Abstract
Evidence about the relevance of the complement system, a highly conserved constituent of the innate immunity response that orchestrates the elimination of pathogens and the inflammatory processes, has been recently accumulated in many different rheumatologic conditions. In rheumatoid arthritis, complement, mainly the classical pathway, contributes to tissue damage especially in seropositive subjects, with complement activation occurring in the joint. Data about complement pathways in psoriatic arthritis are dated and poorly consistent; among patients with Sjögren syndrome, hypocomplementemia exerts a prognostic role, identifying patients at risk of extra-glandular manifestations. Hints about complement involvement in systemic sclerosis have been recently raised, following the evidence of complement deposition in affected skin and in renal samples from patients with scleroderma renal crisis. In vasculitides, complement plays a dual role: on one hand, stimulation of neutrophils with anti-neutrophil cytoplasmic antibodies (ANCA) results in the activation of the alternative pathway, on the other, C5a induces translocation of ANCA antigens, favouring the detrimental role of antibodies. Complement deposition in the kidneys identifies patients with more aggressive renal disease; patients with active disease display low serum levels of C3 and C4. Even though in dermatomyositis sC5b-9 deposits are invariably present in affected muscles, data on C3 and C4 fluctuation during disease course are scarce. C3 and C1q serum levels have been explored as potential markers of disease activity in Takayasu arteritis, whereas data in Behçet disease are limited to in vitro observations. Pregnancies in women with rheumatologic conditions are still burdened by a higher rate of pregnancy complications, thus the early identification of women at risk would be invaluable. A fine-tuning of complement activation is required from a physiological progression of pregnancy, from pre-implantation stages, through placentation to labour. Complement deregulation has been implicated in several pregnancy complications, such as recurrent abortion, eclampsia and premature birth; low complement levels have been shown to reliably identify women at risk of complications. Given its physiologic role in orchestrating pregnancy progression and its involvement as pathogenic effector in several rheumatologic conditions, complement system is an attractive candidate biomarker to stratify the obstetric risk among women with rheumatologic conditions.
Highlights
The management of pregnancy has been revolutionized by the introduction of non-invasive prenatal screening tests, which allow assessing the risk of hypertensive complications and placental insufficiency
It is common practice to monitor complement levels to discriminate between nephritis and pre-eclampsia in systemic lupus erythematosus (SLE) expecting mothers presenting new-onset proteinuria: the serum C3 and C4 levels rise in patients with pre-eclampsia, while disease flares are classically characterized by consumed C3 and C4 and raise of antidsDNA titres (Mok, 2001)
The role of complement in the pathogenesis of rheumatologic conditions has been neglected for years, but evidence of its contribution to disease onset has been recently accumulating in many different conditions in the field of rheumatology
Summary
The management of pregnancy has been revolutionized by the introduction of non-invasive prenatal screening tests, which allow assessing the risk of hypertensive complications and placental insufficiency. Pregnant women with rheumatologic conditions still experience a higher rate of pregnancy morbidity, mainly in terms of intra uterine growth restriction (IUGR), pre-eclampsia, eclampsia and preterm delivery This occurs despite the fact that, in the recent years, awareness about reproductive issues in rheumatology patients have flourished in literature, and all the studies have identified an optimal disease control at conception as the main predictor of an uncomplicated gestational outcome in women with different rheumatologic conditions. After addressing the contribution of complement system to the progression of healthy pregnancy and the detrimental role of complement deregulation in pregnancy complications, this review will focus on the relevance of complement in rheumatologic conditions other than SLE and APS, discussing available evidence about the involvement of complement in disease pathogenesis and about the clinical significance of complement serum levels. We will recapitulate available data on the pregnancy outcome of women with different rheumatologic conditions, in order to clarify the potential role of complement as obstetric surrogate biomarker in these clinical scenarios
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