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Immunodominance and Severe Schistosomiasis Mansoni

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Title: Immunodominance and Severe Schistosomiasis Mansoni


1
Collaborative Course on Infectious
Diseases January 2008
LECTURE 2 Immunodominance and Severe
Schistosomiasis Mansoni
Eduardo Finger ascklepius_at_gmail.com
Harvard School of Public Health Faculdade de
Ciências Médicas da Santa Casa de São Paulo
Brazil Studies Program, DRCLAS, Harvard
University
2
Schistosomiasis mansoni
Eduardo Finger Santa Casa SP 2008
3
Objectives
  • Acquaint students with a basic knowledge of
    schistosomiasis mansoni
  • Illustrate the experience of a few countries in
    trying to deal with schistosomiasis
  • Discuss what can be learned from these examples
    and how that applies to the project

4
  • Schistosomiasis
  • Second most prevalent tropical parasitic disease
    in the world (behind Malaria only)
  • Etiologic agent Schistosoma sp
  • 600 million people at risk in 74 countries
  • 200.000.000 people infected
  • 150.000.000 oligosymptomatic
  • 20.000.000 severe disease
  • Between 200.000 and 800.000 deaths/year

Disease watch n?4 (Nature reviews microbiology,
January 2004)
5
Preferred definitive host of Schistosome sp. in
the wild
6
Geographic distribution of schistosomiasis
WHO archives (2002) WHO Technical Report Series,
No.830, 1993
7
Spread of S. mansoni followed slave trade routes
8
Schistosomiasis route of spread inside Brazil
Memórias do Instituto Oswaldo CruzFundação
Oswaldo Cruz, FiocruzISSN 1678-8060Vol. 99,
Num. s1, 2004, pp. 13-19
9
S.mansoni life cycle
10
Infection
11
Skin penetration by S. mansoni
5min
12
Adult worm habitat
13
Destination of S. mansoni eggs
14
Liver pathology associated with schistosomiasis
  • Morbidity and mortality in schistosomiasis are
    due to granulomas formed around parasite eggs

Pipe-stem fibrosis in the liver
15
Polar forms of chronic schistosomiasis mansoni
  • Intestinal
  • Well tolerated, can last years without
    significant harm to host
  • Low morbidity and mortality
  • Hepatosplenic
  • Important inflammation and fibrosis in portal
    spaces
  • Extensive liver fibrosis produces portal
    hypertension, splenomegaly, ascites,
    portal-systemic shunting and gastrointestinal
    bleeding
  • High morbidity and mortality

16
Clinical presentation of severe schistosomiasis
Portal hypertension
Hepatosplenic shunt
Esophageal varices
Hemorrhages
17
Treatment and control
  • Treatment praziquantel and oxamniquine
  • Reinfection rate is very high.
  • Vaccine strategy not expected to be available
    soon
  • Control strategy massive populational screening
    and treatment. Increase access to treated water.

18
Programs to control schistosomiasis
  • Four pillars
  • Mass chemotherapy (WHO guidelines)
  • Molluscicides (chemical and/or biological)
  • Sanitation (water and sewer treatment)
  • Education
  • Other factor
  • Urbanization

19
Control of Schistosomiasis 4 different
experiences
20
Prevalence of schistosomiasis following PECE
21
Conclusions from the PECE
  • no method is able, in an isolated way, to control
    schistosomiasis and every control program should
    consider the need of multidisciplinary
    application of existing methods
  • the main methods for long term control of
    infection are the implementation of basic
    sanitation conditions, potable water supply, as
    well as sanitary education and community
    participation
  • specific treatment in endemic areas associated to
    intermediary hosts control in "epidemiological
    important" foci is extremely relevant regarding
    short term morbidity control, though not
    sufficient to interrupt disease transmission
  • although schistosomiasis control, in a country
    like Brazil, with great vectors dissemination and
    population mobilization, is a difficult process,
    it is possible through intensification,
    adjustment, and continuity of programs in long
    term
  • it is necessary to develop a critical analysis of
    schistosomiasis control experience in Brazil, in
    order to redirect the program in an effective
    way, aiming to achieve only residual levels of
    infection for the next 20 or 30 years or, even
    better, its full control.
  • Cienc. Cult. vol.55 no.1 São Paulo Jan./Mar 2003
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