Hostname: page-component-586b7cd67f-2brh9 Total loading time: 0 Render date: 2024-11-27T18:35:09.276Z Has data issue: false hasContentIssue false

Comment on Bristow et al.: Dietary calcium: adverse or beneficial effects of supplements?

Published online by Cambridge University Press:  24 August 2015

H. A. Morris*
Affiliation:
School of Pharmacy and Medical Science, University of South Australia, Adelaide, SA 5000, Australia Chemical Pathology, SA Pathology, Adelaide, SA 5000, Australia
Rights & Permissions [Opens in a new window]

Abstract

Type
Invited Commentary
Copyright
Copyright © The Authors 2015 

Adequate Ca nutrition remains a significant issue throughout all stages of life, for bone mineral accrual during growth and maintenance of bone mineral in adulthood. Many individuals do not achieve the recommended daily allowance from their self-selected diets and take Ca supplements( Reference Ross, Taylor and Yaltine 1 ). The paper by Bristow et al.( Reference Bristow, Gamble and Stewart 2 ) reports data on effects of Ca both in the form of supplements and in a meal on acute effects on serum Ca and phosphate levels, with most interesting results relevant to the likelihood of Ca supplements increasing serum levels to cause adverse cardiovascular events.

The most recent thorough review of dietary Ca requirements reached remarkable consistency with previous recommendations without controversy( Reference Ross, Taylor and Yaltine 1 ). These recommendations were based on physiological outcomes, the level of dietary Ca required to achieve Ca balance, and clinical outcomes, including maintenance of bone mineral density and risk of fracture. The recognition that low Ca intakes are common, has stimulated the medical professionals to promote the use of Ca supplements for over 20 years. Ca is a threshold nutrient, such that an intake sufficient to achieve balance between the intake and excretion is required. No further benefit is achieved by increasing dietary intake above this level as any extra Ca is mainly excreted by the bowel but also by the kidney and through the skin. Within this physiological context, randomised controlled trials (RCT) of Ca supplementation and meta-analyses of their outcomes have demonstrated significant reduction in the risk of fracture among post-menopausal women( Reference Tang, Eslick and Nowson 3 , Reference Cauley, Chlebowski and Wactawski-Wende 4 ). Such outcomes have prompted strong endorsement for Ca supplements from authorities, including the US National Institutes of Health requiring the outcomes of clinical trials for osteoporosis to be compared with Ca and vitamin D supplementation, as standard of care rather than a true placebo. The uptake of Ca supplements among the general community has been widespread with some 60 % of the US women over 60 years of age taking a Ca supplement in the period 2003–2006, an increase from 28 % in 1988 to 1994( Reference Gahche, Bailey and Burg 5 ).

Recent secondary analyses of RCT of Ca and/or vitamin supplementation for fractures have indicated mixed results for cardiovascular events, either increased the risk of adverse events, differential effects between men and women, or had no adverse effects( Reference Bristow, Gamble and Stewart 2 , Reference Weaver 6 ). Clearly considerable controversy and confusion remain on this subject. Meta-analyses from RCT are defined as the highest level of evidence, assuming that the design of each study or systematic review has minimised the impact of bias on the results( 7 ). One has to question whether this assumption is often met particularly in the conduct of RCT involving nutrients. For example, the analysis and re-analyses of data from perhaps the largest and longest RCT in this field, the Women’s Health Initiative have provided a variety of results( Reference Gahche, Bailey and Burg 5 ). Of particular interest is that in the original analysis women who were taking their own Ca and vitamin D supplements were not excluded at the commencement of the trial and were allowed to continue this practice, irrespective of whether they were allocated to the active or placebo arms. Re-analyses of these data and inclusion of other subjects based on their baseline-dietary intake demonstrated various health benefits, not indicated by the original analysis for fracture or cardiovascular outcomes( Reference Hsia, Heiss and Ren 8 Reference Prentice, Pettinger and Jackson 10 ). Such variation in outcomes would suggest that the basic assumption of an RCT, randomisation of subjects to minimise the impact of bias on the results, has not been met. It is difficult to estimate how many RCT do not meet this criterion.

An interesting and consistent finding is that dietary Ca is apparently not associated with adverse cardiovascular events, the physiological basis of which is not understood. One hypothesis to explain this difference has been that Ca supplements yield higher levels of circulating Ca than when Ca is taken in food. The paper by Bristow et al.( Reference Bristow, Gamble and Stewart 2 ) reports data on serum Ca and phosphate levels, following a variety of forms of dietary Ca. Increases in blood-ionised Ca, serum-total Ca and phosphate were observed with each intervention, although the increased levels of ionised and total Ca following the dairy meal were not as great as with supplements whether fasting or following a meal, providing evidence for this hypothesis.

The central question arising from this study is the physiological significance of such increases whether for bone or cardiovascular health. The major mechanism by which changes in serum Ca levels modulate physiology is through the Ca-sensing receptor (CaSR)( Reference Hénaut, Boudot and Massy 11 ). Ionised Ca is the ligand for the CaSR, and the increases of blood ionised Ca demonstrated in the Bristow et al. study are sufficient to activate this receptor (0·02–0·05 mmol/l( Reference Goltzman and Hendy 12 )) although the increase following the dairy meal barely achieved this minimum level. For bone health, activation of the CaSR can stimulate bone formation and reduce bone resorption, depending on conditions( Reference Goltzman and Hendy 12 ). For cardiovascular health, activation of CaSR can reduce mineralisation by vascular smooth-muscle cells( Reference Hénaut, Boudot and Massy 11 ). Within the context of chronic kidney disease, cardiovascular deaths are most important and the contributions of elevated blood phosphate to this pathology have been well demonstrated( Reference Palmer, Hayen and Macaskill 13 ). However, Bristow et al. report that the highest phosphate levels are achieved when a meal is involved with the Ca supplement, a condition which one would expect to reduce the risk of adverse outcomes. Finally, although variations of serum Ca of the order demonstrated with Ca supplements have been found in cross-sectional studies to be associated with increased-relative risk of cardiovascular events and coronary artery calcification, the absolute risk of adverse events is very low( Reference Kwak, Kim and Choi 14 , Reference Slinin, Blackwell and Ishani 15 ), suggesting further interactions are involved.

Clearly, these are highly complex interactions and further research is required into the physiological outcomes of variation of serum Ca and phosphate within the range in healthy people. Designs of the relevant RCT providing data for meta-analyses require careful review, particularly with regard to physiology of nutrients. Ca is a threshold nutrient; insufficient intake is detrimental for health, but too much may also be bad for health. As nutritionists and health practitioners, we are required to emphasise that it is the appropriate level of any nutrient including Ca intake that is important for health.

References

1. Ross, CA, Taylor, CL, Yaltine, AL, et al. (editors) (2011) Committee to Review Dietary Reference Intakes for Vitamin D and Calcium. Washington, DC: Institute of Medicine National Academies Press.Google Scholar
2. Bristow, S, Gamble, G, Stewart, A, et al. (2015) Acute effects of calcium citrate with or without a meal, calcium-fortified juice and a dairy meal on serum calcium and phosphate: a randomised cross-over trial. Br J Nutr 113, 15851594.CrossRefGoogle ScholarPubMed
3. Tang, BM, Eslick, GD, Nowson, C, et al. (2007) Use of calcium or calcium in combination with vitamin D supplementation to prevent fracture and bone loss in people aged 50 years and older: a meta-analysis. Lancet 370, 657666.CrossRefGoogle ScholarPubMed
4. Cauley, JA, Chlebowski, RT, Wactawski-Wende, J, et al. (2013) Calcium plus vitamin D supplementation and health outcomes five years after active intervention ended: the Women’s Health Initiative. J Women’s Health (Larchmt) 22, 915929.CrossRefGoogle ScholarPubMed
5. Gahche, J, Bailey, R, Burg, V, et al. (2011) Dietary supplement use among US adults has increased since NHANES III (1988–1994). NCHS Data Brief 61, 18.Google Scholar
6. Weaver, CM (2014) Calcium supplementation: is protecting against osteoporosis counter to protecting against cardiovascular disease? Curr Osteoporos Rep 12, 211218.Google Scholar
7. Australian Government National Health and Medical Research Council (NHMRC) (2009) Additional levels of evidence and grades for recommendations for developers of guidelines. https://www.nhmrc.gov.au/_files_nhmrc/file/guidelines/developers/nhmrc_levels_grades_evidence_120423.pdf (accessed May 2015).Google Scholar
8. Hsia, J, Heiss, G, Ren, H, et al. (2007) Calcium/vitamin D supplementation and cardiovascular disease in women. Circulation 115, 846854.Google Scholar
9. Bolland, MJ, Grey, A, Avenall, A, et al. (2011) Calcium supplements with or without vitamin D and risk of cardiovascular events: reanalysis of the Women’s Health Initiative limited access dataset and meta-analysis. BMJ 342, d2040.CrossRefGoogle ScholarPubMed
10. Prentice, RL, Pettinger, MB, Jackson, RD, et al. (2013) Health risks and benefits from calcium and vitamin D supplementation: Women’s Health Initiative clinical trial and cohort study. Osteoporos Int 24, 567580.Google Scholar
11. Hénaut, L, Boudot, C, Massy, ZA, et al. (2014) Calcimimetics increase CaSR expression and reduce mineralization in vascular smooth muscle cells: mechanisms of action. Cardiovasc Res 101, 256265.Google Scholar
12. Goltzman, D & Hendy, GN (2015) The calcium-sensing receptor in bone-mechanistic and therapeutic insights. Nat Rev Endocrinol 11, 298307.CrossRefGoogle ScholarPubMed
13. Palmer, SC, Hayen, A, Macaskill, P, et al. (2011) Serum levels of phosphorus, parathyroid hormone, and calcium and risks of death and cardiovascular disease in individuals with chronic kidney disease: a systematic review and meta-analysis. JAMA 167, 11191127.Google Scholar
14. Kwak, SM, Kim, JS, Choi, Y, et al. (2014) Dietary intake of calcium and phosphorus and serum concentration in relation to the risk of coronary artery calcification in asymptomatic patients. Arterioscler Thromb Vasc Biol 34, 17631769.Google Scholar
15. Slinin, Y, Blackwell, T, Ishani, A, et al. (2011) Serum calcium, phosphorus and cardiovascular events in post-menopausal women. Int J Cardiol 149, 335340.Google Scholar