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  2. Integrative Genomic Analysis Reveals Four Protein Biomarkers for Platelet Traits

Integrative Genomic Analysis Reveals Four Protein Biomarkers for Platelet Traits

  • Circ Res. 2020 Oct 9;127(9):1182-1194. doi: 10.1161/CIRCRESAHA.119.316447.
Dong Heon Lee 1 2 Chen Yao 1 2 Arunoday Bhan 3 Thorsten Schlaeger 3 Joshua Keefe 1 2 Benjamin A T Rodriguez 1 2 Shih-Jen Hwang 2 Ming-Huei Chen 1 2 Daniel Levy 1 2 Andrew D Johnson 1 2
Affiliations

Affiliations

  • 1 The Framingham Heart Study, Framingham, MA (D.H.L., C.Y., J.K., B.A.T.R., S,-J.H., M.-H.C., D.L., A.D.J.).
  • 2 Population Sciences Branch, Division of Intramural Research, National Heart, Lung and Blood Institute National Institutes of Health, Bethesda, MD (D.H.L., C.Y., J.K., B.A.T.R., S.-J.H., M.-H.C., D.L., A.D.J.).
  • 3 Boston Children's Hospital, Boston, MA (A.B., T.S.).
Abstract

Rationale: Mean platelet volume (MPV) and platelet count (PLT) are platelet measures that have been linked to Cardiovascular Disease (CVD) and mortality risk. Identifying protein biomarkers for these measures may yield insights into CVD mechanisms.

Objective: We aimed to identify causal protein biomarkers for MPV and PLT among 71 CVD-related plasma proteins measured in FHS (Framingham Heart Study) participants.

Methods and results: We conducted integrative analyses of genetic variants associated with PLT/MPV with protein quantitative trait locus variants associated with plasma proteins followed by Mendelian randomization to infer causal relations of proteins for PLT/MPV. We also tested protein-PLT/MPV association in FHS participants. Using induced pluripotent stem cell-derived megakaryocyte clones that produce functional platelets, we conducted RNA-sequencing and analyzed expression differences between low- and high-platelet producing clones. We then performed small interfering RNA gene knockdown experiments targeting genes encoding proteins with putatively causal platelet effects in megakaryocyte clones to examine effects on platelet production. In protein-trait association analyses, ten proteins were associated with MPV and 31 with PLT. Mendelian randomization identified 4 putatively causal proteins for MPV and 4 for PLT. GP-5 (Glycoprotein V), GRN (granulin), and MCAM (melanoma cell adhesion molecule) were associated with PLT, while MPO (myeloperoxidase) showed significant association with MPV in both analyses. RNA-sequencing analysis results were directionally concordant with observed and Mendelian randomization-inferred associations for GP-5, GRN, and MCAM. In siRNA gene knockdown experiments, silencing GP-5, GRN, and MPO decreased PLTs. Genome-wide association study results suggest several of these may be linked to CVD risk.

Conclusions: We identified 4 proteins that are causally linked to PLTs. These proteins may also have roles in the pathogenesis of CVD via a platelet/blood coagulation-based mechanism.

Keywords

biomarkers; cardiovascular diseases; genetics; megakaryocytes; proteomics.

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