Osteoporosis Clinical Trial
Official title:
Change in Free 25(OH)D After High Dose in Vitamin D Deficient Postmenopausal Women
Total 25(OH)D is currently used as a biomarker of vitamin D status. However, there is some
debate as to whether total 25(OH)D is the best marker to use.
It has been suggested that free vitamin D may be better because it may be more biologically
available.
There are also some uncertainties about how we treat vitamin D deficiency. A single dose is
attractive because it is certain that the patient has had the dose and there is no
requirement for ongoing compliance, but it is still not clear what the best dose is to give.
Also, recent studies have highlighted that high dose vitamin D supplementation may increase
the risk of falling in older populations.
The investigators believe that studying how free vitamin D responds to different bolus doses
is the best way address some of the current research gaps, including what is the best
biomarker of vitamin D status, what is the mechanism of vitamin D toxicity and what is a safe
bolus dose to treat deficiency.
The investigators will study changes in total and free 25(OH)D, and also clinical response,
to three different bolus doses of vitamin D (50 000IU, 150 000IU and 500 000IU) in 84 vitamin
D deficient postmenopausal women, over a three month period with 5 study visits. A concurrent
control group of 28 vitamin D sufficient postmenopausal women will also be recruited.
This will allow the investigators to determine how total and free vitamin D change with bolus
dosing and whether there is a disproportionate rise in free 25(OH)D with higher doses that
may lead to hypercalcemia and falls.
The most commonly used measurement of vitamin D status is serum 25-hydroxyvitamin D
(25(OH)D). However there is no clear consensus on the level of 25(OH)D required to protect
against adverse effects of deficiency.
One approach is to define deficiency is the level of 25(OH)D at which there is a secondary
physiological response, such as a rise in parathyroid hormone. However, this approach has not
yielded a clear answer. Total 25(OH)D below 30nmol/l is not always associated with an
increased parathyroid hormone (PTH) response, and total 25(OH)D and PTH do not always respond
to vitamin D supplementation. This suggests that total 25(OH)D measurement may not be the
best biological marker of vitamin D status.
Vitamin D and its metabolites are bound to proteins in the circulation: around 85-90% of
25(OH)D is bound to vitamin D binding protein (DBP), 10-15% is bound to albumin, and less
than 1% is in the free form. DBP protects 25(OH)D from degradation and allows a circulating
store to accumulate.
The free hormone hypothesis suggests that only the unbound 'free' portion of protein bound
hormones is biologically active, and that this should be measured for the accurate assessment
of hormone availability. Calculated free 25(OH)D concentrations have been shown to be better
correlated to bone mineral density (BMD) than total 25(OH)D in a healthy population and to be
more closely related to PTH in patients with end stage renal disease.
The binding capacity of DBP may be overwhelmed in some situations. In female participants
treated with an oral dose of 500,000 IU annually for 3 years there was an increase in the
risk of falls and fractures that was particularly marked in the three month period after each
dose. It has been proposed that there was vitamin D toxicity and possible hypercalcaemia
during this period due to the binding capacity of DBP being overwhelmed by the large increase
in 25(OH)D with a relatively greater increase in free 25(OH)D. However, free vitamin D and
calcium were not measured in the study, so there is not yet evidence to support this
hypothesis.
The investigators will study changes in total and free 25(OH)D, and clinical response to
three different bolus doses of vitamin D (50,000 units, 150,000 units and 500,000 units) in
84 vitamin D deficient (<30nmol/l) postmenopausal women over three months. This will allow
the investigators to determine how free and total 25(OH)D change with bolus dosing and
whether there is a disproportionately high rise in free 25(OH)D with higher doses. This will
also generate a better understanding of what the optimum bolus dose for treatment of vitamin
D deficiency is and whether free 25(OH)D may be a better marker of vitamin D status in some
situations.
Aims of the study:
- To determine the effect of three different vitamin D bolus doses on free 25(OH)D and
total 25(OH)D in vitamin D deficient post-menopausal women.
- To determine the effect of different vitamin D bolus doses on parameters of calcium
metabolism, bone turnover markers and physical function in vitamin D deficient
post-menopausal women.
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