BEVITAL AS

Mix-and-Match

Project-specific panels featuring analytes across 25 categories.

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Mix-and-Match

Project-specific panels featuring analytes across 25 categories.

Request a quote today
Mix-and-match

Home > Metabolomics > Mix-and-Match

Platform organisation

Maximum Flexibility for Individualized Solutions.

Bevital’s targeted metabolomics panels have been designed to be analytically and biologically complementary and are established across dedicated GC- and LC-MS/MS platforms. Our approach allows quantification of diverse, but related classes of both high- and low-abundance metabolites

Our panels offer researchers great flexibility by mixing different metabolites from Bevital’s repertoire and compose individual solutions specific to the demands of their project. Metabolites of interest not yet included may be incorporated into existing assays or established as customized targeted analyses.

Metabolites

Metabolites & Pathways

AGEs

2 markers by GC-MS/MS

Amino acids and metabolites

31 markers by GC- and LC-MS/MS

Acylcarnitines

23 markers by LC-MS/MS

Bile acids

25 markers by LC-MS/MS

Choline oxidation pathway

7 markers by GC- and LC-MS/MS

Citric acid cycle

8 markers by GC-MS/MS

Microbiota derived

17 markers by GC-and LC-MS/MS

NAD
metabolome

14 markers by GC- and LC-MS/MS

One carbon metabolism

16 markers by GC- and LC-MS/MS

Transsulfuration

2 markers by GC-MS/MS

Tryptophan metabolites

19 markers by LC-MS/MS

Urea cycle

4 markers by GC- and LC-MS/MS

Others

2 markers by LC-MS/MS

Pathology

Pathologies

Diabetes

9 markers by GC-, LC-MS/MS and MALDI-TOF MS

Endothelial function

4 markers by LC-MS/MS

Inflammation

6 markers by LC-MS/MS and MALDI-TOF MS

Ketone bodies

2 markers by GC-MS/MS

Liver pathology

1 markers by GC-MS/MS

Neuroactive

4 markers by LC-MS/MS

Oncometabolites

4 markers by GC-MS/MS

Renal function

3 markers by LC-MS/MS and MALDI-TOF MS

Uremic toxin

2 markers by GC- and LC-MS/MS

* Analyses of protein markers by MALDI-MS have been discontinued and will be replaced by alternative methods.

Nutrition

Nutritional Status & Lifestyle

B vitamins

14 markers by LC-MS/MS and microbiological assay

Folate & cobalamin

8 markers by GC- and LC-MS/MS and microbiological assay

Fat soluble vitamins

4 markers by LC-MS/MS

Meat &
fish intake

4 markers by GC- and LC-MS/MS

Tobacco & coffee

3 markers by LC-MS/MS

October 29, 2025
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Statistical power is the probability that a statistical test will correctly reject a false null hypothesis (H0​) when a specific alternative hypothesis (H1​) is true. H0​ is the null hypothesis, which states there is no effect or no difference. H1​ is the alternative hypothesis, which states there is a real effect or difference. Alpha (α) is the probability of a Type I error (a false positive), which is the risk of incorrectly rejecting the H0​ when it is actually true. You set this value before the experiment, commonly at 0.05. Beta (β) is the probability of a Type II error (a false negative), which is the risk of failing to reject the H0​ when it is actually false.

Power is calculated as 1−β. Increasing power means you are decreasing the probability of making a Type II error.

Several factors can be adjusted to increase the power of a statistical test:

  • Effect Size: This is the magnitude of the difference you are trying to detect. A larger effect size is easier to detect, thus increasing power. 

  • Sample Size: The number of observations in a study. A larger sample size provides more information about the population, reducing the margin of error and increasing the power to detect a true effect.

  • Variation: Refers to the spread or standard deviation of the data within the population. Less variation makes it easier to distinguish a real effect from random noise, thereby increasing power.

  • Alpha (): Increasing the alpha level (e.g., from 0.05 to 0.10) also increases power, but at the cost of a higher risk of a Type I error. This trade-off is often undesirable.

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561.

Vollset, S E; Nygârd, O; Refsum, H; Ueland, P M

Coffee and homocysteine Miscellaneous

2000, ISSN: 0002-9165.

Links | BibTeX

562.

Schneede, J; Refsum, H; Ueland, P M

Biological and environmental determinants of plasma homocysteine Journal Article

In: Semin Thromb Hemost, vol. 26, no. 3, pp. 263–279, 2000, ISSN: 0094-6176.

Abstract | Links | BibTeX

562 entries « 29 of 29 »

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