Interestingly, in

IgA nephropathy, glomerular deposition

Interestingly, in

IgA nephropathy, glomerular deposition of ficolin-2 with local lectin pathway activation was associated with more severe renal disease [37]. According to our findings, pregnant women with low circulating levels of ficolin-2 or ficolin-3 have an increased risk for pre-eclampsia. Low ficolin-2 and ficolin-3 levels have already been linked to various pathological conditions, such as combined allergic and infectious respiratory disease in children [38,39], bronchiectasis [40], prematurity, low birth weight and perinatal infections [41], sarcoidosis [42], susceptibility to fever and neutropenia in pediatric cancer patients [43] and to neonatal sepsis [44]. Moreover, our research group has demonstrated recently that low ficolin-3 levels in early follow-up serum samples https://www.selleckchem.com/products/Adriamycin.html are related to the severity and unfavourable outcome of acute ischaemic stroke [45]. Genetic variations were shown to affect ligand binding or circulating levels of ficolins [46–48] and to associate with several disorders, including rheumatic fever and chronic rheumatic heart disease [49], bacterial and cytomegalovirus infections after orthotopic liver transplantation [50,51], and even immunodeficiency [52]. As pre-eclampsia is a multi-factorial disease with genetic components, the role of ficolin gene polymorphisms should be examined in www.selleckchem.com/screening/gpcr-library.html the

future in the risk of this pregnancy-specific disorder. In our study, the similar plasma ficolin-2 and ficolin-3 levels of pre-eclamptic patients regardless of the severity, the time of onset of the disease or the presence Nutlin-3 in vitro of fetal growth restriction might be explained by the complex aetiology of pre-eclampsia. Several genetic, behavioural and environmental factors need to interact to produce the complete picture of this pregnancy-specific disorder. We reported various genetic and soluble factors that were associated with the severity

or complications of pre-eclampsia, including HELLP syndrome and fetal growth restriction [53–56]. Nevertheless, it is also possible that the relatively small sample size of this study prevented the detection of an effect in the subgroup analyses. Although pre-eclampsia is predominantly a disease of primiparas, multiparous women, especially with advanced age or over weight, can also be affected, as in our cases. In conclusion, circulating levels of ficolin-2 are decreased in the third trimester of normal pregnancy. There is a further decrease in plasma ficolin-2 concentrations in pre-eclampsia, which might contribute to the development of the maternal syndrome of the disease through impaired removal of the trophoblast-derived material released into the maternal circulation by the hypoxic and oxidatively stressed pre-eclamptic placenta. We thank Veronika Makó, László Cervenak and Levente Lázár for measuring plasma von Willebrand factor antigen and cell-free fetal DNA concentrations.

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