Complement inhibition in ANCA vasculitis

Complement inhibition in ANCA vasculitis

G Model NEPHRO-1150; No. of Pages 4 Ne´phrologie & The´rapeutique xxx (2019) xxx–xxx Available online at ScienceDirect www.sciencedirect.com Mini ...

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G Model

NEPHRO-1150; No. of Pages 4 Ne´phrologie & The´rapeutique xxx (2019) xxx–xxx

Available online at

ScienceDirect www.sciencedirect.com

Mini review

Complement inhibition in ANCA vasculitis David Jayne Department of medicine, University of Cambridge, Addenbrookes Hospital, Box 115, Level 5, Cambridge CB2 2OQ, UK

A R T I C L E I N F O

A B S T R A C T

Article history: Received 27 March 2019 Accepted 12 April 2019

A role for the alternative complement pathway has emerged in the understanding of ANCA vasculitis pathogenesis. Current therapies of ANCA vasculitis are limited by partial efficacy and toxicity and many patients pursue a relapsing course. Improved therapies are needed. Inhibition of the alternative complement pathway component C5a is attractive due to its role in neutrophil activation and migration, and engagement of other inflammatory and thrombotic mechanisms. Two inhibitors of C5a are in clinical development for ANCA vasculitis: avacopan, an oral C5a receptor inhibitor has demonstrated efficacy, safety and steroid sparing in two Phase II trials; and IFX-1, a monoclonal antibody to C5a which is entering Phase II development. Complement inhibition has the potential to contribute to remission induction protocols achieving a higher quality of remission as well as replacing steroids. Confirmation of safety, especially infective risk, and the potential to replace steroids depends on further studies and a role in relapse prevention needs to be explored.

C 2019 Socie ´ te´ francophone de ne´phrologie, dialyse et transplantation. Published by Elsevier Masson SAS. All rights reserved.

Keywords: ANCA C5a Clinical trial Complement Therapy Vasculitis

1. Introduction ANCA associated vasculitis comprises the syndromes of Wegener’s granulomatosis (now granulomatosis with polyangiitis/GPA) and microscopic polyangiitis/MPA). Churg Strauss syndrome (now eosinophilic granulomatosis with polyangiitis/EGPA) is included due to the phenotypic overlap and a minority with ANCA positivity, definitions enshrined in the Chapel Hill Consensus Conference 2012 statement [1]. The most recent estimates of the incidence and prevalence of AAV are 3/100.000/year and 42/ 100,000 respectively [2]. In addition to aiding classification the ANCA test has facilitated genetic, pathogenetic and treatment studies. Genetic associations are more strongly linked with ANCA serotype (PR3-ANCA or MPO-ANCA) than disease phenotype (GPA or MPA) [3]. The strongest association are with the major histocompatibility complex (HLA DP with GPA and DQ with MPA), the gene encoding proteinase 3 (PRTNs) is associated with PR3-ANCA patients and both serotypes are associated with SERPINA1 (encodes for alpha 1 anti-trypsin) and PTPN22. The latter two associations also relate to pathogenesis because alpha 1 anti-trypsin is a key inhibitor of the serine protease PR3 and PTPN22 is associated with T cell activation, seen across ANCA

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vasculitis. Although preliminary candidate gene studies associated complement factor C3 polymorphisms with ANCA vasculitis, especially the C3F allotype, there have been no complement ‘‘hits’’ in the genome association studies [4,5]. Conventional treatment of AAV with cyclophosphamide and glucocorticoids emerged in the 1970s and has been optimised with more recent clinical trials [6]. However, this combination is not always effective and is toxic. B cell depletion with rituximab was shown to be an effective alternative to cyclophosphamide in two randomised trials (RAVE and RITUXVAS), but the real value of rituximab has been in the control of relapsing and refractory disease and in the minimisation of cyclophosphamide exposure [7–9]. Two significant problems with rituximab remain, there is a high relapse risk after rituximab whether or not an oral immunosuppressive is used, and AAV patients appear particularly susceptible to rituximab induced hypogammaglobulinaemia [10]. The RITUXVAS trial combined rituximab with reduced dose cyclophosphamide in such patients and similar combinations have been explored in observational cohorts [11]. Removal of circulating immune reactants including pathogenic antibodies with plasma exchange has been exploited for severe renal and pulmonary presentations for 40 years with reasonable evidence for benefits on renal function but no long term effects on survival have been shown [12]. Over 75% of GPA and 33% of MPA patients pursue a relapsing course and require long term treatment and follow-up [13]. Oral

https://doi.org/10.1016/j.nephro.2019.04.001 C 2019 Socie ´ te´ francophone de ne´phrologie, dialyse et transplantation. Published by Elsevier Masson SAS. All rights reserved. 1769-7255/

Please cite this article in press as: Jayne D. Complement inhibition in ANCA vasculitis. Ne´phrol ther (2019), https://doi.org/10.1016/ j.nephro.2019.04.001

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immunosuppressives, azathioprine and methotrexate, with or without glucocorticoids have been the most widely used relapse prevention strategy, more recently fixed interval repeat dose rituximab was shown to be more effective than azathioprine in preventing relapse and large observational studies have come to similar conclusions [14]. There remains uncertainty as to how to dose rituximab, and for how long, and the role of the biomarkers ANCA or CD19 counts in relapse prediction [15]. Larger scale clinical studies have resulted from the formation of collaborative networks, especially the European Vasculitis Society, the French Vasculitis Study Group and the Vasculitis Clinical Research Consortium in North America [16]. Limitations of current therapy are the time taken to achieve disease control and treatment toxicity. Early glucocorticoid exposure is the main reversible contributor to the high rates of serious adverse events in the first year, and later glucocorticoid exposure is a major contributor to irreversible damage and incapacity [17]. The key goals for newer agents are:  speed of action;  glucocorticoid sparing;  reduced relapse risk.

2. Complement and vasculitis The definition of the pathology associated with ANCA as being ‘‘pauci-immune’’, as compared to immune complex disease, has suggested the complement system is not a major part of pathogenesis [18]. Despite this classification, histopathologists have consistently reported IgG and C3 deposits in a minority of renal biopsies from patients with AAV, and there has been an association between the amount of IgG deposition and renal prognosis. There is evidence from histologic studies for renal activation of both the alternative and classical complement pathways. C3 fragments and the terminal attack complex are deposited in glomeruli and one report suggested involvement of the classical complement pathway in ANCA negative patients with ‘pauci-immune’ renal vasculitis, where C4d was present [19,20]. Evidence from animal models has shown prevention of vasculitis by complement depletion or by specific inhibition of the complement C5a receptor [21]. Patient studies have found associations of low total complement C3 levels at diagnosis with more severe renal disease and worse renal survival, of higher plasma and urine C5a levels in active disease and of deposition of complement components, including factor B, C3 fragments and the terminal attack complex, in affected glomeruli [22–24]. Low plasma C3 levels have also been associated with thrombotic microangiopathy in AAV [25]. Neutrophil sphingosine 1 appears to enhance C5a dependent neutrophil activation, and its inhibition has impaired the effects of C5a in vitro [26]. C5a signals through the C5a receptor and the C5L2 receptor, the animal studies cited above provide evidence for a key role for the C5a receptor but the function of signalling though C5L2 is unclear [27]. One study found inhibition of C5L2 to reduce neutrophil autoantigen expression indicating a pro-inflammatory role for this receptor [28]. It is also unclear whether other ligands signal through these receptors and whether there will be a difference between receptor inhibition or complement factor neutralisation. Complement factor H is a regulator of alternative pathway activation and plasma levels are depressed with more active disease in AAV and were an independent outcome predictor, this may be related to myeloperoxidase [29,30]. The complement regulatory proteins CD 46, CD 55 and CD 59 are expressed in glomerular and tubular cells in health and one study reported

reduced CD 46 and CD 55 expression in AAV, proportional to the severity of the glomerular disease [31]. The classic pathology model of ANCA vasculitis requires neutrophil priming by Il-1 or TNF, surface translocation of PR3 or MPO then binding of ANCA with cross linkage to Fc receptors triggering neutrophil degranulation, a respiratory burst and release of neutrophil NETs [32]. Impaired deformability of pre-activated neutrophils and upregulation of endothelial cell adhesion molecules promotes local adhesion and endothelial cytotoxicity. Because C5a is a potent neutrophil chemoattractant and primer for neutrophil activation, and activated neutrophils can excite complement activation through release of properdin and other factors, and neutrophil microparticles and neutrophil NETs can form a substrate for the C3 and alternative pathway C5 convertase, a positive feedback loop of neutrophil activation and alternative complement pathway activation has been proposed [20,33,34]. In addition, interactions between the complement and thrombotic systems, such as the C5 convertase on platelet surfaces, have helped to explain the thrombotic component of AAV pathogenesis. Furthermore C5a activated neutrophils relapse microparticles and NETs with tissue factor activity, and thrombin is an alternative C5 convertase [35]. Around 5% of patients with a ‘pauci-immune’ rapidly progressive glomerulonephritis are ANCA negative at diagnosis and the increased glomerular C3 and C9 deposition seen in their biopsies has suggested a classical complement mediated pathology, independent of ANCA that may be variably important in ANCA positive patients [36,37]. It is notable, however, that AAV has not been associated with diseases associated with complement dysregulation, such as, haemolytic uraemic syndrome and that candidate gene studies have not identified genetic abnormalities in complement regulatory proteins.

3. Complement inhibition and vasculitis An oral complement C5a receptor inhibitor, avacopan, developed by Chemocentryx has been evaluated in two Phase II trials in GPA/MPA. The CLEAR trial assessed the efficacy of a 12 week course of avacopan 30 mg twice daily in patients with active GPA/MPA [38]. In the first stage, avacopan was added to standard of care glucocorticoid, the second randomised between avacopan with reduced dose glucocorticoid or standard dose without avacopan, and in third phase avacopan with no glucocorticoid was compared to standard of care glucocorticoid without avacopan. All patients received cyclophosphamide or rituximab. Data from the three stages have been pooled in the published report which found that avacopan with or without low dose prednisolone was not inferior to high dose prednisolone, in fact was numerically superior, in terms of disease response defined by a 50% reduction in Birmingham Vasculitis Activity Score (BVAS) at 12 weeks. There were notably faster falls in proteinuria and haematuria in avacopan treated patients accompanied by faster falls in urinary MCP-1. Surprisingly certain quality of life measures, such as, vitality were superior in the avacopan without glucocorticoid treatment group. A second Phase II trial (CLASSIC) performed in the USA, compared 10 and 30 mg twice daily of avacopan to placebo, both given in addition to standard of care glucocorticoid (NCT02222155). No differences in efficacy of safety were seen although there were trends for a faster fall in BVAS and better GFR recovery in the 30 mg avacopan group. A Phase III trial, ADVOCATE, is currently recruiting which will compare avacopan without glucocorticoid to standard of care glucocorticoid over a 52 week treatment period (NCT02994927). A therapeutic monoclonal antibody that binds C5a, IFX-1, is also in clinical development for AAV, and hidradenitis suppurativa [39]. A Phase II trial has been launched, with design similarities to

Please cite this article in press as: Jayne D. Complement inhibition in ANCA vasculitis. Ne´phrol ther (2019), https://doi.org/10.1016/ j.nephro.2019.04.001

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the CLEAR trials described above (NCT03712345). IFX-1 is administered as an IV preparation and it will be interesting to see whether the different target in the C5 axis will have different efficacy in AAV. Eculizumab binds to C5 preventing production of both C5a and C5b and therefore influencing both alternative pathway activation and development of the terminal attack complex. No formal studies in AAV have been performed but there have been anecdotal reports of benefit in case reports of refractory disease [40]. 4. Conclusions AAV has moved from being a frequently fatal to a routinely controlled, chronic disease. Despite major strides in treatment there is an obvious need for newer therapies. Blockade of the alternative complement pathway may address two current requirements for newer agents in AAV, a faster mode of action and glucocorticoid sparing. The scientific rationale for this approach appears strong through effects of C5a on neutrophil activation and thrombosis, but the total clinical experience remains small, and the contribution of the classical complement pathway in AAV is unclear. Important questions relate to the completeness with which complement blockade will control neutrophil activation, whether a uniform effect will be seen in all patients, how effectively monocyte/ macrophage activity is controlled and whether control of this pathogenetic pathway will be enough to control vasculitis and whether there will be benefits on both remission induction and relapse prevention. To date, no safety signal has been communicated and significant reductions in glucocorticoid related adverse events have been seen. The absence of reliable biomarkers to assess both alternative complement pathway activity and complement mediated neutrophil activation has been a problem, and there remains opportunity to further explore these mechanisms in experimental models and in vitro studies. Funding This project was supported by the Cambridge Biomedical Research Centre. Disclosure of interest David Jayne has received research grants and consulting fees from Chemocentryx, GSK, Roche and Sanofi. He has received consulting fees from Astra-Zeneca, Boehringer-Ingelheim, Celgene, InflaRx and Insmed.

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