Experimental Collapse in Virophysics: Protocol-Resolved Observation, Inference, and Plaque-Assay Blindness

arXiv:2605.27928v1 Announce Type: cross
Abstract: Virological measurements are often treated as reports of virion structure, mechanics, dielectric response, infectivity, or titer. In practice, an experiment observes a protocol-conditioned projection of a richer latent virion–environment ensemble. This paper defines this process as emphexperimental collapse within protocol-resolved virophysics. Its central object is the null-inclusive observation operator (P_mathrmobs,t^varnothing(cdotmid E)=mathcal M_E,t^varnothingP_mathrmref,t), mapping a reference latent ensemble to the observed ensemble generated by protocol (E), including null outcomes. The formulation separates latent-state transformation, detection weighting, readout, and non-observation, making protocol effects explicit components rather than bias terms.
The framework introduces protocol-conditioned latent ensembles, collapse functionals, protocol blindness, observation equivalence, Fisher-information observability, inverse inference, and multi-protocol consistency. It identifies collapse mechanisms including preparation, surface immobilization, mechanical loading, field steering, medium filtering, amplification, censoring, and detection thresholds. As a worked example, the plaque assay estimates an effective protocol-conditioned infectious concentration (Lambda_mathrmPFU=int_Psipi_mathrmPFU(x;E_mathrmPFU)n_mathrmref(x),dx), rather than total particle concentration. This recovers the Poisson plaque-count model and PFU titer formula in the dilute regime; extensions to overdispersion, zero inflation, plaque merging, endpoint dilution, neutralization, and morphology-augmented readouts recast deviations as protocol-conditioned information. Thus, virological data are outputs of explicit protocol kernels, clarifying what measurements report, miss, and how complementary assays can infer hidden latent virion structures.