Journal List > J Clin Neurol > v.8(1) > 1048420

TOOLS
Babacan, Karaoglu, Vurucu, Yesilkaya, Yesilyurt, Cayci, Gulgun, Unay, Akın, and Ozcan: May Long Term Oxcarbazepine Treatment Be Lead to Secondary Hyperparathyroidism?
Original Article
Journal of Clinical Neurology

Journal of Clinical Neurology 2012; 8(1): 65-68.

Published online: 31 March 2012

DOI: https://doi.org/10.3988/jcn.2012.8.1.65

May Long Term Oxcarbazepine Treatment Be Lead to Secondary Hyperparathyroidism?

O. Babacana, A. Karaoglua, S. Vurucub, E. Yesilkayac, O. Yesilyurtd, T. Caycie, M. Gulguna, B. Unayb, R. Akınb, O. Ozcana

aDepartment of Pediatrics, Gulhane Military Medical Faculty, Etlik, Ankara, Turkey.

bDepartment of Pediatrics, Division of Pediatric Neurology, Gulhane Military Medical Faculty, Etlik, Ankara, Turkey.

cDepartment of Pediatrics, Division of Pediatric Endocrinology, Gulhane Military Medical Faculty, Etlik, Ankara, Turkey.

dDepartment of Pharmacology, Gulhane Military Medical Faculty, Etlik, Ankara, Turkey.

eDepartment of Biochemistry, Gulhane Military Medical Faculty, Etlik, Ankara, Turkey.

Correspondence: Abdulbaki Karaoglu, MD. Department of Pediatrics, Gulhane Military Medical Faculty, Etlik, Ankara 06018, Turkey. Tel +90-312-304-1889, Fax +90-312-304-4381, akaraoglu@gata.edu.tr

Received 18 January 2011       Revised 17 June 2011       Accepted 17 June 2011

Copyright © 2012 Korean Neurological Association

(open-access):

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

Abstract

Background and Purpose

The adverse effects of newer antiepileptic drugs are not well-known. This study assessed the impact of oxcarbazepine (OXC) treatment on bone turnover.

Methods

Forty-four children with idiopathic focal (and/or secondarily generalized) epilepsy who had been treated with OXC for more than 1 year were compared with 33 healthy, age- and sex-matched children. Serum calcium, phosphorus, alkaline phosphatase, parathyroid hormone, osteocalcin, calcitonin, and 25-hydroxyvitamin D, and bone mineral density were measured to evaluate and compare bone mineralization between the two groups.

Results

The serum levels of calcium, osteocalcin, 25-hydroxyvitamin D, and bone mineral density did not differ significantly between the study and control groups. However, serum levels of parathyroid hormone, alkaline phosphatase, phosphorus, and calcitonin differed significantly between the two groups.

Conclusions

These findings suggest that OXC treatment leads to secondary hyperparathyroidism with high-turnover bone disease and/or impaired intestinal calcium absorption.

Keywords: oxcarbazepine, bone mineralization, children

Introduction

Long-term use of antiepileptic drugs (AEDs) renders a patient more vulnerable to their side effects,1,2 and the patient must then struggle with these side effects in addition to the primary disease. Although several studies have shown that commonly used AEDs may lead to osteopenia/osteoporosis, osteomalacia, and bone fractures,3,4 there is little information available on the effect of oxcarbazepine (OXC) on bone metabolism.5,6 Mintzer et al.7 demonstrated that OXC monotherapy significantly reduced the level of 25-hydroxyvitamin D (25-OHD), and changed other bone biomarkers in a pattern suggestive of secondary hyperparathyroidism. Although OXC is only a limited enzyme inducer, they stated that OXC may have some dose-dependent cytochrome P-450 (CYP-450) induction properties, or may have an effect on osteoblast proliferation.
It might be possible to avoid the side effects of OXC if the underlying mechanisms were known. Several markers, such as serum levels of 25-OHD and calcium, and bone mineral density (BMD), have been used to identify these side effects. The present study assessed the effects of OXC monotherapy on bone mineralization in terms of the serum levels of parathyroid hormone (PTH), alkaline phosphatase (ALP), calcium, phosphorus, 25-OHD, osteocalcin, and calcitonin, and the BMD.

Methods

This study involved two groups: group 1 comprised 44 children aged between 5 and 15 years with idiopathic focal (and/or secondarily generalized) epilepsy who had been treated with OXC as a first-line AED for at least 1 year,8 while group 2 was the control group that comprised 33 healthy, age- and sex-matched children. Patients with height and weight measurements below the 3rd percentile, using any drug that may affect bone metabolism, receiving any other AED, and with chronic illnesses other than epilepsy were excluded from the study. Serum levels of PTH, ALP, calcium, phosphorus, 25-OHD, osteocalcin, and calcitonin, and the BMD value were evaluated in both groups and statistically compared.
Blood samples were obtained at between 8:00 and 8:30 a.m. after an overnight fast. The serum fraction was obtained by centrifugation (at 2000×g for 10 min at 4℃) after storing the whole blood at room temperature for 1 hour. Serum was stored at -80℃ until analysis. Serum levels of calcium, phosphorus, and ALP were measured spectrophotometrically with an autoanalyzer using commercial kits (AU-2700, Olympus, Hamburg, Germany). The serum level of 25-OHD was determined using a high-performance liquid chromatography system with a fluorescence detector. Serum levels of PTH, osteocalcin, and calcitonin were determined with a chemoluminescence technique using an autoanalyzer with commercial kits (Roche E 170, Roche Diagnostics, Mannheim, Germany).
BMD was assessed using dual-energy X-ray absorptiometry (QDR4500 Elite Hologic, Bedford, MA, USA) in the lumbar spine at levels L2-L4. Approval for this study was obtained from the Medicine Ethics Committee of Gulhane Military Medical Academy Faculty. Informed consent to participate was obtained from the parents of all patients.

Statistical methods

All data analysis was performed using the SPSS 11.5 package program (SPSS, Chicago, IL, USA). Continuous and categorical variables are expressed as mean±SD values and percentages and frequencies, respectively. Comparisons between groups were performed by t-test. The sex distributions for group 1 (study group) and group 2 (control group) were compared by Chi-square test. The level of statistical significance was set at p<0.05.

Results

The study group (group 1; n=44) comprised 22 males (50%) and 22 females (50%) aged between 5 and 15 years (9.65±3.04 years). The control group (group 2; n=33) comprised 17 males (51%) and 16 females (49%), all healthy, aged between 5 and 15 years (10.24±2.86 years). The mean duration of OXC therapy in group 1 was 16 months (12-23 months). The serum levels of PTH, ALP, phosphorous, and calcitonin differed significantly between the study and control groups (p=0.003, 0.011, 0.005, and 0.046, respectively). However, for the serum levels of calcium, osteocalcin, and 25-OHD, and the BMD did not differ significantly between the two groups. The biochemical and bone-turnover parameters are presented in Table 1.

Discussion

Several studies have shown that the affect of AEDs on bone metabolism may lead to osteopenia/osteoporosis, osteomalacia, and bone fractures.4,9 Hypocalcemia in patients with refractory epilepsy may lead to osteopenia and osteoporosis that could eventually increase the number of bone fractures, which makes the follow-up of epileptic patients more difficult.10 The present study detected increased serum levels of PTH, ALP, and phosphorous, decreased serum levels of calcitonin, and normal levels of calcium in patients with idiopathic focal (and/or secondarily generalized) epilepsy who had been receiving OXC monotherapy as a first-line AED for more than 1 year.
Long-term AED treatment is known to affect bone metabolism.7 Although the incidence of bone disease due to AEDs was reported in the literature to be 19-56%, only 8% of those patients had radiologically confirmed rickets.11 The prevalence of osteomalacia in patients receiving long-term AEDs was reported to be 10-30%, while those of hypocalcemia and increased serum levels of ALP were 10-30% and 40%, respectively.12
Many theories have been proposed to explain the effects of AED use in relation to the pathogenesis of bone disease, although the exact mechanism remains to be established.7 An increase in serum PTH levels associated with AED therapy has been reported.7,13-15 Mintzer et al.7 suggested that by inducing the CYP-450-mediated catabolism of 25-OHD to less biologically active metabolites, AEDs lead to a decrease in vitamin-D-mediated bone mineralization and intestinal calcium absorption. This in turn causes a compensatory increase in PTH, which stimulates the production of 1α-hydroxylase, the enzyme responsible for the conversion of 25-OHD to 1,25-dihydroxyvitamin D (1,25-OHD), which explains the maintenance of 1,25-OHD levels seen in AED-treated patients.7 The chronic elevation of PTH required to maintain 1,25-OHD levels, which is referred to as secondary hyperparathyroidism, causes an increase in bone turnover, which leads to long-term loss of bone mass. Similarly, Bouillon et al.15 reported increased PTH levels, low serum 25-OHD levels, and relative hypocalcemia in patients receiving anticonvulsant treatment. In the present study we found increased serum levels of PTH, ALP, and phosphorous, decreased calcitonin levels, and normal serum 25-OHD and calcium levels, which may also be referred to as secondary hyperparathyroidism. In secondary hyperparathyroidism, serum calcium levels are often maintained within the normal range and ALP levels are elevated, which is thought to be related to compensatory stimulation of osteoblastic activity in bone.16
ALP measurement is an adjunct test for assessing high bone turnover.17 High ALP levels are generally related to liver or bone disease, which can be differentiated by a concurrent increase in liver function tests or bone biochemical parameters. The normal liver function tests in the present study suggested to us that high ALP levels are more suggestive of bone disease than liver disease. Verrotti et al.18 reported increased bone-turnover markers independent of vitamin D deficiency in patients receiving AEDs. Another study found normal serum levels of vitamin D metabolites, and bone biopsies revealing increased osteoid formation but normal calcification, accelerated mineralization rate, and decreased mineralization lag time (indicative of increased bone turnover) in patients receiving long-term AED therapy.14 Therefore, OXC might have effects on osteoblastic activity, osteoid formation, and calcification, although osteoblasts may synthesize sufficient osteoid while mineralization may be deficient.
Another suggested mechanism is the ineffective absorption of fat-soluble vitamin D and/or impaired intestinal calcium absorption. In a study of rats that examined the effects of AEDs on intestinal calcium transport, rats treated with phenytoin had markedly decreased calcium absorption.19 OXC may thus have interfered with intestinal calcium absorption in the patients in the present study. The other proposed mechanism is calcitonin deficiency. Calcitonin is a hormone that is produced by the thyroid gland and inhibits osteoclast-mediated bone resorption. In an in vitro study by Vernillo et al.,20 calcitonin secretion was reduced in osteoblastic rat osteosarcoma cells exposed to phenytoin in the culture media, compared with control cells. Thus, calcitonin deficiency may accelerate bone turnover, resulting in increased bone resorption.3 In the present study we found a decrease in calcitonin levels that may have been associated with OXC treatment.
In conclusion, OXC treatment may cause increased serum levels of PTH, ALP, and phosphorous, and decreased levels of calcitonin, which may be due to the induction of CYP-450-mediated catabolism of 25-OHD to less biologically active metabolites, or to high-turnover bone disease or impaired intestinal calcium absorption. In turn, this may cause a compensatory increase in PTH and an increase in bone-turnover markers. It should be kept in mind that OXC treatment may lead to secondary hyperparathyroidism and that such patients should be routinely followed-up with regular PTH, ALP, phosphorous, and calcitonin blood biochemistry testing.

Figures and Tables

Table 1
Demographic and laboratory findings of the patients
jcn-8-65-i001

*t-test, **Chi-square test.

ALP: alkaline phosphatase, BMD: bone mineral density, Ca: calcium, M/F: male/female, NS: not significant, P: phosphorus, PTH: parathyroid hormone.

Acknowledgements

This research was conducted at Gulhane Military Medical Academy.

Notes

The authors have no financial conflicts of interest.

References

1. Dent CE, Richens A, Rowe DJ, Stamp TC. Osteomalacia with long-term anticonvulsant therapy in epilepsy. Br Med J. 1970. 4:69–72.
crossref
2. Bogliun G, Beghi E, Crespi V, Delodovici L, d'Amico P. Anticonvulsant drugs and bone metabolism. Acta Neurol Scand. 1986. 74:284–288.
crossref
3. Pack AM, Morrell MJ. Adverse effects of antiepileptic drugs on bone structure: epidemiology, mechanisms and therapeutic implications. CNS Drugs. 2001. 15:633–642.
crossref
4. Coppola G, Fortunato D, Auricchio G, Mainolfi C, Operto FF, Signoriello G, et al. Bone mineral density in children, adolescents, and young adults with epilepsy. Epilepsia. 2009. 50:2140–2146.
crossref
5. Babayigit A, Dirik E, Bober E, Cakmakci H. Adverse effects of antiepileptic drugs on bone mineral density. Pediatr Neurol. 2006. 35:177–181.
crossref
6. Verrotti A, Greco R, Latini G, Morgese G, Chiarelli F. Increased bone turnover in prepubertal, pubertal, and postpubertal patients receiving carbamazepine. Epilepsia. 2002. 43:1488–1492.
crossref
7. Mintzer S, Boppana P, Toguri J, DeSantis A. Vitamin D levels and bone turnover in epilepsy patients taking carbamazepine or oxcarbazepine. Epilepsia. 2006. 47:510–515.
crossref
8. Berg AT, Berkovic SF, Brodie MJ, Buchhalter J, Cross JH, van Emde Boas W, et al. Revised terminology and concepts for organization of seizures and epilepsies: report of the ILAE Commission on Classification and Terminology, 2005-2009. Epilepsia. 2010. 51:676–685.
crossref
9. Pack AM, Morrell MJ. Epilepsy and bone health in adults. Epilepsy Behav. 2004. 5:Suppl 2. S24–S29.
crossref
10. Pack AM, Gidal B, Vazquez B. Bone disease associated with antiepileptic drugs. Cleve Clin J Med. 2004. 71:Suppl 2. S42–S48.
crossref
11. Crosley CJ, Chee C, Berman PH. Rickets associated with long-term anticonvulsant therapy in a pediatric outpatient population. Pediatrics. 1975. 56:52–57.
crossref
12. Schmitt BP, Nordlund DJ, Rodgers LA. Prevalence of hypocalcemia and elevated serum alkaline phosphatase in patients receiving chronic anticonvulsant therapy. J Fam Pract. 1984. 18:873–877.
13. Hahn TJ, Scharp CR, Richardson CA, Halstead LR, Kahn AJ, Teitelbaum SL. Interaction of diphenylhydantoin (phenytoin) and phenobarbital with hormonal mediation of fetal rat bone resorption in vitro. J Clin Invest. 1978. 62:406–414.
crossref
14. Weinstein RS, Bryce GF, Sappington LJ, King DW, Gallagher BB. Decreased serum ionized calcium and normal vitamin D metabolite levels with anticonvulsant drug treatment. J Clin Endocrinol Metab. 1984. 58:1003–1009.
crossref
15. Bouillon R, Reynaert J, Claes JH, Lissens W, De Moor P. The effect of anticonvulsant therapy on serum levels of 25-hydroxy-vitamin D, calcium, and parathyroid hormone. J Clin Endocrinol Metab. 1975. 41:1130–1135.
crossref
16. Välimäki MJ, Tiihonen M, Laitinen K, Tähtelä R, Kärkkäinen M, Lamberg-Allardt C, et al. Bone mineral density measured by dual-energy x-ray absorptiometry and novel markers of bone formation and resorption in patients on antiepileptic drugs. J Bone Miner Res. 1994. 9:631–637.
crossref
17. Schoppet M, Shanahan CM. Role for alkaline phosphatase as an inducer of vascular calcification in renal failure? Kidney Int. 2008. 73:989–991.
crossref
18. Verrotti A, Greco R, Morgese G, Chiarelli F. Increased bone turnover in epileptic patients treated with carbamazepine. Ann Neurol. 2000. 47:385–388.
crossref
19. Koch HU, Kraft D, von Herrath D, Schaefer K. Influence of diphenylhydantoin and phenobarbital on intestinal calcium transport in the rat. Epilepsia. 1972. 13:829–834.
crossref
20. Vernillo AT, Rifkin BR, Hauschka PV. Phenytoin affects osteocalcin secretion from osteoblastic rat osteosarcoma 17/2.8 cells in culture. Bone. 1990. 11:309–312.
crossref
TOOLS
Similar articles