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Is low Vitamin D just a marker of disease - March 2023

Low vitamin D is a marker for poor health and increased risk for disease: But causality is still unclear in most cases – Oct 2022

Journal of Internal Medicine https://doi.org/10.1111/joim.13582C
Peter Bergman Editorial

It is almost 100 years since Adolf Windaus received the Nobel Prize in chemistry in 1928 for his studies’ on the constitution of sterols and their connection with vitamins’, including vitamin D and its role to prevent rickets [1]. The role of vitamin D to protect the bone has been well known since and has a central role in all medical textbooks. This part of vitamin D metabolism is generally known as the endocrine system, where the liver produces the storage form 25-hydroxyvitamin D (25OHD) and the kidney carries out the conversion into bioactive 1,25-dihydroxyvitamin D (1,25OHD), which mainly regulates calcium balance. In addition, the proform 25OHD can be activated locally in many different cell types, including monocytes, epithelial cells and even in neurons [2, 3]. Local production of the active form of vitamin D (1,25OHD) leads to activation of the vitamin D receptor and subsequent transcription of several hundreds of genes, depending on the cell type and physiological context [4]. This part of vitamin D metabolism is called the paracrine system and has been the focus of intense research during recent years [5]. In parallel with the molecular discoveries of vitamin D metabolism, there has been a rapid increase in observational studies that have found associations between low vitamin D levels and increased risk of many common diseases, including cancer, cardiovascular diseases, respiratory tract infections and Alzheimer's disease as well as all-cause mortality [6-9]. Combined, there has been a solid rationale to perform randomised controlled trials (RCTs) in many of these areas since there is a potential mechanism for beneficial effects and data from observational studies show an increased risk for disease with lower vitamin D levels in plasma. Randomised and placebo-controlled clinical trials of vitamin D supplementation in cancer, cardiovascular diseases and respiratory tract infections have shown both beneficial effects as well as null results [10, 11]. Interestingly, meta-analyses, where results from many RCTs are combined, have shown beneficial effects of vitamin D supplementation on cancer mortality and total mortality as well as reduced risk for respiratory tract infections [12-14]. In addition, Mendelian randomisation studies have shown an inverse association between genetically predicted 25OHD levels and all-cause mortality [15].

It is against this background that Sha et al. set out to obtain further information on the role of vitamin D in reduction of mortality from cancer and other causes, including cardiovascular and respiratory diseases [16]. They used data from the UK Biobank (n = 445,601 participants), including data on the use of vitamin D supplements (over-the-counter drugs or as part of a multivitamin product) and 25OHD levels defined as deficiency (<30 nmol/L) or insufficiency (30 to <50 nmol/L). The outcomes were all-cause and cause-specific mortality, with a focus on mortality due to cardiovascular disease, cancer and respiratory disease. Several covariates were also collected for the adjustment analyses, including demographic and socio-economic factors, which potentially could influence the outcome. The mean age of the cohort was 56.5 years, and a majority were overweight or obese. Interestingly, 21% of the cohort had vitamin D deficiency (<30 nmol/L) and 34.3% had insufficiency (<50 nmol/L). Only 4.3% reported a regular intake of vitamin D supplements, whereas 20.4% reported using multivitamin supplements on a regular basis. Consequently, users of vitamin D or multivitamin supplements had a higher level of 25OHD than nonusers.

Next, the authors analysed determinants associated with vitamin D deficiency. In general, worse health concomitant diseases, obesity, higher blood pressure, poor general health and the latitude of the test centre were factors associated with vitamin D deficiency or insufficiency, whereas the use of vitamin D or multivitamin supplements often had the reverse association, that is, healthier people had a higher tendency to take supplements.

The authors found that both vitamin D deficiency and insufficiency were associated with all-cause mortality and mortality due to cancer, cardiovascular disease (CVD) and respiratory diseases. Five different adjustment models were employed, and the hazard ratios were attenuated with increasing adjustment. The excess mortality was most prominent for CVD, followed by respiratory disease mortality and cancer mortality.

Finally, the association between self-reported vitamin D intake and the outcomes was analysed. Notably, no effect was observed, but after considering concomitant diseases and general health status in the broadest adjustment model, users of vitamin D supplements had 10% lower all-cause mortality and 11% lower cancer mortality, whereas mortality for CVD did not reach statistical significance. The strongest effect was found for respiratory diseases, where self-reported vitamin D intake was associated with 29% decreased mortality.

How should these results be interpreted in the light of available evidence? First, there have been many studies before this one with a similar message, that is, low vitamin D levels are associated with many different diseases, including those discussed here. For example, there is evidence from a large European consortium that low vitamin D levels are associated with increased mortality [17]. We also know that vitamin D has several important functions in the body, apart from regulating calcium homeostasis. A recent example is from the covid area, where vitamin D was found to suppress inflammation in T cells, with potential implications for prevention and treatment of SARS CoV-2 infection [18]. However, despite ample evidence from experimental and observational studies, solid data from RCTs showing beneficial effects against any indication are scarce, with a few exceptions. For example, vitamin D did not prevent CVD or cancer in a large and well-designed RCT [19]. In contrast, in the field of respiratory tract infections, the team around Adrian Martineau has performed two large meta-analyses, one of which is an individual patient data meta-analysis, which found small but statistically significant effects of vitamin D supplementation against respiratory tract infections (RTIs) [13, 14]. However, two recent RCTs could not find any evidence of vitamin D supplementation (or cod liver oil supplementation) against covid-19 [20-22]. Thus, there is still a discrepancy between experimental and observational data on one side and data from RCTs on the other. Why is that? There are three models to consider at this point. The first of these implies that low levels of 25OHD are directly causing the disease. Supplementation would then be the solution and lead to reduced risk of the disease. The other explanation could be a reverse association, that is, that the disease causes low vitamin D levels; for example, if a chronic disease leads to immobilisation indoors without exposure to the sun. The final model is that there is a spurious or ‘false’ association where a third factor leads to both low vitamin D levels and increased risk for the disease. In the paper by Sha et al., for example, subjects with self-reported poor health status had 77% higher odds to have vitamin D deficiency and 19% lower odds of taking vitamin D supplements. Thus, there is a significant risk of the healthy user effect, that is, that healthier people tend to take more supplements, spend more time outdoors and simply avoid diseases to a higher extent than poor, fragile and sick people do. Sha et al. apply an ambitious adjustment approach to avoid this risk, but as the authors point out themselves, it is impossible to adjust for so-called hidden or residual confounders. This means that there could still be additional factors that we cannot adjust for, which could influence the observed associations. Thus, despite the impressive size of the study by Sha et al., we still cannot draw firm conclusions on causality and whether vitamin D supplementation can reduce mortality from CVD, cancer or respiratory diseases.

But which advice should we give to the public, physicians and policy makers about vitamin D deficiency and risk for disease? A pragmatic approach could be to focus on groups at the highest risk for vitamin D deficiency and supplement those <50 nmol/L with 1000–2000 IU/day. This would support the bone, improve immunity and potentially also reduce the risk of respiratory tract infections. Perhaps this strategy could also reduce mortality from CVD, cancer and respiratory disease, as suggested by Sha et al., but solid evidence from bona fide randomised and placebo-controlled clinical trials is still warranted.
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Regarding: Feb 2023

Journal of Internal Medicine https://doi.org/10.1111/joim.13621
William B. Grant, Barbara J. Boucher First published: 22 February 2023
To the Editor,

In a recent editorial, Peter Bergman stated that whether associations between low 25-hydroxyvitamin D [25(OH)D] concentrations and poor health are causally linked was unclear in most cases [1]. His statement was based on the consideration of vitamin D randomized controlled trials (RCTs). However, as discussed at length in a recent review, most vitamin D RCTs have been poorly designed, conducted, and analyzed [2], having been based on guidelines for pharmaceutical drugs rather than on nutrients. Heaney outlined guidelines for trials of nutrients such as vitamin D in 2014 [3]. These guidelines include, for vitamin D, that serum 25(OH)D concentrations of the proposed participants must be measured, and only subjects with low values should be included, that vitamin D doses used must raise 25(OH)D concentrations to values associated with reduced risk in observational studies, and that, therefore, achieved concentrations must be measured. However, most vitamin D RCTs have included many participants with relatively high 25(OH)D concentrations, have used too low vitamin D doses, and did not base their analyses on individual participant 25(OH)D concentrations.

Also overlooked in the editorial is that Mendelian randomization (MR) studies have now demonstrated the causality of vitamin D in reducing risk of several types of disease. In MR studies, data for alleles of genes involved in the vitamin D pathway are used to estimate genetic variations in serum 25(OH)D (genome-wide association studies) using perhaps 100,000 participants and have then examined health outcomes with those gene variants in large study populations. The assumption is that, because individuals are randomized into study groups by the genetic variants they carry, bias due to confounding and reverse causation is avoided [4]. The Hyppönen group, using MR analyses of findings stratified by baseline 25(OH)D concentration (i.e., non-linear analyses), has shown many significant effects of vitamin D in participants with low 25(OH)D concentrations. This methodology has already demonstrated causality for several health outcomes in their hands, including cardiovascular disease, dementia, and all-cause mortality rates, using data from the UK Biobank [4] as well as for hypertension, multiple sclerosis, and type 2 diabetes mellitus by others that they cite [4].

RCTs and MR studies have not supported the causality of vitamin D in the reducing risk of cancers. However, the evidence from observational studies and geographical ecological studies, as well as an understanding of the mechanisms involved, provides sufficient evidence for causality when considered by Hill's criteria for causality in a biological system [5, 6]. It should also be noted that the Vitamin D and Omega-3 Trial (VITAL) [7] had serious shortcomings including that the mean 25(OH)D concentration for those in the vitamin D treatment arm with 25(OH)D data was 30 ng/mL, that the vitamin D dose was 2000 IU/d but that all participants were permitted to take up to 600–800 IU/d vitamin D and to receive solar UVB, and that outcomes were not analyzed in terms of achieved 25(OH)D concentrations. Nevertheless, secondary analyses did find significant reductions for cancer incidence for those with a BMI <25 kg/m2 and overall reductions in the cancer mortality rate whe n the earliest years of data were omitted.
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Authors reply: March 2023

Journal of Internal Medicine https://doi.org/10.1111/joim.13622
Peter Bergman
Dear Editor,

I have read the letter by Dr Grant with great interest [1]. The question whether vitamin D can prevent common diseases, such as hypertension, diabetes and cardiovascular diseases is often debated. The field is somewhat polarised between hard-line sceptics and more positive “believers”. Both teams use a long line of evidence to support their respective views. In my editorial, I tried to shed light on some of the different views in the field and pointed out that there is still a lack of solid results from large, randomised and placebo-controlled clinical trials (RCTs) for most indications. One exception could be the effects on respiratory tract infections, where two large meta-analyses on RCTs have shown a small but statistically significant effects of about 8%–10% [2, 3]. However, two recent RCTs on vitamin D supplementation against COVID-19 failed to show any beneficial effect [4, 5]. These are just a few examples, but it is clear that we lack evidence from bona fide RCTs on the beneficial effects of vitamin D supplementation for most indications.
However, I do agree with Dr Grant that there are many other pieces of evidence that point in favour of vitamin D for many human diseases. For example, there is mechanistic evidence that vitamin D can modulate inflammation in T-cells from patients infected with SARS CoV-2 [6], vitamin D can directly induce antimicrobial peptides in human macrophages and fight tuberculosis [7] and – as an example, the vitamin D receptor is expressed in beta cells in the pancreas [8]. On top of these mechanistic leads, there are many observational studies that show that low vitamin D levels are associated with an increased risk for disease. And, more recently, several studies based on Mendelian randomisation analysis suggest that vitamin D levels can be linked to human disease. Up to this point, I agree with Dr Grant.

Nevertheless, the bar for certainty is higher than a plausible mechanism, observational evidence and Mendelian randomisation analyses and needs to be based on solid RCTs. It is always possible to find problems with available RCTs in the field and claim that they were not performed in the correct way. However, to be able to change paradigms and guidelines, we need solid evidence from RCTs and that is currently lacking for most indications, as I pointed out in my editorial. For medical doctors, including myself, it is important to follow guidelines and regulations. Thus, any clinical decision to start vitamin D supplementation has to be based on solid evidence. Dr Grant has a slightly different platform in this discussion, because he represents a company that produce and sell vitamin D supplements to the public. This difference might not be decisive for his standpoints but is nevertheless important to keep in mind as there could be a conflict of interest here.

To end in a more positive note, there is still a lot to discover in the field of vitamin D and the optimal RCT, which consider all possible confounders, has not yet been performed. Thus, there is more to learn and perhaps we will reach a more solid evidence base in this field in the future. Until then, I recommend a pragmatic approach where vitamin D supplementation should be directed towards risk-groups for vitamin D deficiency, such as the obese, pregnant women, and those with darker skin. A cut-off level of 50 nmol/L will work for most individuals and supplementation with 1000–2000 IU/day will support the bone, improve immunity, and potentially also reduce the risk for respiratory tract infections.
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Vitamin D is not just association - examples of RCTs finding that adding D fights diseases

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100 most-recently updated RCTs in VitaminDWiki - (from 900+)

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Items found: 1002
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Vitamin D supplementation improves muscle strength in healthy adults – meta-analysis of 6 RCT Aug 2014 31 Oct, 2016
Stress after natural disaster reduced by just 1000 IU Vitamin D – RCT Aug 2015 25 Oct, 2016
Tuberculosis not treated by lots of vitamin D for 16 weeks – RCT Sept 2015 21 Oct, 2016
800 IU of vitamin D got most white Danish children to 20 nanograms – RCT Oct 2016 18 Oct, 2016
3000 IU of Vitamin D – not much difference between capsule and spray – RCT Oct 2016 12 Oct, 2016
Cancer risk in older women reduced 32 percent by 2,000 IU of Vitamin D plus Calcium – 4 year RCT Oct 2016 12 Oct, 2016
Antibiotic use cut in half by elderly (over 70) after monthly 60,000 IU of vitamin D – RCT Dec 2013 06 Oct, 2016
Diabetes not treated by 28,000 IU of weekly vitamin D (proven again) – RCT Sept 2016 26 Sep, 2016
Vitamin D – monthly dosing was better than daily with Calcium – RCT Dec 2015 17 Sep, 2016
COPD reduced by 40 percent with monthly 100,000 IU of vitamin D – RCT Jan 2015 17 Sep, 2016
Falls cut in half by 100,000 IU vitamin D monthly - RCT 2016 17 Sep, 2016
Bone fractures after a burn - none if vitamin D, 6 if no vitamin D – RCT May 2015 04 Sep, 2016
Burn victims often have bone fractures, but not if supplemented with vitamin D3 – RCT May 2015 04 Sep, 2016
Gestational Diabetes treated with 50,000 IU every two weeks – RCT Sept 2016 03 Sep, 2016
IBS – 82 percent had low vitamin D, 3,000 IU spray helped a lot – RCT Dec 2015 25 Aug, 2016
Perinatal depression decreased 40 percent with just a few weeks of 2,000 IU of vitamin D – RCT Aug 2016 23 Aug, 2016
2000 IU of vitamin D for just 2 weeks helped in many ways – RCT June 2016 20 Aug, 2016
Leg bone (tibia) grew thicker with 4,000 IU of vitamin D and Calcium – RCT Aug 2016 19 Aug, 2016
Obese need more Vitamin D: Volume dilution, IU per pound, or BMI – RCT Dec 2012 14 Aug, 2016
Obese need 2.5 IU of vitamin D per kg to increase 1 ng (about 3.4 X more) – RCT Sept 2013 14 Aug, 2016
Most Olympic-class Dutch athletes nudged Vitamin D levels above 30 nanograms with 2200 IU daily – RCT July 2016 09 Aug, 2016
Decrease of Alzheimer’s biomarker halted by Resveratrol (perhaps due to vitamin D) – RCT Sept 2015 08 Aug, 2016
Sunscreen used daily vs discretionary: no difference in skin cancer rate – RCT 2016 06 Aug, 2016
5,000 IU daily or 50,000 IU Vitamin D weekly repleted many dark skinned adolescents – RCT Dec 2015 06 Aug, 2016
Childhood asthma still reduced 4 months after 800 IU of Vitamin D daily - RCT Feb 2016 03 Aug, 2016
Pregnancy – adding 35,000 IU Vitamin D weekly was nice, but not enough – RCT April 2016 23 Jul, 2016
Tanning bed twice a month slightly increased vitamin D levels during the winter – RCT Nov 2015 21 Jul, 2016
Wisdom tooth (3rd molar) extraction helped by Vitamin D loading dose – RCT March 2016 17 Jul, 2016
Non-alcoholic fatty liver disease (NAFLD) reduced somewhat by 50,000 IU vitamin D every 2 weeks – RCT Sept 2014 13 Jul, 2016
Vitamin D once during pregnancy reduced infant health care costs (300 times ROI) – RCT Dec 2015 09 Jul, 2016
Infant health costs not reduced by 1 dose of 200,000 IU vitamin D in late pregnancy – RCT Dec 2015 09 Jul, 2016
Decreased need for warfarin after Vitamin D levels optimized – RCT May 2016 04 Jul, 2016
Zinc helps pregnancies – 14 percent fewer preterm births, etc. – Cochrane RCT Feb 2015 14 Jun, 2016
Bone loss not stopped by monthly 48,000 IU of vitamin D – RCT June 2016 14 Jun, 2016
Just 1500 IU of Vitamin D significantly helps Prozac – RCT March 2013 14 Jun, 2016
Insulin resistance during pregnancy improved with 50,000 IU of vitamin D every 2 weeks – RCT April 2013 23 May, 2016
IBS quality of life improved by vitamin D (50,000 IU weekly) – RCT May 2016 17 May, 2016
Magnesium oxide is (surpringly) better than citrate – RCT March 2012 15 May, 2016
Menstrual Pain reduced by vitamin D – RCT Feb 2012 07 May, 2016
500,000 IU of vitamin D cut in half the hospital days following a lung failure – RCT 2015 06 May, 2016
Infants getting 1600 IU vitamin D during first year were more active and leaner at age 3 – RCT Feb 2016 06 May, 2016
Vitamin D improved child muscle mass even without varying dose with weight – RCT Feb 2016 06 May, 2016
Prenatal Vitamin D (35,000 weekly) resulted in 1 cm taller infants at age 1 year – RCT Aug 2013 30 Apr, 2016
Prenatal Vitamin D (35,000 weekly, 3rd trimester) resulted in 1 cm taller infants at age 1 year – RCT Aug 2013 30 Apr, 2016
Bacterial vaginosis reduced 3X by 2,000 IU of vitamin D – RCT June 2015 19 Apr, 2016
Bacterial vaginosis reduced 10 times by 2,000 IU of vitamin D – RCT June 2015 19 Apr, 2016
Five times less mite allergy when vitamin D added in mid pregnancy and to infant – RCT April 2016 17 Apr, 2016
2000 IU vitamin D during pregnancy and 800 IU to infant resulted in less use of antibiotics – RCT April 2014 17 Apr, 2016
Cognition of Alzheimer’s patients improved by daily 4,000 IU of vitamin D – RCT Jan 2015 16 Apr, 2016
Extreme preterm infants need a total of 1,000 IU of vitamin D daily – RCT April 2016 13 Apr, 2016
Infant much healthier if Gestational Diabetic mother got 2 doses of vitamin D – RCT Nov 2014 09 Apr, 2016
Every TB patient benefited from 2 doses of 600,000 IU of vitamin D – RCT Jan 2013 05 Apr, 2016
Tuberculosis treatment greatly helped by injection of 200,000 IU of vitamin D – RCT April 2016 05 Apr, 2016
PMS reduced by half in girls who had low levels of vitamin D – RCT Dec 2015 05 Apr, 2016
800 IU vitamin D for infant and 2000 IU for mother is good, not great – RCT Dec 2013 04 Apr, 2016
Tuberculosis -100 percent cure rate with 10,000 IU of vitamin D daily – RCT 2006 03 Apr, 2016
Vitamin D average level was 33 ng after 400,000 IU in 2 months - RCT July 2015 26 Mar, 2016
Infants getting up to 1600 IU did not increase blood level of vitamin D – RCT March 2016 13 Mar, 2016
Youths need 1500 IU to get even 20 ng of vitamin D – RCT March 2016 10 Mar, 2016
Knee osteoarthritis reduced somewhat by 50,000 IU vitamin D monthly (need more) – RCT Aug 2015 08 Mar, 2016
Staph infections with eczema reduced with 2,000 IU of vitamin D – RCT Oct 2015 13 Feb, 2016
Football Brain injuries prevented by Omega-3 – RCT Jan 2016 08 Feb, 2016
5X fewer school days missed due to asthma if take 2,000 IU vitamin D daily – RCT Feb 2016 05 Feb, 2016
Overweight women got 3X benefits from 8 weeks of Omega-3 – RCT Dec 2015 04 Feb, 2016
More calcium in bones in those teenage girls getting 2,000 IUs daily – RCT Jan 2016 04 Feb, 2016
Inflammation reduced by a single dose of Vitamin D (200,000 IU) – RCT Jan 2016 23 Jan, 2016
Senior muscles increased somewhat with Omega-3 – RCT July 2015 18 Jan, 2016
Gestational Diabetes helped by Vitamin D and Calcium (also less C-section and LGA) – RCT Jan 2016 16 Jan, 2016
Gestational diabetes – Vitamin D and Calcium provided huge benefits – RCT March 2015 13 Jan, 2016
Rate of falls reduced 2X by just 1000 IU of vitamin D – RCT Nov 2015 23 Dec, 2015
4000 IU Vitamin D Safe and Effective For Healthy Pregnant Women – RCT June 2011 18 Dec, 2015
Acute respiratory infection worsened by too infrequent vitamin D supplementation – RCT June 2015 17 Dec, 2015
Overweight women on caloric restriction diet got 3X benefits from 8 weeks of Omega-3 – RCT Dec 2015 15 Dec, 2015
Overweight women got 3X benefits from 8 weeks of Omega-3 and exercise vs placebo – RCT Dec 2015 15 Dec, 2015
Back pain not relieved when vitamin D levels remained below 30 nanograms – RCT Nov 2015 04 Dec, 2015
Depression not reduced when vitamin D levels less than 30 nanograms – RCT Nov 2015 04 Dec, 2015
Schizophrenia treated by 6 months of Omega-3 – RCT Nov 2015 28 Nov, 2015
Seasonal affective disorder not treated by 2800 IU of vitamin D (no surprise) – RCT Aug 2014 15 Nov, 2015
Improved births with 2,000 IU vitamin D during pregnancy in India - RCT Feb 2015 12 Nov, 2015
Vitamin D during pregnancy increases infant levels for two months – RCT Nov 2015 12 Nov, 2015
Fibromyalgia pain reduced with vitamin D intervention that achieved 30-48 ng – RCT Feb 2014 05 Nov, 2015
Musculoskeletal pain reduced with 4,000 IU of vitamin D – RCT April 2015 05 Nov, 2015
Muscle strength of Judo athletes increased 13 percent following single dose of 150,000 IU vitamin D – RCT Nov 2015 05 Nov, 2015
Allergic Rhinitis (hay fever) reduced by just 1,000 IU of vitamin D for 30 days – RCT Sept 2015 02 Nov, 2015
2000 IU of vitamin D during pregnancy got most infants to more than 12 ng (need more) – RCT Aug 2015 21 Oct, 2015
2,000 IU of vitamin D during pregnancy got infants to just above 12 ng – RCT July 2015 21 Oct, 2015
Congestive heart failure in infants virtually cured by 1000 IU of vitamin D – RCT Feb 2012 20 Oct, 2015
Colon Cancer proven again to not be treated by just 1000 IU of vitamin D – RCT Oct 2015 20 Oct, 2015
5,000 IU Vitamin D was not enough to reduce preeclampsia but did help future infant – RCT April 2014 15 Oct, 2015
Colds not decreased if people already vitamin D sufficient – RCT Oct 2012 13 Oct, 2015
Respiratory diseases helped by vitamin D if initially have low level – RCT review Jan 2015 13 Oct, 2015
MRI (8 weeks) cut vitamin D levels of rats in half - RCT July 2015 04 Oct, 2015
MRI (perhaps 400 hours) cut vitamin D levels of rats in half - RCT July 2015 04 Oct, 2015
Chron’s disease helped when vitamin D level raised above 30 ng – RCT Feb 2015 03 Oct, 2015
Gestational diabetes reduced by just two 50,000 IU doses of vitamin D – RCT Nov 2014 02 Oct, 2015
Hypertension reduction sometimes needs more than 4,000 IU of vitamin D for 6 months – RCT Oct 2014 22 Sep, 2015
Post menopausal vaginal dryness treated with vitamin D vaginal suppositories – RCT March 2015 16 Sep, 2015
Monthly 100,000 IU vitamin D supplementation got virtually all vitamin D deficient subjects above 20 ng – RCT April 2014 15 Sep, 2015
Vitamin D given once every two months does not help – proven again – RCT Sept 2015 15 Sep, 2015
Rate of injuries from falls cut in half by just 800 IU of vitamin D and exercise – RCT May 2015 13 Sep, 2015

100 most-recently updated Meta-analyses in VitaminDWiki - (from 600+)

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Is low Vitamin D just a marker of disease - March 2023        
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