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  • Bind to the cell membrane of the pathogen labeling it for phagocytosis
  • Move away from the pathogen and send chemical messages to other immune cells
  • Form damaging pores (holes) in the plasma membrane of the pathogen

Protein from the complement system form the membrane-attack complex (MAC). The MAC can kill certain pathogens by disrupting their osmotic (water) balance. The MAC is especially effective against a broad range of bacteria. Phagocytic cells such as macrophages and neutrophils are attracted to an infection site by a chemical produced by complement.

Inflammatory response

The most well known example of the innate immune response is inflammation    . Inflammation is something everyone has experienced. Stub a toe, cut a finger, or do any activity that causes tissue damage and inflammation will result, with its four characteristics: heat, redness, pain, and swelling (“loss of function” is sometimes mentioned as a fifth characteristic). It is important to note that inflammation does not have to be initiated by an infection, but can also be caused by tissue injuries. The release of damaged cellular contents into the site of injury is enough to stimulate the response, even in the absence of breaks in in the skin that would allow pathogens to enter (by hitting your thumb with a hammer, for example). The inflammatory reaction brings in phagocytic cells to the damaged area to clear cellular debris and to set the stage for wound repair ( [link] ).

The top panel of this figure shows the mast cells detecting an injury and initiating an inflammatory response. The bottom panel shows the increase in blood flow in response to histamine.

This reaction also brings in the cells of the innate immune system, allowing them to get rid of the sources of a possible infection. Inflammation is part of a very basic form of immune response. The process not only brings fluid and cells into the site to destroy the pathogen and remove it and debris from the site, but also helps to isolate the site, limiting the spread of the pathogen. Acute inflammation is a short-term inflammatory response to an insult to the body. If the cause of the inflammation is not resolved, however, it can lead to chronic inflammation, which is associated with major tissue destruction and scarring. Chronic inflammation is ongoing inflammation. It can be caused by foreign bodies, persistent pathogens, and autoimmune diseases such as rheumatoid arthritis.

There are four important parts to the inflammatory response:

  • Tissue Injury. The released contents of injured cells stimulate the release of mast cells which in turn produce chemicals such as histamine, leukotrienes, and prostaglandins. Histamine increases the diameter of local blood vessels, causing an increase in blood flow. Histamine also increases the amount of fluid that leaves the blood and flows into the damaged tissue and causes the swelling associated with inflammation.
    Additionally injured cells attract phagocytes, and basophils which are sources of prostaglandins and leukotrienes. Leukotrienes attract neutrophils and increase blood vessel dialation (widening). Prostaglandins also cause vessel dilation by relaxing vascular smooth muscle and are a major cause of the pain associated with inflammation. Nonsteroidal anti-inflammatory drugs such as aspirin and ibuprofen relieve pain by inhibiting prostaglandin production.
  • Vasodilation. Many inflammatory mediators such as histamine are vasodilators that increase the diameters of local capillaries. This causes increased blood flow and is responsible for the heat and redness of inflamed tissue. It allows greater access of the blood to the site of inflammation.
  • Increased Vascular Permeability. At the same time, inflammatory mediators increase the permeability of the local blood vessels, causing leakage of fluid into the space between the cells, resulting in the swelling, or edema , associated with inflammation.
  • Recruitment of Phagocytes. Leukotrienes are particularly good at attracting neutrophils from the blood to the site of infection by chemical messemger. Cytokines attract more macrophages which are recruited to clean up the debris left over at the site. When local infections are severe, neutrophils are attracted to the sites of infections in large numbers, and as they take in the pathogens and die, their accumulated cellular remains are visible as pus at the infection site.

Overall, inflammation is valuable for many reasons. Not only are the pathogens killed and debris removed, but the increase in vascular permeability encourages the entry of clotting factors, the first step towards wound repair. Inflammation also facilitates the transport of antigen to lymph nodes by dendritic cells for the development of the adaptive immune response.

Chapter review

Innate immune responses are critical to the early control of infections. Whereas barrier defenses are the body’s first line of physical defense against pathogens, innate immune responses are the first line of physiological defense. Innate responses occur rapidly, but with less specificity and effectiveness than the adaptive immune response. Innate responses can be caused by a variety of cells, mediators, and antibacterial proteins such as complement. Within the first few days of an infection, another series of antibacterial proteins are induced, each with activities against certain bacteria, including opsonization of certain species. Additionally, interferons are induced that protect cells from viruses in their vicinity. Finally, the innate immune response does not stop when the adaptive immune response is developed. In fact, both can cooperate and one can influence the other in their responses against pathogens.

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Source:  OpenStax, Mrs. browne's immune modules. OpenStax CNX. Apr 27, 2015 Download for free at https://legacy.cnx.org/content/col11783/1.1
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