The hypereosinophilic syndrome (HES) is a disease characterized by a persistently elevated eosinophil count (≥ 1500 eosinophils/mm³) in the blood for at least six months without any recognizable cause, with involvement of either the heart, nervous system, or bone marrow.^[1]

HES is a diagnosis of exclusion, after clonal eosinophilia (such as leukemia) and reactive eosinophilia (in response to infection, autoimmune disease, atopy, hypoadrenalism, tropical eosinophilia, or cancer) have been ruled out.^[2]

There are some associations with chronic eosinophilic leukemia^[3] as it shows similar characteristics and genetic defects.^[4]

If left untreated, HES is progressively fatal. It is treated with glucocorticoids such as prednisone.^[2] The addition of the monoclonal antibody mepolizumab may reduce the dose of glucocorticoids.^[5]

Classification

In the heart, there are two forms of the hypereosinophilic syndrome, endomyocardial fibrosis and Loeffler's endocarditis.

• Endomyocardial fibrosis (also known as Davies disease) is seen in tropical areas.^[6][7]
• Loeffler's endocarditis does not have any geographic predisposition.

Signs and symptoms

As HES affects many organs at the same time, symptoms may be numerous. Some possible symptoms a patient may present with include:

• Cardiomyopathy^[3]
• Skin lesions^[3]
• Thromboembolic disease^[3]
• Pulmonary disease^[3]
• Neuropathy^[3]
• Hepatosplenomegaly^[3]
• Reduced ventricular size^[3]

Diagnosis

Numerous techniques are used to diagnose hypereosinophilic syndrome, of which the most important is blood testing. In HES, the eosinophil count is greater than 1.5 × 10⁹/L.^[4] On some smears the eosinophils may appear normal in appearance, but morphologic abnormalities, such as a lowering of granule numbers and size, can be observed.^[4] Roughly 50% of patients with HES also have anaemia.^[4]

Secondly, various imaging and diagnostic technological methods are utilised to detect defects to the heart and other organs, such as valvular dysfunction and arrhythmias by usage of echocardiography.^[4] Chest radiographs may indicate pleural effusions and/or fibrosis,^[4] and neurological tests such as CT scans can show strokes and increased cerebrospinal fluid pressure.^[4]

A proportion of patients have a mutation involving the PDGFRA and FIP1L1 genes on the fourth chromosome, leading to a tyrosine kinase fusion protein. Testing for this mutation is now routine practice, as its presence indicates response to imatinib, a tyrosine kinase inhibitor.^[8]

Treatment

Treatment primarily consists of reducing eosinophil levels and preventing further damage to organs.^[4] Corticosteroids, such as Prednisone, are good for reducing eosinophil levels and antineoplastics are useful for slowing eosinophil production.^[4] Surgical therapy is rarely utilised, however splenectomy can reduce the pain due to spleen enlargement.^[4] If damage to the heart (in particular the valves), then prosthetic valves can replace the current organic ones.^[4] Follow-up care is vital for the survival of the patient, as such the patient should be checked for any signs of deterioration regularly.^[4] After promising results in drug trials (95% efficiency in reducing blood eosinophil count to acceptable levels) it is hoped that in the future hypereosinophilic syndrome, and diseases related to eosinophils such as asthma and Churg-Strauss syndrome, may be treated with the monoclonal antibody Mepolizumab currently being developed to treat the disease.^[5] If this becomes successful, it may be possible for corticosteroids to be eradicated and thus reduce the amount of side effects encountered.^[5]

Epidemiology

HES is very rare, with only 50 cases being noted and followed up in the United States between 1971 and 1982,^[4] corresponding roughly to a prevalence of 1 to 2 per million people. The disease is even more uncommon within the paediatric population.^[4]

Patients who lack chronic heart failure and those who respond well to Prednisone or a similar drug have a good prognosis.^[4] However, the mortality rate rises in patients with anaemia, chromosomal abnormalities or a very high white blood cell count.^[4]

References

External links

• DermNet systemic/hypereosinophilic