key: cord-0964193-od19iruh
authors: Pfavayi, Lorraine T.; Denning, David W.; Baker, Stephen; Sibanda, Elopy N.; Mutapi, Francisca
title: Determining the burden of fungal infections in Zimbabwe
date: 2021-06-24
journal: Sci Rep
DOI: 10.1038/s41598-021-92605-1
sha: 64ce57dc21075752632c73e3067eb364cb844154
doc_id: 964193
cord_uid: od19iruh

Zimbabwe currently faces several healthcare challenges, most notably HIV and associated infections including tuberculosis (TB), malaria and recently outbreaks of cholera, typhoid fever and COVID-19. Fungal infections, which are also a major public health threat, receive considerably less attention. Consequently, there is dearth of data regarding the burden of fungal diseases in the country. We estimated the burden of fungal diseases in Zimbabwe based on published literature and ‘at-risk’ populations (HIV/AIDS patients, survivors of pulmonary TB, cancer, chronic obstructive pulmonary disease, asthma and patients receiving critical care) using previously described methods. Where there was no data for Zimbabwe, regional, or international data was used. Our study revealed that approximately 14.9% of Zimbabweans suffer from fungal infections annually, with 80% having tinea capitis. The annual incidence of cryptococcal meningitis and Pneumocystis jirovecii pneumonia in HIV/AIDS were estimated at 41/100,000 and 63/100,000, respectively. The estimated prevalence of recurrent vulvovaginal candidiasis (RVVC) was 2,739/100,000. The estimated burden of fungal diseases in Zimbabwe is high in comparison to other African countries, highlighting the urgent need for increased awareness and surveillance to improve diagnosis and management.

Africa has an estimated population of 1.3 billion people and accounts for about 75% of all the 38 million human immunodeficiency virus (HIV)-infected people in the world. Notably, approximately 50% of all fungal-related deaths due to HIV infections are thought to occur in Africa; however accurate data are lacking 1, 2 . Data generated by the Global Action Funds for Fungal Infections (GAFFI), suggests an estimated 47.6 million Africans suffer from fungal diseases, of which 1.7 million suffer annually from a serious fungal infection 3 . However, these estimates are based on data from only a few African countries, and most likely underestimates the true prevalence.

Fungal diseases are life-threatening and are responsible for a largely silent epidemic, often hidden killers causing substantial morbidity and mortality in susceptible individuals 4 . Patients with fungal infections occur across a huge spectrum of medical conditions often as co-infections or opportunistic infections 5 and are thus treated as separate entities, hindering progress in diagnosis and management of these patients 6 . Only skin, hair, nails and mucosal infections can be clinically diagnosed (with much imprecision) without specific laboratory testing or medical assessment (radiology, mycology, histopathology) with expensive technologies requiring trained personnel. On the other hand, most life-threatening infections require the referred methods to be diagnosed, which is often out of the reach of patients in poor resource settings.

Nonetheless, substantial progress is being made to prevent and manage some of these fungal diseases. Mycetoma and chromoblastomycosis have been included in the World Health Organisation (WHO) list of neglected tropical diseases 7, 8 and new guidelines for the prevention and management of cryptococcal meningitis were recently issued 3 .

Fungal infections such as histoplasmosis, mycetoma, chromoblastomycosis, sporotrichosis, cryptococcal meningitis and tinea capitis [9] [10] [11] [12] [13] have been reported in Zimbabwe, albeit in few and dated reports. Therefore, there Non-HIV-related fungal disease burden. Chronic pulmonary aspergillosis (CPA) is a complication of pulmonary TB that is often diagnosed late and may mimic pulmonary TB. It also affects patients with other pulmonary disorders, notably COPD, after pneumothorax and occasionally those with ABPA and asthma 27 . We estimated 6840 of CPA cases per year. Fungal allergy exacerbates asthma, especially in adults. The prevalence of asthma in adults in Zimbabwe was estimated to be 6.9% using data from Democratic Republic of the Congo 28 . We estimated 14,892 and 19,657 cases per year of ABPA and SAFS respectively. There may be some duplication between these entities as many ABPA patients have severe asthma. Therefore, the true 'fungal asthma' prevalence may be 75% of their total. Cystic fibrosis has not reported from Zimbabwe. Candidaemia and Candida peritonitis were estimated to affect 743 and 111 patients, respectively. We did not estimate Candida peritonitis complicating chronic ambulatory peritoneal dialysis.

RVVC is defined as four or more episodes of vulvovaginal candidiasis per year 29 . We estimated 203,585 RVVC to occur among adult women in the general healthy female population in their fertile years, which may be conservative. Hormone replacement therapy can precipitate RVVC 30 , but we did not estimate this.

Fungal keratitis often occurs following ocular trauma from vegetable material 31, 32 and male agricultural workers are at a greater risk 33 . It often leads to blindness and a recent global estimate found a culture and microscopy positive annual incidence of 14/100,000, which translates into approximately 2080 cases in Zimbabwe. However, assuming that culture and microscopy negative cases are usually cases of fungal keratitis 34 www.nature.com/scientificreports/ this number rises to approximately 2930 cases. Most of the infected eyes will go blind and some will perforate and require removal 34 . Cutaneous fungal infections are very common in southern Africa, but here we focus only on tinea capitis, given its transmissibility, scarring potential and occasional complications of kerion 35 . We estimated 1,806,700 schoolchildren suffering from tinea capitis. The two most frequent dermatophyte species isolated from tinea cases in Zimbabwean children were Trichophyton violaceum and Microsporum audouinii 9 . These species have been shown to be the most frequent dermatophyte species involved in tinea capitis among children in southern Africa [36] [37] [38] [39] . This observation is in accordance with a recent systematic review estimating the burden of tinea capitis among children in Africa 40 . Figure 2 shows tinea capitis infection in two young school boys from rural Zimbabwe.

There were 14 chromoblastomycosis, 3 sporotrichosis and 5 mycetoma cases as reported by Ross and Gelfand in a 10-year survey of histological material 12, 13 . Only four cases of blastomycosis were reported in 1991 41 , however some more recent isolates such as Blastomyces gilchristii have been described 42, 43 . Given that these older estimates are the only available data in Zimbabwe, we cannot use them for a reliable estimate of the current burden. The reports however show that these conditions occur in this population and may be underdiagnosed and under reported.

A diverse range of fungal infections commonly occurs in Zimbabwe. Frequent HIV and TB co-infections contribute to a higher prevalence of some fungal diseases. Each of these conditions on its own or in combination can predispose individuals to fungal diseases 44 . To date, the burden of fungal infections in Zimbabwe has not been documented. Therefore, we conducted this study to estimate the burden of fungal infections/diseases in the country. Our study indicated that over 2 million people [2,212,715 (14. 9%)] suffer from fungal disease annually, a higher number than most African countries. This figure is comparable to that of Senegal 45 and Nigeria 46 with tinea capitis being the most predominant fungal infection.

In Zimbabwe, we found that, following tinea capitis, the most frequent serious fungal diseases were recurrent vulvovaginal candidiasis, oral and oesophageal candidiasis. Vulvovaginal candidiasis (VVC) is a common gynaecological problem occurring among women globally, most commonly caused by Candida albicans 47, 48 .

In previous studies carried out in Zimbabwe among women presenting with symptomatic vaginal discharge, VVC prevalence rates ranged between 25 and 40% 49,50 and we have estimated that 203,585 Zimbabwean women suffer from recurrent episodes. While recurrent vulvovaginal candidiasis (RVVC) is not life threatening, it is a significantly more severe clinical form than VVC. This is because of the recurrence of symptoms defined as four or more episodes per year 29,51 and it is a major health problem for sexually active women. RVVC affects quality of life and is associated with anxiety, depression and a loss of productivity [52] [53] [54] . Our estimates, make the burden of RVVC in Zimbabwe the fifth highest among the Southern African Development Community (SADC) countries with available estimated burdens 44,55-57 and some data indicate that the prevalence of RVCC may be higher in Africa than other continents 54, 58, 59 . Genetic factors have been suggested to be related to the susceptibility of Black/ African women to RVCC. However, comprehensive assessment of the role of genetics in RVCC is still lacking. Likewise, host-related and behavioural factors could also have a role to play 51, 60, 61 .

Oral and oesophageal candidiasis occurs commonly in AIDS patients or those with other immunosuppressive conditions. Oral candidiasis is one of the most common fungal opportunistic infections in immunocompromised individuals 62, 63 and was found to be the most common opportunistic infection in Nigeria 64 and Uganda before the initiation of highly active antiretroviral therapy (HAART) 65 . Fluconazole is the drug of choice in the treatment of oral candidiasis 62 because of its bioavailability and efficacy compared with other antifungal drugs 66, 67 . However, an increase in resistance of Candida species to fluconazole has been reported in some parts of Africa [68] [69] [70] [71] and this is important to note because of the implications for morbidity and mortality rates 71, 72 . www.nature.com/scientificreports/ Cryptococcal meningitis is the leading cause of meningitis in sub-Saharan Africa 44, 73 . Recent studies have shown that an increasing proportion of patients with cryptococcosis are ART-experienced 74, 75 . In Uganda 3% of ART-experienced patients with virological failure were cryptococcal antigen (CrAg) positive 76 with a background rate of 5-10% cryptococcal meningitis. Consequently, to estimate the incidence of cryptococcal meningitis in Zimbabwe we doubled our at-risk population (ART naïve), being cognisant of the fact that virological failure does not always translate to immunodeficiency. We estimated the occurrence of 6086 cases of cryptococcal meningitis per year. We estimated 9429 cases of PCP in HIV/AIDS patients only. Although, PCP is common in children [77] [78] [79] and also occurs in non-HIV infected patients we did not include these in our estimates due to paucity of data.

The prevalence of CPA was estimated at 42/100,000, which was relatively high compared to other African countries [55] [56] [57] . South Africa had the highest prevalence, at 176/100,000 44 . The high number in Zimbabwe could reflect the relatively high burden of tuberculosis 80 and further studies are required to validate this. The diagnosis requires a combination of imaging and Aspergillus IgG antibody testing recently recognised as an Essential Diagnostic by WHO 81 , however these are not routinely done in Zimbabwe. Notably a fifth (19%) of CPA patients who were TB smear negative and GeneXpert negative in Nigeria were incorrectly diagnosed as having pulmonary TB 82 with consequent inappropriate treatment.

Asthma is a significant public health problem in Zimbabwe and is often poorly controlled 83 . Here we estimated that 595,677 adults have asthma. In Zimbabwe fungal sensitisation studies have not been conducted, nonetheless we were able to estimate the burden for ABPA and SAFS, which are collectively known as 'fungal asthma' . Fungal asthma differs from allergic asthma. Although the bronchoconstriction can be alleviated by the bronchodilators and inhaled glucocorticosteroids used in the management of asthma, fungal diseases requires the administration of antifungal agents such as oral itraconazole [84] [85] [86] [87] and voriconazole, which can only be prescribed if an accurate diagnosis has been made. These antifungal agents act by reducing the fungal load, thus minimizing the stimulus for the ongoing inflammatory activity 88 . If inadequately managed fungal asthma can lead to significant complications such as long term steroid toxicity, bronchiectasis and CPA 89 .

A review on the role of antifungals in the management of patients with severe asthma has recently been published 87 . The paper highlights significant studies that confirm lower toxicity of treatment with azoles, particularly itraconazole for ABPA and provide recommendations for the use of antifungal agents in patients with severe asthma, airways fungal infection and fungal colonisation 87 .

Dermatophyte infections, especially tinea capitis, are common among children all over Africa, particularly in areas with poor socioeconomic and sanitary conditions [90] [91] [92] . They are a public health problem due to their contagious nature 55 . Prevalence rates range from 10% to more than 70% in different regions of Africa 9, 40, 93, 94 . The estimate of tinea capitis in this study was based on Zimbabwean data from 1990 9 . However, there may have been changes over time and these figures may not be a true presentation of the current situation in the country. Nonetheless, it remains a common clinical problem.

Mycetoma is a neglected tropical disease caused by fungi or bacteria and mainly affects the skin as well as the underlying tissues 95 . The morbidity due to mycetoma is high 96 Most fungal infection studies in Zimbabwe are dated having been carried out about two decades ago [9] [10] [11] 23 . While these indicate susceptibility in this population, they do not accurately represent the current situation in the country, especially with changes in the epidemiology of HIV whose prevalence has gone down from more than 15% 14 to about 8.7% with 85% of these receiving ART 18 . The health and economic challenges faced by the country with respect to public health priorities, clinical and laboratory expertise, the inadequacy of financial resources militate against the early diagnosis and treatment of fungal infections. Consequently, these health system limitations contribute to high rates of morbidity and mortality 105 .

As most serious fungal infections are opportunistic infections, a majority of the affected individuals are immunocompromised 4 . For example, cryptococcal meningitis, oesophageal candidiasis, PCP as well as aspergillosis are among the most common systemic fungal infections observed in HIV and AIDS patients, thus a combination of the underlying immunocompromised and superimposed fungal infection contributes to a higher risk of mortality 106 . The comorbidities necessitate the co-administration of drugs, resulting in drug-drug interactions (DDIs). In some cases, optimum therapy for fungal infections is contraindicated in conjunction with medicines used to treat co-morbid conditions in an attempt to prevent potential adverse effects and treatment failure 107, 108 .

The preferred treatment for these fungal infections includes the administration of amphotericin B or azole antifungals such as fluconazole, itraconazole and voriconazole. All of these except voriconazole are on Zimbabwe's essential list of medicines 109 and studies from other countries have suggested that renal function should be closely monitored with concomitant use of amphotericin B and tenofovir as both drugs can cause nephrotoxicity. Similarly, combination therapy of zidovudine and amphotericin B may result in anaemia and neutropenia 108 . Hence, as DDIs are often unavoidable in HIV-infected patients, the potential effects of these DDIs cannot be ignored 106 especially in Africa where very few drugs used have been evaluated for DDIs and pharmacogenetics 110 . This will potentially help in the management of patients suffering from co-morbidities as well as broaden our understanding of the effect of these DDIs in different populations. In addition to DDIs there is also a possibility of antifungal resistance 111 . Previous studies have reported fluconazole resistance among C. neoformans complex isolates from Africa 112 www.nature.com/scientificreports/ Study limitations. Despite an exhaustive search in this study, we could not obtain enough local data to use for a precise estimate of the current burden, as most of the available studies were outdated. So, majority of the data used was obtained from other countries, which may introduce some inaccuracies when estimating the burden in Zimbabwe due to socioeconomic and geographical differences 114 . Another significant limitation is the incomplete nature of the estimates: for example, we could not estimate the burden of PCP in children or non-HIV patients, the burden of mycetoma, chromoblastomycosis as well sporotrichosis could not be estimated due to paucity of data despite reports of cases in the country. Nonetheless, our results show that fungal diseases are probably much more common than are documented in clinical practice. Our estimates provide a starting point from which to better understand the extent of the problem in the country and create awareness and propose appropriate studies and interventions to address fungal diseases that are of significant public health importance.

Educating the community about fungal diseases is an important step in raising awareness about the morbidity and mortality associated with these diseases. For most villages and communities across Zimbabwe, the entry point to health and health information dissemination is vested in the Community/Village Health Workers. These people are therefore integral in promoting awareness and assisting in early detection of symptoms associated with fungal diseases. Their knowledge of a community's languages and customs means that they are able to deliver health messages to groups in a culturally appropriate manner, which is also easily understood. This is an effective means of disseminating information to community members resulting in communitybased surveillance, which improves the likelihood of early case detection 115 , as well as reducing the stigma associated with some of the fungal diseases. The medical mycology community in Zimbabwe should therefore work closely with local organisations and community health workers to raise awareness of fungal diseases. Schools are also a good place to promote campaigns aimed at raising awareness about fungal infections. For example, the neglected tropical disease, schistosomiasis, is a public health burden in Zimbabwe 116 . Educational campaigns in schools including essay competitions, drama and 'edutainment' are ways in which awareness about the disease is raised in communities. A similar approach could be used to create awareness about fungi diseases among school children.

To increase the access to better diagnostics locally, a standardised diagnostic algorithm based on clinical signs and symptoms that can be easily identified by primary healthcare professionals 117 can be developed. The algorithm will help in early diagnosis and treatment of fungal diseases as well as ensure wealth of information on fungal diseases affecting the African population. This will allow interventions to be implemented in the primary healthcare setting and has the potential to significantly reduce morbidity and improve quality of life.

This study is the first to estimate the burden of fungal diseases in Zimbabwe and to provide an estimation of its impact on public health. The paucity of data on fungal infections in the country warrants for further epidemiology studies and better diagnostics to aid patient management.

The prevalence and incidence of fungal disease in Zimbabwe were calculated following methods previously described 118, 119 and the applied formulae will be detailed below. The burden was estimated for the general healthy population and for the 'at-risk' populations including HIV/AIDS patients, survivors of pulmonary TB, cancer, chronic obstructive pulmonary disease (COPD), asthma and patients receiving critical care. National or local data were preferred, but where these were unavailable, data were extrapolated from other sources. The annual burden was estimated for each fungal disease and presented as: (i) absolute number of cases per year in the country and (ii) annual rates. The absolute cases were presented as either incidence or prevalence depending on the nature of infection. The annual rates (incidence or prevalence) were calculated using the absolute annual number of cases as the numerator and the entire Zimbabwean population as the denominator. For simplicity, the 2019 Zimbabwean population (n = 14,863,000 120 ) was used regardless of the year from which the numerator data originated. The United Nations population estimates 2019, WHO reports, and The Joint Nations Programme on HIV/AIDS (UNAIDS) were used for the population demographics.

Calculating fungal disease burden. Prevalence or incidence was calculated using data from published studies. Prevalence was calculated for allergic bronchopulmonary aspergillosis (ABPA), severe asthma with fungal sensitisation (SAFS), chronic pulmonary aspergillosis (CPA), recurrent vulvovaginal candidiasis (RVCC), and tinea capitis and the remaining estimates were calculated as annual incidence. Due to paucity of data, we were not able to calculate both prevalence and incidence for each disease.

Prevalence. To calculate the prevalence of ABPA, SAFS, CPA, RVCC, and tinea capitis we applied the same formulae used by GAFFI members to estimate the prevalence of fungal diseases in other countries 55,60,121,122 . Annual incidence. To calculate the incidence of invasive aspergillosis, oesophageal candidiasis, candidemia and Candida peritonitis we applied the same formulae used to estimate the incidence in other countries 55, 60, 121, 122 . For cryptococcal meningitis, Pneumocystis pneumonia and oral candidiasis, instead of calculating a figure based on the denominator, we doubled our at-risk population (ART naïve), being cognisant of the fact that virological failure does not always translate to immunodeficiency. www.nature.com/scientificreports/ The values above and the assumptions made to obtain the accurate denominators were obtained from a systematic literature search detailed below. The assessment of the quality of the source data, country profile and assumptions made for the analyses are detailed below.

Published papers were identified from four databases: PubMed, Web of Science, EMBASE and Google Scholar. The following search terms were used: fungal infection, fungal burden, fungal epidemiology, Zimbabwe, Southern Africa, and Africa. A second search included the same searches using the following diseases: Cryptococcus/cryptococcal, Candida/thrush, Aspergillus/aspergillosis, histoplasmosis, asthma, leukaemia, chronic obstructive pulmonary disease (COPD), Pneumocystis pneumonia/Pneumocystis jirovecii pneumonia (PJP)/Pneumocystis carinii pneumonia, chronic pulmonary aspergillosis (CPA), aspergilloma, allergic bronchopulmonary aspergillosis (ABPA), severe asthma with fungal sensitisation (SAFS), tinea/ ringworm. We used HIV data to estimate the burdens of cryptococcal meningitis (CM), candidiasis and Pneumocystis jirovecii pneumonia (PCP). Asthma, chronic obstructive pulmonary disease and tuberculosis data were used to estimate the presumed burden of allergic bronchopulmonary aspergillosis (ABPA) and chronic pulmonary aspergillosis (CPA). Burdens of candidaemia and Candida peritonitis were derived from critical care and/ or cancer patients' data.

Papers presenting incidence or prevalence of any fungal disease were evaluated using an adapted Grading of Recommendations, Assessment, Development and Evaluations (GRADE) score 123 based on the following features: diagnostic accuracy, study size (using a cut-off of > 10 cases), year of study, with more recent studies scoring higher, type of publication, with original research article scoring more, methodology and country, with studies from Zimbabwe scoring higher (Table 2) . Those with an adapted GRADE mean score of > 2 were deemed acceptable and enabled a minimum estimation of the country burden of fungal diseases (Table 3) . Papers with a mean score < 2 were excluded in the estimation of the country's burden of fungal diseases but were discussed in the review. Table 4 18, 120 . National TB data were obtained from the World Health Organization (WHO) 80 . National prevalence data for lung cancer, chronic obstructive pulmonary disease (COPD), diabetes and incidence data for acute myeloid leukemia (AML) were obtained from the 2016 Global Burden of Disease study 134 . To estimate the burden for HIV-related fungal diseases, we have assumed a 7-year linear decline in CD4 count to < 200 × 10 6 /l, of those not on ART, doubled to reflect those on ART who fail with ARV resistance or default (at risk of opportunistic infections). www.nature.com/scientificreports/ Assumptions from other published reports were used to identify the most accurate denominators to use for our estimates and these are summarised in Table 5 . In brief, PCP frequency was estimated by assuming 11% of newly diagnosed HIV/AIDS adults with the risk spread over 2 years 24 . The prevalence of AIDS patients presenting with cryptococcal meningitis was assumed to be 7.1% based on a study by Rajasingham et al. 131 among antiretroviral therapy (ART)-naive HIV patients. Chronic pulmonary aspergillosis (CPA) prevalence was estimated using the previously described approach taken by Denning et al. 141 , where the number of annual PTB cases with cavities (22%) was multiplied by the incidence of CPA in cavities (22%) and the number of PTB cases without cavities (78%) was multiplied by CPA incidence (2%). An estimation of a 5-year prevalence of CPA was made, assuming a 15% annual mortality or surgical cure rate 130 . To calculate all cases of CPA, PTB was assumed to be the underlying disorder in 67% of cases 142 . Invasive aspergillosis was estimated in haematological and lung malignancies, HIV/AIDS and COPD. It was assumed that 10% of acute myeloid leukemia (AML) patients develop IA and that an equal number of cases are found in non-AML haematological patients while 1.3% of admitted COPD patients 124 , 2.6% of lung cancer patients 127 and 4% HIV/AIDS patients who died develop IA 125 . ABPA estimation was made assuming that 2.5% of adult asthmatics have ABPA 130, 143 and although ABPA also occurs in cystic fibrosis, no estimate of the prevalence of this disease in Zimbabwe was attainable. The estimate of SAFS was as estimated at 33% of the most severe asthmatics (10%) 89 .

Oral candidiasis was assumed to affect 90% of untreated HIV patients over 12 months, based on a study in Tanzania 144 . Oesophageal candidiasis was assumed to affect 20% of advanced HIV disease patients and 0.5% of HIV patients on ARV treatment 145, 146 . Mucormycosis was estimated to occur at a rate of 0.2/100,000 (literature estimate) 25 . Candidaemia cases were estimated assuming it occurs at a rate of 5 per 100,000 with 30% in ICU (critical care and post-surgical patients) and 70% in cancer and other immunocompromised and hospitalised patients 128 . For Candida peritonitis (intrabdominal candidiasis), we assumed that the rate was half of the ICU candidemia rate 129 . The estimated prevalence of RVVC was established assuming a frequency rate of 6% in adult women 132 . Tinea capitis was estimated at 29% prevalence amongst schoolchildren in Zimbabwe 9 . [124] [125] [126] [127] Chronic pulmonary aspergillosis Tuberculosis, COPD Assumed that 22% of those with and 2% of those without cavities after TB develop CPA; that pulmonary tuberculosis is the underlying diagnosis in 67% of all CPA cases 141 Allergic bronchopulmonary aspergillosis Asthma Assumed to occur in 2.5% of adult asthmatics 28, 130, 143 Severe asthma with fungal sensitisation Severe asthma Assumes 33% of worst 10% of adult asthmatics 89 Candidemia 5/100,000 (mean of 2-11/100,000) with 30% in ICU (critical care and post-surgical patients) and 70% in cancer and other immunocompromised patients 128 Candida 

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We thank all the members of the Parasite Immuno-epidemiology Group at the University of Edinburgh for their valuable comments in shaping this manuscript. 

This research was commissioned by the National Institute for Health Research (NIHR) Global Health Research programme (16/136/33) using UK aid from the UK Government. The views expressed in this publication are those of the authors and not necessarily those of NIHR or the Department of Health and Social Care. LTP, FM and ENS are supported by OAK Foundation. DWD undertook this work without external funding.

LTP, FM., SB. and ENS have no competing interests to declare. DWD and family hold Founder shares in F2G Ltd, a University of Manchester spin-out antifungal discovery company. He acts or has recently acted as a consultant to Pulmatrix, Pulmocide, Zambon, iCo Therapeutics, Mayne Pharma, Biosergen, Bright Angel Therapeutics, Cipla and Metis. He sits on the DSMB for a SARS CoV2 vaccine trial. In the last 3 years, he has been paid for talks on behalf of Dynamiker, Hikma, Gilead, Merck, Mylan and Pfizer. He is a longstanding member of the Infectious Disease Society of America Aspergillosis Guidelines group, the European Society for Clinical Microbiology and Infectious Diseases Aspergillosis Guidelines group.

Correspondence and requests for materials should be addressed to L.T.P.

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