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Case Report

Aspergillus Section Fumigati Pneumonia and Oxalate Nephrosis in a Foal

by
Jasmine Hattab
1,
Antonella Vulcano
2,
Silvia D’Arezzo
2,
Fabiana Verni
3,
Pietro Giorgio Tiscar
1,
Giovanni Lanteri
4,
Emil Gjurcevic
5,
Umberto Tosi
1 and
Giuseppe Marruchella
1,*
1
Faculty of Veterinary Medicine, University of Teramo, Loc. Piano d’Accio, 64100 Teramo, Italy
2
Laboratorio di Microbiologia Banca Biologica e Cell Factory, Istituto Nazionale Malattie Infettive “Lazzaro Spallanzani”, via Portuense 292, 00149 Rome, Italy
3
Veterinary Practitioner, Loc. Convento, 64023 Teramo, Italy
4
Department of Chemical, Biological, Pharmaceutical and Environmental Sciences, Viale G. Palatucci, 98168 Messina, Italy
5
Department for Biology and Pathology of Fish and Bees, Faculty of Veterinary Medicine, University of Zagreb, Heinzelova 55, 10 000 Zagreb, Croatia
*
Author to whom correspondence should be addressed.
Pathogens 2021, 10(9), 1087; https://doi.org/10.3390/pathogens10091087
Submission received: 3 August 2021 / Revised: 24 August 2021 / Accepted: 24 August 2021 / Published: 26 August 2021
(This article belongs to the Special Issue Parasites of the Third Millennium)
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Abstract

:
Equine pulmonary aspergillosis is a rare deep mycosis often due to the hematogenous spread of hyphae after gastrointestinal tract disease. We describe herein the main clinic-pathological findings observed in a foal, which spontaneously died after showing diarrhea and respiratory distress. Necropsy and histopathological investigations allowed to diagnose pulmonary aspergillosis, which likely developed after necrotic typhlitis-colitis. Biomolecular studies identified Aspergillus section Fumigati strain as the causative agent. Notably, severe oxalate nephrosis was concurrently observed. Occasionally, oxalate nephropathy can be a sequela of pulmonary aspergillosis in humans. The present case report suggests that the renal precipitation of oxalates can occur also in horses affected by pulmonary aspergillosis and could likely contribute to the fatal outcome of the disease.

1. Introduction

Aspergillus species are worldwide-distributed filamentous fungi (mold) which thrive in the soil as saprophytes and occasionally infect animals as opportunistic pathogens [1]. Equine aspergillosis is an uncommon but severe respiratory disease which can affect the sinonasal cavities, the guttural pouches or the lung parenchyma [2]. As a general rule, an immunosuppressive state and host-debilitating conditions predispose to fungal diseases, including aspergillosis. Horses usually become infected through the inhalation of fungal spores. Nevertheless, equine pulmonary aspergillosis (EPA) is often characterized by multifocal-to-disseminated embolic lesions which result from the hematogenous spread of hyphae after acute enteritis [2,3].
Aspergillus sp. can synthesize oxalic acid, which reacts with blood and tissue calcium to precipitate as oxalate crystals, at physiologic pH values [4]. In humans, the demonstration of such crystals in cytology specimens (e.g., in sputum) is useful to diagnosing Aspergillus infections, most commonly the Aspergillus niger group [5]. Likewise, the precipitation of oxalates within the foci of an Aspergillus infection has been reported in veterinary medicine (mostly in avian species). In a recent retrospective study, Payne et al. [6] observed the deposition of oxalates in 14 out of 38 cases of aspergillosis (Aspergillus sp., Aspergillus fumigatus, Aspergillus niger, Aspergillus versicolor), including 2 out of 15 horses.
We describe herein the peculiar clinic-pathological findings observed in a foal affected by pulmonary aspergillosis and oxalate nephrosis.

2. Case Description

The present case occurred in a Quarter Horse breed, 10-month-old male foal which belonged to a stable housing a total of 10 animals (five mares and five young horses less than two-years-old) in central Italy. The animal under study was kept in a single box provided with an external paddock and was fed with hay ad libitum and flaked feed. The foal was treated with a broad-range anthelmintic drug (ivermectin, Eqvalan®, Boehringer Ingelheim Animal Health, Milan, Italy) and vaccinated twice for influenza and tetanus at six and seven months of age (Equilis Prequenza Te®, MSD Animal Health, Milton Keynes, UK).
During the first decade of January 2020, the foal suddenly got prostrated, out of food and tachypneic. Within 24 h, the clinical picture severely worsened, with fever (42 °C), dyspnea, tachycardia and profuse watery diarrhea. At that time, the foal was treated with isotonic fluids (Ringer’s lactate, 15–20 L/die i.v.), antimicrobials (benzylpenicillin plus dihydrostreptomycin, Combiotic®, ACME srl, Cavriago, Italy, 10 mL/die i.m.), vitamin B complex (Dobetin B1-10000®, Ecuphar Italia srl, Milan, Italy 10 mL/die i.m.) and diosmectite (Smigol, ACME srl, Cavriago, Italy, 150 g/BID per os). However, the clinical signs further worsened, and the foal spontaneously died 48 h after the onset of the disease and was then necropsied.
A wide range of tissue samples (stomach, intestine, spleen, liver, kidneys, lungs, heart, lymph nodes) was promptly fixed in 10% neutral buffered formalin, embedded in paraffin and routinely processed for histopathological investigations (hematoxylin and eosin stain, H&E). Due to the precarious field conditions, no further sampling for microbiological investigations was carried out.
Grossly, the most relevant lesions affected the large intestine and the lungs. In more detail, the mucosa of the cecum and colon appeared necrotic, with abundant watery content filling their lumina. Microscopically, the intestinal mucosa was diffusely necrotic, infiltrated by inflammatory cells (mainly polymorphonuclear cells) and covered by bacterial aggregates; the lamina propria was strongly hyperemic, with scattered inflammatory cells seen also in this layer.
Both lungs appeared severely hyperemic and edematous. Moreover, disseminated nodules (2–5 mm in diameter) were appreciated at palpation throughout the lung parenchyma. Microscopically, pulmonary nodules appeared intensely hyperemic, the alveolar walls were thickened and congested. Foci of necrosis and hemorrhages were also seen, infiltrated by macrophages and polymorphonuclear cells. A huge number of branching septate fungal filaments, morphologically resembling Aspergillus sp., were detected inside the alveolar lumina, within the necrotic-hemorrhagic areas and the blood vessels (Figure 1). When subpleural nodules were investigated, the inflammatory reaction also involved the pleural surface, with numerous hyphae embedded within the fibrinous exudate which covered the visceral pleura.
Considering the microscopic findings, a formalin-fixed nodule was submitted for biomolecular study, aiming to identify the causative agent. A polymerase chain reaction assay targeting a highly conserved region of the 28S large ribosomal subunit (28S rDNA) was used as screening for the detection of clinically relevant fungi [7]. Section-level identification was achieved by sequence analysis followed by nucleotide BLAST analysis (https://blast.ncbi.nlm.nih.gov/Blast.cgi; accessed on: 29 July 2021). The results showed a 99% identity with Aspergillus fumigatus (GenBank: MH869824.1).
Remarkably, severe and extensive nephrosis was observed. Translucent and fan-shaped crystals filled almost all renal tubules, with no evidence of nephritis or fibrosis (Figure 2). The morphology of such crystals closely resembled that of calcium oxalates. The observation of H&E-stained sections under polarized light showed that crystals were strongly birefringent (Figure 3), thus confirming that they consisted of calcium oxalates. Careful examinations of the slides ruled out the deposition of oxalates in other tissues and organs.
Altogether, clinic-pathological and laboratory findings allowed us to diagnose Aspergillus section Fumigati strain pneumonia with concurrent severe oxalate nephrosis.

3. Discussion

EPA is widely recognized as a rare disease condition. In the largest case series currently available, Sweeney and Habecker [8] reported an estimated prevalence lower than 0.04%, i.e., 29 out of 73,000 horses admitted to a veterinary teaching hospital. Up to date, a total of 71 EPA cases have been recorded on the MEDLINE database (http://www.ncbi.nlm.nih.gov/pubmed/; accessed on: 16 July 2021) entering “horse, lung, aspergillosis” as keywords (see Table 1 for further details).
According to what was repeatedly reported in the literature, the present case of EPA most likely occurred after acute typhlitis-colitis, which disrupted the mucosal barrier of the large intestine and allowed the hematogenous spreading of fungi. The presence of disseminated lesions scattered throughout the parenchyma of both lungs, along with the detection of hyphae in the blood vessels, further support such a pathogenetic hypothesis. Slocombe and Slauson [3] hypothesized a synergistic relationship between acute enterocolitis by Salmonella sp. and EPA, although they often isolated different bacterial species from the intestine of horses affected by pulmonary aspergillosis (namely, Escherichia coli, Klebsiella sp., Staphylococcus aureus, Clostridium perfringens, Proteus sp., Actinobacillus equuli). In the present case report, pathological findings argue in favor of a bacterial etiology of typhlitis-colitis, which unfortunately could not be further investigated.
In veterinary medicine, oxalate nephrosis is frequently observed in dogs and cats due to ethylene glycol toxicity, as well as in small ruminants after the ingestion of plants of various genera (e.g., Oxalis, Rumex) which can accumulate oxalates. The production of oxalic acid is a common feature of filamentous fungi and is catalyzed by oxaloacetate hydrolase (OAH) [19]. In particular, some fungi (e.g., Aspergillus niger, Aspergillus flavus) can produce large amounts of oxalates on feedstuffs, which may represent another potential cause of poisoning [20]. Aspergillus fumigatus is less commonly recognized as an oxalate-producing pathogen [21]. It would be interesting to investigate the expression and activity of Aspergillus section Fumigati OAH to know whether differences exist in oxalate production among strains and/or under different culture conditions.
Generally, the horse is considered resistant to oxalate-induced nephrosis. In this animal species, acute poisoning results from exposure to very high dosage of oxalates in food and causes fatal gastroenteritis, while prolonged exposure to that chemical is known to induce osteodystrophia fibrosa [20]. Hypothetically, the food may have been the source of poisoning in the case described herein. However, this scenario is unlikely, considering that all the other horses living in the same stable and fed with the same hay and feedstuff did not show any clinical signs. Moreover, the subsequent analysis of the hay and feedstuffs demonstrated that the level of fungi and mycotoxin contamination was in the range of normality (data not shown).
Reasonably, we consider that oxalate nephrosis occurred as a secondary event after mycotic pneumonia. In this respect, the timing of pulmonary and renal lesions, which both developed in a short period, argues in favor of a direct pathogenetic link between an Aspergillus infection and oxalate deposition in renal tubules. Moreover, fatal cases of oxalate nephrosis occurred in humans after pulmonary Aspergillus niger group infection [22,23,24,25,26,27,28,29]. Likewise, cases of renal oxalosis have been rarely documented in wild ruminants, namely an elk (Cervus elaphus nelsoni) affected by Aspergillus fumigatus pneumonia [30] and a white tail deer (Odocoileus virginianus) with pneumonia and encephalitis caused by Aspergillus fumigatus [31].We remark that in wild ruminants, as well as in several human cases, the renal precipitation of oxalate crystals was not associated with the local infection by Aspergillus sp., and that oxalates were not always detected in lung lesions. Therefore, we speculate that oxalates, which are produced in the pulmonary foci of an Aspergillus infection, can reach the renal parenchyma through the bloodstream accumulating in the renal tubules, where the microenvironment is optimal for their precipitation.
As far as the horse is concerned, the presence of oxalate crystals has been reported only in two cases of aspergillosis (see Table 1 for details). In the first case, both fungi and oxalates were present in lungs and kidneys. In the second case, oxalates were seen in the renal parenchyma, while they remained undetected in the site of Aspergillus sp. infection (i.e., lung). In both cases, the renal deposition of oxalates was restricted to a single tubule, thus being of poor clinical significance [6].

4. Conclusions

The present case report supports that EPA should be suspected whenever a severe respiratory syndrome occurs after a gastrointestinal tract disease, particularly when antimicrobials prove to be ineffective [8]. Aspergillus fumigatus is the most commonly documented cause of EPA, although the identification of the causative agent often remains at the genus level. In this respect, biomolecular techniques provide useful tools in identifying the pathogen, even when a fungal culture cannot be performed. Finally, oxalate nephrosis can represent a severe, clinically relevant sequela of EPA—as occasionally observed in human medicine—thus likely contributing to the fatal outcome of the disease.

Author Contributions

Pathological investigations, J.H., G.L., E.G. and G.M.; clinical management of the animal under study, F.V. and U.T.; biomolecular investigations, S.D. and A.V.; supervision, writing—review and editing, G.M., J.H. and P.G.T. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

Ethical review and approval were waived for this study. The present case report involved a client-owned animal, demonstrated a high standard of veterinary care and involved informed client consent.

Informed Consent Statement

Not applicable.

Data Availability Statement

No new data were created or analyzed in this study. Data sharing is not applicable to this article.

Acknowledgments

The authors gratefully thank Alfreda Tonelli for kindly revising the English format of the manuscript.

Conflicts of Interest

The authors declare no conflict of interests.

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Pathogens 10 01087 g001 550
Figure 1. Foal. Pulmonary nodule. Several fungi were present inside the alveolar lumina (a), within necrotic-hemorrhagic foci (b) as well as in the blood vessel wall (black asterisk indicates the lumen of the same vessel). In some microscopic fields (b,c), dichotomous branching hyphae were seen. Hematoxylin and eosin stain. Final magnification 400×.
Figure 1. Foal. Pulmonary nodule. Several fungi were present inside the alveolar lumina (a), within necrotic-hemorrhagic foci (b) as well as in the blood vessel wall (black asterisk indicates the lumen of the same vessel). In some microscopic fields (b,c), dichotomous branching hyphae were seen. Hematoxylin and eosin stain. Final magnification 400×.
Pathogens 10 01087 g001
Pathogens 10 01087 g002 550
Figure 2. Foal. Kidney. Typical fan-shaped, oxalate crystals were seen in the lumina of renal tubules, both in transverse (a) and longitudinal (b) section (black arrowheads). The precipitation of oxalates affected most of renal tubules (c, black arrowheads), which appeared distended, their epithelium being no longer detectable (ac). Hematoxylin and eosin stain. Final magnification 400×.
Figure 2. Foal. Kidney. Typical fan-shaped, oxalate crystals were seen in the lumina of renal tubules, both in transverse (a) and longitudinal (b) section (black arrowheads). The precipitation of oxalates affected most of renal tubules (c, black arrowheads), which appeared distended, their epithelium being no longer detectable (ac). Hematoxylin and eosin stain. Final magnification 400×.
Pathogens 10 01087 g002
Pathogens 10 01087 g003 550
Figure 3. Foal. Kidney. At very low magnification, the precipitation of countless oxalate crystals was evident (a). At higher magnification, the typical birefringence, with radiating spokes, could be appreciated (b). Polarized light microscopy, hematoxylin and eosin stain. Final magnification 25× (a), 400× (b).
Figure 3. Foal. Kidney. At very low magnification, the precipitation of countless oxalate crystals was evident (a). At higher magnification, the typical birefringence, with radiating spokes, could be appreciated (b). Polarized light microscopy, hematoxylin and eosin stain. Final magnification 25× (a), 400× (b).
Pathogens 10 01087 g003
Table
Table 1. Cases of pulmonary aspergillosis so far reported in the horse.
Table 1. Cases of pulmonary aspergillosis so far reported in the horse.
Number of EPA CasesPredisposing FactorsAspergillus SpeciesSites of Infection (Other Than Lung)Sites of Oxalates PrecipitationReference
19Enterocolitis (n = 14), intensive corticosteroid treatment (n = 2), urolithiasis (n = 1), myelogenous leukemia (n = 1), hemangiosarcoma (n = 1)Aspergillus sp. (n = 17), Aspergillus fumigatus (n = 2)Kidneys (n = 2), brain (n = 1)Not reported[3]
11Not reportedAspergillus sp. (n = 11), Aspergillus fumigatus (n = 2), Aspergillus glaucus (n = 1), Aspergillus flavus (n = 1)Colon (n = 1), kidney (n = 1), heart (n = 1), skeletal muscle (n = 1), guttural pouches (n = 1)Lungs (n = 1) and kidneys (n = 2)[6]
29Loss of integrity of the gastrointestinal tract (n = 25)Aspergillus sp.Not specified organs (n = 12)Not reported[8]
2NoneAspergillus fumigatusKidneys, myocardium, brainNot reported[9]
1Cushing’s syndromeAspergillus sp.NoneNot reported[10]
1LeukemiaAspergillus sp.GutNot reported[11]
1Exposure to high spore countAspergillus nigerNoneNot reported[12]
1Ehrlichia risticii infection, acute enteritis NoneNot reported[13]
1Volvulus of the colon and peritonitisAspergillus sp.HeartNot reported[14]
2Sarcocystis neurona infection (n = 1), small intestine obstruction (n = 1)Aspergillus sp.NoneNot reported[15]
1UnknownAspergillus fumigatusNoneNot reported[16]
1EnterocolitisAspergillus fumigatusColonNot reported[17]
1Myelomonocytic leukemiaAspergillus sp.NoneNot reported[18]
Gastrointestinal disorders appear as the most common predisposing factor (43 cases, i.e., 60.56%). The identification of the causative agent often does not go beyond the genus level; however, Aspergillus fumigatus is the most commonly identified species in EPA (8 cases, i.e., 11.26%). Oxalate crystals have been only reported in two horses.
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MDPI and ACS Style

Hattab, J.; Vulcano, A.; D’Arezzo, S.; Verni, F.; Tiscar, P.G.; Lanteri, G.; Gjurcevic, E.; Tosi, U.; Marruchella, G. Aspergillus Section Fumigati Pneumonia and Oxalate Nephrosis in a Foal. Pathogens 2021, 10, 1087. https://doi.org/10.3390/pathogens10091087

AMA Style

Hattab J, Vulcano A, D’Arezzo S, Verni F, Tiscar PG, Lanteri G, Gjurcevic E, Tosi U, Marruchella G. Aspergillus Section Fumigati Pneumonia and Oxalate Nephrosis in a Foal. Pathogens. 2021; 10(9):1087. https://doi.org/10.3390/pathogens10091087

Chicago/Turabian Style

Hattab, Jasmine, Antonella Vulcano, Silvia D’Arezzo, Fabiana Verni, Pietro Giorgio Tiscar, Giovanni Lanteri, Emil Gjurcevic, Umberto Tosi, and Giuseppe Marruchella. 2021. "Aspergillus Section Fumigati Pneumonia and Oxalate Nephrosis in a Foal" Pathogens 10, no. 9: 1087. https://doi.org/10.3390/pathogens10091087

APA Style

Hattab, J., Vulcano, A., D’Arezzo, S., Verni, F., Tiscar, P. G., Lanteri, G., Gjurcevic, E., Tosi, U., & Marruchella, G. (2021). Aspergillus Section Fumigati Pneumonia and Oxalate Nephrosis in a Foal. Pathogens, 10(9), 1087. https://doi.org/10.3390/pathogens10091087

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