Chronic Hypoparathyroidism Clinical Trial
Official title:
CALCIUM CITRATE vs CALCIUM CARBONATE FOR THE MANAGEMENT OF CHRONIC HYPOPARATHYROIDISM
Hypoparathyroidism is an endocrinopathy characterized by a deficient secretion or action of PTH associated with low calcium level. According to the European guideline (2015), standard treatment includes oral calcium salts and active vitamin D metabolites to relieve symptoms of hypocalcaemia, maintain serum calcium levels in the low normal range and improve the patient's QoL Calcium carbonate is most often used and less expensive than other calcium preparations and contains the highest concentration of elemental calcium per gram (42%). It requires gastric hydrochloric acid to form carbonic acid (H2CO3) that immediately decomposes into water (H2O) and carbon dioxide (CO2). CO2 is responsible for its side effects such as flatulence, constipation and general gastrointestinal disorders. Therefore, in some patients it is better to find an alternative to calcium carbonate. Calcium citrate should be recommended to patients with achlorhydria or on treatment with proton pump inhibitors (PPI) as well as to patients who preferred to take supplements outside mealtimes. furthermore, patients with hypoparathyroidism have an increased risk of kidney stones. Kidney stones are formed by calcium salts, among which the most frequent ones are calcium-oxalate (70-80%), followed by calcium-phosphate and uric acid. Citrate salts are widely used in the treatmentof nephrolithiasis, since have shown an inhibitory effect on kidney stone formation. Up to now, there are no studies aimed to investigate the efficacy of calcium citrate in the management of subjects with chronic hypoparathyroidism. In particular, we will investigate if calcium citrate compared to calcium carbonate does not affect the risk of renal stones, if it is able to maintain normal calcium levels and, if it has an impact on QOL, in subjects with chronic hypoparathyroidism.
BACKGROUND Hypoparathyroidism is an endocrinopathy characterized by a deficient secretion or
action of PTH associated with low calcium level. It can be primary (inadequate PTH activity),
or secondary (peripheral resistance to PTH).
The most common cause of chronic Hypoparathyroidism is the postsurgical one: it is usually
secondary to previous thyroid surgery but may also occur following parathyroidectomy or other
cervical surgical procedures. Transient Hypoparathyroidism occurs in 30-60% of patients
undergoing total or subtotal thyroidectomy. About 60-70% of cases of postoperative
hypocalcaemia resolve within 4-6 weeks after surgery. About 15-25% of patients will develop
chronic Hypoparathyroidism. The risk of chronic Hypoparathyroidism is closely related to the
number of parathyroid glands remaining in situ at operation.
Hypocalcemia is defined as serum calcium level (albumin adjusted total calcium or ionized
calcium) below the lower limit of the reference range (target range).
In literature there are not data that suggest which is the best serum calcium level to
maintain during treatment, but the aim is to maintain serum calcium level in the lower part
or slightly below the lower limit of the reference range (adjusted serum calcium level
<2.1-2.3 or S-Ca2+ between 1.05-1.15mmol/L), serum phosphate levels within the reference
range, serum calcium-phosphate product below 4.4 mmol2/l2 (55 mg2/dl2), 24-hurinary calcium
excretion <7.5 mmol/2h (300 mg/24h) in men, <6.25 mmol/24h (250 mg/24h) in women, or <0.1
mmol/kg per 24 h (4 mg/kg per 24h) in both sexes.
In addition to hypocalcemia, patients affected by chronic hypoparathyroidism have a higher
risk of renal implications such as urolithiasis and renal impairment because lack of PTH
reduces calcium absorption and phosphate excretion causing hypercalciuria and
hyperphosphatemia.
Moreover, many patients with hypoparathyroidism complain of reduced quality of life (QOL) in
ways that are difficult to quantify but that are nevertheless of concern. Biochemical control
with standard therapy is rarely accompanied by improved functioning or sense of well-being.
Complaints of cognitive dysfunction are common, with the term brain fog typically described
by patients. In support of these issues, large cohort studies from Denmark have shown
increased risk of hospitalization for depression and affective disorders, renal impairment
and infections, whereas the risk for cancer and overall mortality was not increased.
According to the European guideline (2015), standard treatment includes oral calcium salts
and active vitamin D metabolites to relieve symptoms of hypocalcaemia, maintain serum calcium
levels in the low normal range and improve the patient's QoL An adequate daily intake of
calcium from diet and supplements is advisable. Different calcium salts are available as
supplements because elemental calcium is highly reactive so it has to be combined with other
substances. These preparations differ in the concentration of elemental calcium per gram.
Calcium carbonate is most often used and less expensive than other calcium preparations and
contains the highest concentration of elemental calcium per gram (42%). It requires gastric
hydrochloric acid to form carbonic acid (H2CO3) that immediately decomposes into water (H2O)
and carbon dioxide (CO2). CO2 is responsible for its side effects such as flatulence,
constipation and general gastrointestinal disorders. Therefore, in some patients it is better
to find an alternative to calcium carbonate. Calcium citrate, for example, should be
recommended to patients with achlorhydria or on treatment with proton pump inhibitors (PPI)
as well as to patients who preferred to take supplements outside mealtimes.
Previous studies showed that calcium citrate, in comparison to calcium carbonate, causes
greater increment in serum calcium concentration and urinary calcium excretion in parallel
with greater suppression of serum PTH, after Roux-en-Y Gastric bypass and this datum suggests
both the pharmacokinetic and pharmacodynamic superiority of calcium citrate.
Calcium citrate is also better adsorbed than calcium carbonate after panproctocolectomy, so
in a condition of a general enteric malabsorption.
Up to now, there are no studies aimed to investigate the efficacy of calcium citrate in the
management of subjects with chronic hypoparathyroidism. In particular, the investigators will
test the efficacy of calcium citrate in maintaining normal calcium level compared to
carbonate calcium in subjects with chronic hypoparathyroidism. Moreover, the investigators
will evaluate the impact of calcium citrate on QOL in this kind of patients compared to the
gold standard therapy (carbonate calcium).
MATERIALS AND METHODS Each subject will participate in two phases of the study and each phase
will last one month. Once every 2 weeks blood and a morning urine sample will be drawn. For
all the study period, participants will be instructed to maintain a predetermined dietary
calcium intake (800 mg/day) with sodium (100 mEq/day) restrictions. All subjects will
complete a questionnaire on quality of life at 0, +2, +4 week, during both phases. The
investigators will use the Rand 36-Item Short Form Health Survey (version 1.0) to evaluate
the QOL.
Phase 1: According to a block randomization scheme, subjects will be assigned to a calcium
supplement (Drug A or Drug B) at the same total amount of elemental calcium that they had
taken before the study enrollment. The dose of Vitamin D will be equal to the daily dose
taken prior to the study, and will not be changed during the study period.
Phase 2: subjects will be shift to the opposite Drug (from drug A to drug B or from drug B to
drug A) at the same total amount of elemental calcium that they had taken during the last
week of the phase 1.
SAMPLE SIZE CALCULATION
1. Based on the assumption that the within-patient standard deviation of the calcium
oxalate saturation is 0.5, to demonstrate that calcium citrate does not affect the
calcium oxalate saturation, a total of 24 patients need to be enrolled in this study.
This sample size will allow to detect a difference of 0.43 points at a two-sided 5%
significance level with a probability of type II error of 20%.
2. to demonstrate that calcium citrate is as effective as calcium carbonate in maintaining
serum Ca within the acceptable clinical range. To this end, we will study a sample of 21
people already treated with calcium and vitamin D supplementation. Our hypothesis is
that at the end of the study period, the mean Ca concentration will not be different
from the ideal value (9 mg/dl), accepting a 10% variation as the equivalence limit
(i.e., accepting as equivalent values between 8.1 and 9.9 mg/dl). Under these
assumptions, we would need 11 patients to show equivalence between the two treatments,
with a alpha error probability of 5% and a beta error probability of 10%20. With the
available sample size, we will be able to establish equivalence with an equivalence
limit of 0.7 (i.e., values between 8.3 and 9.7 mg/dl).
;
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Completed |
NCT05239221 -
AZP-3601 SAD and MAD Study in Healthy Subjects and Patients With Hypoparathyroidism
|
Phase 1/Phase 2 | |
| Completed |
NCT02910466 -
A Study of Extended Use of Recombinant Human Parathyroid Hormone (rhPTH(1-84)) in Hypoparathyroidism
|
Phase 4 | |
| Active, not recruiting |
NCT05778071 -
Evaluation of the Safety and Efficacy of Eneboparatide (AZP-3601) in Patients With Chronic Hypoparathyroidism
|
Phase 3 | |
| Completed |
NCT05214274 -
Multicenter Registry Study of Chronic Hypoparathyroidism in Chinese Adults
|
||
| Withdrawn |
NCT03878953 -
A Clinical Study of rhPTH(1-84) Treatment in Japanese Participants With Chronic Hypoparathyroidism
|
Phase 3 |