1. Schistosomiasis Li Qian
Department of Infectious Diseases, Huashan Hospital, Fudan University

2. Topics Definition The Pathogen Epidemiology Etiology and Life Cycle
The topics include Definition, The Pathogen, Epidemiology, Etiology and Life Cycle, Pathobiology, Clinical manifestations, Diagnosis and Treatment.
Definition
The Pathogen
Epidemiology
Etiology and Life Cycle
Pathobiology
Clinical manifestations
Diagnosis
Treatment

3. DEFINITION
Schistosomiasis is one of the most important parasitic diseases of humans and is a global public health problem in the developing world.
Schistosomiasis is one of the most important parasitic diseases of humans and is a global public health problem in the developing world.

4. DEFINITION
The disease is caused by trematodes of the genus Schistosoma, which cause periportal fibrosis and liver cirrhosis owing to deposition of eggs in the small portal venules.
Schistosoma mansoni and Schistosoma japonicum lead to liver disease.
The disease is caused by trematodes of the genus Schistosoma, which cause periportal fibrosis and liver cirrhosis owing to deposition of eggs in the small portal venules.
Schistosoma mansoni and Schistosoma japonicum lead to liver disease.

5. History
Schistosomiasis is known as bilharzia or bilharziosis in many countries, after German physician Theodor Bilharz, who first described the cause of urinary schistosomiasis in 1851.
The first doctor who described the entire disease cycle was Pirajá da Silva in 1908.
It was a common cause of death for Ancient Egyptians in the Greco-Roman Period.

6. The Pathogen
Five major species of Schistosoma affect humans
Five major species of Schistosoma affect humans: S. mansoni, S. haematobium, S. japonicum, S. intercalatum, and S. mekongi.
Other Schistosoma species that occasionally infect humans include S. bovis, S. mattheei, and some avian schistosomes.

7. The Pathogen
These species differ biologically from one another. however, the species of Schistosoma that infect humans share some common factors.
These species differ biologically from one another and in their geographic distribution and the type of disease that they produce.
The schistosomes are digenetic parasitic trematodes. Although they are morphologically distinct, the species of Schistosoma that infect humans share some common factors.

8. The Pathogen
The large male (0.6 to 2.2 cm × 2 to 4 mm) has a ventral gynecophoric canal in which the female (1.2 to 2.6 cm × 1 to 2 mm) is held during copulation.
The large male (0.6 to 2.2 cm × 2 to 4 mm) has a ventral gynecophoric canal in which the female (1.2 to 2.6 cm × 1 to 2 mm) is held during copulation.

9. EPIDEMIOLOGY
Schistosomiasis occurs mainly in rural agricultural and periurban areas.
Infection with S. mansoni is found in parts of South America, Africa, and the Middle East.
Infection with S. japonicum is found in the Far East, mostly China and the Philippines.
In China, 0.67% of the population may be infected, according to CDC statistical report at 2008.
Schistosomiasis occurs mainly in rural agricultural and periurban areas.

10. EPIDEMIOLOGY Infection sources Mode of transmission
Infection with S. mansoni is found in parts of South America, Africa, and the Middle East.
Infection with S. japonicum is found in the Far East, mostly China and the Philippines.
In China, 0.67% of the population may be infected, according to CDC statistical report at 2008.
Infection sources
Mode of transmission
Susceptible population

11. Infection sources Patients reservoir host- animal reservoirs
cows,pigs(S. japonicum)
Rodents, monkeys, and baboons have been found infected in nature, but the role of these animals as reservoirs does not seem to be epidemiologically important.

12. mode of transmission human exposure to cercariae.
3 links in parasitic epidemiology
The endemicity of schistosomiasis depends on the urban disposal of urine (S. haematobium) and feces (S. mansoni, S. japonicum, S. intercalatum, S. mekongi),
the presence of suitable snail hosts
human exposure to cercariae.
The endemicity of schistosomiasis depends on the urban disposal of urine (S. haematobium) and feces (S. mansoni, S. japonicum, S. intercalatum, S. mekongi), the presence of suitable snail hosts, and human exposure to cercariae.

13. Snail
The freshwater snail intermediate hosts are Biomphalaria spp in Africa and Biomphalaria glabrata (Australorbis) and Tropicarbis in South America and the West Indies.
The freshwater snail intermediate hosts are Biomphalaria spp in Africa and Biomphalaria glabrata (Australorbis) and Tropicarbis in South America and the West Indies.

14. Susceptible population
Humans are susceptible to the Schistosoma.
young adults
Summer and autumn

15. Schistosoma life cycle
6 weeks
Adult worms live in the mesenteric veins (S. mansoni, S. japonicum, S. mekongi, and S. intercalatum) or in the venous plexus around the lower ends of the ureters and the urinary bladder (S. haematobium).
In these sites, they start their sexual reproduction by releasing eggs.
Eggs of S. haematobium may be trapped in the intestines and bladder and may escape to the intestinal or bladder lumen.
Following asexual multiplication in the snail, the development of cercariae, the infective forms for humans, takes 4 to 7 weeks.
After leaving the snails, the cercariae can survive in fresh water for almost 72 hours.
When penetration of the skin in the human host occurs, the cercariae lose their tails and change into schistosomula.
Schistosomula migrate to the lungs and, in about 6 weeks, mature to adult worms and descend to their final habitat.
Viable eggs can be seen in excretions (i.e., stool or urine) 5 to 9 weeks after cercarial penetration.
5 to 9 weeks
72 hours
4 to 7 weeks

16. Schistosome life cycle
After being excreted with feces or urine into fresh water, the eggs hatch and release ciliated motile miracidia that penetrate into the snail intermediate host.

17. Snail- intermediate host
cercariae
Egg
Snail- intermediate host
Schistosoma

20. Adult worms live in the mesenteric veins (S. mansoni, S. japonicum, S
Adult worms live in the mesenteric veins (S. mansoni, S. japonicum, S. mekongi, and S. intercalatum) or in the venous plexus around the lower ends of the ureters and the urinary bladder (S. haematobium). In these sites, they start their sexual reproduction by releasing eggs. Once deposited in the host, eggs may stay in the mesenteric vein, be trapped in the intestines, escape to the intestinal lumen, and migrate by portal blood to the liver (S. mansoni, S. japonicum). Eggs of S. haematobium may be trapped in the intestines and bladder and may escape to the intestinal or bladder lumen. After being excreted with feces or urine into fresh water, the eggs hatch and release ciliated motile miracidia that penetrate into the snail intermediate host. Following asexual multiplication in the snail, the development of cercariae, the infective forms for humans, takes 4 to 7 weeks. After leaving the snails, the cercariae can survive in fresh water for almost 72 hours. When penetration of the skin in the human host occurs, the cercariae lose their tails and change into schistosomula. Schistosomula migrate to the lungs and, in about 6 weeks, mature to adult worms and descend to their final habitat. Viable eggs can be seen in excretions (i.e., stool or urine) 5 to 9 weeks after cercarial penetration. The lifespan of the worms ranges from 5 to 10 years.

21. Etiology and Life Cycle
Once deposited in the host, eggs may stay in the mesenteric vein, be trapped in the intestines, escape to the intestinal lumen, and migrate by portal blood to the liver (S. mansoni, S. japonicum).
The lifespan of the worms ranges from 5 to 10 years.
Once deposited in the host, eggs may stay in the mesenteric vein, be trapped in the intestines, escape to the intestinal lumen, and migrate by portal blood to the liver (S. mansoni, S. japonicum).
The lifespan of the worms ranges from 5 to 10 years. It means 即使没有治疗，10年后schistosome也会die.

22. Humans become infected after contact with water that contains the infective stage (cercaria) of schistosomes.
cercarial dermatitis:Pruritus is one of the commonest symptoms .

23. PATHOBIOLOGY
Adult worms release eggs in the venules of the mesentery, and the eggs enter the liver through the portal vein, where they become lodged in the terminal branches of the portal venules.
The lodged eggs cause a granulomatous inflammation, and the lesions are healed by periportal fibrosis.
S. japonicum is more virulent than S. mansoni because its infection produces ten times more eggs.
Humans become infected after contact with water that contains the infective stage (cercaria) of schistosomes.

24. PATHOBIOLOGY
Because the habitat of S. mansoni, S. japonicum, S. mekongi, and S. intercalatum worms is the mesenteric blood vessels, the intestines are involved primarily, and egg embolism results in secondary involvement of the liver.
In the liver, the granulomas result in perisinusoidal obstruction of portal blood flow, portal hypertension, splenomegaly, esophageal varices, and portosystemic collateral circulation.
Because the habitat of S. mansoni, S. japonicum, S. mekongi, and S. intercalatum worms is the mesenteric blood vessels, the intestines are involved primarily, and egg embolism results in secondary involvement of the liver.

25. PATHOBIOLOGY
Liver cell perfusion is not reduced; consequently, liver function test results remain normal for a long time. In schistosome-infected populations, the intensity of infection increases during the first 2 decades of life as children accumulate worms and then declines.
Liver cell perfusion is not reduced; consequently, liver function test results remain normal for a long time. In schistosome-infected populations, the intensity of infection increases during the first 2 decades of life as children accumulate worms and then declines.

26. CLINICAL MANIFESTATIONS
Clinical manifestations of schistosomiasis are divided into
-schistosome dermatitis
-acute schistosomiasis
-chronic schistosomiasis
Clinical manifestations of schistosomiasis are divided into schistosome dermatitis, acute schistosomiasis, and chronic schistosomiasis.

27. CLINICAL MANIFESTATIONS
A pruritic papular rash occurs within 24 hours after the penetration of cercariae and reaches maximal intensity in 2 to 3 days.
A pruritic papular rash occurs within 24 hours after the penetration of cercariae and reaches maximal intensity in 2 to 3 days.

28. CLINICAL MANIFESTATIONS ( Acute schistosomiasis )
Acute schistosomiasis occurs usually 20 to 50 days after primary exposure.
The clinical syndrome (i.e., fever, chills, liver and spleen enlargement, and marked eosinophilia) originally described for S. japonicum infection, and still common for this species, is increasingly being diagnosed in Brazil in individuals with S. mansoni infection.
The clinical syndrome (i.e., fever, chills, liver and spleen enlargement, and marked eosinophilia) originally described for S. japonicum infection, and still common for this species, is increasingly being diagnosed in Brazil in individuals with S. mansoni infection.

29. CLINICAL MANIFESTATIONS (Acute schistosomiasis )
Malaise, diarrhea, weight loss, cough, dyspnea, chest pain, restrictive respiratory insufficiency and pericarditis are important findings in this phase.
Malaise, diarrhea, weight loss, cough, dyspnea, chest pain, restrictive respiratory insufficiency, and pericarditis are important findings in this phase.

30. CLINICAL MANIFESTATIONS ( Acute schistosomiasis )
Acute disease is not observed in individuals living in endemic areas of schistosomiasis because of the downmodulation of the immune response by antigens or idiotypes transferred from mother to child.
Acute schistosomiasis is becoming a frequent and major clinical problem in nonimmune individuals from urban regions who are exposed for the first time to a heavy infection in an endemic area.
Although asymptomatic in endemic areas, acute schistosomiasis is becoming a frequent and major clinical problem in nonimmune individuals from urban regions who are exposed for the first time to a heavy infection in an endemic area.

31. CLINICAL MANIFESTATIONS (chronic schistosomiasis)
Abdominal pain, irregular bowel movements and blood in the stool are the main symptoms of intestinal involvement.
In chronic schistosomiasis, abdominal pain, irregular bowel movements, and blood in the stool are the main symptoms of intestinal involvement.

32. CLINICAL MANIFESTATIONS
Patients may remain asymptomatic until the manifestation of hepatic fibrosis and portal hypertension develops.
Patients may remain asymptomatic until the manifestation of hepatic fibrosis and portal hypertension develops.

33. CLINICAL MANIFESTATIONS
Hepatic fibrosis is caused by a granulomatous reaction to Schistosoma eggs that have been carried to the liver.
As it have been mentioned, hepatic fibrosis is caused by a granulomatous reaction to Schistosoma eggs that have been carried to the liver.

34. CLINICAL MANIFESTATIONS
Hepatic fibrosis is caused by a granulomatous reaction to Schistosoma eggs that have been carried to the liver.
As it have been mentioned, hepatic fibrosis is caused by a granulomatous reaction to Schistosoma eggs that have been carried to the liver.

35. CLINICAL MANIFESTATIONS
Hematemesis from bleeding esophageal or gastric varices may occur. In such cases, anemia and decreasing levels of serum albumin are observed.
Hematemesis from bleeding esophageal or gastric varices may occur. In such cases, anemia and decreasing levels of serum albumin are observed.

36. CLINICAL MANIFESTATIONS
A few patients have severe hepatosplenic disease with decompensated liver disease. Jaundice, ascites, and liver failure are then observed.
A few patients have severe hepatosplenic disease with decompensated liver disease. Jaundice, ascites, and liver failure are then observed.

37. CLINICAL MANIFESTATIONS
In hospitalized adult patients with S. japonicum infection, cerebral schistosomiasis occurs in 1.7 to 4.3%.
It may occur as early as 6 weeks after infection.
In hospitalized adult patients with S. japonicum infection, cerebral schistosomiasis occurs in 1.7 to 4.3%.
It may occur as early as 6 weeks after infection.

38. CLINICAL MANIFESTATIONS
In S. haematobium infection, the main organ system involved is the urinary tract.
The acute granulomatous response to parasite eggs in the early stages causes urinary tract disease, such as urethral ulceration and bladder polyposis.
In S. haematobium infection, the main organ system involved is the urinary tract.
The acute granulomatous response to parasite eggs in the early stages causes urinary tract disease, such as urethral ulceration and bladder polyposis.

39. CLINICAL MANIFESTATIONS
In chronic disease, usually in older patients, granulomas at the lower end of the ureters obstruct urinary flow and may cause hydroureter and hydronephrosis.
Bladder fibrosis and calcification are also seen in this phase. Up to 70% of infected individuals have hematuria, dysuria, or urinary frequency.
In chronic disease, usually in older patients, granulomas at the lower end of the ureters obstruct urinary flow and may cause hydroureter and hydronephrosis.
Bladder fibrosis and calcification are also seen in this phase. Up to 70% of infected individuals have hematuria, dysuria, or urinary frequency.

40. CLINICAL MANIFESTATIONS
An increased incidence of squamous cell carcinoma of the bladder has been reported in endemic areas of S. haematobium infection, but the mechanism of carcinogenesis is unknown.
S. haematobium eggs have occasionally been found in the lungs, with subsequent focal pulmonary arteritis and pulmonary hypertension.
An increased incidence of squamous cell carcinoma of the bladder has been reported in endemic areas of S. haematobium infection, but the mechanism of carcinogenesis is unknown.
S. haematobium eggs have occasionally been found in the lungs, with subsequent focal pulmonary arteritis and pulmonary hypertension.

41. DIAGNOSIS Blood routine examination Liver function test
Liver ultrasonic CT
Antibodies detection:Several serologic tests for detection of IgM, IgG, and IgA antibodies to Schistosoma antigens are available.
Examination of feces-the eggs
Rectum tissue biopsy

42. Ultrasonography allows determination of the degree of liver fibrosis.
After S. haematobium infection is diagnosed, assessment of urinary tract disease by ultrasonography is recommended.

43. Several serologic tests for detection of IgM, IgG, and IgA antibodies to Schistosoma antigens are available.
Serologic tests are important in the diagnosis of acute infection because the symptoms are not specific and the finding of eggs in stool may reflect chronic infection.
Seroconversion occurs within 4 to 8 weeks of infection but cannot distinguish active infection from a history of exposure.

44. DIAGNOSIS
Quantification of circulating antigens in serum and urine is an alternative for the diagnosis of schistosome infection.
However, the sensitivity of the method decreases in patients with light infection (<100 eggs per gram of feces).
Quantification of circulating antigens in serum and urine is an alternative for the diagnosis of schistosome infection.
However, the sensitivity of the method decreases in patients with light infection (<100 eggs per gram of feces).

45. Basis for DIAGNOSIS History of epidemiology:infested water contanct
Clinical manifestation
Laboratory tests
Differentiation diagnosis

46. DIAGNOSIS
A definitive diagnosis of schistosomiasis can be made only by finding schistosome eggs in feces, urine, or a biopsy specimen, usually from the rectum.
Schistosomal eggs typically have lateral or terminal spines and are easy to detect on microscopic examination of feces or on a rectal biopsy.
A definitive diagnosis of schistosomiasis can be made only by finding schistosome eggs in feces, urine, or a biopsy specimen, usually from the rectum.
Schistosomal eggs typically have lateral or terminal spines and are easy to detect on microscopic examination of feces or on a rectal biopsy.

47. DIAGNOSIS
A history of contact with contaminated water and appropriate clinical manifestations are important steps in establishing the diagnosis.
Because schistosome eggs may be few, concentration by sedimentation should be performed.
A history of contact with contaminated water and appropriate clinical manifestations are important steps in establishing the diagnosis.
Because schistosome eggs may be few, concentration by sedimentation should be performed.

48. DIAGNOSIS Rectal biopsy may be used for those with light infection.
In patients with chronic S. mansoni and S. japonicum infection and liver disease, the diagnosis is sometimes made by documentation of eggs in liver specimens.
For S. mansoni and S. japonicum, the Kato-Katz thick smear method is used.
Rectal biopsy may be used for those with light infection.
In patients with chronic S. mansoni and S. japonicum infection and liver disease, the diagnosis is sometimes made by documentation of eggs in liver specimens.

49. DIAGNOSIS
S. mekongi and S. intercalatum infection is diagnosed by examination of the stool for eggs.
Urine examination for S. haematobium eggs can be performed by direct or concentration methods.
Samples should be obtained at midday, when excretion of eggs is maximal.
Rectal biopsy may be performed in patients with light infection and negative urine results.
Ultrasonography allows determination of the degree of liver fibrosis.
S. mekongi and S. intercalatum infection is diagnosed by examination of the stool for eggs.
Urine examination for S. haematobium eggs can be performed by direct or concentration methods.
Samples should be obtained at midday, when excretion of eggs is maximal.
Likely, as I mention in last slide, rectal biopsy may be performed in patients with light infection and negative urine results.

50. TREATMENT
Chemotherapy is by far the major method for control and cure of schistosomiasis.
Three compounds are in use metrifonate, oxamniquine, and praziquantel, and all three are included in the World Health Organization’s list of essential drugs.
Chemotherapy is by far the major method for control and cure of schistosomiasis.
Three compounds are in use metrifonate, oxamniquine, and praziquantel, and all three are included in the World Health Organization’s list of essential drugs.

51. Praziquantel
a pyrazinoisoquinoline derivative, is the drug of choice for the treatment of schistosomiasis for four reasons:
high efficacy against all schistosome species and against cestodes,
lack of serious short-term and  long-term side effects,
administration as a single oral dose
competitive cost is cheap.
Praziquantel, a pyrazinoisoquinoline derivative, is the drug of choice for the treatment of schistosomiasis for four reasons:
-high  efficacy against all schistosome species and against cestodes,
-lack of serious short-term and  long-term side effects,
-administration as a single oral dose,
-competitive cost.

52. TREATMENT
The standard recommended treatment consists of a single dose of praziquantel, 40 mg/kg, for S. mansoni, S. haematobium, and S. intercalatum infection.
In S.japonicum infection, a total dose of 60 mg/kg is recommended, split into two or three doses in a single day.
S. mekongi may require two treatments at 60 mg/kg body weight. 
The standard recommended treatment consists of a single dose of praziquantel, 40 mg/kg, for S. mansoni, S. haematobium, and S. intercalatum infection.
In S. japonicum infection, a total dose of 60 mg/kg is recommended, split into two or three doses in a single day.
S. mekongi may require two treatments at 60 mg/kg body weight. 

53. TREATMENT With these dosages of praziquantel, recorded cure
rates are 75 to 85% for 
S. haematobium, 63 to 85% for S. mansoni, 80 to 90% for S. japonicum, 89% for S. intercalatum, and 60 to 80% for double infections 
with S. mansoni and S. haematobium. 
S. mekongi may require two treatments at 60 mg/kg body weight. With these dosages of praziquantel, recorded cure rates are 75 to 85% for S. haematobium, 63 to 85% for S. mansoni, 80 to 90% for S. japonicum, 89% for S. intercalatum, and 60 to 80% for double infections with S. mansoni and S. haematobium. 

54. TREATMENT The most common side effects observed with
praziquantel or oxamniquine are related to the gastro- intestinal tract: abdominal pain or discomfort, nausea, vomiting, anorexia, and diarrhea. 
The most common side effects observed with praziquantel or oxamniquine are related to the gastrointestinal tract: abdominal pain or discomfort, nausea, vomiting, anorexia, and diarrhea. 

55. TREATMENT These symptoms can be observed in up to 50% of
patients but are usually well tolerated. 
Other side effects are related to the central nervous 
system (e.g., headache, dizziness, drowsiness) and the 
skin (e.g., pruritus, eruptions) or may be nonspecific (
e.g., fever, fatigue).
These symptoms can be observed in up to 50% of patients but are usually well tolerated. 
Other side effects are related to the central nervous system (e.g., headache, dizziness, drowsiness) and the skin (e.g., pruritus, eruptions) or may be nonspecific (e.g., fever, fatigue).

56. TREATMENT In general, the cumulative experience from a large
number of studies allows the conclusion that 
praziquantel is an extremely well tolerated drug 
that requires minimal medical supervision and is 
therefore particularly suitable for mass chemotherapy  programs. 
In general, the cumulative experience from a large number of studies allows the conclusion that praziquantel is an extremely well tolerated drug that requires minimal medical supervision and is therefore particularly suitable for mass chemo-therapy  programs. 

57. TREATMENT
Although a reduction in the intensity of infection and morbidity has been documented after mass chemotherapy, provision of clean water, use of molluscicides (kill the snail), and adequate sanitation should also be implemented to control the disease.
Although a reduction in the intensity of infection and morbidity has been documented after mass chemotherapy, provision of clean water, use of molluscicides, and adequate sanitation should also be implemented to control the disease.

58. TREATMENT
The mortality rate is 0.05% for severe S. mansoni infection and 1.8% for severe S. japonicum infection. 
Bleeding from esophageal varices is the most 
serious complication. 
Chronic infection can lead to hepatocellular 
carcinoma.
The mortality rate is 0.05% for severe S. mansoni infection and 1.8% for severe S. japonicum infection. 
Bleeding from esophageal varices is the most serious complication. 
Chronic infection can lead to hepatocellular carcinoma.

59. Summary of schistosomiasis(1)
Schistosomiasis occurs mainly in rural agricultural and periurban areas in the developing world.
Five major species of Schistosoma affect humans.
The intermediate hosts is snail.
Eggs, causing the portal hypertension and liver fibrosis, is very important in pathobiology and diagnosis.
Schistosomiasis occurs mainly in rural agricultural and periurban areas in the developing world.
Five major species of Schistosoma affect humans.
The intermediate hosts is snail.
Eggs, causing the portal hypertension and liver fibrosis, is very important in pathobiology and diagnosis.

60. Summary of schistosomiasis(2)
Rectal biopsy may be used for those with light infection.
Metrifonate, oxamniquine, and praziquantel are included in the WHO’s list of essential drugs.
Praziquantel is well tolerated and effective for different clinical forms of schistosomiasis.
Rectal biopsy may be used for those with light infection.
Metrifonate, oxamniquine, and praziquantel are included in the WHO’s list of essential drugs.
Praziquantel is well tolerated and effective for different clinical forms of schistosomiasis.

61. 谢谢!
谢谢!