GOMES, F. F. R.; SALES, K. S.; http://lattes.cnpq.br/5135709776057958; http://lattes.cnpq.br/2886577053520251; GOMES, Francisco Fábio Rodrigues.; SALES, Kelsen dos Santos.
Résumé:
Pregnancy can lead to the occurrence of Thrombotic Microangiopathy (TMA), chacterized by presence of microangiopathic hemolytic anemia and existence of thrombus in the
microcirculation. Not very frequent conditions, but determine high maternalfetal morbimortality, such as HemolyticUremic Syndrome (HUS), Thrombotic Thrombocitopenic Purpura (TTP) and HELLP Syndrome. The present study intends to identify factors related to
thrombotic microangiopathic in pregnant women, by analysis of scientific publications. The
method was an integrative licterature review, using the descriptors thrombotic
microangiopathy, pregnancy; consulted data base were PubMed, LILACS and SciELo, from
August,2003 to September, 2014. Through detailed analysis of six selected articles the results
of this review was possible, with elaboration of sinoptic boards of obtained data. Evidences point to an inappropriate cleavage of multimers of Von Willebrand factor (vWF), due to ADAMTS13 deficiency in TTP; endothelial activation as responsible for thrombotichemolytic state that occurs in gravidic diathesis of HELLP Syndrome; and the desregulation of alternative complement pathway involved in the atypical HUS, these are the main
pathophysiologic mechanisms inveolved in TMAs, however, sometimes, differenciation among the three major microangiopathic syndromes metioned is a hard task, remaining in this context the obscurity of intersectional or undifferenciated states, thus, on many occasions, supportive therapy is the most effective management of such syndromes. The main factors related to TMAs seen were: alteration of the activity of ADAMTS13, complement regulatory gene mutation, pregnancy stage, maternal age, parity, laboratorial alterations, and
abnormalities of the alternative complement pathway. We conclude the spectrum of
thrombotic microangiopathic diseases during pregnancy have multifactorial characteristics and there is a lot to be discoverd about its real pathophysiological mechanism, as well as about the differentiation factors of TMAs, in order to provide a better clinical therapeutic management.