AI Article Synopsis

  • Circulatory shock is traditionally defined as low blood pressure with poor tissue blood supply, categorized into subtypes like distributive and hypovolemic based on different causes, such as infection or trauma.
  • Recent findings suggest that there is significant variability in how patients respond to treatments, which may complicate the understanding of previous clinical trial results.
  • The review emphasizes the importance of identifying specific biological markers in patients to tailor treatments better, promoting a more personalized approach in intensive care settings.

Article Abstract

Circulatory shock is defined syndromically as hypotension associated with tissue hypoperfusion and often subcategorized according to hemodynamic profile (e.g., distributive, cardiogenic, hypovolemic) and etiology (e.g., infection, myocardial infarction, trauma, among others). These shock subgroups are generally considered homogeneous entities in research and clinical practice. This current definition fails to consider the complex pathophysiology of shock and the influence of patient heterogeneity. Recent translational evidence highlights previously under-appreciated heterogeneity regarding the underlying pathways with distinct host-response patterns in circulatory shock syndromes. This heterogeneity may confound the interpretation of trial results as a given treatment may preferentially impact distinct subgroups. Re-analyzing results of major 'neutral' treatment trials from the perspective of biological mechanisms (i.e., host-response signatures) may reveal treatment effects in subgroups of patients that share treatable traits (i.e., specific biological signatures that portend a predictable response to a given treatment). In this review, we discuss the emerging literature suggesting the existence of distinct biomarker-based host-response patterns of circulatory shock syndrome independent of etiology or hemodynamic profile. We further review responses to newly prescribed treatments in the intensive care unit designed to personalize treatments (biomarker-driven or endotype-driven patient selection in support of future clinical trials).

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10435428PMC
http://dx.doi.org/10.1186/s40635-023-00531-5DOI Listing

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