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Rabies Poliomyelitis Prion Disease

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Title: Rabies Poliomyelitis Prion Disease


1
RabiesPoliomyelitisPrion Disease
  • Nani Kurniani, dr., SpS(K)
  • Dept. of Neurology
  • Hasan Sadikin Hospital
  • Bandung

2
Introduction
Rabies
  • Is a zoonosis ? encephalitis
  • Infect mammals (dogs, bats, wild carnivores)
  • Public Health problem
  • Etiology Lyssavirus 4 serotypes
  • family rhabdoviridae
  • Preventable
  • Curable?

3
Introduction
Rabies
  • 100 mortality
  • Death 25,000 people/year
  • Post exposure prophylaxis 4million people/year
  • 90 live in developing countries
  • The risk of contracting rabies from a bite wound
    is 5-80
  • depend on incidence of rabies in endemic species
    or other terrestrial animals in the region

4
Pathogenesis
Rabies
  • The virus is believed to be capable of infecting
    all warm-blooded creatures
  • Almost all cases of human rabies occur due to the
    bite of an infected animal
  • Other possible route of transmission
  • Aerosol
  • Person-to-person corneal transplantation

5
Pathogenesis
Rabies
  • Route of infection
  • Virus in the saliva of infected animals
  • The bite
  • Inoculation in local tissue
  • Transmission of the virus to the CNS
  • Axonal transport
  • Direct transmission without prior local
    replication
  • Initial local replication followed by transmission

6
Pathogenesis
Rabies
  • Route of infection
  • Rate of transmission 8 20 (up to100) mm/day
  • Dorsal root ganglia ? spinal cord ? the brain
  • Subsequent widespread infection to limbic system,
    hippocampus, brainstem and cerebellum
  • Centrifugal spread back to the peripheral sites ?
    salivary glands, corneal cells ? transmission to
    other person
  • At end stage, virtually all organs are involved

7
Clinical
Rabies
  • History
  • History of an animal bite is given ? suspicion
    of rabies!
  • In any suspected cases, identify the following
  • Nature of the interaction with the animal (eg,
    provoked attack or unexpected)
  • Strange animal behavior (eg, nocturnal animal out
    during the daytime)
  • Vaccination status of the animal for rabies
  • Patients usually come when the sign of
    encephalitis has been present ? difficult to
    obtain anamnesis
  • Rabies progresses over 7-14 days
  • mean time between initial presentation and death
    16.2 days

8
Clinical
Rabies
  • Prodrome
  • Patients have presented to Emergency Departments
    with nonspecific fever and pharyngitis
  • Most prodromes last from 2-10 days
  • Initial symptoms of pain or paresthesias at the
    site of bite or scratch begin during the prodrome
  • ? The only symptoms
  • Fever, headache, and anorexia may also be present

9
Clinical
Rabies
  • Neurologic stage (2-7 days)
  • Aphasia
  • Incoordination
  • Paresis
  • Paralysis
  • Mental status changes
  • Hyperactivity

10
Clinical
Rabies
  • Late symptoms
  • Hypotension
  • Coma
  • Disseminated intravascular coagulation (DIC)
  • Cardiac arrhythmias
  • Cardiac arrest
  • Fatality

11
Clinical
Rabies
  • Physical findings
  • High fever with rapidly progressive encephalitis
  • Myoclonus
  • Increased lacrimation
  • Hypersalivation
  • Agitation
  • Anxiety

12
Clinical Presentation
Rabies
  • 2 forms of rabies furious and paralytic
  • Both forms progress to paralysis of pharyngeal
    and respiratory muscles, seizures, and coma with
    death in 1-3 weeks
  • Most common in humans furious form
  • Also common in cats
  • Many animals, including bats, exhibit dumb rabies
    (paralytic form)

13
Diagnostics
Rabies
  • Definitive Brain biopsy
  • In suspected human cases
  • skin biopsy from the nape of the neck
  • smear of corneal epithelial cells (less
    preferable)
  • Rise in specific neutralizing antibodies by rapid
    fluorescent focus inhibition test (RFFIT)
  • often not documented in true rabies cases (have
    died before the 2nd test can be done)
  • more useful to ascertain serostatus in immunized
    animals and humans
  • Viral culture saliva, CSF, and brain

14
Treatment
Rabies
  • For the human patients
  • Thorough cleaning of all bite and scratch wounds
  • soap and water
  • and/or 2 benzalkonium chloride
  • or povidone/iodine solution for at least 10
    minutes
  • Administer human rabies immune globulin (20
    IU/kg)
  • as much of the dose as possible infiltrated in
    and around the wound (if wound location allows)
  • the rest INTRAMUSCULARLY in the gluteal region
  • Equine rabies immunoglobulin may be available ?
    beware of serum sickness and anaphylaxis!

15
Treatment
Rabies
  • For the human patients
  • Wound care as needed, debridement, antibiotic
    administration if needed
  • Measures to prevent bacterial infection when
    warranted also are indicated
  • Check tetanus status ? Tetanus prophylaxis if
    indicated
  • Decision regarding postexposure prophylaxis

16
Treatment
Rabies
  • For the suspected animals
  • Determine rabies immune status of the biting
    animal
  • Determine the nature of the interaction
  • Uncommon animal behavior
  • Provoked attacks are less likely due to rabies
  • Quarantine, etc

17
Vaccine
Rabies
  • Available vaccines
  • human diploid cell vaccine (HDCV) ? for I.D.
  • rabies vaccine adsorbed (RVA) ? I.M.
  • Purified chick embryo cell vaccine ? I.M.
  • Immunity lasting approximately 2 years

18
Prevention
Rabies
  • Prophylaxis is recommended for any routine
    contact with animals at risk.
  • Intact skin contact with urine, blood, or feces
    of an animal has not been shown to constitute
    exposure, except in bats
  • High risk groups
  • Veterinarian
  • Rabies diagnostic lab. staff
  • Animal handlers
  • Wildlife officers
  • Any person who lives in (or travel to) endemic
    area

19
Prevention
Rabies
  • Human rabies immune globulin and vaccine are
    recommended for bites and exposures
  • regardless of the period between exposure and
    treatment
  • unless the individual is previously vaccinated
    and rabies antibodies can be detected
  • Postexposure prophylaxis
  • Dosage 1mL IM
  • in deltoid or upper outer thigh in infants.
  • The 5-dose schedule is as follows
  • day 0
  • day 3
  • day 7
  • day 14
  • day 28

20
Prevention
Rabies
  • Factors to be considered before PEP
  • Is it an open wound?
  • Nature of bites
  • provoked bites are less likely to require
    prophylaxis
  • Presence of rabies in the locality
  • History of vaccination
  • Bats?
  • PEP is recommended in any contact with bats
  • Even in the absence of a bite or scratch

21
Prevention
Rabies
  • Rabies control
  • Notification of cases and destruction of animals
    with signs or bitten by suspected rabid animals
  • Quarantine pets that have bitten people
  • Mass immunization
  • Pets registration

22
Poliomyelitis
23
Introduction
Poliomyelitis
  • Enteroviral infection
  • genus enterovirus, family picornaviridae
  • 3 types
  • Multiplication in GI tract, but are particularly
    neurotropic
  • 4 different forms of manifestation
  • inapparent infection (90-95)
  • abortive poliomyelitis
  • nonparalytic poliomyelitis
  • paralytic poliomyelitis

24
Introduction
Poliomyelitis
  • Aggressive immunization programs ? significant ?
    of worldwide prevalence
  • Indonesia??
  • Mortality more frequently in paralytic form ?
    associated with complications such as respiratory
    failure

25
Clinical Presentation
Poliomyelitis
  • Inapparent infection and abortive polio
  • Nonspecific symptoms, usually resolve within a
    few days (less than 5 days)
  • Fever
  • Headache
  • Nausea
  • Vomiting
  • Abdominal pain
  • Oropharyngeal hyperemia
  • Normal neurological examination

26
Clinical Presentation
Poliomyelitis
  • Nonparalytic poliomyelitis
  • Symptoms described above
  • AND
  • Nuchal rigidity
  • More severe headache
  • Back and lower extremity pain
  • Meningitis with lymphocytic pleocytosis (usually)

27
Clinical Presentation
Poliomyelitis
  • Paralytic poliomyelitis
  • Compromise of the motor neurons may be localized
    or widespread
  • Frequent finding asymmetric loss of muscle
    function
  • involvement of major muscle groups
  • Muscle atrophy several weeks later
  • Recovery may be complete, partial, or absent
  • May involve spinal muscles only
  • in more severe form, bulbar involvement

28
Clinical Presentation
Poliomyelitis
  • Postpoliomyelitis syndrome
  • weakness or fatigue involving groups of muscles
    that were initially affected
  • May last long

29
Diagnostics
Poliomyelitis
  • Viral cultures from CSF, stool, and throat
  • Acute and convalescent serum for antibody
    concentrations against the 3 polioviruses.
  • Confirms the diagnosis if
  • IgG titers increase 4 folds
  • Positive IgM titer during the acute stage

30
Treatment
Poliomyelitis
  • Medical Care
  • No antivirals are effective
  • Treatment is MAINLY supportive
  • Analgetics for headache/pain
  • Laxative for fecal impaction
  • Mechanical ventilation
  • For patients with bulbar paralysis

31
Treatment
Poliomyelitis
  • Tracheostomy if needed
  • Catheterization if needed
  • Physical therapy (in paralytic form)
  • Frequent mobilization to avoid development of
    chronic decubitus ulcerations
  • Active and passive motion exercises during the
    convalescent stage

32
Prevention
Poliomyelitis
  • Oral attenuated poliovirus vaccine
  • Has been used since early 1960s
  • Major disadvantage vaccine-associated paralytic
    poliomyelitis (VAPP)
  • Although attenuated, the virus may occasionally
    become neurotropic ? wild-type virus infection
  • Schedule
  • 2, 4, and 6 months of age
  • PLUS a booster at age 4 years
  • A new monovalent oral poliovirus type 1 vaccine
    (mOPV1) was introduced in India in April 2005
  • Targeted to eliminate some of the last poliovirus
    reservoirs

33
Prognosis
Poliomyelitis
  • Bulbar paralytic poliomyelitis
  • is associated with the highest rate of
    complications
  • mortality rate is as high as 60
  • Spinal poliomyelitis less fatal
  • Inapparent or abortive poliomyelitis recover
    without significant sequelae

34
Prion-related diseases
35
Introduction
Prion
  • Large group of related neurodegenerative
    conditions
  • Affect both animals and humans
  • Includes
  • Creutzfeldt-Jakob disease (CJD) ? human
  • Gerstmann-Sträussler-Scheinker (GSS) ? human
  • Bovine spongiform encephalopathy (BSE, or "mad
    cow disease") ? cattle
  • Chronic wasting disease (CWD) ? mule deer and elk
  • Scrapie ? sheep

36
Introduction
Prion
  • Prion protein
  • abnormal conformation of a host-encoded
    glycoprotein
  • can be inherited
  • can be transmitted
  • can infect normal surroundings
  • Long incubation periods
  • Once clinical symptoms begin ? rapidly
    progressive
  • All prion diseases are fatal
  • No effective form of treatment currently

37
Introduction
Prion
  • 1st description of scrapie ? over 250 years ago
  • Manifestation
  • Hyperexcitability
  • Itching
  • Ataxia
  • Paralysis ? death
  • First transmission was demonstrated in 1943
    within a population of Scottish sheep that was
    accidentally inoculated against a common virus
    using a formalin extract of lymphoid tissue from
    an animal with scrapie

38
Pathophysiology
Prion
  • Unifying feature
  • Similar neuronal loss, gliosis, and
    characteristic spongiform change in the gray
    matter of the CNS
  • Amyloid plaques in many of these conditions
  • In 10 of patients with CJD amyloid in the
    cerebellum or in the cerebral hemispheres
  • In all cases of GSS multicentric cerebellar
    plaques
  • Different immunoreactivity with amyloid plaque in
    Alzheimer disease

39
Route of Transmission
Prion
  • Route of transmission is not clear yet
  • Lymphoid organs are believed to be involved in
    the early stages of prion diseases
  • Hematogenic spread of prions to the CNS is also
    suggested
  • Three cases of vCJD infection associated with
    blood transfusion have also been observed
  • Other studies have implicated the distinct CD11c
    dendritic cell population in prion neuroinvasion
  • Prions can also reach the brain via the
    parasympathetic vagus nerve

40
Epidemiology
Prion
  • Mortality/morbidity
  • Relentlessly progressive and invariably lead to
    death
  • Mean duration of illness
  • sporadic CJD 8 months
  • vCJD 14 months
  • Familial CJD 26 months
  • GSS 60 months

41
Epidemiology
Prion
  • Sex
  • No sex preponderance
  • Mean age of onset
  • Sporadic CJD 62 years
  • vCJD 28 years
  • Familial CJD, GSS 45-49 years

42
Clinical Presentation
Prion
  • (sporadic) Creutzfeldt-Jakob disease
  • Rapidly progressive multifocal neurological
    dysfunction
  • Myoclonic jerks involving either the entire body
    or a limb
  • Spontaneous or precipitated by auditory or
    tactile stimuli
  • Cerebellar dysfunction also occurs.
  • Global severe cognitive impairment in terminal
    stage
  • Death in about 8 months.
  • Definite, probable and possible CJD

43
Diagnostics
Prion
  • Initial workup laboratory tests as for dementia
  • Rule out other conditions
  • toxic and/or metabolic condition that can cause
    dementia
  • paraneoplastic syndrome
  • Imaging Studies
  • MRI is the most important
  • PET
  • Contrast CT-scan of the chest, abdomen, pelvis to
    rule out malignancy
  • EEG
  • Characteristic finding periodic or
    pseudoperiodic paroxysms of sharp waves or spikes
    on a slow background

44
Diagnostics
Prion
  • Lumbar puncture (LP) in all suspected cases
  • Check the opening pressure
  • cell count, protein, glucose, bacterial cultures,
    viral cultures, VDRL, cryptococcal antigen, and
    acid-fast bacilli (AFB)
  • CSF findings
  • typically normal in sporadic CJD
  • CSF protein may be elevated slightly (never gt100
    mg/dL)
  • Patognomonic 14-3-3 protein
  • Brain biopsy

45
Treatment
Prion
  • Medical Care
  • Discontinue any medication that could impair
    memory or cause confusion
  • Therapeutic interventions are under current
    development
  • Consultations
  • Neurologist
  • Infectious disease specialist
  • Diet No dietary restrictions are necessary
  • Activity Activity is unrestricted

46
Prevention
Prion
  • Prion diseases may spread by iatrogenic means
  • ? not to reuse EEG and/or electromyography (EMG)
    needles, surgical instruments, and other tools
    that have been exposed to a patient with prion
    disease
  • Prion agent is remarkably resistant to
    inactivation ? routine sterilization procedures,
    such as autoclaving, are ineffective

47
Prognosis
Prion
  • The prionoses are rapidly progressive
  • Median survival duration (time from diagnosis to
    death)
  • 8 months in sporadic CJD
  • 60 months in GSS
  • Patients with familial prion-related disease tend
    to have a longer course than those with sporadic
    disease

48
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