Neutrophils are actively involved in the protection of our body against pathogen infection, but the consequences of their activation contribute significantly to pathogenesis of various diseases. This is why neutrophil-mediated responses should be finely tuned, and therapeutic interventions should balance between targeting neutrophil functions and uncontrolled neutrophil activation. Several decades ago, Elmer Becker wrote a great article: “The short and happy life of neutrophil activation,” where he described the importance of neutrophil functions to human physiology (Becker 1990). The novel coronavirus pandemic COVID-19 again demonstrated a critical role of neutrophils. An increased neutrophil-to-lymphocyte ratio (Liu et al., 2020) and the release of neutrophil extracellular traps (NETs) (Zuo et al., 2020) predicted severe illness at SARS-CoV-2 infection. Excessive NETs formation can be involved in the development of the «cytokine storm» and immunothrombosis, which are the main cause of severe complications associated with COVID-19. Therefore, neutrophil can be a pathogenic marker and drug target of COVID-19 (for review see Chiang et al. (2020)). A detailed study of these cells is extremely important for medicine and pharmacology, and the aim of this topic is to gather new trends in pharmacological approaches targeting neutrophilic inflammation.