SAMPLE The Greater Risk? Disease vs. Vaccine
The Greater Risk? SA M PL E Disease vs. Vaccine Introduction The Greater Risk? Disease vs. Vaccine is a set of quick reference cards for immunization staff. The intention is to educate healthcare personnel to accurately portray disease risk vs. vaccine risk. The front of each card discusses the disease and the back details the vaccine, offering an instant, factual comparison. Hesitant parents don’t recognize the dangers of getting a vaccine preventable disease. Sharing this additional information assists them in making an informed decision. The Greater Risk? Disease vs. Vaccine The Vaccine Preventable Disease Community Program Snohomish Health District in Everett, Washington. 3020 Rucker Avenue, Suite 208, Everett, WA 98201 www.snohd.org © Snohomish Health District. To request additional copies or for permission to re-use content, contact: 425.339.5234 The Greater Risk? Disease vs. Vaccine Table of Contents • Safety Considerations in Vaccination • Diphtheria • Haemophilus influenzae Type B • Hepatitis A • Hepatitis B • Human Papilloma Virus • Influenza • Measles • Meningococcal Disease • Mumps • Pertussis • Pneumococcal Disease • Polio • Rotavirus • Rubella • Tetanus • Varicella Safety Considerations in Vaccination UNIVERSAL CONTRAINDICATION FOR ALL VACCINES: A severe allergic (anaphylactic) reaction to a previous dose or a vaccine ingredient. 2. CONTRAINDICATION: A condition in a patient that greatly increases the chance of a serious adverse reaction. A contraindication can be permanent or temporary (i.e. pregnancy). 3. PRECAUTION: A condition in a patient that might increase the chance of a serious adverse event. 4. FALSE CONTRAINDICATIONS: Mild illness; antibiotic therapy; disease exposure or convalescence; pregnant or immunocompromised person in the household; breastfeeding; preterm birth; allergy to products not present in vaccine; allergy that is not anaphylactic; family history of adverse events; Tuberculin skin test (affects the timing of a vaccine, but doesn’t prevent it being given); multiple vaccines due at one visit. 5. IMMUNE COMPROMISED INDIVIDUALS: PL M LIVE VACCINES can cause severe or fatal reactions in immunocompromised persons due to uncontrolled replication of the vaccine virus. Examples of diseases causing immunosuppression: Congenital immunodeficiency, leukemia, lymphoma, generalized malignancy. Drugs causing immunosuppression: chemotherapy, corticosteroids. SA E 1. INACTIVATED VACCINES can be given if indicated. Hematopoietic Cell Transplant: re-vaccinate with inactivated vaccines 6 months after transplant. 6. RECENT USE OF ANTIBODY CONTAINING BLOOD PRODUCTS may delay some vaccines because the blood product antibodies may interfere with vaccine antibody production. 7. Always consult package insert for specific manufacturer information. 8. Always carefully screen a recipient for any contraindications or precautions. Diphtheria Transmission Respiratory tract droplets; cutaneous diphtheria by contact with skin lesions. Incubation 2 to 5 days, range 1-10 days. Symptoms Low grade fever, sore throat, a membrane in the nose or throat, very swollen neck glands. Contagious Highly contagious. M PL E Agent Toxin-producing bacteria Corynebacterium diphtheria. SA Heart, kidney and neurological problems because the toxin affects protein production in all body cells. Possible complications Pneumonia, respiratory failure. Airway can be blocked by a membrane resulting in coma and death. Disease risk Severe disease is usually in the unimmunized. Overall fatality rate is 5%-10% but up to 20% in children under 5 and adults over 40. Treatment Anti-toxin and antibiotics; active vaccination during convalescence. Diphtheria Vaccine(s) Diphtheria in combination with tetanus toxoid as DT (pediatric), as Td (adult), with tetanus and pertussis as DTaP and Tdap. Appearance After reconstitution and/or shaking, combination vaccine is a white cloudy liquid. Read package insert for description and specific directions. Dose/route 0.5ml IM. Vaccine risk Local reactions (redness, swelling, pain) are common. An exaggerated local (Arthus) reaction occurs occasionally. A severe reaction may occur 1:1 million doses administered. Fever, hives, neurological complications are rare. False Contraindications Minor illness, pregnancy, immunosuppression. Haemophilus influenzae type b disease (HIB) Bacteria. Infection can occur in a variety of sites: brain, lungs, heart, joints, blood stream, bones, abdomen. Transmission Inhalation of respiratory tract droplets or direct contact with respiratory tract secretions. Incubation Unknown. Symptoms The most severe symptoms occur when bacteria enter bloodstream. Symptoms depend on site affected (i.e. fever, irritability, stiff neck with meningitis; life-threatening airway obstruction with epiglottitis). Contagious Limited, but increased in household, child care or institutional setting. Possible complications Hearing impairment or neurological damage (15% - 30% of survivors), serious breathing problems. Death rate is 2%-5% regardless of antibiotic therapy. Disease risk High risk populations: children up to age 5, older children and adults with anatomic or functional asplenia, sickle cell disease, immunodeficiency, chemotherapy, HIV infection and recipients of a hematopoietic stem cell transplant. Treatment Antibiotics and supportive care. SA M PL E Agent Haemophilus influenzae type b disease (HIB) Vaccine(s) Both single antigen and combination vaccines are conjugated. Not all vaccines are interchangeable. Consult package insert to verify vaccine dose # and age are appropriate for patient. Appearance Generally, the vaccine is a clear to whitish suspension. Consult package insert for description and other specific information. Dose/route 0.5ml IM. Vaccine risk Swelling, redness, pain at the injection site have been reported by 5%-30% of recipients and usually resolve within 12-24 hours. No known association between HIB vaccine and any serious adverse events. Contraindications To preserve immunological response to later vaccines, infants under 6 weeks should not be immunized. False Contraindication Minor illness. Hepatitis A RNA virus of the picornavirus group. Transmission Most commonly fecal-oral; can be by personal contact, contaminated food or water. Incubation 15 to 50 days, average of 28 days. Symptoms Fever, malaise, jaundice, loss of appetite, nausea. Contagious Symptomatic infection occurs in up to 30% of children under 6; very few have jaundice. In older children and adults, jaundice occurs in 70% of the cases; symptoms last less than 2 months but 10%-15% have prolonged or relapsing disease for as long as 6 months. Possible complications Death from severe hepatitis A is more common in people with underlying liver disease. About 100 people die of Hep A annually in the U.S. Adult hospitalization rates are 11%-22%. Average work loss is 27 days. Adults over 40 are at higher risk for serious outcomes. SA M PL E Agent Disease risk Increased risk: international travel, household or personal contact with a child attending a child care facility during a food-borne outbreak, men who have sex with men, and illegal drug users. Treatment Supportive measures. Immune globulin IM within 2 weeks post-exposure or pre-exposure to protect infants under12 months traveling out of country. Infants over 12 months, older children and adults under 40: give dose #1. Adults over 40 should initially receive both IG and dose #1 of vaccine. Hepatitis A Vaccine(s) Inactivated whole-virus vaccine. Two brands are interchangeable and have a pediatric and an adult version. Available in single antigen or combination A/B vaccine for adults needing both. Appearance Generally, all brands are a cloudy white suspension. Consult package insert for manufacturer’s description and other specific information. Dose/route 0.5ml IM. Vaccine risk Mild and self-limited local reaction reported by 20%-50% of recipients. Up to 10% complain of malaise, fatigue, low-grade fever. No known severe reactions have been related to vaccine. False Contraindications Pregnancy, immunocompromised status. Hepatitis B Transmission Infected blood or body fluids (serum, semen, saliva). Commonly via contaminated needles or syringes; sexual contact with infected persons; during birth for infants of infected mothers. Incubation 45 to 160 days, average of 90 days. Contagious M PL Symptoms E Agent Hepadnaviridae virus. Remains infectious on environmental surfaces for more than 7 days at room temperature. Infants and children under 5 have milder acute illness than older children and adults. Symptoms vary from loss of appetite, nausea, pain in joints, malaise to jaundice and severe hepatitis. About 2 billion worldwide have been infected, and more than 350 million have lifelong chronic infection; many do not know they are chronically infected. Virus causes acute and chronic hepatitis, scarring of the liver and up to 80% of liver cancer. A person becomes chronically infected when acute infection does not clear, leading to lifetime contagion. Disease risk About 25% of chronically infected people die prematurely of liver cancer; their risk is 300 times greater than those not chronically infected. When a pregnant woman acquires HBV infection, it can cause severe disease in the mother and chronic infection in the fetus. Treatment Supportive care; interferon. SA Possible complications Hepatitis B Vaccine(s) Two single antigen recombinant vaccines with adult and pediatric versions; two combination vaccines: DTaP + IPV + HepB and HepA + HepB. Appearance General appearance is a cloudy, white suspension. Consult package insert for description and specific information. Dose/route 0.5ml or 1.0ml IM; depends on vaccine, age, risk factors. Vaccine risk Mild local reaction and minimal systemic complaints of fatigue, headache, irritability reported in up to 20%. Severe reaction occurs about 1:1 million doses given. Precaution Immunocompromised people can be vaccinated, but response may not be optimal. False Contraindication Pregnancy. Considerations At least 90% of newborns of infected moms will develop chronic infection. Between age 1 and 5 years 25%-50% develop chronic infection. Only 2%-6% of older children and adults become chronically infected. (HPV) Human Papillomavirus Transmission Close contact, primarily sexual contact; rarely to a newborn through the birth canal at delivery, or from non-genital sites. Incubation Unknown, but estimated to range from 3 months to several years; occasionally as long as 10 years Symptoms Most infections are painless and clear spontaneously; when infection persists, it is the primary risk factor for developing abnormal cells and cancers including cervical, anal, vaginal, vulvar, penile, and some head and neck cancers. It may take more than a decade for abnormal cells to become cancerous. PL M Incidence of infection is 40% by 24 months after first sexual intercourse. More than 80% of sexually-active women are infected by age 50. Men get and transmit genital warts and can develop cancers. SA Contagious E Agent Forty types of human papillomaviruses (HPV) can infect the genital tract. Types 16, 18, 31 and 45 are most associated with cancer; many others cause genital warts. Possible complications HPV is thought to be responsible for 70% of cervical cancer, 90% of anal cancer, 40% of vulvar, vaginal, or penile cancers and 12% of oral and pharyngeal cancers. Disease risk About 12,000 new cervical cancer cases and about 4,000 deaths in the U.S. annually. Numbers much higher worldwide in countries where women do not have regular Pap smears. Treatment Vaccination is key in the prevention of cervical cancer. Regular Pap testing is still indicated. A variety of treatments used to eliminate the lesions. Human Papillomavirus (HPV) Vaccine(s) Vaccines use recombinant DNA technology. One is bivalent (HPV2) and one is quadrivalent (HPV4). Both vaccines are licensed for females 9-26. Males 9-26 receive only the HPV4 vaccine to protect against genital warts and cancer. Appearance Both vaccines are cloudy, white liquids. Consult package insert for description and specific instructions. Dose/route 0.5ml IM. Vaccine risk Mild local reactions reported 20%-90% of the time. A fever of 100 degrees in the 15 days following either vaccine was reported by 10%-13% of recipients. Fainting has been reported by adolescents who received additional vaccines at same visit; observe for 15 minutes following vaccine. No serious adverse events have been proven related to HPV vaccine. Contraindication Although not associated with any adverse pregnancy outcomes, should be delayed until after delivery. Precaution Immunosuppressed females can be vaccinated, but vaccine efficacy may be less. False Contraindications Mild illness, breastfeeding. Consideration The catch up schedule uses the same intervals as the routine recommendation. Seattle policemen in masks during influenza epidemic, Dec 1918 Influenza (the ‘flu’) Transmission Person-to-person via respiratory droplets created by coughing or sneezing. Incubation 1 to 4 days, with an average of 2 days. Symptoms Sudden onset of fever accompanied by chills, headache, malaise, muscle aches, mild cough; next sore throat, nasal congestion, runny nose, worsening cough. Less common are bloodshot eyes, abdominal pain, nausea, vomiting, diarrhea. SA M PL E Agent Virus of the orthomyxovirus family. The viruses are separated into groups A, B or C. Contagious Highly contagious. Highest attack rates occur among school-age children who spread flu secondarily to siblings and adults. Possible complications Pneumonia (secondary bacterial) is the most common complication. Other complications include Reye’s syndrome, inflammation of heart muscle, death. Disease risk Majority of deaths occur in persons 65 and older (90%), young children, those with underlying medical conditions. Hospitalization rates of children birth to 4 are similar to persons 65 years of age or older. Treatment Supportive care, antiviral medications, antibiotics for secondary bacterial infections. Influenza (the ‘flu’) Vaccine(s) Recommended annually for everyone 6 months or older. All vaccines are multi-valent and contain group A and group B strains. The C group is mild and infrequent so is not in the vaccine. There are several versions of vaccine: injectable inactivated (TIV), high dose inactivated injectable (TIV), intradermal, live attenuated nasal mist (LAIV). Appearance Vaccine appearance varies with the brand. Consult package insert for description and other specific information. Dose/route TIV dose 0.25 ml or 0.5 ml IM; Intradermal 0.1 ml IM with a micro injector; nasal mist 0.2 ml divided with 0.1 ml sprayed into each nostril. Vaccine risk TIV: local reaction (15%-20%). Fever and malaise uncommon; allergic reactions rare; neurological reactions very rare. LAIV: runny nose and headache (10%-40%). Intradermal: no serious adverse reactions have been identified. Contraindications LAIV: Asthma, a recent wheezing episode, reactive airway disease or other chronic pulmonary or heart condition, metabolic disease such as diabetes, kidney disease or abnormal hemoglobin, such as sickle cell disease, children and adolescents receiving long-term aspirin therapy, immunosuppression, pregnancy, history of severe allergy to egg, severe illness or nasal congestion. Precautions LAIV: History of Guillian Barre’ syndrome within 6 weeks of a previous dose; do not give until 48 hours after stopping anti-viral therapy; do not administer anti-viral medications for 2 weeks after receipt of LAIV. TIV and Intradermal: History of Guillian Barre’ syndrome within 6 weeks of a previous dose. False Contraindications TIV and Intradermal: Pregnancy, breastfeeding, immunosuppressed status. Measles A paramyxovirus. Transmission Primarily person-to-person via large respiratory droplets. Airborne transmission via virus containing droplets in the air for up to 2 hours after a contagious patient leaves a room. Incubation From exposure to first symptoms 10 to 12 days; fever increases over 2-4 days, peaking as high as 103 to 105 degrees F; Koplik spots from 1-2 days before to 1-2 days after the rash. Symptoms Fever, cough, runny nose, redness of the eyes, generalized, raised, red rash. Contagious Highly contagious with an attack rate >90% among susceptible persons. Maximum communicability is from onset of early symptoms to the first 3-4 days of the rash. M PL E Agent Disease risk Sub acute sclerosing panencephalitis (SSPE) is a rare degenerative disease thought to be caused by persistent measles infection in the brain. Onset is about 7-10 years after the measles and it causes progressive deterioration of behavior and intellect, inability to control voluntary muscles, seizures and eventual death. It occurs in 5–10 cases per million reported cases. Treatment Supportive care. SA Possible complications Complications occur in 30% of cases and are more common in children under 5 and adults 20 and older. Pneumonia is the most common cause of death (60%) in children. Acute encephalitis is most common in adults with a death rate of 15%. Lasting neurological damage present in 25%; death is reported in 0.2% of the cases in the U.S. Measles Vaccine(s) Live attenuated vaccine in combination with mumps and rubella (MMR) and with mumps, rubella, and varicella (MMRV). Vaccination is not contraindicated when given within 72 hours of exposure. Immune globulin within 6 days may prevent or decrease the severity of measles. Appearance Lyophilized powder turns to a clear yellow liquid when reconstituted. Dose/route 0.5ml SC. Vaccine risk About 5% have transient rash. Fever > 103 degrees F without other symptoms 6-12 days after vaccination is reported 5%-15%. Children with history of febrile seizures may have seizures. Temporary low platelets occur in from 1:25,000 to 1:2,000,000 doses administered. Central nervous system conditions such as encephalitis occur in less than 1:1,000,000 doses administered. Contraindications Children with egg allergy are at extremely low risk of a severe allergic reaction. Contraindications: Pregnancy or becoming pregnant within 4 weeks after vaccination. Precautions Those who have recently received blood products containing antibodies need to delay vaccination to avoid interference with immune response; those with history of low platelets need to weigh the benefits versus the risk. False Contraindications Close contact with pregnant woman, breastfeeding. Considerations About 49% of deaths are among children younger than 5. Ninety percent of fatal cases occur in those without history of immunization. Blacks and Hispanics are at higher risk than white nonHispanics. Meningococcal Transmission Droplets of bacteria-containing mucus or secretions from the nose and throat of colonized persons; person-to-person, close contact in crowded conditions (i.e. college dorms or military barracks) required for spread. Incubation 3-4 days, range of 2 to 10 days. Symptoms Most common form is meningitis: rapid onset fever, headache, stiff neck, sometimes accompanied by nausea, vomiting, sensitivity to light, altered mental status. Bloodstream infection occurs without meningitis 5%-20% of the time: fever, a red/purple rash, often accompanied by low blood pressure, shock, acute adrenal hemorrhage, multi-organ failure. Least common forms are pneumonia (5% to 15% of cases), arthritis (2%), epiglottitis (1%). SA M PL E Agent Bacterium Neisseria meningitidis; strains A, B, C, Y, and W-135 cause almost all invasive disease. Contagious In households, only 3%-4% had secondary cases and most had one case. This translates into 2-4 cases per 1,000. However, that is 500-800 times the risk in the general population. Possible complications The case fatality rate of invasive disease is 9%12%; and up to 40% for meningococcemia. Disease risk Up to 20% of survivors have permanent conditions, such as hearing loss, neurological damage or amputation of finger(s) or limb(s). Treatment Antibiotics; management of shock and increased intracranial pressure. Meningococcal Vaccine(s) Quadrivalent polysaccharide (MPSV4); quadrivalent conjugate (MCV4). Those with ongoing risk (i.e. microbiologists, military recruits, travelers) should be vaccinated every 5 years. If 1st dose MPSV4 or MCV4 at age 2 – 6 years, vaccinate 3 years later. If the 1st dose > 7 years of age, vaccinate 5 years later. People with persistent complement deficiency and functional or anatomical asplenia should receive a 2-dose primary series given 2 months apart and booster every 5 years. Appearance MPSV4 is a clear, colorless liquid after reconstitution. For MCV4 vaccines, consult package insert for description and specific information. Dose/route MPSV4 0.5ml SC; MCV4 vaccines 0.5mlIM. Vaccine risk MPS4: local reaction (48%), fever up to 3%, malaise and headache within 7 days are reported up to 60% of the time, but only 3% were reported as severe. MCV4 reactions: similar to MPSV4. Precautions If moderately or severely acutely ill, delay until improved. There have been no documented adverse events among pregnant women or newborns (MPSV); there is no data for MCV4. False Contraindications Pregnancy, breastfeeding, immunosuppression. Considerations People with deficiencies in the terminal common complement pathway, functional or anatomic asplenia and HIV are high risk for disease. Mumps A paramyxovirus. Transmission Contact with infected respiratory tract secretions. Incubation 14 to 18 days (range 14 to 25 days). Symptoms Early symptoms: muscle aches, loss of appetite, malaise, headache, low grade fever. Parotitis (swelling of the parotid and other salivary glands) is the most common sign (30%-40%) and occurs within the first 2 days and resolves after 10 days. About one third of infections do not cause swollen glands and appear to be a respiratory tract infection. Contagious Contagious from 3 days before to the fourth day of active disease. SA M PL E Agent Possible complications Symptomatic meningitis (headache and stiff neck) occur in 15% and usually resolves completely. Bilateral testicular inflammation affects about 30% of post-pubertal males, with about 50% having some degree of testicular atrophy, although sterility is rare. Post-pubertal females (5%) may experience ovarian inflammation. Asymptomatic septic meningitis occurs in 50%-60% of cases. Disease risk The least common complications are pancreatitis, joint pain, and kidney inflammation. Deafness occurs in 1: 20,000 reported cases; it is one sided (80%), of sudden onset and permanent. Inflammation of heart muscle with EKG changes is seen in 3%-15%, but usually with complete recovery. Treatment Supportive. Mumps vaccine has not shown to be effective in preventing mumps after exposure. Mumps Vaccine(s) Live-attenuated mumps vaccine is combined with measles and rubella (MMR) and with measles, rubella, and varicella (MMRV). Appearance Once reconstituted, MMR is a yellow clear liquid. Dose/route 0.5 ml SC. Vaccine risk Reactions to MMR are more likely related to the measles or rubella portions of the vaccine (i.e. fever, rash, and joint pain). Severe reactions to the vaccine are very rare. Contraindications Pregnancy, moderate to severe acute illness and immunocompromise due to disease or medication. Precautions Low-dose alternate-day topical or aerosolized steroid preparations or persons who have discontinued steroid therapy for one month or chemotherapy for 3 months can be vaccinated; recent treatment with a blood product may delay vaccination. Most anaphylactic reactions to MMR are not related to egg allergy, but to some other vaccine components, such as gelatin. Considerations Adults are more likely to have severe disease and die from mumps or its complications. Women in the first trimester of pregnancy who contract mumps have increased risk of spontaneous abortion. Pregnancy should be avoided for 28 days after mumps immunization. Pertussis (Whooping Cough) Toxin-producing bacterium Bordetella pertussis. Transmission Close contact with cases via aerosolized droplets. Neither infection nor immunization provides lifelong immunity. Incubation 7 to 10 days, with a range of 5 to 21 days. Symptoms There are three stages of pertussis. The catarrhal stage is characterized by runny nose, sneezing, low grade fever, cough that becomes increasingly severe for 1-2 weeks. The paroxysmal stage is characterized by bursts of rapid coughing with a long inspiration (the ‘whoop’ heard in older children and adults) but the cough does not effectively remove the thick mucus; infants and young children appear very ill, distressed and bluish, some even stop breathing; vomiting mucus after coughing exhausts them; this stage can last up to ten weeks. The convalescent stage is when symptoms gradually resolve over many more weeks; paroxysms often recur with URIs for many months. SA M PL E Agent Contagious As many as 80% of immunized household contacts of a symptomatic case acquire infection due to waning immunity of vaccine. Older siblings, adolescents and adults with mild or asymptomatic disease expose infants. Possible complications Less serious complications include ear infection, loss of appetite, and dehydration. Adolescents and adults may have difficulty sleeping, urinary stress incontinence, or even rib fractures from the violent coughing. The increased pressure of severe paroxysms can result in a collapsed lung, bloody nose, subdural hematomas, hernias, rectal prolapse. Disease risk Those at highest risk of serious complication or death are infants under 6 month. The most common complication is bacterial pneumonia (1 in 20). Neurological complications are more common in infants. One in eighty has seizures or some other neurological issue. Treatment Supportive care; antibiotics for close contacts to prevent disease. Pertussis (Whooping Cough) Vaccine(s) Subunit vaccines contain multiple, purified and inactivated components of B.pertussis cells and vary by manufacturer. Clinical judgment or an outbreak in the community can affect recommendations. A woman who becomes pregnant should receive one Tdap dose either after 20 weeks gestation or immediately postpartum. There is no minimum interval between Tdap and the last tetanus containing vaccine. Appearance A slightly cloudy suspension. Check package insert for description and specific information. Dose/route 0.5ml IM. Vaccine risk DTaP: High fever is reported by 3%-5%; prolonged crying for 3 or more hours reported 1:1,000 doses; local reaction reported by 20%-40%. Severe reactions occur in about 1:1,000,000 doses administered. Tdap: Fever reported in 1.4%, local reaction 21%-66%. Other adverse reactions include GI symptoms, headache, fatigue. No serious adverse reactions have been proven to be caused by Tdap. Contraindications DTaP: Encephalopathy not due to another identifiable cause within 7 days of vaccination and moderate or severe acute illness. Tdap: Encephalopathy as above. Precautions DTaP: Fever of 105 degrees F within 48 hours, not due to another identified cause; collapse or shock like state; inconsolable crying for more than 3 hours; convulsions with or without fever occurring within 3 days. Tdap: History of Guillain Barre’ syndrome within 6 weeks of a previous dose; moderate or severe acute illness; history of a severe local reaction following a prior dose of a vaccine containing tetanus and/or diphtheria toxoids. Pneumococcal Transmission Person-to-person via respiratory droplet contact; people who are colonized (have the bacteria in their respiratory tract but have no symptoms) may develop active infection. Incubation Varies with the site of infection, as short as 1-3 days. Symptoms Pneumonia: abrupt onset of fever, chills, pleuritic chest pain, purulent productive cough, shortness of breath, rapid breathing, poor oxygenation, rapid heart rate, malaise, weakness. Meningitis: stiff neck, fever, altered mental status. Depending on the site of infection: ear pain, chest pain, pus in the eyes. SA M PL E Agent Streptococcus pneumoniae bacterium causes various infections: sepsis, meningitis, acute ear infections, sinusitis, community-acquired pneumonia, pleurisy, eye infections. Contagious An estimated 5%-70% of healthy adults, and 21%-59% of children are colonized (have the bacteria in their respiratory tract but don’t appear ill) and are contagious to others. Possible complications There are 3,000 to 6,000 cases of pneumococcal meningitis a year. The bacteria are found in 28%-55% of middle ear aspirants. Pneumococcal pneumonia causes about 175,000 hospitalizations annually. Complications include: infection of the pleural space, inflammation of the heart muscle, bronchial obstruction with collapse of the lung, formation of a lung abscess. Bacteremia is most common in children, 50,000 cases annually. Disease risk People at highest risk: decreased immune function, anatomic or functional asplenia, chronic heart, lung, liver, or kidney disease, CSF leak, and cigarette smokers. Fatality rate of pneumonia is 5%-7%, but much higher in the elderly. Fatality rate of bacteremia is about 20%, but it can be as high as 60% in the elderly. Death rate for pneumococcal meningitis is about 30%, but as high as 80% in the elderly. Treatment Antibiotics and supportive care. Pneumococcal Vaccine(s) A polysaccharide (PPSV23) and a conjugate vaccine (PCV13) are available, each with its own recommendations. Appearance After vigorous shaking, PCV13 is a homogenous, white suspension. Do not use if it does not resuspend. PPSV23 is clear and colorless. Consult package insert for specific information. Dose/route PCV 13 0.5ml IM; PPSV 0.5ml SC. Vaccine risk PPSV23: 30%-50% report a local reaction. PCV13: <1% have a high fever; up to 50% complain of local reactions and about 8% are considered to be severe (i.e. pain that interferes with limb movement). Localized reactions are more common with the 4th dose and include fever within 7 days (24%-35%). Generalized symptoms: poor appetite and irritability reported by up to 80% of recipients. There are no known serious adverse events caused by either vaccine. Contraindication The safety of PPSV23 has not been studied in pregnant women. Polio A Picornaviridae virus. There are three strains (P1, P2, and P3) and immunity to one strain does not produce significant immunity to the others. Transmission Fecal-oral and respiratory routes. Before and after illness onset, the virus is found in the throat (for about 1 week) and is shed in feces for several weeks. Incubation Asymptomatic or nonparalytic poliomyelitis 3 to 6 days; paralytic polio 7-21 days. Symptoms Up to 95% of all polio infections are asymptomatic but the virus is still transmitted to others. About 4%-8% of polio cases consist of a minor, non-specific illness with no evidence of central nervous system involvement. This is called abortive poliomyelitis and the recovery is less than a week. Minor symptoms are often followed by diminished deep tendon reflexes, severe muscle aches, spasms in the limbs or back. After days or weeks, strength returns, but is asymmetrical. Many persons recover completely and muscle function returns to some degree. Weakness or paralysis still present after 12 months is usually permanent. Less than 1% of cases result in paralysis. M PL E Agent Poliovirus is highly infectious, for the susceptible household contacts it is nearly 100% for children and 90% of adults. Possible complications There are three types of paralytic polio: bulbar, spinal, and bulbarspinal. Bulbar is uncommon and leads to weakness of muscles innervated by the cranial nerves. Spinal is most common and leads to asymmetrical paralysis of the legs. Bulbarspinal is a combination of the two and is the next most common after spinal. Disease risk Death rate for paralytic polio is 2%-5% among children and up to 15%-30% among adults. It increases to 25%-75% with bulbar involvement. Adults who contracted paralytic polio during childhood may develop the noninfectious postpolio syndrome 30-40 years later, which is characterized by slow but significant onset of muscle pain and increasing weakness. Treatment Supportive care. SA Contagious Polio Vaccine(s) Inactivated polio vaccine (IPV) is the only vaccine available in the U.S. It contains all 3 strains and is available in multi-dose vials. There are three combination vaccines: DTaP + IPV + Hib; DTaP + IPV + Hep B, DTaP + IPV. Consult package insert of combination vaccines to determine appropriate age(s) and dose(s). Appearance IPV is a clear, colorless liquid. Dose/route The dose is 0.5 ml SC or IM. Vaccine risk No serious adverse reactions to IPV are documented. Mild local reaction can occur. Contraindications IPV contains trace amounts of streptomycin, neomycin, and polymixin B, but if the allergy is only a local skin reaction, vaccinate as indicated. Precaution Moderate or severe acute illness. False Contraindications Breastfeeding, an infant with diarrhea, a minor URI with or without fever, moderate local reaction to a previous dose, current antibiotic therapy, and recovering from an acute illness. Considerations Although considered eradicated in the U.S., vulnerable travelers can contract it, bring it back and infect others. Rotavirus Transmission Oral-fecal route, close contact or indirect contact with infected persons. Incubation Usually less than 48 hours. Symptoms The first infection is usually the most severe. Infection may be asymptomatic, cause self-limited watery diarrhea or may result in severe dehydrating diarrhea with fever and vomiting. Up to 33% have a fever >102 degrees F. Gastrointestinal symptoms last 3 to 7 days. PL M Highly contagious with nearly universal infection by age 5. Spreads easily within families, institutions, hospitals and child care settings. The virus can be found on toys and hard surfaces. SA Contagious E Agent RNA virus from the family Reoviridae; can remain viable on surfaces in the environment for weeks or months unless the surface is disinfected. Most common cause of severe diarrhea requiring health care in children. Possible complications Infection can lead to severe diarrhea, dehydration, electrolyte imbalance, metabolic acidosis. Children who are immunocompromised by congenital immunodeficiency, by solid organ or bone marrow transplants may experience severe or prolonged gastroenteritis and have evidence of abnormalities in multiple organ systems, particularly the kidney and liver. Disease risk Rotavirus infection accounts for 2.5% of all hospitalizations of children. About 20% of adult household contacts will develop symptomatic infection. Treatment Oral or IV fluids, and supportive care. Rotavirus Vaccine(s) RV1 is a live attenuated vaccine containing one strain of human rotavirus. RV5 has five reassortment rotaviruses. First dose at least 6 weeks but not later than 14 weeks, 6 days. Last dose no later than 8 calendar months, 0 days. Appearance RV1 is a clear colorless fluid; RV5 is pale, clear yellow liquid and may have a pink tint. Dose/route Both are given orally, before any injections, so the infant is less upset. If an infant vomits the vaccine, do not repeat the dose. Vaccine risk Adverse events noted in clinical trials include vomiting (15%-18%), diarrhea (9%-24%), irritability (13%-62%), fever (40% -43%). However the rate of these complaints is the same as unvaccinated infants. Contraindications Severe latex allergy (RV1 has latex in the oral applicator), a history of intussusceptions, severe combined immunodeficiency disease (SCID). Precautions Altered immune competence; acute, moderate or severe gastroenteritis; other acute, moderate or severe illness; children who are immunocompromised require clinical judgment weighing risk versus benefit; infants with HIV may be immunized due to the considerably attenuated vaccine strains versus wild. False Contraindication Breastfeeding. Rubella (German Measles) Rubivirus. Transmission Direct or droplet contact with nose and throat secretions. Up to 50% of infections are asymptomatic. Crosses the placenta during pregnancy causing birth defects and Congenital Rubella Syndrome (CRS). Incubation 14 days, range of 12 to 23 days. Symptoms In children, rash is usually the first sign and a prodrome (early warning signs) is rare. Older children and adults have a 1 to 5 day prodrome with low-grade fever, malaise, swollen lymph glands, and upper respiratory infection before the rash. The rash begins on the face and then progresses head to foot. It lasts about 3 days and may itch. Contagious Most contagious when the rash first appears. Virus may shed from 7 days before to 5-7 days or more after the rash onset. Possible complications Complications generally occur more often in adults than children. M PL E Agent Treatment Supportive care. SA Disease risk Rubella in a pregnant woman can cause fetal death, spontaneous abortion, premature delivery. Congenital Rubella Syndrome (CRS) occurs up to 80% of the time causing a variety of birth defects: deafness, eye defects (cataracts, glaucoma, retinopathy and abnormally small eyes), heart defects, neurological abnormalities, small head, mental retardation, bone lesions, spleen enlargement, hepatitis, low platelets. Other complications: encephalitis occurs in 1:6,000 cases and death estimates are up to 50%; hemorrhagic symptoms occur in 1:3,000, more often in children; gastrointestinal, cerebral, or kidney hemorrhages. A rare, late complication is a progressive inflammation of the white and gray matter of the brain. Sometimes symptoms can be delayed from 2 to 4 years, as in the development of diabetes. Up to 70% of adult women have joint pain and inflammation, but they rarely become chronic. Rubella (German Measles) Vaccine(s) Live attenuated vaccine available in MMR and MMRV. Those born before 1957 are considered immune. Health care workers and pregnant women are held to a stricter standard and must have either laboratory proof of immunity or 2 valid doses of a rubella containing vaccine. Clinical diagnosis is unreliable and should not be considered in assessing immune status. Appearance The vaccine is a clear yellow liquid after reconstitution. Dose/route 0.5ml SC. Vaccine risk Post vaccination complaints of fever and rash are usually related to the measles component of the vaccine. In about 25% of female adolescents and female adults, joint inflammation and pain can follow, lasting 1-3 weeks and fully resolving. Severe allergic reactions to the vaccine are rare. Contraindications Pregnancy or becoming pregnant within 4 weeks after vaccination, immunodeficiency resulting from leukemia, lymphoma, generalized malignancy, immune deficiency disease or immunosuppressive therapy. Precautions Those using an alternate day topical or aerosolized steroid preparation, steroid therapy discontinued for 1 month or chemotherapy for 3 months can be immunized, delay vaccination until a moderate or severe illness is improved. Tetanus (Lock Jaw) Transmission Spores are widely distributed in soil and in the feces of many animals. Bacteria enter the body via a wound. In the low oxygen conditions, spores germinate and produce toxin which spreads through the blood stream and lymphatic system. Incubation 3-21 days. The shorter the incubation period, the higher the chance of death. Symptoms In local tetanus muscle contraction is in the same area as the wound. Contractions persist for weeks and may precede generalized tetanus. Only about 1% of cases are fatal. Cephalic tetanus is a rare type that occasionally occurs with otitis media or following a head injury; there is involvement of the cranial nerves, especially in the face. Generalized tetanus is the most common type (80%); lock jaw is followed by a stiff neck, difficulty in swallowing, and rigidity of abdominal muscles; additional symptoms are fever, sweating, elevated blood pressure, episodic rapid heart rate; spasms occur frequently, last several minutes, and continue for 3-4 weeks; complete recovery may take months; fatality rate is about 11%. Neonatal tetanus occurs in infants born without protective passive immunity from the mother because she is inadequately immunized for tetanus; worldwide it kills more than 257,000 infants annually. SA M PL E Agent An exotoxin produced by the bacterium Clostridium tetani; the bacteria produce spores that can survive autoclaving and chemical agents. Contagious Tetanus is the only vaccine-preventable disease that is not spread person-to-person. Tetanus disease does not result in immunity Possible complications Spasms of the vocal cords and/or spasms of the muscles of respiration can compromise breathing. Secondary infections may include sepsis from indwelling catheters, hospital-acquired pneumonias, and bed sores. Disease risk Pulmonary embolism is a particular problem for the elderly and illegal drug users. Aspiration pneumonia is a common late complication (present in 50%-70% of autopsied cases). Treatment Support measures for an adequate airway. Tetanus Immune Globulin (TIG) helps remove unbound toxin. Once stable, actively immunize. Tetanus (Lock Jaw) Vaccine(s) Tetanus toxoid is available as a single antigen as well as in combination with other antigens: DTaP; DT (pediatric use); Td; Tdap (adult use). Appearance The vaccine is a white homogenous cloudy suspension. Dose/route 0.5ml IM. Vaccine risk Injection site reactions are common; a nodule at the injection site may take weeks to resolve. Systemic symptoms (i.e. fever) are uncommon. Exaggerated local (Arthus-like) reactions (painful swelling from shoulder to elbow) are reported after receiving a dose of a diphtheria-tetanus vaccine, usually in adults who have received excessive doses of tetanus toxoid. Contraindications If a contraindication exists for a multiantigen vaccine, TIG should be considered for serious injuries. Moderate or severe illness is also a contraindication. Considerations Immunization is critical. Major, dirty wounds should be treated with both TIG and tetanus toxoids. Persons with uncertain immunization history or incomplete primary series need TIG for immediate passive immunity and a tetanus vaccine for priming their immune system so that they have the most benefit from completing their primary series. Varicella (chickenpox) A virus of the herpes family. Transmission The virus comes in contact with the respiratory tract or the conjunctiva. Person-to-person requires direct contact, airborne droplets, infected respiratory secretions, or contact with shingles lesions. Incubation 14-16 days and range 10-21 days. Symptoms A generalized, itchy, blistery rash; lesions are in varying stages of development and resolution (crusting), mild fever, malaise. Reactivation of the virus years later results in shingles. Post herpetic neuralgia is pain that persists for weeks or months after shingles lesions heal. Contagious Very contagious with secondary attack rates as high as 90%. PL E Agent Disease risk Among persons 15-19, the death rate is 2.7:100,000 cases but among adults 30-49 the death rate is 25.2:100,000. Treatment Antiviral drugs; supportive care. Immune globulins (VariZIG or IGIV) may prevent or modify varicella disease if given soon enough. Administration of varicella vaccine within 72 hours (and possibly up to 120 hours) after contact may prevent or cause a less severe case. SA M Possible complications Adults have more severe disease and a higher incidence of complications. Infected skin lesions are the most common cause of hospitalization and outpatient medical visits. Pneumonia may follow and is more common in children. Maternal varicella from 5 days before to 2 days after delivery may result in an overwhelming infection of the neonate with a death rate as high as 30%. Immunocompromised persons are at high risk of severe disease that may become hemorrhagic. Other complications: encephalitis, aseptic meningitis, Reye’s syndrome, Guillian Barre’ Syndrome, low platelets, kidney inflammation, heart muscle inflammation, arthritis, hepatitis. Varicella (Chickenpox) Vaccine(s) Single antigen, live attenuated vaccine; may be available in combination as MMRV. Healthcare personnel need either laboratory evidence of immunity or 2 valid documented doses. Appearance A clear colorless to pale yellow liquid when reconstituted. Dose/route 0.5ml SC. Vaccine risk Local reactions are reported by 19% of children and by 24% of adolescents and adults. A varicella-like rash at the injection site is reported by 3% of children and 1% of adolescents and adults after the second dose. A generalized varicella-like rash is reported after the second dose by 4%-6% of recipients and by 1% of adolescents and adults. Severe reactions are very rare. Contraindications Pregnancy or becoming pregnant within 4 weeks after vaccination, immunosuppression due to disease or medication. Precautions HIV infected children with CD4 T-lymphocyte percentage >15% and older children and adults with a CD4 count of >200 per microliter may be considered for single antigen varicella, but should not receive MMRV; moderate or severe acute illness; history of seizures regardless of cause. Consult a reference for those who have recently received antibody containing blood products. False Contraindications Receiving low dose alternate day topical, replacement or aerosolized steroid preparations; those whose steroid therapy has been discontinued for 1 month or chemotherapy for 3 months. Citations: American Academy of Pediatrics. In Pickering LK, Baker CJ, Kimberlin DW, Long SS, eds. Red Book: 2009 Report of the Committee on Infectious Diseases. 28th ed. Elk Grove Village, IL: American Academy of Pediatrics; 2009 Centers for Disease Control and Prevention. Epidemiology and Prevention of VaccinePreventable Diseases. Atkinson W, Wolfe S, Hamborsky J, eds. 12th ed. Washington DC: Public Health Foundation, 2011. Disclaimer: Information in The Greater Risk? Disease vs. Vaccine is current at time of printing. The most up-to-date information regarding vaccines and vaccine-preventable diseases is available at http://www.cdc.gov/vaccines/vpd-vac/default.htm. The Greater Risk? Disease vs. Vaccine Snohomish Health District Vaccine Preventable Disease Community Program 3020 Rucker Avenue, Suite 208 Everett, WA 98201 Published April, 2012
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