key: cord-0909290-ckl3v2jq
authors: Iqbal, Zohaib; Ho, Jan Hoong; Adam, Safwaan; France, Michael; Syed, Akheel; Neely, Dermot; Rees, Alan; Khatib, Rani; Cegla, Jaimini; Byrne, Christopher; Qureshi, Nadeem; Capps, Nigel; Ferns, Gordon; Payne, Jules; Schofield, Jonathan; Nicholson, Kirsty; Datta, Dev; Pottle, Alison; Halcox, Julian; Durrington, Paul; Soran, Handrean
title: Managing hyperlipidaemia in patients with COVID-19 and during its pandemic: An expert panel position statement from HEART UK
date: 2020-09-15
journal: Atherosclerosis
DOI: 10.1016/j.atherosclerosis.2020.09.008
sha: 0cfb6fc0ac28025c6f79c86acf1a3423bb538030
doc_id: 909290
cord_uid: ckl3v2jq

BACKGROUND & AIMS: The emergence of the novel severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) which causes Coronavirus Disease 2019 (COVID-19) has resulted in a worldwide pandemic. SARS-CoV-2 is highly contagious and its severity highly variable. The fatality rate is unpredictable but is amplified by several factors including advancing age, atherosclerotic cardiovascular disease, diabetes mellitus, hypertension and obesity. A large proportion of patients with these conditions are treated with lipid lowering medication and questions regarding the safety of continuing lipid-lowering medication in patients infected with COVID-19 have arisen. Some have suggested they may exacerbate their condition. It is important to consider known interactions with lipid-lowering agents and with specific therapies for COVID-19. This statement aims to collate current evidence surrounding the safety of lipid-lowering medications in patients, who have COVID-19. We offer a consensus view based on current knowledge and we rated the strength and level of evidence for these recommendations. METHODS: Pubmed, Google scholar and Web of Science were searched extensively for articles using search terms: SARS-CoV-2, COVID-19, coronavirus, Lipids, Statin, Fibrates, Ezetimibe, PCSK9 monoclonal antibodies, nicotinic acid, bile acid sequestrate, nutraceuticals, red yeast rice, Omega-3-Fatty acids, Lomitapide, hypercholesterolaemia, dyslipidaemia and Volanesorsen. RESULTS: & Conclusions: There is no evidence currently that lipid lowering therapy is unsafe in patients with COVID-19 infection. Lipid-lowering therapy should not be interrupted because of the pandemic or in patients at increased risk of COVID-19 infection. In patients with confirmed COVID-19, care should be taken to avoid drug interactions, between lipid-lowering medications and drugs that may be used to treat COVID-19, especially in patients with abnormalities in liver function tests.

• Patients should continue with their advised diet and lifestyle measures and should not interrupt their pharmacologic treatment because of the COVID-19 pandemic (I, A). • Oral lipid lowering medications can be suspended temporarily in patients with confirmed COVID who are too unwell for oral administration (I, E-EO). • In rare and inherited disorders such as Homozygous Familial Hypercholesterolemia (HoFH), Heterozygous Familial Hypercholesterolemia (HeFH), Familial Chylomicronaemia Syndrome (FCS) it would be good practice to consult with a lipid specialist to assess specific risks and therapeutic challenges (Ia, E-EO). • Continue lipid lowering therapy in patients with confirmed diagnosis of COVID-19 and abnormal liver functions tests (LFTs) unless alanine transaminase (ALT) or aspartate transaminase (AST) rises progressively (1, B-R). • Stop lipid lowering therapy and monitor if ALT or AST is greater than 3 times the upper limit of normal (I, B-R).

• Creatine kinase measurements should be considered when clinically indicated and in patients who are critically ill. Discontinue statin therapy temporarily if creatine kinase rises 10-fold to levels about 2,000 IU/L or more in asymptomatic patients or at a lower levels of 5-fold upper limit of normal in symptomatic patients (I, B-R). • Reassess and consider recommencing oral lipid lowering medications in patients who recover before or soon after they leave hospital (1, B-NR).

The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), which causes Coronavirus

Disease 2019 (COVID- 19) , infects cells of the respiratory tract via receptor-mediated endocytosis after interaction with the angiotensin converting enzyme receptor 2 (ACE2) protein [1] . Lipid lowering therapy is generally considered safe; however, there are theoretical concerns regarding their contribution to infectivity and safety in patients with COVID-19 pneumonia or acute respiratory distress syndrome (ARDS). Baseline characteristics of patients who required critical care unit admission due to COVID-19 from Lombardy, Italy, revealed that there was an 18% prevalence of hypercholesterolaemia as a co-morbid condition [2] . In a case series of patients suffering from COVID- 19, 35 .3% of patients were found to have underlying atherosclerotic cardiovascular disease and this was associated with a 50% fatality rate [3] . Similarly, data from New York showed that 26%

of patients hospitalised because of COVID-19 were reported to have hyperlipidaemia as a co-morbid condition and 10% were known to have coronary artery disease [4] . In non-hospitalised COVID-19

patients, however, the prevalence of hyperlipidaemia and coronary artery disease (CAD) was 11% and 2%, respectively. Of the hospitalised patients, there was a similar prevalence of hyperlipidaemia (27% vs. 24%) and CAD (12% vs. 9%) in those admitted to critical care vs. discharged from hospital (and thereby not requiring any ventilatory or other supportive therapy). In a multivariate regression analysis assessing risk factors for hospitalisation, including age, cancer, chronic kidney disease, CAD, hypertension, hyperlipidaemia, heart failure, obesity, pulmonary disease, race, male sex and tobacco use, the odds ratio (OR) for hyperlipidaemia (OR 0.67; p=0.003) suggested a relative reduction in the individual proportional risk for hospital admission [4] . However, the authors did not mention how many of the hyperlipidaemic patients were on statins or other lipid lowering therapies. Hu et al.

recently reported lower serum cholesterol levels amongst COVID-19 patients [5] , leading some to suggest temporary cessation of lipid lowering therapy [6] . However, lipid parameters often fall in cytokine-mediated inflammation as a consequence of the acute phase response rather than having a causative or pathological contribution towards infection [7] [8] [9] . It is reasonable to assume that patients with previous history of myocardial injury are at higher risk for further events, thereby justifying the need for maintaining their lipid lowering therapy as far as possible [3] .

J o u r n a l P r e -p r o o f 

Patients with no symptoms or diagnosis of COVID-19 should continue their lipid-lowering medications, as well as other cardio-protective therapies, as usually prescribed. Our general advice is consistent with previous assessments and recommendations [11] [12] [13] .

There is no need to withhold lipid-lowering medications during the COVID-19 pandemic. This is especially important in patients who are at high risk of cardiovascular disease, in whom stopping lipid-lowering therapy can increase the risk of an atherosclerotic vascular event.

J o u r n a l P r e -p r o o f Patients treated for hyperlipidaemia should continue with their advised diet and lifestyle   measures and should not interrupt their pharmacologic treatment because of the COVID-19 pandemic (I, A).

-Lipid lowering medications can be suspended temporarily in patients with confirmed COVID-19, who are too unwell to receive medications orally (I, E-EO).

-Creatine kinase measurements should be considered when clinically indicated and in patients who are critically ill. We recommend stopping statin therapy if creatine kinase rises 10-fold to levels above 2,000 IU/L in asymptomatic patients or at a lower level of 5-fold upper limit of normal in symptomatic patients (I, B-R).

-It is important to reassess and recommence oral lipid lowering medications in patients who recover before or soon after they leave hospital (I, B-NR).

-In rare and inherited disorders such as homozygous familial hypercholesterolemia (HoFH) (see below), heterozygous familial hypercholesterolemia (HeFH), familial chylomicronaemia syndrome (FCS). it would be good practice to consult with a lipid specialist to assess specific risks and therapeutic (see recommendations 10 and 11 below) challenges (Ia, E-EO).

Abnormal liver function tests are increasingly recognised as a feature of COVID-19 infection with a prevalence as high as 37.2% at admission [14] . There is some evidence to suggest that men are affected more than women, and older age and higher initial viral load increase predisposition [15] . It is not clear if COVID-19 causes direct liver injury or if this is part of the wider systemic inflammatory response syndrome. Nonetheless, it is important to recognise hepatic injury in COVID-19 patients as the majority of lipid lowering therapies are metabolised in the liver.

-Continue lipid lowering therapy in patients with confirmed diagnosis of COVID-19 and abnormal liver functions tests (LFTs) unless alanine Transaminase (ALT) or Aspartate Transaminase (AST) rises progressively (1, B-R).

-Stop therapy and monitor if ALT or AST is greater than 3 times the upper limit of normal (I, B-R).

-Reassess and consider recommencing oral lipid lowering medications in patients who recover before or soon after they leave hospital (1, B-NR).

Statins are 3-hydroxy-3-methyl-glutaryl-CoA reductase inhibitors. They have shown great efficacy in treating a variety of lipid disorders whilst also providing mortality benefits against cardiovascular disease [16, 17] . Studies on the pharmacodynamic properties of statins have shown they have pleiotropic properties with effects that may modulate inflammation [18] , sepsis [19] , immunity [20] , and vasomotor tone [21] . Of relevance in the current COVID-19 pandemic is the effect of statins on ACE2 receptor expression. Pharmacologic blockade of the renin-angiotensin-aldosterone system has generally been shown to upregulate ACE2 expression in a variety of tissues [22] . This has led some to question the safety of such therapies in patients who test positive for COVID-19 with advocates for both sides [23] [24] [25] . Shin et al. showed that a combination of fluvastatin and insulin upregulated ACE2 expression in murine cardiac muscle cells [26] . A study by Tikoo et al. found that atorvastatin can upregulate ACE2 expression in cardiac tissue when animals were fed high cholesterol diets [27] . rosuvastatin upregulated ACE2 expression in murine vascular smooth muscle cells [29] . Conclusions from these data highlight the beneficial role of statins in mediating attenuation of cardiovascular risk, however, amidst the current COVID-19 pandemic, there is concern about pharmacologic upregulation of the ACE2 receptor, for example with ACE-inhibitor treatment. A joint statement by the Council on Hypertension and the European Society of Cardiology has advised physicians to continue treatment with their current regimen, even though these drugs can raise ACE2 levels [30] .

The safety of the ACE-inhibitor therapy has been subsequently been evaluated in observational studies, which did not show any adverse outcome [31, 32] . Given the current lack of sufficient convincing evidence to confirm adverse outcomes and benefits of these drugs, the American Society for Preventive Cardiology advised that patients should continue their cardioprotective drugs [13] .

Emerging evidence suggests that ACE2 blockade may indeed be beneficial [25, 33] . Importantly, no human or animal data exist on the relationship between pulmonary ACE2 receptors and statin therapy. Furthermore, statins could be efficient SARS-CoV-2 main protease inhibitors and, in theory, may alleviate COVID-19 symptoms [34] .

One study has demonstrated endothelial cell involvement across vascular beds of different organs in a series of patients with COVID-19, suggesting that SARS-CoV-2 infection facilitates the induction of inflammation of the endothelium in several organs as a direct consequence of viral involvement and of the host inflammatory response [35] . In addition, induction of apoptosis and pyroptosis may have inflammatory anti-cytokine drugs, ACE inhibitors, and statins. Indeed, a recent study reported that use of ACE inhibitors or statins was associated with better survival among patients with Covid-19 [10] .

Bilateral diffuse alveolar damage with cellular fibromyxoid exudates has been found in COVID-19

infection [36] . These changes may cause acute respiratory distress syndrome (ARDS), with a reported prevalence in COVID-19 of 8.2% [37] . A systematic review from 2019 concluded that in ARDS patients, statins make little or no difference to early mortality or duration of ventilation, suggesting their safety in this setting [38] . A UK-based observational study of 2067 patients suggested that statins may impart a mortality benefit in patients with community acquired pneumonia [39] . In contrast, however, a multicentre cohort study from the United States found no evidence of protection conferred by statins on clinical outcomes in a similar cohort [40] . A metaanalysis found that although statin treatment was associated with decreased mortality after pneumonia, there was attenuation of this effect in certain subgroups and it was indicated that no robust conclusions could be drawn without a dedicated randomised clinical trial [41] . Data on protectiveness of statins in viral pneumonias are also inconsistent with studies reporting benefit [42] [43] [44] or no benefit [45] . Pertinently, in another coronavirus related disease, Middle Eastern

Respiratory Syndrome (MERS), statins were postulated to protect against mortality [46] . There are also some studies which have shown a beneficial role of statins in sepsis [47] , and this is not unfounded given their anti-oxidant, anti-inflammatory and immunomodulatory properties [48, 49] .

Longer-term data are required, however, before such claims can be substantiated. Notwithstanding the somewhat conflicting data on the benefits of statin use in pneumonia, no studies so far have demonstrated a negative effect on outcome. Patients with tuberculosis, receiving statin treatment responded more rapidly to anti-tuberculous drugs and had lower rates of reactivation [50] . This effect is likely to be due to the decrease in circulating low-density lipoprotein cholesterol (LDL-C) rather than to a direct effect on the bacterium itself or the macrophage foam cellsm which are its host in the tuberculoma, because very little statin survives its first pass through the liver to reach the lungs [51] .

Red yeast rice (RYR), a nutraceutical that inhibits HMG-CoA reductase and reduces LDL-C [52] , is used by some patients who are intolerant to statins [53] . 

Lipid metabolism changes in patients with acute illness and sepsis; high density lipoprotein cholesterol (HDL-C) tends to lose its anti-inflammatory effect and LDL-C tends to be more susceptible to atherosclerotic modifications [51] . Furthermore, atherosclerotic plaques may become more vulnerable to rupture predisposing to an acute cardiovascular event, so it is importance to continue with lipid modifying agents except in cases where risks outweigh benefits.

Statin therapy should be continued in patients with confirmed diagnosis of COVID-19 (1, C-LD) but should be stopped, or dose reduced if:

-ALT or AST rises progressively. Stop statin therapy and monitor if ALT or AST is greater than 3

times the upper limit of normal (1, B-R).

-There is a significant drug-drug interaction identified (table 2) . Consider reducing the dose or change to another statin (table 2) (1, C-LD).

-We recommend stopping statin therapy if creatine kinase rises 10-fold to levels about 2,000 IU/L or more in asymptomatic patients or at a lower level of 5-fold upper limit of normal in symptomatic patients (1, B-R).

-If there is evidence of myositis, renal function should be monitored (1, B-NR).

-If treatment is suspended, a further individualised risk vs. benefit assessment should be conducted to restart treatment soon after the patient's condition has stabilised (1, B-NR).

Fibrates are peroxisome proliferator-activated receptor alpha (PPAR-α) agonists and are used primarily in the treatment of hypertriglyceridemia [54] . Elevated triglyceride levels are associated with inflammation [55] , and used as part of the H-Score, which determines the presence of secondary haemophagocytic lymphohistiocytosis, an under-recognised hypercytokinaemia syndrome thought to occur in COVID-19 infection [56] . Similar to statins, fibrates are also known to have anti-inflammatory properties and have been suggested as a potential anti-viral agent [44] .

Indeed, it has been shown that gemfibrozil confers survival benefits in mice infected with severe H2N2 influenza [57] , and prolonged survival has been demonstrated in mice when combined with oseltamivir [58] . Despite these animal data, there are no studies on the effects of fibrates on respiratory viral infections in humans. A case report described an association between eosinophilic pneumonia and clofibrate [59] . Fibrates are generally well tolerated with the major concerns being muscle-related side effects [60] . Although the absolute risk is very small, there is an aggregated risk of myopathy and myositis when used in combination with statins, in particular gemfibrozil (which is no longer recommended in combination with statin therapy) [61, 62] . Notwithstanding their good J o u r n a l P r e -p r o o f tolerability, evidence suggests that they may cause a mildly reversible elevated creatinine [63] , a slight increase propensity towards cholelithiasis [64] and an augmented response of anti-coagulants such as warfarin [65] .

Fibrates are primarily used for hypertriglyceridaemia [66] . Fibrates are metabolised by cytochrome P450 isoenzyme 2C9 (CYP2C9) whilst may also mildly inhibit this enzyme [67] , they are renally excreted, and therefore doses should be reduced in patients with an eGFR <60 ml/min/1.73m 2 and stopped if the eGFR drops below 15 ml/min/1.73m 2 [62] . No drug interactions have been reported between the commonly used fibrates and the proposed drugs on trial for treating COVID-19 (table   3) .

Fibrate therapy should be continued in patients with and without a confirmed diagnosis of COVID-19

(1, C-LD) unless:

-There is a significant drug-drug interaction identified (table 3) (1, C-LD).

-ALT or AST rises progressively, when fibrate therapy should be stopped if ALT or AST is greater than 3 times the upper limit of normal (1, B-R).

-There is clinical evidence and/or biochemical evidence of myopathy or if creatine kinase is greater than five times upper limit of normal (1, B-R).

-Acute kidney injury with deteriorating estimated glomerular filtration rate (eGFR) (1, B-NR).

-Assess drug interactions if oral anticoagulants are initiated (1, C-LD).

-If treatment is suspended, further assessment should be conducted to restart treatment soon after the patient's condition has stabilised (1, B-NR).

Ezetimibe selectively blocks the Niemann-Pick C1-like Protein (NPC1L1) in the jejunal brush border, resulting in the inhibition of dietary cholesterol absorption [68] and was shown to reduce LDL-C and ASCVD risk [68] [69] [70] . Ezetimibe is considered a safe therapeutic option with few side effects and no known drug interactions with the proposed medications being trialled for COVID-19. No trials reporting long-term outcome of ezetimibe use in viral or bacterial pneumonia have been conducted.

Ezetimibe therapy should be continued in patients with confirmed diagnosis of COVID-19 (1, C-LD) unless:

J o u r n a l P r e -p r o o f -There is a significant drug-drug interaction identified (table 4) (1, C-LD).

-ALT and/or AST rises above 3 times the upper limit of normal (1, B-R).

-If treatment is suspended, further assessment should be conducted to restart treatment soon after the patient's condition has stabilised (1, B-NR).

Proprotein convertase subtilisin/kexin type 9 (PCSK9) monoclonal antibodies are novel drugs that reduce LDL-C to previously unprecedented levels [71] . They reduce cardiovascular events [72] [73] [74] , are well tolerated and safe [75] . However, given their novelty, longer term safety data is still required. The PCSK9 protein is often upregulated during sepsis and inflammation and is postulated to have a detrimental effect on host response and survival [76, 77] . This has led some to argue for a possible role of PCSK9 monoclonal antibodies in treating the dysregulated immune response during infection [78] . However, a review by Ruscica et al. found no significant reductions in high-sensitivity C-reactive protein in patients receiving PCSK9 monoclonal antibodies from clinical trial data [79] .

Whilst there is some evidence that PCKS9 inhibitors may modulate the inflammatory response in atherosclerosis, their utility in dampening inflammation and benefit during sepsis is a matter of debate. Although an increased frequency of nasopharyngeal symptoms and flu-like syndrome have been reported amongst recipients in PCSK9 monoclonal antibody studies [75] , it is unclear whether this translates into an increased susceptibility to respiratory viruses such as COVID-19. Flu-like symptoms are a class effect of monoclonal antibodies and therefore such results are unsurprising [80] .

Whilst very limited drug-drug interaction data is available, pharmacokinetic data indicates that likely they are safe, as drug elimination occurs via saturable binding to PCSK9, with no clinically significant differences in patients with hepatic or renal impairment or with other concomitant drug use [81] .

Vuorio et al. recommended the continuation of these drugs in patients who have familial hypercholesterolaemia (FH) and have contracted COVID-19 [12] . The rationale for this was that patients with FH are at higher risk of atherosclerotic cardiovascular events.

PCSK9 monoclonal antibodies should be continued in all patients with a confirmed diagnosis of COVID-19 (table 4 ).

-In critically ill patients, treatment can be paused until recovery and discharge from the critical care unit (1, E-EO).

-If treatment is suspended or delayed, a further individualised risk vs. benefit assessment should be conducted to restart treatment soon after patient's condition has stabilised (1, B-NR).

Eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA) in sufficient amounts reduce triglyceride levels [82] [83] [84] , and have been associated with favourable effects on various markers of cardiovascular risk such as reduced blood pressure [85, 86] , and decreased platelet aggregation [87] .

Their anti-inflammatory properties [88] , and potential role in atherosclerotic plaque stability, have also been described [89, 90] . Despite this, there remains some controversy surrounding the evidence for cardiovascular outcome benefits [91] [92] [93] [94] . Most recently, the REDUCE-IT (Reduction of Cardiovascular Events with EPA-Intervention Trial) study demonstrated a significant decrease in residual risk of cardiovascular events in patients with atherosclerotic cardiovascular disease and elevated triglyceride levels [95] . There is no available evidence on the use of omega-3 fatty acids in acute infection or illness although there are no clear mechanistic reasons that raise safety concerns.

There are no significant drug interactions between possible trial therapies for COVID19 and omega-3 fatty acids (table 4) . It has been suggested that they may prolong bleeding time [96] , however, clinical trials have not shown adverse outcomes in relation to this [97, 98] .

Omega-3 fatty acids can be continued in patients with confirmed diagnosis of COVID-19 unless:

-The patient is critically ill (1, C-EO).

-If treatment is suspended, a further individualised risk vs. benefit assessment should be conducted to restart treatment when patient's condition has improved (1, B-NR).

The bile acid sequestrants such as cholestyramine, colesevalam and colestipol are highly positive charged molecules, which interact with negatively charged bile acids preventing their absorption in the intestines [99] . They are not absorbed themselves and therefore do not interact pharmacologically with other agents; however, they may inhibit the absorption of a number of orally administered drugs [100] .

In the absence of cardiovascular outcome data and given the potential for interfering with drug absorption, it would be reasonable that bile acid sequestrants are discontinued in patients diagnosed with COVID-19 (1, C-LD).

Niacin positively impacts apo-B containing lipoproteins whilst favourably increasing apo A1 [101, 102] . This translates into reductions in LDL-C and triglycerides whilst concomitantly raising HDL-C [103, 104] . Despite the lack of cardiovascular efficacy when added to background statin therapy [105] , its ubiquitous use continues worldwide [101, 106] . Niacin often causes facial flushing as a side effect, which sometimes limits its use in general practice [107] . Niacin undergoes conjugation with glycine in the liver producing its major metabolite, nicotinuric acid, which is excreted in urine [103] .

Niacin has been shown to attenuate endotoxemic lung inflammation in animal models [108] , however, hard data in human viral infections is lacking. No reports questioning its safety profile have been reported during the previous SARS and MERS outbreaks.

Niacin therapy can be continued in patients without COVID-19, however, in the absence of consistent clinical trials evidence to support cardiovascular events prevention, we recommend discontinuing niacin temporarily in patients diagnosed with COVID-19 (1, C-LD).

Homozygous familial hypercholesterolemia confers high cardiovascular risk from a very young age [109, 110] . Atherosclerotic plaque burden is high and there is particular concern about stopping lipid lowering therapies. Treatment is based on maximum tolerated oral lipid lowering agents, PCSK9

inhibitors and lipoprotein apheresis [109] [110] [111] . In addition, lomitapide has been developed specifically for the condition [111] .

Lomitapide inhibits microsomal triglyceride transfer protein (MTP) in hepatocytes and enterocytes, reducing apoB-containing lipoprotein particles secreted into the circulation [112] . It is currently used as adjunctive therapy for HoFH, achieving LDL-C reductions of 35.6% to 45.5% in Phase III and extension trials [113, 114] . This is consistent with real world clinical experience reported so far, with 68% and 42% of patients achieving LDL-C <100 mg/dl (2.5 mmol/l) and <70 mg/dl (1.8 mmol/l), respectively [115] . Its mechanism of action also explains the adverse events of hepatic steatosis and elevated transaminases.

Lomitapide is metabolised in the liver through CYP3A4 and lomitapide is also an inhibitor of CYP3A4 [116] . Its excretion occurs through both renal and intestinal routes. There are therefore significant potential drug interactions, with strong and moderate CYP3A4 inhibitors being contraindicated.

Macrolide antibiotics, potent enzyme inhibitors, are common antimicrobial options in the treatment of pneumonia and therefore likely the most frequent drug interaction to be encountered in the management of COVID-19. Similarly, the concurrent use of protease inhibitors lopinavir and ritonavir, both predicted to markedly increase exposure to lomitapide through potent CYP3A4 inhibition, is contraindicated.

Due to the rarity of HoFH, there is currently no available data on the effect of lomitapide on outcomes in acute infection or illness. Monitoring is required with the use of lomitapide because of possible liver injury. This is dose related and, if interacting drugs are necessary, it should be discontinued.

Patients with HoFH are at high risk of cardiovascular events and any proposed changes to therapy in these patients should be discussed with a lipid specialist familiar with the management of the condition. If a patient with HoFH is admitted into hospital, a discussion between the acute hospital team and lipid specialist should occur at the earliest opportunity. For specific treatment strategies we recommend:

-For statins, evolocumab, ezetimibe, fibrates, omega-3 fatty, bile acids sequestrants please refer to the recommendations above.

-Lipoprotein apheresis is safe and should be continued if logistically possible (1a, C-LD).

-Lomitapide should be continued in patients with confirmed diagnosis of COVID-19 (1a, C-EO) unless:

o There is a drug-drug interaction identified (table 4) . Lomitapide can be temporarily discontinued in acutely ill patients and/or those who are started on anti-microbial medication with significant drug-drug interactions (table 4) increased risk of acute pancreatitis [117] . The cornerstone of current management is a low-fat intake. Volanesorsen is a newly licensed antisense oligonucleotide inhibitor of apolipoprotein CIII (Apo CIII) [118] . [119] . It is delivered on a 2-weekly basis via a subcutaneous injection and its major side effects include injection site reactions and thrombocytopaenia [119] . Emerging evidence suggests that low platelet count is associated with an increased risk of severe disease and mortality in patients with COVID-19 [120] [121] [122] . Whether this is directly causative is unknown; however, mechanisms for COVID-19-induced thrombocytopaenia have been suggested [123] . Based on these data, it is currently felt that the safest option would be to withhold treatment until the patient recovers.

Any proposed changes to therapy in patients with FCS should be discussed with a lipid specialist familiar with the management of the condition. If a patient with FCS is admitted into hospital, a discussion between the acute hospital team, lipid specialist and dietitians should occur at the earliest opportunity. For specific treatment strategies, we recommend:

-Very-low fat diet should be maintained in all patients including those on par-enteral feeding

(1, C-LD).

-Oil based medications drugs, like propofol, should be avoided in patients who need assisted ventilation and sedation (1, C-LD).

-For statins, fibrates and other lipid lowering medications, please refer to the recommendations above.

-We recommend Volanesorsen is temporarily withheld in FCS patients with confirmed diagnosis of COVID-19 (1, C-EO).

-Further assessment should be conducted to restart treatment when the patient has recovered (1, C-LD).

-Low platelet count during COVID-19 infection should not be used to permanently withhold treatment (C-LD).

Many studies show a favourable effect of statin therapy in acutely ill patients and some studies show no statistically significant impact on outcome; reassuringly, however, no study to date has demonstrated harm. Lipid-lowering therapy has a well-established role in both the primary and secondary prevention of atherosclerotic cardiovascular disease and therefore, in the absence of J o u r n a l P r e -p r o o f much needed trial data, it follows that these drugs should be continued wherever possible.

Importantly, COVID19 is a new disease with a scarce evidence base upon which to make recommendations; however, with the rapid evolution of clinical studies, inevitably guidelines may need further revision. CYP34A [124, 125] CYP34A [126] CYP2C9 [125] CYP2C9 [124, 125] CYP2C9 minimal [125] CYP34A [125] J o u r n a l P r e -p r o o f a.

Increased risk of Hepatoxicity 

Characterization of spike glycoprotein of SARS-CoV-2 on virus entry and its immune cross-reactivity with SARS-CoV

Baseline Characteristics and Outcomes of 1591

Patients Infected With SARS-CoV-2 Admitted to ICUs of the Lombardy Region

Cardiovascular Implications of Fatal Outcomes of Patients With Coronavirus Disease 2019 (COVID-19)

Factors associated with hospital admission and critical illness among 5279 people with coronavirus disease 2019 in New York City: prospective cohort study

Covid-19: a remote assessment in primary care

Regulation of low-density lipoprotein cholesterol by intestinal inflammation and the acute phase response

Association Between Low-Density Lipoprotein Cholesterol Levels and Risk for Sepsis Among Patients Admitted to the Hospital With Infection

Lipid profile associated with the systemic inflammatory response syndrome and sepsis in critically ill patients

Further evolution of the ACC/AHA clinical practice guideline recommendation classification system: a report of the American College of Cardiology/American Heart Association Task Force on Clinical Practice Guidelines

Brief recommendations on the management of adult patients with familial hypercholesterolemia during the COVID-19 pandemic

Familial hypercholesterolemia and COVID-19: triggering of increased sustained cardiovascular risk

Continuity of care and outpatient management for patients with and at high risk for cardiovascular disease during the COVID-19 pandemic: A scientific statement from the American Society for Preventive Cardiology

Clinical Features of COVID-19-Related Liver Damage

COVID-19 and liver dysfunction: Current insights and emergent therapeutic strategies

ACC/AHA guideline on the treatment of blood cholesterol to reduce atherosclerotic cardiovascular risk in adults: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines

Cholesterol, not just cardiovascular risk, is important in deciding who should receive statin treatment

Inflammation, immunity, and HMG-CoA reductase inhibitors: statins as antiinflammatory agents?

Statins, inflammation, and sepsis: hypothesis

Immune modulatory effects of statins

Effects of statins on vascular wall: vasomotor function, inflammation, and plaque stability

COVID-19, ACE2 and the Cardiovascular Consequences

COVID-19 and Angiotensin-Converting Enzyme Inhibitors and Angiotensin Receptor Blockers: What Is the Evidence?

Renin-Angiotensin-Aldosterone System Inhibitors in Patients with Covid-19

Angiotensin-converting enzyme inhibitors and angiotensin II receptor blockers are not associated with severe COVID-19 infection in a multi-site UK acute hospital trust

The effect of fluvastatin on cardiac fibrosis and angiotensin-converting enzyme-2 expression in glucose-controlled diabetic rat hearts

Tissue specific up regulation of ACE2 in rabbit model of atherosclerosis by atorvastatin: role of epigenetic histone modifications

Atorvastatin induced increase in homologous angiotensin I converting enzyme (ACE2) mRNA is associated to decreased fibrosis and decreased left ventricular hypertrophy in a rat model of diabetic cardiomyopathy

Effects of rosuvastatin on expression of angiotensinconverting enzyme 2 after vascular balloon injury in rats

Position statement of the ESC council on hypertension on ACE-inhibitors and angiotensin receptor blockers

Renin-angiotensin-aldosterone system blockers and the risk of Covid-19

Renin-angiotensin-aldosterone system inhibitors and risk of Covid-19

Renin-angiotensin system inhibitors improve the clinical outcomes of COVID-19 patients with hypertension

Statins and the COVID-19 main protease: in silico evidence on direct interaction

Endothelial cell infection and endotheliitis in COVID-19

Pathological findings of COVID-19 associated with acute respiratory distress syndrome. The Lancet respiratory medicine 2020

ECMO for ARDS due to COVID-19

Pharmacological agents for adults with acute respiratory distress syndrome

Statin therapy in patients with communityacquired pneumonia

Understanding the potential role of statins in pneumonia and sepsis

Is Statin Use Associated with Reduced Mortality After Pneumonia? A Systematic Review and Meta-analysis

Influenza morbidity and mortality in elderly patients receiving statins: a cohort study

Statins and the risk of pneumonia: a populationbased, nested case-control study

Treating influenza with statins and other immunomodulatory agents

Statin use and risk of community acquired pneumonia in older people: population based case-control study

Decrease the Fatality Rate of Middle East Respiratory Syndrome Infection

Statins and sepsis in patients with cardiovascular disease: a population-based cohort analysis

Beyond the laboratory: clinical implications for statin pleiotropy

Evidence for more intensive cholesterol lowering

Statin treatment is associated with a decreased risk of active tuberculosis: an analysis of a nationally representative cohort

Acquired low cholesterol: diagnosis and relevance to safety of low LDL therapeutic targets

The Role of Nutraceuticals in Statin Intolerant Patients

Red Yeast Rice Preparations: Are They Suitable Substitutions for Statins?

High-density lipoprotein cholesterol raising: does it matter?

Similar but not the same: Differential diagnosis of HLH and sepsis

COVID-19: consider cytokine storm syndromes and immunosuppression

Increased survival after gemfibrozil treatment of severe mouse influenza

Combinations of oseltamivir and fibrates prolong the mean survival time of mice infected with the lethal H7N9 influenza virus

Lipid-lowering drugs and risk of myopathy: a population-based follow-up study

Myopathy and rhabdomyolysis associated with lovastatin-gemfibrozil combination therapy

Safety considerations with fibrate therapy

Fenofibrate increases creatininemia by increasing metabolic production of creatinine

Effect of gemfibrozil on biliary lipid metabolism in normolipemic subjects

Interaction between fenofibrate and warfarin

European Guidelines on cardiovascular disease prevention in clinical practice: The Sixth Joint Task Force of the European Society of Cardiology and Other Societies on Cardiovascular Disease Prevention in Clinical Practice (constituted by representatives of 10 societies and by invited experts) Developed with the special contribution of the European Association for Cardiovascular Prevention & Rehabilitation (EACPR)

Benefits and risks of the treatment with fibrates--a comprehensive summary

Ezetimibe therapy: mechanism of action and clinical update

Perrone-Filardi P. Safety and efficacy of ezetimibe: A meta-analysis

Acute Coronary Syndromes

PCSK9 inhibitors: mechanisms of action, metabolic effects, and clinical outcomes

Clinical efficacy and safety of achieving very low LDL-cholesterol concentrations with the PCSK9 inhibitor evolocumab: a prespecified secondary analysis of the FOURIER trial

Evolocumab and Clinical Outcomes in Patients with Cardiovascular Disease

Cardiovascular Efficacy and Safety of Bococizumab in High-Risk Patients

Efficacy and safety of PCSK9 monoclonal antibodies

PCSK9 at the crossroad of cholesterol metabolism and immune function during infections

PCSK9 and infection: A potentially useful or dangerous association?

PCSK9 inhibitors in sepsis: a new potential indication?

PCSK9 inhibition and inflammation: A narrative review

The safety and side effects of monoclonal antibodies

n-3 fatty acids and serum lipoproteins: human studies

A review of the effect of omega-3

polyunsaturated fatty acids on blood triacylglycerol levels in normolipidemic and borderline hyperlipidemic individuals

Effects of icosapent ethyl on lipid and inflammatory parameters in patients with diabetes mellitus-2, residual elevated J o u r n a l P r e -p r o o f triglycerides (200-500 mg/dL), and on statin therapy at LDL-C goal: the ANCHOR study

Omega-3 fatty acids and cardiovascular disease: effects on risk factors, molecular pathways, and clinical events

Long-chain omega-3 fatty acids eicosapentaenoic acid and docosahexaenoic acid and blood pressure: a meta-analysis of randomized controlled trials

Long-term effects of dietary marine omega-3 fatty acids upon plasma and cellular lipids, platelet function, and eicosanoid formation in humans

Effect of marine-derived n-3 polyunsaturated fatty acids on C-reactive protein, interleukin 6 and tumor necrosis factor α: a meta-analysis

Association of n-3 polyunsaturated fatty acids with stability of atherosclerotic plaques: a randomised controlled trial

Eicosapentaenoic acid therapy is associated with decreased coronary plaque instability assessed using optical frequency domain imaging

Omega-3 dietary supplements and the risk of cardiovascular events: a systematic review

disease: a meta-analysis of randomized, double-blind, placebo-controlled trials

Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Fatty Acids and Outcomes Research Consortium (FORCe)

Polyunsaturated fatty acid biomarkers and coronary heart disease: pooling project of 19 cohort studies

Association of dietary, circulating, and supplement fatty acids with coronary risk: a systematic review and meta-analysis

Cardiovascular risk reduction with icosapent ethyl for hypertriglyceridemia

Expert opinion: omega-3 fatty acids and bleeding-cause for concern?

Fish oil LC-PUFAs do not affect blood coagulation parameters and bleeding manifestations: Analysis of 8 clinical studies with selected patient groups on omega-3-enriched medical nutrition

Effects of n−3 Fa^y Acid Supplements in Diabetes Mellitus

Hypercholesterolaemia -practical information for non-specialists

Mechanism of Action of Niacin

Effect of extended-release niacin on high-density lipoprotein (HDL) functionality, lipoprotein metabolism, and mediators of vascular inflammation in statin-treated patients

Niacin and its metabolites: role of LC-MS/MS bioanalytical methods and update on clinical pharmacology. An overview

Safety and tolerability of extended-release niacin with laropiprant

Niacin for primary and secondary prevention of cardiovascular events

Use of niacin in the United States and Canada

Safety review of combination drugs for hyperlipidemia

Niacin attenuates lung inflammation and improves survival during sepsis by downregulating the nuclear factor-κB pathway

HEART UK statement on the management of homozygous familial hypercholesterolaemia in the United Kingdom

Homozygous familial hypercholesterolaemia: new insights and guidance for clinicians to improve detection and clinical management. A position paper from the Consensus Panel on Familial Hypercholesterolaemia of the European Atherosclerosis Society

Long-term treatment with evolocumab added to conventional drug therapy, with or without apheresis, in patients with homozygous familial hypercholesterolaemia: an interim subset analysis of the open-label TAUSSIG study

Recent advances in elucidating the role of the microsomal triglyceride transfer protein in apolipoprotein B lipoprotein assembly

Long-term efficacy and safety of the microsomal triglyceride transfer protein inhibitor lomitapide in patients with homozygous familial hypercholesterolemia

Efficacy and safety of a microsomal triglyceride transfer protein inhibitor in patients with homozygous familial hypercholesterolaemia: a single-arm, open-label, phase 3 study

THREE-YEAR DATA FROM THE LOMITAPIDE OBSERVATIONAL WORLDWIDE EVALUATION REGISTRY (LOWER)

Identification and diagnosis of patients with familial chylomicronaemia syndrome (FCS): Expert panel recommendations and proposal of an "FCS score

Volanesorsen: First Global Approval

Volanesorsen and Triglyceride Levels in Familial Chylomicronemia Syndrome

Thrombocytopenia is associated with severe coronavirus disease 2019 (COVID-19) infections: A meta-analysis

Thrombocytopenia and Its Association with Mortality in Patients with COVID-19

Association between platelet parameters and mortality in coronavirus disease 2019: Retrospective cohort study

Mechanism of thrombocytopenia in COVID-19 patients

Hyperlipidaemia 3Ed: Diagnosis and Management

Drug-drug interactions that interfere with statin metabolism

Clinical pharmacokinetics of fibric acid derivatives (fibrates)

Efficacy and safety of fixed dose combination of atorvastatin and hydroxychloroquine: a randomized, double-blind comparison with atorvastatin alone among Indian patients with dyslipidemia

Cardiovascular considerations for patients, health care workers, and health systems during the coronavirus disease

Statin therapy improves response to interferon alfa and ribavirin in chronic hepatitis C: a systematic review and meta-analysis

The Effects of Melatonin on Elevated Liver Enzymes during Statin Treatment

Rhabdomyolysis a result of azithromycin and statins: an unrecognized interaction

The clinical significance of statins-macrolides interaction: comprehensive review of in vivo studies, case reports, and population studies

Statin toxicity from macrolide antibiotic coprescription: a population-based cohort study

Cardiovascular safety of tocilizumab: A systematic review and network meta-analysis

Statin drug interactions and related adverse reactions: an update

Disease-drug-drug interaction involving tocilizumab and simvastatin in patients with rheumatoid arthritis

Hydroxychloroquine or chloroquine with or without a macrolide for treatment of COVID-19: a multinational registry analysis. The Lancet

Drug interactions with fibric acids

Lack of an Effect of Ritonavir Alone and Lopinavir-Ritonavir on the Pharmacokinetics of Fenofibric Acid in Healthy Volunteers

Use of fibrates in the management of hyperlipidemia in HIV-infected patients receiving HAART

Gemfibrozil Concentrations are Significantly Decreased in the Presence of Lopinavir/ritonavir

Management of protease inhibitor-associated hyperlipidemia

Effect of dexamethasone on ciprofibrate-induced cell proliferation and peroxisome proliferation

Pharmacokinetic drug interactions of macrolides

Emerging Fixed-Dose Combination Treatments for Hyperlipidemia

Paradoxical decrease of an adipose-specific protein, adiponectin, in obesity

Fish oil in recent onset rheumatoid arthritis: a randomised, double-blind controlled trial within algorithm-based drug use

Lipid-Lowering Therapy in HIV-Infected Patients: Relationship with Antiretroviral Agents and Impact of Substance-Related Disorders

Impact of obesity and omega-3 polyunsaturated fatty acids on fibrogenesis and responsiveness to antiviral therapy in chronic hepatitis C

Can eicosapentaenoic acid maintain the original ribavirin dose or affect the response during the treatment course of chronic hepatitis C virus (HCV) patients?

Prophylaxis for ribavirin-related anemia using eicosapentaenoic acid in chronic hepatitis C patients

Omega-3 fatty acids in the prevention of interferon-alphainduced depression: results from a randomized, controlled trial

Polyunsaturated fatty acids levels and initial presentation of somatic symptoms induced by interferon-alpha therapy in patients with chronic hepatitis C viral infection

The clinical benefits of long-term supplementation with omega-3 fatty acids in cystic fibrosis patients -A pilot study

We acknowledge HEART UK for providing logistic support and support from Lipid Disease Fund,

Research/Wellcome Trust Clinical Research Facility. Table 1A 

Not directly studied but likely safe-Recommend: Continue Not directly studied but likely safe-Recommend: Continue Not directly studied but likely safe-Recommend: Continue Not directly studied. Recommend: to withhold treatment temporarily. Azithromycin is a weak CYP3A4 inhibitor and is predicted to increase exposure to lomitapide. Recommend: to withhold treatment temporarily.

Not directly studied but likely safe-Recommend: Continue Not directly studied but likely safe-Recommend: Continue Not directly studied but likely safe-

Not directly studied -Recommend: to withhold treatment temporarily.

Not directly studied but likely safe-Recommend: Continue Not directly studied but likely safe-Recommend: Continue Not directly studied but likely safe-

Not directly studies. Some references suggest that lomitapide may slightly increase levels of ivermectin. Recommend: to withhold treatment temporarily.