key: cord-0787670-w2pj9e3h
authors: Wang, Charlie; Rademaker, Marius; Baker, Christopher; Foley, Peter
title: COVID‐19 and the use of immunomodulatory and biologic agents for severe cutaneous disease: An Australian/New Zealand consensus statement
date: 2020-05-03
journal: Australas J Dermatol
DOI: 10.1111/ajd.13313
sha: 1a51ed0b7e0043d57c87a5a0400348a79e1b9fef
doc_id: 787670
cord_uid: w2pj9e3h

Patients on immunomodulators, including biologic agents and new small molecular inhibitors, for cutaneous disease, represent a potentially vulnerable population during the COVID‐19 pandemic. There is currently insufficient evidence to determine whether patients on systemic immunomodulators are at increased risk of developing COVID‐19 disease or more likely to have severe disease. As such, clinicians need to assess the benefit‐to‐risk ratio on a case‐by‐case basis. In patients with suspected or confirmed COVID‐19 disease, all immunomodulators used for skin diseases should be immediately withheld, with the possible exception of systemic corticosteroid therapy, which needs to be weaned. In patients who develop symptoms or signs of an upper respiratory tract infection, but COVID‐19 is not yet confirmed, consider dose reduction or temporarily cessation for 1–2 weeks. In otherwise well patients, immunomodulators and biologics should be continued. In all patients, and their immediate close contacts, the importance of preventative measures to minimise human‐to‐human transmission cannot be overemphasised.

The emergence of the 2019 novel coronavirus SARS-CoV-2, the cause of the COVID-19 pandemic, is the pre-eminent public health issue of this decade. There has been significant global concern due to the widespread and uncertain modes of transmission, and severe disease in a significant proportion. Patients on immunomodulators, including biologic agents and small molecular inhibitors, for cutaneous disease, represent a potentially vulnerable population who require specialised care and advice. Experience and research evidence on COVID-19 is limited; however, we aim to provide guidance for dermatologists and other clinicians in managing and counselling patients who are on immunomodulators.

COVID-19 is the disease caused by an enveloped singlestrand RNA virus from the coronaviridae family -SARS-CoV-2. Coronaviruses are so-named due to characteristic 'crown-like' projections visible on electron microscopy. Coronaviruses are subdivided into four genera (alpha, beta, gamma and delta) and typically infect birds and mammals. Seven species in the alpha-and beta-coronavirus genera are known to cause human disease from animal-to-human spillover. Other notable disease outbreaks have been caused by coronaviridae including SARS-CoV in 2002-2003 and MERS-CoV in 2012-ongoing. 1 Understanding of transmission of SARS-CoV-2 remains incomplete, although it appears to share similar transmission characteristics as SARS-CoV-1. 2 Human-to-human transmission is thought to occur predominantly via droplets; transmission via fomites is especially relevant as the virus has been shown to be viable for up to 48-72 h on plastic and steel surfaces. 2 Many health services are also assuming airborne precautions, particularly for aerosolised procedures, due to the uncertainty and rapid spread. Indeed, SARS-CoV-2 remained viable in aerosols for around 3 h. 2 Detection of the virus in stool samples of COVID-19 patients may suggest potential faecal-oral transmission or asymptomatic shedding in faeces. 3 It may also persist on human hair. Transmission from asymptomatic or minimally symptomatic hosts has also been reported, raising the possibility of infectivity during the incubation period. 4,5

The median incubation period for COVID-19 is around 4 to 5 days, but can extend to 1 month. 6, 7 Severity of the disease peaks around day 7-10, whilst viral shedding usually persists for 3-4 weeks. In most cases, the clinical signs and symptoms are indistinguishable from upper respiratory tract infections. Most commonly reported symptoms in hospitalised cases include the following: 6, 7, 8 • Fever (in almost all) • Cough (often dry)

Severe disease occurs in around 5-15% of patients and is primarily due to the development of pneumonia/pneumonitis and respiratory failure. 6, 9 Cardiovascular disease, chronic pulmonary disease, hypertension, diabetes and other chronic medical comorbidities were common in severe, hospitalised cases 8 and may be predictors of poor outcome. Smoking may also be a risk factor. Mortality estimates remain imprecise; however, recent case-fatality rates around 2-3% were reported in China. 9 Older age is the most important predictor for mortality, with a 15% fatality ratio in patients over the age of 80 in Chinese cohorts. 9 Children seem to be at much lower risk of severe disease (especially over the age of 5), 10 but may be a significant vector for infection.

From previous coronavirus outbreaks, immunosuppression is thought to increase susceptibility and cause more severe infection, 11, 12 although this is usually in the context of disease driven immunosuppression (e.g. severe inflammatory bowel disease and cancer). Case reports also describe atypical presentations of coronavirus infections in immunocompromised hosts, including prolonged incubation periods, persistent asymptomatic viral shedding, diarrhoea, weight loss and encephalitis as primary manifestations. 13, 14, 15, 16 Initial Chinese observational studies on COVID-19 did not report a high rate of immunocompromised patients in severe hospitalised cases; however, this is likely underestimated due to a difference in demography compared to Western populations. Overall, there is currently insufficient evidence to suggest that COVID-19 infection is aggravated by immunomodulators used in skin disease; however, all COVID-19 infections should be considered serious and a precautionary approach is necessary.

A range of immunomodulators, including conventional immunomodulators, biologics and newer small-molecule inhibitors, are used in autoimmune and immune-mediated skin diseases. Most conventional immunomodulators are associated with an increased risk of infection. The risk is usually dose-dependent, varies with each agent and often relates more to the underlying health condition being treated. Table 1 summarises commonly used non-biologic immunomodulators and their infection risks. Although immunomodulatory in action, retinoids (including acitretin, isotretinoin, alitretinoin), dapsone and phosphodiesterase (PDE)-4 inhibitors are not immunosuppressive.

Recently, biologic agents such as monoclonal antibodies and small-molecule agents such as Janus kinase (JAK) and PDE-4 inhibitors have provided a novel approach in the treatment of various skin diseases. By targeting single molecules or proteins that are critical in the disease pathogenesis, immunomodulation is thought to be more selective. Table 2 summarises the short-term rates of upper respiratory tract infection and serious infection in pivotal phase III clinical trials for biologics and small-molecule agents.

Overall, some biologics and small-molecule inhibitors have a small increase in upper respiratory tract infections or nasopharyngitis in clinical trials; however, infections are usually mild or self-limiting and serious infection rates are very low. There is no high-quality evidence to suggest that biologics used in otherwise healthy dermatology patients is associated with an increased rate of severe infection or more severe influenza illnesses. On the other hand, patients with severe skin disorders (e.g. severe psoriasis) are inherently at increased risk of developing pneumonias, of any cause. 17 Furthermore, discontinuation of biologic therapy may result in a loss of treatment response when rechallenged and/or development of drug antibodies. If cessation of a biologic is being considered due to the pandemic, patients should be unambiguously counselled on the aforementioned risks. Please consider registering your patient with the Australasian Psoriasis Registry (or equivalent international registry) so experiences can be shared. Nonetheless, transmission prevention measures should be emphasised in all patients and their immediate contacts, as this is likely the most effective measure to prevent SARS-CoV-2 infection.

• There is currently insufficient evidence to determine whether dermatology patients on systemic immunomodulators are at increased risk of developing COVID-19 infection or more likely to have severe disease; as such clinicians need to assess the benefit-to-risk ratio on a case-by-case basis. • Patient factors that may indicate a higher risk of severe COVID-19 disease include the following:

a Age over 60. b Uncontrolled or multiple chronic comorbidities including, but not limited to cardiovascular or chronic pulmonary disease, chronic kidney disease, diabetes, hypertension and some malignancies.

c High doses or multiple immunomodulators. d History of severe or recurrent respiratory tract infections.

• For most patients who are low-risk, immunomodulators should be continued. • Dose reductions (see Table 3 on possible lower dosages) or drug cessation may be considered in those who are identified as high risk; however, care should be taken with dose reduction of corticosteroid therapy. • Dose reduction or cessation of immunomodulators and biologics is not necessary in most children.

Corticosteroid therapy during the COVID-19 pandemic

• Corticosteroids are significantly immunosuppressive at dosages above 20 mg predniso(lo)ne equivalent; longterm use of such dosages during the pandemic should be avoided. • Use of predniso(lo)ne at 15 mg or more for 3 weeks is also associated with adrenal axis suppression. 18 • We recommend against sudden cessation or significant dose reductions due to risks of adrenal insufficiency. Indeed, corticosteroid therapy may need to be increased in times of physiological stress including COVID-19, acute respiratory distress syndrome and other serious infection. • If reduction of corticosteroid therapy is indicated to mitigate infection risk during the pandemic, a graduated reduction is advised, aiming for a dose of ≤10 mg of predniso(lo)ne or equivalent. 

• In patients with suspected or confirmed COVID-19 infection, all immunomodulators used for skin diseases should be immediately withheld, with the possible exception of corticosteroid therapy (as outlined above). 

In all patients, we emphasise the importance of preventative measures to minimise human-to-human transmission, including but not limited to: 19 • Regular washing of hands with soap and water; especially prior to applying creams to the face and body. Delay using emollient hand creams for 10-30 min after washing hands. • Avoid touching of face, eyes or mouth with unwashed hands. • Covering mouth and nose whilst coughing or sneezing.

• Avoiding overseas or interstate travel.

• Staying at home unless for medical care or necessary work. • Avoid sharing of household items such as cutlery and towels. • Regular cleaning of high-touch everyday objects.

• Wearing a face mask is not necessary if you are well.

• Practice good social-distancing techniques -this includes standing at least a metre and a half from the person standing next to you. • Stop shaking hands, hongi, kissing or hugging as a greeting. • Avoiding large gatherings, crowded places, or enclosed spaces (e.g. lifts). • For cleaning around the house, any usual household detergent should be effective at killing SARS-CoV-2. • Follow the current advice from your state/federal government regarding non-essential activities.

In addition, we recommend annual influenza vaccination (except live intranasal influenza vaccines) for all and pneumococcal vaccination in appropriate populations. Note that vaccine effectiveness may be diminished by higher dosages of some immunomodulators.

In addition to minimising risk, it is important to consider rational use of health-care resources during the COVID-19 pandemic:

• Consider conducting follow-up visits by telemedicine. 20 • Consider reducing the frequency of routine monitoring investigations. 21 • Re-enforce advice to improve comorbidities, in particular smoking and obesity. • For omalizumab, after the first injections, consider letting patients self inject at home.

This consensus statement draws upon the knowledge and experience of dermatologists specialised in the care of the immunosuppressed patient. More data and studies are required in characterising COVID-19 disease and its 

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