| Literature DB >> 23340319 |
Meinrad Peterlik1, Enikoe Kállay, Heide S Cross.
Abstract
Through a systematic search in Pubmed for literature, on links between calcium malnutrition and risk of chronic diseases, we found the highest degree of evidence for osteoporosis, colorectal and breast cancer, as well as for hypertension, as the only major cardiovascular risk factor. Low calcium intake apparently has some impact also on cardiovascular events and disease outcome. Calcium malnutrition can causally be related to low activity of the extracellular calcium-sensing receptor (CaSR). This member of the family of 7-TM G-protein coupled receptors allows extracellular Ca2+ to function as a "first messenger" for various intracellular signaling cascades. Evidence demonstrates that Ca2+/CaSR signaling in functional linkage with vitamin D receptor (VDR)-activated pathways (i) promotes osteoblast differentiation and formation of mineralized bone; (ii) targets downstream effectors of the canonical and non-canonical Wnt pathway to inhibit proliferation and induce differentiation of colorectal cancer cells; (iii) evokes Ca2+ influx into breast cancer cells, thereby activating pro-apoptotic intracellular signaling. Furthermore, Ca2+/CaSR signaling opens Ca2+-sensitive K+ conductance channels in vascular endothelial cells, and also participates in IP(3)-dependent regulation of cytoplasmic Ca2+, the key intermediate of cardiomyocyte functions. Consequently, impairment of Ca2+/CaSR signaling may contribute to inadequate bone formation, tumor progression, hypertension, vascular calcification and, probably, cardiovascular disease.Entities:
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Year: 2013 PMID: 23340319 PMCID: PMC3571650 DOI: 10.3390/nu5010302
Source DB: PubMed Journal: Nutrients ISSN: 2072-6643 Impact factor: 5.717
Actual and recommended dietary calcium intake in different population groups of selected countries.
| Country | Age (years) | RDA a (mg/day) | Calcium intake (mg/day) | Study | |
|---|---|---|---|---|---|
| Gender | |||||
| Male | Female | ||||
|
| |||||
| Austria | 19–79 | 1000–1300 | 561 (±290) b | 576 (±309) b | Kudlacek |
| Belgium | 75–80 | 1300 | 748 (324–1166) e | 676 (287–1101) e | Amorim Cruz |
| Denmark | 70–75 | 1300 | 544 (127–1812) e | Andersen | |
| France | 75–80 | 1300 | 620 (402–1010) e | 635 (428–944) e | Amorim Cruz |
| Germany | 18–79 | 1000–1300 | 1181 (902–1535) e | 1082 (849–1379) e | Hintzpeter |
| Netherlands | 75–80 | 1300 | 1036 (725–1447) e | 1010 (612–1616) e | Amorim Cruz |
| Poland | 70–75 | 1300 | 325 (86–851) e | Andersen | |
|
| |||||
| Lebanon | 10–16 | 1300 | 873 (793–952) d | 673 (595–750) d | Salamoun |
|
| |||||
| Canada | 18–35 | 1000 | 562 (0–2630) e | Rubin | |
| USA | 31–50 | 1000 | 1118 (±25) b | 864 (±20) b | Bailey |
| USA | >55 | 1300 | 611 (381–892) e | Lappe | |
| Brazil | 16–20 | 1300 | 659 (596–721) d | 881 (730–1032) d | Peters |
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| Bangladesh | 16–40 | 1000 | 180 c | Islam | |
| Indonesia | 18–40 | 1000 | 270 (239–302) d | Green | |
| Malaysia | 18–40 | 1000 | 386 (353–420) d | Green | |
| China | >55 | 1300 | 485 (±253) b | Kruger | |
| Japan | 65–75 | 1300 | 527 (±195) b | Nakamura | |
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| |||||
| Australia | 20–94 | 1000–1300 | 643 (±340) b | Pasco | |
a RDA, recommended daily allowance according to the 2011 report on Dietary Reference Intakes for Calcium and Vitamin D of the Institute of Medicine, National Academy of Sciences USA [6]; b mean (±SD); c median (90% CI); d median (95% CI); e mean (range).
Figure 1The extracellular calcium-sensing receptor (CaSR) senses, amplifies and transduces minute variations in [Ca2+]o into various intracellular signaling pathways. Bold arrows indicate coupling to stimulatory G proteins, dotted arrows indicate coupling to inhibitory G proteins. Only cell-specific pathways relevant for the diseases mentioned in the text are shown (for more details on CaSR-activated pathways, see Magno et al. [119]).
Figure 2Cooperative signaling from Ca2+/CaSR and 1,25-(OH)2D3/VDR on Wnt pathways and formation of mineralized bone.
Figure 3Cooperative signaling from Ca2+/CaSR and 1,25-(OH)2D3/VDR on Wnt pathways inhibits proliferation and promotes differentiation of colonocytes and of colorectal cancer cells.