Vaccination

Last updated: August 29, 2023

Summary

Vaccination is a very effective measure for providing immunity to many infectious diseases. The discovery of vaccines played a central part in the eradication of smallpox and helped significantly reduce the incidence of potentially severe diseases such as poliomyelitis and measles. Live vaccines (attenuated, i.e. noninfective pathogens), inactivated vaccines (subunits or complete pathogens), viral vector vaccines, and nucleic acid vaccines (DNA, RNA, mRNA, or viral replicons) are used to achieve active immunization, which enables the host's immune system to build up a sustained immune response to specific pathogens. The immune response may be measured and quantified by assessing the antibody titer. In the event of potential disease (e.g., after exposure to high-risk pathogens), if the immune system is unable to produce sufficient antibodies fast enough, passive immunization can offer immediate short-term protection via direct injection of pooled antibodies for many conditions. Modern vaccines are usually well-tolerated, and adverse events are rare. However, the intervals between vaccine administration and possible contraindications must be considered.

For ACIP vaccination recommendations, see “Immunization schedule.”

Definition

Vaccine
- A product (e.g., dead or weakened organism) that provides immunity from a disease
- May be administered through injection, orally, or nasally
Vaccination: administration of a vaccine that induces an active immune reaction in form of cellular and/or humoral response, providing immunity against a pathogen
Immunization
- The process by which a person becomes protected from a disease
- Vaccines and recovering from some infections cause immunization.

References:^[1]

Aims of routine immunization

Herd immunity
- Once a certain percentage of the population has received immunization, non-vaccinated individuals (e.g., children too young to receive vaccination) will also be protected.
- Mass vaccination: Vaccination of a large number of people in the shortest possible time after the outbreak of an epidemic, with the goal of herd immunity.
Eradication of disease
- High immunization rates over prolonged periods of time can achieve eradication of certain diseases. ^[2]
- To date, only two diseases have been eradicated by human efforts: smallpox (1980) and rinderpest (2011).
Lower incidence and associated risks: The Haemophilus influenzae type b (Hib) vaccine has decreased the number of cases of invasive Hib disease (e.g., pneumonia, bacteremia, meningitis, epiglottitis, infectious arthritis) in children younger than 5 by more than 99%. ^[3]

Passive immunization

Mechanism of action
- Injection of preformed antibodies induces a rapid humoral response against a specific pathogen
- Provides only temporary protection, as antibodies have a half-life of ∼ 3 weeks and their titers decrease over time.
Examples
- Antitoxins
- Humanized monoclonal antibodies
- Maternal immunoglobulins that are transmitted via breast milk (IgA) or cross the placenta (IgG) to provide passive immunity
Indications
- Acute, post-exposure elimination of a pathogen
  - Viruses: rubella, rabies, hepatitis B
  - Toxins: tetanus, botulinum, diphtheria
- Rhesus incompatibility prevention
Application: Vaccines are available for intramuscular as well as for intravenous injection .
Combination
- Simultaneous vaccination
  - Two different passive vaccines may be administered simultaneously.
  - An inactivated active and a passive vaccine may be administered simultaneously (e.g., in acute hepatitis A, hepatitis B, rabies, or tetanus infection). ^[4]
- After transfusion of certain blood products and/or immunoglobulin therapy, live vaccines should be delayed depending on the estimated amount of IgG in the transfusion. ^[5]^[6]

“Passive immunization Helps Beat The Disease Rapidly:” HBV, Botulinum, Tetanus, Diphtheria, and Rabies are indications for passive immunization.

Active immunization

General information
- In active immunity, the body's immune system reacts to the presence of antigens by producing antibodies.
- In general, a combination of different active vaccinations is possible.
- Slow onset, but immunity usually lasts for years or even a lifetime.
- Besides vaccines and toxoids, natural infections lead to active immunization as well.
Classification
- Live attenuated vaccines
- Inactivated vaccines
  - Whole vaccines
  - Subunit vaccines
    - Protein-based (subunit and toxoid vaccines)
    - Polysaccharide-based
- Viral vector vaccines
- Nucleic acid vaccines (DNA, RNA, mRNA, or viral replicons)

Current vaccination recommendations for the US can be found in the “Immunization schedule.”

Vaccine types Standard vaccine development Accelerated vaccine development during the SARS-CoV-2 pandemic

Live attenuated vaccines

Definition: Modified functioning virus or bacterium that can replicate in the patient's body but does not cause disease.
Mechanism of action
- Similar to an infection with a “wild” pathogen and induces a cellular and humoral immune response.
- Specific B-cells against an antigen are formed; , which induces a potent, lifelong immune response
Administration
- Oral vaccine or subcutaneous/intramuscular injection in children > 12 months
- Not indicated in children < 9 months; (the rotavirus vaccine is an exception, which is first given at 6 weeks of age)
- Second dose usually recommended to “catch” non-responders (not as a boost)
- Multiple live vaccines can be given simultaneously, but if given at different times they should be at least 4 weeks apart to avoid possible interference.
- May be administered simultaneously with inactivated vaccines
Available vaccines
- MMR: prevents measles, mumps and rubella infections
- Varicella: against varicella-zoster virus (VZV)
- Zoster: prevents reactivation of latent VZV (i.e., shingles)
- Yellow fever
- Rotavirus
- Influenza (intranasal)
- Smallpox
- Adenovirus
- Oral polio, Sabin (no longer available in the US)
- BCG
- Typhoid (oral, Ty21a)
Special considerations
- Very rarely, live attenuated vaccines may become virulent again and are thus often contraindicated in immunodeficient individuals and pregnant women .
- HIV-positive individuals can be vaccinated with live attenuated vaccines (e.g., MMR and varicella) if their CD4 cell count is ≥ 200 cells/mm³.
- Adenovirus vaccine is given in its nonattenuated form to military recruits.

“TYler And Paul Burnt their INFamous ROasted YELLOW-RUBy CHICKEN MEAt Very MUch”: TYphoid, Adenovirus, Polio, BCG, INFluenza, ROtavirus, YELLOW fever, RUBella, CHICKENpox, MEAsles, Varicella, and MUmps are live attenuated vaccines.

Comparison of intramuscular (IM) and subcutaneous (SC) injection

References:^[7]^[8]

Inactivated vaccines

Overview of inactivated vaccines
	Whole vaccines	Subunit vaccines
	Whole vaccines	Protein-based		Polysaccharide-based
Characteristics	Whole inactivated or dead pathogens (using chemicals or heat) that are unable to replicate Surface epitopes remain unchanged, since they are important for triggering an adequate immune response. Cause a weaker immune response, but are considered to be safer than live vaccines	Inactive antigenic subunits of pathogens that provoke the most effective immune response Weaker immune response and more expensive But lower risk of adverse reactions	Toxoids are bacterial toxins in which the toxicity has been inactivated while immunogenicity is maintained through intact receptor binding sites. Immune system reacts to exposure with production of antibodies against bacterial toxins → protective immunization	Bacterial cell wall polysaccharide Conjugate polysaccharide vaccine is linked to a protein
Available vaccines	Polio (Salk; inactivated vaccine) Hepatitis A Rabies Typhoid (Vi polysaccharide; IM) Influenza Pertussis (cellular vaccine) Cholera Japanese encephalitis Tick-borne encephalitis	Subunit Hepatitis B (using the HBsAg) Influenza Pertussis (acellular vaccine) HPV (specifically types 6, 11, 16, and 18) Anthrax	Toxoid vaccine Diphtheria (C. diphtheria) Tetanus (Clostridium tetani)	Hib (conjugate vaccine) Pneumococcal vaccine PCV13 (conjugate vaccine) PPSV23 (unconjugated vaccine) Meningococcal vaccine (conjugate vaccine; various strains of Neisseria meningitidis) Salmonella typhi
Mechanism of action	Mostly humoral immune response Number of circulating antibodies decreases over time			Polysaccharides induce a relative T cell-independent B-cell response and therefore achieve sufficient immunization only in adults and older children. In conjugate vaccines, the carrier protein activates T-cells, which stimulate a more rapid and long-lasting immune response, especially in infants and toddlers.
Special considerations	Less affected by circulating antibodies than live vaccines			Not consistently immunogenic in infants
Administration	Usually injected into the deltoid muscle (alternatively, e.g., in infants, injected into the vastus lateralis muscle) First dose does not provide protective immunity Multiple doses required Periodic “boosts” necessary to ensure sufficiently high antibody titers Inactivated vaccines may generally be combined with other vaccines without any time interval in between

“Beware of Hepatitis A on your TRIP:” Hepatitis A, Typhoid fever, Rabies, Influenza, and Poliomyelitis.

References:^[9]^[10]

Viral vector vaccines

Definition: an unrelated virus (e.g., adenovirus, vesicular stomatitis virus, influenza virus) is modified to be used as a nonpathogenic vector that delivers genetic code to cells containing instructions for the production of the desired antigen. ^[11]
Mechanism of action
- There are two types of viral vector vaccines: replicating and nonreplicating
  - Nonreplicating vector vaccines: enter the cells and induce the production of vaccine antigens, but cannot produce new viral particles
  - Replicating vector vaccines
    - Enter the cells, inducing the production of new viral particles
    - New viral particles go on to infect other host cells, leading to the production of further viral and vaccine antigens
- Induce both humoral and cellular immune responses
Administration: usually injected intramuscularly, but can also be administered intranasally, intradermally, and orally
Available vaccines
- Ebola virus vaccine (rVSV-ZEBOV; Ervebo)
- COVID-19 vaccine (Janssen COVID-19 vaccine, Vaxzevria, Sputnik V vaccine)
Special considerations
- Preexisting immunity to the virus that serves as the vector may affect the effectiveness of a vaccine. ^[12]
- Less strict storage and handling conditions than nucleic acid vaccines
- Viral vectors are genetically stable and lack a viral genome and nonstructural proteins. Therefore, they do not interact or integrate into the host's DNA and are nonpathogenic.

Mechanism of action of viral vector-based COVID-19 vaccines

Nucleic acid vaccines

RNA vaccines ^[13]^[14]

Definition: a vaccine based on mRNA that delivers genetic code containing instructions for the production of the desired antigen to cells
Mechanism of action
- Two types of mRNA vaccines: nonreplicating and self-amplifying
  - Nonreplicating mRNA vaccines: contain the sequence of the desired antigen and the 5′ and 3′ untranslated regions
  - Self-amplifying mRNA vaccines: contain the sequence of the desired antigen and the viral replication machinery (e.g., RNA polymerase) that enables intracellular RNA amplification
- Both types induce humoral as well as cellular immune responses.
Administration
- Injected intramuscularly or intradermally
- Require multiple doses
Available vaccines: COVID-19 vaccines (e.g., Comirnaty, Spikevax) contain modified mRNA embedded in lipid nanoparticles that encodes for the spike protein mRNA sequence of SARS-CoV-2
Special considerations
- mRNA is a nonintegrating platform that is degraded by normal cellular processes. Due to its transitory nature, mRNA does not interact or integrate into the DNA and bears no risk of insertional mutagenesis. (e.g., COVID-19 vaccines are safe to use during pregnancy)
- There is no potential risk of infection as mRNA is nonpathogenic.
- Require strict cold-chain
- Different techniques can be used to deliver the vaccine (e.g., injection of naked mRNA or encapsulated within nanoparticles or polyplex)

Mechanism of action of mRNA-based COVID-19 vaccines

DNA vaccines ^[15]

Definition: A specific antigen-coding DNA sequence is introduced using a genetically engineered plasmid to induce endogenous antigen production in the host.
Mechanism of action
- After entering the cells, the vaccine antigen is expressed from the DNA construct.
- Induce both humoral and cellular immune responses
Administration
- Intramuscularly or intradermally
- Require multiple doses
Available vaccines: No DNA vaccines have been approved for human use in the United States.
Special considerations
- Potential advantages observed in animal models are improved vaccine stability and the use of nonpathogenic agents.
- In order to properly deliver the vaccine and ensure cellular uptake, injection needs to be followed by electroporation.

Vaccine administration

Clinical Skills: Administering Vaccinations Comparison of intramuscular (IM) and subcutaneous (SC) injection

Adverse effects of vaccination

Common adverse effects ^[16]^[17]^[18]

Affects ∼ 1/3
Usually begin within the first 48–72 hours after administration and last 1–2 days
Symptoms
- Local swelling, redness, and pain at the injection site
- Low-grade fever (postvaccination fever)
- Headaches
- Fatigue
- Flu-like symptoms
Live attenuated vaccine: can cause mild form of the disease, usually appearing within 1–3 weeks of administration; : usually caused by replication of the attenuated vaccine strain

Rare adverse effects ^[16]^[17]^[18]

Cardiovascular complications: observed in young men who received mRNA vaccines (COVID-19 vaccines) ^[19]
Serious allergic reaction (generally < 1 per million doses)
Live attenuated vaccine: attenuated course of the disease following immunization (e.g., vaccine-related measles)
Vaccine injury (∼ 1/1,000,000): permanent injury from a vaccination or a vaccine-related complication (e.g., encephalopathy, seizures, brachial neuritis)

There is no link between autism and vaccines or their ingredients. ^[20]^[21]

Contraindications for vaccination

Precautions

General precautions
- A precaution is a condition in the recipient that might increase the risk for serious adverse reactions or interfere with a vaccine's ability to produce immunity.
- Generally, vaccination should be deferred when a precaution is present, except when the benefits of protection outweigh the risks.
- Acute moderate or severe illness (with or without fever)
Special precautions
- Rotavirus vaccine: uncorrected GI tract malformation (e.g., Meckel's diverticulum)
- Egg protein-containing vaccines: allergic reactions other than urticaria (e.g., angioedema, bronchospasm) to egg products
- Pertussis vaccine: progressive or unstable neurologic disorders (e.g., uncontrolled epilepsy, infantile spasms, progressive encephalopathy) ^[22]
- Tetanus toxoid-containing vaccines
  - Development of Guillain-Barré syndrome within 6 weeks of a previous dose
  - Arthus reaction after a previous dose ^[22]

Contraindications ^[23]

General contraindications
- Vaccines are generally contraindicated in recipients with conditions that increase the risk for severe vaccine reactions or in whom the vaccine may exacerbate the condition.
- Previous severe adverse reactions (e.g., anaphylaxis)
- Severe adverse reactions to a vaccine component (e.g., egg protein in yellow fever vaccine, yeast in hepatitis B vaccine)
Contraindications to live vaccines
- Rotavirus vaccine
  - Severe combined immunodeficiency (SCID)
  - History of intussusception ^[24]
- Pertussis vaccines: risk of encephalopathy (e.g., prolonged seizures, decreased level of consciousness, coma) within 7 days following a previous dose
- Live, attenuated virus vaccinations ^[22]
  - Pregnant individuals
  - Immunodeficient individuals (e.g., individuals receiving chemotherapy or long-term immunosuppressive therapy, individuals with congenital immunodeficiencies, patients with HIV and severe immunocompromise)
  - Individuals receiving IVIG therapy (e.g., for Kawasaki disease)
False contraindications ^[25]^[26]
- Fever within 48 hours
- Current or recent mild illness (e.g., rhinorrhea, otitis media, mild diarrhea)
- Current or recent antibiotic therapy (exception is oral live typhoid vaccine )
- Current or recent low-dose and/or short-term steroid use (i.e., < 2 mg/kg/day or < 20 mg/day, < 14 days)
- Previous mild or moderate localized cutaneous reaction (e.g., swelling, redness, soreness) following any vaccination
- Preterm infants
  - Should be immunized according to chronological age, not gestational age
  - The exception is the hepatitis B vaccine: vaccination should be delayed by a month or until hospital discharge for infants weighing < 2 kg born to HBsAg-negative mothers.
  - Adjustment according to weight: no dose adjustment is needed

All children should be immunized with the standard doses of vaccines according to their chronological age; doses should not be adjusted to weight or height.

Special patient groups

Immunizations during pregnancy, vaccinations in preterm infants, and vaccinations in individuals with HIV are detailed in the “Immunization schedule” article.

Pathogens affecting unvaccinated children

Pathogens affecting unvaccinated and underimmunized individuals
	Disease	Clinical features		Treatment
Measles virus	Measles	Prodromal catarrhal phase (High) fever Koplik spots Coryza, cough, conjunctivitis Exanthem phase (High) fever, malaise Generalized lymphadenopathy Erythematous, maculopapular, blanching, partially confluent exanthem Begins behind the ears along the hairline Disseminates to the rest of the body toward the feet (palm and sole involvement is rare) Transformation into brown discoloration and desquamation can occur in severely affected areas.		Symptomatic treatment Vitamin A supplementation Postexposure prophylaxis (see “Prevention” in “Measles”)
Rubella virus	Rubella	Prodromal phase Low-grade fever, malaise, sore throat, conjunctivitis, cough Postauricular and suboccipital lymphadenopathy Exanthem phase Fine, nonconfluent, pink, maculopapular exanthem Begins on the head, typically behind the ears Extends to the trunk and extremities, sparing the palms and soles Polyarthritis		Symptomatic treatment See “Treatment” in “Rubella.”
Varicella zoster virus	Chickenpox	Prodromal phase: low-grade fever, malaise Exanthem phase Hundreds of severely pruritic lesions in varying stages of development (e.g., papules, vesicles, and crusted pustules) Lesions first manifest centrally (i.e., on the face, scalp, and trunk) and spread to the extremities.		Symptomatic treatment Antiviral therapy for high-risk patients : acyclovir, valacyclovir See “Treatment for chickenpox.”
Mumps virus	Mumps	Prodromal phase: fever, malaise Classic course Inflammation of the salivary glands Most commonly parotitis Usually unilateral Possible orchitis (see “Complications” in “Mumps”)		Symptomatic treatment See “Treatment” in “Mumps.”
Corynebacterium diphtheriae	Diphtheria	Respiratory diphtheria Grayish-white pseudomembranes over the posterior pharyngeal wall and/or tonsils Cervical lymphadenopathy and nuchal soft tissue swelling (bull neck) Foul-smelling breath Difficulty breathing, inspiratory stridor Cutaneous diphtheria		Isolation precautions Airway support Antibiotic therapy: penicillin G OR erythromycin Diphtheria antitoxin See “Treatment” in “Diphtheria.”
Haemophilus influenzae type b	Epiglottitis	High fever Sore throat Dysphagia and odynophagia Drooling Muffled voice (“hot potato voice”) Respiratory distress, tripod position		Airway management in epiglottitis Empiric IV antibiotics Third-generation cephalosporin, such as cefotaxime or ceftriaxone OR beta-lactam with a beta-lactamase inhibitor, such as ampicillin/sulbactam or amoxicillin/clavulanate Consider ajunctive therapy with steroids (dexamethasone OR methylprednisolone). See “Treatment for epiglottitis.”
Haemophilus influenzae type b	Bacterial meningitis	Classic triad: fever, headache, and neck stiffness Photophobia Nausea, vomiting Malaise Altered mental status, seizures	Sore throat, pharyngitis	Isolation precautions Obtain CSF studies and begin empiric antibiotic therapy for bacterial meningitis. Tailor antimicrobial therapy once the pathogen has been identified. For H. influenzae type b and S. pneumoniae: adjuvant dexamethasone For H. influenzae type b and N. meningitidis: Give contacts postexposure chemoprophylaxis for bacterial meningitis. See “Management” and “Treatment” in “Meningitis.”
Streptococcus pneumoniae			Sinusitis, pharyngitis
Neisseria meningitidis			Myalgia Possibly petechial or purpuric rash Possibly Waterhouse-Friderichsen syndrome
Poliovirus	Viral meningitis Poliomyelitis		Gastroenteritis Sore throat Myalgia Asymmetric flaccid paralysis Most commonly affects the leg muscles Usually more severe in proximal muscles	Mechanical ventilation in patients with respiratory failure Supportive treatment See “Treatment” in “Polio.”
Clostridium tetani	Tetanus	Painful muscle spasms and rigidity Trismus, risus sardonicus, opisthotonus Possibly laryngospasm/respiratory muscle spasms, autonomic dysfunction (e.g., circulatory arrest)		Airway support Wound cleaning and debridement Antibiotic treatment: metronidazole OR penicillin G Active and passive immunization (see “Tetanus prophylaxis”) Supportive treatment See “Treatment” in “Tetanus.”
Bordetella pertussis	Pertussis	Prodromal catarrhal phase: URTI symptoms Paroxysmal stage Intense paroxysmal coughing (often occurring at night) Followed by a deep, loud inhalation or high-pitched whooping sound Posttussive vomiting (common) Convalescent stage: Cough may persist for several weeks.		Supportive treatment Oxygen administration with humidification Antibiotic treatment: macrolides such as azithromycin, clarithromycin, or erythromycin See “Treatment” in “Pertussis.”
Hepatitis A virus	Hepatitis A	Right upper quadrant pain, tender hepatomegaly Fever, malaise Anorexia, nausea, vomiting Jaundice, pruritus		Supportive treatment Consider antiviral therapy for chronic hepatitis B. Nucleoside analogues or nucleotide analogues (e.g., tenofovir, entecavir) PEG-IFN-α See “Treatment” in “Hepatitis A” and “Management of hepatitis B infection.”
Hepatitis B virus	Hepatitis B

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