Púrpura trombocitopênica trombótica
Revisado por Dr Colin Tidy, MRCGPÚltima atualização por Dr Toni Hazell, MRCGPLast updated 15 Dez 2022
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What is thrombotic thrombocytopenic purpura?
Thrombotic thrombocytopenic purpura (TTP) is a rare form of thrombotic microangiopathy. It is characterised by:
Microangiopathic haemolysis.
Thrombocytopenia.
Neurological abnormalities.
Febre.
Renal dysfunction.
The diagnosis of TTP should be treated as a medical emergency. Without treatment the mortality is 90% and around half of all deaths occur within 24 hours of presentation; however, this can be greatly reduced with prompt treatment with plasma exchange.1
Patogênese
Voltar ao conteúdoCongenital and acute acquired TTP are due to a deficiency of von Willebrand factor cleaving protein, also known as ADAMTS1.1
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How common is TTP? (Epidemiology)
Voltar ao conteúdoThe incidence is rising as there is greater recognition of the condition.
TTP is rare, with a reported incidence of 6 per 1,000,000 per year in the UK.1
It is most common in adults, although it has been reported in neonates and nonogenarians. The peak occurs in the fourth decade of life.
It is more common in females than in males; the ratio is 3:2.
What causes thrombotic thrombocytopenic purpura? (Aetiology)
Voltar ao conteúdoPregnancy and the postpartum state account for 10-25% of cases of TTP. The course of the syndrome is not altered by termination of pregnancy. It occurs in greater frequency in patients with HIV infection and may be the initial presenting syndrome. TTP may also be associated with autoimmune disease and cancer and may also be iatrogenic, related to drugs such as quinine and simvastatin.The most common form of TTP is idiopathic.
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TTP symptoms
Voltar ao conteúdoThere may be a prodrome resembling a flu-like illness, including fever, fatigue and generalised malaise and arthralgias. A patient can present with:1
Thrombocytopenia (epistaxis, bruising, petechiae, gingival bleeding, haematuria, menorrhagia, gastrointestinal bleeding, retinal haemorrhage, haemoptysis).
Confusion, headache, paresis, aphasia, dysarthria, visual problems, encephalopathy, coma.
Fever, pallor, jaundice (haemolytic anaemia), fatigue, arthralgia, myalgia.
Proteinuria, micro-haematuria, raised urea and creatinine.
Chest pain, heart failure, arrhythmias, hypotension.
Dor abdominal.
Hemiparesis, hemiplegia or seizure - 35% of children with TTP present in this way.
Exame
Voltar ao conteúdoThis may be normal. However, you may find:
Febre.
Purpura - non-palpable small purpuric spots or petechiae occur with thrombocytopenia, ie platelet count <50 x 109/L.
Erupção púrpura

© Usuário: Hektor, CC BY-SA 3.0, via Wikimedia Commons
Jaundice - secondary to haemolysis.
Hipertensão grave.
Neurological problems as above.
Esplenomegalia.
Investigações2
Voltar ao conteúdoBlood smear shows fragmented erythrocytes, ie schistocytes. This is consistent with haemolysis. Schistocytes are a hallmark of the disease but there are no guidelines as to the number of schistocytes required to differentiate TTP from other thrombotic microangiopathies.
Renal function tests; creatinine level is mildly elevated in about half of patients.
Coagulation studies are non-diagnostic.
LDH level is extremely elevated. This is released from ischaemic or necrotic tissue cells.
Indirect bilirubin level is elevated.
Reticulocyte count is elevated.
Urinalysis shows proteinuria and microscopic haematuria.
Pre-treatment measurement of ADAMTS13 activity levels and anti-ADAMTS13 antibodies may be done in secondary care.1
Serological tests for HIV, hepatitis B virus and hepatitis C virus, autoantibody screen and a pregnancy test (when appropriate) should be performed at presentation.1
Diagnóstico diferencial1
Voltar ao conteúdoAutoimmune haemolysis/Evans' syndrome.
Pregnancy-associated - eg, síndrome HELLP.
Drugs - eg, quinine, simvastatin, interferon, calcineurin inhibitors.
Malignant hypertension.
Infections - typically, viral (cytomegalovirus, adenovirus, herpes simplex virus) or severe bacterial (meningococcus, pneumococcus), fungal.
Autoimmune disease (lupus nephritis, acute scleroderma).
Vasculite.
Síndrome hemolítico-urêmica (diarrhoea positive/negative).
Malignidade.
Catastrophic síndrome do anticorpo antifosfolipídeo.
TTP treatment and management
Voltar ao conteúdoIntravenous (IV) plasma exchange
IV plasma exchange is also called plasmapheresis. It is the present gold standard of treatment for TTP. During the plasma exchange, the inhibitory antibodies are removed and the plasma is replenished with the deficient protease.
Plasma exchange should be initiated as soon as possible, preferably within 4-8 hours.1
Infusion of fresh frozen plasma (FFP) 30 mL/kg can be used until the patient can be transferred to a facility where plasma exchange is available.
Glucocorticoid steroid and antiplatelet agents are used. Steroids often are administered prior to plasma exchange. Steroids have no proven added benefit over plasmapheresis alone, but some patients respond to high-dose prednisone (200 mg/day) alone, without plasma therapy.
Haemorrhage is a concern with antiplatelet therapy and its benefit has not been proven.3
Rituximab:
Recently the use of rituximab, a monoclonal anti-CD20 antibody, has also become mainline treatment.4
In acute idiopathic TTP with neurological or cardiac pathology (associated with a high mortality) rituximab, a monoclonal anti-CD20 antibody, should be considered on admission, in combination with plasma exchange and steroids.1
Patients with refractory or relapsing immune-mediated TTP should be offered rituximab.1
Increased plasma exchange and/or rituximab therapy are the agents of choice in relapsing disease.1
In patients with an acute episode of TTP, initial treatment with rituximab, plasma exchange and corticosteroids result in remission in over 90% of patients within 14 to 21 days. Rituximab may also decrease the frequency of subsequent relapses.4
Outros tratamentos:1
Red cell transfusion should be administered according to clinical need, especially if there is cardiac involvement.
Folate supplementation is required during active haemolysis.
Platelet transfusions are contra-indicated in TTP unless there is life-threatening haemorrhage.
Thromboprophylaxis with low molecular weight heparin (LMWH) is recommended once platelet count has reached >50 x 109/L.
The use of antiplatelet agents in TTP is unproven but low-dose aspirin may be given during platelet recovery (platelet count >50 x 109/L).
Cirurgia
Splenectomy is sometimes used but has limited proven benefit, and significant risks, with a mortality of 40% if carried out during acute TTP.1
Other measures
Supportive care for end-organ damage may be required - eg, haemodialysis for acute kidney injury.
NB: platelet transfusions are contra-indicated due to the risk of causing further thrombotic events - the only exception might be in the case of life-threatening haemorrhage.1
Prognóstico
Voltar ao conteúdoImproved treatment has improved mortality associated with acute episodes, from 90% to about 10-20%.1 About one third of survivors experience a relapse within the subsequent ten years.
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Leitura adicional e referências
- Thrombotic Thrombocytopenic Purpura, Congenital, TTP; Herança Mendeliana Online no Homem (OMIM)
- Guidelines on the diagnosis and management of thrombocytopenic purpura and other thrombotic microangiopathies; British Committee for Standards in Haematology (2012)
- Blombery P, Scully M; Management of thrombotic thrombocytopenic purpura: current perspectives. J Blood Med. 2014 Feb 5;5:15-23. doi: 10.2147/JBM.S46458. eCollection 2014.
- Lammle B, Kremer Hovinga J, Studt JD, et al; Thrombotic thrombocytopenic purpura. Hematol J. 2004;5 Suppl 3:S6-11.
- Lim W, Vesely SK, George JN; The role of rituximab in the management of patients with acquired thrombotic thrombocytopenic purpura. Blood. 2015 Mar 5;125(10):1526-31. doi: 10.1182/blood-2014-10-559211. Epub 2015 Jan 8.
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About the authorView full bio

Dra. Toni Hazell, MRCGP
MBBS, BSc, MRCGP, DFSRH, Dip GU med, DRCOG, DCH (London, UK, 2000)
Dr. Toni Hazell qualified from St. Mary’s Hospital Medical School and did her VTS at Northwick Park Hospital.
About the reviewerView full bio

Dr Colin Tidy, MRCGP
Médico Generalista, Autor Médico
MBBS, MRCGP, MRCP (Paediatrics), DCH
Dr Colin Tidy é um médico do NHS, baseado em Oxfordshire.
Histórico do artigo
As informações nesta página são escritas e revisadas por clínicos qualificados.
Próxima revisão prevista para: 14 Dez 2027
15 Dez 2022 | Última versão

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