A new trauma frontier: Exploratory pilot study of platelet transcriptomics in trauma patients

Alexander T Fields; Man-Cheung Lee; Fahima Mayer; Yale A Santos; Cedric M V Bainton; Zachary A Matthay; Rachael A Callcut; Nasima Mayer; Joseph Cuschieri; Kord M Kober; Roland J Bainton; Lucy Zumwinkle Kornblith

doi:10.1097/TA.0000000000003450

A new trauma frontier: Exploratory pilot study of platelet transcriptomics in trauma patients

J Trauma Acute Care Surg. 2022 Feb 1;92(2):313-322. doi: 10.1097/TA.0000000000003450.

Authors

Alexander T Fields¹, Man-Cheung Lee, Fahima Mayer, Yale A Santos, Cedric M V Bainton, Zachary A Matthay, Rachael A Callcut, Nasima Mayer, Joseph Cuschieri, Kord M Kober, Roland J Bainton, Lucy Zumwinkle Kornblith

Affiliation

¹ From the Department of Surgery (A.T.F., Y.A.S., Z.A.M., J.C., L.Z.K.), Department of Anesthesia (M.-C.L., F.M., C.M.V.B., N.M., R.J.B.), Zuckerberg San Francisco General Hospital and the University of California, San Francisco; and Bakar Computational Health Sciences Institute (R.A.C., K.M.K.), University of California, San Francisco, San Francisco, California.

Abstract

Background: The earliest measurable changes to postinjury platelet biology may be in the platelet transcriptome, as platelets are known to carry messenger ribonucleic acids (RNAs), and there is evidence in other inflammatory and infectious disease states of differential and alternative platelet RNA splicing in response to changing physiology. Thus, the aim of this exploratory pilot study was to examine the platelet transcriptome and platelet RNA splicing signatures in trauma patients compared with healthy donors.

Methods: Preresuscitation platelets purified from trauma patients (n = 9) and healthy donors (n = 5) were assayed using deep RNA sequencing. Differential gene expression analysis, weighted gene coexpression network analysis, and differential alternative splicing analyses were performed. In parallel samples, platelet function was measured with platelet aggregometry, and clot formation was measured with thromboelastography.

Results: Differential gene expression analysis identified 49 platelet RNAs to have differing abundance between trauma patients and healthy donors. Weighted gene coexpression network analysis identified coexpressed platelet RNAs that correlated with platelet aggregation. Differential alternative splicing analyses revealed 1,188 splicing events across 462 platelet RNAs that were highly statistically significant (false discovery rate <0.001) in trauma patients compared with healthy donors. Unsupervised principal component analysis of these platelet RNA splicing signatures segregated trauma patients in two main clusters separate from healthy controls.

Conclusion: Our findings provide evidence of finetuning of the platelet transcriptome through differential alternative splicing of platelet RNA in trauma patients and that this finetuning may have relevance to downstream platelet signaling. Additional investigations of the trauma platelet transcriptome should be pursued to improve our understanding of the platelet functional responses to trauma on a molecular level.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Blood Coagulation Disorders / etiology*
Blood Coagulation Disorders / genetics*
Blood Platelets / metabolism*
Female
Gene Expression Profiling
Humans
Male
Pilot Projects
Platelet Activation
Platelet Aggregation
RNA / metabolism*
Thrombelastography
Transcriptome*
Wounds and Injuries / complications*

Substances

RNA

Abstract

Publication types

MeSH terms

Substances

Grants and funding