Middle East respiratory syndrome coronavirus infection medical therapy

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: João André Alves Silva, M.D. [2]

Overview

Middle East Respiratory Syndrome (MERS) is a viral respiratory illness. It is caused by an emerging coronavirus, specifically a betacoronavirus called MERS-CoV (Middle East Respiratory Syndrome Coronavirus), first discovered in 2012. Being a relatively novel virus, there is no virus-specific prevention or treatment options for MERS patients. Outbreaks of MERS-CoV represent a great social challenge due to the fact that there is very limited time to develop and test new pharmaceutical drugs. The common clinical presentations documented so far include Acute Respiratory Distress Syndrome (ARDS), renal failure, pericarditis and disseminated intravascular coagulation. Therefore and due to the absence of antiviral therapy, supportive care should focus mainly in the prevention and monitoring of these conditions. Until now, supportive medical care has been the only treatment option, however, repurpose of drugs for other viruses and illnesses is presenting as an attractive alternative for MERS-CoV.^[1][2]

Medical Therapy

MERS represents a great challenge in terms of treatment because it is caused by a relatively novel virus to which there is no approved therapy yet. According to the International Severe Acute Respiratory & Emerging Infection Consortium (ISARIC), supportive medical care continues to be the approved treatment for MERS. The search for broad-spectrum inhibitors aiming to minimize the impact of coronavirus infection remains the major goal. Recent studies are showing the potential use of other drugs and therapies to treat the MERS-CoV, which are based on the experience of treatment of other coronaviruses like the SARS virus. This repurposing of drugs has advantages such as: better availability, lower cost and known safety and tolerability profiles. However, lack of evidence makes these new therapies uncertain.^[1]

Cell and animal studies have shown conflicting results: the combination of ribavirin with interferon α-2b in a cell study reduced viral replication^[3]; another study in rhesus monkeys with combination of intramuscular ribavirin and interferon α-2b, the group that received the treatment did not develop breathing abnormalities nor radiographic evidence of pneumonia^[4]; however, when tried in 5 critically ill patients in Saudi Arabia, this combination was inefficient in all cases, leading to a fatal outcome.^[5]

Despite the absence of a specific therapy, some approaches are considered to be more worth of experimentation than others. These include:^{[6][7][8][2][9]}

• Convalescent plasma - this therapy, along with others that involve antibodies for the MERS-CoV has the strongest evidence for intervention. Plasma from patients who recovered from MERS-CoV infection contains neutralizing antibodies, which represents the best therapy to neutralize the extracellular virus.
• Interferon - there is supporting evidence from in vitro (SARS virus and MERS-CoV) and in vivo (SARS virus) studies that interferon inhibits viral replication, especially when administered in the early course of the disease. Additionally it is commonly more available than plasma.
• Corticosteroids - there is no evidence of the benefit in the mortality rate and their use is only recommended in a planned treatment regimen or when the benefits of the drug outweigh the potential harms. When used, constant monitoring is mandatory and the ideal timing is the early course of the disease, during the period of maximal inflammatory response.
• Ribavirin - the most commonly used drug in the treatment of SARS. Due to the controversial results of clinical trials relating to the use of ribavirin for MERS and its high level of toxicity in humans, some experts recommend the withhold of the drug.

Supportive Care

The supportive medical care aims to minimize as much as possible the damages caused by MERS. It is divided into 4 categories, according to the clinical status of the patient. These categories include:^[2]

Early recognition

This section focuses on the early recognition of symptoms and management of patients with severe acute respiratory infections. This includes:^[2]

• Recognition of severe manifestations of acute respiratory infections, such as pneumonia or sepsis
• Prevention of infection by implementing measures like droplet or airborne precautions
• Providing oxygen therapy to patients with severe acute respiratory infections, presenting with hypoxemia or shock
• Specimen collection for laboratory testing, from upper and lower respiratory tracts
• Empiric antibiotics until diagnosis of is confirmed
• Careful fluid administration in patients with severe acute respiratory infections, even in the absence of shock, since volume overload may jeopardize oxygenation
• Monitoring of possible clinical deterioration of patients with severe acute respiratory infections
• Avoidance of high-dose systemic corticosteroids to prevent side-effects such as opportunistic infections and avascular necrosis

ARDS

This section focuses on management of patients who deteriorate and develop ARDS. It includes:^[2]

• Recognition of severe cases where oxygen therapy may not be enough and a higher flow system may be required
• Mechanical ventilation in patients with respiratory distress or hypoxemia that does not resolve with high-flow oxygen therapy
• Non-invasive ventilation (NIV) in cases of immunosuppression or in ARDS that does not present with lack of consciousness or cardiac failure, under constant monitoring in an ICU environment. It is important not to delay endotracheal intubation if NIV is unsuccessful.
• Endotracheal intubation for mechanical ventilation
• In patients with ARDS, use of a lung-protective ventilation with a low pressure ventilation protocol, has shown to reduce mortality in ARDS patients^[10][11]
• Adjunctive therapeutics in patients with severe ARDS particularly if ventilation targets are not achieved, such as neuromuscular blockage or repositioning the patient to a prone position^[12][13]
• Fluid management in ARDS patients, in the absence of shock, in order to decrease duration of mechanical ventilation

Septic Shock

This section targets the adequate management of septic shock. It includes:^[2]

• Recognition of septic shock in the presence of persistent hypotension after fluid administration or signs of peripheral hypoperfusion, followed by resuscitation
• Administration of intravenous crystalloids in septic shock
• In persistent shock it is recommended use of:

• vasopressors, such as norepinephrine, epinephrine and dopamine, preferably through a central venous catheter and at the minimal dosage to insure an SBP >90 mmHg
• concomitant IV hydrocortisone (<200 mg/day) or prednisolone (<75 mg/day) administration

Prevention of Complications

This section is mainly based on preventing possible complications. It includes:^[2]

• Daily evaluation for spontaneous breathing
• Titration of sedation to a specific target
• Prevent ventilator-related pneumonia by:

• preferring oral intubation
• performing frequent antiseptic oral care
• adjusting the patient to a reclined position
• preferring a closed suctioning system
• changing the ventilator circuit for every patient
• monitoring the status of heat moisture exchanger
• reducing intermittent mandatory ventilation

• Prevention of venous thromboembolism with pharmacological prophylaxis, in the absence of contraindications. If contraindications are present, it is suggested the prophylactic use of a mechanical device for pneumatic compression
• Prevention of infection through catheter manipulation^[14]
• Avoid prolonged immobilization by turning the patient every 2 hours
• Reduce formation of gastric ulcers by administration of early enteric nutrition along with an Histamine H2 receptor blocker or a PPI
• Reduce weakness by immobilization

References

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