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Postprandial metabolic responses of serum calcium, parathyroid hormone and C-telopeptide of type I collagen to three doses of calcium delivered in milk

Published online by Cambridge University Press:  30 April 2014

Marlena C. Kruger*
Affiliation:
Institute of Food, Nutrition and Human Health, Massey University, Private Bag 11222, Palmerston North, New Zealand
Pamela R. von Hurst
Affiliation:
Institute of Food, Nutrition and Human Health, Massey University, Private Bag 102 904, North Shore Mail Centre, Auckland, New Zealand
Christine L. Booth
Affiliation:
Institute of Food, Nutrition and Human Health, Massey University, Private Bag 11222, Palmerston North, New Zealand
Barbara Kuhn-Sherlock
Affiliation:
Fonterra Research and Development Centre, Private 11029, Palmerston North, 4442, New Zealand
Joanne M. Todd
Affiliation:
Fonterra Co-Operative Group Ltd, Private Bag 92032, 9 Princes Street, Auckland, New Zealand
Linda M. Schollum
Affiliation:
Fonterra Research and Development Centre, Private 11029, Palmerston North, 4442, New Zealand
*
* Corresponding author: Dr Marlena C. Kruger, email m.c.kruger@massey.ac.nz

Abstract

Acute doses of Ca rapidly increase serum Ca and reduce bone resorption concomitant with a reduction in serum parathyroid hormone (PTH) levels. The physiological response to a dose of Ca in milk and to a Ca salt may be different. The present study investigated Ca absorption patterns with increasing levels of fortification in milk, and the response to one dose of a Ca salt. A group of twenty-eight Asian women aged 20–45 years volunteered to attend the laboratory over several weeks. The fasted volunteers were randomised to one of three experimental drinks: 200 ml skimmed milk containing 250, 500 or 1000 mg Ca. A subgroup of seven volunteers also received a calcium gluconate/carbonate salt containing 1000 mg Ca in 200 ml water. Serial blood samples and urine were collected for 5 h from baseline. Different doses of Ca in milk resulted in a graded response in serum corrected Ca, PTH and C-telopeptide of type I collagen (CTx) but not ionised Ca. Serum Ca increased in response to all milk drinks and from 2 to 5 h the blood Ca levels were significantly different for the 250 and 1000 mg doses, as was the integrated response between the loads. The PTH response to the two higher doses was significantly more than following the 250 mg dose. The integrated response for CTx and urinary Ca between all three doses of Ca in milk was significantly different. A dose of Ca salt elicited a more immediate response reaching a plateau faster, and declining faster to baseline. Fortified milk is a safe matrix for delivering larger doses of Ca.

Information

Type
Metabolism and Metabolic Studies
Creative Commons
Creative Common License - CCCreative Common License - BY
The online version of this article is published within an Open Access environment subject to the conditions of the Creative Commons Attribution license .
Copyright
Copyright © The Author(s) 2014
Figure 0

Table 1. Nutrient composition of the single meal consumed during each 1 d study

Figure 1

Table 2. Baseline characteristics of the study population(Mean values, standard deviations and ranges; n 28)

Figure 2

Table 3. Dietary nutrient intake from 3 d food diaries(Mean values, standard deviations and ranges; n 28)

Figure 3

Fig. 1. (A) Change in serum calcium adjusted for albumin from baseline over time for each milk drink: 250 mg dose (□); 500 mg dose (); 1000 mg dose (). Values are means, with 95 % CI represented by vertical bars. There was an effect of drink × time (P = 0·005). (B) AUC for serum calcium concentration over the 5 h period. Values are means, with 95 % CI represented by vertical bars. a,b,c Mean values with unlike letters were significantly different (P < 0·001).

Figure 4

Fig. 2. Change in serum ionised calcium from baseline over time for each milk drink: 250 mg dose (□); 500 mg dose (); 1000 mg dose (). Values are means, with 95 % CI represented by vertical bars.

Figure 5

Fig. 3. (A) Change in serum parathyroid hormone (PTH) from baseline over time for each milk drink: 250 mg dose (□); 500 mg dose (); 1000 mg dose (). Values are means, with 95 % CI represented by vertical bars. (B) AUC for change in serum PTH from baseline to end point. Values are means, with 95 % CI represented by vertical bars. a,b Mean values with unlike letters were significantly different (P < 0·001).

Figure 6

Fig. 4. (A) Change in serum C-telopeptide of type I collagen (CTx) over time for each milk drink: 250 mg dose (□); 500 mg dose (); 1000 mg dose (). Values are means, with 95 % CI represented by vertical bars. (B) AUC for change in serum CTx from baseline to end point. Values are means, with 95 % CI represented by vertical bars. a,b Mean values with unlike letters were significantly different (P = 0·001).

Figure 7

Fig. 5. (A) Urinary calcium:creatinine ratio differences from baseline as measured at three time points during 6 h for each milk drink: 250 mg dose (□); 500 mg dose (); 1000 mg dose (). Values are means, with 95 % CI represented by vertical bars. (B) AUC for change in urinary calcium:creatinine ratio from baseline to end point. Values are means, with 95 % CI represented by vertical bars. a,b Mean values with unlike letters were significantly different (P < 0·021).

Figure 8

Fig. 6. (A) Change in serum ionised calcium from baseline over time for the tablet containing 1000 mg calcium (•) or the milk delivering 1000 mg calcium (). Values are means, with 95 % CI represented by vertical bars. (B) Change in serum parathyroid hormone (PTH) levels over time after a dose of 1000 mg as the salt (•) or in milk (). Values are means, with 95 % CI represented by vertical bars. * Mean value was significantly different from that for the salt (P < 0·05).