Fatal Influenza A(H1N1) Respiratory Tract Infection in a Patient Having Psoriasis Treated With Infliximab

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Background The use of biologic agents represents a remarkableadvance for patients with psoriasis and psoriatic arthritiswho have experienced an incomplete response to other therapeuticmodalities. Decreased mortality and improved quality of lifehave been reported in patients undergoing treatment with theseagents. Increased risk ofbacterial, viral, granulomatous, andopportunistic infections also has been associated with the useof these medications. Enhanced patient education, watchful monitoringto promote early detection of infections, discontinuation ofthe medication when clinical symptoms are identified, and immediateavailability of supportive care are advised to balance the benefitof treatment with biologic agents against the potential riskof infection. Herein, we discuss the risk of infection and themonitoring and vaccination guidelines in patients having psoriasistreated with biologic agents.

Observations A woman with obesity and psoriasis that hadpreviously been successfully treated with efalizumab (Raptiva)for 3 years was started on a regimen of infliximab (Remicade)to treat a flare. She died 1 week after her first infusion ofinfliximab and was found to have had influenza A(H1N1).

Conclusions We report the first case to date of a patientwith psoriasis who died of influenza A(H1N1) respiratory tractinfection while undergoing treatment withinfliximab. Furtherobservations are needed to make a causal association.

INTRODUCTION

Tumor necrosis factor (TNF) is a proinflammatory cytokine producedpredominantly by macrophages and T cells that facilitates theonset of a broad spectrum of biologicactivity that enhancesthe inflammatory response and the body's ability to defend itselfagainst infection. Treatments targeted against TNF representa remarkableadvance in improving the clinical symptoms andin possibly slowing the progression of several diseases.

Elevated levels of TNF have been detected in the serum and theepidermis of psoriatic plaques, in the serum and synovial fluidof patients with rheumatoid arthritis and those with ankylosingspondylitis, and in the serum and gut mucosa of patients withCrohn disease.¹ Elevated TNF levels at the sites of inflammationare the direct causeof tissue damage. Tumor necrosis factorlevels are also elevated systemically in these chronic inflammatorydiseases. Herein, we report a fatal case of influenza A(H1N1)in a patient with obesity and extensive psoriasis who was founddead 1 week after her initial infusion of infliximab (Remicade)to treat a flare.

REPORT OF A CASE

A 55-year-old woman with psoriasis since childhood had failedtreatment with numerous topical therapies. Weighing 94 kg, thepatient was obese, with a body mass index (calculated as weightin kilograms divided by height in meters squared) of 49.3. Shehad an excellent clinical response to efalizumab (Raptiva) therapy,which wasadministered at a dose of 1 mg/kg of body weight perweek for 3 years. She was encouraged to consider other optionsafter reports of cases of progressive multifocal leukoencephalopathyin patients who had been using the medication for more than3 years. Efalizumab therapy was discontinued, and the patientexperienced a severe flare in her psoriasis several weeks later.Because of her weight and data demonstrating lesser responsesof psoriasis to other biologic agents,² infliximab was initiatedata dose of 5 mg/kg as a therapeutic agent. Friends of thedecedent reported that the patient had experienced upper respiratorytract symptoms 4 days after the infusion. She was then discovereddead in her home 1 week after her initial infusion with infliximab.While using biologic agents for her psoriasis, she had receivedyearly inactivated influenza vaccines and purified protein derivative(PPD) skin tests.

An autopsy revealed no external signs of trauma. Important findingsincluded an enlarged heart and granular kidneys, consistentwith chronic hypertension. The larynx and trachea exhibitedareas of ulceration with tan-yellow exudate, and the lungs weremarkedly congested and edematous (2250 g) with scattered areasof firm and hemorrhagic parenchyma. Histologic sections ofthelungs revealed vascular congestion and intraparenchymal hemorrhagewith hyaline membrane formation, increased interstitial andairspace cellularity, type 2 pneumocyte hyperplasia, and focalintraalveolar fibrin deposition. These findings were consistentwith diffuse alveolar damage, the pathologic correlate of severeacute respiratory syndrome. The laryngeal and tracheal mucosaeexhibited acute and chronic inflammation with ulceration, aswell as fibrinous exudate and cellular debris, consistent witha necrotizing process. Given the recent outbreak of influenzaA(H1N1) in the area and the gross pulmonary findings in thecase, there was a high suspicion of this influenza in the patient.Nasopharyngeal swabs were tested by polymerase chain reactionand were positive for novel influenza A(H1N1).

COMMENT

Tumor necrosis factor blockers have demonstrated remarkableresults in improving the clinical symptoms of rheumatoid arthritis,³ psoriatic arthritis,^4-5 and psoriasis⁶ and ininhibiting theprogression of disease in patients with rheumatoid arthritis.Sustained and significant increases in physical function andquality-of-life measures have been observed in patients treatedwith these medications.⁷ This improvement has resulted in clinicallymeaningful functional benefits that include fewer disabilities,higher employment rates, and lower health care costs.⁸

Studies^1, 9-18 report an increased incidence of serious infectionsassociated with the administration of biologic therapy (anti-TNFagents).

Patients having rheumatoid arthritis treated with TNF antagonistshave dramatically decreased mortality,^14, 19 as well as significantand clinically relevant improvement in physical function andquality of life, inhibition of progressive disease, and sustainedimprovement in the signs and symptoms of inflammation.⁷ TheBritish Society for Rheumatology Biologics Register reporteda marked reduction in the incidence of myocardial infarctionamong patients receiving anticytokine agents.^14, 16 A Scandinavianregistry reported that treatment with TNF blockers is associatedwith a50% lower incidence of first cardiovascular events amongpatients with rheumatoid arthritis.¹⁹

The startlingly high 50% decrease in 5-year mortality from cardiovascularevents among patients with rheumatoid arthritis¹⁹ who have receivedTNF blockers compared with other therapies must be balancedagainst the anticipated adverse effects of these biologic agents,which decrease inflammation and immune response. Although anincrease in infections and malignant neoplasms has been reported,^1, 9-18 the incidence has not reached sufficient clinical significanceto decrease the overall mortality rate among patients receivingthese medications.

Bongartz et al¹² reported a significant increase in seriousinfections among patients treated with TNF antagonists, as wellas a dose-dependent increase in the risk of malignant neoplasms.Pharmacokinetic investigations have demonstrated that infliximabdosages higher than 3 mg/kg every 8 weeks lead to a high riskof overexposure, with an excessive binding of TNF.²⁰ Nestorovsuggested that lower dosages of the medication should be preferredbased on a review of the published clinical trials, which demonstrateda statistically insignificant difference in clinical efficacybetween low-dose anti-TNF antibody treatment (adalimumab, 20mg every other week, or infliximab, 1 mg/kg every 4 weeks) andthe substantially higher recommended dosages. Factors that needto be considered in determining the final dosage include medicalhistory, clinical response to previous therapeutic agents, degreeof disability, and disease progression. However, Nestorov didnot consider the development of antichimeric antibodies, whichhave been shown to increase in patients treated with low-doseinfliximab.²¹

According to Listing et al,¹⁷ the German biologics register(RABBIT [German acronym for rheumatoid arthritis-observationof biologic therapy]) documented a 2.7 to 2.8 times higher incidenceofserious infections among patients receiving biologic agents(etanercept or infliximab) compared with control subjects anda 3.3 to 4.1 times higher incidence of adverse events in general.Although almost one-third of the increase in the rate of adverseevents could be attributed to differences in individual patientcharacteristics (eg, age, disease severity, comorbid conditions,and exposure to other immunosuppressive drugs), most of theincrease was likely caused by the use of TNF inhibitors. Susceptibilityto all types of infections is higher among patients receivinganti-TNF therapy, but the highest incidences of infections arefor sepsis, urinary tract infections, bone and joint infections,lower respiratory tract infections (especially pneumonia), bacterialskin infections (erysipelas), and subcutaneous tissue infections.^1, 14 The rate of serious infections associated with the useof biologic agents documented by Listing et al¹⁷ is similarto rates reported by others.^7, 22-24

Patients receiving TNF antagonists have chronic inflammatorydisease and are already predisposed to infections. This riskincreases with age, disease severity, immunosupression fromothertherapeutic modalities, and other comorbid conditions.^17, 25 The suggestion that the risk is higher for bacterialinfections than for viral infections is anecdotal and requiresfurther confirmation.¹⁷

In Spain, the risk of tuberculosis was reported to be increased20-fold among patients treated with infliximab vs control subjects.²⁶ The risk of granulomatous infection is higher among patientstreated with the monoclonal TNF antibodies infliximab and adalimumabthan with the soluble TNF receptor fusion protein etanercept;this difference is explained by the different modes ofaction.²⁷ The Spanish registry disclosed a 78% decrease in the rateof active tuberculosis among patients treated with biologicagents after screening and management guidelines for latenttuberculosis were initiated.²⁶ Our patient described hereinwas screened by PPD testing before initiation of treatment witha biologic agent, and she was subsequently screened on an annualbasis. All PPD test results were negative.

Increased bacterial, viral, granulomatous, and opportunisticinfections have been reported^1, 9-18 in patients receiving TNFantagonists. The desired mechanism of action in TNF antagoniststhat exerts powerful anti-inflammatory effects, which minimizethe symptoms, severity, and progression of inflammatory disease,also blunts the inflammatory response to infection. In additionto older subjects, patients at high risk of developing seriousinfections include those receiving glucocorticosteroids andthose having chronic disorders, more severe manifestations ofdisease, and comorbid conditions (eg, diabetes mellitus, heartdisease, and obesity).

Our patient had developed biopsy specimen–documented herpeszoster during treatment with efalizumab. The literature aboutthe risk of infections in patients treated with TNF antagonistspredominantly discusses bacterial infections and tuberculosis.To our knowledge, fewer data are available about the incidenceof viral infections among these patients. Herpes zoster hasbeen one of the more commonly reported adverse effects of anti-TNFagents. Strangfeld and Listing¹ observed that treatment withthe monoclonal anti-TNF antibodies adalimumab and infliximabisassociated with an increased risk of herpes zoster. Thisrisk was independent of age, disease severity, or glucocorticosteroiduse and was absent in patients treated with the receptor fusionprotein etanercept. The increased risk of herpes zoster dueto inflammation associated with disease vs due to treatmentwith immunosuppressive drugs could not be distinguished in theirstudy.

Several reports of bacterial infection followed by fatal sepsishave heightened concern about the use of TNF antagonists.^17, 26, 28 However, the few randomized controlled trials availableare underpowered, and definitive conclusions about the associationbetween sepsis and TNF antagonist treatment cannot be made.^7, 17, 23 In our patient, the temporal relationship and the factthat infliximab is immunosuppressive (with data showing increasedupper and lower respiratory tract infections^1, 9-18) raise thesuspicion of a causal relationship, but no conclusion can bemade solely based on this case report.

The recent global presentation of influenza A(H1N1) heightensconcern among physicians that this virus may increase the riskof serious infections in patients undergoing treatment withTNFantagonists. The potential for the fast spread of this virusamong susceptible populations and the difficulties in developinga vaccine and initiating an inoculation program against thisrapidly mutating entity may pose a significant danger to patientsreceiving this class of medication.

The Medical Board of the National Psoriasis Foundation has setforth guidelines for monitoring and vaccinating patients treatedwith biologic agents for psoriasis.²⁹ Intensive patient educationto heighten awareness about early symptoms of infection andcareful monitoring of patients treated with these medicationsare essential. Early detection of infection by routine historyand physical examination and the initiation of immediate supportivecare are critical because the sign-symptom complex may be bluntedsecondary to the anti-inflammatory effects of these medications.Tumor necrosis factor antagonists should be discontinued whenthere is clinical suspicion of an infection and should not bereinitiated until the condition of the patient is stabilized.

Evidence is lacking about whether vaccination is effective inpreventing serious infections among patients treated with biologicagents, nor is there convincing evidence that vaccination isineffective. Package inserts for biologic agents give recommendationsabout vaccination. Before administration of biologic agents,standard vaccines should be administered when appropriate,includingthe following: tetanus, human papillomavirus, varicella, herpeszoster, influenza, pneumococcal, hepatitis A and B, meningococcal,and measles-mumps-rubella. Thereafter, patients should receivean annual inactivated influenza vaccine.²⁹

We are uncertain whether the outcome in the case reported hereinwould have been better if the patient had received influenzaA(H1N1) vaccination before infusion of infliximab (this vaccinewas unavailable before her death). With respect to antiviraltherapy, given the outcome of this case it may be prudent toadvise patients receiving biologic agents to report any upperrespiratory tract symptoms early and to consider treatment withantiviral agents such as oseltamivir (Tamiflu). Further observationsand studies are needed to make any conclusions.

AUTHOR INFORMATION

Correspondence: Amir A. Larian, MD, Department of Dermatology,Mount Sinai School of Medicine, 5 E 98th St, Fifth Floor, NewYork, NY 10029 This e-mail address is being protected from spambots. You need JavaScript enabled to view it. .

Accepted for Publication: January 26, 2010.

Author Contributions: All authors had full access to all thedata in the study and take responsibility for the integrityof the data and the accuracy of the data analysis.Acquisitionof data: Kling, Larian, Scordi-Bello, and Lebwohl. Analysisand interpretation of data: Kling, Larian, Scordi-Bello, andEmer. Drafting of the manuscript: Klingand Larian. Criticalrevision of the manuscript for important intellectual content:Larian, Scordi-Bello, Emer, and Lebwohl. Administrative, technical,and material support: Larian and Emer.Study supervision: Lebwohl.

Financial Disclosure: None reported.

Author Affiliations: Departments of Dermatology (Mr Kling and Drs Larian, Emer, and Lebwohl) and Pathology (Dr Scordi-Bello), Mount Sinai School of Medicine, New York, New York.

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Fatal Influenza A(H1N1) Respiratory Tract Infection in a Patient Having Psoriasis Treated With Infliximab