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Treatment , Prophylaxis and prevention of Influenza

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Title: Treatment , Prophylaxis and prevention of Influenza


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(No Transcript)
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Treatment , Prophylaxis and prevention of
Influenza
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symptom-based therapy(In uncomplicated)
  • acetaminophen for the relief of headache, myalgia
    and fever(use of salicylates should be avoided in
    childrenlt18 years of age association of
    salicylates with Reye's syndrome.
  • Treatment with cough suppressants generally is
    not indicated, although codeine-containing
    compounds may be employed if the cough is
    particularly troublesome.
  • rest and maintain hydration during acute illness

4
Specific Antiviral Agent for influenaza
  • neuraminidase inhibitors Oseltamivir (tamiflu)
  • Zanamivir (relenaz)
  • M2 Inhibitors
  • Amantadine (symmetrol)
  • Rimantadine

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Specific antiviral therapy (continued)
  • If begun within 48 h of the onset of illness,
    reduced the duration of systemic and respiratory
    symptoms of influenza by 50

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Specific antiviral therapy (drug)
  • amantadine and rimantadine for influenza A
  • Zanamivir and oseltamivir for both influenza A
    and influenza B

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Specific antiviral therapy (M2 Inhibitors)
  • amantadine and rimantadine inhibit by
    interfering with the uncoating of virus after
    infection of the cell , interaction with the
    influenza A M2 matrix protein, during which the
    ion channel function of M2 is inhibited.
  • A substitution of a single amino acid at
    critical sites in the M2 protein can result in a
    virus that is resistant to amantadine and
    rimantadine

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Specific antiviral therapy (M2 Inhibitors)
  • 5 to 10 who receive amantadine mild CNS side
    effects, primarily jitteriness , anxiety,
    insomnia, or difficulty in concentrating
    (disappear upon cessation of the drug)( with old
    age , TMP/SMZ , antihistamine anticholnegic ).
  • Rimantadine equally efficacious , less frequent
    CNS side effects than is amantadine.
  • In adults, the usual dose of amantadine
    (cap100mg) or rimantadine is 200 mg/d for 3 to 7
    days.

9
Specific antiviral therapy (M2 Inhibitors)
  • For prophylaxis, the compounds must be
    administered daily for the period at risk (i.e.,
    the peak duration of the outbreak). For therapy,
    amantadine or rimantadine is generally
    administered for 5 to 7 days
  • excreted via the kidney, the dose should be
    reduced to lt100 mg/d in elderly and in renal
    insufficiency (creatinine clearance (Cr,) rate of
    lt50 mL/min)

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Specific antiviral therapy (M2 Inhibitors)
  • Amantadine is not metabolized and is excreted
    almost entirely by the kidney,
  • Rimantadine is extensively metabolized to
    hydroxylated derivatives

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Specific antiviral therapy (neuraminidase
inhibitors )
  • Both zanamivir and oseltamivir act through
    competitive and reversible inhibition of the
    activesite of influenza A and B viral
    neuraminidases (essential for release of the
    virus from infected cell) and have relatively
    little effect on mammalian cell enzymes.
  • zanamivir and oseltamivir are active against
    strains resistant to amantadine and rimantadine.

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Specific antiviral therapy (neuraminidase
inhibitors )
  • Zanamivir(has low oral bioavailability)
    (belister pack 5 mg), inhaled orally 10 mg
    twice a day for 5 days,
  • oseltamivir (cap 75) , orally 75 mg twice a
    day for 5 days,
  • Zanamivir may exacerbate bronchospasm in
    asthmatic patients, and oseltamivirhas been
    associated with nausea and vomiting, ( reduced by
    drug administration with food)

13
Specific antiviral therapy (neuraminidase
inhibitors )
  • Zanamivir and oseltamivir treatment of
    influenza in adults and in children (those gt_7
    years old for zanamivir and those gt 1 year old
    for oseltamivir) who have been symptomatic for
    lt_2 days.
  • Oseltamivir is approved for prophylaxis of
    influenza in individuals gt 13 years of age

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Specific antiviral therapy (continued)
  • Resistant viruses
  • frequently during treatment with amantadine or
    rimantadine and can be transmitted among family
    members.
  • resistance infrequent with zanamivir or
    oseltamivir

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therapy (primary influenza pneumonia )
  • maintaining oxygenation and is most appropriately
    undertaken in an intensive care unit, with
    aggressive respiratory and hemodynamic support as
    needed.
  • When an acute respiratory distress syndrome
    develops, fluids must be administered cautiously,
    with close monitoring of blood gases and
    hemodynamic function

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therapy (bacterial complications )
  • secondary bacterial pneumonia.
  • Gram's staining and culture of respiratory
    secretions, such as sputum or transtracheal
    aspirates.(or empirical antibiotics effective
    against the most common bacterial pathogens (S.
    pneumoniae, S. aureus, and H. influenzae)

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clinical management of human infection with avian
influenzaA (H5N1)
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Summary of treatment modalities for human A(H5N1)
virus infection
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Summary of treatment modalities for human
A(H5N1)virus infection
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Summary of treatment modalities for human
A(H5N1)virus infection
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Summary of treatment modalities for human
A(H5N1)virus infection
22
Summary of treatment modalities for human
A(H5N1)virus infection
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Summary of treatment modalities for human
A(H5N1)virus infection
24
Summary of treatment modalities for human
A(H5N1)virus infection
25
Summary of treatment modalities for human
A(H5N1)virus infection
26
PROPHYLAXIS
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PROPHYLAXIS(vaccines)
  • inactivated influenza vaccines(highly purified)
    influenza A and B viruses circulated during the
    previous influenza season.
  • 50 to 80 protection.
  • reactions. 5 of individuals low-grade fever and
    mild systemic symptoms 8 to 24 h
  • one-third mild redness or tenderness at the
    vaccination site
  • (produced in eggs,)individuals with true
    hypersensitivity to egg products should be
    desensitized or not be vaccinated.

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PROPHYLAXIS(vaccines)
  • 1976 swine influenza vaccine increased
    frequency of Guillain-Barre syndrome, ( since
    1976 generally have not been)
  • during the 19921993 and 19931994 influenza
    seasons, slightly more than one case per million
    among vaccine recipients.

29
PROPHYLAXIS(vaccines)
  • recommends for any individual gt6 months of age
    who is at an increased risk for complications of
    influenza, (Table).
  • inactivated ("killed"), safely to
    immunocompromised patients.
  • not associated with exacerbations of chronic
    nervous-system diseases such as multiple
    sclerosis.
  • administered early in the autumn before influenza
    outbreaks occur and then annually

30
PROPHYLAXIS(vaccines)
  • a live attenuated influenza vaccine intranasal
    spray.
  • by reassortment of currently circulating strains
    of influenza A and B virus with a cold-adapted,
    attenuated master strain.
  • well tolerated and highly efficacious (92
    protective)
  • protection against a circulating influenza virus
    that had drifted antigenically away from the
    vaccine strain.
  • for use in healthy children and adults from 5 to
    49years of age.

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PROPHYLAXIS(vaccines)
  • a live attenuated influenza vaccine 0.5 ml
    sprayer , 5-9 years 1 or 2 doses interanasal
    (4-10 w) , 9-49 1 2 doses interanasal
  • inactivated influenza vaccines IM
  • agegt 13 years0.5 ml 1
  • age 4-12 years0.5 ml 2 (4 w)
  • age 6- 48 m. 0.25 ml 2 (4 w)

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PROPHYLAXIS(Chemoprophylaxis)
  • amantadine or rimantadine, 100 to 200 mg/d, (
    70 to 100 against influenza A infection) .
  • Chemoprophylaxis with oseltamivir (75 mg/d by
    mouth) ( 84 to 89 against influenza A and B).
  • for high-risk individuals who have not received
    influenza vaccine or in a situation where the
    vaccines previously administered are relatively
    ineffective because of antigenic changes in the
    circulating virus.

33
PROPHYLAXIS(Chemoprophylaxis)
  • During an outbreak antiviral chemoprophylaxis
    with inactivated vaccine,(drugs do not interfere
    with an immune response to the vaccine. In fact,
    there is evidence that the protective effects of
    chemoprophylaxis and vaccine may be additive.)
  • concurrent administration of chemoprophylaxis and
    the live attenuated vaccine may interfere with
    the immune response to the vaccine.

34
PROPHYLAXIS(Chemoprophylaxis)
  • Chemoprophylaxis control nosocomial outbreaks
    of influenza.
  • For prophylaxis, administration should be
    instituted promptly when influenza activity is
    detected and must be continued daily for the
    duration of the outbreak.
  • Amantadine and rimantadine are approved for
    prophylaxis in adults and in children(gt1years)
    oseltamivir is approved for prophylaxis in adults
    and in children(gt13 years old) .

35
PROPHYLAXIS(Chemoprophylaxis)
  • Persons at High Risk Who Are Vaccinated After
    Influenza Activity Has Begun(for persons at high
    risk during the time from vaccination until
    immunity has developed. Children aged lt9 years
    who receive influenza vaccine for the first time
    can require 6 weeks of chemoprophylaxis (i.e.,
    chemoprophylaxis for 4 weeks after the first dose
    of vaccine and an additional 2 weeks of
    chemoprophylaxis after the second dose).)

36
PROPHYLAXIS(Chemoprophylaxis)
  • Persons Who Provide Care to Those at High Risk
    (employees of hospitals, clinics, and
    chronic-care facilities household members
    visiting nurses and volunteer workers)
  • Persons Who Have Immune Deficiencies (HIV,
    chiefly those with advanced HIV disease)

37
PROPHYLAXIS(Chemoprophylaxis)
  • When outbreaks occur in institutions,
    chemoprophylaxis should be administered to all
    residents, regardless of whether they received
    influenza vaccinations during the previous fall,
    and should continue for a minimum of 2 weeks. If
    surveillance indicates that new cases continue to
    occur, chemoprophylaxis should be continued until
    approximately 1 week after the end of the outbreak

38
PROPHYLAXIS(Chemoprophylaxis)
  • Chemoprophylaxis also can be offered to
    unvaccinated staff members who provide care to
    persons at high risk.
  • Chemoprophylaxis should be considered for all
    employees, regardless of their vaccination
    status, if the outbreak is suspected to be caused
    by a strain of influenza virus that is not
    well-matched to the vaccine

39
PROPHYLAXIS(Chemoprophylaxis)
  • In addition to nursing homes, chemoprophylaxis
    also can be considered for controlling influenza
    outbreaks in other closed or semiclosed settings
    (e.g., dormitories or other settings in which
    persons live in close proximity).

40
Household Contact Treatment
  • Frequent handwashing
  • N95 masks/eye protection (feasible?)
  • Monitor temperature twice daily for 7 days
  • Quarantine

41
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    ?????? ?? ?????
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    ????? ????
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42
Influenza Prevention What Can We Do?
  • Stay home when sick
  • Respiratory hand hygiene
  • Cover your cough
  • Wash hands and/or
  • use alcohol hand gel
  • Avoid touching eyes, nose, mouth
  • Implement social distancing measures
  • Masks?
  • Pandemic preparedness planning

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Health Care Worker Surveillance
  • Record temperature twice daily

Prophylaxis
Normal
Abnormal Symptoms
Remove from workplace
Evaluate for influenza
Treatment
45
Infection control considerations /Isolation
facilities
  • appropriate precaution measures
  • wear eye protection, gowns, gloves and
    particulate respirators that are at least as
    effective as the NIOSH-certified N95, EU FFP2 or
    equivalent
  • an airborne precaution room (mechanically or
    naturally ventilated rooms with at least 12 air
    exchanges/hour and safe airflow), in a single
    well-ventilated room, or in a negative pressure
    room when available.

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Special infection control considerations during
ventilatory support therapy
  • endotracheal intubation, as well as possibly NPPV
    and oxygen therapy, were risk factors for SARS
    nosocomial transmission, although inconsistent
    use of PPE is a key confounding variable in such
    studies

48
Special infection control considerations during
ventilatory support therapy
  • supplemental oxygen via mask dispersion of
    potentially infectious aerosols
  • Oxygen masks with an expiratory port and HEPA
    filter will reduce aerosol production

49
Special infection control considerations during
ventilatory support therapy
  • HEPA filters should be attached to the expiratory
    ports of ventilators, and a closed tracheal
    suctioning system used for aspiration of
    respiratory secretions to reduce generation and
    spread of infectious aerosols.

50
Special infection control considerations during
ventilatory support therapy
  • To minimize the risk of nosocomial infection, it
    is important to maintain adequate medical ward
    ventilation during application of oxygen therapy
    or NPPV. If NPPV is to be used, a closed system
    with a head helmet and an expiratory port HEPA
    filter is recommended whenever possible

51
CONTROL
52
VACCINATION
CONTROL
DEPOPULATIO
QURANTINE
53
Transmission of AI virus A/H5N1 to humans
  • From infected animals to humans
  • contact with respiratory secretions, faeces,
    contaminated feathers, blood from infected birds.
  • Environmental contamination
  • Raw food consumption (?)
  • From a patient to health care
  • personnel/family members

54
Asias particularities Live Animal Markets
55
AI Transmission issues
  • Need to better understand the kind of close
    contacts with poultry that pose a risk to public
    health.
  • Clear need to improve biosecurity and hygiene at
    live animal markets

56
Control of animal outbreaks
  • Stamping out policies
  • Destruction of infected flocks and surrounding
    flocks.
  • Strengthening disease surveillance
  • Delay of 3-6 months before restocking
  • Vaccination
  • Need for biosecurity capabilities
  • Implications for trade

57
Benefits of fit testing
  • Study 25 volunteers, 21 models of N-95
    respirators
  • Without fit testing, 95 of the tests had up to
    33 leakage
  • With fit testing, 95 of the tests had no more
    than 4 leakage

58
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59
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60
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  • ???? ???? ?? ??? ??????? (MP AI )

61
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    N99 - N-95 ) ????? - ???? - ???? - ) ??????
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62
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63
REFERENCES
  • Treanor J. Influenza Virus. In Mandell, Douglas,
    and Bennett's Principles and Practice of
    Infectious diseases. 6th ed. New York
    Elsevier/Churchill Livingstone 2005chap 162
  • Kasper,HARRISONS Principles of Internal
    Medicine 16th ed.2005 chap.171
  • Clinical management of human infection with avian
    influenza A (H5N1) virus ,Updated advice 15
    August 2007 ,wold health organization
  • Prevention and Control of Influenza
    Recommendations of the Advisory Committee on
    Immunization Practices (ACIP) , Morbidity and
    Mortality Weekly Report , July 28, 2006 / Vol. 55
    / No. RR-10, department of health and human
    services Centers for Disease Control and
    Prevention
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