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-==An Introduction to General Pathology==
+#REDIRECT[[:Category:General Pathology]]
-* The term '''pathology''' is derived from:
-** '''Pathos''', or suffering
-** '''Logos''', or reasoning/logic.
-* Pathology is defined as the study of disease including:
-** '''Aetiology''' - causal factor(s)
-** '''Pathogenesis''' - the development of the disease within the body.
-** '''Lesions''' - the observable structural changes in the tissues and fluids of the body.
-** '''Pathophysiology''' - the functional changes in diseased tissues.
-** '''Sequel''' - the consequences of the disease in the body.
-** '''Remote effects''' - the effect of disease in one tissue on other tissues in the body.
-===Lesions===
-* Lesions are the abnormalities or changes seen in living tissues due to disease.
-* Observed in
-** The live animal
-** Tissues surgically removed from the live animal
-*** Biopsy/ excision
-** Animals soon after death
-*** Necropsy, post-mortem examination.
-====Decription of Lesions====
-* Descriptions of lesions is very important
-* Whole organs, tissues or individual lesions are described under headings such as
-*# Size
-*# Shape
-*# Colour
-*# Weight
-*#* Generally in relation to body weight
-*# Texture and Consistency
-*# Appearance of the cut surface
-*# Contents of hollow organs
-*# Position, relationships and effects on adjacent tissues
-*'''See [[General Pathology - Recognition and Description of Lesions|Recognition and Description of Lesions]]'''
-===Disease===
-====Definition and Type====
-* '''Disease''' is  a definite morbid (illness producing) process, having a characteristic train of symptoms or signs.
-** May affect the whole body or any of its parts.
-** The disease's aetiology, pathology and prognosis may be known or unknown.
-* There are two main categories of disease.
-*# '''Acute'''
-*#* Characterised by sudden onset and short duration.
-*#* The outcome of acute disease may be:
-*#** Death
-*#** Resolution due to host defence response or clinical therapy
-*#** Progression to chronic disease
-*# '''Chronic'''
-*#* Characterised by insidious onset and protracted course.
-*#* The outcome of chronic disease may be:
-*#** Progressive destruction of tissue
-*#*** Compromises funtion and  endangers life,
-*#** The halting of the course of disease, with tissue repair by scarring.
-====Factors Involved in the Development of Disease====
-* There are three factors which conspire with each other to produce disease.
-*# '''The individual animal'''.
-*#* In particular, the animal's nutritional and immune status
-*#** This is modified by:
-*#*** Recent or concurrent disease
-*#*** Previous exposure to the agent(s) responsible
-*# '''The disease-causing agent(s)'''.
-*#* Most do not cause a uniform pattern of disease
-*#** Host defences are important in determining the presentation of the disease.
-*#* An agent's capacity to produce disease depends upon:
-*#** The dose
-*#** The virulence of the agent
-*#* Several agents may be involved.
-*#** Usually one agent debilitates, allowing others to exert a greater effect within the body
-*#* The presence of an agent does not necessarily mean it is the cause of the disease!
-*#* A pathogenic agent may be absent from the tissues, due to:
-*#** Clinical therapy
-*#** Host defence systems
-*# '''Environment''', for example:
-*#* Overcrowding of animals
-*#* Mixing animals from differing origins
-*#** Carriers are allowed to infect susceptible animals.
-*#*** Carriers are animals which harbour the pathogenic agent but do not show signs of disease.
-*#* Changes in management routine
-====Types of Agents Causing Disease====
-# '''Infectious organisms'''
-#* [[Viruses|Viruses]]
-#* [[Bacteria|Bacteria]]
-#* [[Fungi|Fungi]]
-#* [[Parasites|Parasites]]
-# '''Physical'''
-#* Trauma
-#* Pressure
-#* Heat
-#* Cold
-#* Radiation
-# '''Chemical'''
-#* Toxic organic and inorganic substances
-#* Toxins produced by infectious organisms
-# '''Nutritional'''
-#* Deficiencies of vitamins and trace elements
-#* Excess vitamins and trace elements
-# '''Genetic defects'''
-#* There is a very wide range of potential defects.
-#** Some are incompatible with life
-#** Others affect specific systems within the body
-====Aspects of Disease====
-* There are many aspects of a disease that must be considered in order to understand it in full.
-*# '''Incidence'''
-*#* How much of the disease is present?
-*#* Where is the disease found?
-*#* In what species is the disease seen?
-*# '''Aetiology'''
-*#* Causal agent(s)
-*#* Predisposing factors
-*# '''Transmission'''
-*#* How is the disease spread between individuals?
-*#* Is the disease zoonotic?
-*# '''Pathogenesis'''
-*#* How the causal agent(s) exert their effect within the body.
-*# '''Diagnosis'''
-*#* History
-*#* Clinical findings
-*#** Clinical examination
-*#** Clinical pathology
-*#* Biopsy or post-mortem examination
-*# '''Prognosis and Treatment'''
-*# '''Control and Prevention'''
-*#* The ideal situation
-====Post-Mortem Examination====
-* Post-mortem examination (PME) investigates the observable structural changes in the animal.
-* Information relating to the disease withing the body or specific tissue is gained from PME.
-** This includes information on the disease's
-*** Aetiology (cause).
-*** Pathogenesis (development).
-* Several types of changes are encountered at post-mortem examination.
-*# Those due to the '''disease'''
-*#* Lesions
-*# Those occuring '''immediately prior to death'''
-*#* Agonal
-*# Those occuring '''after death'''
-*#* Post-mortem
-====Techniques Involved in Pathological Examination====
-* '''Fluid examination'''
-** E.g. blood, urine, discharges from orifices and so on.
-* '''Cytology'''
-** Examination of cells in smears, aspirates and fluids.
-* '''Necropsy'''
-** Visual examination of the gross changes in the dead body.
-* '''Histopathology'''
-** Microscopic examination of:
-*** Tissues selected from the dead body after necropsy.
-*** Biopsy/excision materials from lesions in the living animal.
-* '''Histochemistry'''
-** Microscopic visualisation of enzymatic activity in tissues.
-* '''Immunological methods'''
-** Specific antibody activity can be detected in tissues and fluids.
-*** Examination of serum can show prior exposure to a particular infectious agent (i.e. specifice antibodies).
-** Specific antigens can be detected in tissues.
-*** When linked to a marking agent (e.g. a fluorescent dye), an antibody can localise its antigen in the tissue.
-* '''Electronmicroscopy'''
-** Electronmicrosopcy shows fine detail of the surfaces or internal structures of cells.
-* '''Bacteriology/ Virology/ Parasitology'''
-** These techniques allow the isolation and identification of pathogenic bacteria, viruses and parasites.
-* '''Toxicology'''
-** Analysis of tissues for particular poisons and toxins.
-==General Pathology - Contents==
-===[[General Pathology - Recognition and Description of Lesions|Recognition and Description of Lesions]]===
-===[[General Pathology - Degenerations and Infiltrations|Degenerations and Infiltrations]]===
-===[[General Pathology - Necrosis|Necrosis]]===
-==Necrosis==
-Necrosis
-The term necrosis means death of cells within the living body.
-Two things happen when necrosis occurs:
-a. further changes can take place in the tissue itself; and
-b. the surrounding unaffected living tissue can react against this necrotic tissue.
-Causes of Necrosis.
-There are three main causes of necrosis:
-. loss of blood supply - tissues depend upon their blood supply to remain alive,
-. non-living agents such as chemicals or physical injuries,
-. living agents such as bacteria, viruses, fungi or parasites.
-. Loss of blood supply
-.A diminished blood supply to a tissue is called ischaemia. This type of necrosis is called
-ischaemic necrosis, also called infarction - defined as necrosis of a portion of tissue due to
-an interruption (usually sudden) in the blood supply to that portion. The effects of
-ischaemia on a tissue will vary according to:
-a. the type of tissue affected - some tissues are more susceptible than others.
-b. the type of cell in the tissue - the general rule is that parenchymatous cells, the
-essential functioning cells, are more susceptible than the stromal supporting cells.
-c. the metabolic activity of the tissue - very active organs i.e. those that work continuously
-are more susceptible.
-d. whether or not there is a good or potential collateral blood supply
-There are three ways in which tissue ischaemia can be brought about
-a. compression of the blood vessel
-from without e.g. too tight a bandage
-will cause tissue ischaemia. A
-common cause of tissue ischaemia is
-strangulation of the intestine by a
-twist upon itself, or a mass such a
-lipoma ( a relatively common growth
-of mature fat tissue ) forms in the
-mesentery, becomes pedunculated (
-attached by a fine band of the
-mesentery) and can encompass a
-portion of intestine. Initially, the
-compression of the mesenteric veins
-will prevent outflow of blood leading
-to congestion and swelling of the
-affected portion. When the arterial
-supply becomes occluded or cannot
-supply sufficient blood to the tissue
-because of pressure in the swollen
-intestine and its vessels, the affected area undergoes an ischaemic necrosis with disastrous
-sequelae of rupture and peritonitis or gangrene and toxaemia due to absorption of toxic
-products of the necrosis and intestinal bacteria.
-b. a narrowing of the lumen e.g. thickening of the wall in arteriosclerosis.
-c. blocking of the lumen of the vessel, important causes are thrombi and emboli. Renal
-vessels are commonly affected. See the effects of emboli in Circulatory Disorders.
-. The action of physical or chemical agents.
-The physical agents include burns, cold, frostbite, X-rays, pressure, and actual pinching or
-crushing of the tissue. The necrosis is direct in the case of burns and indirect in the case of
-crushing or pinching which causes occlusion of the vessels supplying the tissue which will
-undergo necrosis. Chemical agents may be directly caustic or corrosive in action or exert
-their effects when absorbed and metabolised to a more toxic substance.
-. Living agents - their effect is either through their toxic effects on cells or their
-colonisation of the cells.
-Appearance of necrotic lesions
-In a typical necrotic lesion there are three zones.
-. Where the effect of the causal agent is maximal, there is a sphere of necrosis.
-. A little further away, the tissue will be damaged but not yet dead, and so there is a
-zone of degeneration short of death.
-. Still farther away, where the effect of the agent is insufficient to cause death or
-degeneration of cells, we have a zone where the body is reacting to the dead tissue
-Gross and histological features of necrotic tissue.
-. Colour change in the tissue. In contrast to living tissue, dead tissue tends to be paler,
-partly because there is no circulation in dead tissue
-. Consistency (texture) of the tissue. The appearance of the centre of the necrotic lesion
-will vary according to the
-. type of agent responsible and
-. the tissue in which it is acting.
-This appearance may give a clue to the agent responsible, and the types of necrosis
-encountered are based on their gross description
-a. Coagulation necrosis
-Gross: The necrotic lesion will be
-firmer and dryer on the cut surface. The
-gross appearance still resembles
-somewhat the nearby living tissue. It is
-a feature of bacteria which produce
-toxins, infarction, and some foci of
-viral replication.
-Micro: the general architecture of the
-tissue is preserved. Certain changes
-present can be recognised in an ordinary
-H&E section, and are related to loss of
-cellular detail.
-a. the cells may appear somewhat
-larger and their outline may be lost
-b. the cytoplasm appears structureless
-and homogenous.
-c. there are nuclear changes - the most important
-There are three types of nuclear change.
-i. Pyknosis - Greek for dense - is a
-condition in which the normal nuclear
-structure is replaced by a very dense,
-heavily staining, somewhat smaller angular
-mass of chromatin.
-ii. Karyorrhexis - Greek karyon =
-nucleus; rhexis = breaking up. This
-appearance is rather the reverse of the
-above. It appears as though the nucleus has
-exploded rather than condensed in the
-cytoplasm, and irregular-sized bits of dense
-nuclear material are found scattered
-throughout the centre of the cytoplasm.
-iii. Karyolysis - this means dissolution of the nucleus. The nuclear staining with
-haematoxylin becomes fainter and only the ghost outline of the nucleus remains.
-Apoptosis - is a term used to denote the programmed death of scattered single cells in living
-tissues. Unlike necrosis, there is no reaction to the death of the cell. It is thought that some
-cells are programmed to die - a form of cell regulation in a tissue - unless there is a change in
-circumstances in a tissue that require them to continue living. One such circumstance is the
-development of tumours in which cellular regulation is absent. Cellular apoptosis is thought
-to be important in deleting extra cells produced in embryogenesis, in cyclical physiological
-changes in the genital tract of females, in the death of lymphocytes, in graft rejection, and in
-cellular death by the same injurious substances that cause necrosis in higher doses.
-The cells undergoing
-apoptosis lose their
-connections with their
-neighbours and shrink; the
-nucleus becomes pyknotic;
-and the cytoplasm becomes
-eosinophilic. The cell
-breaks up into fragments
-that are engulfed by
-neighbouring cells or local
-macrophages. Their
-remnants can be seen in the
-neighbouring cells’ cytoplasm.
-b. Liquefactive (Colliquative)
-Necrosis.
-Gross: In the brain where there is a lot of
-lipid, the intracellular enzymatic changes
-make it softer and more fluid in nature. This
-is known as 'malacia'. Initially it becomes
-swollen with a gelatinous, sometimes bloodtinged
-appearance due to disruption of the
-blood vessels but later becomes fluid.
-Micro: the microscopic appearance will
-not resemble the nearby living tissue as it
-may have already lost any semblance of the
-nearby living tissue because it is becoming
-a fluid.
-Another type of liquefactive necrosis,
-quite important is pus formation which
-occurs when the organism causing the initial
-necrosis in the tissue, is capable of attracting
-to the necrotic area large numbers of
-neutrophils and also capable of killing them.
-These are the so-called pyogenic bacteria.
-When the neutrophils die they release
-proteolytic enzymes which digest the dead
-tissue and also more incoming neutrophils.
-The liquid formed is called pus, and it is
-composed mainly of the dead and dying
-neutrophils together with the remnants of
-the necrotic tissue cells.
-In favourable cases, the neutrophils may
-eventually kill the organisms, but in most cases
-the organisms persist, all the time producing
-more pus. This produces an expanding
-sphere of pus that is called an abscess. The
-pressure will build up and if near to the skin
-will cause pressure on the overlying skin, and
-when the pressure is sufficient or the surgeon
-lances it, the abscess will burst discharging the
-pus, and hopefully with it the organisms responsible. This is nature’s way of ridding the body
-of an injurious agent.
-Micro: In the case of an
-abscess, the necrotic area will
-show varying stages of
-degeneration of the
-neutrophils, ranging from
-nearly normal neutrophils, to
-pyknosis, karyorrhexis and
-karyolysis, and finally to a
-homogenous structureless
-admixture of remnants staining
-faintly bluish.
-As this sphere of pus is
-forming, there is a host
-inflammatory response directed against it. This is composed of a capsule of fibrous tissue in
-which there are many blood vessels on its inner surface, which transport the vast number of
-neutrophils into the necrotic centre. This is called the 'pyogenic membrane'. In superficial
-abscesses, when the abscess has discharged to the surface, this membrane can be viewed as a
-crater that has a reddish somewhat ragged lining. Where the abscess is deep within an organ
-such as the liver, there is nowhere to discharge to, and the fibrous capsule around the pus is
-markedly thickened. .
-c. Caseation necrosis.
-The necrotic tissue appears grossly like
-cheese. The colour varies from white to
-grey to yellowish. In sheep it appears
-whitish while in cattle there may be a
-yellowish tinge. The fluid content also
-varies giving a dry crumbling consistency
-in some cases to being more like cottage
-cheese in others. It is really a mixture of
-coagulation and liquefactive necrosis,
-and is a feature of necrosis caused by
-some specific organisms.
-Micro: On histological section, there is a
-complete loss of the architecture, the
-necrotic material being purplish in colour
-due to random intermixing of the
-components that stain with haematoxylin
-and eosin i.e. bits of nuclear material
-interspersed with cytoplasmic fragments.
-This type of necrosis is a feature of
-granulomatous (tumour-like
-proliferation of chronic inflammatory
-cells) processes such as tuberculosis in
-some species, as in the ox, pig and sheep.
-The necrotic tissue is not derived
-principally from the organ in which it
-occurs, but from a special type of host
-inflammatory cell - the macrophage -
-which is sent into the tissue in large
-numbers to engulf the organism. The
-organism has defences against the enzymes of the macrophages and is quite willing to
-continue to grow and multiply within these macrophages eventually causing their death. In
-some granulomas, the macrophages will combine together and form giant cells.
-Fungi and parasites also cause granulomas.
-Calcification. In the condition of calcification, calcium salts are deposited within the
-necrotic tissue in an effort to make it more inert. It is seen quite commonly in necrosis in
-cattle and sheep, and is a common feature in lesions which show caseation necrosis, and
-usually indicates a lesion of long standing. Such calcified necrotic tissue can be appreciated
-grossly. The deposits of calcium salts can be palpated and on cutting into the necrotic
-portion, the calcified material may be both felt as a gritty substance and heard by a grating
-sound against the knife.
-The colour is usually chalk-white but may have a yellowish green tinge if the inciting cause
-is a parasite. Parasites attract a large number of eosinophils that are responsible for this
-colour. This type of calcium deposition in necrotic tissue is called dystrophic calcification.
-It is an attempt to make the tissue more inert. It does not result from elevated levels of
-calcium in the blood.
-Micro: In sections stained by H&E, calcium has a
-distinctive dark blue colour. You may also see some
-shattering of the calcium and adjacent tissue due to the
-effect of the microtome knife
-passing through it. It blunts the knife and there may be
-score marks throughout the rest of the section. Difficulty
-sometimes arises in distinguishing calcium from
-bacterial colonies that stain a similar colour. A
-definitive special stain for calcium is to stain the
-section with silver nitrate (the von Kossa method).
-The calcium stains black.
-Sequel to necrosis
-These will vary in relation to the causes of necrosis, but by and large it is important to
-distinguish between dead tissue on the surface of the body and dead tissue in the depths of
-the body; a piece of dead skin as compared with a portion of dead liver.
-Dead tissue on the surface can be shed and is said to slough, whereas dead tissue in the centre
-of the liver cannot naturally be shed from the surface. Something else happens to it. It can
-either be absorbed or replaced by fibrous tissue, or it can be enclosed by fibrous tissue. This
-is part of the process of inflammation - the response of the body to local injury. It is a
-general rule that small areas of necrosis become absorbed and replaced by fibrous tissue
-(scars) while larger areas become encapsulated by fibrous tissue, the necrotic portion
-remaining in the centre. This effectively cuts off any contact with living tissue, and allows
-perhaps further changes to occur within the necrotic portion to make it more inert. The
-encapsulated portion is called a sequestrum. It can be, as mentioned before, be calcified to
-make it more inert.
-When necrosis occurs on an epithelial surface, two things may happen depending upon the
-depth of the necrosis. In a case like 'Foot and Mouth' where the necrosis is confined to the
-middle and outer layers of the epithelium, the remaining underlying germinal layer divides
-and replaces the shed portion. This type of necrosis confined to the epithelium is called an
-erosion. It leaves no scar.
-When the necrosis extends below the basement membrane of the epithelium as might be
-caused by an applied corrosive substance or a burn, the body reacts to this interruption in the
-integrity of the epithelium with an underlying inflammatory reaction attempting to repair the
-deficit by fibrous tissue. This type of necrosis is called ulceration, and the resultant
-contraction of the fibrous tissue leaves a scar.
-Fat necrosis
-This is confined to the fat depots of the body.
-It has a very distinctive appearance grossly: instead
-of the fat being semi- translucent and malleable, it
-shows areas of focal opacity and is very hard in
-consistency. This appearance is due to the
-intracellular fat after the fat cells have died, being
-broken down into fatty acids which combine with
-Ca++, Na+ and K+ ions to forms soaps. These soaps
-are substances foreign to the body and they provoke a
-host inflammatory response. Unlike fat, they do not
-dissolve out in routine preparation of sections,
-These areas of fat necrosis remain indefinitely, may
-show great scarring, and quite often calcify. It occurs
-principally in two ways in the body.
-a. Enzymatic necrosis of fat. This happens when there is a release of pancreatic enzymes
-into the neighbouring mesenteric fat, the release being caused by a damaged pancreas e.g.
-due to an adjacent tumour.
-b. Traumatic necrosis of fat. This is seen in the
-subcutaneous tissue following trauma to the area.
-It is quite common in the brisket of recumbent
-animals due to the prolonged pressure on the area.
-It is worth mentioning here another condition of fat that can also undergo necrosis and
-calcify. This is the so-called lipomatosis that occurs for some unknown reason in Channel
-Island breeds of cattle. In this condition, there are focal areas of increased fat in the
-mesentery. They often surround several loops of the gut, and if they become necrotic, they
-may strangle the enclosed gut with disastrous consequences for the animal.'
-Gangrene
-Gangrene is a post-necrotic change, and in some cases is the ultimate degradation of necrotic
-tissue. The tissue is already dead. There are two main types
-a. Wet gangrene - life threatening
-b. Dry gangrene - non life threatening
-a. Wet gangrene can either be due to:
-a. the agent which initially kills the tissue, further putrefying it, or
-b. the gangrene may be due to dead tissue killed by some other means being invaded by
-organisms which putrefy it.
-In other words the former may be viewed as a primary gangrene, while the latter is
-secondary.
-An example of the former is gangrenous mastitis of the udder of the cow caused by
-Staphylococcus aureus, the organism killing the tissue and then putrefying it.
-An example of secondary gangrene is that which occurs when a portion of gut twists on its
-mesentery or when a lipomatous mass attached to a strand of mesentery, loops around a piece
-of intestine as depicted earlier with regard to tissue ischaemia. The blood supply to the gut is
-cut off, and the affected portion becomes necrotic. Wet gangrene supervenes when the
-putrefactive organisms that are normally present in the gut invade the dead tissue.
-A further cause of wet gangrene is when a ligature around an extremity causes ischaemic
-necrosis of tissue distal to it and the necrotic tissue becomes invaded with putrefactive
-bacteria.
-The gross appearance is of a swollen puffy tissue cold to the touch and with a horrible smell
-owing to the hydrogen sulphide (the smell of rotting flesh) produced in the putrefying tissue.
-In comparison to other dead tissue the zone of inflammation between the dead putrefying
-tissue and living tissue is indistinct. This type of gangrene is overwhelming disastrous for the
-animal unless treated quickly and effectively, as the organisms produce potent toxins either
-themselves or in their breakdown of the dead tissue and the animal rapidly succumbs to
-toxaemia.
-A variation of wet gangrene is that produced by Clostridia organisms such as Clostridium
-chauvei and C. septicum whereby they also form gas. This is called gas gangrene. The
-conditions of Blackleg and Clostridia contamination of wounds produce this type of
-gangrene.
-Dry gangrene, on the other hand, is not life threatening. This is really mummification
-(like an Egyptian mummy) of an extremity, such as the tail, foot or ears of animals. There is
-an occlusion of the blood supply to the extremity. The tissue becomes necrotic.
-Because of air circulating around the extremity, water is drawn out of the tissue, drying and
-preserving it. There is little if any bacterial growth in the tissue and it eventually sloughs off.
-In small animals crushing of the tail may cause this by cutting off the blood supply.
-In large animals, it is seen commonly following a septicaemic condition in which bacteria
-are growing and passing around in the circulation. An embolus blocks the blood supply.
-When seen in calves, the possibility of Salmonellosis must be kept in mind. Other causes
-are frostbite and ergot poisoning.
-Finally, necrosis is irreversible.
-===Causes of Necrosis===
-===Gross and Histological Features of Necrotic Lesions===
-====Coagulation Necrosis====
-====Liquefactive Necrosis====
-====Caseation Necrosis====
-===Sequel to Necrosis===
-====Fat Necrosis====
-====Gangrene====
-==Post Mortem Change==
-===Types of Post Mortem Change===
-====Rigor Mortis====
-====Post Mortem Clotting of Blood====
-====Hypostatic Congestion====
-====Post Mortem Imbibition of Blood====
-====Inbibition of Bile Pigment====
-====Gaseous Distenstion of the Alimentary Tract====
-====Autolysis====
-====Putrefaction====
-==Pigmentation and Calcification==
-===Exogenous Pigmentation===
-====Carbon (Anthracosis)====
-====Pneumoconiosis====
-====Carotenoids====
-===Endogenous Pigmentation===
-====Melanin====
-====Blood Pigments====
-=====Haemoglobin=====
-=====Haemosiderin=====
-=====Haematin=====
-=====Jaundice=====
-=====Haematoidin=====
-=====Porphyria=====
-====Lipofuscin====
-===Mineralisation===
-====Calcification====
-=====Dystrophic=====
-=====Metastatic (Hypercalcaemia)=====
-==Circulatory Disorders==
-===Introduction====
-====Venous Congestion and Hyperaemia====
-====Oedema====
-====Dehydration====
-====Shock====
-====Haemorrhage====
-=====Rhexis=====
-=====Diapedesis=====
-====Haemostasis====
-====Thrombus====
-=====Causes=====
-=====Evolution=====
-=====Embolism=====
-=====Post Mortem Clots=====
-====Disseminated Intravascular Coagulation====
-==Inflammation==
-===Cardinal Signs===
-===Causes===
-===Acute===
-====Introduction====
-====Sequence of Events====
-====Fluids====
-=====Serous=====
-=====Catarrhal=====
-=====Fibrinous=====
-=====Diptheritic=====
-=====Haemorrhagic=====
-=====Purulent=====
-=====Functions of Exudate=====
-=====Sequel to Exudation=====
-====Cells====
-=====Neutrophils=====
-=====Eosinophils=====
-=====Mast Cells=====
-=====Basophils=====
-===Chronic===
-====Introduction====
-====Cells====
-=====Macrophages=====
-=====Lymphocytes=====
-====Types====
-=====Granulomatous Inflammation=====
-=====Granulation Tissue=====
-=====Lymphocytic Inflammation=====
-===Changes in Inflammatory Cells Circulating in Blood===
-====Neutrophilia====
-====Neutopenia====
-====Eosinophilia====
-====Eosinopenia====
-====Lymphocytosis====
-====Lymphopenia====
-====Plasma Cells====
-====Monocytosis====
-===Role of The Lymph Node in Inflammation===
-===Healing and Repair===
-====Introduction====
-====Repair====
-=====Regeneration=====
-=====Replacement=====
-====In Particular Tissues====
-=====Skin=====
-======First Intention======
-======Second Intention======
-=====Bones=====
-=====Respiratory Tract=====
-=====Alimentary Tract=====
-=====Urinary Tract=====
-=====Genital Tract=====
-=====Central Nervous System=====
-==Growth Disorders==
-===Congenital===
-====Causes====
-====Malformations====
-=====Cyclops=====
-=====Bulldog Calf=====
-=====Cleft Palate=====
-=====Cystic Kidney=====
-=====Spina Bifida=====
-=====Hydrocephalus=====
-=====Cerebellar Hypoplasia=====
-=====Skeletal Malformations=====
-=====Skin Defects=====
-=====Muscular Defects=====
-=====Cardiac Defects=====
-=====Sexual Organ Malformation=====
-=====Metabolic Diseases=====
-===Growth Disorders During Life===
-====Atrophy====
-====Hypertrophy====
-====Hypoplasia====
-====Hyperplasia====
-====Metaplasia====
-====Dysplasia====
-====Anaplasia====
-====Neoplasia====
-=====Benign Tumours=====
-=====Malignant Tumours=====
-=====Aetiology of Tumours=====
-=====Phases of Tumour Growth=====
-=====Tumour Classification and Nomenclature=====

Difference between revisions of "General Pathology"

Latest revision as of 12:42, 15 February 2011

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