One of the most prominent candidate molecules that can provide strong antiviral defense is IFN. Hence, we tested IFN response in A549 cells upon treatment with ME/CFS or HC serum. We observed a strong decrease in mRNA levels of IFN-β, IFIT-1, and ICAM-1 within the A549 cells in presence of ME/CFS serum in comparison with HC serum (Fig. 5D–F). Then we asked whether the secretory IFN response in isolated PBMCs is higher in ME/CFS patients. For this we used a different cohort of 22 CFS patients and 22 HC. Upon challenge with LPS, we found lower levels of secreted TNF-α (p < 0.01) and IFN-γ (p < 0.05) from CFS patient PBMCs compared with HC (Supplemental Fig. 2B). No significant differences were seen for IL-1 and IL-5. These results ruled out a potential role of IFN response in the mitochondrial fragmentation and antiviral response in ME/CFS patients.
