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Dr: Wael H.Mansy , MD Assistant Professor College of Pharmacy King Saud University

Cell injury. Dr: Wael H.Mansy , MD Assistant Professor College of Pharmacy King Saud University. Study objectives. • Compare and contrast the various forms of cellular adaptation . What is the purpose of these adaptive changes?

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Dr: Wael H.Mansy , MD Assistant Professor College of Pharmacy King Saud University

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  1. Cell injury Dr: Wael H.Mansy, MD Assistant Professor College of Pharmacy King Saud University

  2. Study objectives • Compare and contrast the various forms of cellular adaptation. What is the purpose of these adaptive changes? • Discuss the two underlying mechanisms by which cellular injury can occur. • List the various classifications of cellular injury that can occur and give examples of each. • Describe the major manifestations that present when cells are injured. Why does each of these manifestations occur? • Define apoptosis and necrotic cell death. How do they differ? • List the specific types of cellular necrosis that may occur along with their distinct characteristics. • Define gangrene and gas gangrene. • Discuss the two mechanisms by which tissue repair occurs. Give examples of specific cell types that will utilize each repair mechanism. • List the steps involved in wound repair along with the key features of each step. • List various factors that can impair wound healing. • What is a keloid scar? Why does it occur?

  3. Cell injury • When the cell is exposed to any injurious agent or stress ,a consequence of events follows, that is loosely termed cell injury.Cell injury is reversible up to certain point. • To survive, cells must have the ability for adaptation to variable conditions. This process of adaptation can involve changes in cellular size, number or type. • If the stimulus persist or severe enough from the beginning , cell death occur .

  4. Five Cellular Adaptations to Injury: • Atrophy • Hypertrophy • Hyperplasia • Metaplasia • Dysplasia Cell Adaptation to Injury

  5. Cell Adaptation to Injury 1) Atrophy • It means Decrease or shrinkage in cellular size. • That is either Physiological or Pathological • Pathologic atrophy occur due to ↓ ↓ ↓ in : • Workload • Pressure • Use • Blood supply • Nutrition • Hormonal Stimulation • Nervous Stimulation • Atrophy is generally a reversible process, except for atrophy caused by loss of nervous innervations to a tissue. • Causes of atrophy include prolonged bed rest, disuse of limbs or tissue, poor tissue nutrition and ischemia.

  6. Cell Adaptation to Injury 3) Hypertrophy • Increase in cell size and tissue mass. • Occurs when a cell or tissue is exposed to an increased workload. • Occurs in tissues that cannot increase cell number as an adaptive response. • Hypertrophy may be : • normal physiologic response, such as the increase in muscle mass that is seen with exercise • pathologic as in the case of the cardiac hypertrophy that is seen with prolonged hypertension. • or compensatory process, when one kidney is removed, for example, the remaining kidney hypertrophies to increase its functional capacity.

  7. Cell Adaptation to Injury 2) Hyperplasia • Increase in number of cells resulting from increased rate of cellular division. • It is either: • Physiologic process, as in the breast and uterine hyperplasia that occurs during pregnancy, • Pathologic: such as Benign Prostatic Hyperplasia (BPH) and gingival hyperplasia (overgrowth of gum tissues) that maybe seen in certain patients receiving the drug phenytoin. • or compensatory mechanism:for example, when a portion of the liver is surgically removed, the remaining hepatocytes (liver cells) increase in number to preserve the functional capacity of the liver.

  8. Cell Adaptation to Injury 4) Metaplasia • The conversion of one cell type to another cell type that might have a better chance of survival under certain circumstances. • Metaplasia occurs in response to chronic irritation or inflammation. • An example of metaplasia is: • in the respiratory passages of chronic cigarette smokers, following years of exposure to irritating cigarette smoke, the ciliated columnar epithelium lining the respiratory passages gradually converts to stratified squamous epithelium which although be better to survive to the cigarette smoke, they lack the cilia of the columnar epithelial cells that are necessary for clearing particulates from the surfaces of the respiratory passages.

  9. Cell Adaptation to Injury 5) Dysplasia • A derangement of cell growth that leads to tissues with cells of varying size, shape and appearance. • Generally occurs in response to chronic irritation and inflammation. Dysplasia may be a strong precursor to cancer in certain instances such as in the cervix or respiratory tract. However, dysplasia is an adaptive process and as such does not necessarily lead to cancer. In many cases, the dysplastic cells revert to their former structure and function.

  10. Classification of Cellular injury • Physical injury • Mechanical trauma • Temperature extremes (burn injury, frostbite) • Electrical current • Chemical injury • Chemicals, toxins, heavy metals, solvents, smoke, • pollutants, drugs, gases • Radiation injury • Ionizing radiation — gamma rays, X rays • Non-ionizing radiation — microwaves, infrared, laser • Biologic agents • Bacteria, viruses, parasites • Nutritional injury • Malnutrition • Obesity

  11. Cellular injury Although the causes of cellular injury are many , the underlying mechanisms of cellular injury usually fall into one of two categories: • free radical injury • hypoxic injury

  12. Cellular injury 1)Free radical injury • Free radicals are highly reactive chemical species that have one or more unpaired electrons in their outer shell. • Examples of free radicals includesuperoxide (O−2),hydroxyl radicals (OH−) and hydrogen peroxide(H2O2). • Free radicals are generated as by-products of normal cell metabolism and are inactivated by free radical–scavenging enzymes within the body such as Catalase and glutathione peroxidase. • Injury to cells occur when: • excess free radicals are formed from exogenous sources or • the free radical protective mechanisms fail.

  13. Cellular injury 1)Free radical injury • Free radicals are highly reactive and can injure cells through: 1. Peroxidation of membrane lipids. 2. Damage of cellular proteins. 3. Mutation of cellular DNA. • Exogenous sources of free radicals include tobacco smoke, organic solvents, pollutants, radiation and pesticides. • Free radical injury has been implicated as playing a key role in: 1.The normal aging process. 2.Number of disease states such as diabetes mellitus, cancer, atheroscelrosis, Alzheimer’s disease and rheumatoid arthritis.

  14. Cellular injury 2)Hypoxic cell injury • Hypoxia is: • a lack of oxygen in cells and tissues that generally results from ischemia. • • The hypoxic cellular injury process is either: • reversible, if oxygen is quickly restored, • Or irreversible and lead to cell death. Certain tissues such as the brain are particularly sensitive to hypoxic injury. Death of brain tissues can occur only 4 to 6 minutes after hypoxia begins.

  15. Cellular injury 2)Hypoxic cell injury • During periods of hypoxia: • Aerobic metabolism of the cells begins to fail. • This leads to dramatic decreases in energy production (ATP) within the cells. • Hypoxic cells begin to swell as energy-driven processes begin to fail, (such as ATP-driven ion pumps). • The pH of the extracellular environment begins to decrease as waste products begin to accumulate, such as lactic acid, a product of anaerobic metabolism. • Accumulation of intracellular calcium, which is normally closely regulated within cells. There are a number of calcium-dependent protease enzymes present within cells that become activated in the presence of excess calcium and begin to digest important cellular constituents.

  16. Reversible and Irreversible Cell Injury Irreversible: Reversible:  Decrease generation Sever of ATP mitochondrial  Loss of cell changes membrane integrity Persistent or Extensive damage excessive  Defects in protein to plasma membranes injury synthesis, and DNA damage Swelling of lysosomes

  17. Manifestation of Cellular injury • 1. Cellular swelling • Caused by an accumulation of water due to the failure of energy driven ion pumps. Breakdown of cell membrane integrity and accumulation of cellular electrolytes may also occur. • Cellular swelling is considered to be a reversible change.

  18. Manifestation of Cellular injury • 2. Cellular accumulations • In addition to water, injured cells can accumulate a number of different substances as metabolism and transport processes begin to fail. • Substances that can be accumulated in injured cells may include fats, proteins, glycogen, calcium, uric acid and certain pigments such as melanin. • These accumulations are generally reversible but can indicate a greater degree of cellular injury. Accumulation of these substances can be so marked that enlargement of a tissue or organ may occur (for example, fatty accumulation in an injured liver).

  19. Cell death Cell death falls into two main categories: • Apoptosis: controlled, “pre-programmed” cell death • Necrotic cell death: unregulated, enzymatic digestion of a cell and its components.

  20. Morphological characteristics of pyknosis and other forms of nuclear destruction

  21. Cell death 1) Apoptosis • A controlled, “pre-programmed” cell death that occurs with aging and normal wear and tear of the cell. • Apoptosis may be a mechanism to eliminate worn-out or genetically damaged cells. Certain viral infections (the Epstein–Barr virus, for example) may activate apoptosis within an infected cell, thus killing both the host cell and infecting virus. • It has been theorized that cancer may arise as a failure of normal apoptosis in damaged or mutated cells.

  22. Cell death 2) Necrosis • Occurs as a result of irreversible cellular injury. • Involves the unregulated, enzymatic digestion (“autolysis”) of a cell and its components. • Different types of tissues tend to undergo different types of necrosis. • Three main types of necrosis have been identified: • Liquefaction necrosis • Caseous necrosis • Coagulative necrosis

  23. Cell death 2) Necrosis Main types of necrosis have been identified: • Liquefaction necrosis • Digestive enzymes released by necrotic cells soften and liquefy dead tissue. • Occurs in tissues, such as the brain, that are rich in hydrolytic enzymes.

  24. Cell death 2) Necrosis • Caseous necrosis • Dead tissue takes on a crumbly, “cheese like” appearance. Dead cells disintegrate but their debris is not fully digested by hydrolytic enzymes. • Occurs in conditions like tuberculosis where there is prolonged inflammation and immune activity.

  25. Cell death 2) Necrosis • Coagulative necrosis • Dead tissues appear firm, gray and slightly swollen. • Often occurs when cell death results from ischemia and hypoxia. The acidosis denatures cellular proteins and hydrolytic enzymes. • Seen with myocardial infarction, for example.

  26. Gangrene is the clinical term used when a large area of tissue undergoes necrosis. Gangrene may be classified as dry gangrene or wet gangrene • With dry gangrene, the skin surrounding the affected area shrinks, wrinkles and turns black. • In contrast, wet gangrenepresents with an area that is cold, wet from tissue exudates and swollen. • A gas gangrenemay also occur if the area of necrosis becomes infected with bacteria that produce gases as a by-product.

  27. Effects of necrosis  Loss of function of dead area (kidney, brain).  Necrotic area can become a focus for infection.  May evoke certain systematic changes (inflammation, fever).  Necrotic tissue often leak its constituent enzyme in to the blood stream (CPK, AST).

  28. Fate of necrotic tissue  As a result of inflammatory response, necrotic tissue is ultimately demolished and removed.  Replace of necrotic tissue with regenerative cells or scar tissue.  If necrotic tissue is located on surface, leaving a gap of continuity of the surface (ulcer).  If necrotic tissue is neither demolished nor cast off, it is often encapsulated by fibrous connective tissue & ultimatly is impregnated with calcium salts precipitated from the circulation (calcification).

  29. Pathologic Calcification  Is the abnormal tissue disposition of calcium salt  Types of pathologic calcification: Dystrophic calcification 1. Metastatic calcification 2. 324 PHCL

  30. Pathologic Calcification 1. Dystrophic calcification  It occurs despite normal serum levels of calcium and in the absence of derangements seen in area of caseous necrosis. 324 PHCL

  31. Pathologic Calcification 2.Metastatic calcification  Occurs not because of an abnormality of tissues, but because an abnormal concentration of calcium (Hypercalcemia)  Causes of hypercalcemia: 1. Hyperparathyroidism 2.Destruction of bone tissue (e.g. multiple myeloma) 3. Vitamin D-related disorders (e.g. Vitamin D intoxication) 4. Renal failure

  32. Tissue repair Injured or damaged tissues can be repaired in one of two ways: • By regeneration • By connective tissue replacement • The mechanism used for repair will depend upon the type of cells that were injured. • Certain cells in the body are fully or partially capable of regenerating after an injury, whereas, • other cell types are not capable of regeneration and can only be replaced with connective (scar) tissue.

  33. Tissue repair 1) By regeneration • With regeneration, the injured tissue is repaired with the same tissue that was lost. A full return of function occurs and afterward there is little or no evidence of the injury. • Repair by regeneration can occur only in : • labile cells (cells that continue to divide throughout life), such as those of the skin, oral cavity and bone marrow. or • stable cells (cells that have stopped dividing but can be induced to regenerate under appropriate conditions of injury) such as hepatocytes of the liver.

  34. Tissue repair 2) By connective tissue replacement • Certain cells such as nerve cells and cardiac muscle cells are fixed cells and cannot undergo regeneration under any circumstances. These cell types are capable of repairing injuries through connective tissue replacement. • Repair by connective tissue replacement Involves the replacement of functional tissue with nonfunctional connective tissue (collagen). • Full function does not return to the injured tissue. • Scar tissue remains as evidence of the injury.

  35. Systemic factors influencing wound healing Local factors influencing wound healing • Infection • Mechanical factors • Foreign bodies • Size, location • and types of wound Nutrition Metabolic status Circulatory status Hormones

  36. Tissue repair Factors That Impair Wound Healing: • Malnutrition • Poor blood flow and hypoxia • Impaired immune response (immunosuppressive drugs, diseases affecting immune function such as HIV and diabetes) • Infection of wound • Foreign particles in the wound • Old age (decreased immune activity, poor circulation, poor nutrition)

  37. Complications of healing • 1.Proud flesh (piece of granulation tissue above the surfce of wound). • 2.Keloid(genetic abnormality in collagen in healing wound leading to protrusion). • 3.Hernia (internal or incisional-portion of tissue entrapt and may become gangrenous) • 4.Stricture (when scar encircle a tubular structure) • 5.Contracture (scar tissue is shorten and more dense and compact). • 6.Adhesions (when serosal sufaces are inflamed and not resolve serosal surfaces may bind) • 7.Traumatic neuroma (regenerative prolifration of nerve fibers into area of healing causing painfull lump.

  38. Tissue repair Keloid scars • Large, raised scars that result from oversynthesis of collagen and decreased collagen breakdown. Keloid scars are often unsightly and may extend beyond the original boundaries of the wound. • A familial tendency for keloid scar formation has been observed with a greater occurrence in blacks than whites

  39. والحمد لله رب العالمين

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