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General pathology

General pathology. Introduction to pathology Literal translation of the word pathology is the study (logos) of suffering (Pathos). It is a discipline that bridges clinical practice and basic sciences. Pathology is concerned with the study of diseases in a scientific way .

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General pathology

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  1. General pathology

  2. Introduction to pathology Literal translation of the word pathology is the study (logos) of suffering (Pathos). It is a discipline that bridges clinical practice and basic sciences. Pathology is concerned with the study of diseases in a scientific way. It comprises a wide base of scientific data and investigative techniques that are essential practice of modern medicine. Pathology in essence consists of two sets of related changes that are seen in various diseases: 1. Structural 2. Functional

  3. The range of these changes is from those affecting sub-cellular organelles (molecular pathology) up to the alterations seen by the naked eye (gross pathology). Pathology is a dynamic science in that its contents are continuously subjected to changes, revisions and expansions. This is because there are always new scientific methods and findings that in turn shed more light on, add or modify an already established knowledge of various diseases. The ultimate goal of pathology is the identification of the cause or causes of disease (etiology) as well as the mechanisms (pathogenesis) that can eventuate in; • Disease prevention &/or 2. Successful therapy

  4. Cellular Injury and Adaptation Each cell in the body is devoted to carry specific functions, which are dependent on the machinery and metabolic pathways present within the cell. This functional specificity is genetically determined. Normally the cells of the body are in equilibrium with the external environment. They maintain their internal machinery in a dynamically stable and steady state; this is called homeostasis i.e. the supply of raw material (substrates) and O2 are well coordinated with the production of the materials or jobs required.

  5. In the presence of external disturbances that lend to upset the fine equilibrium, changes within the cells occur through internal regulatory mechanisms that counteract the external changes. In other words the cells are able to handle normal (physiological) and sometimes, abnormal (pathological) demands without get injured; to achieve this, a number of changes inside the cells occur that eventually lead to a new but altered steady state. These induced changes are referred to as adaptations.

  6. The aim of adaptations is to preserve cell viability i.e. prevent cell injury. The increase in muscle mass (as in athletes or heavy mechanical workers) is a reflection of an increase in the size of individual muscle fibers so that when the muscle is subjected to excess workload, this will be shared by the thick and strong muscle fibers and thus each fiber is spared excess work and thus escapes injury. This protective adaptation is referred to as hypertrophy. Hypertrophy may be physiological as that of the uterus in pregnancy orpathological as that of the left ventricle in systemic hypertension.

  7. Opposite to the above is the adaptive response atrophy in which there is a decrease in the size and function of cells and consequently the size of the organ or tissue containing them. If the limits of adaptive capability of the cells are exceeded (persistence of the injurious agent), or when no adaptive response is possible (sudden severe injurious agent that leaves no time for adaptive responses to take place), a sequence of events follows that are collectively known as cell injury

  8. Cell injury is divided into 1. Reversible cell injury 2. Irreversible cell injury • Reversible cell injury indicates that the changes will regress and disappear when the injurious agent is removed; the cells will return to normal, morphologically and functionally. • Irreversible cell injury occurs when the injury persists or when it is severe from the outset. • Here the cell alterations reach the point of no return and progression to cell death is inevitable.

  9. Take an example: • If the blood supply to a portion of the heart musculature is cut off for few minutes and then restored; the muscle cells will sustain reversible injury i.e. after restoration of the blood it will recover and function normally (as in angina pectoris). • But if cessation of blood continues for 60 minutes and then restored the myocardial cells in this instance sustain irreversible injury that terminates invariably to death. • So there is a spectrum cellular changes in response to injurious agent ranging from adaptation to cell death .

  10. Classification (categorization) of injurious agents • Injurious agents can be categorized as follows: • 1. Oxygen deprivation (hypoxia) • 2. Physical agents • 3. Chemical agents • 4. Infectious agents • 5. Immunological reactions • 6. Genetic derangement • 7. Nutritional imbalances

  11. Hypoxia This refers to a decrease in oxygen supply to the cells. It acts through interference with oxidative respiration of the cells. • Hypoxia results from: A. Loss of blood supply (ischemia), which is the most common cause and occurs when arterial flow is interfered with by e.g. narrowing of the lumen of an artery by atherosclerosis, thrombi or emboli. B. Inadequate blood oxygenation due to for e.g. cardiac failure and/or respiratory failure. C. Decrease in the oxygen-carrying capacity of the blood e.g. anemia and carbon mono-oxide poisoning.

  12. Depending on the severity & duration of hypoxia, the cells may show one of the following changes: 1. Adaptive atrophy 2. Injury( reversible or irreversible) For e.g. if the femoral artery is narrowed, the muscles of the leg shrink in size (atrophy). This adaptive response continues till there is a balance between the metabolic needs of the cells (low in this instance) and the available oxygen supply. More severe hypoxia (for e.g. when there is more severe narrowing or complete occlusion of the artery) will induce injury (reversible then irreversible that progresses to cell death).

  13. Physical agents: that include • -Mechanical trauma • -Thermal injury; a. hyperthermia (extreme heat) b. hypothermia (deep cold) • -Electrical injury; a. burn b. ventricular fibrillation • -Radiation; a. direct effect b. indirect effect (free-radical formation)

  14. Chemical agents: that include - Simple chemicals such as glucose and salts in hypertonic concentrations - Oxygen in high concentration - Poisons such as arsenic or cyanide - Air pollutants - Insecticides - Occupational exposure e.g. to asbestos. - Social poisons such as alcohol and narcotic - drugs.

  15. Infectious agents: these include viruses, bacteria, fungi and parasites. Immunological reactions; these are primarily protective defense mechanisms against for e.g. infectious agents. However, sometimes they are harmful and injurious; this occurs in two situations: A. Hypersensitivity reactions (triggered for e.g. by drugs). B. Directed to self-antigens (autoimmune diseases).

  16. Genetic derangement: exemplified by the wide range of hereditary diseases that range from those that are the result of gross chromosomal defects leading to severe congenital malformations e.g.Down's syndrome ,to those that are caused by a single amino acid substitution in the structure of hemoglobin that leading to the synthesis of abnormal Hb e.g. HbS in sickle cell anemia.

  17. Nutritional imbalances - Deficiency: as of proteins-caloric malnutrition or vitamins deficiency etc. - Excess: as of lipids that leads to obesity with all its consequences including fatty change in cells and predisposition to atherosclerosis.

  18. Mechanisms of Cell Injury The biochemical mechanisms responsible for cell injury are complex. There are however, a number of principles that are relevant to most forms of cell injury: 1-The cellular response to injurious stimuli depends on thetype of injury, its duration, and its severity. Thus, small doses of a chemical toxin or brief periods of ischemia may induce reversible injury, whereas large doses of the same toxin or more prolonged ischemia might result either in instantaneous cell death or in slow, irreversible injury leading in time to cell death. .

  19. 2.The consequences of cell injury depend on the type, state,and adaptability of the injured cell. The cell’s nutritional and hormonal status and its metabolic needs are important in its response to injury 3- Cell injury results from functional and biochemical abnormalitiesin one or more of several essential cellular components

  20. Cellular and biochemical sites of damage in cell injury

  21. The most important targets of injurious stimuli are: (1) aerobic respiration involving mitochondrial oxidative phosphorylation and production of ATP; (2)the integrity of cell membranes, on which the ionic and osmotic homeostasis of the cell and its organelles depends; (3) protein synthesis; (4) The cytoskeleton; and (5) The integrity of the genetic apparatus of the cell

  22. A. DEPLETION OF ATP ATP depletion and decreased ATP synthesis are frequently associated with both hypoxic and chemical (toxic) injury . High-energy phosphate in the form of ATP is required for many synthetic and degradative processes within the cell. These include membrane transport, protein synthesis, lipogenesis, and the deacylation – reacylation reactions necessary for phospholipid turnover. *ATP is produced in two ways; The major pathway in mammalian cells is oxidative phosphorylationof adenosine diphosphate. The second is the glycolytic pathway, which can generate ATP in the absence of oxygen using glucose derived either from body fluids or from the hydrolysis of glycogen.

  23. Functional and morphologic consequences of decreased intracellular ATP during cell injury :

  24. 1-The activity of the plasma membrane energy-dependent sodium pump is reduced. Failure of this active transport system, due to diminished ATP concentration and enhanced ATPase activity, causes sodium to accumulate intracellularly and potassium to diffuse out of the cell. The net gain of solute is accompanied by isosmotic gain of water, causing cell swelling, and dilation of the endoplasmic reticulum . 2-Cellular energy metabolism is altered. 3-Failure of the Ca2+ pump leads to influx of Ca2+, with damaging effects on numerous cellular components.

  25. 4 -Structural disruption of the protein synthetic apparatus With prolonged or worsening ATP depletion, reduction in protein synthesis occurs due to; a. Detachment of ribosomes from the rough endoplasmic reticulum b. Dissociation of polysomes into monosomes. 5 -In cells deprived of oxygen or glucose, proteins may become misfolded, and misfolded proteins trigger a cellular reaction called the unfolded protein response that may lead to cell injury and even death. Protein misfolding is also seen in cells exposed to stress, such as heat, and when proteins are damaged by enzymes (such as Ca2+-responsive enzymes) and free radicals.

  26. B. mitochondrial damage: Mitochondria are important targets for virtually all types of injurious agent, including hypoxia & toxins. Mitochondria can be damage by: 1. Increase in cytoplasmic Ca++ 2. Oxidative stress 3. Breakdown of phospholipids by activated phospholipase.

  27. Injury to mitochondria leads to increased permeability of its membrane that result in leakage from the mitochondria of H+ and cytochrome C. The former leads to loss of mitochondrial membrane potential, which is critical for mitochondrial oxidative phosphorylation thus leading to ATP depletion. Leakage of cytochrome C can trigger apoptotic cell death

  28. . Mitochondrial dysfunction in cell injury.

  29. C. INFLUX OF INTRACELLULAR CALCIUM AND LOSS OF CALCIUM HOMEOSTASIS Calcium ions are important mediators of cell injury. Cytosolic free calcium is maintained at extremely low concentrations(<0.1 μmol) compared with extracellular levels of 1.3 mmol, and most intracellular calcium is sequestered in mitochondria and endoplasmic reticulum. Such gradients are modulated by membrane-associated, energy-dependent Ca2+, Mg2+-ATPases. Ischemia and certain toxins cause an early increase in cytosolic calcium concentration, owing to the net influx of Ca2+ across the plasma membrane and the release of Ca2+ from mitochondria and endoplasmic reticulum .

  30. Sustained rises in intracellular Ca2+ subsequently result from nonspecific increases in membrane permeability. Increased Ca2+ in turn activates a number of enzymes, with potential deleterious cellular effects. The enzymes known to be activated by calcium include ATPases,phospholipases, proteases and endonucleases . Increased intracellular Ca2+ levels also result in increased mitochondrial permeability and the induction of apoptosis. * Although cell injury often results in increased intracellular calcium and this in turn mediates a variety of deleterious effects, including cell death, loss of calcium homeostasis is not always a proximal event in irreversible cell injury

  31. Sources and consequences of increased cytosolic calcium in cell injury

  32. D-ACCUMULATION OF OXYGEN-DERIVED FREE RADICALS (OXIDATIVE STRESS) Cells generate energy by reducing molecular oxygen to water. During this process, small amounts of partially reduced reactive oxygen forms are produced as an unavoidable byproduct of mitochondrial respiration. Some of these forms are free radicals that can damage lipids, proteins, and nucleic acids. They are referred to as reactive oxygen species. Cells have defense systems to prevent injury caused by these products. An imbalance between free radical-generating and radical scavenging systems results in oxidative stress, a condition that has been associated with the cell injury seen in many pathologic conditions. Free radical–mediated damage contributes to such varied processes as chemical and radiation injury, ischemia-reperfusion injury (induced by restoration of blood flow in ischemic tissue), cellular aging, and microbial killing by phagocytes.

  33. Free radicals may be initiated within cells in several ways: a-Absorption of radiant energy (e.g., ultraviolet light, x-rays). For example, ionizing radiation can hydrolyze water into hydroxyl (OH) and hydrogen (H) free radicals. b-Enzymatic metabolism of exogenous chemicals or drugs (e.g., carbon tetrachloride [CCl4] can generate CCl3). c-The reduction-oxidation reactions that occur during normal metabolic processes. d-Transition metals such as iron and copper donate or accept free electrons during intracellular reactions and catalyze free radical formation, as in the Fenton (H2O2 + Fe2+ <---- Fe3+ + OH + OH-). e-Nitric oxide (NO), an important chemical mediator generated by endothelial cells, macrophages, neurons, and other cell types can act as a free radical and can also be converted to highly reactive peroxynitrite anion (ONOO-) as well as NO2 and NO3-. The effects of these reactive species are wide-ranging , but three reactions are particularly relevant to cell injury: 1-Lipid peroxidation of membranes. 2-Oxidative modification of proteins. 3-Lesions in DNA. *In many pathologic processes, the final effects induced by free radicals depend on the net balance between free radical formation and termination

  34. E. DEFECTS IN MEMBRANE PERMEABILITY Early loss of selective membrane permeability leading ultimately to overt membrane damage is a consistent feature of most forms of cell injury. Membrane damage may affect the mitochondria, the plasma membrane, and other cellular membranes. In ischemic cells, membrane defects may be the result of a series of events involving ATP depletion and calcium-modulated activation of phospholipases. The plasma membrane, however, can also be damaged directly by certain bacterial toxins, viral proteins, lytic complement components, and a variety of physical and chemical agents.

  35. :Several biochemical mechanisms may contribute to membrane :damage 2-Loss of membrane phospholipids1- Mitochondrial dysfunction 3- Cytoskeletal abnormalities. 4- Reactive oxygen species. 5- Lipid breakdown products

  36. Reperfusion injury It has been noted that many of the effects of ischemic injury seem to occur not during the ischemic episode itself but when perfusion (blood flow) is reestablished to an area of tissue that has been ischemic. The re-flowed blood encounters cells with already disrupted membrane from the initial ischemia. Among other consequences of this membrane dysfunction that is particularly important in this context is impairment of calcium transport out of the cell and from organelles (such as mitochondria). The rise of intracellular Ca ++ causes activation of oxygen-dependent free radicals that lead eventually to cell damage. The necrosis of reperfusion injury appears to be of the apoptotic rather than of the conventional type

  37. Factors influencing the severity of the cell injury:Types, duration & severity of the injurious agent.Types of the affected cells: cells differ in their susceptibility to the effects of the injurious agent; for e.g.

  38. Reversible cell injury Ischemia is one of the commonest causes of the cell injury. - Ischemia leads to hypoxia. This in turn result in reduction of the available ATP. -The cell, as a result of hypoxia, switches over to anaerobic glycolysis (in an attempt to maintain energy supply). -The glycogen stores get depleted with an increase in the concentration of intracellular lactic acid(a byproduct of anaerobic glycolysis). -Lack of` ATP results in failure of sodium-potassium pump with resultant influx of sodium into the cell & this is accompanied by water (to insure isotonicity). The result is swelling of the cell. Additionally the lowering of intracellular pH (by lactic acid) interferes with the proper functions of enzymes

  39. Examples of reversible cell injury 1. Acute cellular swelling (hydropic change, hydropic degeneration) This is an early change in many examples of reversible cell injury. The extra-fluid may be seen by light microscopy as in increase in size of the cell with pallor of the cytoplasm (cloudy swelling). With further water accumulation clear vacuoles are created within the cytoplasm (vacuolar degeneration) 2. Fatty change

  40. Irreversible cell injury Mitochondrial damage is one of the most reliable early features of this type of injury. In irreversible injury the damage to cell membrane is most severe than in reversible injury, resulting in leakage of the cellular constitutes outside their normal confines. This also results in liberation and activation of lysosomal enzymes (proteinases, nucleases etc.), which are also normally bounded by membranes. These liberated and activated enzymes digest both cytoplasmic and nuclear components (autolysis). The end result is total cell necrosis, which is the morphological expression of cell death.

  41. Cell Death There are two modes of cell death 1. Necrosis 2. Apoptosis Necrosis Necrosis is defined as the morphological changes that follow cell death in a living tissue or organ. Necrosis results from the degrading action of enzymes on irreversibly damaged cells with denaturation of cellular proteins. In necrosis, there are cytoplasmic as well as nuclear changes.

  42. Cytoplasmic changes In the hematoxylin-eosin stain (H&C), the hematoxylin stains acidic materials (including the nucleus) blue where as eosin stains alkaline materials (including the cytoplasm) pink. The necrotic cell is more eosinophilic than viable cells :(i.e. more intensely pinkish) this is due to 1. Loss of cytoplasmic RNA (RNA is acidic so stains with hematoxylin bluish) i.e. loss of basophilia. 2. Increase binding of eosin (which is responsible for the pinkish color of the cytoplasm) to the denaturated proteins. The cell may have more glassy homogeneous appearance than normal cells; this is due to loss of the glycogen particles (which normally gives a granular appearance to cytoplasm)

  43. Nuclear changes The earliest change is chromatin clumping, which is followed by one of two changes; 1. The nucleus may shrinks & transformed into small wrinkled basophilic mass (pyknosis), with time there is progressive disintegration of the chromatin with subsequent disappearance of the nucleus altogether (karylysis) or 2. The nucleus may break into many; clumps (karyorrhexis). In 1 to 2 days, the nucleus in a dead cell completely disappears

  44. Types of cell necrosis 1. Coagulation (coagulative) necrosis. 2. Liquefaction (liquefactive) necrosis. 3. Fat necrosis 4. Caseous necrosis. 5. Gangrenous necrosis. 6. Fibrinoid necrosis. 1. Coagulation necrosis Results from sudden sever ischemia in such organs as the heart ,kidney etc. Microscopically; the fine structural details of the affected tissue (and cells) are lost but their outlines are maintained. -The nucleus is lost • The cytoplasm is converted into homogeneous deeply eosinophilic and structureless material. • - The basic tissue architecture is preserved for at least several -days

  45. 2. Liquefaction necrosis Seen in two situations 1. Brain infarcts i.e. ischemic destruction of brain tissue. 2. Abscesses i.e. suppurative bacterial infection Liquefaction necrosis is characterized by complete digestion of dead cells by enzymes and thus the necrotic area is eventually liquefied i.e. converted into a cyst filled with debris and fluid

  46. 3. Fat necrosis This is a specific pattern of cell death seen in adipose tissue due to action of lipases. It is most commonly seen in acute pancreatitis. The released fatty acids from necrotic cells, complex with calcium to create calcium soaps. These are seen grossly as chalky white deposits. Fat necrosis can also be induced by mechanical trauma as in female breast (traumatic fat necrosis)

  47. 4. Caseous necrosis (caseation) This combines the features of coagulative & liquefactive necrosis. It is encountered principally in the center of tuberculous granuloma. The body is response to tuberculous infection is a specific form of chronic inflammation referred to as granulomatous inflammation. The morphological unit of this called granuloma. Grossly; the caseous material is soft , friable, whitish- gray cheesy material Microscopically; the area is surrounded by granulomatous inflammation. It has distinctive amorphous granular pinkish debris

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