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Personalized, disease-stage specific, rapid identification of immunosuppression in sepsis. | LitMetric

AI Article Synopsis

  • - The study addresses the challenge of overlapping biological data in sepsis that complicates personalized medical decision-making, particularly when key indicators like neutrophil percentages don't clearly differentiate between survivors and non-survivors of sepsis.
  • - Two methodologies were applied to analyze data from over 4,000 blood samples: a reductionist approach focusing on individual variables, and a non-reductionist approach that examined the interactions among various dimensions related to leukocytes and patient outcomes.
  • - The non-reductionist method proved more effective, identifying distinct patient subsets that correlated with survival rates, and outlining five stages of immune response which predict outcomes, thereby aiding personalized treatment strategies.

Article Abstract

Introduction: Data overlapping of different biological conditions prevents personalized medical decision-making. For example, when the neutrophil percentages of surviving septic patients overlap with those of non-survivors, no individualized assessment is possible. To ameliorate this problem, an immunological method was explored in the context of sepsis.

Methods: Blood leukocyte counts and relative percentages as well as the serum concentration of several proteins were investigated with 4072 longitudinal samples collected from 331 hospitalized patients classified as septic (n=286), non-septic (n=43), or not assigned (n=2). Two methodological approaches were evaluated: (i) a reductionist alternative, which analyzed variables in isolation; and (ii) a non-reductionist version, which examined interactions among six (leukocyte-, bacterial-, temporal-, personalized-, population-, and outcome-related) dimensions.

Results: The reductionist approach did not distinguish outcomes: the leukocyte and serum protein data of survivors and non-survivors overlapped. In contrast, the non-reductionist alternative differentiated several data groups, of which at least one was only composed of survivors (a finding observable since hospitalization day 1). Hence, the non-reductionist approach promoted personalized medical practices: every patient classified within a subset associated with 100% survival subset was likely to survive. The non-reductionist method also revealed five inflammatory or disease-related stages (provisionally named 'early inflammation, early immunocompetence, intermediary immuno-suppression, late immuno-suppression, or other'). Mortality data validated these labels: both 'suppression' subsets revealed 100% mortality, the 'immunocompetence' group exhibited 100% survival, while the remaining sets reported two-digit mortality percentages. While the 'intermediary' suppression expressed an impaired monocyte-related function, the 'late' suppression displayed renal-related dysfunctions, as indicated by high concentrations of urea and creatinine.

Discussion: The data-driven differentiation of five data groups may foster early and non-overlapping biomedical decision-making, both upon admission and throughout their hospitalization. This approach could evaluate therapies, at personalized level, earlier. To ascertain repeatability and investigate the dynamics of the 'other' group, additional studies are recommended.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11558526PMC
http://dx.doi.org/10.3389/fimmu.2024.1430972DOI Listing

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