(A) Schematic representation of rhinovirus Common Cold (CC) model. ACE2, angiotensin-converting enzyme 2; ICAM-1, intercellular adhesion molecule 1; sACE2 and sIL-4Rα, soluble variants of transmembrane proteins. (B) Schematic representation of COVID-19 cytokine model. (C) Albuminuria following CC cocktail dose X or control saline in BALB/cJ and BALB/c mice (n = 5 mice/group). (D) Dose-response effect of CC cocktail on albuminuria in BALB/cJ mice (n = 4 – 6 mice/group). (E) Albuminuria following injection of individual CC cocktail components dose X in BALB/cJ mice (n = 4–5 mice/group). (F) Albuminuria after injecting CC cocktail dose X/2, or X/2 minus individual components, in BALB/cJ mice (n = 4 to 11 mice/group). BALB/c mice do not develop albuminuria at dose X/2. (G) CC cocktail dose X/15 induced albuminuria in podocyte-specific Zhx2-deficient Zhx2^fl/fl NPHS2 promoter–Cre^+/+ and control Zhx2^fl/fl mice (n = 3 mice/group). (H) COVID-19 cocktail dose X/2 induced albuminuria in BALB/c mice (n = 6 mice/group). (I) COVID-19 cocktail dose X/2 induced albuminuria in BALB/cJ mice (n = 5–6 mice/group). (J) Dose-response effect of Cocktail D on albuminuria in BALB/cJ mice (n = 4 mice/group). (K) Albuminuria in BALB/c and BALB/cJ mice after injecting individual components (dose X) of COVID-19 cocktails (n = 6 mice/group). (L) Albuminuria after injecting Cocktail C dose X/2 or Cocktail C dose X/2 minus individual components that target podocytes in BALB/c mice (n = 5–6 mice/group). (M) Cocktail C dose X/5 induced albuminuria in Zhx2^fl/fl NPHS2 promoter–Cre^+/+ and control Zhx2^fl/fl mice (n = 7–8 mice/group; age 18 weeks). * P < 0.05; ** P < 0.01; *** P < 0.001; **** P < 0.0001, 1-way Anova (Dunnett, C, K, M; FDR, method of Benjamini, Krieger, and Yekutieli [FDR-BKY], F, L), multiple t test comparisons (Holm-Šídák, D, E, F, H, I, J; FDR-BKY, L), and simple t test, 1 tailed (green asterisk, G). Data represent mean ± SEM.