Red man syndrome (RMS) is an anaphylactoid reaction caused by the rapid infusion of the glycopeptide antibiotic vancomycin. RMS consists of a pruritic, erythematous rash to the face, neck, and upper torso, which may also involve the extremities to a lesser degree. Symptoms may include weakness, angioedema, and chest or back pain. RMS is caused by vancomycin through the direct and non-immune-mediated release of histamine from mast cells and basophils. The amount of histamine release is generally related to the dose of vancomycin infused and the rate of infusion. RMS is generally associated with more rapid infusion rates but can be seen following slower infusion rates and after several days of transfusion. Practitioners using vancomycin should be aware of this reaction, its prevention, and treatment.[1][2][3]
RMS most frequently occurs with intravenous vancomycin but may rarely occur from oral or intraperitoneal vancomycin.[4][5][6] It is often related to a rapid infusion rate of vancomycin (1 gram in less than 1 hour). The current treatment recommendations are to administer vancomycin at a rate no faster than 1 gram/hour or 10 mg/min. RMS most often begins 4 to 10 minutes from the start of the first dose of intravenous vancomycin. It may occur later during the infusion or begin shortly after dose completion. RMS may occur from later doses as far out as seven days.[1][2]
The increased incidence of methicillin/oxacillin-resistant Staphylococcus aureus, multiresistant Staphylococcus epidermidis, penicillin-resistant Streptococcus pneumoniae, and metronidazole-resistant Clostridium difficile has led to an increase in the use of vancomycin. Vancomycin is commonly used to treat bacterial endocarditis, abscesses with cellulitis, postoperative wound infections, infected surgically placed devices, and central line-associated bloodstream infections.[7][2]
There are case studies of RMS occurring from other antibiotics such as rifampin, cefepime, teicoplanin, ciprofloxacin, and amphotericin B.[3][8][9][1]
RMS is the most frequent adverse reaction to intravenous vancomycin. It occurs in 4% to 50% of infected patients treated with intravenous vancomycin. Patients under 40 years of age are at greatest risk of severe RMS reactions. Severe reactions include angioedema, hypotension, tachycardia, weakness, muscle spasms, and chest or back pain in addition to a rash of the face, neck, and upper torso. RMS usually is mild and easily managed. There are rare cases of life-threatening RMS reactions.[1]
Vancomycin was discovered in 1952 in soil obtained from the jungles of Borneo. Initial preparations of the antibiotic lacked purification and were brown. Therefore, many referred to vancomycin as "Mississippi mud." Clinicians initially thought RMS, otic, and renal toxicity were secondary to impurities in vancomycin. However, even after vancomycin was purified, RMS continued to be observed. Animal and several human studies indicate vancomycin activates the degranulation of mast cells and basophils increasing histamine release. The amount of histamine release has been correlated with the dose and the rate of vancomycin infusion. However, not all studies correlate elevated histamine levels with severe cases of RMS and suggest histamine metabolism may also be delayed due to inhibition of histamine N-methyltransferase and diamine oxidase enzymes.[7][1]
The clinical presentation of RMS can vary, ranging from minor pruritus to occasionally life-threatening symptoms. Symptoms may occur as soon as four minutes after initiating the first dose until up to seven days after dose completion. Patients with infections treated with intravenous vancomycin are at risk of developing RMS. The signs and symptoms of RMS include:[1][2]
The diagnosis of RMS is made clinically and does not depend on laboratory or other tests. Severe cases should be differentiated from IgE-mediated anaphylactic reactions.[2]
When a patient develops RMS, the intravenous antibiotic infusion should be stopped immediately. Supportive care should be provided. H1 (diphenhydramine) and H2 antihistamines (ranitidine or cimetidine) are used in the management of RMS. Future doses of vancomycin may be given at decreased infusion rates in most cases.[1]
Mild cases (mild flushing and mild pruritus) can be managed with antihistamines such as diphenhydramine 50 mg by mouth or intravenously and ranitidine 50 mg intravenously. Most episodes will resolve within 20 minutes, and the vancomycin may be restarted at 50% of the original rate. Future doses should be given at the new, slower rate, typically over two hours.[10]
Moderate to severe cases (severe rash, hypotension, tachycardia, chest pain, back pain, muscle spasms, weakness, angioedema) should be managed according to severity. Patients with severe symptoms should be evaluated for anaphylaxis or other serious cause for their symptoms before assuming red man syndrome. If, after careful evaluation, the patient is determined to have RMS, antihistamines such as diphenhydramine and ranitidine can both be started intravenously. Normal saline intravenous boluses are used to treat hypotension. After the symptoms resolve, the vancomycin can be restarted and given over four hours. If alternative antibiotics to vancomycin are available, they should be used. If vancomycin must be continued, patients should be premedicated with diphenhydramine 50 mg intravenously and ranitidine 50 mg intravenously 1 hour before each dose, and vancomycin should be administered over four hours under close observation.[11][12]
If the symptoms of anaphylaxis are present, such as altered mental status, hypotension, stridor, difficulty breathing, wheezing and hives, treatment should be started immediately for anaphylaxis, and the patient needs emergency care. Epinephrine should be given early, and the patient may have an epinephrine auto-injector with them, which can be used. [11][12] Emergency medical services, if available, should be activated immediately to expedite further patient treatment and transport to definitive care.
Patients requiring a rapid infusion of vancomycin may be pre-treated with diphenhydramine and ranitidine. However, the best preventive measure to avoid RMS is maintaining infusion rates below 10 mg/min.[13][14]
RMS should be differentiated from an anaphylactic reaction. Both RMS and anaphylactic reactions will have similar findings of pruritus, erythematous rash, and tachycardia. Anaphylactic reactions involve stridor, angioedema, hives, and wheezing from bronchospasm. Anaphylactic reactions are IgE mediated and require prior exposure. RMS is a rate-related anaphylactoid adverse reaction which most often occurs during the first exposure to intravenous vancomycin.[11][12]
The prognosis for patients with RMS is excellent with appropriate management. Vancomycin may be used again after an episode of RMS. Appropriate precautions and treatment guidelines should be followed. Normal intravenous saline should be used to treat hypotension, and other supportive care measures should be provided.
Red man syndrome is caused by the release of histamine from basophils and mast cells by antibiotics such as vancomycin. Symptoms include a red rash, hypotension, tachycardia, angioedema, etc. Although most of the cases are manageable, some can be life-threatening.
Healthcare providers should be made aware of the presentation of red man syndrome as well as the management of this condition to improve patient outcomes. Patients should be provided with the most appropriate care and educated on the condition.
Key Points
To help maximize patient care and patient safety, it is important for the healthcare team to:
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