Minimizing fungal disease deaths will allow the UNAIDS target of reducing annual AIDS deaths below 500 000 by 2020 to be realized

(a). Pneumocystis pneumonia

It is not known how many patients with AIDS develop PCP. The incidence or point prevalence varies substantially, increasing as gross domestic product increases [33], from rates as low as 1.5% to as high as approximately 60%, partly depending on the population studied and diagnostic methods applied. Using a low median estimate of a 15% rate of PCP in those with fewer than 200 × 10⁶ l⁻¹ CD4 cells [34–36], an estimated 450 000 develop PCP annually among the 2 988 000 with a CD4 count less than 200 × 10⁶ l⁻¹. Those who default from ART or develop antiretroviral resistance are also at risk, but it is difficult to estimate this caseload, so 450 000 is probably a substantial underestimate.

All patients with PCP and AIDS who are not treated die. Diagnosis is usually clinical, but the presentation is often atypical, late and indistinguishable from bacterial pneumonia and pulmonary TB [37]. Molecular diagnosis from sputum, induced sputum or bronchoscopy fluid is the most sensitive and specific means of confirming the diagnosis; microscopy with silver or giemsa staining is about 75% sensitive, immunofluorescence microscopy about 90% compared with 95% for molecular diagnosis, but highly specific [38–44]. In the absence of bronchoscopy in children, induced sputum or nasopharyngeal aspiration with molecular detection is required [45,46]. Beta 1,3-d glucan is almost always detectable in the serum of patients with PCP, so can be used as a ‘rule-out’ test, but is non-specific if elevated [47]. Diagnosis with ‘typical’ clinical features tends to be late and carries a higher mortality than earlier, outpatient therapy. Treatment with high-dose cotrimoxazole (trimethoprim/sulfamethoxazole) is readily available throughout of the world.

Assuming that 60% of patients are treated and 70% of them survive, as is the case in most LMICs [45,48], the current annual mortality estimate from PCP is approximately 260 000 (table 1). If better diagnostics are instituted, with good clinical guidelines, the diagnosis and treatment rate should rise to 90%, and will include earlier diagnosis before hospitalization. If we assume that this improved diagnosis and treatment rate reduces deaths by 50% by 2020, then 238 750 lives will be saved that year (figure 1), and cumulatively more than 500 000 over 5 years. This estimation includes the assumption of an annual 5% fall in the rate of PCP attributable to combined rollout of 90–90–90 and prophylactic cotrimoxazole [49]. Unfortunately, neither cotrimoxazole prophylaxis nor ART are fully protective [50–53], so PCP will continue to occur despite excellent ART adoption, and HIV units need to able to diagnose and treat it.

Additionally, there is a strong case for improving the diagnosis of PCP because use of high-dose cotrimoxazole carries much toxicity. Adverse reactions of high-dose cotrimoxazole include nausea and vomiting (90%), reduced oral intake in already malnourished patients, neutropenia (50%), pruritic rashes (33%), elevated liver function tests (33%) and significant anaemia (20%) [54,55]. A negative molecular test on a good-quality specimen virtually rules out the diagnosis of PCP and unnecessary exposure to harm can be avoided.

(b). Disseminated histoplasmosis

The number of DH cases in AIDS has been estimated to be between 100 000 and 300 000 [56,57]. Very high rates are confined to certain countries and localities. For example in Fortaleza, Brazil, 164 (43%) of 378 consecutively hospitalized HIV patients had DH [58] and in Venezuela, autopsies of patients with AIDS revealed histoplasmosis in 29 of 66 (44%) [59]. These focal hotspots make global estimations of burden challenging, especially as only one study has addressed the frequency of DH in AIDS in Africa [60], whereas histoplasmosis has been documented across the continent for over 40 years [61].

The fungus that causes DH is Histoplasma capsulatum, a slow growing, small, intracellular yeast that enters the body via inhalation. Bat guano is its primary ecological niche, and there is substantial seasonal variation in case numbers. The clinical presentation of DH is subtly different from TB in patients with AIDS, with more gastrointestinal and fewer respiratory features, pyrexia and usually some degree of pancytopenia, also seen as part of HIV infection itself. Most patients with DH in the context of AIDS are in their 30s, and death without therapy usually occurs in 10–14 days. The fungus typically takes two weeks to grow on mycological media and does not grow on media used for bacterial culture. Patients with CD4 counts < 200 × 10⁶ l⁻¹ are at most risk [62]. Rapid diagnosis can be achieved by careful examination of a blood film (40% sensitivity), bone marrow examination (more than 90% sensitivity), antigen detection in serum or urine (70–90% sensitivity) [63] and molecular methods on blood (more than 95% sensitivity). Greatly improved detection rates and reduced mortality have been shown with use of either antigen detection or molecular methods [64,65].

The antifungal agents of choice for DH are amphotericin B and itraconazole; fluconazole is not effective for DH in AIDS. Improved outcomes with early diagnosis and appropriate therapy can achieve 85% survival [66,67].

Taking the most conservative estimate of annual incidence, of 100 000 cases and assuming that the diagnosis is only made in 40% of patients currently with a 50% survival in those treated, including relapse deaths [68,69], we would anticipate about 80 000 annual deaths attributable to DH. In centres without rapid diagnosis, but a high awareness of DH, current mortality rates are more than 45% [64,70], whereas those diagnosed rapidly have a mortality of less than 30% [62,71].

If antigen and/or PCR were made available in all high incidence communities in the Americas (assumed to be approx. 70% global coverage), and both itraconazole and amphotericin B were also used, we would anticipate a reduction of approximately 60% of DH deaths by 2020. This translates into a survival gain of 48 000 lives annually by 2020 (figure 1), and cumulatively 132 000 lives over 5 years.

(c). Chronic pulmonary aspergillosis complicating tuberculosis in HIV-positive patients

CPA is a progressive and usually fatal complication of multiple pulmonary disorders, notably TB, chronic obstructive pulmonary disease and those with non-tuberculous mycobacterial infections [72]. Its radiological and clinical manifestations are similar to TB, although fever is uncommon and it is often mistaken for smear-negative TB. The detection in serum of Aspergillus fumigatus IgG is the key diagnostic test, [73] but is barely available in LMICs. Treatment options are amphotericin B or itraconazole, or the newer azoles and echinocandins, and are approximately 60% effective [72,73]. ART rollout is unlikely to reduce the incidence of CPA as it is an infection of non-immunocompromised patients, but reduction in pulmonary TB cases will.

About 935 000 patients developed pulmonary TB in the context of HIV infection in 2013 (table 2). Of these, approximately 360 000 died and 73% of these deaths occurred in the African region. In all pulmonary TB patients diagnosed in 2012 whose sputum was analysed by microscopy, 1 900 000 of 4 400 000 (43%) were smear negative [8]; of the 400 000 deaths, approximately 172 000 were, therefore, in smear-negative patients. Later culture confirmation of TB is expected in approximately 19–39% of these patients [74,75], leaving 104 900–139 300 (mean 122 000) without confirmed TB. In an unpublished study of 39 HIV positive, smear-negative patients in Kampala with very low CD4 counts, 26% had elevated Aspergillus IgG antibodies and 40% of these patients died within two months [76]. In HIV-negative patients, the Aspergillus IgG antibody detection method used in this Kampala study had a 96% sensitivity and 98% specificity for CPA [77]. We have, therefore, conservatively estimated that 26% of these 172 000 (40 248) deaths are attributable to CPA, as false negatives are likely in this highly immunocompromised group.

In addition, there were 255 850 HIV-infected survivors of ‘smear-negative’ TB in 2013. Another prospective study showed that 2–7 years after TB treatment, 8.5% of Ugandan patients had CPA, whether HIV infected or not [78]. This is a conservative rate, as detectable Aspergillus antibodies were found in 34% of post-TB patients in UK in the 1960s, and 30% of those during treatment for pulmonary TB in Iran [79,80]. Assuming that 8.5% of the annual 595 000 survivors of TB (both smear-positive and negative) develop CPA in 1 year, 53 645 would be affected. However, the chronicity of CPA certainly underestimates the magnitude of this problem. Figures from older, non-HIV-infected patient series from Korea and Japan puts the first-year mortality after presentation at approximately 30% [81]. These two figures combined yield a conservative mortality estimate of more than 56 250 HIV-infected patients dying of CPA annually.

If the diagnosis and treatment of CPA are enabled by provision of Aspergillus IgG testing, and availability of itraconazole and amphotericin B treatments, for 60% of patients, and is 60% effective (i.e. mortality reduction to 12%), then mortality should fall to 20 600 (figure 1). If the rollout of diagnosis and therapy improves from an arbitrary low baseline of 5% to 60% by 2020, then the cumulative lives saved would be at least 87 800.

(d). Actions required to improve outcomes

Early diagnosis and treatment of the most common fungal diseases are important steps in preventing AIDS-related deaths. The actions described in table 4 would have a major impact on survival, especially if undertaken widely across high and middle HIV burden countries. A disease systems analysis from Tanzania highlighted the failure to address opportunistic infections as a major cause of mortality [82]. The predictive scenarios are illustrative of the potential impact of targeting fungal diseases in AIDS and cannot be definitive, given the poverty of accurate data on incidence for most communities. ART rollout through 90–90–90 is important, but insufficient to reduce deaths. Progress will be incomplete because ART coverage will not be 100% and ART reduces the incidence of most co-infections but not all.

The 2013 WHO cryptococcal disease guidelines [25] recommend antigen screening for early detection of asymptomatic antigenaemia with the low-cost point of care lateral flow assay, and treatment with amphotericin B and flucytosine for meningitis. Only some LMICs have established screening for cryptococcal antigen in those with low CD4 cell counts, a critically important intervention. The Diflucan Partnership Programme funded by Pfizer provides fluconazole for established disease, not prevention of meningitis in those with asymptomatic antigenaemia, so alternative sources and funding are required. Amphotericin B and/or flucytosine are not available in many countries owing to various constraints including lack of registration, despite being on the WHO Essential Medicines List (EML) [83].

PCP is a major AIDS-defining illness. Diagnosis is usually empirical and based on severity and sometimes obvious, but late clinical features. Concurrent bacterial infection with PCP is common [84,85], and some deaths attributed to bacterial pneumonia may mask PCP cases. Microscopy is simple and inexpensive, and should be more widely used (see www.microfungi.net). Many molecular diagnostic tests are available but require a frozen transport chain and reliable electricity and are also expensive. Diagnosis with the β 1,3-d glucan test as a rule-out test will not be feasible for many settings owing to high costs of this assay. A low-cost diagnostic test is required for LMICs. While the best therapy, co-trimoxazole, is almost universally available, and the WHO has issued guidelines on its use for prophylaxis, there are no WHO guidelines on treatment of PCP, although the American Thoracic Society has issued management recommendations [86]. There is a need for clear guidelines for LMICs including recommendation on the use of corticosteroids for presumptive PCP in high TB burden countries.

The annual incidence of histoplasmosis is not known in many countries in which it is endemic. This is a barrier to adoption of the commercially available rapid ELISA-based antigen assays now commercially available, and simple low-cost lateral flow assay that will be available soon. Despite its importance in the treatment of histoplasmosis, itraconazole is not on the WHO EML, affecting availability in many countries. Similar to PCP neither the WHO nor Pan American Health Organization (PAHO), where the largest burden of disease falls, have developed guidelines for the treatment of histoplasmosis; publication and dissemination would improve both diagnosis and treatment and prevent deaths.

The annual incidence and 5-year point prevalence of CPA after TB were estimated using 2007 TB data and published in 2011; 372 385 incident cases per year and a prevalence of 1 173 881 (range 852 048–1 372 457) patients affected [87]. At that time there were no data related to frequency and diagnosis of CPA in HIV-infected patients. Since then, a prospective survey in HIV-positive and -negative patients in Uganda has been completed; both groups developed CPA at the same frequency after pulmonary TB and raised Aspergillus antibodies are found in both groups [78]. Therefore, it is reasonable to assume similar rates of CPA in HIV-positive and -negative patients. Furthermore, a high frequency (26%) of raised Aspergillus antibodies and a two-month 40% mortality were found in a group of hospitalized smear- and mycobacterial culture-negative patients in Kampala, clearly indicating that many HIV patients have pulmonary aspergillosis. Whether these cases are strictly CPA or represent invasive aspergillosis [88,89] is conjecture, but in either case they are potentially responsive to antifungal therapy, if diagnosed early enough. Diagnosis of CPA requires radiology and Aspergillus IgG antibody detection. Fungal cultures for Aspergillus spp. are insensitive for CPA, not specific and may be laboratory contaminants. Recent European guidelines on the diagnosis and management of CPA are helpful [72], but additional research on the frequency of CPA, when TB patients should be tested and the best interventions in HIV-infected patients are all required.

These estimates of lives saved ignore other potentially fatal but treatable fungal diseases in AIDS, including oesophageal and invasive candidiasis [89,90], paracoccidioidomycosis [91], coccidioidomycosis [91,92], blastomycosis [93] and Talaromyces (Penicillium) marneffei infection [94,95]. Enhancing capability to diagnose fungal diseases worldwide is required [57].