Frankie Carr, Biological Sciences, Summer 2021
Figure: A neutrophil (yellow) ejecting a NET (green) to capture invading bacteria (purple) that are attacking a red blood cell (orange).
Image Source: Wikimedia Commons
Neutrophils are a type of white blood cell involved in the innate immune response in most animal immune systems. These cells are among the most numerous in the circulatory systems of many organisms; in fact, they are the single most abundant white blood cell in humans and make up to about 50% of the total blood cells in chimpanzees (Amulic et al., 2012; Stacey et al., 2021). Not only are they incredibly prevalent in the blood, neutrophils are generally among the “first-responders” to an immune reaction. Drawn to sites of inflammation via the activation of the endothelial cells of the blood vessels, neutrophils undergo a process called “extravasation” and enter the damaged tissue. Once there, the neutrophils will respond to the situation based on what signals are being presented to it by tissue cells as well as the source of inflammation, which can range from bodily damage to foreign pathogens. These responses include phagocytosing (engulfing and digesting) threats and damaged cells. Another such response is that of releasing granules (self-contained organelles that contain various immunological effector molecules that either directly fight pathogens and/or recruit other immune cells to the scene) and/or reactive oxygen species (which are inflammatory and damaging to microbe and host alike). Additionally, they can bind to microbes with effector surface proteins (often directly or indirectly destroying pathogens). Finally, they can undergo apoptosis (deliberate death of the cell) to release Neutrophil Extracellular Traps (NETs) (Amulic et al., 2012).
This last function, the intentional self-destruction of a cell to release a web-like trap is a process known as NETosis. NETs consist of DNA-binding proteins called histones, nuclear and mitochondrial DNA, and proteins with antimicrobial effects (see Figure 1 above). The DNA components provide the scaffolding and rope-like constitution of the NET. They were only recently discovered in 2004. First thought to mainly target bacteria and their virulence factors, which are effector molecules that are responsible for infection and/or damage to the host (Brinkmann et al., 2004), it is now known that NETs effectively target and neutralize bacteria, fungi, viruses, and possibly even multicellular parasites, (Papayannopoulos, 2018). It has been shown that the protein composition of the NET varies by the stimulus that induced the cell to destroy itself but all NETSs contain high amounts of antimicrobial proteins (Amulic et al., 2012; Papayannopoulos, 2018), especially the protease Neutrophil Elastase (Amulic et al., 2012; Brinkmann et al., 2004; Papayannopoulos, 2018).
It was recently seen that upon binding to antigen-bound IgA class antibodies (proteins produced by B and plasma cells that are specific for a given antigen and predominantly found at mucous membranes), neutrophils undergo NETosis, releasing a slew of antiviral compounds that have been shown to trap and kill viruses. Thus, at the various mucous membranes (like those that line the mouth, nose, and urethra), if the immune system has fought off a given virus and thus possesses B cells capable of producing antibodies against it, it will likely prevent reinfection by that virus via the NETs produced by this interaction. This may play a role in immunity conferred onto individuals by vaccines against different viruses, including polio and SARS-CoV-2, for example (Stacey et al., 2021).
NETs, like many immune functions, can have negative consequences for the host. Because NETs expose the immune system to the intracellular materials of cells of the body, they run the risk of allowing for the development of an autoimmune response to various self-antigens. This autoimmunity may result in systemic lupus erythematosus (SLE), a disease marked by widespread inflammation and tissue damage along with red rashes on the skin, amd other diseases (Amulic et al., 2012; Papayannopoulos, 2018). Furthermore, in releasing inflammatory molecules, NETs may result in further damage or a delay in repair to damage in various tissues (Papayannopoulos, 2018). In fact, this very possibility has been known to occur in severe cases of COVID-19, with there being significantly higher levels of NET components and neutrophils in the blood of patients who are required to be put on ventilators due to the infection and immune cell-mediated damage to the lungs (Zuo et al., 2020). Additionally, these molecules may result in the blocking of various blood vessels by causing inflammation and trapping various cells and molecules, including the blood clot forming platelets. The total effect is a large, sticky clot formed by NET and platelet-plug alike, resulting in various problems including the painful and dangerous Deep Vein Thrombosis (DVT), wherein a blot clot forms in a vein that is deep beneath the surface of the skin (Amulic et al., 2012; Papayannopoulos, 2018). In attempting to fight off some sort of infection, neutrophils and their NETs may end up doing more harm to the host than good.
While much has been discovered about NETs recently, we still have much to learn about this undoubtedly vital function of neutrophils. For example, it has been shown that they can release NETs without total destruction of themselves (although with the intentional release of some nuclear, but no mitochondrial, DNA) in response to Staphylococcus aureus bacteria (Pilsczek et al., 2010). This mechanism, whether it is unique to a response against S. aureus, and why it is not more widely used is certainly worth further research. Future studies will hopefully be able to reveal to us how to help optimize and regulate the NET response, providing maximal protection and minimal damage to our bodies when our neutrophils employ these molecular traps.
References
Amulic, B., Cazalet, C., Hayes, G. L., Metzler, K. D., & Zychlinsky, A. (2012). Neutrophil Function: From Mechanisms to Disease. Annual Review of Immunology, 30(1), 459–489. https://doi.org/10.1146/annurev-immunol-020711-074942
Brinkmann, V., Reichard, U., Goosmann, C., Fauler, B., Uhlemann, Y., Weiss, D. S., Weinrauch, Y., & Zychlinsky, A. (2004). Neutrophil Extracellular Traps Kill Bacteria. Science, 303(5663), 1532–1535. https://doi.org/10.1126/science.1092385
Papayannopoulos, V. (2018). Neutrophil extracellular traps in immunity and disease. Nature Reviews Immunology, 18(2), 134–147. https://doi.org/10.1038/nri.2017.105
Pilsczek, F. H., Salina, D., Poon, K. K. H., Fahey, C., Yipp, B. G., Sibley, C. D., Robbins, S. M., Green, F. H. Y., Surette, M. G., Sugai, M., Bowden, M. G., Hussain, M., Zhang, K., & Kubes, P. (2010). A novel mechanism of rapid nuclear neutrophil extracellular trap formation in response to Staphylococcus aureus. Journal of Immunology (Baltimore, Md.: 1950), 185(12), 7413–7425. https://doi.org/10.4049/jimmunol.1000675
Researchers discover unique “spider web” mechanism that traps, kills viruses. (2021, June 29). ScienceDaily. https://www.sciencedaily.com/releases/2021/06/210629101244.html
Stacey, H. D., Golubeva, D., Posca, A., Ang, J. C., Novakowski, K. E., Zahoor, M. A., Kaushic, C., Cairns, E., Bowdish, D. M. E., Mullarkey, C. E., & Miller, M. S. (2021). IgA potentiates NETosis in response to viral infection. Proceedings of the National Academy of Sciences, 118(27). https://doi.org/10.1073/pnas.2101497118
Zuo, Y., Yalavarthi, S., Shi, H., Gockman, K., Zuo, M., Madison, J. A., Blair, C., Weber, A., Barnes, B. J., Egeblad, M., Woods, R. J., Kanthi, Y., & Knight, J. S. (2020). Neutrophil extracellular traps in COVID-19. JCI Insight, 5(11). https://doi.org/10.1172/jci.insight.138999