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Chagas Disease.Care & specialists in United Kingdom

In United Kingdom, chagas Disease is managed by tropical medicines. Chagas disease is a chronic parasitic infection caused by the protozoan Trypanosoma cruzi, transmitted primarily by triatomine bugs (kissing bugs) in Latin America and increasingly through congenital transmission, blood transfusion, organ transplantation, and oral routes worldwide. The Pan American Health Organization estimates that approximately 6-7 million people are infected globally, with roughly 30,000 new cases and 10,000 deaths per year, and over 75 million people at risk in 21 endemic countries from Mexico to Argentina.

aliases · Chagas disease (American trypanosomiasis)· American trypanosomiasis· Mal de Chagas· Enfermedad de Chagas· reviewed May 14, 2026

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

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§ 01

What it is

Chagas disease (ICD-10: B57.0 acute Chagas disease with heart involvement; B57.1 acute without heart involvement; B57.2-B57.5 chronic with various organ involvement), also called American trypanosomiasis, is a zoonotic infection caused by the kinetoplastid protozoan Trypanosoma cruzi. The parasite cycles between mammalian reservoirs (dogs, rodents, opossums, armadillos) and bloodsucking triatomine vectors of the genera Triatoma, Rhodnius, and Panstrongylus that defecate during or after feeding, depositing T. cruzi trypomastigotes near the bite or on mucous membranes. The parasite enters through breached skin or conjunctiva, transforms into amastigotes within host cells (especially cardiac and smooth muscle), and replicates intracellularly.

key facts

Prevalence: Approximately 6-7 million people infected globally (WHO/PAHO 2024); 75 million at risk in 21 endemic Latin American countries
Demographics: Predominantly affects rural and impoverished populations in Latin America; congenital transmission rate 1-12% from infected mothers; growing migrant cases in North America and Europe
Avg. age: Acute infection often in childhood in endemic areas; chronic complications appear 10-30 years later, peaking ages 40-60
Global cases: About 30,000 new cases and 10,000 deaths annually; 300,000+ people with Chagas live in the United States and 100,000+ in Europe
Specialist: Tropical Medicine

§ 02

How you might notice it

01Asymptomatic acute infection in 95% of cases; symptoms develop in only a minority of newly infected adults.

02Romana sign — painless unilateral periorbital edema with conjunctivitis and preauricular lymphadenopathy at the conjunctival site of inoculation, lasting 3-8 weeks.

03Chagoma — indurated erythematous swelling at the bite site, often on the face or arm, with regional lymphadenopathy.

04Fever, malaise, headache, myalgia, anorexia, and hepatosplenomegaly during the acute phase 4-8 weeks after exposure.

§ 03

How it’s diagnosed

diagnosis

Diagnosis is divided by phase. In the acute phase, microscopic detection of motile trypomastigotes in fresh blood, Giemsa-stained thick smears, or by concentration techniques (Strout method, microhematocrit) is the gold standard; sensitivity is high in the first 6-8 weeks. PCR amplification of T. cruzi DNA from blood is more sensitive in acute infection and is also positive in early congenital cases. In the chronic phase, parasitemia is intermittent and below the threshold for microscopy, so diagnosis relies on serology. Two different serological tests using different antigen preparations (ELISA, indirect immunofluorescence, indirect hemagglutination, chemiluminescence) are required for confirmation per WHO recommendations; a discordant result triggers a third test. PCR can support diagnosis in chronic infection and is used to assess parasitemia in immunocompromised patients and post-treatment. After diagnosis, every patient undergoes a baseline cardiac workup: 12-lead ECG, chest X-ray, transthoracic echocardiogram, and 24-hour Holter monitoring when available. The Brazilian Andrade classification and the BENEFIT-trial Rassi score (age, ECG findings, LV systolic function, BNP/proBNP, NYHA class) stratify cardiac risk. Gastrointestinal evaluation in symptomatic patients includes barium swallow for megaesophagus and barium enema or colonoscopy for megacolon. Pregnant women from endemic regions are screened serologically, and infants of seropositive mothers undergo PCR at birth and serology at 9-10 months. Immunocompromised patients (HIV, transplant) have surveillance PCR to detect reactivation early.

Key tests

Microscopy of fresh blood and Giemsa-stained thick smearsGold standard for acute Chagas — direct visualization of motile trypomastigotes

T. cruzi PCR (qualitative and quantitative)Detects parasite DNA; useful in acute infection, congenital diagnosis, and immunocompromised patients with suspected reactivation

§ 04

Treatment & cost

medical treatments

✓Benznidazole 5 mg/kg/day in 2 divided doses for 60 days (adults); 5-8 mg/kg/day for 60 days (children)
✓Nifurtimox 8-10 mg/kg/day in 3 divided doses for 60-90 days (adults)
✓Heart failure pharmacotherapy (ARNI/ACEi/ARB, beta-blockers, mineralocorticoid antagonists, SGLT2 inhibitors)
✓Amiodarone 200 mg daily after loading

surgical options

Implantable cardioverter-defibrillator (ICD)Annual appropriate ICD therapy in 25-40% of Chagas patients implanted for primary prevention; mortality reduction in secondary prevention

Cardiac resynchronization therapy (CRT)Symptomatic and functional improvement in 50-65% at 6 months; modest mortality reduction in cohort studies

Heart transplantation1-year survival 80-85%, 5-year survival 60-70%; outcomes comparable to non-Chagas cardiomyopathy at high-volume centers

Pneumatic dilation and Heller myotomy for megaesophagusSymptomatic improvement in 70-85% after Heller myotomy; pneumatic dilation efficacy lower in advanced Chagas megaesophagus

§ 05

Causes & risk factors

known causes

Vector-borne transmission by triatomine bugs: The primary route in rural endemic Latin America. Triatomine bugs (kissing bugs) of the genera Triatoma, Rhodnius, and Panstrongylus feed on blood at night and defecate near the bite; T. cruzi trypomastigotes in the feces enter through the bite wound, conjunctiva, or scratched skin. Modernized housing has dramatically reduced vector transmission in endemic countries.
Congenital transmission: Transplacental transmission from a chronically infected mother occurs in 1-12% of pregnancies. Treatment of girls and women of childbearing age before pregnancy reduces transmission; treatment during pregnancy is not recommended due to teratogenicity of benznidazole and nifurtimox.
Blood transfusion and organ transplantation: Historically a major route in endemic countries, largely controlled by routine donor screening. Remaining cases occur in non-endemic regions where screening is incomplete. Solid organ transplantation from infected donors can cause severe acute disease in recipients.
Oral transmission from contaminated food and drink: Increasingly recognized cause of outbreaks in the Brazilian Amazon, particularly from acai pulp, guava juice, and palm wine contaminated with crushed triatomine bugs. Oral transmission produces high parasitic inoculum and more severe acute disease with higher rates of myocarditis.
Reactivation from immunosuppression: HIV (especially when CD4 below 200), solid organ transplantation, hematopoietic stem cell transplant, high-dose chemotherapy, and biologic immunosuppression can reactivate chronic Chagas, producing fulminant myocarditis, meningoencephalitis, or skin lesions with high parasitemia.
Laboratory accident: Rare cause among researchers and clinicians working with cultured parasites or infected tissue. Post-exposure benznidazole within 7-14 days prevents established infection in most cases.

§ 06

Living with it

01Improve housing in endemic areas: replace mud, adobe, and palm thatch with plaster, brick, or concrete to deny triatomines a refuge.

02Use insecticide-treated bed nets and seal cracks and crevices in rural homes; ongoing indoor residual spraying through national programs.

03Screen all blood and organ donors for T. cruzi in endemic and migrant-receiving countries.

04Pasteurize and refrigerate fruit pulps (acai, guava) and palm wine in the Brazilian Amazon to prevent oral transmission.

05Screen pregnant women from endemic regions and treat infants of seropositive mothers in the first year of life.

06Educate travelers to rural Latin America about triatomine bugs, bed precautions, and avoidance of homes with mud or thatched walls.

recommended foods

•Heart-healthy Mediterranean-style diet with vegetables, whole grains, lean protein, and olive oil
•Soft, small-frequency meals if megaesophagus is present, with adequate liquid intake

§ 07

When to seek help

why see a tropical medicine

Patients with positive Chagas serology should be referred to infectious disease or tropical medicine for confirmation, staging, and antiparasitic treatment decisions. Concurrent cardiology evaluation is essential because cardiac involvement determines prognosis. Gastroenterology and surgery are involved when megaesophagus or megacolon is present.

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01Sudden cardiac death from ventricular arrhythmias — the leading cause of mortality; risk reduced by ICD in selected high-risk patients.

02Progressive heart failure with reduced ejection fraction, the second leading cause of mortality.

03Thromboembolism from left ventricular apical aneurysm clots — strokes, peripheral embolism, mesenteric ischemia.

04Megaesophagus complications including aspiration pneumonia, esophageal cancer (small but increased risk), and severe weight loss.

05Megacolon complications including fecaloma, volvulus, and bowel perforation.

06Congenital Chagas in offspring of untreated women of childbearing age — preventable by pre-pregnancy treatment.

Related conditions

LeishmaniasisAnother protozoal infection co-endemic in Latin America; both are neglected tropical diseases requiring specialist diagnosis.Read →SchistosomiasisNeglected tropical disease with chronic organ damage; shares public-health control framework.Read →MalariaVector-borne parasitic disease relevant to travelers from Latin America; differential diagnosis of fever in returning travelers.Read →FilariasisNeglected tropical disease and shared WHO mass treatment frameworks; different clinical pattern but similar epidemiologic context.Read →HIV/AIDSHIV immunosuppression can reactivate chronic Chagas; co-infection requires combined management.Read →

Easily confused with

vs. Chagas Disease

LeishmaniasisBoth are protozoal infections endemic to Latin America. Leishmaniasis is transmitted by sand flies and presents as cutaneous, mucocutaneous, or visceral disease with characteristic skin or splenic involvement. Chagas disease is transmitted by triatomine bugs and primarily affects heart and gastrointestinal tract over decades. Microscopy and serology distinguish the two parasites.Compare →

vs. Chagas Disease

MalariaMalaria is mosquito-transmitted with cyclical fevers and Plasmodium parasites on blood smear within days of exposure. Chagas disease has a brief acute phase often asymptomatic, followed by decades of latency and slowly progressive cardiac or gastrointestinal disease. Both can occur in returning travelers from endemic regions.Compare →

vs. Chagas Disease

SchistosomiasisSchistosomiasis is acquired through freshwater contact with cercariae and causes hematuria, bloody diarrhea, or hepatosplenic disease. Chagas disease is vector-borne or congenitally transmitted and causes cardiac and gastrointestinal manifestations. Eosinophilia is more typical of schistosomiasis than Chagas.Compare →

vs. Chagas Disease

FilariasisFilariasis is mosquito-transmitted and causes lymphatic obstruction and microfilaria in nocturnal blood smears. Chagas disease produces cardiomyopathy and megaviscera rather than lymphedema. Geography and clinical pattern distinguish them.Compare →

Often appears alongside

Anemia →HIV/AIDS →

Types and stages

Acute Chagas diseaseFirst 4-8 weeks after primary infection. Usually asymptomatic in adults; symptomatic cases (especially children) feature Romana sign, chagoma, fever, lymphadenopathy, hepatosplenomegaly, and rarely myocarditis or meningoencephalitis. Parasitemia is high and microscopically detectable.

Indeterminate chronic phaseAsymptomatic seropositive state with normal ECG, chest X-ray, esophagogram, and barium enema. Affects 60-70% of chronically infected individuals; may persist for life. Annual rate of progression to determinate disease is 2-5%.

Chronic Chagas cardiomyopathy20-30% of chronically infected adults. Pathology: dilated cardiomyopathy with conduction system fibrosis, ventricular aneurysms (especially apical), arrhythmias, thromboembolism, and sudden death. Staged by ECG, echocardiogram, and biomarkers (Andrade or BENEFIT classification).

Chronic digestive Chagas disease5-10% of chronically infected patients, more common in Brazil and southern cone countries. Manifests as megaesophagus (dysphagia, regurgitation, weight loss) and megacolon (chronic constipation, fecaloma, volvulus) from autonomic denervation of the enteric nervous system.

Congenital Chagas disease1-12% transmission rate from chronically infected mother to fetus. Most newborns are asymptomatic; symptomatic cases present with prematurity, low birth weight, hepatosplenomegaly, jaundice, and rarely meningoencephalitis or myocarditis. Treatment in the first year of life cures over 90% of cases.

Reactivation in immunosuppressed patientsHIV, transplantation, and immunosuppressive therapy can cause reactivation of chronic Chagas with high parasitemia and severe myocarditis or meningoencephalitis. Mortality is high without prompt antiparasitic therapy.

Living with Chagas Disease

Timeline

Antiparasitic treatment course: 60 days for benznidazole, 60-90 days for nifurtimox. Side effects typically appear in the first 2-3 weeks and may necessitate dose adjustment. Side effects largely resolve within 4-8 weeks of completion. Parasitologic response is assessed by serology over 1-3 years; persistent positive serology does not necessarily indicate treatment failure. Heart failure management is lifelong with annual review.

Lifestyle

01Complete the full 60-90 day antiparasitic course exactly as prescribed; do not stop because side effects improve.
02Attend regular cardiology follow-up (annual ECG and echocardiogram in indeterminate disease; every 6 months in cardiomyopathy).
03Follow heart-healthy diet (low salt, moderate protein, vegetables, fish) and limit alcohol to under 2 units per day.
04Avoid donating blood, organs, or tissue once diagnosed.
05Take cardiac medications including anticoagulants exactly as prescribed; monitor for bleeding.
06Inform all healthcare providers of the diagnosis at every encounter; carry a card or wear an alert.

Daily management

01Take antiparasitic and cardiac medications at the same time daily.
02

Complementary approaches

Vector control programs (indoor residual insecticide spraying)Cornerstone of regional public-health response; combined with housing improvement reduces vector transmission by over 80% in endemic regions. Important community-level intervention rather than individual therapy.

Universal blood and organ donor screeningImplemented in all endemic countries since the 1990s and in the United States since 2007. Reduced transfusion-associated Chagas to virtual elimination in screened systems.

Choosing a doctor

Choose an infectious disease specialist with documented experience in Chagas disease, ideally affiliated with a center participating in WHO-PAHO Chagas networks. In non-endemic countries, multidisciplinary Chagas clinics combining tropical medicine, cardiology, and obstetrics offer the most comprehensive care.

Patient support resources

WHO Chagas disease fact sheet →Authoritative global epidemiology, transmission, and treatment guidance for clinicians and patients.

Pan American Health Organization (PAHO) Chagas information →Regional surveillance, control program data, and patient resources for the Americas.

CDC Parasites — Chagas Disease →US Centers for Disease Control patient information including travel precautions and clinician resources.

DNDi (Drugs for Neglected Diseases initiative) Chagas program →Research and access program with patient information, treatment access advocacy, and clinical trial updates.

§ 08

Frequently asked

What is Chagas disease in simple terms?

Chagas disease is a chronic infection caused by the parasite Trypanosoma cruzi, spread by kissing bugs in Latin America. Most people have no symptoms initially. Decades later, about 30% develop heart problems and 10% develop digestive complications. Antiparasitic drugs cure most acute cases.

How is Chagas disease transmitted?

Main routes are bites of infected triatomine (kissing) bugs in rural Latin America, congenital transmission from mother to baby (1-12%), blood transfusion, organ transplantation, and oral transmission through food contaminated with bug feces. The disease is not transmitted person-to-person by casual contact.

What are the symptoms of Chagas disease?

Acute infection (4-8 weeks after exposure) is usually asymptomatic; some patients develop the Romana sign (eye swelling), fever, and lymphadenopathy. Chronic disease develops over decades and includes heart failure, arrhythmias, sudden cardiac death, megaesophagus with dysphagia, and megacolon with constipation.

How is Chagas disease diagnosed?

Acute disease is diagnosed by detecting parasites in blood under microscopy or by PCR. Chronic disease requires two different serological tests (ELISA, IFA, IHA, chemiluminescence) on a blood sample. Cardiac and gastrointestinal evaluation follows confirmation. Pregnant women and infants from endemic regions are routinely screened.

How is Chagas disease treated?

Antiparasitic therapy with benznidazole 5 mg/kg/day for 60 days or nifurtimox 8-10 mg/kg/day for 60-90 days is first-line. Treatment cures over 90% of acute cases and 30-60% of chronic indeterminate cases. Heart failure and arrhythmias require standard cardiac therapy and devices.

Is Chagas disease curable?

Acute and early chronic Chagas can be cured with benznidazole or nifurtimox in over 90% of acute cases and 30-60% of indeterminate cases. Established cardiomyopathy is not curable with antiparasitic drugs but can be controlled with heart failure therapy and devices.

How long does Chagas disease take to develop?

Acute phase lasts 4-8 weeks after infection, usually without symptoms. The indeterminate chronic phase lasts decades. Cardiac and gastrointestinal complications typically develop 10-30 years after initial infection. Some patients remain asymptomatic for life.

Can Chagas disease be transmitted from mother to baby?

Yes. Transplacental transmission occurs in 1-12% of pregnancies in chronically infected mothers. All pregnant women from endemic regions should be screened. Infants of seropositive mothers are tested at birth (PCR) and 9-10 months (serology). Treatment in the first year cures over 90% of congenital cases.

Where is Chagas disease found?

Endemic to rural Latin America from Mexico to Argentina, with highest prevalence in Bolivia (6.1% national). Approximately 300,000 infected people live in the United States and over 100,000 in Europe, almost all migrants from endemic regions. Travel-acquired cases in non-endemic countries are rare.

What is the Romana sign?

The Romana sign is painless unilateral periorbital swelling with conjunctivitis and preauricular lymphadenopathy at the conjunctival inoculation site, occurring during acute Chagas. It develops when triatomine bug feces are rubbed into the eye and lasts 3-8 weeks. It is one of the few specific signs of acute infection.

Does Chagas disease cause heart problems?

Yes. Chagas cardiomyopathy develops in 20-30% of chronically infected adults after 10-30 years of latency. Features include arrhythmias (especially ventricular), heart failure, conduction abnormalities, apical aneurysm with thrombus, and sudden cardiac death. Annual ECG and echocardiogram detect progression.

What is megaesophagus?

Megaesophagus is autonomic denervation of the esophageal nerves causing progressive dysphagia, regurgitation, weight loss, and aspiration risk. It develops in 5-10% of chronic Chagas patients and is graded by barium swallow. Treatment includes pneumatic dilation, Heller myotomy, and rarely esophagectomy.

What is the BENEFIT trial?

BENEFIT (2015) was a large randomized trial of benznidazole versus placebo in established Chagas cardiomyopathy. It showed parasitologic reduction but no improvement in clinical outcomes over 5 years. Treatment of advanced cardiomyopathy is therefore optional and focused on parasitic load reduction.

Are kissing bugs in the United States?

Triatomine bugs exist in southern US states, particularly Texas, Arizona, and New Mexico, and have caused rare locally acquired cases. Most US Chagas cases occur in migrants from endemic Latin America. US blood donors are routinely screened to prevent transfusion-transmitted Chagas.

Should I be screened for Chagas?

Screening is recommended for people born in endemic Latin American regions, those with mothers from endemic regions, recipients of blood or organs from such donors, and prior to immunosuppression in at-risk patients. Pregnant women from endemic regions are screened in early pregnancy.

Are benznidazole side effects severe?

Benznidazole causes rash in 30%, gastrointestinal upset, peripheral neuropathy, and leukopenia. About 10-15% of patients discontinue therapy due to side effects. Clinical and laboratory monitoring during treatment allows dose adjustment. Most side effects resolve within 4-8 weeks after stopping.

Can Chagas disease cause sudden death?

Yes. Sudden cardiac death is the leading cause of mortality in Chagas cardiomyopathy, accounting for 55-65% of deaths. Risk factors include LV dysfunction, ventricular arrhythmias, syncope, and apical aneurysm. Implantable defibrillators reduce risk in high-risk patients.

Can immunosuppression reactivate Chagas?

Yes. HIV with CD4 below 200, solid organ transplant, hematopoietic stem cell transplant, and high-dose immunosuppression can reactivate chronic Chagas with severe myocarditis or meningoencephalitis. Pre-immunosuppression screening and PCR monitoring detect reactivation early.

Is Chagas disease contagious?

Chagas disease is not transmitted by casual person-to-person contact, kissing, or sharing utensils. The parasite requires the triatomine vector, congenital transmission, transfusion, transplant, or ingestion of contaminated food to spread. Health workers handling cultures need biosafety precautions.

Can I donate blood with Chagas disease?

No. People diagnosed with Chagas disease should not donate blood, organs, tissue, or sperm. Blood and organ donor screening is mandatory in endemic countries and in the United States since 2007 to prevent transfusion- and transplant-associated transmission.

How can I prevent Chagas disease?

Improve housing in endemic areas, use insecticide-treated bed nets, screen all blood and organ donors, pasteurize fruit pulps in the Amazon, screen pregnant women from endemic regions, and treat infants born to infected mothers. Travelers should avoid mud, adobe, and palm-thatched houses at night.

§ 09

Sources & references

01
Bern C. 2015. Chagas' disease. N Engl J Med 373(5):456-466.accessed 2026-05-14
02
Morillo CA, Marin-Neto JA, Avezum A, et al. 2015. Randomized trial of benznidazole for chronic Chagas' cardiomyopathy (BENEFIT). N Engl J Med 373(14):1295-1306.accessed 2026-05-14
03
Nunes MCP, Beaton A, Acquatella H, et al. 2018. Chagas cardiomyopathy: an update of current clinical knowledge and management (AHA scientific statement). Circulation 138(12):e169-e209.accessed 2026-05-14
04
World Health Organization. 2024. Chagas disease (American trypanosomiasis) fact sheet. WHO Geneva.accessed 2026-05-14
05
Pinazo MJ, Cancino-Faure B, Murillo-Solano C, et al. 2017. Standardization of PCR for Chagas disease diagnosis. Trop Med Int Health 22(8):980-989.accessed 2026-05-14
06

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