Difference between revisions of "Equine Protozoal Myeloencephalitis"

This article is still under construction.

Description

A progressive, infectious,^[1]neurological disease of horses, endemic in the USA^[2] and only encountered elsewhere in imported equids.^[3] EPM is one of the most frequently diagnosed neurological conditions of the Western Hemisphere^[4] and the principal differential for multifocal, asymmetric progressive central nervous system (CNS) disease.^[1] As it can resemble any neurological disorder, EPM must be considered in any horse with neurological signs if it resides in the Americas or if it has been imported from that area^[2][5] The disease is not contagious.^[1]

Aetiology

EPM results from infection of the CNS by the apicomplexan parasite Sarcocystis neurona or, less frequently, its close relative Neospora hughesi.^[6][7] These protozoans develop within neurons^[4] causing immediate or inflammatory-mediated neuronal damage. The organisms migrate randomly through the brain and spinal cord causing asymmetrical lesions of grey and white matter and thus multifocal lower and upper motor neuron deficits.^[1]

Epidemiology

In endemic areas of the United States, around a quarter of referrals for equine neurological disease are attributed to EPM.^[8] According to the United States Department of Agriculture, the average incidence of the disease is 14 cases per 10,000 horses per year. However, the challenges of obtaining a definitive diagnosis may mean this figure is an underestimate.^[4] The disease has been identified in parts of Central and South America, southern Canada and across most of the USA..^[4] EPM is noted occasionally in other countries, in horses that have been imported from the Americas.^[9][10] It is likely that these animals underwent transportation carrying a silent but persistent infection. There have been reports of EPM in horses that have not travelled to or from endemic regions,^[4] although cross-reacting antigens on the immunoblot test may explain this discrepancy. ^[4]

The route of infection remains unconfirmed,^[1] but there is an increased risk associated with a young age (1-4 years)^[11]and autumn months.^[12] The reported age range for EPM cases is currently 2 months^[2] to 24 years.^[13] Thoroughbreds, Standardbreds and Quarterhorses are most frequently affected across the US and Canada.^[14] This may relate to a breed predispostion or alternatively, managemental factors associated with these breeds.^[15] Showing, racing and stress^[16] have been linked to a greater risk of clinical disease.^[17]

Increasing age and environmental temperature have been associated with an increased seroprevalence of S. neurona.^[18] Seroprevalence for this species is typically higher than for N. hughesi.^[4]Other risk factors for EPM include the presence of opossums, rats, mice and woodland, increased population density of humans and horses, bedding horses on shavings or wood chips and the use of purchased grain.^[4]Case clustering may operate where all the risk factors occur, but the majority of cases appear in isolation.^[4]

Life Cycle

Life cycle diagram of Sarcocystis neurona. Created by the Agricultural Research Service, the research agency of the United States Department of Agriculture, July 2005. Sourced from the USDA Agricultural Research Service page on EPM/Sarcocystis neurona, located via WikiMedia Commons.

See here for further details of the life cycle of Sarcocystis neurona.

The causative pathogen(s) have been isolated from species other than the horse including zebra, domestic cat, Canadian lynx, sea otter, straw-necked ibis, mink, raccoon and sunk. (Furr)

Signalment

Mostly Standardbreds and Thoroughbreds aged 1-6years.^[1] Foal infection may be possible.^[2]

Clinical Signs

The disease onset may be acute, peracute or chronic. An insidious onset ataxia is most typical and with such cases, the clinical examination may reveal a bright, alert horse, perhaps with some focal muscle atrophy.^[4] In all cases, the clinical signs are referable to diffuse focal and multifocal lesions of the white and grey matter of the spinal cord and brain.^[3] The three characteristic 'As' (ataxia, asymmetry, atrophy) suggest multifocal or diffuse disease, but are not pathognomonic for EPM.^[4]

Lesions of the brainstem, cerebrum or cerebellum are less frequently recognized than those of the spinal cord. Horses with severe EPM may be unable to stand or swallow and, if left untreated, progress to recumbency within 14 days to 6 months.^[1] This deterioration may occur smoothly or spasmodically,^[21] but is likely to result in death. It has been suggested that rapidly progressive presentations reflect brainstem lesions.^[4]

Diagnosis

Differential Diagnoses

The protozoan can migrate to any region of the CNS^[2], thus the differential list comprises almost all diseases of this system.

Sarcocystis neurona stages and lesions. (A). Cross section of spinal cord of horse with focal areas of discoloration (arrows) indicative of necrosis. Unstained. (B). Section of spinal cord of a horse with severe EPM. Necrosis, and a heavily infected neuron (arrows), all dots (arrows) are merozoites. H and E stain . (C). Higher magnification of a dendrite with numerous merozoites (arrows). One extracellular merozoite (arrowhead) and a young schizont (double arrowhead). (D). Section of brain of an experimentally-infected mouse stained with anti-S. neurona antibodies. Note numerous merozoites (arrows). (E). Immature schizonts in cell culture. A schizont with multilobed nucleus (arrow) and a schizont with differentiating merozoites (arrowheads). Giemsa stain. (F). Mature sarcocysts with hairlike villar protrusions (double arrowheads) on the sarcocyst wall. H and E stain. (G). Mature live sarcocyst with numerous septa (arrows) and hairlike protrusions on the sarcocyst wall (double arrowheads). Unstained. (H). An oocyst with two sporocysts each with banana-shaped sporozoites. Unstained. Created by the Agricultural Research Service, the research agency of the United States Department of Agriculture, July 2005. Sourced from the USDA Agricultural Research Service page on EPM/Sarcocystis neurona, located via WikiMedia Commons.

Pathology

Widespread lesions of the CNS are typically observed in horses.^[4]

Gross exam

Lesions may be up to several centimetres across.^[4] They range from mild discolouration to multifocal areas of haemorrhage and/or malacia^[21] of the brain, spinal cord and less commonly, peripheral nerves.^[4]

Histopathology

Microscopically, both grey and white matter may be affected with focal to diffuse areas of nonsuppurative inflammation, necrosis and neuronal destruction. Perivascular infiltrates comprise lymphocytes, macrophages, plasma cells, giant cells, eosinophils and gitter cells.^[4] In around 25% of cases, schizonts or merozoites may be found in the neuronal cytoplasm.^[21] Less frequently, protozoa parasitize intravascular and tissue neutrophils and eosinophils, capillary endothelial cells and myelinated axons^[4][21]. Free merozoites may be seen in necrotic regions. If organisms are absent, the diagnosis relies on recognition of the inflammatory changes described above.^[21]

Treatment

Antiprotozoals

The Food and Drug Administration (FDA) has approved four treatments for use in horses with EPM, but not all of these are commercially available:^[26]

• Sulfadiazine and pyrimethamine combination, ('RebalanceTM', Antiprotozoal Oral Suspension, IVX Animal Health): administered PO daily for a minimum of 90 days. Due to availability and ease of administration, some use an off-label regimen of trimethoprimsulfa tablets with pyrimethamine tablets. Mode of action: trimethoprim, sulfadiazine, and pyrimethamine all inhibit enzymes of folic acid synthesis. Efficacy: 61.5% improvement by one clinical grade.(98 in furr)Potential adverse effects: bone marrow suppression (mild anaemia, leucopenia, neutropenia, thrombocytopenia), fever, anorexia, depression, acute worsening of ataxiam altered reproductive performance in stallions (19 in IVIS 4), congenital defects(20 in IVIS 4) and abortion. Folic acid deficiency may also cause gastrointestinal disturbances such as glossitis.(18 in IVIS 4) Blood dyscrazias are typically self-limiting and resolve on withdrawal of treatment.^[4]

• Ponazuril (Marquis(R), Bayer Animal Health): PO daily for 28 days, use in pregnant animals is off-label. Mode of action: ponazuril is a triazinetrione that targets the “apicoplast” organelle and inhibits the respiratory chain. Efficacy: well absorbed PO, achieves steady state therapeutic concentration in CSF within 3 days(100 in Furr), clinical response within 10 days, 60% improvement by at least one clinical grade, 8% relapse within 90 days of stopping treatment(91 in Furr). Potential adverse effects: none in a multi-centre field study^[26], no systemic toxicity even at high doses.(101 in Furr)However, the manufacturer reports signs that may have been related to treatment including blisters on nose and mouth, skin rash or hives, loose stools, mild colic, and a seizure.^[26]

• Diclazuril: PO, daily for 28 days, approved by FDA for use as top-dress tablet but not commercially available Mode of action: chemically similar to ponazuril but mechanism of action unknown. Efficacy: one study reported clinical improvement in 58% of cases.(98 in Furr) Potential adverse effects: none found in one efficacy study.^[4] Reported problems in a multi-centre field study included worsening neurologic status and laminitis but these were not proven to be related to treatment.^[26]

• Nitazoxanide, NTZ ('Navigator(R)', Idexx Pharmaceuticals): no longer commercially available in the US. Mode of action: a member of the 5-nitrothiazole class of antiparasitics that inhibits the pyruvate:ferredoxin oxidoreductase (PFOR) enzyme dependent electron transfer reaction essential for anaerobic energy metabolism.^[26] Efficacy: 60% success rate in an FDA-regulated study.(98 in Furr) Potential adverse effects: adverse effects and death at high doses(98), fever, anorexia, diarrhoea, lethargy, depression and laminitis recorded at lower doses. Toxic signs usally resolve upon cessation of treatment.^[4] Caution: 'administration of nitazoxanide can disrupt the normal microbial flora of the gastrointestinal tract leading to enterocolitis. Deaths due to enterocolitis have been observed while administering the recommended dose in field studies.(IVIS 4)

Prolonged, off-license treatment is often instigated after 1 month, based on repeated clinical examination. Even successfully treated cases may remain immunoblot positive for long periods, thus aiming for seronegativity is unrealistic.^[4] A lack of response to treatment suggests that the diagnosis should be re-assessed. Another month's worth of treatment is recommended for partial responders.^[4]

Ancillary medication

• NSAIDs: DMSO IV as 10% solution, thought to reduce CSF pressure and improve clinical status. Recommended for severe cases of EPM or to avoid worsening inflammation that may be induced by parasite kill(Furr). Caution: DMSO may cause intravascular haemolysis.^[1]
• Corticosteroids: a short course of dexamethasone may be beneficial whilst waiting for antiprotozoals to take effect. However, use is controversial because cell-mediated immunity is required to control parasites(Pasq) and stress is a proposed risk factor for EPM.(Furr)
• Immunomodulators: Levamisole influences T-cell mediated immunity and enhances phagocytosis. Parapox ovis virus (PPOV) immunomodulator (Zylexis, Pfizer Animal Health, Kalamazoo, Mich). This vaccine has been shown to upregulate the secretion of cytokines including IFN-γ in several species (110 in Furr). IFN-γ is thought to be essential for the clearance of S neurona, thus PPOV may be useful in EPM.(Furr)
• Multiple vitamin B supplement.^[1]

Supportive management

Box rest with deep bedding and good footing or turn out in a flat, grassy field. Ensure all obstacles are removed and avoid turning out ataxic animals with dominant herd mates. Recumbent horses will require dedicated support and a sling if available. (Furr)

Prognosis

Depends on duration and severity of neurological signs^[3] but clinical resolution is more likely if the condition is diagnosed and treated early.^[2] With standard therapy, involving 6-8months of ponazuzril or pyrimethamine-sulfadiazine (V), there is a recovery rate of around 25% and an improvement in 60-75% of cases.^[42] A good prognosis might be expected if there is an improvement in clinical signs within two weeks of commencing anti-protozoal and anti-inflammatory treatment (V). The prognosis will be guarded to poor^[1] for a horse with severe irreversible neuronal damage or one that has not been diagnosed or treated appropriately (V).

Prevention

Prophylaxis

A killed vaccine, developed using S.neurona merozoites, was conditionally licensed for use in horses.^[43] The vaccine proved to be ineffective in the prevention of EPM and has since been removed from the market.^[4] There is evidence to suggest that the antiprotozoal, ponazuril, may be useful prophylactically to reduce the incidence and severity of clinical signs.^[44] Implementing such a regime prior to and during stressful events may be beneficial, although the cost is likely to be prohibitive.^[4]Protocols involving intermittent administration of ponazuril may also show promise in the prevention of EPM.^[45]

References