasis and normal parathyroid function show hypophosphatemia and
reduced renal phosphate reabsorption i.e. a renal phosphate leak (6-8) with resulting
hyperphosphaturia. To date, little is known on fibroblast growth factor (FGF23) levels in
patients with calcium nephrolithiasis (6). The authors demonstrated that FGF23 was increased
in stone formers with renal phosphate leak when compared to controls. Also serum FGF23
concentration was strongly inversely associated with serum phosphate levels and rate of
tubular phosphate re-absorption, respectively. This study suggests a role of FGF23 in the
pathogenesis of calcium nephrolithiasis, however, more studies are necessary to confirm
these findings. More, the influence of other novel factors involved in hyperphosphaturia has
not been identified yet, such as Klotho.
FGF23 is crucial for phosphate homeostasis including physiological and pathophysiological
conditions such as X-linked hypophosphatemic rickets and it seems that FGF23 is probably the
most important regulator of serum phosphate and calcitriol (1,25(OH)2D3) levels in addition
to parathyroid hormone (PTH) produced by the parathyroid gland (9-13). FGF23 is produced by
osteocytes and osteoblasts, secreted in response to phosphate, and 1,25(OH)2D3, binds to the
FGF receptor (FGFR)/Klotho complex, and acts as a phosphaturic hormone by reducing the
expression of both sodium dependent phosphate cotransporters, namely NaPi2a and NaPi2c in
renal proximal tubule cells (14). There is some evidence of PTH induced expression and
secretion of FGF23 and on the other hand FGF23 decreases 1,25(OH)2D3 production and thus
stimulates PTH production. In chronic kidney disease (CKD) patients, FGF23 is involved in
CKD-related mineral and bone disorder (CKD-MBD) and has been shown to be an independent and
probably more critical cardiovascular risk factor than phosphate (14).
Novel factors such as Klotho and Sclerostin, which are involved in the
bone-kidney-parathyroid endocrine axis, have been identified recently. Klotho is a putative
aging suppressor gene and its deficiency results in osteopenia, hyperphosphaturia, and
calcification. Klotho is mainly expressed in the kidney but also in the parathyroid gland
and acts as a FGF23 specific co-receptor mediating FGF23 participation in the
bone-kidney-parathyroid endocrine axis as described above. Interestingly, secreted Klotho is
also able to induce phosphaturia independently of FGF23 (15).
Sclerostin is a protein secreted by osteocytes that inhibits bone formation by osteoblasts.
Deficiency of Sclerostin causes van Buchem disease and sclerosteosis, both rare sclerosing
bone disorders, respectively. Interestingly, in humans, Sclerostin mRNA is expressed in
several tissues, with high levels in the kidney whereas Sclerostin protein is only
restricted to osteocytes. The exclusive effect of Sclerostin on bone formation and its
deficiency causing bone disorders suggest a potential role of this molecule also in other
diseases where bone homeostasis may be disarranged such as nephrolithiasis (16-18).
However, the potential role of FGF23, Klotho, and Sclerostin in nephrolithiasis is still
poorly under-stood or even unexplored. The aim of this study is to test if levels of FGF23,
Klotho, and Sclerostin are differentially regulated in kidney stone formers. Given the large
number of kidney stone patients worldwide, the better understanding of the pathogenesis of
kidney disease may provide the basis for the design of more individualized and specifically
targeted therapeutics for this patient cohort.
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