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Oral Disease and Atherosclerosis May Be Associated with Overlapping Metabolic Pathways.

Author information

Affiliations

  • 1. Department of Oral and Craniofacial Sciences, School of Dental Medicine, University of Pittsburgh, Pittsburgh, PA, USA.
      Authors
    • Bezamat M 1
    • Baxter DJ 1
    • Shaffer JR 1
    • Marazita ML 1
    (4 authors)
  • 2. Heart and Vascular Institute, University of Pittsburgh Medical Center, Pittsburgh, PA, USA.
      Authors
    • Saeed A 2
    • Reis SE 2
    (2 authors)
  • 3. Department of Statistics, University of Pittsburgh, Pittsburgh, PA, USA.
      Authors
    • McKennan C 3
    • Duan J 3
    (2 authors)
  • 4. Center for Biostatistics and Data Science, Institute for Informatics, Data Science, and Biostatistics (I2BD), Washington University in St. Louis, School of Medicine, St. Louis, MO, USA.
      Authors
    • Zhou R 4
    • Liu L 4
    • Las Fuentes L 4
    (3 authors)
  • 5. Department of Epidemiology, University of Michigan School of Public Health, Ann Arbor, MI, USA.
      Authors
    • Foxman B 5
    (1 author)
    • Show all (6)

ORCIDs linked to this article

JDR Clinical and Translational Research, 09 Oct 2024, :23800844241280383
https://doi.org/10.1177/23800844241280383 PMID: 39385367 

Abstract 

Objectives

Dental caries and periodontitis are among the most prevalent chronic diseases worldwide and have been associated with atherosclerotic cardiovascular diseases (ASCVD). This study aimed to determine (1) the independent associations between subclinical ASCVD markers (carotid intima media thickness [CIMT] and coronary artery calcification [CAC]) and quantitative indices of oral disease including the decayed, missing, and filled teeth (DMFT) index, gingivitis parameters, periodontal status, and number of teeth lost and (2) the extent to which metabolites altered in individuals with oral disease overlapped with those altered in individuals with ASCVD.

Methods

We used data from 552 participants recruited through the Dental Strategies Concentrating on Risk Evaluation project. Oral examinations were conducted, and CIMT and CAC were measured. Multiple linear regression models were constructed with CIMT and CAC as dependent variables in the epidemiologic analysis. In the metabolomic analysis, logistic or linear regression was used to test 1,228 metabolites for association with each phenotype adjusted for age, sex, race, blood pressure, smoking, diabetes, cholesterol, high-sensitivity C-reactive protein, and interleukin-6.

Results

None of the oral disease markers were significant predictors of ASCVD markers in the fully adjusted models. However, critical lipid and lipid-signaling pathway metabolites were significantly associated with gingivitis, periodontitis, and DMFT: the lysophospholipid pathway (odds ratio [OR] = 2.29, false discovery rate [FDR]-adjusted P = 0.038) and arachidonate with gingivitis (OR = 2.35, FDR-adjusted P = 0.015), the sphingolipid metabolism pathway with periodontitis (OR = 2.09, FDR-adjusted P = 0.029), and borderline associations between plasmalogen and lysophospholipid pathways and DMFT (P = 0.055). Further, the same metabolite from the sphingolipid metabolism pathway, sphingomyelin (d17:1/14:0, d16:1/15:0), was inversely associated with both CIMT (β = -0.14, FDR-adjusted P = 0.014) and gingivitis (OR = 0.04, FDR-adjusted P = 0.033).

Conclusions

The discovery of a common sphingomyelin metabolite in both disease processes is a novel finding suggesting that gingivitis and periodontitis may be associated with some overlapping metabolic pathways associated with ASCVD and indicating potential shared mechanisms among these diseases.

Knowledge transfer statement

The same metabolites may be altered in atherosclerosis and oral disease. Specifically, a common sphingomyelin metabolite was inversely associated with gingivitis and carotid intima media thickness, a subclinical marker of atherosclerotic cardiovascular disease. These findings can provide valuable insights for future mechanistic studies to establish potential causal relationships, with the hope of influencing disease prevention and targeted early treatment.

Full text links 

Read article at publisher's site: https://doi.org/10.1177/23800844241280383

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Funding 

Funders who supported this work.

NIDCR NIH HHS (1)

National Heart, Lung, and Blood Institute (1)

Pennsylvania Department of Health (1)

national institutes of health (4)