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Necrosis

February 28, 2023

For other uses, see Necrosis (disambiguation).
Not to be confused with Narcosis.

Necrosis (from Ancient Greek νέκρωσις (nékrōsis) 'death') is a form of cell injury which results in the premature death of cells in living tissue by autolysis.[1] Necrosis is caused by factors external to the cell or tissue, such as infection, or trauma which result in the unregulated digestion of cell components. In contrast, apoptosis is a naturally occurring programmed and targeted cause of cellular death. While apoptosis often provides beneficial effects to the organism, necrosis is almost always detrimental and can be fatal.[2]

Structural changes of cells undergoing necrosis and apoptosis

Cellular death due to necrosis does not follow the apoptotic signal transduction pathway, but rather various receptors are activated and result in the loss of cell membrane integrity[3] and an uncontrolled release of products of cell death into the extracellular space.[1] This initiates in the surrounding tissue an inflammatory response, which attracts leukocytes and nearby phagocytes which eliminate the dead cells by phagocytosis. However, microbial damaging substances released by leukocytes would create collateral damage to surrounding tissues.[4] This excess collateral damage inhibits the healing process. Thus, untreated necrosis results in a build-up of decomposing dead tissue and cell debris at or near the site of the cell death. A classic example is gangrene. For this reason, it is often necessary to remove necrotic tissue surgically, a procedure known as debridement.[citation needed]

Classification

Structural signs that indicate irreversible cell injury and the progression of necrosis include dense clumping and progressive disruption of genetic material, and disruption to membranes of cells and organelles.[5]

Morphological patterns

There are six distinctive morphological patterns of necrosis:[6]

  1. Coagulative necrosis is characterized by the formation of a gelatinous (gel-like) substance in dead tissues in which the architecture of the tissue is maintained,[6] and can be observed by light microscopy. Coagulation occurs as a result of protein denaturation, causing albumin to transform into a firm and opaque state.[5] This pattern of necrosis is typically seen in hypoxic (low-oxygen) environments, such as infarction. Coagulative necrosis occurs primarily in tissues such as the kidney, heart and adrenal glands.[5] Severe ischemia most commonly causes necrosis of this form.[7]
  2. Liquefactive necrosis (or colliquative necrosis), in contrast to coagulative necrosis, is characterized by the digestion of dead cells to form a viscous liquid mass.[6] This is typical of bacterial, or sometimes fungal, infections because of their ability to stimulate an inflammatory response. The necrotic liquid mass is frequently creamy yellow due to the presence of dead leukocytes and is commonly known as pus.[6] Hypoxic infarcts in the brain presents as this type of necrosis, because the brain contains little connective tissue but high amounts of digestive enzymes and lipids, and cells therefore can be readily digested by their own enzymes.[5]
  3. Gangrenous necrosis can be considered a type of coagulative necrosis that resembles mummified tissue. It is characteristic of ischemia of lower limb and the gastrointestinal tracts. If superimposed infection of dead tissues occurs, then liquefactive necrosis ensues (wet gangrene).[8]
  4. Caseous necrosis can be considered a combination of coagulative and liquefactive necrosis,[5] typically caused by mycobacteria (e.g. tuberculosis), fungi and some foreign substances. The necrotic tissue appears as white and friable, like clumped cheese. Dead cells disintegrate but are not completely digested, leaving granular particles.[5] Microscopic examination shows amorphous granular debris enclosed within a distinctive inflammatory border.[6] Some granulomas contain this pattern of necrosis.[9]
  5. Fat necrosis is specialized necrosis of fat tissue,[9] resulting from the action of activated lipases on fatty tissues such as the pancreas. In the pancreas it leads to acute pancreatitis, a condition where the pancreatic enzymes leak out into the peritoneal cavity, and liquefy the membrane by splitting the triglyceride esters into fatty acids through fat saponification.[6] Calcium, magnesium or sodium may bind to these lesions to produce a chalky-white substance.[5] The calcium deposits are microscopically distinctive and may be large enough to be visible on radiographic examinations.[7] To the naked eye, calcium deposits appear as gritty white flecks.[7]
  6. Fibrinoid necrosis is a special form of necrosis usually caused by immune-mediated vascular damage. It is marked by complexes of antigen and antibodies, referred to as immune complexes deposited within arterial walls[6] together with fibrin.[6]

Other clinical classifications of necrosis

  1. There are also very specific forms of necrosis such as gangrene (term used in clinical practices for limbs which have had severe hypoxia), gummatous necrosis (due to spirochaetal infections) and hemorrhagic necrosis (due to the blockage of venous drainage of an organ or tissue).
  2. Some spider bites may lead to necrosis. In the United States, only spider bites from the brown recluse spider (genus Loxosceles) reliably progress to necrosis. In other countries, spiders of the same genus, such as the Chilean recluse in South America, are also known to cause necrosis. Claims that yellow sac spiders and hobo spiders possess necrotic venom have not been substantiated.
  3. In blind mole rats (genus Spalax), the process of necrosis replaces the role of the systematic apoptosis normally used in many organisms. Low oxygen conditions, such as those common in blind mole rats' burrows, usually cause cells to undergo apoptosis. In adaptation to higher tendency of cell death, blind mole rats evolved a mutation in the tumor suppressor protein p53 (which is also used in humans) to prevent cells from undergoing apoptosis. Human cancer patients have similar mutations, and blind mole rats were thought to be more susceptible to cancer because their cells cannot undergo apoptosis. However, after a specific amount of time (within 3 days according to a study conducted at the University of Rochester), the cells in blind mole rats release interferon-beta (which the immune system normally uses to counter viruses) in response to over-proliferation of cells caused by the suppression of apoptosis. In this case, the interferon-beta triggers cells to undergo necrosis, and this mechanism also kills cancer cells in blind mole rats. Because of tumor suppression mechanisms such as this, blind mole rats and other spalacids are resistant to cancer.[10][11]

Causes

 
Necrotic leg wound caused by a brown recluse spider bite

Necrosis may occur due to external or internal factors.

External factors

External factors may involve mechanical trauma (physical damage to the body which causes cellular breakdown), damage to blood vessels (which may disrupt blood supply to associated tissue), and ischemia.[12] Thermal effects (extremely high or low temperature) can result in necrosis due to the disruption of cells.[citation needed]

In frostbite, crystals form, increasing the pressure of remaining tissue and fluid causing the cells to burst.[citation needed] Under extreme conditions tissues and cells die through an unregulated process of destruction of membranes and cytosol.[13]

Internal factors

Internal factors causing necrosis include: trophoneurotic disorders (diseases that occur due to defective nerve action in a part of an organ which results in failure of nutrition); injury and paralysis of nerve cells. Pancreatic enzymes (lipases) are the major cause of fat necrosis.[12]

Necrosis can be activated by components of the immune system, such as the complement system; bacterial toxins; activated natural killer cells; and peritoneal macrophages.[1] Pathogen-induced necrosis programs in cells with immunological barriers (intestinal mucosa) may alleviate invasion of pathogens through surfaces affected by inflammation.[1] Toxins and pathogens may cause necrosis; toxins such as snake venoms may inhibit enzymes and cause cell death.[12] Necrotic wounds have also resulted from the stings of Vespa mandarinia.[14]

Pathological conditions are characterized by inadequate secretion of cytokines. Nitric oxide (NO) and reactive oxygen species (ROS) are also accompanied by intense necrotic death of cells.[12] A classic example of a necrotic condition is ischemia which leads to a drastic depletion of oxygen, glucose, and other trophic factors and induces massive necrotic death of endothelial cells and non-proliferating cells of surrounding tissues (neurons, cardiomyocytes, renal cells, etc.).[1] Recent cytological data indicates that necrotic death occurs not only during pathological events but it is also a component of some physiological process.[12]

Activation-induced death of primary T lymphocytes and other important constituents of the immune response are caspase-independent and necrotic by morphology; hence, current researchers have demonstrated that necrotic cell death can occur not only during pathological processes, but also during normal processes such as tissue renewal, embryogenesis, and immune response.[12]

Pathogenesis

Pathways

Until recently, necrosis was thought to be an unregulated process.[15] However, there are two broad pathways in which necrosis may occur in an organism.[15]

The first of these two pathways initially involves oncosis, where swelling of the cells occurs.[15] Affected cells then proceed to blebbing, and this is followed by pyknosis, in which nuclear shrinkage transpires.[15] In the final step of this pathway cell nuclei are dissolved into the cytoplasm, which is referred to as karyolysis.[15]

The second pathway is a secondary form of necrosis that is shown to occur after apoptosis and budding.[15] In these cellular changes of necrosis, the nucleus breaks into fragments (known as karyorrhexis).[15]

Histopathological changes

Further information: Myocardial infarction diagnosis

The nucleus changes in necrosis and characteristics of this change are determined by the manner in which its DNA breaks down:

Other typical cellular changes in necrosis include:

On a larger histologic scale, pseudopalisades (false palisades) are hypercellular zones that typically surround necrotic tissue. Pseudopalisading necrosis indicates an aggressive tumor.[17]

  •  

    Pyknosis in a bile infarct

  •  

    Cytoplasmic hypereosinophilia (seen in left half of image)

  •  

    Pseudopalisading seen around necrosis in glioblastoma

Treatment

There are many causes of necrosis, and as such treatment is based upon how the necrosis came about. Treatment of necrosis typically involves two distinct processes: Usually, the underlying cause of the necrosis must be treated before the dead tissue itself can be dealt with.[citation needed]

  • Debridement, referring to the removal of dead tissue by surgical or non-surgical means, is the standard therapy for necrosis. Depending on the severity of the necrosis, this may range from removal of small patches of skin to complete amputation of affected limbs or organs. Chemical removal of necrotic tissue is another option in which enzymatic debriding agents, categorised as proteolytic, fibrinolytic or collagenases, are used to target the various components of dead tissue.[18] In select cases, special maggot therapy using Lucilia sericata larvae has been employed to remove necrotic tissue and infection.[19]
  • In the case of ischemia, which includes myocardial infarction, the restriction of blood supply to tissues causes hypoxia and the creation of reactive oxygen species (ROS) that react with, and damage proteins and membranes. Antioxidant treatments can be applied to scavenge the ROS.[20]
  • Wounds caused by physical agents, including physical trauma and chemical burns, can be treated with antibiotics and anti-inflammatory drugs to prevent bacterial infection and inflammation. Keeping the wound clean from infection also prevents necrosis.
  • Chemical and toxic agents (e.g. pharmaceutical drugs, acids, bases) react with the skin leading to skin loss and eventually necrosis. Treatment involves identification and discontinuation of the harmful agent, followed by treatment of the wound, including prevention of infection and possibly the use of immunosuppressive therapies such as anti-inflammatory drugs or immunosuppressants.[21] In the example of a snake bite, the use of anti-venom halts the spread of toxins whilst receiving antibiotics to impede infection.[22]

Even after the initial cause of the necrosis has been halted, the necrotic tissue will remain in the body. The body's immune response to apoptosis, which involves the automatic breaking down and recycling of cellular material, is not triggered by necrotic cell death due to the apoptotic pathway being disabled.[23]

In plants

If calcium is deficient, pectin cannot be synthesized, and therefore the cell walls cannot be bonded and thus an impediment of the meristems. This will lead to necrosis of stem and root tips and leaf edges.[24] For example, necrosis of tissue can occur in Arabidopsis thaliana due to plant pathogens.[citation needed]

Cacti such as the Saguaro and Cardon in the Sonoran Desert experience necrotic patch formation regularly; a species of Dipterans called Drosophila mettleri has developed a p450 detoxification system to enable it to use the exudates released in these patches to both nest and feed larvae.[citation needed]

See also

 
Wikimedia Commons has media related to Necrosis.

References

  1. ^ a b c d e Proskuryakov SY, Konoplyannikov AG, Gabai VL (2003). "Necrosis: a specific form of programmed cell death?". Exp. Cell Res. 283 (1): 1–16. doi:10.1016/S0014-4827(02)00027-7. PMID 12565815.
  2. ^ Kasper DL, Zaleznik DF (2001). "Gas gangrene, antibiotic associated colitis, and other Clostridial infections". In Stone RM (ed.). Harrison's principles of internal medicine self-assessment and board review (15th ed.). New York: McGraw-Hill, Medical Pub. Division. pp. 922–927. ISBN 978-0071386784.
  3. ^ Nirmala GJ, Lopus M (2020). "Cell death mechanisms in eukaryotes". Cell Biol Toxicol. 36 (2): 145–164. doi:10.1007/s10565-019-09496-2. PMID 31820165. S2CID 208869679.
  4. ^ Rock, Kenneth (2008). "The inflammatory response to cell death". Annual Review of Pathology. 3: 99–126. doi:10.1146/annurev.pathmechdis.3.121806.151456. PMC 3094097. PMID 18039143.
  5. ^ a b c d e f g Craft J, Gordon C, Tiziani A, Huether SE, McCance KL, Brashers VL (2010). Understanding pathophysiology (1st ed.). Chatswood, N.S.W.: Elsevier Australia. ISBN 978-0729539517.
  6. ^ a b c d e f g h i j k l Kumar V, Abbas AK, Aster JC, Fausto N (2010). Robbins and Cotran pathologic basis of disease (8th ed.). Philadelphia, PA: Saunders/Elsevier. pp. 12–41. ISBN 978-1416031215.
  7. ^ a b c McConnell TH (2007). The nature of disease: pathology for the health professions. Baltimore, Mar.: Lippincott Williams & Wilkins. ISBN 978-0781753173.
  8. ^ Sattar (2015). Fundamentals of Pathology (2015th ed.). Chicago, IL: Pathoma LLC. p. 5. ISBN 978-0-9832246-2-4.
  9. ^ a b Stevens A, Lowe JS, Young B, Deakin PJ (2002). Wheater's basic histopathology: a colour atlas and text (4th ed.). Edinburgh: Churchill Livingstone. ISBN 978-0443070013.
  10. ^ Saey, Tina Hesman (5 November 2012). "Cancer cells self-destruct in blind mole rats". Science News. Society for Science and the Public. from the original on 19 June 2013. Retrieved 27 November 2012.
  11. ^ Gorbunova V, Hine C, Tian X, Ablaeva J, Gudkov AV, Nevo E, Seluanov A (2012). "Cancer resistance in the blind mole rat is mediated by concerted necrotic cell death mechanism". Proc. Natl. Acad. Sci. U.S.A. 109 (47): 19392–6. Bibcode:2012PNAS..10919392G. doi:10.1073/pnas.1217211109. PMC 3511137. PMID 23129611.
  12. ^ a b c d e f Raffray M, Cohen GM; Cohen (1997). "Apoptosis and necrosis in toxicology: a continuum or distinct modes of cell death?". Pharmacol. Ther. 75 (3): 153–77. doi:10.1016/s0163-7258(97)00037-5. PMID 9504137.
  13. ^ Nazarian RM, Van Cott EM, Zembowicz A, Duncan LM (2009). "Warfarin-induced skin necrosis". J. Am. Acad. Dermatol. 61 (2): 325–32. doi:10.1016/j.jaad.2008.12.039. PMID 19615543.
  14. ^ Yanagawa, Youichi (10 October 1980). "Cutaneous hemorrhage or necrosis findings after Vespa mandarinia (wasp) stings may predict the occurrence of multiple organ injury: A case report and review of literature". Clinical Toxicology. 45 (7): 803–807. doi:10.1080/15563650701664871. PMID 17952752. S2CID 11337426.
  15. ^ a b c d e f g Kroemer G, Galluzzi L, Vandenabeele P, Abrams J, Alnemri ES, Baehrecke EH, Blagosklonny MV, El-Deiry WS, Golstein P, Green DR, Hengartner M, Knight RA, Kumar S, Lipton SA, Malorni W, Nuñez G, Peter ME, Tschopp J, Yuan J, Piacentini M, Zhivotovsky B, Melino G, Nomenclature Committee on Cell Death 2009 (January 2009). "Classification of cell death: recommendations of the Nomenclature Committee on Cell Death 2009". Cell Death Differ. 16 (1): 3–11. doi:10.1038/cdd.2008.150. PMC 2744427. PMID 18846107.
  16. ^ page 320 2020-08-04 at the Wayback Machine in: Alberto M Marchevsky; Bonnie Balzer; Fadi W Abdul-Karim (2014). Intraoperative Consultation E-Book: A Volume in the Series: Foundations in Diagnostic Pathology. Elsevier Health Sciences. ISBN 978-0-323-32299-7. from the original on 2020-08-07. Retrieved 2020-01-03.
  17. ^ Wippold FJ, Lämmle M, Anatelli F, Lennerz J, Perry A (2006). "Neuropathology for the neuroradiologist: palisades and pseudopalisades". AJNR Am J Neuroradiol. 27 (10): 2037–41. PMC 7977220. PMID 17110662.
  18. ^ Singhal A, Reis ED, Kerstein MD (2001). "Options for nonsurgical debridement of necrotic wounds". Adv Skin Wound Care. 14 (2): 96–100, quiz 102–3. doi:10.1097/00129334-200103000-00014. PMID 11899913.
  19. ^ Horobin AJ, Shakesheff KM, Pritchard DI (2005). "Maggots and wound healing: an investigation of the effects of secretions from Lucilia sericata larvae upon the migration of human dermal fibroblasts over a fibronectin-coated surface". Wound Repair Regen. 13 (4): 422–33. doi:10.1111/j.1067-1927.2005.130410.x. PMID 16008732. S2CID 7861732.
  20. ^ Eum HA, Cha YN, Lee SM (2007). "Necrosis and apoptosis: sequence of liver damage following reperfusion after 60 min ischemia in rats". Biochem. Biophys. Res. Commun. 358 (2): 500–5. doi:10.1016/j.bbrc.2007.04.153. PMID 17490613.
  21. ^ Cooper KL (2012). "Drug reaction, skin care, skin loss". Crit Care Nurse. 32 (4): 52–9. doi:10.4037/ccn2012340. PMID 22855079.
  22. ^ Chotenimitkhun R, Rojnuckarin P; Rojnuckarin (2008). "Systemic antivenom and skin necrosis after green pit viper bites". Clin Toxicol. 46 (2): 122–5. doi:10.1080/15563650701266826. PMID 18259959. S2CID 6827421.
  23. ^ Edinger AL, Thompson CB; Thompson (2004). "Death by design: apoptosis, necrosis and autophagy". Curr. Opin. Cell Biol. 16 (6): 663–9. doi:10.1016/j.ceb.2004.09.011. PMID 15530778.
  24. ^ Capon B (2010). Botany for gardeners (3rd ed.). Portland, OR: Timber Press. ISBN 978-1-60469-095-8.

External links

  • Undersea and Hyperbaric Medical Society. . Archived from the original on 5 July 2008. Retrieved 25 July 2008.
  • Secondary necrosis of a neutrophil

February 28, 2023
necrosis, other, uses, disambiguation, confused, with, narcosis, from, ancient, greek, νέκρωσις, nékrōsis, death, form, cell, injury, which, results, premature, death, cells, living, tissue, autolysis, caused, factors, external, cell, tissue, such, infection, . For other uses see Necrosis disambiguation Not to be confused with Narcosis Necrosis from Ancient Greek nekrwsis nekrōsis death is a form of cell injury which results in the premature death of cells in living tissue by autolysis 1 Necrosis is caused by factors external to the cell or tissue such as infection or trauma which result in the unregulated digestion of cell components In contrast apoptosis is a naturally occurring programmed and targeted cause of cellular death While apoptosis often provides beneficial effects to the organism necrosis is almost always detrimental and can be fatal 2 Structural changes of cells undergoing necrosis and apoptosis Cellular death due to necrosis does not follow the apoptotic signal transduction pathway but rather various receptors are activated and result in the loss of cell membrane integrity 3 and an uncontrolled release of products of cell death into the extracellular space 1 This initiates in the surrounding tissue an inflammatory response which attracts leukocytes and nearby phagocytes which eliminate the dead cells by phagocytosis However microbial damaging substances released by leukocytes would create collateral damage to surrounding tissues 4 This excess collateral damage inhibits the healing process Thus untreated necrosis results in a build up of decomposing dead tissue and cell debris at or near the site of the cell death A classic example is gangrene For this reason it is often necessary to remove necrotic tissue surgically a procedure known as debridement citation needed Contents 1 Classification 1 1 Morphological patterns 1 2 Other clinical classifications of necrosis 2 Causes 2 1 External factors 2 2 Internal factors 3 Pathogenesis 3 1 Pathways 3 2 Histopathological changes 4 Treatment 5 In plants 6 See also 7 References 8 External linksClassification EditStructural signs that indicate irreversible cell injury and the progression of necrosis include dense clumping and progressive disruption of genetic material and disruption to membranes of cells and organelles 5 Morphological patterns Edit There are six distinctive morphological patterns of necrosis 6 Coagulative necrosis is characterized by the formation of a gelatinous gel like substance in dead tissues in which the architecture of the tissue is maintained 6 and can be observed by light microscopy Coagulation occurs as a result of protein denaturation causing albumin to transform into a firm and opaque state 5 This pattern of necrosis is typically seen in hypoxic low oxygen environments such as infarction Coagulative necrosis occurs primarily in tissues such as the kidney heart and adrenal glands 5 Severe ischemia most commonly causes necrosis of this form 7 Liquefactive necrosis or colliquative necrosis in contrast to coagulative necrosis is characterized by the digestion of dead cells to form a viscous liquid mass 6 This is typical of bacterial or sometimes fungal infections because of their ability to stimulate an inflammatory response The necrotic liquid mass is frequently creamy yellow due to the presence of dead leukocytes and is commonly known as pus 6 Hypoxic infarcts in the brain presents as this type of necrosis because the brain contains little connective tissue but high amounts of digestive enzymes and lipids and cells therefore can be readily digested by their own enzymes 5 Gangrenous necrosis can be considered a type of coagulative necrosis that resembles mummified tissue It is characteristic of ischemia of lower limb and the gastrointestinal tracts If superimposed infection of dead tissues occurs then liquefactive necrosis ensues wet gangrene 8 Caseous necrosis can be considered a combination of coagulative and liquefactive necrosis 5 typically caused by mycobacteria e g tuberculosis fungi and some foreign substances The necrotic tissue appears as white and friable like clumped cheese Dead cells disintegrate but are not completely digested leaving granular particles 5 Microscopic examination shows amorphous granular debris enclosed within a distinctive inflammatory border 6 Some granulomas contain this pattern of necrosis 9 Fat necrosis is specialized necrosis of fat tissue 9 resulting from the action of activated lipases on fatty tissues such as the pancreas In the pancreas it leads to acute pancreatitis a condition where the pancreatic enzymes leak out into the peritoneal cavity and liquefy the membrane by splitting the triglyceride esters into fatty acids through fat saponification 6 Calcium magnesium or sodium may bind to these lesions to produce a chalky white substance 5 The calcium deposits are microscopically distinctive and may be large enough to be visible on radiographic examinations 7 To the naked eye calcium deposits appear as gritty white flecks 7 Fibrinoid necrosis is a special form of necrosis usually caused by immune mediated vascular damage It is marked by complexes of antigen and antibodies referred to as immune complexes deposited within arterial walls 6 together with fibrin 6 Other clinical classifications of necrosis Edit There are also very specific forms of necrosis such as gangrene term used in clinical practices for limbs which have had severe hypoxia gummatous necrosis due to spirochaetal infections and hemorrhagic necrosis due to the blockage of venous drainage of an organ or tissue Some spider bites may lead to necrosis In the United States only spider bites from the brown recluse spider genus Loxosceles reliably progress to necrosis In other countries spiders of the same genus such as the Chilean recluse in South America are also known to cause necrosis Claims that yellow sac spiders and hobo spiders possess necrotic venom have not been substantiated In blind mole rats genus Spalax the process of necrosis replaces the role of the systematic apoptosis normally used in many organisms Low oxygen conditions such as those common in blind mole rats burrows usually cause cells to undergo apoptosis In adaptation to higher tendency of cell death blind mole rats evolved a mutation in the tumor suppressor protein p53 which is also used in humans to prevent cells from undergoing apoptosis Human cancer patients have similar mutations and blind mole rats were thought to be more susceptible to cancer because their cells cannot undergo apoptosis However after a specific amount of time within 3 days according to a study conducted at the University of Rochester the cells in blind mole rats release interferon beta which the immune system normally uses to counter viruses in response to over proliferation of cells caused by the suppression of apoptosis In this case the interferon beta triggers cells to undergo necrosis and this mechanism also kills cancer cells in blind mole rats Because of tumor suppression mechanisms such as this blind mole rats and other spalacids are resistant to cancer 10 11 Causes Edit Necrotic leg wound caused by a brown recluse spider bite Necrosis may occur due to external or internal factors External factors Edit External factors may involve mechanical trauma physical damage to the body which causes cellular breakdown damage to blood vessels which may disrupt blood supply to associated tissue and ischemia 12 Thermal effects extremely high or low temperature can result in necrosis due to the disruption of cells citation needed In frostbite crystals form increasing the pressure of remaining tissue and fluid causing the cells to burst citation needed Under extreme conditions tissues and cells die through an unregulated process of destruction of membranes and cytosol 13 Internal factors Edit Internal factors causing necrosis include trophoneurotic disorders diseases that occur due to defective nerve action in a part of an organ which results in failure of nutrition injury and paralysis of nerve cells Pancreatic enzymes lipases are the major cause of fat necrosis 12 Necrosis can be activated by components of the immune system such as the complement system bacterial toxins activated natural killer cells and peritoneal macrophages 1 Pathogen induced necrosis programs in cells with immunological barriers intestinal mucosa may alleviate invasion of pathogens through surfaces affected by inflammation 1 Toxins and pathogens may cause necrosis toxins such as snake venoms may inhibit enzymes and cause cell death 12 Necrotic wounds have also resulted from the stings of Vespa mandarinia 14 Pathological conditions are characterized by inadequate secretion of cytokines Nitric oxide NO and reactive oxygen species ROS are also accompanied by intense necrotic death of cells 12 A classic example of a necrotic condition is ischemia which leads to a drastic depletion of oxygen glucose and other trophic factors and induces massive necrotic death of endothelial cells and non proliferating cells of surrounding tissues neurons cardiomyocytes renal cells etc 1 Recent cytological data indicates that necrotic death occurs not only during pathological events but it is also a component of some physiological process 12 Activation induced death of primary T lymphocytes and other important constituents of the immune response are caspase independent and necrotic by morphology hence current researchers have demonstrated that necrotic cell death can occur not only during pathological processes but also during normal processes such as tissue renewal embryogenesis and immune response 12 Pathogenesis EditPathways Edit Until recently necrosis was thought to be an unregulated process 15 However there are two broad pathways in which necrosis may occur in an organism 15 The first of these two pathways initially involves oncosis where swelling of the cells occurs 15 Affected cells then proceed to blebbing and this is followed by pyknosis in which nuclear shrinkage transpires 15 In the final step of this pathway cell nuclei are dissolved into the cytoplasm which is referred to as karyolysis 15 The second pathway is a secondary form of necrosis that is shown to occur after apoptosis and budding 15 In these cellular changes of necrosis the nucleus breaks into fragments known as karyorrhexis 15 Histopathological changes Edit Further information Myocardial infarction diagnosis Karyolysis and contraction band necrosis in myocardial infarction heart attack The nucleus changes in necrosis and characteristics of this change are determined by the manner in which its DNA breaks down Karyolysis the chromatin of the nucleus fades due to the loss of the DNA by degradation 6 Karyorrhexis the shrunken nucleus fragments to complete dispersal 6 Pyknosis the nucleus shrinks and the chromatin condenses 6 Other typical cellular changes in necrosis include Cytoplasmic hypereosinophilia on samples with H amp E stain 16 It is seen as a darker stain of the cytoplasm The cell membrane appears discontinuous when viewed with an electron microscope This discontinuous membrane is caused by cell blebbing and the loss of microvilli 6 On a larger histologic scale pseudopalisades false palisades are hypercellular zones that typically surround necrotic tissue Pseudopalisading necrosis indicates an aggressive tumor 17 Pyknosis in a bile infarct Cytoplasmic hypereosinophilia seen in left half of image Pseudopalisading seen around necrosis in glioblastomaTreatment EditThere are many causes of necrosis and as such treatment is based upon how the necrosis came about Treatment of necrosis typically involves two distinct processes Usually the underlying cause of the necrosis must be treated before the dead tissue itself can be dealt with citation needed Debridement referring to the removal of dead tissue by surgical or non surgical means is the standard therapy for necrosis Depending on the severity of the necrosis this may range from removal of small patches of skin to complete amputation of affected limbs or organs Chemical removal of necrotic tissue is another option in which enzymatic debriding agents categorised as proteolytic fibrinolytic or collagenases are used to target the various components of dead tissue 18 In select cases special maggot therapy using Lucilia sericata larvae has been employed to remove necrotic tissue and infection 19 In the case of ischemia which includes myocardial infarction the restriction of blood supply to tissues causes hypoxia and the creation of reactive oxygen species ROS that react with and damage proteins and membranes Antioxidant treatments can be applied to scavenge the ROS 20 Wounds caused by physical agents including physical trauma and chemical burns can be treated with antibiotics and anti inflammatory drugs to prevent bacterial infection and inflammation Keeping the wound clean from infection also prevents necrosis Chemical and toxic agents e g pharmaceutical drugs acids bases react with the skin leading to skin loss and eventually necrosis Treatment involves identification and discontinuation of the harmful agent followed by treatment of the wound including prevention of infection and possibly the use of immunosuppressive therapies such as anti inflammatory drugs or immunosuppressants 21 In the example of a snake bite the use of anti venom halts the spread of toxins whilst receiving antibiotics to impede infection 22 Even after the initial cause of the necrosis has been halted the necrotic tissue will remain in the body The body s immune response to apoptosis which involves the automatic breaking down and recycling of cellular material is not triggered by necrotic cell death due to the apoptotic pathway being disabled 23 In plants EditIf calcium is deficient pectin cannot be synthesized and therefore the cell walls cannot be bonded and thus an impediment of the meristems This will lead to necrosis of stem and root tips and leaf edges 24 For example necrosis of tissue can occur in Arabidopsis thaliana due to plant pathogens citation needed Cacti such as the Saguaro and Cardon in the Sonoran Desert experience necrotic patch formation regularly a species of Dipterans called Drosophila mettleri has developed a p450 detoxification system to enable it to use the exudates released in these patches to both nest and feed larvae citation needed See also Edit Wikimedia Commons has media related to Necrosis Avascular necrosis Frostbite Gangrene Necrotizing fasciitis Osteonecrosis of the jaw Toxic epidermal necrolysis NecroptosisReferences Edit a b c d e Proskuryakov SY Konoplyannikov AG Gabai VL 2003 Necrosis a specific form of programmed cell death Exp Cell Res 283 1 1 16 doi 10 1016 S0014 4827 02 00027 7 PMID 12565815 Kasper DL Zaleznik DF 2001 Gas gangrene antibiotic associated colitis and other Clostridial infections In Stone RM ed Harrison s principles of internal medicine self assessment and board review 15th ed New York McGraw Hill Medical Pub Division pp 922 927 ISBN 978 0071386784 Nirmala GJ Lopus M 2020 Cell death mechanisms in eukaryotes Cell Biol Toxicol 36 2 145 164 doi 10 1007 s10565 019 09496 2 PMID 31820165 S2CID 208869679 Rock Kenneth 2008 The inflammatory response to cell death Annual Review of Pathology 3 99 126 doi 10 1146 annurev pathmechdis 3 121806 151456 PMC 3094097 PMID 18039143 a b c d e f g Craft J Gordon C Tiziani A Huether SE McCance KL Brashers VL 2010 Understanding pathophysiology 1st ed Chatswood N S W Elsevier Australia ISBN 978 0729539517 a b c d e f g h i j k l Kumar V Abbas AK Aster JC Fausto N 2010 Robbins and Cotran pathologic basis of disease 8th ed Philadelphia PA Saunders Elsevier pp 12 41 ISBN 978 1416031215 a b c McConnell TH 2007 The nature of disease pathology for the health professions Baltimore Mar Lippincott Williams amp Wilkins ISBN 978 0781753173 Sattar 2015 Fundamentals of Pathology 2015th ed Chicago IL Pathoma LLC p 5 ISBN 978 0 9832246 2 4 a b Stevens A Lowe JS Young B Deakin PJ 2002 Wheater s basic histopathology a colour atlas and text 4th ed Edinburgh Churchill Livingstone ISBN 978 0443070013 Saey Tina Hesman 5 November 2012 Cancer cells self destruct in blind mole rats Science News Society for Science and the Public Archived from the original on 19 June 2013 Retrieved 27 November 2012 Gorbunova V Hine C Tian X Ablaeva J Gudkov AV Nevo E Seluanov A 2012 Cancer resistance in the blind mole rat is mediated by concerted necrotic cell death mechanism Proc Natl Acad Sci U S A 109 47 19392 6 Bibcode 2012PNAS 10919392G doi 10 1073 pnas 1217211109 PMC 3511137 PMID 23129611 a b c d e f Raffray M Cohen GM Cohen 1997 Apoptosis and necrosis in toxicology a continuum or distinct modes of cell death Pharmacol Ther 75 3 153 77 doi 10 1016 s0163 7258 97 00037 5 PMID 9504137 Nazarian RM Van Cott EM Zembowicz A Duncan LM 2009 Warfarin induced skin necrosis J Am Acad Dermatol 61 2 325 32 doi 10 1016 j jaad 2008 12 039 PMID 19615543 Yanagawa Youichi 10 October 1980 Cutaneous hemorrhage or necrosis findings after Vespa mandarinia wasp stings may predict the occurrence of multiple organ injury A case report and review of literature Clinical Toxicology 45 7 803 807 doi 10 1080 15563650701664871 PMID 17952752 S2CID 11337426 a b c d e f g Kroemer G Galluzzi L Vandenabeele P Abrams J Alnemri ES Baehrecke EH Blagosklonny MV El Deiry WS Golstein P Green DR Hengartner M Knight RA Kumar S Lipton SA Malorni W Nunez G Peter ME Tschopp J Yuan J Piacentini M Zhivotovsky B Melino G Nomenclature Committee on Cell Death 2009 January 2009 Classification of cell death recommendations of the Nomenclature Committee on Cell Death 2009 Cell Death Differ 16 1 3 11 doi 10 1038 cdd 2008 150 PMC 2744427 PMID 18846107 page 320 Archived 2020 08 04 at the Wayback Machine in Alberto M Marchevsky Bonnie Balzer Fadi W Abdul Karim 2014 Intraoperative Consultation E Book A Volume in the Series Foundations in Diagnostic Pathology Elsevier Health Sciences ISBN 978 0 323 32299 7 Archived from the original on 2020 08 07 Retrieved 2020 01 03 Wippold FJ Lammle M Anatelli F Lennerz J Perry A 2006 Neuropathology for the neuroradiologist palisades and pseudopalisades AJNR Am J Neuroradiol 27 10 2037 41 PMC 7977220 PMID 17110662 Singhal A Reis ED Kerstein MD 2001 Options for nonsurgical debridement of necrotic wounds Adv Skin Wound Care 14 2 96 100 quiz 102 3 doi 10 1097 00129334 200103000 00014 PMID 11899913 Horobin AJ Shakesheff KM Pritchard DI 2005 Maggots and wound healing an investigation of the effects of secretions from Lucilia sericata larvae upon the migration of human dermal fibroblasts over a fibronectin coated surface Wound Repair Regen 13 4 422 33 doi 10 1111 j 1067 1927 2005 130410 x PMID 16008732 S2CID 7861732 Eum HA Cha YN Lee SM 2007 Necrosis and apoptosis sequence of liver damage following reperfusion after 60 min ischemia in rats Biochem Biophys Res Commun 358 2 500 5 doi 10 1016 j bbrc 2007 04 153 PMID 17490613 Cooper KL 2012 Drug reaction skin care skin loss Crit Care Nurse 32 4 52 9 doi 10 4037 ccn2012340 PMID 22855079 Chotenimitkhun R Rojnuckarin P Rojnuckarin 2008 Systemic antivenom and skin necrosis after green pit viper bites Clin Toxicol 46 2 122 5 doi 10 1080 15563650701266826 PMID 18259959 S2CID 6827421 Edinger AL Thompson CB Thompson 2004 Death by design apoptosis necrosis and autophagy Curr Opin Cell Biol 16 6 663 9 doi 10 1016 j ceb 2004 09 011 PMID 15530778 Capon B 2010 Botany for gardeners 3rd ed Portland OR Timber Press ISBN 978 1 60469 095 8 External links EditLife In The Fast Lane toxicology Conundrum 018 Undersea and Hyperbaric Medical Society Necrotizing Soft Tissue Infections Archived from the original on 5 July 2008 Retrieved 25 July 2008 Secondary necrosis of a neutrophil Retrieved from https en wikipedia org w index php title Necrosis amp oldid 1139889883, wikipedia, wiki, book, books, library,

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