Biosystems. 2026 Jun 26. pii: S0303-2647(26)00171-1. [Epub ahead of print]266
105861
Biological immune regulation depends not only on detecting molecular signals, but on assigning those signals functional status. The same antigenic, inflammatory, or damage-associated input may support tolerance, activation, repair, resolution, suppression, or memory depending on tissue context, prior history, co-stimulation, regulatory state, and inflammatory load. This paper proposes immune signal-status misclassification as a conservative systems-level framework for cases in which immune systems assign inappropriate biological status to signals: harmless inputs treated as danger, self-related signals treated as threat, resolved damage treated as ongoing injury, or transient activation treated as persistent inflammatory demand. The proposal builds on established immunological concepts rather than replacing them. Pattern-recognition receptors, PAMP/DAMP signaling, danger and injury models, immune tolerance, and trained immunity already imply that immune response depends on context and history rather than signal presence alone. The contribution here is to make explicit a status-assignment layer: the operation by which a biological system assigns a signal the status of harmless, dangerous, self, damaged, repair-relevant, tolerogenic, inflammatory, or persistently threatening. A minimal toy model shows how prior danger-status assignment can maintain later danger assignment after an initiating signal declines. An illustrative public-data reanalysis of GEO accession GSE67472 shows how a documented three-gene type-2 inflammatory signature can be used to operationalize immune-status structure in airway epithelial transcriptomic data. Because the asthma subgroups in our reanalysis were reconstructed from the same signature used to define the score, this analysis is not treated as independent validation. The toy model and public-data example are used only to show how the framework can be formalized and operationalized. The central claim is narrow: some immune failures may involve wrong biological status assignment or failed status resolution, in addition to abnormal signal intensity or molecular pathway activation. Five falsifiable predictions are derived, including the context-history prediction that signal-plus-history models should outperform signal-only models near ambiguous threshold conditions, and the resolution prediction that recovery should be predicted by status-transition markers beyond raw inflammatory burden.
Keywords: Asthma endotypes; Chronic inflammation; DAMPs; Danger signaling; Immune tolerance; Signal classification; Status assignment; Systems immunology; Trained immunity