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Schistosomiasis.Care & specialists in United Kingdom

In United Kingdom, schistosomiasis is managed by tropical medicines. Schistosomiasis is a chronic parasitic disease caused by blood flukes of the genus Schistosoma, acquired when freshwater contaminated with the larval form (cercariae) penetrates intact human skin during bathing, wading, or fishing. The World Health Organization estimates roughly 251 million people require preventive treatment each year, with more than 90% of cases concentrated in sub-Saharan Africa and over 200,000 deaths annually from late complications.

aliases · Schistosomiasis (bilharzia, snail fever)· Bilharzia· Snail fever· Esquistossomose· reviewed May 14, 2026

Reviewed by AIHealz Medical Editorial Board · Tropical MedicineLast reviewed May 13, 2026

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§ 01

What it is

Schistosomiasis (ICD-10: B65), also called bilharzia or snail fever, is a chronic infection by trematode flatworms of the genus Schistosoma. Five species infect humans: Schistosoma mansoni and Schistosoma japonicum cause intestinal and hepatosplenic disease through eggs lodged in mesenteric venules; Schistosoma haematobium causes urogenital disease through eggs trapped in vesical venules and the bladder wall; Schistosoma mekongi affects the lower Mekong basin; and Schistosoma intercalatum and Schistosoma guineensis cause focal intestinal disease in central and west Africa. The life cycle requires a specific freshwater snail intermediate host — Biomphalaria for S. mansoni, Bulinus for S.

key facts

Prevalence: Approximately 251 million people require preventive treatment annually (WHO 2024); estimated 779 million live in transmission areas
Demographics: More than 90% of cases occur in sub-Saharan Africa; school-age children and adolescents carry the highest egg burden; men in occupational water contact (fishing, irrigation) at elevated risk
Avg. age: Peak intensity of infection age 10-15 years; chronic complications appear after 5-15 years of continuous re-exposure
Global cases: Roughly 200,000-280,000 deaths per year from schistosomiasis-related complications; 1.6 million disability-adjusted life-years lost annually (GBD 2021)
Specialist: Tropical Medicine

§ 02

How you might notice it

01Painless visible blood at the end of urination (terminal hematuria), the hallmark of urogenital schistosomiasis, often appearing in school-age boys 2-6 months after first exposure.

02Frequency, urgency, dysuria, and suprapubic pain from bladder-wall inflammation and granulomas in chronic S. haematobium infection.

03Intermittent bloody or mucoid diarrhea with crampy abdominal pain in intestinal schistosomiasis caused by S. mansoni, S. japonicum, or S. mekongi.

04Itchy maculopapular rash at the site of cercarial penetration within hours of freshwater exposure (cercarial dermatitis or swimmer's itch).

§ 03

How it’s diagnosed

diagnosis

Diagnosis begins with travel and exposure history — every freshwater contact in an endemic region within the past five years matters. In the acute phase, marked peripheral eosinophilia (often above 1,500/µL) combined with fever and recent exposure is highly suggestive of Katayama syndrome, but egg-shedding is usually negative for 6-8 weeks after infection. The reference standard for chronic infection is microscopic detection of characteristic eggs: a terminal-spined egg in urine for S. haematobium and a lateral-spined egg in stool for S. mansoni; S. japonicum eggs are small and round with a lateral knob. The Kato-Katz thick-smear technique on stool and filtration of 10 mL of midday urine for S. haematobium remain the WHO-recommended quantitative methods. Sensitivity falls in light infections; in returning travelers and chronic cases serology (ELISA or immunoblot for soluble worm antigens) is more sensitive but cannot distinguish active from past infection. The circulating cathodic antigen (CCA) urine cassette is a point-of-care test that detects active worm infection within 20 minutes and is now widely used in field surveys. Cystoscopy with bladder biopsy is reserved for hematuria with negative urinalysis or to assess fibrosis, and ultrasound of liver, spleen, kidneys, ureters, and bladder grades organ damage. In suspected neuroschistosomiasis, MRI with gadolinium and CSF eosinophilia support the diagnosis.

Key tests

Urine microscopy with filtration for S. haematobium eggsConfirms urogenital schistosomiasis by visualizing terminal-spined eggs

Stool microscopy (Kato-Katz thick smear)Confirms intestinal schistosomiasis and quantifies eggs per gram

Schistosoma serology (ELISA, immunoblot)Detects antibody to soluble worm or egg antigen; most useful in travelers, returning expatriates, and light or early infections

§ 04

Treatment & cost

medical treatments

✓Praziquantel (40 mg/kg single oral dose for S. mansoni/haematobium; 60 mg/kg for S. japonicum/mekongi)
✓Repeat praziquantel at 4-8 weeks
✓Oxamniquine (15 mg/kg single oral dose)
✓Corticosteroids (prednisolone 1 mg/kg/day, 5-7 days)

surgical options

Endoscopic band ligation of esophageal varicesEradication of varices in 80-90% of patients over 3-6 sessions; rebleeding rate roughly halved compared with no banding

Splenectomy with esophagogastric devascularization (Sugiura/Hassab)Long-term rebleeding rates of 10-20% in published series; mortality under 5% in centers with expertise

Bladder reconstruction or ureteric reimplantationSymptomatic improvement in 70-85% of selected patients; ureteric reimplant success roughly 90% in non-irradiated tissue

Radical cystectomy for schistosomiasis-associated bladder cancer5-year overall survival 40-55% for cT2 disease in modern series; under 20% once locally advanced

§ 05

Causes & risk factors

known causes

Schistosoma haematobium infection acquired in freshwater: Cercariae released by infected Bulinus snails penetrate intact human skin during bathing, washing, or fishing. Schistosomula migrate via lungs to the liver, mature to adult worms, and pair-bond in the vesical venous plexus. Eggs deposited in the bladder wall trigger granulomas and the urogenital syndrome. This species is endemic across sub-Saharan Africa, the Nile valley, and the Arabian peninsula.
Schistosoma mansoni infection acquired in freshwater: Cercariae from Biomphalaria snails enter through skin and adult worms pair in the inferior mesenteric venous plexus. Eggs lodge in the intestinal wall and liver, producing intestinal and hepatosplenic disease. S. mansoni is endemic in sub-Saharan Africa, the Arabian peninsula, Brazil, Suriname, Venezuela, and the Caribbean.
Schistosoma japonicum, mekongi, intercalatum, and guineensis infection: S. japonicum (China, Philippines, Indonesia) uses the Oncomelania snail and produces the heaviest egg burden, the most aggressive hepatic fibrosis, and the highest rate of central-nervous-system involvement. S. mekongi is restricted to the Mekong basin, S. intercalatum and S. guineensis to central and west Africa.
Repeated exposure to contaminated freshwater bodies: Lakes, rivers, irrigation canals, dams, fishponds, and ricepaddies in transmission areas are the typical sources. Even brief exposure (under one minute) can transmit infection if cercarial density is high. Dam construction (Aswan High Dam, Senegal River Diamond, Three Gorges) has historically expanded transmission by creating new snail habitat.
Lack of safe water, sanitation, and hygiene (WASH): Open defecation and urination near water bodies maintain the parasite life cycle. Communities without piped water rely on infected streams for bathing, laundry, and recreation. WHO modeling links 40-60% of regional transmission risk to inadequate sanitation infrastructure.

§ 06

Living with it

01Avoid all freshwater contact (swimming, wading, washing) in lakes, rivers, and irrigation canals in endemic regions; saltwater and properly chlorinated pools are safe.

02Towel-dry vigorously immediately after accidental freshwater exposure and shower with soap as soon as possible — does not eliminate risk but may reduce cercarial penetration.

03Use waterproof footwear and waders for unavoidable occupational water contact and limit duration of exposure.

04Boil, filter, or chemically treat drinking and bathing water in transmission areas; cercariae are killed by water held above 50 °C for five minutes.

05Participate in school- or community-based mass drug administration when offered, even in the absence of symptoms.

06Improve sanitation and water access (latrines, piped water) at the community level — the only sustainable intervention that interrupts transmission.

recommended foods

•Iron-rich foods (lean red meat, liver, lentils, dark leafy greens, fortified cereals) to address chronic anemia
•

§ 07

When to seek help

why see a tropical medicine

Tropical medicine and infectious disease specialists confirm species, exclude co-infections (malaria, strongyloides, HIV), and decide on repeat dosing or steroid cover, especially in Katayama syndrome and neuroschistosomiasis. Hepatology, urology, or gynecology referral is needed once portal hypertension, bladder fibrosis, or female genital schistosomiasis is diagnosed.

Find specialists →

01Bladder fibrosis with reduced capacity, frequency, urgency, and recurrent bacterial urinary infection — detect early with ultrasound bladder-wall thickness and post-void residual.

02Squamous-cell carcinoma of the bladder in chronic S. haematobium infection; new gross hematuria after age 30 in an endemic patient warrants cystoscopy.

03Bilateral hydronephrosis and obstructive uropathy progressing to chronic kidney disease — annual ultrasound and creatinine in heavy infections.

04Hepatic periportal (Symmers') fibrosis, splenomegaly, and esophageal varices with potentially fatal hematemesis — screen with abdominal ultrasound and surveillance endoscopy.

05Female genital schistosomiasis with infertility, dyspareunia, and a roughly 3-fold increased risk of HIV acquisition.

Related conditions

FilariasisAnother helminth infection sharing tropical geography, WHO mass drug administration platforms, and lymphatic or genital morbidity.Read →LeishmaniasisCo-endemic in sub-Saharan Africa and parts of Asia; another neglected tropical disease causing hepatosplenomegaly and pancytopenia in its visceral form.Read →StrongyloidiasisSoil- and water-associated helminth co-endemic with schistosomiasis; commonly screened together in returning travelers with eosinophilia.Read →AmebiasisAnother parasitic cause of bloody diarrhea and tropical hepatic disease; both feature in the differential for travelers.Read →Yellow FeverShares sub-Saharan African transmission geography; both are targets of integrated neglected-tropical-disease and vaccination programs.Read →

Easily confused with

vs. Schistosomiasis

MalariaBoth cause fever and eosinophilia after African travel, but malaria produces parasitemia visible on thick-and-thin blood films within 7-30 days of bite, has no consistent urinary or hepatosplenic egg pathology, and responds to artemisinin-based therapy. Schistosomiasis presents weeks later with hematuria, bloody stool, or Katayama syndrome and shows eggs on stool or urine microscopy.Compare →

vs. Schistosomiasis

AmebiasisBoth cause bloody diarrhea in tropical regions. Amebiasis (Entamoeba histolytica) typically produces flask-shaped colonic ulcers, liver abscess (not periportal fibrosis), and is diagnosed by stool antigen, PCR, or trophozoite microscopy. Schistosomiasis lodges eggs in the bowel wall and produces periportal hepatic fibrosis with splenomegaly.Compare →

vs. Schistosomiasis

StrongyloidiasisBoth cause eosinophilia in returning travelers. Strongyloides stercoralis causes serpiginous larva currens skin lesions, gastrointestinal symptoms, and life-threatening hyperinfection in immunosuppression. Diagnosis is by stool agar-plate culture or serology. Schistosomiasis produces hematuria, bloody diarrhea, or hepatosplenomegaly, and is treated with praziquantel rather than ivermectin.Compare →

vs. Schistosomiasis

TuberculosisGenitourinary tuberculosis can mimic urogenital schistosomiasis with sterile pyuria and hematuria. TB shows acid-fast bacilli on urine smear or culture, often with constitutional symptoms and lung findings, and responds to multidrug antitubercular therapy rather than praziquantel.

Often appears alongside

Anemia →Malaria →Hepatitis →

Types and stages

Urogenital schistosomiasis (S. haematobium)Adult worms pair in pelvic venous plexuses; eggs deposit in the bladder wall, ureters, seminal vesicles, prostate, cervix, vagina, and fallopian tubes. Classic presentation is painless terminal hematuria. Long-term sequelae include bladder fibrosis, hydronephrosis, infertility, female genital schistosomiasis, and squamous-cell bladder cancer.

Intestinal schistosomiasis (S. mansoni, S. mekongi, S. intercalatum, S. guineensis)Adult worms live in mesenteric venules; eggs traverse the bowel wall and lodge in the intestinal mucosa. Causes intermittent bloody diarrhea, abdominal pain, and eventually polypoid colitis.

Hepatosplenic schistosomiasisLate consequence of intestinal infection. Eggs swept to the liver via portal circulation trigger periportal Symmers' fibrosis without true cirrhosis; portal hypertension, splenomegaly, and esophageal varices follow. Hepatocellular function is usually preserved until very late.

Acute schistosomiasis (Katayama syndrome)A serum-sickness-like febrile illness 14-84 days after primary infection, most often seen in non-immune travelers exposed to S. mansoni or S. japonicum. Driven by immune complexes against migrating schistosomula and early egg deposition.

NeuroschistosomiasisRare ectopic egg deposition in the central nervous system. S. japonicum has a predilection for the brain (causing seizures, focal deficits); S. mansoni and S. haematobium more often involve the spinal cord with transverse myelitis or cauda-equina syndrome.

Living with Schistosomiasis

Timeline

Acute symptoms resolve within 1-2 weeks of praziquantel. Eosinophilia, hematuria, and stool egg counts typically normalize within 3 months. Ultrasound evidence of bladder-wall thickening and hydronephrosis regresses over 6-12 months. Hepatic periportal fibrosis does not regress fully but stabilizes after parasitological cure. Female genital schistosomiasis lesions improve over 6-24 months in 60-80% of women treated early.

Lifestyle

01Complete the full prescribed dose of praziquantel with a meal to maximize absorption and tolerability.
02Return for follow-up urine or stool testing 4-12 weeks after treatment to confirm cure; re-treat if eggs persist.
03Avoid further freshwater contact for at least 8 weeks after treatment to prevent rapid re-infection.
04Limit alcohol intake during treatment and in the presence of liver fibrosis to reduce additional hepatic injury.
05Maintain iron- and protein-rich nutrition during recovery from chronic anemia and growth faltering.
06Disclose travel and water-exposure history to any clinician evaluating hematuria, abdominal pain, eosinophilia, or unexplained varices.

Daily management

01Take praziquantel with food at the prescribed dose, split across the day for the 60 mg/kg regimen.

Complementary approaches

Artemisinin derivatives (artemether, artesunate)Active against migrating immature schistosomula and complement praziquantel in some endemic settings; not approved for first-line treatment but studied for chemoprophylaxis in occupational cohorts.

Mass drug administration with praziquantelWHO-endorsed community-level approach treating school-age children and at-risk adults annually or biennially. Reduces prevalence, intensity, and morbidity at the population level even when individual cure is incomplete.

Choosing a doctor

Look for a clinician with documented work in tropical infectious disease, ideally affiliated with a WHO-collaborating centre, a travel-medicine clinic, or a national reference laboratory that performs schistosome serology and CCA testing. For complications, choose a hepatologist or urologist who manages portal hypertension or bladder reconstruction at high volume.

Patient support resources

WHO Schistosomiasis Programme →Authoritative global epidemiology, treatment guidelines, and mass drug administration data.

Schistosomiasis Control Initiative (SCI Foundation) →Non-governmental partner that delivers praziquantel to schoolchildren in 16 African countries.

CDC Yellow Book — Schistosomiasis →Practical travel-medicine guidance on exposure, diagnosis, and post-travel testing.

FAST Package (Female-genital Schistosomiasis) →WHO-endorsed clinical pocket guide for recognizing and managing female genital schistosomiasis.

§ 08

Frequently asked

What is schistosomiasis in simple terms?

Schistosomiasis is a parasitic disease caused by blood flukes that live in human veins after entering through skin exposed to contaminated freshwater. Eggs released by the worms cause damage to the bladder, intestines, liver, or genitals over many years. It is treated with a single oral dose of praziquantel.

How do you catch schistosomiasis?

Infection occurs when freshwater containing larvae (cercariae) released from infected snails contacts intact skin. Bathing, wading, washing clothes, or working in lakes, rivers, dams, or irrigation canals in endemic regions transmits the parasite. Saltwater, chlorinated pools, and brief hand contact with treated water do not transmit infection.

What are the first signs of schistosomiasis?

Early signs include an itchy skin rash within 24 hours of freshwater exposure and, weeks later, fever, fatigue, muscle aches, and cough during the Katayama phase. Visible blood in urine or stool typically appears 2-6 months after first exposure. Many infections cause no early symptoms and are detected only on screening.

Is praziquantel the only treatment for schistosomiasis?

Praziquantel is first-line for all five human schistosome species at 40 mg/kg (60 mg/kg for S. japonicum and S. mekongi). Oxamniquine is a second-line option for S. mansoni only. Severe symptoms during the acute phase are managed with short-course corticosteroids alongside praziquantel.

How long does schistosomiasis take to cause damage?

Damage develops over years of unresolved infection. Children in endemic regions can show bladder-wall thickening within 1-2 years; significant hepatic periportal fibrosis usually appears after 5-15 years of heavy exposure. Bladder cancer related to S. haematobium typically presents in the fourth or fifth decade.

Can schistosomiasis be cured?

Active worm infection is cured in 60-90% of patients with a single 40 mg/kg dose of praziquantel; egg shedding falls by more than 90%. A second dose at 4-8 weeks raises cure rates further. Established organ damage such as severe bladder fibrosis or hepatic fibrosis does not fully reverse but stabilizes.

Is schistosomiasis contagious between people?

Schistosomiasis is not contagious from person to person. Transmission requires the freshwater snail intermediate host, so eggs passed in urine or stool must reach a body of fresh water containing the right species of snail to continue the life cycle. Sexual transmission has not been documented.

What does urinary schistosomiasis look like?

The hallmark is painless visible blood at the end of urination, usually in school-age boys and young men in endemic regions. Other features include frequency, urgency, dysuria, and lower abdominal pain. Long-term changes include bladder calcifications, hydronephrosis, and an increased risk of squamous-cell bladder cancer.

How is schistosomiasis diagnosed in travelers?

Returning travelers are screened with serology (ELISA), full blood count for eosinophilia, urine filtration, and three stool samples on consecutive days. Serology becomes positive 6-12 weeks after exposure. The CCA urine cassette can detect active S. mansoni infection at the point of care.

How can I prevent schistosomiasis when traveling?

Avoid swimming or wading in lakes, rivers, and irrigation canals in endemic regions. If exposure occurs, towel-dry vigorously and shower as soon as possible. Boil or filter drinking and bathing water, and seek pre-travel advice on testing and possible empirical post-exposure treatment.

Can children take praziquantel?

Yes. Praziquantel 40 mg/kg as a single oral dose is safe and effective in children aged 4 years and older, and WHO has approved formulations for younger preschool children. School-based mass drug administration with praziquantel is the largest deworming program in the world.

Does schistosomiasis cause infertility?

Female genital schistosomiasis can cause cervical, vaginal, fallopian, and ovarian lesions, leading to infertility, ectopic pregnancy, and chronic pelvic pain. In men, seminal vesicle and prostatic involvement can impair fertility. Early diagnosis and praziquantel treatment improve outcomes in 60-80% of women.

What is Katayama syndrome?

Katayama syndrome is an acute serum-sickness-like illness 4-8 weeks after first exposure, with fever, urticaria, myalgia, cough, hepatosplenomegaly, and marked eosinophilia. It is treated with corticosteroids (prednisolone 1 mg/kg/day for 5-7 days) plus praziquantel, with a repeat praziquantel dose 4-8 weeks later.

Does schistosomiasis increase HIV risk?

Yes, in women. Female genital schistosomiasis causes mucosal lesions and increased local immune activation that approximately triple the risk of HIV acquisition during heterosexual exposure. Treating female genital schistosomiasis is now part of WHO-recommended HIV-prevention strategies in endemic settings.

Is bilharzia the same as schistosomiasis?

Yes. Bilharzia is the common name, especially in Africa, named after Theodor Bilharz who identified the parasite in 1851. Schistosomiasis is the medical term. Snail fever is another colloquial name, particularly for the Asian S. japonicum form.

How long do schistosoma worms live in the body?

Adult worm pairs typically live 3-10 years in human blood vessels, but documented survival of more than 30 years has been reported in untreated migrants. Without treatment, egg-laying continues for the lifetime of the worms, driving cumulative organ damage.

Can schistosomiasis come back after treatment?

Praziquantel does not produce immunity, so re-infection from continued freshwater exposure in endemic regions is common. Children may be re-infected within 6-18 months without behavior change or improved water and sanitation. Travelers without further exposure rarely relapse.

Is schistosomiasis found outside Africa?

Yes. S. mansoni is endemic in Brazil, Venezuela, Suriname, parts of the Caribbean, and the Arabian peninsula. S. japonicum persists in China, the Philippines, and Indonesia. S. mekongi is restricted to the Mekong basin in Laos and Cambodia. Imported cases occur worldwide via travel and migration.

Does swimming in the ocean cause schistosomiasis?

No. Human schistosome species require a freshwater snail intermediate host and cannot survive in saltwater. Cercarial dermatitis (swimmer's itch) caused by bird schistosomes can occur in fresh or brackish water but does not progress to systemic infection.

What follow-up is needed after schistosomiasis treatment?

Repeat urine and stool microscopy at 4-12 weeks confirm parasitological cure; a second dose of praziquantel is given if eggs persist. Abdominal and pelvic ultrasound at 6 and 12 months tracks organ recovery. Travelers without re-exposure usually need no further follow-up after cure is confirmed.

Is praziquantel safe in pregnancy?

Yes. WHO 2006 expert consultation and subsequent reviews concluded that praziquantel is safe in pregnancy and breastfeeding, and pregnant women in endemic regions are now included in mass drug administration. Untreated maternal schistosomiasis is associated with anemia, low birth weight, and poorer infant growth.

§ 09

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