Modeling a methylmalonic acid–derived change point for serum vitamin B-12 for adults in NHANES

dc.contributor.author Bailey, Regan
dc.contributor.author Durazo-Arvizu, Ramon
dc.contributor.author Carmel, Ralph
dc.contributor.author Green, Ralph
dc.contributor.author Pfeiffer, Christine
dc.contributor.author Sempos, Christopher
dc.contributor.author Carriquiry, Alicia
dc.contributor.author Yetley, Elizabeth
dc.contributor.department Statistics
dc.date 2018-02-17T06:21:09.000
dc.date.accessioned 2020-07-02T06:57:34Z
dc.date.available 2020-07-02T06:57:34Z
dc.date.issued 2013-01-01
dc.description.abstract <p>Background: No consensus exists about which cutoff point should be applied for serum vitamin B-12 (SB-12) concentrations to define vitamin B-12 status in population-based research. Objective: The study’s aim was to identify whether a change point exists at which the relation between plasma methylmalonic acid (MMA) and SB-12 changes slope to differentiate between inadequate and adequate vitamin B-12 status by using various statistical models. Design:We used data on adults ($19 y; n = 12,683) from NHANES 1999–2004—a nationally representative, cross-sectional survey. We evaluated 6 piece-wise polynomial and exponential decay models that used different control levels for known covariates. Results: The MMA-defined change point for SB-12 varied depending on the statistical model used. A linear-splines model was determined to best fit the data, as determined by the approximate permutation test; 3 slopes relating SB-12 and MMA and resulting in 2 change points and 3 subgroups were shown. The first group (SB-12 ,126 pmol/L) was small and had the highest MMA concentration (median: 281 nmol/L; 95% CI: 245, 366 nmol/L; n = 157, 1.2%); many in this group could be considered at high risk of severe deficiency because combined abnormalities of MMA and homocysteine were very frequent and the concentrations themselves were significantly higher. The highest SB-12 group (SB-12 .287 pmol/ L; n = 8569, 67.6%) likely had adequate vitamin B-12 status (median MMA: 120 nmol/L; 95% CI: 119, 125 nmol/L). The vitamin B-12 status of the sizable intermediate group (n = 3957, 33%) was difficult to interpret. Conclusions: The 3 distinct slopes for the relation between SB-12 and MMA challenges the conventional use of one cutoff point for classifying vitamin B-12 status. In epidemiologic research, the use of one cutoff point would fail to separate the small, severely deficient group from the intermediate group that has neither normal nor clearly deficient vitamin B-12 concentrations (ie, unknown vitamin B-12 status). This intermediate group requires further characterization.</p>
dc.description.comments <p>This article is from <em>American Journal of Clinical Nutrition</em> 98 (2013): 460, doi: <a href="http://dx.doi.org/10.3945/ajcn.113.061234" target="_blank">10.3945/ajcn.113.061234</a>.</p>
dc.format.mimetype application/pdf
dc.identifier archive/lib.dr.iastate.edu/stat_las_pubs/27/
dc.identifier.articleid 1032
dc.identifier.contextkey 7855525
dc.identifier.s3bucket isulib-bepress-aws-west
dc.identifier.submissionpath stat_las_pubs/27
dc.identifier.uri https://dr.lib.iastate.edu/handle/20.500.12876/90587
dc.language.iso en
dc.source.bitstream archive/lib.dr.iastate.edu/stat_las_pubs/27/2013_CarriquiryAL_ModelingMethlmalonicAcid.pdf|||Fri Jan 14 23:05:22 UTC 2022
dc.source.uri 10.3945/ajcn.113.061234
dc.subject.disciplines Biochemical Phenomena, Metabolism, and Nutrition
dc.subject.disciplines Statistics and Probability
dc.subject.keywords cyanocobalamin
dc.subject.keywords homocysteine
dc.subject.keywords methylmalonic acid
dc.subject.keywords amino acid blood level
dc.subject.keywords drug exposure
dc.subject.keywords population research
dc.subject.keywords vitamin blood level
dc.subject.keywords vitamin supplementation
dc.subject.keywords vitamin B 12
dc.title Modeling a methylmalonic acid–derived change point for serum vitamin B-12 for adults in NHANES
dc.type article
dc.type.genre article
dspace.entity.type Publication
relation.isAuthorOfPublication 6ddd5891-2ad0-4a93-89e5-8c35c28b0de4
relation.isOrgUnitOfPublication 264904d9-9e66-4169-8e11-034e537ddbca
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