Open AccessAtypical uraemic haemolytic syndrome in pregnancy
Author(s) -
Ángel Augusto Pérez-Calatayud,
Jesús Carlos BrionesGarduño,
Mercedes del Pilar Álvarez-Goris,
Ricardo Sánchez Zamora,
Angélica Ariadna Torres Aguilar,
Rosa Elba Mendoza-Mórales
Publication year - 2016
Publication title -
cirugía y cirujanos (english edition)
Language(s) - English
Resource type - Journals
ISSN - 2444-0507
DOI - 10.1016/j.circen.2016.06.012
Subject(s) - thrombotic microangiopathy , medicine , preeclampsia , autoantibody , complement system , antiphospholipid syndrome , complement factor i , immunology , gene , disease , pregnancy , immune system , biology , antibody , genetics
Atypical haemolytic uraemic syndrome is one of the main variants of thrombotic microangiopathy, and is characterised by excessive complement activation in the microvasculature. It is also characterised by the clinical triad; non-immune haemolytic anaemia, thrombocytopenia, and acute renal failure. In addition, 60% of patients have mutations in the genes encoding complement regulators (factor H, factor I, membrane cofactor proteins, and thrombomodulin), activators (factor B and C3), as well as autoantibodies against factor H. Multiple factors are required for the disease to manifest itself, including a trigger and gene mutations with adequate penetration. Being one of the differential diagnoses of preeclampsia–eclampsia and HELLP syndrome means that the clinician must be familiar with the disease due to its high mortality, which can be modified with early diagnosis and comprehensive treatment
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