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Vitamin D Binding Protein


178 items in Vitamin D Binding Protein category

See also Vitamin D Receptor   Genetics   CYP27B1

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Vitamin D Binding Protein (GC) gene can decrease the bio-available Vitamin D that can get to cells,

  • GC is not the only such gene - there are 3 others, all invisible to standard Vitamin D tests
  • The bio-available calculation does not notice the effect of GC, CYP27B1, CYP24A1, and VDR
  • The actual D getting to the cells is a function of measured D and all 4 genes
  • There is >2X increase in 8+ health problems if have poor VDBP (GC)
  • It appears that VDBP only blocks oral vitamin D,

Increased risk of health problems if poor VDBP

Increased
Risk
Health Problem
11 XPreeclampsia
6.5XT1D in SA Blacks
6 XFood Allergy
5 XPTSD
4 X, 5XKidney Cancer
4 XPoor Response to Oral Vitamin D
3 XEar infection
2.8 X MS
2.5 XSevere Autism
2 X Colorectal Cancer
2 XProstate Cancer -in those with dark skins
1.3 XInfertility

VDBP is NOT directly detected by vitamin D blood tests

in Visio for 2023


MS and Vitamin D Binding Protein 7 studies


TB and Vitamin D Binding Protein - 4 studies


Breathing and Vitamin D Binding Protein - 7 studies


Infant-Child and Vitamin D Binding Protein - 8 studies


Pregnancy and Vitamin D Binding Protein - 10 studies


Vitamin D Binding Protein and Its Gene Polymorphisms —The Risk of Malignant Tumors and Other Diseases - Oct 2020

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178 VDBP studies


Low response to Vitamin D can be improved in many ways


See also web

  • Meta-analysis of vitamin D-binding protein and cancer risk Sept 2015
    • "Results: We found a borderline decrease in cancer risk for subjects with high compared to low levels of DBP"
    • "We included 28 independent studies concerning: basal cell carcinoma, bladder, breast, colon-rectum, endometrium, liver, esophagus, stomach, melanoma, pancreas, prostate and kidney. "

Vitamin D Binding Protein mutations are not noticed by the Vitamin D Test – March 2024

Factors to take into account when interpreting 25-hydroxy-vitamin D serum levels
Acta Clin Belg. 2024 Mar 7:1-6. doi: 10.1080/17843286.2024.2327218 – PDF behind a $65 paywall
Joris R Delanghe 1, Marijn M Speeckaert 2 3, Thomas Maenhout 1

Background: Assessing vitamin D status, typically evaluated using serum or plasma 25-hydroxy vitamin D [25(OH)D] concentration, is complex because of various influencing factors.

Methods: Seasonality significantly affects intra-individual variability in 25(OH)D levels. This variation can be addressed by employing cosinor functions that are tailored to the geographical location of the patient to correct for seasonal effects. In addition to seasonality, genetic factors, such as DBP polymorphism and body composition, particularly adiposity, play crucial roles. Dialysis patients with DBP 2-2 phenotype exhibit higher vitamin D requirements. Genotyping/phenotyping of DBP allows for better tailored vitamin D supplementation. The lipid-soluble nature of vitamin D also interacts with plasma components such as serum triglycerides, which can influence vitamin D measurements. Adiposity, which is negatively correlated with vitamin D concentration, necessitates body mass-based mathematical adjustments for accurate vitamin D assessment in subjects with extreme BMI values.

Conclusions: Accordingly, vitamin D replacement therapy must be personalized, taking into account factors such as body size and seasonal variations, to effectively reach the target serum 25(OH)D concentrations.

Introduction (from DeepDyve)
Owing to a markedly increased interest in the role of vitamin D in human health, the determination of 25- hydroxy vitamin D [25(OH)D] in serum or plasma has become a frequently requested laboratory test [1 ]. This rise in popularity can be attributed not only to the growing recognition of the wide-ranging health impli­cations of vitamin D [2,3] but also to significant advancements in the effectiveness of vitamin D analysis techniques [3].

The intraindividual biological variability (CVI) has been reported to be 4.7% for 25-hydroxy vitamin D. In contrast, interindividual variation (CVG), repre­senting diverse homeostatic points among subjects within the same population, was significantly higher at 64.3% for 25(OH)D [4]. The calculated reference change value (RCV) for 25(OH)D was 18.0%. These data indicate that interindividual variation markedly surpasses intraindividual variation in 25(OH)D levels [4].

On top of the biological variation of 25(OH) vitamin D, in moderate and Arctic climates, vitamin D levels exhibit significant seasonal variability, pri­marily due to changes in sunlight exposure. This variability becomes more pronounced with increas­ing distance from the equator, with studies indicat­ing a marked decrease in vitamin D synthesis in populations at higher latitudes. The biological mechanisms underlying this phenomenon, includ­ing the reduced capacity of the skin to synthesize vitamin D under lower UV conditions, warrant further discussion [5,6].
Vitamin D, a fat-soluble vitamin, relies on a specific transport protein, known as the vitamin D binding protein (DBP), for its circulation in the bloodstream. This binding protein plays a crucial role in the bioavail- abilitv and metabolic reoulation of vitamin D. nosino a complex challenge for interpreting the vitamin D status from serum or plasma 25(OH)D concentra­tions. The complexities of this relationship, particularly in different physiological and pathological states, emphasize the need for a more nuanced approach to vitamin D analysis [7].

Most clinical laboratories tend to oversimplify the interpretation of vitamin D status by comparing test results with generic 'summer' and 'winter' reference values. These seasonal reference values, which are often inadequately defined, fail to offer a comprehensive cor­rection for individual variability and geographical differ­ences, leading to potential misinterpretations in vitamin D status assessment. The scientific basis for these refer­ence values, as well as alternative methodologies that might provide more accurate assessments, are areas ripe for exploration [8-10].
Most clinical laboratories tend to oversimplify the interpretation of vitamin D status by comparing test....


Studies of VDBP and diseases: Pregnancy 10, Skin - Dark 8, Breathing 7, Infant-Child 7, Multiple Sclerosis 6, Virus 6, Cardiovascular 6, Diabetes 5, Autoimmune 4, Cancer - Other 4, Obesity 4, Tuberculosis 4 – Jan 2024

Vitamin D Binding Protein        
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14479 VDBP2.jpg admin 28 Oct, 2020 368.38 Kb 1531
14478 VDBP1.jpg admin 28 Oct, 2020 583.07 Kb 1599
14477 VDBP tumors, etc..pdf admin 28 Oct, 2020 1.04 Mb 757