Impaired peripheral mononuclear cell metabolism in patients at risk of developing sepsis: A cohort study

Velma Herwanto; Ya Wang; Maryam Shojaei; Alamgir Khan; Kevin Lai; Amith Shetty; Stephen Huang; Tracy Chew; Sally Teoh; Marek Nalos; Mandira Chakraborty; Anthony S McLean; Benjamin M P Tang

doi:10.2478/jccm-2026-0010

Abstract

Introduction

Dysregulated immune responses are central to progression of sepsis and closely associated with impaired cellular metabolism. However, most existing studies have focused on late-stage sepsis, leaving metabolic alterations during earlier stages of infection poorly characterised. This study aimed to determine whether immune cell metabolic impairment is already present during uncomplicated infection, prior to the development of sepsis, and to evaluate its potential as an early indicator of immune dysfunction and risk of progression.

Materials and methods

Forty patients with sepsis (fulfilling Sepsis-3 criteria) and 27 patients with uncomplicated infection were recruited from the emergency department along with 20 healthy volunteers. Whole blood samples were collected to assess gene expression, cytokine levels, and cellular metabolic functions, including mitochondrial respiration, oxidative stress, and apoptosis in immune cells.

Results

Mitochondrial respiration was significantly impaired in immune cells from both uncomplicated infection and sepsis patients compared with healthy controls (p < 0.05), with more pronounced impairment in established sepsis. Downregulation of BCL2 and BBC3 gene expression was observed in sepsis patients (p < 0.05), but not in uncomplicated infection, potentially contributing to differences in the severity of metabolic impairment. Impaired mitochondrial respiration was significantly associated with increased mitochondrial oxidative stress (p < 0.05), which was elevated in uncomplicated infection and further increased in sepsis. Oxidative stress levels also correlated with tumour necrosis factor-α (r = 0.330) and the expression of CYCS, TP53, SLC25A24, and TSPO (rs = −0.4926, −0.4422, 0.4382, and 0.4835, respectively). Despite these metabolic alterations, no significant differences in immune cell apoptosis were observed between uncomplicated infection and sepsis patients.

Conclusions

Immune cell metabolic dysfunction is present in patients with uncomplicated infection before the clinical onset of sepsis. Early mitochondrial dysfunction and oxidative stress may represent promising targets for further investigation as early biomarkers of immune dysfunction and sepsis risk.

References

Rhee C, Klompas M. Sepsis trends: increasing incidence and decreasing mortality, or changing denominator? J Thorac Dis. 2020;12:S89–100.
Search in Google Scholar Back to article
Jarczak D, Kluge S, Nierhaus A. Sepsis-Pathophysiology and therapeutic concepts. Front Med (Lausanne). 2021;8:628302.
Search in Google Scholar Back to article
Cao M, Wang G, Xie J. Immune dysregulation in sepsis: experiences, lessons and perspectives. Cell Death Discov. 2023;9:465.
Search in Google Scholar Back to article
Liu Z, Ting Y, Li M, Li Y, Tan Y, Long Y. From immune dysregulation to organ dysfunction: understanding the enigma of sepsis. Front Microbiol. 2024;15:1415274.
Search in Google Scholar Back to article
Nedel W, Deutschendorf C, Portela LVC. Sepsis-induced mitochondrial dysfunction: A narrative review. World J Crit Care Med. 2023;12(3):139–52.
Search in Google Scholar Back to article
Preau S, Vodovar D, Jung B, Lancel S, Zafrani L, Flatres A, et al. Energetic dysfunction in sepsis: a narrative review. Ann Intensive Care. 2021;11:1004.
Search in Google Scholar Back to article
Carré JE, Orban J-C, Re L, Felsmann K, Iffert W, Bauer M, et al. Survival in critical illness is associated with early activation of mitochondrial biogenesis. Am J Resp Crit Care Med. 2010;182(6):745–51.
Search in Google Scholar Back to article
Brealey D, Brand M, Hargreaves I, Heales S, Land J, Smolenski R, et al. Association between mitochondrial dysfunction and severity and outcome of septic shock. Lancet. 2002;360:219–23.
Search in Google Scholar Back to article
Hu D, Prabhakaran HS, Zhang Y-Y, Luo G, He W, Liou Y-C. Mitochondrial dysfunction in sepsis: mechanisms and therapeutic perspectives. Crit Care. 2024;28:292.
Search in Google Scholar Back to article
Wen M, Cai G, Ye J, Liu X, Ding H, Zeng H. Single-cell transcriptomics reveals the alteration of peripheral blood mononuclear cells driven by sepsis. Ann Transl Med. 2020;8(4):125.
Search in Google Scholar Back to article
Ferreira BL, Sousa MB, Leite GGF, Brunialti MKC, Nishiduka ES, Tashima AK, et al. Glucose metabolism is upregulated in the mononuclear cell proteome during sepsis and supports endotoxin-tolerant cell function. Front Immunol. 2022;13:1051514.
Search in Google Scholar Back to article
Bone RC, Balk RA, Cerra FB, Dellinger RP, Fein AM, Knaus WA, et al. Definitions for sepsis and organ failure and guidelines for the use of innovative therapies in sepsis. The ACCP/SCCM Consensus Conference Committee. American College of Chest Physicians/Society of Critical Care Medicine. Chest. 1992;101(6):1644–55.
Search in Google Scholar Back to article
Singer M, Deutschman CS, Seymour CW, Shankar-Hari M, Annane D, Bauer M, et al. The Third International Consensus Definitions for Sepsis and Septic Shock (Sepsis-3). JAMA. 2016;315(8):801–10.
Search in Google Scholar Back to article
Agilent Technologies Inc. Agilent Seahorse XF cell mito stress test kit, 3rd ed, manual part number 103016-400. 2024.
Search in Google Scholar Back to article
Dranka BP, Benavides GA, Diers AR, Giordano S, Zelickson BR, Reily C, et al. Assessing bioenergetic function in response to oxidative stress by metabolic profiling. Free Radic Biol Med. 2011;51(9):1621–35.
Search in Google Scholar Back to article
Gharamti AA, Samara O, Monzon A, Montalbano G, Scherger S, DeSanto K, et al. Proinflammatory cytokines levels in sepsis and healthy volunteers, and tumor necrosis factor-alpha associated sepsis mortality: A systematic review and meta-analysis. Cytokine. 2022;158:156006.
Search in Google Scholar Back to article
da Silva FP, Machado MCC. Septic shock and the aging process: a molecular comparison. Front Immunol. 2017;8:1389.
Search in Google Scholar Back to article
Chen Y, Zhou Z, Min W. Mitochondria, oxidative stress and innate immunity. Front Physiol. 2018;9:1487.
Search in Google Scholar Back to article
Mihaljevic O, Zivancevic-Simonovic S, Jovanovic D, Drakulic SM, Vukajlovic JT, Markovic A, et al. Oxidative stress and DNA damage in critically ill patients with sepsis. Mutat Res Genet Toxicol Environ Mutagen. 2023;889:503655.
Search in Google Scholar Back to article
Pinchuk I, Weber D, Kochlik B, Stuetz W, OlivierToussaint, Debacq-Chainiaux F, et al. Gender- and age-dependencies of oxidative stress, as detected based on the steady state concentrations of different biomarkers in the MARK-AGE study. Redox Biology. 2019;24:101204.
Search in Google Scholar Back to article
Ferrer R, Iba T. Mitochondrial damage in sepsis. Juntendo Iji Zasshi. 2024;70(4):269–72.
Search in Google Scholar Back to article
Qian S, Wei Z, Yang W, Huang J, Yang Y, Wang J. The role of BCL-2 family proteins in regulating apoptosis and cancer therapy. Front Oncol. 2022;12:985363.
Search in Google Scholar Back to article
Martinou J-C, Youle RJ. Mitochondria in apoptosis: Bcl-2 family members and mitochondrial dynamics. Developmental Cell. 2011;21(1).
Search in Google Scholar Back to article
Weber GF, Chousterman BG, He S, Fenn AM, Nairz M, Anzai A, et al. Interleukin-3 amplifies acute inflammation and is a potential therapeutic target in sepsis. Science. 2015;347(6227):1260–5.
Search in Google Scholar Back to article
Guo Y, Luan L, Wang J, Patil N, Bohannon J, Rabacal W, et al. Interleukin-15 enables septic shock by maintaining natural killer cell integrity and function. J Immunol. 2017;198(3):1320–33.
Search in Google Scholar Back to article
Sygitowicz G, Sitkiewicz D. Molecular mechanisms of organ damage in sepsis: an overview. Braz J Infect Dis. 2020;24(6):552–60.
Search in Google Scholar Back to article
Tong R, Ding X, Liu F, Li H, Liu H, Song H, et al. Classification of subtypes and identification of dysregulated genes in sepsis. Front Cell Infect Microbiol. 2023;13:1226159.
Search in Google Scholar Back to article
Ivanov AV, Bartosch B, Isaguliants MG. Oxidative stress in infection and consequent disease. Oxid Med Cell Longev. 2017;2017:3496043.
Search in Google Scholar Back to article
Kong C, Song W, Fu T. Systemic inflammatory response syndrome is triggered by mitochondrial damage. Molecular Medicine Reports. 2022;25:147.
Search in Google Scholar Back to article
Cheng S-C, Scicluna BP, Arts RJW, Gresnigt MS, Lachmandas E, Giamarellos-Bourboulis EJ, et al. Broad defects in the energy metabolism of leukocytes underlie immunoparalysis in sepsis. Nature Immunol. 2016;17(4):406–13.
Search in Google Scholar Back to article
Liu W, Liu T, Zheng Y, Xia Z. Metabolic reprogramming and its regulatory mechanism in sepsis-mediated inflammation. J Inflamm Res. 2023;16:1195–207.
Search in Google Scholar Back to article
Angajala A, Lim S, Phillips JB, Kim J-H, Yates C, You Z, et al. Diverse roles of mitochondria in immune responses: novel insights into immuno-metabolism. Front Immunol. 2018;9:1605.
Search in Google Scholar Back to article
Lvovschi V, Arnaud L, Parizot C, Freund Y, Juillien G, Ghillani-Dalbin P, et al. Cytokine profiles in sepsis have limited relevance for stratifying patients in the emergency department: A prospective observational study. PLoS One. 2011;6(12):e28870.
Search in Google Scholar Back to article
Katerji M, Filippova M, Duerksen-Hughes P. Approaches and methods to measure oxidative stress in clinical samples: research applications in the cancer field. Oxid Med Cell Longev. 2019;2019:1279250.
Search in Google Scholar Back to article
Dikalov SI, Harrison DG. Methods for detection of mitochondrial and cellular reactive oxygen species. Antioxid Redox Signal. 2014;20(2):372–82.
Search in Google Scholar Back to article
Duplessis C, Gregory M, Frey K, Bell M, Truong L, Schully K, et al. Evaluating the discriminating capacity of cell death (apoptotic) biomarkers in sepsis. J Intensive Care. 2018;6:72.
Search in Google Scholar Back to article