Whole blood transcriptomics identifies subclasses of pediatric septic shock

Jamie O Yang; Matt S Zinter; Matteo Pellegrini; Man Yee Wong; Kinisha Gala; Daniela Markovic; Brian Nadel; Kerui Peng; Nguyen Do; Serghei Mangul; Vinay M Nadkarni; Aaron Karlsberg; Dhrithi Deshpande; Manish J Butte; Lisa Asaro; Michael Agus; Anil Sapru; Study Site Investigators for CAF-PINT

doi:10.1186/s13054-023-04689-y

Whole blood transcriptomics identifies subclasses of pediatric septic shock

Crit Care. 2023 Dec 8;27(1):486. doi: 10.1186/s13054-023-04689-y.

Authors

Jamie O Yang¹, Matt S Zinter², Matteo Pellegrini³, Man Yee Wong⁴, Kinisha Gala⁴, Daniela Markovic⁵, Brian Nadel⁶, Kerui Peng⁶, Nguyen Do⁴, Serghei Mangul^{6

7}, Vinay M Nadkarni⁸, Aaron Karlsberg⁶, Dhrithi Deshpande⁶, Manish J Butte⁹, Lisa Asaro¹⁰, Michael Agus¹⁰, Anil Sapru¹¹; Study Site Investigators for CAF-PINT

Collaborators

Study Site Investigators for CAF-PINT:
Michael Agus, Vijay Srinivasan, Ranjit S Chima, Neal J Neal, Christopher Newth, Amanda B Hassinger, Kris Bysani, Edward Vincent Faustino, Faustino Hirshberg, Kupper Wintergerst, Janice E Sullivan, Adam Schwarz, Lauren Sorce, Lauren Marsillio, Natalie Cvijanovich, Heidi Flori, Flori Pham, Mary Dahmer, Myke Federman, Kayley Wong, Sitaram S Vangala, Matteo Pellegrini, Brunilda Balliu, Kinisha P Gala, Sholeen Nett, Marcy Singleton, Neethi Pinto, Grace Chong, Shirley Viteri, Anil Sapru, Patrick McQuillen, Matt Zinter, Kerry Coughlin-Wells, Kyle Hughes, Jaclyn French, Meghan Fitzgerald, Martha Sisko, Kelli Howard, Rhonda Jones, Debbie Spear, Peter Eldridge, Jeni Kwok, Haiping Qiao, Tracey Monjure, Joana Tala, Sarah A Kandil, Tyler Quinn, Jennifer Lilley, Kristen Lee, Cathy Flores, Ofelia Vargas-Shiraishi, Avani Shukla, Becky Brumfield, Cheryl Stone, Chaandini Jayachandran, Theresa Kirkpatrick, Tanaya Deshmukh, Manvita Mareboina, Nguyen Do, Neda Ashtari, Anna Ratiu, Dean Jarvis, Mary McNally, Karlyn Martini, Chiara Rodgers, Ramany John, Teresa Mulholland, Gwen Pellicciotti, Shrey Goel, Mustafa Alkhouli, Anne McKenzie, Denise Villarreal-Chico

Affiliations

¹ UCLA Department of Internal Medicine, David Geffen School of Medicine, Los Angeles, CA, USA.
² UCSF Department of Pediatrics, San Francisco, CA, USA.
³ UCLA Department of Molecular, Cell, and Developmental Biology, Los Angeles, CA, USA.
⁴ Division of Pediatric Critical Care, UCLA Department of Pediatrics, UCLA Mattel Children's Hospital, Los Angeles, CA, USA.
⁵ UCLA Department of Medicine Statistics Core, Los Angeles, CA, USA.
⁶ USC Department of Clinical Pharmacy, USC Alfred E Mann School of Pharmacy and Pharmaceutical Sciences, Los Angeles, CA, USA.
⁷ Department of Quantitative and Computational Biology, USC Dornsife College of Letters, Arts and Sciences, Los Angeles, CA, USA.
⁸ Department of Anesthesiology and Critical Care Medicine, Children's Hospital of Philadelphia, and Perelman School of Medicine, University of Pennsylvania, Philadelphia, PA, USA.
⁹ Division of Immunology, Allergy, and Rheumatology, UCLA Department of Pediatrics, Los Angeles, CA, USA.
¹⁰ Department of Pediatrics, Division of Medical Critical Care, Boston Children's Hospital, Harvard Medical School, Boston, MA, USA.
¹¹ Division of Pediatric Critical Care, UCLA Department of Pediatrics, UCLA Mattel Children's Hospital, Los Angeles, CA, USA. anilsapru@g.ucla.edu.

Abstract

Background: Sepsis is a highly heterogeneous syndrome, which has hindered the development of effective therapies. This has prompted investigators to develop a precision medicine approach aimed at identifying biologically homogenous subgroups of patients with septic shock and critical illnesses. Transcriptomic analysis can identify subclasses derived from differences in underlying pathophysiological processes that may provide the basis for new targeted therapies. The goal of this study was to elucidate pathophysiological pathways and identify pediatric septic shock subclasses based on whole blood RNA expression profiles.

Methods: The subjects were critically ill children with cardiopulmonary failure who were a part of a prospective randomized insulin titration trial to treat hyperglycemia. Genome-wide expression profiling was conducted using RNA sequencing from whole blood samples obtained from 46 children with septic shock and 52 mechanically ventilated noninfected controls without shock. Patients with septic shock were allocated to subclasses based on hierarchical clustering of gene expression profiles, and we then compared clinical characteristics, plasma inflammatory markers, cell compositions using GEDIT, and immune repertoires using Imrep between the two subclasses.

Results: Patients with septic shock depicted alterations in innate and adaptive immune pathways. Among patients with septic shock, we identified two subtypes based on gene expression patterns. Compared with Subclass 2, Subclass 1 was characterized by upregulation of innate immunity pathways and downregulation of adaptive immunity pathways. Subclass 1 had significantly worse clinical outcomes despite the two classes having similar illness severity on initial clinical presentation. Subclass 1 had elevated levels of plasma inflammatory cytokines and endothelial injury biomarkers and demonstrated decreased percentages of CD4 T cells and B cells and less diverse T cell receptor repertoires.

Conclusions: Two subclasses of pediatric septic shock patients were discovered through genome-wide expression profiling based on whole blood RNA sequencing with major biological and clinical differences. Trial Registration This is a secondary analysis of data generated as part of the observational CAF-PINT ancillary of the HALF-PINT study (NCT01565941). Registered March 29, 2012.

Keywords: Adaptive immunity; Gene expression; RNA-Seq; Sepsis; Subclassification.

MeSH terms

Child
Gene Expression Profiling
Humans
Observational Studies as Topic
Prospective Studies
Randomized Controlled Trials as Topic
Sepsis* / genetics
Shock, Septic* / therapy
Transcriptome

Associated data

ClinicalTrials.gov/NCT01565941

Abstract

MeSH terms

Associated data

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