Introduction
Psoriasis is a chronic, immune-mediated inflammatory dermatological disease that affects nearly 150 million people worldwide. It is associated with a significant disease burden, a marked negative impact on patients quality of life,1 and places enormous pressure on health systems globally.24 In recent years attention has focused on the inflammatory processes underpinning the pathophysiological changes in psoriasis. In particular, cutaneous inflammation in psoriasis is linked to chronic systemic low-grade inflammation, which is thought to underlie the associations of psoriasis with comorbidities such as psoriatic arthritis, mood disorders including depression, and a range of cardiometabolic disorders that include myocardial infarction, hypertension, obesity, type 2 diabetes, non-alcoholic fatty liver disease (NAFLD), dyslipidemia, and hyperuricemia.3,5
One comorbidity of psoriasis that is increasingly recognized as clinically relevant is NAFLD.3,6,7 NAFLD is characterized by excessive hepatic fat storage and is strongly associated with obesity, type 2 diabetes, and metabolic syndrome. Over time, NAFLD can progress to a more severe, inflammatory disease termed non-alcoholic steatohepatitis (NASH) and eventually to the development of cirrhosis.8 NAFLD is the most common liver disease and its prevalence is rising rapidly. US studies have reported a 1035% prevalence in the general population with an average of between 20 and 30%.9 The global prevalence of NAFLD is estimated to be 25%.10,11 The presence of NASH in the general population is difficult to ascertain since it can be confirmed only by liver biopsy. However, rates between 1.5 and 6.5% have been reported.9,10,12 NASH is a potentially progressive disease that can lead to cirrhosis in 1225% of cases within a 10-year period, and it is associated with increased risks for hepatocellular carcinoma and cardiovascular- and liver-related deaths.8,13,14
NAFLD has been shown to occur 1.5 to 3 times more frequently in patients with psoriasis than in the general population.3,11,15 Prevalences of NAFLD ranging up to 65% have been reported in this patient population.16 The increased risk of NAFLD in psoriasis patients is not surprising, as the two diseases share a common link with the metabolic syndrome. However, there may be an association between psoriasis and NAFLD that is independent from the metabolic syndrome, hinging directly on the chronic low-grade systemic inflammatory burden characteristic of these two conditions.5 Importantly, when psoriasis co-occurs with NAFLD the disease severity and morbidity of both conditions may be greater.17
The aim of this review is to evaluate the recent literature on the clinical and pathophysiological associations linking psoriasis with NAFLD, independently of the metabolic syndrome, focusing on the chronic low-grade inflammation underpinning the two disorders. Second, we aimed to assess the potential hepatotoxic and hepatoprotective effects of currently approved systemic psoriasis therapies, in particular dimethyl fumarate (DMF), an oral small molecule with pleiotropic effects that could positively impact NAFLD, focusing on the chronic low-grade inflammation underpinning the two disorders. Second, we aimed to assess the potential hepatotoxic and hepatoprotective effects of currently approved systemic psoriasis therapies, in particular dimethyl fumarate (DMF), an oral small molecule with pleiotropic effects that could positively impact NAFLD.
For this narrative review, a targeted search of PubMed up to 14 July 2021 was conducted using the following search strategies: psoriasis with (a) non-alcoholic fatty liver disease/NAFLD (n = 96), (b) hepatotoxicity 1/1/2010 to 14/7/2021 (n = 72), and (c) hepatoprotection (n = 14); psoriasis treatment with (a) hepatotoxicity 1/1/2010 to 14/7/2021 (n = 68), and (b) hepatoprotection (n = 11). Relevant papers were identified by reviewing abstracts or full papers (if required), and by contributory articles cited in the selected references. The bibliography was augmented by key articles known to the authors and, finally, by individual drug data identified via a search of LiverTox (https://www.ncbi.nlm.nih.gov/books/NBK548744/).
NAFLD is the most common chronic liver disease worldwide and, in the majority of patients, is strongly associated with metabolic risk factors such as obesity, diabetes mellitus, and dyslipidemia. Individuals with metabolic syndrome have a 4- to 11-fold increased risk of developing NAFLD.18 NAFLD is characterized by fat deposition in the liver, in the absence of viral diseases such as hepatitis B or C, significant alcohol consumption, use of steatosis-stimulating drugs such as methotrexate, steroids, amiodarone and tamoxifen, or certain hereditary conditions including Wilsons disease and cholesteryl ester storage syndrome.19,20
NAFLD includes a wide spectrum of liver conditions with two main histological forms: simple hepatic steatosis (fat deposited, but no damage to liver cells) and NASH, which is characterized by hepatic inflammation that can lead to liver fibrosis. The aberrant pathophysiological processes underlying the progression to NASH are not fully understood, but are thought to include an imbalance of fatty acid metabolism leading to steatosis, and an elevated inflammatory response as a result of oxidative/metabolic stress and dysregulated cytokine production.21 Potential consequences of these processes are the development of lobular hepatitis with perivenular/pericellular (chicken wire) fibrosis, NAFLD-associated cirrhosis and liver failure and, albeit infrequently, hepatocellular carcinoma (Figure 1).5,22
Figure 1 Spectrum of non-alcoholic fatty liver disease (NAFLD). Data from these studies.5,22
In terms of clinical presentation, the majority of NAFLD cases are either asymptomatic or have nonspecific symptoms such as fatigue and abdominal pain, and/or abnormal liver function test results. NAFLD can be diagnosed if > 5% hepatic steatosis is shown by liver ultrasound in the absence of excessive alcohol use.8 The assessment for potential NASH requires additional testing using non-invasive assessment for liver fibrosis such as vibration-controlled transient elastography or magnetic resonance elastography. However, to confirm the diagnosis of NASH, histopathologic assessment of a liver biopsy is required.
Treatment of NAFLD is limited to optimal management of comorbid conditions such as type 2 diabetes and dyslipidemia, and lifestyle modifications aiming at 710% weight loss through caloric restriction and exercise.8 Weight loss and increased physical activity/exercise can help normalize liver enzyme levels, reduce hepatic inflammation and improve insulin resistance, steatosis and liver histology.23 There are currently no approved pharmacological therapies for NAFLD; oral vitamin E and pioglitazone are options that have shown modest clinical benefits.
The first published evidence in 2001 of a link between psoriasis and NAFLD involved three overweight/obese patients with NASH as confirmed by liver biopsy.24 Since then, various observational and controlled studies have highlighted an increased prevalence of NAFLD in patients with psoriasis.2529 For example, in a large Dutch population-based study (2292 participants aged 55 years) the prevalence of NAFLD was 46% in 118 patients with psoriasis and 33% in individuals without psoriasis.27 Importantly, while elderly study participants with psoriasis were 70% more likely to have NAFLD than those without psoriasis (crude odds ratio [OR] 1.70, 95% confidence interval [CI] 1.172.46), the increased risk was found to be independent of common risk factors such as smoking, alcohol consumption, and the presence of metabolic syndrome and its component disorders. A recent single-center cross-sectional study from Spain reported a 52% prevalence of NAFLD among a cohort of 71 patients with psoriasis.15 Of note, 14% of patients had liver fibrosis as diagnosed with transitional vibration-controlled elastography. A large population-based cohort study, using UK data from 197,130 patients with psoriasis and 1,279,754 matched controls, reported an elevated risk for incident cases of NAFLD among psoriasis patients without systemic therapy (adjusted hazard ratio [HR] 1.18, 95% CI 1.071.30) and an even higher risk for those receiving systemic therapy (adjusted HR 2.23, 95% CI 1.732.87) compared with the control group.30 The risk for incident NAFLD was also increased among patients with psoriatic arthritis, in particular for those receiving systemic therapy (adjusted HR 2.11, 95% CI 1.552.87). In line with these results, a 2015 systematic review and meta-analysis including 7 case-control studies found that patients with psoriasis had a 2-fold increased risk of NAFLD compared with controls (6 studies; n = 267,761; OR 2.15, 95% CI 1.572.94).31 The risk of NAFLD was significantly greater in patients with psoriatic arthritis (3 studies; n = 505 patients; OR 2.25, 95% CI 1.373.71) and in patients with severe psoriasis (2 studies; 51,930 patients, OR 2.07, 95% CI 1.592.71) compared to those with mild psoriasis. Recently, this meta-analysis was updated to include 2 additional studies (for a total of > 3 million patients and nearly 250,000 with NAFLD).32 The analysis was extended to investigate potential risk factors for NAFLD in psoriasis patients which included hypertension, male sex, hyperglycemia and obesity. Reaffirming the findings of the original systematic review, there was a strong association between psoriasis and NAFLD independent of confounders.
In several studies, the presence and severity of psoriasis were associated with a higher prevalence and greater severity of NAFLD, and NAFLD was a strong predictor of higher Psoriasis Area and Severity Index (PASI) scores.25,28,29,31,33 Using Control Attenuation Parameter to assess the degree of fatty liver and body surface area severity of psoriasis, Gandha et al confirmed a positive correlation between the two disorders.34 Furthermore, the progression to more severe forms of liver disease appeared to be higher in patients with psoriasis.35 Roberts et al reported that 48 of 103 (47%) psoriasis patients had NAFLD and 23 of 103 (22%) had biopsy-confirmed NASH, of whom 35% had stage 23 fibrosis.35 The prevalence of NASH was markedly higher than the 12% previously reported in patients with similar demographic characteristics but without psoriasis in the same medical center. Moreover, concomitant NAFLD in patients with psoriasis may confer a higher 10-year cardiovascular risk compared to psoriasis patients without NAFLD.36
In summary, the epidemiologic association between NAFLD and psoriasis is particularly strong given the high prevalence and increased incidence observed among patients with psoriasis. Importantly, this association is more evident in patients with severe psoriasis compared with those with mild psoriasis and is independent of common traditional risk factors such as smoking, alcohol consumption, and the presence of metabolic syndrome and its component disorders.5,31,32
Psoriasis and NAFLD are amongst a number of multifactorial disorders (including cardiovascular diseases and metabolic syndrome) whose pathogenesis is not fully understood, but involves complex interactions between genetic, immunological and environmental factors (Figure 2).5,3742
Figure 2 Common risk factors and associations between psoriasis (PsO) and non-alcoholic fatty liver disease (NAFLD). Reprinted from Prussick RB, Miele L. Non-alcoholic fatty liver disease in patients with psoriasis: a consequence of systemic inflammatory burden? Br J Dermatol. 2018;179(1):1629. 2018 The Authors. British Journal of Dermatology published by John Wiley & Sons Ltd on behalf of British Association of Dermatologists.5
The pathophysiology of psoriasis is characterized by sustained, self-amplifying inflammatory responses that lead to uncontrolled keratinocyte proliferation and dysfunctional differentiation. Disturbances in both innate and adaptive cutaneous immune responses are responsible for psoriatic inflammation.43 Activation of the innate immune system driven by endogenous signals and cytokines coexists with an auto-inflammatory response in some patients and with T cell-driven auto-immune reactions in others. Thus, psoriasis exhibits traits of an auto-immune disease on an auto-inflammatory background,44,45 with both mechanisms overlapping and possibly potentiating one another. T helper (Th)-1, Th17 and Th22 cells and some of their associated pro-inflammatory cytokines, such as interleukin (IL)-17A and IL-22 and tumor necrosis factor alpha (TNF-) are critically involved in sustaining and maintaining psoriasis.4548 The IL-23/IL-17 immune axis is considered to have a pivotal role in the pathogenesis of psoriasis; in line with this, IL-17- and IL-23-antagonists are highly effective treatments for psoriasis.49,50
The pathogenesis of NAFLD is complex and involves multiple pathways. Important pathophysiological mechanisms include genetic factors, insulin resistance and hyperinsulinemia, oxidative stress and hepatocyte lipotoxicity, hepatic inflammation, fibrosis, and gastrointestinal dysbiosis.21,38,5155 The various factors are encompassed in a multiple hit model for NAFLD development and progression.21,56 In the early stages of NAFLD, insulin resistancepossibly related to an increase in pro-inflammatory cytokinesplays a pivotal role by increasing the release of circulating free fatty acids, followed by abnormal accumulation of triglycerides in liver cells and hepatic steatosis. This may be followed by a phase in which simple steatosis transitions into steatohepatitis as a result of an increased inflammatory response. Additional pathways subsequently involved in NAFLD progression include mitochondrial dysfunction and liver apoptosis, increased oxidative stress, activation of the profibrogenic transforming growth factor- (TGF-) pathway, and hepatic stellate cell activation and injury.5
While the exact underlying mechanisms must still be fully clarified, both psoriasis and NAFLD are strongly associated with low-grade, chronic inflammation, peripheral insulin resistance, and increased levels of oxidative stress.40,57 Elevated insulin resistance and increased release of inflammatory cytokines are also characteristic of the metabolic syndrome and obesity. Adipose tissue produces adipocytokines (or adipokines) such as adiponectin, leptin and resistin, as well as pro-inflammatory cytokines which play important roles in the pathogenesis of both psoriasis and NAFLD.
Besides the important role of adipose tissue in mediating the interplay between skin and liver, (severe) psoriasis may have a direct impact on NAFLD, possibly via mechanisms beyond overweight and obesity. Indeed, NAFLD in the general population can also occur among individuals who are not obese and have a normal body mass index. These individuals are labelled as lean NAFLD.58 Interestingly, compared to healthy subjects, individuals with lean NAFLD have higher mean serum C-reactive protein (CRP) levels, suggesting that systemic inflammation might be one of the pathogenic factors.58
The secretion of pro-inflammatory cytokines from psoriatic tissue into the general circulation may reinforce the prevailing systemic pro-inflammatory milieu associated with NAFLD. IL-6, IL-17, TNF- and CRP produced by the liver (hepatokines) and psoriatic skin have reciprocal direct effects on these organs (Figure 3). The pro-inflammatory effects of adipocytokines and hepatokines are summarized in Table 1. Importantly, there may be a bi-directional relationship between psoriasis and NAFLD through pro-inflammatory pathways, postulated as the hepato-dermal axis.48 Circulating pro-inflammatory cytokines such as TNF- and IL-17 derived from psoriatic skin, upon reaching the liver, could impact liver inflammation and insulin resistance. Conversely, pro-inflammatory mediators stemming from hepatic inflammation could contribute to the onset or exacerbation of cutaneous inflammation in psoriasis. Pro-inflammatory immune modulators released by adipose tissue and the liver are involved in the promotion of hepatic fibrogenesis in NAFLD as well as psoriasis pathogenesis.5,40,48,59 TNF-, for example, is involved in psoriasis inflammation and has been shown to be an independent predictor of hepatic fibrogenesis and disease progression.60 Another relevant cytokine in this context is IL-17, which plays a central role in psoriasis pathogenesis. IL-17 is able to induce hepatic stellate cells activation and subsequent collagen production.50,61 By doing so, IL-17 facilitates the progression from simple liver steatosis to steatohepatitis.50,61,62
Table 1 Cytokine Levels and Effects of Adipocytokines and Hepatokines in Psoriasis and Non-Alcoholic Fatty Liver Disease (NAFLD)
Figure 3 Possible mechanisms linking dysfunctional visceral adipose tissue, psoriatic skin and steatosis.
Abbreviations: CRP, C-reactive protein; IL-6, interleukin-6; IL-17, interleukin-17; NAFLD, non-alcoholic fatty liver disease; NASH, non-alcoholic steatohepatitis; PAI-1, plasminogen activator inhibitor-1; TGF-, transforming growth factor-beta; TNF-, tumor necrosis factor alpha.
Notes: Reproduced from Mantovani A, Gisondi P, Lonardo A, et al. Relationship between non-alcoholic fatty liver disease and psoriasis: a novel hepato-dermal axis? Int J Mol Sci. 2016;17(2):217.48
High circulating (or hepatic) levels of proprotein convertase subtilisin kexin type-9 (PCSK9) have been shown to play a key role in muscle and liver lipid storage, adipose energy storage and hepatic fatty acids and triglycerides storage and secretion. These effects contribute to involvement of the enzyme in the pathogenesis of both NAFLD63 and psoriasis.64
Other shared pathways between psoriasis and NAFLD include modulation of lipid and glucose metabolism, which both play an important role in the development of metabolic syndrome and keratinocyte proliferation in psoriasis.
In summary, there is significant overlap in the pathophysiological factors underlying psoriasis and NAFLD, mostly relating to pathways involving inflammation, oxidative stress, and glucose and lipid metabolism.
Given the strong pathophysiological links between psoriasis and NAFLD and the high prevalence of NAFLD among psoriasis patients, dermatologists should always screen for possible liver disease in their psoriasis patients. A good understanding of the potential hepatic effects of systemic treatments prescribed for patients with psoriasis would also be clinically important. NAFLD-promoting drugs should be avoided, especially in high-risk patients. On the other hand, systemic therapies that reduce systemic inflammation may have a positive influence and mitigate the risk of developing NAFLD. Below, we summarize hepatotoxic and potential hepatoprotective effects of currently approved systemic psoriasis therapies with a focus on NAFLD.
Hepatotoxic risk is associated with the administration of a number of conventional drugs used in the treatment of psoriasis. Evidence for currently approved systemic psoriasis treatments is presented in Table 2.6587 Patients prescribed these medications should be monitored carefully for hepatotoxicity.
Table 2 Potential Hepatotoxic Effects of Some of the Most Commonly Used Systemic Therapies Used in the Treatment of Moderate to Severe Psoriasis
Perhaps the most substantive evidence, and concern, regarding potential hepatotoxicity relates to methotrexate.6570 Early signs of negative effects of methotrexate on liver function include elevated hepatic transaminase levels, but of even greater concern are methotrexate-induced histological changes including aggravation of underlying fatty liver to NAFLD and steatohepatitis with possible fibrosis and cirrhosis.71,72 These more serious adverse hepatic effects have been reported to occur in about 5% of patients treated with chronic, low-dose methotrexate, although rarely in patients without additional clinical risk factors for hepatotoxicity, such as pre-existing liver disease, excessive alcohol abuse, hepatitis B or C, central obesity and type 2 diabetes.71 Given the hepatotoxic concerns, use of methotrexate is preferably avoided in these high-risk psoriasis patient groups, including those with established NAFLD, and methotrexate is contraindicated if bilirubin values are > 5 mg/dl.73
Cyclosporin may cause dose-dependent, reversible increases in serum bilirubin and liver enzymes, with post-marketing experience reporting hepatotoxicity and liver injury.65,68,74 Cyclosporin can also potentially worsen NAFLD by increasing serum lipid levels.75 Close monitoring of liver function test enzymes and lipid parameters is recommended as abnormal values may necessitate dose reductions.68,74,76 Another frequently occurring adverse event associated with cyclosporin use is hypertension, which would be expected to negatively impact NAFLD.
Cases of liver enzyme increases ( 3 upper limit of normal [ULN]) and elevation of total bilirubin levels ( 2 ULN) have been reported infrequently for dimethyl fumarate (DMF), with resolution after treatment discontinuation. Assessment of serum aminotransferases (eg, alanine aminotransferase [ALT], aspartate aminotransferase [AST]) and total bilirubin levels are recommended prior to treatment initiation and during treatment.68,77 DMF is considered to be a possible rare cause of liver toxicity.78
Acitretin has been associated with transient increases in liver enzymes, but hepatotoxicity has been reported rarely.65 As acitretin frequently causes hyperlipidemia, use is preferably avoided in patients with or at high risk of NAFLD.11,75,79,80
No hepatotoxic effects have been documented for apremilast65 and no routine laboratory monitoring is required. Apremilast is considered to be an unlikely cause of apparent liver injury.78
There is evidence of hepatotoxic risk with TNF- inhibitors such as infliximab, adalimumab, certolizumab and etanercept65,8183 and guidelines advocate monitoring liver enzymes during treatment.65 Furthermore, compared with conventional systemic therapies for psoriasis (methotrexate and cyclosporin), treatment with TNF inhibitors (adalimumab, infliximab and etanercept) was found to be associated with significant increases in bodyweight and body mass index in a network meta-analysis (6 studies and 862 psoriasis patients).84 Increases in body weight might be associated with a reduction in the therapeutic response and/or exacerbations of comorbidities, although this needs to be confirmed in prospective studies. TNF inhibitors should be used cautiously in patients with or at high risk of NAFLD.
Other biologicals such as anti-IL17 agents (brodalumab, ixekizumab and secukinumab) and ustekinumab (anti-IL12/23) have been less widely investigated, but have generally exhibited minimal hepatotoxicity (Table 2). A retrospective study of 44 psoriasis patients receiving ustekinumab identified 6 cases (13.6%) of mild elevated transaminases, with no cases of severe hypertransaminasemia.85 Overall, the reported rate of mild-to-moderate serum aminotransferase elevations following ustekinumab therapy was 0.5% to 1.4%. There have been no reports of treatment-related symptomatic acute liver injury or jaundice linked to ustekinumab therapy.78 Interestingly, limited data found no increases in bodyweight in patients treated with ustekinumab.84,88
Analysis of over 3000 patients in clinical trials of the IL-17 antagonist secukinumab in psoriasis showed low rates of serum liver enzyme elevations compared to placebo and no cases of treatment-related liver injury. Post-marketing data have revealed no reports of liver injury due to secukinumab therapy.78 Similarly, clinical trials (> 3000 patients) and post-marketing studies of the anti-IL-17 biologic brodalumab have shown no evidence of liver enzyme elevation nor liver injury attributable to the agent.78 Comparable rates of serum liver enzyme elevations with the IL-17 antagonist ixekizumab and placebo were found in clinical trials, with no treatment-related cases of liver injury. Although post-marketing approval experience with ixekizumab is relatively limited, no cases of treatment-related liver injury have been reported.78 For newer anti-IL-23 biologics recently approved for the treatment of psoriasis (eg, guselkumab, risankizumab, and tildrakizumab), no evidence of acute liver injury or reactivation of hepatitis B or worsening of hepatitis C has been reported to date, but clinical experience with these agents is very limited (Table 2).
Assessment of hepatoprotection can be derived from several different research pathways including in vitro experiments, animal models and monitoring of potential biomarkers (Table 3).89108 Given the common etiology of inflammation between psoriasis and NAFLD, it might be postulated that systemic therapies for psoriasis that attenuate systemic inflammation may also have beneficial effects on NAFLD by targeting pro-inflammatory cytokines.109 However, to date, clinical data are scarce for any direct hepatoprotective effects of systemic psoriasis treatments.
Methotrexate has exhibited beneficial effects on cardiovascular inflammation91,92 as well as decreasing serum levels of PCSK9, which is a likely marker of improved lipid metabolism (Table 3).89 However, a large placebo-controlled RCT failed to show any benefits of methotrexate on the risk of cardiovascular events.110 Furthermore, the potential hepatotoxic risks associated with methotrexate therapy, as discussed earlier, would generally preclude its use in patients with NAFLD.
From the clinical study of Krahel et al,89 acitretin treatment was shown to increase PCSK9 levels, but there was no correlation between these elevated levels and markers of liver function such as transaminases in hepatic steatosis and NASH in high-risk patients (Table 3). Fibroblast growth factors (FGFs) 21 and 23 are markers for cardiometabolic disorders which are common in psoriasis. In one small trial, acitretin was reported to decrease FGF-21 by three-fold which was significantly greater than the reduction observed with methotrexate.90 In an earlier small clinical trial, it was shown that patients with chronic psoriasis treated with acitretin had reduced retinol-binding protein-4 levels and decreased insulin resistance.111 Given the link between psoriasis and increased insulin resistance/diabetes these changes could be clinically meaningful if confirmed in a larger study.111
There is a paucity of data on the potential hepatoprotective effects of cyclosporin. In a small group of patients with moderate to severe psoriasis, comorbidity with diabetes or metabolic syndrome did not affect the efficacy of cyclosporin.93 In another clinical study, cyclosporin significantly improved patients psoriasis symptoms and this was associated with increased transcription activity of TGF1 at the end of treatment in those with or without diabetes, and with or without metabolic syndrome.112 Through inhibition of the enzyme cyclophilin, cyclosporin has shown beneficial effects on liver fibrosis and cirrhosis in some patients. However, calcineurin-related toxicity has limited the possibility of long-term therapy and has required that dosages be kept low.113
Apremilast is a phosphodiesterase 4 inhibitor shown to be clinically effective in patients with psoriasis and/or psoriatic arthritis and also acts as a metabolic modulator. In individual cases, apremilast was shown to improve glucose metabolism114 and lipid profile.115 Similar findings were reported in a 1-year open observational study (Table 3).94
DMF, and its active metabolite monomethylfumarate (MMF), are of particular interest in the context of this review due to their unique multiple mechanisms of action (Figure 4).102,103,105,116,117 These include immunomodulatory and anti-inflammatory mechanisms that are potentially advantageous in psoriatic patients with comorbid NAFLD (Table 3). 116 For example, DMF/MMF regulates cellular responses to oxidative stress by modulating intracellular glutathione levels.102 DMF/MMF also reduces oxidative stress through activation of Nrf2 (nuclear factor erythroid 2related factor 2) which stimulates cytoprotective and anti-inflammatory factors such as HO-1 (heme oxygenase-1);103,106,116 and through inhibiting genes regulated by the transcription factor HIF-1 (hypoxia-inducible factor 1-alpha) and STAT3/STAT1 (signal transducer and activator of transcription) pathways.116 MMF is an agonist for hydroxy-carboxylic acid receptor 2 (HCA2/ GPR109A [G protein-coupled receptor 109A]) which inhibits neutrophil adhesion and recruitment by COX-1 (cyclooxygenase 1) and PGE2 (prostaglandin E2).116 Fumaric acid esters significantly reduced total cholesterol, low-density lipoprotein and apolipoprotein B levels in a prospective trial involving psoriasis patients.96 In animal models, DMF has shown potential to ameliorate acetaminophen-induced hepatic injury in mice,107 as well as liver ischemia/reperfusion injury in rats.104 Improvement of liver function and anti-oxidant status might prove to be a promising treatment approach in patients with psoriasis and comorbid NAFLD.
Figure 4 Proposed mechanisms of action of dimethyl fumarate/monomethyl fumarate (DMF/MMF).
Note: Data from these studies.102,103,105,116,117
Adalimumab was shown to reduce key markers of systemic inflammation including glycoprotein acetylation, CRP, IL-6 and TNF and this was associated with beneficial cardiovascular effects such as improved endothelial dysfunction as measured by flow-mediated dilation.95,96 TNF- inhibitors have been reported to improve insulin resistance in patients with rheumatoid arthritis118,119 and ankylosing spondylitis,118,120 but not in obese patients with either type 2 diabetes121 or metabolic syndrome.122,123 Seitz et al investigated the impact of TNF- inhibitors on the presence of liver fibrosis in patients with psoriatic arthritis and rheumatoid arthritis treated with methotrexate.124 Patients with psoriatic arthritis had a higher incidence of liver steatosis and hyperlipidemia and in this study. TNF- inhibitors exerted a protective effect against the development of liver fibrosis.
Secukinumab has been shown to have neutral effects on fasting plasma glucose, lipid parameters and liver enzymes, while reducing levels of CRP, a marker for systemic inflammation. It was also associated with a reduction in markers of oxidative stress. Secukinumab produced greater improvement in arterial elasticity, coronary artery function and myocardial deformation indices compared with methotrexate and cyclosporin. However, no data are available on the impact of these effects on liver function.97,98
Ustekinumab significantly decreases pro-inflammatory cytokines, such as TNF-, IL-1b, IL-17a and IL-6. VCAM-1 was significantly reduced by ustekinumab at 12 weeks, although this effect was not sustained at 1 year. Overall, ustekinumab transiently reduced aortic vascular inflammation at 12 weeks and, longer term, produced a more durable reduction in inflammatory cytokines associated with cardiovascular disease.101 No published studies have investigated the impact of this effect on liver inflammation and function.
NAFLD is an increasingly prevalent and clinically important comorbidity occurring in up to 65% of patients with psoriasis. The occurrence of NAFLD in psoriasis can have significant morbidity and mortality potential. There are multiple pathophysiological pathways that link psoriasis with NAFLD, in particular systemic inflammation and insulin resistance. Reducing systemic inflammatory burden may provide an opportunity to reduce the progression or even ameliorate NAFLD.
A number of conventional drugs used in the treatment of psoriasis are associated with hepatotoxic risk. Most evidence relates to use of methotrexate which, along with other NAFLD-promoting drugs, is best avoided in psoriasis patients with clinical risk factors for hepatotoxicity or established NAFLD. Despite the expectation that systemic psoriasis treatments might reduce the progression of or even ameliorate NAFLD by targeting pro-inflammatory cytokines, clinical data for direct hepatoprotective effects of these therapies are relatively scarce. Through its pleiotropic mechanisms of action contributing to its anti-inflammatory activity, DMF may have additional hepatoprotective effects of possible advantage in psoriatic patients with NAFLD.
However, real-world data on the effects of DMF in patients with psoriasis and concomitant NAFLD is currently lacking, and further studies with DMF and other systemic psoriasis therapies in routine clinical practice would be needed to inform therapeutic decision-making strategies for psoriasis patients with NAFLD.with DMF and other systemic psoriasis therapies in routine clinical practice would be needed to inform therapeutic decision-making strategies for psoriasis patients with NAFLD.
The authors thank Dr Rob Furlong and Dr Steve Clissold on behalf of Content Ed Net, Spain for editorial support, which was sponsored by Almirall, Barcelona, Spain, and performed in line with Good Publishing Practice (GPP-3) guidelines.
This article was supported by an unrestricted educational grant from Almirall, Barcelona, Spain.
DMWB is a consultant/speaker for AbbVie, Almirall, Celgene, Eli Lilly, Galderma, Janssen, LEO Pharma, Novartis, and Regeneron/Sanofi Genzyme. IK is an employee of Almirall, Barcelona, Spain. SP is a consultant/speaker for AbbVie, Almirall, Celgene, Eli Lilly, Galderma, Janssen, LEO Pharma, Novartis, UCB, and Pfizer. The authors report no other conflicts of interest in this work.
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