Definition

• An adverse drug reaction (ADR) is an undesired pharmacological response that occurs when a drug is given for the appropriate purpose.
• The etiology of a drug reaction can be immunologic, toxic, or idiosyncratic in nature.
• Drug allergy is due to an immune response that is mediated by drug-specific antibody or T cells.

Classification

• Type A reactions are predictable, often dose dependent, and related to the pharmacokinetics of the drug. They comprise up to 80% of all ADRs (e.g., hepatic failure due to overdose of acetaminophen, sedative side effects of antihistamines, drug–drug interactions, and gastrointestinal bacterial alteration after antibiotics).
• Type B reactions are unpredictable and are not related to the dose or the drug’s pharmacokinetics. They account for 10%–15% of all ADRs.
  • Immune-mediated adverse reactions can be from a variety of mechanisms. They usually occur on reexposure to the offending drug.
  • Nonimmunologic reactions (pseudoallergic or anaphylactoid) are caused by IgE-independent degranulation of mast cells.

Epidemiology

• ADRs are reported to account for 10%–15% of hospitalized patients.¹
• Mortality from ADRs is significant and ranges from 0.14% to 0.32%.²
• Lifetime prevalence of drug-induced anaphylaxis is 0.05%–2%.¹ The most common drugs causing IgE-mediated anaphylaxis are penicillins and anesthetic agents given during the perioperative period. Drug-induced anaphylaxis is seen predominantly in older age group.

Etiology

• β-Lactam antibiotics are the most common drug class allergy in United States, which includes penicillins, penicillin derivatives (ampicillin and amoxicillin), cephalosporins, monobactams, and carbapenems. Penicillin allergy is the most prevalent antibiotic allergy of this class. About 8% of patients in healthcare report have a penicillin allergy.³
  • About 90% patients with history of penicillin allergy will be able to tolerate penicillins, as most patients outgrow their allergy over time.⁴ Given the lower likelihood of having true penicillin allergy, antimicrobial stewardship programs have been developed to decrease use of β-lactam alternatives.
• Hospitalized patients with a history of penicillin allergy have been shown to have a longer hospital stay with increased incidence of vancomycin-resistant Enterococcus, methicillin-resistant Staphylococcus aureus, and Clostridioides difficile infections compared to patients without a reported penicillin allergy.⁵
• The chemical structure of penicillins results in their high immunogenicity with a reactive β-lactam ring that covalently binds with carrier proteins to form a hapten, which stimulates an immune response.
  • The major determinant of immunogenicity of penicillin is the benzylpenicilloyl form seen in 93% of tissue-bound penicillin.
  • The minor antigenic determinants are all remaining penicillin conjugates. They comprise benzylpenicillin, benzylpenicilloate, and benzylpenilloate.
• The cross-reactivity between β-lactam antibiotics is variable and largely determined by their side-chain structure attached to the β-lactam ring.
  • Risk of a cross-reaction between a penicillin and cephalosporin that do not share the same side chain is <2%. Cross-reactivity between penicillin and monobactams is 0%, between penicillin and carbapenems is <1%, and between cephalosporins and carbapenems is <1%.⁶
  • Patients with amoxicillin allergy should avoid cefadroxil, cefprozil, and cefatrizine as all these drugs share same R-group side chain.
  • The monobactam aztreonam does share an identical R1-group side chain as ceftazidime and is cross-reactive.
• Sulfonamide allergy
  • There is an increase in allergy to sulfonamides in patients with HIV compared to the general population. Trimethoprim–sulfamethoxazole hypersensitivity occurs in 60% of HIV-positive patients compared to 5% of HIV-negative patients.⁷
  • Type I IgE-mediated reactions to sulfonamides are not common. The most frequently seen reaction is a maculopapular rash (T cell–mediated) that develops 7–12 days after initiating the drug. Other reactions include urticaria and, less commonly, anaphylaxis, Stevens–Johnson syndrome (SJS), and toxic epidermal necrolysis (TEN). Cross-reactivity between antibiotic and nonantibiotic sulfa-containing medications is low.⁸ Patients with sulfonamide antibiotic allergy were more likely to react to penicillin than a sulfonamide nonantibiotic.⁸
• NSAIDs and aspirin can cause IgE-mediated urticaria, angioedema, and anaphylaxis. It can also exacerbate urticaria in patients who have chronic urticaria. Exacerbation of respiratory symptoms in patients with underlying asthma is referred to as aspirin-exacerbated respiratory disease (AERD). AERD is composed of a triad consisting of asthma, NSAID sensitivity, and nasal polyposis. COX2 inhibitors are generally safe to administer in these patients. Aspirin desensitization followed by daily aspirin therapy in AERD patients improves asthma exacerbations, oral steroid use, reduced nasal polyps, and sinus infections. Certain asthma biologics can also be used in patients with AERD.

Pathophysiology

The immunologic mechanisms for drug hypersensitivity are demonstrated in the Gell and Coombs classification of hypersensitivity (Table 11-1 - Immunologically Mediated Drug Reactions).

Risk Factors

Factors that increase a patient’s risk of an ADR include size and structure of drug, route of exposure (cutaneous most immunogenic), dose, duration, frequency, gender (women > men), genetic factors (HLA type, history of atopy), prior drug reaction, coexisting medical illnesses, and concurrent medical therapy.

Clinical Presentation

• A history is essential for making the diagnosis of an allergic drug reaction. Questions should be directed at establishing the following information: sign and symptoms, timing of the reaction, purpose of the drug, other medications the patient is receiving, prior exposure to drug or related drug, and history of other allergic drug reactions.
• Urticaria, angioedema, wheezing, and anaphylaxis are all characteristics of IgE-mediated (type 1) reactions.
  • Symptoms do not typically occur on the first exposure to the medication unless the patient has been exposed to a structurally related medication. On reexposure, however, symptoms tend to manifest acutely (often <1 hour).
  • IgE-mediated reactions tend to worsen with repeated exposure to the offending medication.
  • Non–IgE-mediated reactions (anaphylactoid) can be clinically indistinguishable from IgE-mediated reactions because the final common pathway for their reaction is mast cell degranulation.
• Maculopapular exanthemas are the most common cutaneous manifestation of drug allergy.
  • These reactions are mediated by T cells and typically delayed in onset, first occurring between 2 and 14 days of exposure to culprit medications. It can occur sooner with subsequent exposures. Lesions typically begin on the trunk, especially in dependent areas, and spread to the extremities.
  • Rarely, these rashes can progress to a more serious drug reaction involving blistering of the skin and/or end-organ involvement.
• DRESS (Drug Reaction with Eosinophilia and Systemic Symptoms) is a serious life-threatening ADR, often presenting as rash and fever with systemic involvement, and can manifest as hepatitis, eosinophilia, pneumonitis, lymphadenopathy, and nephritis.
  • Symptoms tend to present 2–6 weeks after introduction of medication and resolve few weeks to months after stopping the offending agent. Certain viral infections such as Epstein–Barr virus, human herpesvirus (HHV)-6, HHV-7, and cytomegalovirus are associated with increased risk of complications.
  • First described with antiepileptic (carbamazepine) agents but has also been reported to occur with allopurinol, NSAIDs, some antibiotics, and β-blockers.
• Erythema multiforme (EM), SJS, and TEN are all serious drug reactions primarily involving the skin.
  • EM is characterized most typically by target lesions. SJS and TEN manifest with varying degrees of sloughing of the skin and mucous membranes (<10% in SJS and >30% in TEN). Risk factors being HIV, hematological malignancy, systemic lupus erythematosus, and bone marrow transplant.
  • Readministration or future skin testing with the offending drug is absolutely contraindicated.