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Hepatitis C nonA, nonB, Hepatitis

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Some will experience anorexia, malaise, and abdominal pain. Jaundice occurs in a small percentage of patients ... Transmission = aersolized rodent excreta = inhaled ... – PowerPoint PPT presentation

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Title: Hepatitis C nonA, nonB, Hepatitis


1
Hepatitis C ( non-A, non-B, Hepatitis)
  • Hepacivirus Hepatitis Virus C
  • Enveloped, positive-sense RNA
  • Six major serotypes
  • Clinical Progression
  • Initially most patients are asymptomatic
    (subclinical)
  • Only slight elevation of liver enzymes
  • Some will experience anorexia, malaise, and
    abdominal pain
  • Jaundice occurs in a small percentage of patients
  • Pathologically the patient has chronic active
    hepatitis
  • Incubation period 6-7 weeks seroconversion
    8-9 weeks
  • This will ultimately progress to chronic liver
    disease
  • 70-90 will develop chronic disease
  • With time, many of these patients will develop
    cirrhosis
  • 5-25 of these will develop hepatocellular
    carcinoma

2
Hepatitis C Diagnosis and Epidemiology
  • Diagnosis
  • Serological detection of Anti-HVC antibodies
  • Antibodies only indicate exposure, but do not
    stage the disease - EIA
  • Antibodies titers tend to be low
  • Nucleic acid detection
  • Detects circulating HVC- RNA
  • Uses RT-PCR methods converts viral RNA to DNA
  • Epidemiology
  • Reservoir humans throughout the world
  • 170 million chronic carriers worldwide
  • Transmission Person-to-Person, direct/indirect,
    blood-body fluids
  • Most common cause of post-transfusion hepatitis
  • Mortality
  • 8000 10,000 death/year in U.S from end-stage
    liver disease
  • High Risk Groups
  • IV drug users, hemophiliacs, blood transfusion
    recipients, sex, health care workers

3
BunyaViruses - Characteristics
  • spherical, enveloped, negative sense, segmented,
    single-stranded RNA
  • three strands of negative sense RNA
  • two envelope glycoprteins no matrix protein
  • genomes associated with the RNA dependent RNA
    polymerase ( L protein)
  • replicated in the cytoplasm
  • most are Arthropod Borne Viruses
  • Clinical Diseases
  • Hanatavirus Pulmonary Syndrome
  • Hemorrhagic Fever
  • California Encephalitis
  • LaCrosse Encephalitis

4
BunyaViruses Clinical Diseases
  • Hantavirus Pulmomary Syndrome
  • prodrome of fever and muscle aches followed by
    interstitial pulmonary edema, respiratory
    failure, and death
  • Encephalitis
  • sudden onset of fever, headache, lethargy,
    vomiting
  • seizues occur in 50 of patients with
    encephalitis
  • Hemorrhagic Fever
  • petechial hemorrhage, ecchymosis, epistaxis,
    hematemesis, melena, bleed of the gums

5
BunyaVirus Encephalities
  • Symptoms classical encephalitis
  • Acute onset of severe bifrontal headache and
    fever ( 38 -40C)
  • Some vomiting, lethary, and convulsions
  • Death from seizures lt 1 fatality rate
  • CaliforniaEncephalitis Virus Complx
  • LaCross Virus an Othobunyavirus
  • Major cause of encephalitis and aseptic
    meningitis in children in the upper midwest
  • Reservoir small mammals
  • Squirrels, chipmunks, rabbits
  • Transmission animal-to-human, indirect,
    arthropod-borne, mosquitoes
  • Mostly Aedes triseriatus ( oviposits in tree
    holes)

6
BunyaVirus Hemorrhagic Fevers
  • Many in the world
  • None in U.S.
  • High Mortality

7
HantaVirus Pulmonary Syndrome
  • Etiological Agent
  • HantaVirus Sin Nombre Virus ( a Bunyavirus)
  • Symptoms
  • Acute onset of fever, headache, and myalgia
  • Followed by rapidly progressive pulmonary edema
  • Patient dies from respiratory compromise
  • No signs of hemorrhage
  • Pathogenesis
  • Virus infects the endothelial cells and
    macrophages of the lung, heart, spleen, and lymph
    nodes
  • Essence of disease is functional impairment of
    vascular endothelium
  • Epidemiology
  • Reservoir deer mouse (Peromysus maniculatus)
  • Transmission aersolized rodent excreta
    inhaled
  • Disease is not common, but has a 30 mortality
    rate

8
Retroviruses - Characteristics
  • enveloped, positive sense, RNA viruses ( 80 -
    120nm)
  • particles carry two identical copies of
    positive-stranded RNA
  • genome is not infectious does not encode for a
    polymerase
  • three genes which encode polyproteins
  • gag group specific antigen on capsid
  • pol polymerase, protease, integrase
  • env envelope glycoproteins proteolytic
    cleavage of this polyprotein produces the
    individual envelope glcoproteins
  • LTR sequences encode promotors and enhanaces
    assocatiaed with transcription
  • envelope conatains two glycoproteins
  • gp 41 and gp 120 both cleaved from the env
    polyprotein gp160
  • gp 120 establishes tissue trophism and
    antigenicity also subject to antigenic drift
  • gp 41 promotes cell - to - cell fusion

9
RetroVirus - Characteristics
  • cone-shaped core (Lentivirinae) carries several
    enzymes
  • RNA dependent DNA polymerase (reverse
    transcriptase) 10 - 50 copies
  • integrase promotes integration(recombination) of
    viral genone into cell DNA
  • t-RNAs serve as primers for the action of
    reverse transcriptase
  • the viral DNA copy becomes a cellular gene
    through integration into the host cells
    chromosomes
  • Subfamilies of Retroviruses
  • Oncornavirinae HTLV-1, HTLV-2
  • Lentivirinae HIV -1, HIV -2

10
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11
RetroVirus Viral Cycle
  • Adsorption
  • gp 120 binds the virus to cells prossessing CD4
    receptors this establishes the tissue(cell)
    trophism
  • T- helper cells
  • macrophages, dentritic cells, and microglial
    cells
  • accessory receptor (transmembrane G - protein)
    also defines the trophism
  • Penetration
  • the adsorption process brings the gp41 into
    contact with the host cell membrane which the
    promotes the fusion of the virus with the cell
  • some retroviruses enter by endocytosis and do not
    untilize gp41

12
RetroVirus Viral Cycle
  • Transcription and Replication
  • when genome is released into the cytoplasm, the
    t-RNA acts to facilitate the synthesis of a
    negative sense DNA through the action of reverse
    transcriptase
  • the RT, then acts as a ribonuclease and digests
    the positive RNA strand
  • then the negative sense DNA is used as the
    template for the positive sense complementary DNA
    strand double stranded DNA
  • the DNA which results is circular DNA is longer
    than the original RNA
  • double stranded cDNA is delivered to the nucleus
  • DNA is then spliced into the host chromosome
    through the action of viral integrase once
    integrated the viral DNA is transcribed as a
    cellular gene
  • using host cell DNA dependent RNA polymerase II
  • replication of viral genome occurs via
    transcription of the integrated viral DNA to RNA
    replicas since virus acts as a cellular gene,
    this process depends upon the cells ability to
    read LTR and use the enhancer/promotors
  • other products of this transcription include m
    -RNAs for the gag, pol, and env polyproteins

13
RetroVirus Virus Cycle
  • Accessory Gene Products
  • tat/rev
  • nef
  • vif/vpu
  • Assembly
  • viral glycoproteins are cleaved from the
    polyproteins( gag, pol, env) glycosalated, and
    processed by the endoplasmic reticulum and Golgi
    then incorporated into the host cell membrane
  • viral genome replicas, together with t-RNA, viral
    protease, and other enzyme products bind to the
    cell membrane in areas expressing the envelope
    glycoproteins
  • Release
  • the virus is released from the host cell via
    budding
  • acquires its glycoprotein envelope
  • once the virus exits the cell, it is not
    infectious until the viral protease carried in
    the particle cleaves the gag and gag-pol
    polyproteins this intraviral cleavage releases
    the reverse transcriptase and forms the virion
    core
  • many anti-AIDS drugs target the viral protease

14
RetroViruses
  • Viral Pathogenesis/Cytopathology Fig 61-8
  • virus primarily infects the CD 4 cells including
    the cells of macrophage lineage monocytes,
    macrophages, dendritic cells of skin, microglial
    cells
  • the local tissue macrophage is the initial site
    of viral infection/replication
  • this results in persistent low level productive
    infection with virus being shed into the blood
    and body fluids
  • gt viral load with viremia mononucleosis-like
    symptoms
  • monocytes and macrophages are persistently
    infected and continually seed virus into the
    circulation major reservoir for virus
    distribution
  • initial CD 4 T-cell infection occurs in the lymph
    nodes
  • lytic infection of T-cells
  • synctia formation with cells expressing larges
    amounts of CD 4 antigen
  • CD 4 and fusin chemokine receptors required to
    establish this phase
  • some people lack chemokine receptors and are
    immune to AIDS
  • genetic or constitutional immnity lt 2 of human
    population
  • late disease involves lymph node changes, and
    death of CD 4 T-Cells
  • this is immunosupresson with not T-cells (or T dh)

15
RetroViruses - Pathogenesis
  • Additional Points about HIV Cytopathology
  • 1. Since cells of the monocyte-macrophage lineage
    circulate throughout the body, they play a
    significant role in the spread of the virus
  • 2. HIV induces several cytopathic effects in CD 4
    T-cells which lead to their death.
  • accumulation of circular non-integrated DNA,
    changes in cell membrane permeability, syncytia
    formation, and apoptosis(programed death)
  • 3. Macrophages do not exhibit significant
    cytolysis because they express fewer CD 4
    receptors cytolysis occurs most readily in cells
    expressing the greatest amount of CD -4 receptors
  • 4. expression of the nef protein is essential
    for the progression to the state called AIDS
  • 5. CD 8 T-cells also play a role in the
    progression of AIDS

16
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17
Lentivirus Acquired Immunodeficiency
  • Acquired Immunodeficiency Syndrome (AIDS) phases
    of AIDS
  • asymptomatic - initially the viral load in low
    and infection occurs without symptoms
  • symptoms of early infection may resemble
    influenza or mononucleosis
  • lymphadenopathy may accompany or follow(persist)
    this stage
  • asymptomatic with chronic lymadenopathy
  • virus is replicating within the lymph nodes
    during this phase
  • during this stage ARC may occur\
  • lymphadenopathy with fever, weight loss, and
    malaise
  • mild opportunistic infections, diarrhea, night
    sweat, fatigue
  • gradually deterioration of the immune response
  • indicated by repeated opportunistic infections
    (Table 61-5)
  • such infection parallels the decline in CD 4
    T-cells to lt 450/dl
  • complete immunosupression or full-blown AIDS
  • occurs when T-cells decline to 200/dl or less
  • virus load in high at this point high levels of
    virus and p24 in blood

18
AIDS - Diagnosis
  • Symptoms of Immunosuppression repeated
    opportunistic infections
  • Laboratory Diagnosis Table 61-6
  • Antigen detection detection of p24 viral
    antigen, reverse transcriptiase, or viral RNA is
    indicative of recent infection
  • Serology detects presence of antibody against
    viral glycoprotein antigens ELISA, Western Blott
  • serology does not detect early infection only
    after 6 - 8 weeks of infection does antibody
    appear
  • Culture not routinely performed only
    epidemiologically important
  • Epidemiology
  • Reservoir
  • Modes of Transmission
  • Rick Groups
  • Control
  • Education
  • Screening Table 61-6

19
Deltaretrovirus Human Lymphotrophic Viruses
  • Leukemia Viruses HTLV -1
  • Acute T-cell lymphocytic leukemia in Adults (
    ATLL)
  • Fatal within one year of diagnosis
  • Neoplasia of the CD 4 (mature T-cells)
  • long latency of 30 - 50 years
  • not a cytolytic infection, but infected cells
    exhibit growth changes which are not associated
    with oncogenes
  • malignant cells are pleomorphoric with biloulated
    nuclei flower cells
  • elevated WBC with lymphocytosis ( T- cells) and
    skin lesions
  • transmitted by person -to - person, blood and
    blood fluids
  • direct sexual,
  • blood transfusion, IV. Drugs, etc.

20
Hepatitis Viruses
  • Classsification
  • Picornavirus Hepatitis Virus A
  • Hepatitis Virus A
  • Short Incubation Hepatitis 15 -60 days (avg 30
    days)
  • Unlike on picornaviruses, HVA is not cytolytic
    and is released by exoctyosis
  • HVA adsorbs to receptors on liver cells
    (heptacytes) and Kupffers cells
  • No apparent cytopathological effects persistent
    infection
  • Liver pathology is due to the action of natural
    killer cells and cytotoxic T-cells which lyse the
    virally infected cells
  • Jaundice usually accompanies the appearance of
    virus specific antibody
  • Immunity due to virus specific antibody is life
    long
  • Flavivirus Hepatitis Virus C
  • Hepatitis Virus C
  • Incubation period of 14 -180 day(avg 7 - 21 days)
  • Basis for 90 of NANB hepatitis
  • Generally establishes persistent, non-lytic
    infection, leading to chronic disease
  • Transmitted parenterally(transfusion) and sexually

21
Coronaviruses - Characteristics
  • Classification
  • Positive sense RNA
  • Encodes a RNA dependent RNA polymerase (L)
  • Enveloped
  • Glycoproteins E2 functions a both VAP and fusion
    protein
  • Other glycoproteins

22
Coronaviruses - Diseases
  • Acute rhinitis
  • Common cold second most common cause of acute
    rhinitis 15-20 of cases
  • Replicates best in cell of the upper respiratory
    tract which function at 33-35 C
  • Viral Cycle
  • Typical positive sense RNA,enveloped virus cycle
    except that the positive sense RNA buds into the
    Endoplasmic Reticulum, acquires it envelope, and
    is released from the cell by exocytosis
  • Recovery
  • Antibody synthesis bring resolution to symptoms,
    but the immunity is short lived because of little
    IgA in the respiratory tissues
  • Diagnosis
  • Four fold increase in specific serum IgG not
    routinely performed
  • Prevention
  • Prevent respiratory droplet transmission
  • No vaccine

23
Caliciviruses- Caliciviridae
  • Classification
  • Positive sense RNA
  • Much like picornaviruses 27 nm
  • Non-enveloped
  • Human Disease
  • Viral gastroenteritis
  • Diarrhea, vomiting, variable fever, non-bloody
    stool
  • Etiological agent is Norwalk Virus ( genus
    Norovius)
  • Infects the intestinal brush border giving rise
    to a non-absorptive diarrhea

24
Caliciviruses
  • Viral Cycle
  • Cycle is the same as picornavirus cycle
  • Diagnosis
  • Virus or viral antigen can be easily detected in
    the stool using RIA or Elisa
  • Epidemiology
  • P-P, indirect, fecal oral, mode of transmission
  • Source are food, water, or shellfish
  • 60 of all nonbacterial gastroenteritis involves
    Norwalk virus( esp in epidemics)
  • 3 of gastroenteritis from day care facilities
  • Prevention
  • Interrupt fecal-oral transmission
  • Chlorinate water, etc
  • No vaccine

25
Picornavirus- Aphthovirus
  • Foot and Mouth Disease Virus
  • Positive sense RNA, 24 nm,
  • Non-enveloped, 7 serotypes
  • Disease
  • Foot and Mouth Disease
  • Human
  • Fever, salivation, vesiculation of mucous
    membranes
  • Vesicles on palms, soles, fingers, toes
  • Cattle
  • Viremia leads to excretion of virus in urine
  • Vesicles in mouth and on feet which rupture and
    release active virus
  • Mortality is low
  • But sick cattle do not thrive, protein synthesis
    decreases, they loose weight, and milk production
    decreases significantly

26
Aphthovirus Foot and Mouth Disease
  • Epidemiology Mode of Transmission
  • Animal to person, direct contact
  • Animal to person, ingestion of infected meat
  • Animal to animal, urine contaminated materials
  • Animal to animal, vesicular fluids for mouth and
    feet
  • Concerns
  • Virus survives for long periods outside of host
  • Virus is resistant to inactivation
  • Disease is highly contagious
  • Control
  • Destroy and burn (incinerate) infected animals
  • Vaccines current vaccines provide only short
    term immunity
  • New Vaccines using recombinant DNA technology
    are more promising, but are not perfected and not
    widely available

27
Prions - Characteristics
  • Classification
  • Unconventional, non-microbial agents
  • They are not viruses
  • They are not bacteria
  • Chemically, they are protease resistant,
    hydrophobic glycoproteins having no detectable
    nucleic acid component
  • Filterable - lt 100 nm
  • Modified host protein
  • Resistant to inactivation by heat, chemicals, and
    radiation

28
Prions - Diseases
  • Diseases spongiform encephalopathies
  • Human
  • Creutzfeldt-Jakob Diseae
  • Bovine Spongiform Encephalopathy mad cow
    disease
  • Sheep
  • Scrapie the original prion disease
  • Cattle
  • Bovine Spongiform Encephalopathy
  • CJD progressive chronic dementia, ataxia, and
    myoclonus
  • Death in 5 12 months

29
Prion Diseases
  • Pathogenesis hypothesis
  • Normal human cells process a cell surface
    protein, cellular prion protein, PrPc
  • Abnormal prion protein, scrapie prion protein,
    PrPsc, binds to the PrPc on human cells causing
    the cellular protein to change into the abnormal
    type which is shed from the cell and accumulates
    as amyloid-like plaques.
  • Since the cell looses this protein, it replaces
    the PrPc, which is again changed by the PrPsc
    Cycle repeats itself
  • Genetics PrPc is encoded by a single cellular
    gene. The changes in this gene are not completely
    understood, by appear to involve a single
    point-mutation

30
Prion Epidemiology
  • Scrapie was the original prion protein
  • It developed in infected sheep
  • Transmission correlated with the ingestion of
    sheep brains or material with contains sheep
    brains
  • Cattle fed grain containing dried sheep brain
    protein develop bovine spongioform
    encephalopathy aka mad cow disease
  • Humans who consume sheep brains or nervous system
    tissue from infected cattle develop CJD
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