A systematic review of the role of eculizumab in systemic lupus erythematosus-associated thrombotic microangiopathy

Systemic lupus erythematosus (SLE) is a severe, systemic autoimmune condition that is characterised by inflammation and organ damage. SLE patients experience a loss of tolerance towards self-antigens due to auto-reactive B cells that produce autoantibodies, particularly against double-stranded DNA (dsDNA) and nuclear antigens. These autoantibodies correlate closely with disease activity and are used for diagnostic and prognostic evaluation [1]. Approximately 9.7/10,000 people in the UK suffer from SLE and people of Black Caribbean ethnicity have a higher incidence and prevalence of the disease; they are also more likely to have worsened disease manifestations compared to people of White ethnicity [2]. Lupus nephritis (LN) is one of the most common and damaging manifestations of SLE that affects approximately 40% of patients and leads to end-stage renal failure within 5 years in approximately 10% [3]. Although evidenced-based therapeutic strategies are in place for LN (for instance use of disease modifying anti-rheumatic drugs (DMARDs) such as cyclophosphamide and mycophenolate mofetil [4]) and there are international recommendations for therapy (including the Single Hub and Access point for paediatric Rheumatology in Europe (SHARE) initiative recommendations [5]), many patients do not respond to therapy and the outcomes for LN are still poor (approximately 44% of patients will enter remission [6]).

LN occurs in response to pathogenic autoantibodies in SLE binding IgG to form immune complexes which deposit in the kidney and result in damage, in part through activation of the complement cascade and innate immune system [7‐10]. Thrombotic microangiopathy (TMA) is a form of endothelial injury that can occur in the kidneys of 1–4% of LN patients [11] where it appears to correlate with the most severe clinical manifestations and is associated with a high mortality [12].

The complement system is part of the innate immune response involved in recognition and opsonisation of invading pathogens, it also plays important roles in maintaining homeostasis through clearance of apoptotic debris and immune complexes [13]. Complement plays an important role in LN – deficiencies in components of the complement system (C1q, C2 and C4) are prevalent in LN patients [14], particularly those that have a disease onset in childhood [15]. There is evidence to suggest that the alternative complement system can be pathogenically activated in SLE by the increased presence of immune complexes leading to overactivation of the terminal complement complex (C5b-9) and tissue damage [13, 16‐18]. The kidney is particularly sensitive to immune complex deposition and thus complement-mediated damage [18, 19]. This is demonstrated through the increased levels of C5a and C5b-9 in the plasma of patients with active lupus nephritis [18].

Eculizumab is a recombinant fully humanised IgG2/IgG4 monoclonal antibody that binds C5 and thus prevents the formation of the terminal complement complex [20]. It is currently used successfully in the treatment of atypical haemolytic uraemic syndrome (aHUS) and paroxysomal nocturnal hemoglobinuria (PNH) [21, 22]. Eculizumab use is currently being explored in the treatment of other types of glomerulonephritis in which complement dysregulation is implicated including IgA nephropathy [23] and Shiga toxin-producing Escherichia coli (STEC-HUS) [24]. In view of its mode of action, eculizumab has also been considered for use in LN.

The aim of this project was to determine the role of eculizumab as adjunctive therapy in patients with LN. The objectives were to perform a systematic literature review using the PICOS framework – (P)articipants – all ages, sexes and ethnicities included, (I) ntervention – those who received complement inhibition therapy for their SLE, (C) omparison – before and after complement inhibition therapy, (O)utcome – any measurable outcome and (S)tudy design – any study design.

The role of the complement cascade in LN is well evidenced; deficiencies in components of the complement cascade can lead to monogenic lupus (C1q, C2 and C4) [14] and low levels of C3 and C4 are assessed in the clinic to monitor disease activity. Further glomerular deposition of complement is almost universally seen in histological analysis. A study of 222 Chinese patients with active LN demonstrated that the alternative complement pathway may be important in the pathogenesis of LN and that factor Bb may be a biomarker for measuring disease activity [18]. Another study of 30 LN patients showed increased deposition of C9 in glomerular biopsy tissue in patients with worse disease compared to those with a more mild phenotype suggesting that the terminal complement complex (C5b-9) may be a suitable biomarker for LN disease activity [41].

Despite the above evidence that complement is important in the pathogenesis of LN, current therapies for LN are broad spectrum immunosuppressants and complement inhibitors are not routinely used. Eculizumab is both effective and safe in the treatment of aHUS [42]. It is well recognised that LN patients can develop secondary aHUS and TMA. However, despite the efficacy of eculizumab in aHUS patients this is not used as first line treatment in these patients. This review summarises case reports and studies that suggest that the use of eculizumab in LN complicated by TMA can be beneficial to patients with excellent response rates described after a short course of treatment. Further only 3 patients reported adverse events during eculizumab therapy suggesting that the safety profile of the drug is good. Eculizumab may have a role in refractory LN but this systemic literature review did not reveal any reported cases and the cost of this drug may be prohibitive [43].

TMA is seen in a subset of LN patients (1–4%) [11] and a small study of 11 patients demonstrated that 60% of these had complement regulatory protein mutations previously associated with aHUS [44]. No other studies have analysed the association between SLE patients with complement mutations and the prevalence of TMA however this is an area that requires more investigation.

Further mechanistic work is required to determine whether it is possible to identify patients with LN who may benefit from these medications as it may be possible to stratify patients. Correlating clinical phenotype with markers of complement activation would help to determine which patients should receive complement inhibition, at what point in disease course, and when is it safe to stop. The use of adjunctive treatment such as Eculizumab to current management protocols may improve the suboptimal renal outcomes in patients with LN.

One limitation of this study is that data related to the serological or non-renal parameters of disease is only available for four of the 30 patients included. This data may provide increased evidence on the risks or benefits of using eculizumab for LN-associated TMA in SLE patients.

This systematic review has demonstrated that clinically, eculizumab is a treatment option in secondary aHUS or TMA in patients with LN. Patients with refractory LN may benefit from adjunctive treatment with complement inhibition but further studies are required to define its role in this disease.