Delayed Processing of Chilled Whole Blood for 24 Hours Does Not Affect the Concentration of the Majority of Micronutrient Status Biomarkers

Kerry S Jones; Sarah R Meadows; Karen Chamberlain; Damon A Parkington; Dave Collins; Polly Page; Albert Koulman

doi:10.1093/jn/nxab267

Delayed Processing of Chilled Whole Blood for 24 Hours Does Not Affect the Concentration of the Majority of Micronutrient Status Biomarkers

J Nutr. 2021 Nov 2;151(11):3524-3532. doi: 10.1093/jn/nxab267.

Authors

Kerry S Jones¹, Sarah R Meadows^{1

2}, Karen Chamberlain², Damon A Parkington¹, Dave Collins³, Polly Page^{2

3}, Albert Koulman¹

Affiliations

¹ Nutritional Biomarker Laboratory, Medical Research Council Epidemiology Unit, University of Cambridge, Cambridge, UK.
² Medical Research Council Elsie Widdowson Laboratory, Cambridge, UK.
³ Medical Research Council Epidemiology Unit, University of Cambridge, Cambridge, UK.

Abstract

Background: The measurement of micronutrient status is essential to understand the health of individuals and populations, but there are limited data on the stability of micronutrients in whole blood.

Objectives: The objective was to investigate the effects of delayed processing of whole blood on the stability of 25 micronutrient and selected clinical biomarkers.

Methods: Blood from 16 healthy adults was collected into EDTA, lithium heparin (LH), or serum tubes. Samples were processed within 2 hours of collection ("2-hour processed") or mailed overnight (boxed with frozen cold packs) before processing ("24-hour processed"). Micronutrient and clinical biomarker concentrations were quantified with validated methods. The concentration percentage difference between the 2- and 24-hour processed samples was calculated and was compared against quality specifications determined from intra- and interindividual variations.

Results: All analytes had a sample type where the percentage difference concentration between 2-hour and 24-hour processed samples was ≤4% and was acceptable based on calculated limits, including for biomarkers of vitamin A, vitamin D, thiamin, folate, vitamin B-12, iron (ferritin), and zinc status and for selected clinical markers, C-reactive protein, HDL and total cholesterol, and triglycerides. EDTA plasma vitamin C was lower compared to the 2-hour processed sample (geometric mean, 43%; 95% CI: 36%-49%). Pyridoxal-5-phosphate (vitamin B-6 biomarker) decreased, with differences from the 2-hour processed samples of -8% (95% CI: -13% to -2%) and -14% (95% CI: -18% to -9%) in LH plasma and serum, respectively.

Conclusions: In blood collected from adult participants, delayed processing of chilled whole blood for 24 hours did not materially affect the measured concentrations of the majority of micronutrients and selected clinical biomarkers. This suggests that for these analytes, adherence to a 2-hour processing protocol may be unnecessary. This knowledge is valuable and may help to simplify logistics for sample transport and processing of blood samples for micronutrient status assessment.

Keywords: NDNS; micronutrients; nutrition surveys; nutritional assessment; vitamin.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Biomarkers
Folic Acid
Humans
Micronutrients*
Nutritional Status
Vitamin B 12
Vitamins*

Substances

Biomarkers
Micronutrients
Vitamins
Folic Acid
Vitamin B 12

Grants and funding

MC_U105960384/MRC_/Medical Research Council/United Kingdom