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Crimson College of Technology (Pokhara University)

HOST AND VIRUS INTERACTION

Health & Medicine
1 of 37
UNIT II HOST AND VIRUS INTERACTION rambahadurkhadka00@gmail. com
INTRODUCTION  An appreciation of the potential adverse outcomes of infection in the individual cell is key to understanding the impact of viral infection in complex tissue and indeed the whole host animal.  Cellular tropism of viruses is determined by the presence of appropriate cellular receptors and frequently, cell-type specific transmission factor.  Viruses typically encode genes that modulate host-cell function for their own benefit and of course the host has elaborate innate defense to restrict viral functions.  Thus the viral and cellular factor that influence the outcome of infection are often in delicate balance and easily shifted one way or the other.
STAGES OF VIRAL INFECTION :-  Primary infection occurs when virus enters the body through different portals.  The viruses then enter into the blood streams and targeted to different organs, the stage is known as viremia.  After entry into the predilected site they start their replication and transmitted to different organ and may shed outside through body secretions, the condition is referred as secondary infection (infection of brain tissue by encephalitis virus and liver by the hepatitis virus).
1. Primary infection-  Infection of cells in the general location where virus enters. Common for example with cold viruses and Diarrhea causing viruses. Many viruses including HIV initially infect cells in the infected area. 2. Viremia-  Virus enters the blood system and can be detected in the blood stream. Not all viruses do this. Some remain only localized. 3. Secondary infection-  Infection of other organ of cell types by the virus. Many viruses have high affinity for specific organs due to the presence of receptors or specific cell metabolic functions.  Examples are infection of salivary glands by mumps virus, brain tissue by encephalitis virus, and liver tissue by hepatitis virus.
 Virus infection causes a wide variety of potentiality victorious changes in the many different kinds of cells that occur in the animal host.  The disruption of cellular function, the induction of cell death or transformation or the activation of an inappropriate immune response are all potentiality manifested as disease by the infected host.  Although virus induced changes at the cellular, sub-cellular and molecular level are most commonly studied in cultured cells, additional insight has been gained through the use of organ culture, transcription of infected cells and tissues back into experimental animals, and the experiment uses of genetically modified laboratory animal in conjunction with molecular clo9nes of individual viruses.  Many virus-cell interactions are transient and asynchronous, involving intermediate steps on the pathway, each featuring dynamic interactions between different viral and cellular components.
TYPES OF VIRUS-CELL INTERACTION  Viral infection may be Cytocidal or non cytocydal and productive or non- productive that is, not all infection leads to cell death or the production and release of new versions.  How-ever critical changes can occur in virus infected cells regardless of whether the infection is productive or not.  Some of the most important of all non productive virus cell interactions are those associated with persistent infections or latent infections  The term persistent infection simply describes an infection that lasts a long time.  The term latent infection describes an infection that "exists but is not exhibited," i.e., an infection in which infectious virions is not formed.
 In either case, the virus or its genome is maintained indefinitely in the cell, either by the integration of the viral nucleic acid into the host cell DNA or by carriage of the viral nucleic acid in the form of an episome. In these instances, the cell survives, indeed may divide repeatedly.  In some instances such cells never release virions, in others the infection may become productive when induced by an appropriate stimulus.  Persistent or latent infections may also be associated with cell transformation. The various types of interaction that can occur between virus and cell are summarized
1. CYTOCIDAL CHANGES IN VIRUS-INFECTED CELLS  Cytopathic viruses kill the cells in which they replicate.  When a monolayer of cultured cells is inoculated with a cytopathic virus, the first round of infection yields progeny virus that spreads through the medium to infect adjacent as well as distant cells in the culture may become infected.  The resulting cell damage is known as a cytopathic effect (CPE).  Cytopathic effect can usually be observed by low-power light microscopy of unstained cell cultures.  The nature of the cytopathic effect is often characteristic of the particular virus involved and is therefore an important preliminary clue in the identification of clinical isolates .  Fixation and staining of infected cell monolayers may reveal further diagnostic details.
Mechanisms of Cell Damage:- 1) Inhibition of Host Cell Nucleic Acid Synthesis 2) Inhibition of Host Cell RNA Transcription 3) Inhibition of Processing of Host Cell mRNAs 4) Inhibition of Host Cell Protein Synthesis 5) Cytopathic Effects of Toxic Viral Proteins 6) Cytopathic Changes Involving Cell Membranes 7) Cell Membrane Fusion and Syncytium Formation (cell fusion)
Mechanisms of Cell Damage
2. NON-CYTOCIDAL CHANGES IN VIRUS-INFECTED CELLS:-  Non-Cytocidal viruses usually don’t kill cell in which they will replicate.  They cause persistent infection, in which infected cell produce and release virions but overall cellular metabolism is little affected.  In many instances the infected cells even continue grow and divided.  This type of virus-cell interaction is found in cells infected in several RNA viruses by A. Effect of Non-Cytocidal Viral Infection on Function of Specialized Cell B. Inclusion Bodies (virus specific intracellular globular masses produced in host during replication) C. Polarity of Viral Infection D. Ultrastructural Changes in Virus-Infected Cells
Immunological outcomes of heterologous viral infections.
PATHOGENEIS OF VIRAL INFECTIONS:- Viral Entry Three requirements must be satisfied to ensure successful infection in an individual host: • Sufficient virus must be available to initiate infection • Cells at the site of infection must be accessible, susceptible, and permissive for the virus • Local host anti-viral defense systems must be absent or initially ineffective. To infect its host, a virus must first enter cells at a body surface. Common sites of entry include the mucosal linings of the Respiratory tract, alimentary tract , and urogenital tracts, skin, congenital, Conjunctiva.
Respiratory Tract  The most common route of viral entry is through the respiratory tract.  The combined absorptive area of the human lung is almost 140 m2.  Humans have a resting ventilation rate of 6 liters of air per minute, which introduces large numbers of foreign particles and aerosolized droplets into the lungs with every breath.  Viruses enter the host through droplets expelled from the nose or mouth of infected persons during talking, coughing or sneezing.  Viruses may enter the respiratory tract in the form of aerosolized droplets expelled by an infected individual by coughing or sneezing, or through contact with saliva from an infected individual.  Larger virus-containing droplets are deposited in the nose, while smaller droplets find their way into the airways or the alveoli.  To infect the respiratory tract successfully, viruses must not be swept away by mucus, neutralized by antibody, or destroyed by alveolar macrophages.
Urogenital Tract  Some viruses enter the urogenital tract as a result of sexual activities.  The urogenital tract is well protected by physical barriers, including mucus and low pH (in the case of the vagina).  Normal sexual activity can result in minute tears or abrasions in the vaginal epithelium or the urethra, allowing viruses to enter.  Some viruses infect the epithelium and produce local lesions (e.g., certain human papillomaviruses, which cause genital warts).  Other viruses gain access to cells in the underlying tissues and infect cells of the immune system (e.g., human immunodeficiency virus type 1), or sensory and autonomic neurons (in the case of herpes simplex viruses).
Eyes  The epithelium covering the exposed part of the sclera and the conjunctivae is the route of entry for several viruses.  Every few seconds the eyelid passes over the sclera, bathing it in secretions that wash away foreign particles.  There is usually little opportunity for viral infection of the eye, unless it is injured by abrasion. Direct inoculation into the eye may occur during ophthalmologic procedures or from environmental contamination (e.g., improperly sanitized swimming pools).  In most cases, replication is localized and results in inflammation of the conjunctiva (conjunctivitis). Systemic spread of the virus from the eye is rare, although it does occur (e.g., paralytic illness after enterovirus 70 conjunctivitis).  Herpesviruses can also infect the cornea at the site of a scratch or other injury. This infection may lead to immune destruction of the cornea and blindness.
Skin  The skin of most animals is an effective barrier against viral infections, as the dead outer layer cannot support viral growth.  Entry through this organ occurs primarily when its integrity is breached by breaks or punctures.  Replication is usually limited to the site of entry because the epidermis is devoid of blood or lymphatic vessels that could provide pathways for further spread.  Other viruses can gain entry to the vascularized dermis through the bites of arthropod vectors such as mosquitoes, mites, ticks, and sandflies.  Even deeper inoculation, into the tissue and muscle below the dermis, can occur by hypodermic needle punctures, body piercing or tattooing, animal bites, or sexual contact when body fluids are mingled through skin abrasions or ulcerations.
Routes of virus entry into the host
Alimentary Tract  The alimentary tract is a common route of infection and dispersal.  Eating, drinking, and some social activities routinely place viruses in the alimentary tract.  It is designed to mix, digest, and absorb food, providing a good opportunity for viruses to encounter a susceptible cell and to interact with cells of the circulatory, lymphatic, and immune systems.  It is an extremely hostile environment for a virus.  The stomach is acidic, the intestine is alkaline, digestive enzymes and bile detergents abound, mucus lines the epithelium, and the lumen surfaces of intestines contain antibodies and phagocytic cells  The hostile environment of the alimentary tract actually facilitates infection by some viruses. For example, reovirus particles are converted by host proteases in the intestinal lumen into infectious subviral particles, the forms that subsequently infect intestinal cells
Viral Spread  Following replication at the site of entry, virus particles can remain localized, or can spread to other tissues .  Local spread of the infection in the epithelium occurs when newly released virus infects adjacent cells.  These infections are usually contained by the physical constraints of the tissue and brought under control by the intrinsic and immune defences.  An infection that spreads beyond the primary site of infection is called disseminated.  If many organs become infected, the infection is described as systemic.
 For an infection to spread beyond the primary site, physical and immune barriers must be breached.  After crossing the epithelium, virus particles reach the basement membrane .  The integrity of that structure may be compromised by epithelial cell destruction and inflammation.  Below the basement membrane are sub-epithelial tissues, where the virus encounters tissue fluids, the lymphatic system, and phagocytes.  All three play significant roles in clearing foreign particles, but also may disseminate infectious virus from the primary site of infection. View of the intestinal wall, showing a typical M cell surrounded by enterocytes
Hematogenous Spread  Viruses that escape from local defenses to produce a disseminated infection often do so by entering the bloodstream (hematogenous spread). Virus particles may enter the blood directly through capillaries, by replicating in endothelial cells, or through inoculation by a vector bite.  viremia = presence of infectious virus particles in the blood. T  hese virions may be free in the blood or contained within infected cells such as lymphocytes Active viremia is produced by virus replication, while passive viremia results when virus particles are introduced into the blood without viral replication at the site of entry (injection of a virus suspension into a vein).  Progeny virions released into the blood after initial replication at the site of entry constitute primary viremia.  secondary viremia =Delayed appearance of a high concentration of infectious virus in the blood is termed secondary viremia.
Neural Spread  Many viruses spread from the primary site of infection by entering local nerve ending.  For certain viruses (e.g., rabies virus and alpha herpesviruses), neuronal spread is the definitive characteristic of their pathogenesis.
Organ Invasion  Once virions enter the blood and are dispersed from the primary site, any subsequent replication requires invasion of new cells and tissues.  Three main types of blood vessel-tissue junctions provide routes of tissue invasion
The Liver, Spleen, Bone Marrow, and Adrenal Glands  These tissues are characterized by the presence of sinusoids lined with macrophages. Such macrophages, known as the reticuloendothelial system, function to filter the blood and remove foreign particles.  They often provide a portal of entry into various tissues.  For example, viruses that infect the liver usually enter from the blood. The presence of virus particles in the blood invariably leads to the infection of Kupffer cells, the macrophages that line the liver sinusoids NOTE:- Tropism Most viruses do not infect all the cells of a host but are restricted to specific cell types of certain organs. The spectrum of tissues infected by a virus is called tropism. For example, an enterotropic virus replicates in the gut, whereas a neurotropic virus replicates in cells of the nervous system. Some viruses are pantropic, infecting and replicating in many cell types and tissues.
HOST RESPONSE TO VIRUS INFECTION:-  The out come of virus infection depends on the virulence of the infecting strain and resistance offered by the host  The mechnism of the host resistance my be of following types :- 1. NON-SPECIFICE RESPONSES (NON-IMMUNOLOGICAL) A. Age B. Hormones C. Malnutrition D. Body Temperature E. Phagocytosis F. Inferferons (ALFA,BETA,GAMMA) 2.IMMUNOLOGICAL RESPONSES A. Abtibody-Mediated Immunity B. Cell-Mediated Immunity (CMI)
1. NON-SPECIFIC RESPONSES:- A. AGE:-  Most of the viral infections tend to be most serious of extrems of life.  Rotaviruses case severe disese only in infants. B. HORMONES:-  Corticostriods administration enhances most viral infections.  Without judgment the use of steriods in the treatment of herpetoconjunctivitis may casues blindnes. C. MALNUTRITION:-  It interferes with the humoral and cell-mediated immune responses therefore it can increase viral infection.
D.BODY TEMPERATURE:-  Most of the viral infections are accompained by fever.  Fever may act as a natural defence mechanism against viral infections as most viruses are inhibited by temperaturea above 39 Deg.c. E.PHAGOCYTOSIS:-  Macrphages phagocytose viruses and are important in clearing viruses from blood-stream.  Polymorphonuclear leucocyte don not play any significant role. F. INTERFERONS:-  IFNs are family of glycoproteins produced by cells on induction by viral or non-viral microbs.  These have antiviral activity by inhabiting protein synthesis. TYPES:- i. IFN-ALFA:- Produced by leucocytes having antiviral activity. ii. IFN-BETA:-Produced by fibroblasts and epithelial cells having antiviral activity. iii. IFN-GAMMA:- Produced by T-Lymphocytes and NK cells having immunoregulatory functions. Alfa and beta produced three enzymes (synthetase,Rnase L and Protein Kinase) and inhibit protein synthesis.
IMMUNOLOGICAL RESPONES TO VIRAL INFECTION:- Viruses in general are good antigens and induce both the ANTIBODY-MEDIATED IMMUITY CELL-MEDIATED IMMUNITY
A. ANTIBODY-MEDIATED IMMUITY  IgG & IgM play a important role in blood and tissues while IgA is more important in mucosal surfaces.  All three antibodies may act in the following ways:- i. Neutralisation of virus which prevents attachment, penetration or subsequent events. ii. Lysis by complement or destruction by phagoctes or killer (K) lymphocytes. iii. Immune opsonisation of virus for phagocytosis and destruction of virus by macrophages. B. CELL-MEDIATED IMMUNITY (CMI)  CMI prevents infection of target organs and promotes recovery from diseases by destroying virus and virus-infected cells.  Mechanisms involved are i. Cytolysis by cytotoxic T-Cels and NK Cells ii. Antibody-Dependent cell mediated cytotoxicity iii. Antibody- Complement-mediated cytotoxicity.
CONCLUSION  The non-specific host defences function early in the encounter with virus to prevent or limit infection while the specific host defences function after infection in recovery immunity to subsequent challenges.  Although the host defence mechanisms involved in a particular viral infection will vary depending on the virus, dose and portal of entry.
THANK YOU

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host and virus interaction

  • 2. INTRODUCTION  An appreciation of the potential adverse outcomes of infection in the individual cell is key to understanding the impact of viral infection in complex tissue and indeed the whole host animal.  Cellular tropism of viruses is determined by the presence of appropriate cellular receptors and frequently, cell-type specific transmission factor.  Viruses typically encode genes that modulate host-cell function for their own benefit and of course the host has elaborate innate defense to restrict viral functions.  Thus the viral and cellular factor that influence the outcome of infection are often in delicate balance and easily shifted one way or the other.
  • 3. STAGES OF VIRAL INFECTION :-  Primary infection occurs when virus enters the body through different portals.  The viruses then enter into the blood streams and targeted to different organs, the stage is known as viremia.  After entry into the predilected site they start their replication and transmitted to different organ and may shed outside through body secretions, the condition is referred as secondary infection (infection of brain tissue by encephalitis virus and liver by the hepatitis virus).
  • 4.
  • 5. 1. Primary infection-  Infection of cells in the general location where virus enters. Common for example with cold viruses and Diarrhea causing viruses. Many viruses including HIV initially infect cells in the infected area. 2. Viremia-  Virus enters the blood system and can be detected in the blood stream. Not all viruses do this. Some remain only localized. 3. Secondary infection-  Infection of other organ of cell types by the virus. Many viruses have high affinity for specific organs due to the presence of receptors or specific cell metabolic functions.  Examples are infection of salivary glands by mumps virus, brain tissue by encephalitis virus, and liver tissue by hepatitis virus.
  • 6.  Virus infection causes a wide variety of potentiality victorious changes in the many different kinds of cells that occur in the animal host.  The disruption of cellular function, the induction of cell death or transformation or the activation of an inappropriate immune response are all potentiality manifested as disease by the infected host.  Although virus induced changes at the cellular, sub-cellular and molecular level are most commonly studied in cultured cells, additional insight has been gained through the use of organ culture, transcription of infected cells and tissues back into experimental animals, and the experiment uses of genetically modified laboratory animal in conjunction with molecular clo9nes of individual viruses.  Many virus-cell interactions are transient and asynchronous, involving intermediate steps on the pathway, each featuring dynamic interactions between different viral and cellular components.
  • 7.
  • 8. TYPES OF VIRUS-CELL INTERACTION  Viral infection may be Cytocidal or non cytocydal and productive or non- productive that is, not all infection leads to cell death or the production and release of new versions.  How-ever critical changes can occur in virus infected cells regardless of whether the infection is productive or not.  Some of the most important of all non productive virus cell interactions are those associated with persistent infections or latent infections  The term persistent infection simply describes an infection that lasts a long time.  The term latent infection describes an infection that "exists but is not exhibited," i.e., an infection in which infectious virions is not formed.
  • 9.
  • 10.  In either case, the virus or its genome is maintained indefinitely in the cell, either by the integration of the viral nucleic acid into the host cell DNA or by carriage of the viral nucleic acid in the form of an episome. In these instances, the cell survives, indeed may divide repeatedly.  In some instances such cells never release virions, in others the infection may become productive when induced by an appropriate stimulus.  Persistent or latent infections may also be associated with cell transformation. The various types of interaction that can occur between virus and cell are summarized
  • 11. 1. CYTOCIDAL CHANGES IN VIRUS-INFECTED CELLS  Cytopathic viruses kill the cells in which they replicate.  When a monolayer of cultured cells is inoculated with a cytopathic virus, the first round of infection yields progeny virus that spreads through the medium to infect adjacent as well as distant cells in the culture may become infected.  The resulting cell damage is known as a cytopathic effect (CPE).  Cytopathic effect can usually be observed by low-power light microscopy of unstained cell cultures.  The nature of the cytopathic effect is often characteristic of the particular virus involved and is therefore an important preliminary clue in the identification of clinical isolates .  Fixation and staining of infected cell monolayers may reveal further diagnostic details.
  • 12. Mechanisms of Cell Damage:- 1) Inhibition of Host Cell Nucleic Acid Synthesis 2) Inhibition of Host Cell RNA Transcription 3) Inhibition of Processing of Host Cell mRNAs 4) Inhibition of Host Cell Protein Synthesis 5) Cytopathic Effects of Toxic Viral Proteins 6) Cytopathic Changes Involving Cell Membranes 7) Cell Membrane Fusion and Syncytium Formation (cell fusion)
  • 14. 2. NON-CYTOCIDAL CHANGES IN VIRUS-INFECTED CELLS:-  Non-Cytocidal viruses usually don’t kill cell in which they will replicate.  They cause persistent infection, in which infected cell produce and release virions but overall cellular metabolism is little affected.  In many instances the infected cells even continue grow and divided.  This type of virus-cell interaction is found in cells infected in several RNA viruses by A. Effect of Non-Cytocidal Viral Infection on Function of Specialized Cell B. Inclusion Bodies (virus specific intracellular globular masses produced in host during replication) C. Polarity of Viral Infection D. Ultrastructural Changes in Virus-Infected Cells
  • 15. Immunological outcomes of heterologous viral infections.
  • 16. PATHOGENEIS OF VIRAL INFECTIONS:- Viral Entry Three requirements must be satisfied to ensure successful infection in an individual host: • Sufficient virus must be available to initiate infection • Cells at the site of infection must be accessible, susceptible, and permissive for the virus • Local host anti-viral defense systems must be absent or initially ineffective. To infect its host, a virus must first enter cells at a body surface. Common sites of entry include the mucosal linings of the Respiratory tract, alimentary tract , and urogenital tracts, skin, congenital, Conjunctiva.
  • 17.
  • 18. Respiratory Tract  The most common route of viral entry is through the respiratory tract.  The combined absorptive area of the human lung is almost 140 m2.  Humans have a resting ventilation rate of 6 liters of air per minute, which introduces large numbers of foreign particles and aerosolized droplets into the lungs with every breath.  Viruses enter the host through droplets expelled from the nose or mouth of infected persons during talking, coughing or sneezing.  Viruses may enter the respiratory tract in the form of aerosolized droplets expelled by an infected individual by coughing or sneezing, or through contact with saliva from an infected individual.  Larger virus-containing droplets are deposited in the nose, while smaller droplets find their way into the airways or the alveoli.  To infect the respiratory tract successfully, viruses must not be swept away by mucus, neutralized by antibody, or destroyed by alveolar macrophages.
  • 19.
  • 20. Urogenital Tract  Some viruses enter the urogenital tract as a result of sexual activities.  The urogenital tract is well protected by physical barriers, including mucus and low pH (in the case of the vagina).  Normal sexual activity can result in minute tears or abrasions in the vaginal epithelium or the urethra, allowing viruses to enter.  Some viruses infect the epithelium and produce local lesions (e.g., certain human papillomaviruses, which cause genital warts).  Other viruses gain access to cells in the underlying tissues and infect cells of the immune system (e.g., human immunodeficiency virus type 1), or sensory and autonomic neurons (in the case of herpes simplex viruses).
  • 21. Eyes  The epithelium covering the exposed part of the sclera and the conjunctivae is the route of entry for several viruses.  Every few seconds the eyelid passes over the sclera, bathing it in secretions that wash away foreign particles.  There is usually little opportunity for viral infection of the eye, unless it is injured by abrasion. Direct inoculation into the eye may occur during ophthalmologic procedures or from environmental contamination (e.g., improperly sanitized swimming pools).  In most cases, replication is localized and results in inflammation of the conjunctiva (conjunctivitis). Systemic spread of the virus from the eye is rare, although it does occur (e.g., paralytic illness after enterovirus 70 conjunctivitis).  Herpesviruses can also infect the cornea at the site of a scratch or other injury. This infection may lead to immune destruction of the cornea and blindness.
  • 22. Skin  The skin of most animals is an effective barrier against viral infections, as the dead outer layer cannot support viral growth.  Entry through this organ occurs primarily when its integrity is breached by breaks or punctures.  Replication is usually limited to the site of entry because the epidermis is devoid of blood or lymphatic vessels that could provide pathways for further spread.  Other viruses can gain entry to the vascularized dermis through the bites of arthropod vectors such as mosquitoes, mites, ticks, and sandflies.  Even deeper inoculation, into the tissue and muscle below the dermis, can occur by hypodermic needle punctures, body piercing or tattooing, animal bites, or sexual contact when body fluids are mingled through skin abrasions or ulcerations.
  • 23. Routes of virus entry into the host
  • 24. Alimentary Tract  The alimentary tract is a common route of infection and dispersal.  Eating, drinking, and some social activities routinely place viruses in the alimentary tract.  It is designed to mix, digest, and absorb food, providing a good opportunity for viruses to encounter a susceptible cell and to interact with cells of the circulatory, lymphatic, and immune systems.  It is an extremely hostile environment for a virus.  The stomach is acidic, the intestine is alkaline, digestive enzymes and bile detergents abound, mucus lines the epithelium, and the lumen surfaces of intestines contain antibodies and phagocytic cells  The hostile environment of the alimentary tract actually facilitates infection by some viruses. For example, reovirus particles are converted by host proteases in the intestinal lumen into infectious subviral particles, the forms that subsequently infect intestinal cells
  • 25. Viral Spread  Following replication at the site of entry, virus particles can remain localized, or can spread to other tissues .  Local spread of the infection in the epithelium occurs when newly released virus infects adjacent cells.  These infections are usually contained by the physical constraints of the tissue and brought under control by the intrinsic and immune defences.  An infection that spreads beyond the primary site of infection is called disseminated.  If many organs become infected, the infection is described as systemic.
  • 26.  For an infection to spread beyond the primary site, physical and immune barriers must be breached.  After crossing the epithelium, virus particles reach the basement membrane .  The integrity of that structure may be compromised by epithelial cell destruction and inflammation.  Below the basement membrane are sub-epithelial tissues, where the virus encounters tissue fluids, the lymphatic system, and phagocytes.  All three play significant roles in clearing foreign particles, but also may disseminate infectious virus from the primary site of infection. View of the intestinal wall, showing a typical M cell surrounded by enterocytes
  • 27. Hematogenous Spread  Viruses that escape from local defenses to produce a disseminated infection often do so by entering the bloodstream (hematogenous spread). Virus particles may enter the blood directly through capillaries, by replicating in endothelial cells, or through inoculation by a vector bite.  viremia = presence of infectious virus particles in the blood. T  hese virions may be free in the blood or contained within infected cells such as lymphocytes Active viremia is produced by virus replication, while passive viremia results when virus particles are introduced into the blood without viral replication at the site of entry (injection of a virus suspension into a vein).  Progeny virions released into the blood after initial replication at the site of entry constitute primary viremia.  secondary viremia =Delayed appearance of a high concentration of infectious virus in the blood is termed secondary viremia.
  • 28. Neural Spread  Many viruses spread from the primary site of infection by entering local nerve ending.  For certain viruses (e.g., rabies virus and alpha herpesviruses), neuronal spread is the definitive characteristic of their pathogenesis.
  • 29. Organ Invasion  Once virions enter the blood and are dispersed from the primary site, any subsequent replication requires invasion of new cells and tissues.  Three main types of blood vessel-tissue junctions provide routes of tissue invasion
  • 30. The Liver, Spleen, Bone Marrow, and Adrenal Glands  These tissues are characterized by the presence of sinusoids lined with macrophages. Such macrophages, known as the reticuloendothelial system, function to filter the blood and remove foreign particles.  They often provide a portal of entry into various tissues.  For example, viruses that infect the liver usually enter from the blood. The presence of virus particles in the blood invariably leads to the infection of Kupffer cells, the macrophages that line the liver sinusoids NOTE:- Tropism Most viruses do not infect all the cells of a host but are restricted to specific cell types of certain organs. The spectrum of tissues infected by a virus is called tropism. For example, an enterotropic virus replicates in the gut, whereas a neurotropic virus replicates in cells of the nervous system. Some viruses are pantropic, infecting and replicating in many cell types and tissues.
  • 31. HOST RESPONSE TO VIRUS INFECTION:-  The out come of virus infection depends on the virulence of the infecting strain and resistance offered by the host  The mechnism of the host resistance my be of following types :- 1. NON-SPECIFICE RESPONSES (NON-IMMUNOLOGICAL) A. Age B. Hormones C. Malnutrition D. Body Temperature E. Phagocytosis F. Inferferons (ALFA,BETA,GAMMA) 2.IMMUNOLOGICAL RESPONSES A. Abtibody-Mediated Immunity B. Cell-Mediated Immunity (CMI)
  • 32. 1. NON-SPECIFIC RESPONSES:- A. AGE:-  Most of the viral infections tend to be most serious of extrems of life.  Rotaviruses case severe disese only in infants. B. HORMONES:-  Corticostriods administration enhances most viral infections.  Without judgment the use of steriods in the treatment of herpetoconjunctivitis may casues blindnes. C. MALNUTRITION:-  It interferes with the humoral and cell-mediated immune responses therefore it can increase viral infection.
  • 33. D.BODY TEMPERATURE:-  Most of the viral infections are accompained by fever.  Fever may act as a natural defence mechanism against viral infections as most viruses are inhibited by temperaturea above 39 Deg.c. E.PHAGOCYTOSIS:-  Macrphages phagocytose viruses and are important in clearing viruses from blood-stream.  Polymorphonuclear leucocyte don not play any significant role. F. INTERFERONS:-  IFNs are family of glycoproteins produced by cells on induction by viral or non-viral microbs.  These have antiviral activity by inhabiting protein synthesis. TYPES:- i. IFN-ALFA:- Produced by leucocytes having antiviral activity. ii. IFN-BETA:-Produced by fibroblasts and epithelial cells having antiviral activity. iii. IFN-GAMMA:- Produced by T-Lymphocytes and NK cells having immunoregulatory functions. Alfa and beta produced three enzymes (synthetase,Rnase L and Protein Kinase) and inhibit protein synthesis.
  • 34. IMMUNOLOGICAL RESPONES TO VIRAL INFECTION:- Viruses in general are good antigens and induce both the ANTIBODY-MEDIATED IMMUITY CELL-MEDIATED IMMUNITY
  • 35. A. ANTIBODY-MEDIATED IMMUITY  IgG & IgM play a important role in blood and tissues while IgA is more important in mucosal surfaces.  All three antibodies may act in the following ways:- i. Neutralisation of virus which prevents attachment, penetration or subsequent events. ii. Lysis by complement or destruction by phagoctes or killer (K) lymphocytes. iii. Immune opsonisation of virus for phagocytosis and destruction of virus by macrophages. B. CELL-MEDIATED IMMUNITY (CMI)  CMI prevents infection of target organs and promotes recovery from diseases by destroying virus and virus-infected cells.  Mechanisms involved are i. Cytolysis by cytotoxic T-Cels and NK Cells ii. Antibody-Dependent cell mediated cytotoxicity iii. Antibody- Complement-mediated cytotoxicity.
  • 36. CONCLUSION  The non-specific host defences function early in the encounter with virus to prevent or limit infection while the specific host defences function after infection in recovery immunity to subsequent challenges.  Although the host defence mechanisms involved in a particular viral infection will vary depending on the virus, dose and portal of entry.

Editor's Notes

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