Description of the evidence collection method:

Active searches were made on the Pubmed/MEDLINE, Scielo/LILACS and Cochrane Library databases, using the following descriptive terms (MeSH terms): Vaccines, Vaccination, Immunization, Immunization Schedule*, Immunization Programs, Mass vaccination, Vaccines, Inactivated; Vaccines Attenuated, Vaccines,Synthetic; Antiviral Agents, Antibodies, Viral; Virus Shedding*, Disease Notification, Disease Outbreaks, Influenza Vaccines, Influenza A Virus, Influenza, Human/prevention & control, Bacterial Vaccines, Vaccines, Acellular; Antibodies, Bacterial; Diphtheria Vaccine, Pertussis Vaccine, Bordetella pertussis*, Diphtheria/prevention & control; Whooping Cough; Vaccines, Combined; DTPP vaccine, Diphtheria-Tetanus-Pertussis Vaccine, Diphteria Tetanus acellular Pertussis Vaccines, Tetanus, Poliovirus Vaccine, Inactivated; BCG Vaccine,TuberculinTest, Tuberculosis, Pulmonary/prevention & control, Tuberculosis,Tuberculosis,Pulmonary; Pneumococcal Vaccines, Streptococcal Vaccines, Pneumococcal Infection/prevention & control, 23-valente pneumococcal capsular polysaccharide vaccine, heptavalent pneumococcal conjugate vaccine, Splenectomy, Diabetes Mellitus, Diabetes Complications, Anemia, Sickle Cell, Hemoglobinopathies, Pulmonary Disease, Chronic Obstructive; HIV Infections, HIV Seropositivity, AIDS, Acquired Immunodeficiency Syndrome, Cerebrospinal Fluid Rhinorrhea, cerebrospinal fluid leak (CSF), Smoking, Alcohol-Related Disorders, Alcoholism, complications, bacteremia, Liver Cirrhosis, Alcoholic, Immunosuppression, Dose-Response Relationship, Immunologic, Immunizations Programs, Immunization, Secondary; Patient Participation, Dose-Response Relationship, Immunologic; Risk, administration & dosage*; adverse effects*, mortality, Cost-Benefit Analysis, Injections, Intramuscular; Injections, Intradermal; administration, intranasal; utilization, prevention & control; Immunity, Maternally-Acquired; Pregnancy, Pregnancy Complications, Infectious.

Objective

To present alternatives to existing vaccines for the prevention of infectious respiratory diseases in adults, with their recommendations, adverse effects and contraindications.

Introduction

Despite the large advancements in Public Health resulting from immunization, there are still deaths or illness caused by diseases that could be prevented using vaccines.

Vaccination, initially focused exclusively on the child and adolescent range, was extended to all ages. The adult and elderly immunization schedule of the National Adult and Elderly Vaccination Program from the Ministry of Health (MH) is presented below Table 1, and includes some of the vaccines, such as hepatitis and yellow fever immunization, since the focus is on the prevention of respiratory diseases in adults and the elderly.

The vaccines used in adults for the prevention of infectious diseases include four diseases with a high level of invasiveness and morbidity, which contribute to increasing mortality in our patients.

Is there a benefit to the use of flu vaccines?

Flu symptoms are mostly caused by the influenza virus, notably types A and B, the latter on a lower scale.

The high rate of mutation of the virus’ antigenic structure contributes to increasing the annual incidence of the disease at determined times of the year, and justifies the need for annual vaccination, since the protection given by the flu vaccine is temporary³3 Neuzil KM, Maynard C, Griffin MR, Heagerty P. Winter respiratory viruses and health care use: a population-based study in the northwest United States. Clin Infect Dis 2003;37:201-7. (B). Cases of flu used to occur at cold times of the year. In the north region of Brazil, they occur mostly in the rainy period, which coincides with the winter in the Northern Hemisphere (December to February). In the other regions of the country, the peak incidence occurs between May and August. This variability continually challenges the immunological system to carry out its defensive role against the aggression of new variants of the virus circulating in the community. The incidence of hospitalization owing to complications resulting from influenza is 0.8 (CI 95% 0.1-1.15) per 1000 people/year in the age range 18-49 years, and 1.06 (CI 95% 7.5-13.6) per 1000 people/year in patients over 65 years³3 Neuzil KM, Maynard C, Griffin MR, Heagerty P. Winter respiratory viruses and health care use: a population-based study in the northwest United States. Clin Infect Dis 2003;37:201-7. (B).

Aware of this information, specialists coordinated by the US Centers for Disease Control (CDC) and the World Health Organization (WHO) met to decide, based on data derived from sentinel laboratories spread all over the world, on the composition of the flu vaccine to be given from May to October in the Southern Hemisphere and from November to April in the Northern Hemisphere¹1 Brazilian Ministry of Health. Vaccination calendar for adults and the elederly. Available at: http://portal.saude.gov.br/portal/saude/visualizar_texto.cfm? Idtxt=21464. Access on: 11/5/2011..⁴4 Gershon AA, Gardner P, Peter G, Nichols K, Orenstein W. Quality standards for immunization. Guidelines from the Infectious Diseases Society of America. Clin Infect Dis 1997;25:782-6., ⁵5 www.cdc.gov Acesso em: 12/16/11., ⁶6 www.who.int/in Acesso em: 12/16/11. (D).

The vaccine used in Brazil is the trivalent type, with inactivated fragmented viral particles7(D), with a recommended adult dose of 0.5 mL intramuscularly in the deltoid region.

Inactive seasonal flu vaccines have been used since 1940⁸8 Fiore AE, Bridges CB, Cox NJ. Seasonal influenza vaccines. Curr Top Microbiol Immunol 2009;333:43-82. (D). The vaccine is inactivated using formaldehyde, uses thimerosal as a preservative and is produced by viral growth in embryonated chicken eggs. Given the greater power of mutation of type A, the composition of the vaccine normally contains two antigenic variants of type A and one variant of type B. There is a benefit to the use of inactivated trivalent vaccine in relation to the attenuated vaccine. The inactivated form leads to a higher number of serum antibodies and there is a tendency for a lower number of vaccine reactions (0.5% versus 0.8%), but with no significant differences. Patients immunized with inactivated vaccine that subsequently develop flu symptoms have lower fever intensity⁹9 Lai H, Aronow WS, Gutwein AH. Prevalence of influenza vaccination and pneumococcal vaccination in elderly and high-risk patients seen in a university general medicine clinic. Am J Ther 2008;15:528-30. (B).

The vaccine is formally contraindicated for individuals allergic to eggs or egg derivatives or who have presented allergies to previous doses. For patients with previous diagnosis of Guillain-Barré syndrome, the use of the vaccine should be studied carefully⁸8 Fiore AE, Bridges CB, Cox NJ. Seasonal influenza vaccines. Curr Top Microbiol Immunol 2009;333:43-82. (D). There is also voluntary refusal of the vaccine, even in patients considered as high risk¹⁰10 Forrest BD, Steele AD, Hiemstra L, Rappaport R, Ambrose CS, Gruber WC. A prospective, randomized, open-label trial comparing the safety and efficacy of trivalent live attenuated and inactivated influenza vaccines in adults 60 years of age and older. Vaccine 2011;29:3633-9. (B).

In general, the use of inactivated vaccine is well tolerated, few collateral effects being described. Pain in the vaccination site is the most frequent adverse effect, potentially reaching 46% of injections. Low intensity fever and light systemic symptoms such as fatigue (24%), headache (19%) and myalgia (18%) may occur 8 to 24 hours after immunization¹¹11 Song JY, Cheong HJ, Woo HJ, Wie SH, Lee JS, Chung MH, et al. Immunogenicity and safety of trivalent inactivated influenza vaccine: a randomized, doubleblind, multi-center, phase 3 clinical trial in a vaccine-limited country. J Korean Med Sci 2011;26:191-5. (A).

The medical literature has demonstrated that the systematic use of flu vaccines does not decrease the prevalence of the clinical symptoms of flu¹²12 www.eswi.org Acesso em: 12/16/11..¹³13 www.nih.gov Acesso em: 12/16/11. (D), however it causes a significant reduction in cases of pneumonia, hospital admissions and death caused by the illness. There is a fall of 27%¹⁴14 Thompson DL, Jungk J, Hancock E, Smelser C, Landen M, Nichols M, et al. Risk factors for 2009 pandemic influenza A (H1N1)-related hospitalization and death among racial/ethnic groups in New Mexico. Am J Public Health 2011;101:1776-84. (B) to 32%¹⁵15 Nichol KL, Margolis KL, Wouremna J, von Sternberg T. Effectiveness of influenza vaccine in the elderly. Gerontology 1996;42:274-9. (B) in the number of hospitalizations for pneumonia or flu, and a reduction of 37%¹⁶16 Diego C, Vila-Córcoles A, Ochoa O, Rodriguez-Blanco T, Salsench E, Hospital I, et al. Effects of annual influenza vaccination on winter mortality in elderly people with chronic heart disease. Eur Heart J 2009;30:209-16. (B), 45%¹⁵15 Nichol KL, Margolis KL, Wouremna J, von Sternberg T. Effectiveness of influenza vaccine in the elderly. Gerontology 1996;42:274-9. (B), 48%¹⁴14 Thompson DL, Jungk J, Hancock E, Smelser C, Landen M, Nichols M, et al. Risk factors for 2009 pandemic influenza A (H1N1)-related hospitalization and death among racial/ethnic groups in New Mexico. Am J Public Health 2011;101:1776-84..¹⁷17 Nichol KL, Nordin J, Mullooly J, Lask R, Fillbrandt K, Iwane M. Influenza vaccination and reduction in hospitalizations for cardiac disease and stroke among the elderly. N Engl J Med 2003;348:1322-32. (B), and even 50%¹⁷17 Nichol KL, Nordin J, Mullooly J, Lask R, Fillbrandt K, Iwane M. Influenza vaccination and reduction in hospitalizations for cardiac disease and stroke among the elderly. N Engl J Med 2003;348:1322-32. (B) in the risk of death for all causes in the winter14(B). It also reduces the number of office visits (17% for pneumonia or flu and 6.4% for visits due to any respiratory condition) as well as reducing the cost of hospitalization by 30.7%¹⁵15 Nichol KL, Margolis KL, Wouremna J, von Sternberg T. Effectiveness of influenza vaccine in the elderly. Gerontology 1996;42:274-9. (B). Flu vaccines reduce the risk of hospitalization for cardiac diseases by 19% (p<0.001), and between 16 and 23% for cerebrovascular diseases (p<0.018 and p<0.001, respectively)¹⁷17 Nichol KL, Nordin J, Mullooly J, Lask R, Fillbrandt K, Iwane M. Influenza vaccination and reduction in hospitalizations for cardiac disease and stroke among the elderly. N Engl J Med 2003;348:1322-32..¹⁸18 Sandoval C, Walter SD, Krueger P, Smieja M, Smith A, Yusuf S, et al. Risk of hospitalization during influenza season among a cohort of patients with congestive heart failure. Epidemiol Infect 2007;135:574-82. (B), as well as reducing mortality for cardiac causes in 37% of the cases¹⁶16 Diego C, Vila-Córcoles A, Ochoa O, Rodriguez-Blanco T, Salsench E, Hospital I, et al. Effects of annual influenza vaccination on winter mortality in elderly people with chronic heart disease. Eur Heart J 2009;30:209-16..¹⁸18 Sandoval C, Walter SD, Krueger P, Smieja M, Smith A, Yusuf S, et al. Risk of hospitalization during influenza season among a cohort of patients with congestive heart failure. Epidemiol Infect 2007;135:574-82. (B).

In principle, any person over 6 months of age can use the vaccine annually; however, in general, on account of limited stocks, it is recommended for the vaccine to be administered preferably to the following groups of people⁷7 Hurley LP, Wortley P, Allison MA, O’Leary S, Daley MF, Babbel C, et al. Seasonal influenza vaccination in adults: practice and attitudes about collaborative delivery with community vaccinators. Vaccine 2011;29:8649-55. (D):

Recomendation

The flu vaccine available in Brazil is the trivalent type with fragmented and inactivated viral particles, whose application should be done intramuscularly and annually. The use of the flu vaccine is indicated for special groups of adults¹1 Brazilian Ministry of Health. Vaccination calendar for adults and the elederly. Available at: http://portal.saude.gov.br/portal/saude/visualizar_texto.cfm? Idtxt=21464. Access on: 11/5/2011..⁴4 Gershon AA, Gardner P, Peter G, Nichols K, Orenstein W. Quality standards for immunization. Guidelines from the Infectious Diseases Society of America. Clin Infect Dis 1997;25:782-6., ⁵5 www.cdc.gov Acesso em: 12/16/11., ⁶6 www.who.int/in Acesso em: 12/16/11. ⁷7 Hurley LP, Wortley P, Allison MA, O’Leary S, Daley MF, Babbel C, et al. Seasonal influenza vaccination in adults: practice and attitudes about collaborative delivery with community vaccinators. Vaccine 2011;29:8649-55. (D). The vaccine does not reduce the clinical symptoms of the illness, but enables significant reductions in pneumonias, hospital admissions and death caused by flu¹⁴14 Thompson DL, Jungk J, Hancock E, Smelser C, Landen M, Nichols M, et al. Risk factors for 2009 pandemic influenza A (H1N1)-related hospitalization and death among racial/ethnic groups in New Mexico. Am J Public Health 2011;101:1776-84. (B) ¹²12 www.eswi.org Acesso em: 12/16/11..¹³13 www.nih.gov Acesso em: 12/16/11. (D). It is formally contraindicated in individuals allergic to eggs or egg derivatives and to those who have displayed allergies in previous doses⁸8 Fiore AE, Bridges CB, Cox NJ. Seasonal influenza vaccines. Curr Top Microbiol Immunol 2009;333:43-82. (D).

Is there benefit to the use of pertussis vaccines?

There are three vaccines against whooping cough for adults licensed in Brazil¹⁹19 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular). Booster..,²⁰20 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated),²¹21 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated). (D). These vaccines are only available in private services²²22 Brazilian Association of Immunization. Vaccination calendar for adults and the elederly, 2011. Available at: http://www. sbim. org.br/sbim_ calendarios_2011_adulto.pdf. Access on: 11/5/2011. (D).

The first vaccine, licensed in 2001, is composed of a combination of three components against diphtheria, tetanus and acellular pertussis (dTpa)¹⁹19 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular). Booster.. (D). The other two vaccines were licensed in Brazil in 2011 but being used at a global level since 2005²⁰20 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated).²¹21 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated). (D). Both combine components against diphtheria, tetanus, acellular pertussis and inactivated poliomyelitis (dTpa-IPV)²⁰20 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated).²¹21 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated). (D).

All of the vaccines have aluminum phosphate adjuvant and 2-phenoxyethanol and polysorbate 80 excipients. The vaccines may contain traces of neomycin, streptomycin, polymyxin B, glutaraldehyde and formaldehyde¹⁹19 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular). Booster..,²⁰20 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated),²¹21 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated). (D). They are presented in the form of a suspension, in single dose syringes of 0.5 mL, ready to use¹⁹19 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular). Booster..,²⁰20 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated),²¹21 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated). (D).

It is recommended for booster vaccination against diphtheria, tetanus and whooping cough¹⁹19 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular). Booster..,²⁰20 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated),²¹21 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated). (D), as between the decades of 1970 and 1980 there were resurgences of whooping cough in various parts of the world²⁴24 Quinn HE, McIntyre PB. The impact of adolescent pertussis immunization, 2004-2009: lessons from Australia. Bull World Health Organ 2011;89:666-74. (B), resulting from the low presence of antibodies for these diseases in individuals over 40 years, even in patients that completed the full basic vaccination scheme²⁵25 Grimprel E, von Sonnenburg F, Sänger R, Abitbol V, Wolter JM, Schuerman LM, et al. Combined reduced-antigen content diphtheria-tetanus-acellular pertussis and polio vaccine (dTpa-IPV) for booster vaccination of adults. Vaccine 2005;23:3657-67. (B). Brazil, like the whole of Latin America, has maintained the certificate granted by the WHO for eradication of the poliomyelitis virus¹1 Brazilian Ministry of Health. Vaccination calendar for adults and the elederly. Available at: http://portal.saude.gov.br/portal/saude/visualizar_texto.cfm? Idtxt=21464. Access on: 11/5/2011..⁶6 www.who.int/in Acesso em: 12/16/11. (D).

Administration should be intramuscular, preferably in the deltoid muscle, and may be applied from the age of 11 years, that is, the vaccine may be given to adolescents, adults and the elderly¹⁹19 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular). Booster..,²⁰20 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated),²¹21 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated).,²²22 Brazilian Association of Immunization. Vaccination calendar for adults and the elederly, 2011. Available at: http://www. sbim. org.br/sbim_ calendarios_2011_adulto.pdf. Access on: 11/5/2011. (D).

The recommended vaccination schedule depends on three situations of the vaccine status.

1º If the basic vaccination scheme is complete - substitute the booster dose of dT with dTpa or dTpa-IPV. If the individual has already received the booster dose with adult diphtheria or tetanus or adult double bacteria (dT), there is no need for an interval of the dose with dTpa or dTpa-IPV as a booster for the diseases not covered in the dT²⁶26 Centers for Disease Control and Prevention (CDC). Updated recommendations for use of tetanus toxoid, reduced diphtheria toxoid and acellular pertussis (Tdap) vaccine from the Advisory Committee on Immunization Practices, 2010. MMWR 2011;60:13-15. (D);

2º If the basic vaccination scheme is incomplete (one or two doses of the tetanic component received over the lifespan) – complete the scheme of 3 doses by applying:

3º If the vaccination scheme has not been carried out or is unknown - proceed with vaccination at an interval of 0, 2, and 6 months. With the first dose of dTpa or dTpa-IPV and subsequent doses with dT²²22 Brazilian Association of Immunization. Vaccination calendar for adults and the elederly, 2011. Available at: http://www. sbim. org.br/sbim_ calendarios_2011_adulto.pdf. Access on: 11/5/2011. (D).

In special situations, the interval between the 1st and 2nd doses may be reduced to 1 month, between the 2nd and 3rd doses, maintain the interval of 6 to 12 months²⁷27 Centers for Disease Control and Prevention (CDC). Recommended adult immunization schedule – United States, 2011. MMWR Morb Mortal Wkly Rep 2011;60:1-4. (D).

The vaccination against whooping cough is especially recommended in adults that live with or care for infants aged less than one year, given they are the main transmitters of Bordetella pertussis to this group²²22 Brazilian Association of Immunization. Vaccination calendar for adults and the elederly, 2011. Available at: http://www. sbim. org.br/sbim_ calendarios_2011_adulto.pdf. Access on: 11/5/2011. (D). Health professionals, especially those operating in newborn, pediatric, geriatric and oncology units should also be vaccinated²⁷27 Centers for Disease Control and Prevention (CDC). Recommended adult immunization schedule – United States, 2011. MMWR Morb Mortal Wkly Rep 2011;60:1-4. (D).

Only in september of 2011, the use of the anti-pertussis vaccine in patients aged over 65 years was cleared by the U.S. Food and Drug Administration (FDA)²⁷27 Centers for Disease Control and Prevention (CDC). Recommended adult immunization schedule – United States, 2011. MMWR Morb Mortal Wkly Rep 2011;60:1-4. (D), as well as for patients with special clinical conditions such as chronic pneumopathy, heart disease, diabetes, HIV or other immunodeficiency conditions, chronic liver diseases, chronic alcoholism, asplenia and kidney failure. It is known that the morbidity of the disease is higher in these groups²⁶26 Centers for Disease Control and Prevention (CDC). Updated recommendations for use of tetanus toxoid, reduced diphtheria toxoid and acellular pertussis (Tdap) vaccine from the Advisory Committee on Immunization Practices, 2010. MMWR 2011;60:13-15.,²⁷27 Centers for Disease Control and Prevention (CDC). Recommended adult immunization schedule – United States, 2011. MMWR Morb Mortal Wkly Rep 2011;60:1-4.,²⁸28 Centers for Disease Control and Prevention (CDC). FDA approval of expanded age indication for a tetanus toxoid reduced diphitheria and acellular pertussis vaccine. MMWR Morb Mortal Wkly Rep 2011;60:1279-80. (D). Reinforcement with dTpa or dTpa-IPV induces a better immunological response in adults between 55 and 64 years of age than those aged over 65, with a larger population and greater follow-up time necessary to evaluate the results in the latter population²⁹29 Van Damme P, McIntyre P, Grimprel E, Kuriyakose S, Jacquet JM, Hardt K, et al. Immunogenicity of the reducedantigen-content dTpa vaccine (Boostrix(®) in adults 55 years of age and over: a sub-analysis of four trials. Vaccine 2011;29:5932-9. (B).

Some studies are evaluating the safety and importance of vaccination in pregnant women. The Brazilian Immunization Association (SBIm) and the Advisory Committee on Immunization Practices in the USA (ACIP) suggest for the vaccine to be given after the 20th week of pregnancy, or post-partum, if the mother has not been vaccinated previously, while there is no clearance on the vaccines for this specific group³⁰30 Centers for Disease Control and Prevention (CDC). Updated recommendations for use of tetanus toxoid, reduced diphtheria toxoid and acellular pertussis vaccine (Tdap) in pregnant women and persons who have or anticipate having close contact with an infant aged <12 months. Advisory Committee on Immunization Practices (ACIP), 2011.MMWR Morb Mortal Wkly Rep 2011;60:1424-6..³¹31 Brazilian Association of Immunization. Vaccination calendar for Women, 2011. Available at: http://www.sbim.org.br/sbim_ calendarios_ 2011_mulher.pdf. Access on: 11/5/2011. (D).

The vaccines are effective and immunogenic, and various studies have shown satisfactory antibody production response at the booster dose. This data may be correlated with an effective clinical protection response against whooping cough³²32 Halperin SA, Smith B, Russel M, Scheifele D, Mills E, Hasselbach P, et al. Adult formulation of a five component acellular pertussis vaccine combined with diphtheria and tetanus toxoids and inactivated poliovirus vaccine is safe and immunogenic in adolescents and adults. Pediatr Infect Dis J 2000;19:276-83. (A) ²⁵25 Grimprel E, von Sonnenburg F, Sänger R, Abitbol V, Wolter JM, Schuerman LM, et al. Combined reduced-antigen content diphtheria-tetanus-acellular pertussis and polio vaccine (dTpa-IPV) for booster vaccination of adults. Vaccine 2005;23:3657-67. (B).

In 2004, after some provinces in Canada introduced dTpa with a fifth component (Haemophilus influenzae type B) in adolescents between 14 and 16 years, an important reduction of 84% was observed in the disease in this age range, as well as groups with a lower age range, due to the probable effect of herd immunity³³33 Greemberg DP, Doemland M, Bettinger JA, Scheifele DW, Halperin SA; IMPACT Investigators, et al. Epidemiology of pertussis and Haemophilus influenza type B disease in Canada with exclusive use of a diphtheria-tetanus-acellular pertussis-inactivated poliovirus-Haemophilus influenzae type B pediatric combination vaccine and an adolescent-adult tetanusdiphtheria-acellular pertussis vaccine: implications for disease prevention in the United States. Pediatr Infect Dis J 2009;28:521-8. (B).

In the same year, Australia introduced a booster with dTpa for adolescents between 15 and 17 years. However, owing to the elevated incidence of the disease in adolescents, some states such as New South Wales expanded the age range of the immunization program to 12 to 17 years and noted an effectiveness of 78% (CI 95% 60.7-87.6)³³33 Greemberg DP, Doemland M, Bettinger JA, Scheifele DW, Halperin SA; IMPACT Investigators, et al. Epidemiology of pertussis and Haemophilus influenza type B disease in Canada with exclusive use of a diphtheria-tetanus-acellular pertussis-inactivated poliovirus-Haemophilus influenzae type B pediatric combination vaccine and an adolescent-adult tetanusdiphtheria-acellular pertussis vaccine: implications for disease prevention in the United States. Pediatr Infect Dis J 2009;28:521-8. (B), that is, the disease was reduced from 124 to 40.4/100,000³⁴34 Rank C, Quinn HE, McIntyre PB. Pertussis vaccine effectiveness after mass immunization of high school students in Australia. Pediatr Infect Dis J 2009;28:152-3. (B). It was therefore shown that the booster dose could be used as an effective tool to control the disease³²32 Halperin SA, Smith B, Russel M, Scheifele D, Mills E, Hasselbach P, et al. Adult formulation of a five component acellular pertussis vaccine combined with diphtheria and tetanus toxoids and inactivated poliovirus vaccine is safe and immunogenic in adolescents and adults. Pediatr Infect Dis J 2000;19:276-83. (A) ³⁴34 Rank C, Quinn HE, McIntyre PB. Pertussis vaccine effectiveness after mass immunization of high school students in Australia. Pediatr Infect Dis J 2009;28:152-3.,³³33 Greemberg DP, Doemland M, Bettinger JA, Scheifele DW, Halperin SA; IMPACT Investigators, et al. Epidemiology of pertussis and Haemophilus influenza type B disease in Canada with exclusive use of a diphtheria-tetanus-acellular pertussis-inactivated poliovirus-Haemophilus influenzae type B pediatric combination vaccine and an adolescent-adult tetanusdiphtheria-acellular pertussis vaccine: implications for disease prevention in the United States. Pediatr Infect Dis J 2009;28:521-8.,³⁵35 Viney KA, McAnulty JM, Campbell-Lloyd S. Pertussis in New South Wales, 1993-2005: the impact of vaccination policy on pertussis epidemiology. N S W Public Health Bulletin 2007;06:55-61. (B).

In relation to the adverse effects of anti-pertussis vaccines for adults, there is a very similar safety profile to that observed in the dT vaccine, which is widely used in the national immunization program2(D). The most common adverse effects are local reactions such as pain (61 to 69.2%), edema (17.6 to 25.6%) and erythema (21.1 to 27.1%)³⁵35 Viney KA, McAnulty JM, Campbell-Lloyd S. Pertussis in New South Wales, 1993-2005: the impact of vaccination policy on pertussis epidemiology. N S W Public Health Bulletin 2007;06:55-61. (B). Systemic adverse effects may occur, such as headache (30 to 31%), body temperature above 37.5ºC (5.5 to 8%), fatigue (28.1 to 28.9%), and gastrointestinal symptoms (15.9 to 17.5%)³⁶36 Blatter M, Friedland LR, Weston WM, Li P, Howe B. Immunogenicity and safety os a tetanus toxoid, reduced diphteria toxoid and three-component acellular pertussis vaccine in adults 19-64 years of age. Vaccine 2009;27:765-72. (B).

The vaccines are contraindicated in cases of allergies of an anaphylactic nature to previous vaccinations or to any of the components of the vaccine³⁷37 Bricks LF. Coqueluche. In: Neto VA, ed. Atualizações, orientações e sugestões sobre Imunizações. 1ª ed. São Paulo: Segmento Farma; 2011. p.167-75. (D). People with previous cases of encephalopathy without an identifiable cause in a 7-day period after the previous dose of vaccines containing pertussis components should only receive dT³⁷37 Bricks LF. Coqueluche. In: Neto VA, ed. Atualizações, orientações e sugestões sobre Imunizações. 1ª ed. São Paulo: Segmento Farma; 2011. p.167-75. (D).

Recommendation

The anti-pertussis vaccines available in Brazil are acellular and present components against diphtheria, tetanus and whooping cough (dTpa)¹⁹19 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular). Booster.. (D) or components against diphtheria, tetanus, whooping cough and inactivated polio (dTpa-IPV)²⁰20 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated).²¹21 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated). (D). The booster vaccine depends on the situation of the basic vaccine status in childhood²²22 Brazilian Association of Immunization. Vaccination calendar for adults and the elederly, 2011. Available at: http://www. sbim. org.br/sbim_ calendarios_2011_adulto.pdf. Access on: 11/5/2011..²⁷27 Centers for Disease Control and Prevention (CDC). Recommended adult immunization schedule – United States, 2011. MMWR Morb Mortal Wkly Rep 2011;60:1-4. (D) and is recommended because the antibodies of these diseases are low in individuals over 40 years²⁴24 Quinn HE, McIntyre PB. The impact of adolescent pertussis immunization, 2004-2009: lessons from Australia. Bull World Health Organ 2011;89:666-74. (B). Adults that live or work with infants less than one year old should receive a single booster²³23 Carvalho AP, Pereira EM. Acellular pertussis vaccine for adolescents. J Pediatr 2006;82(3 Suppl):515-24. (B) ²²22 Brazilian Association of Immunization. Vaccination calendar for adults and the elederly, 2011. Available at: http://www. sbim. org.br/sbim_ calendarios_2011_adulto.pdf. Access on: 11/5/2011..²⁷27 Centers for Disease Control and Prevention (CDC). Recommended adult immunization schedule – United States, 2011. MMWR Morb Mortal Wkly Rep 2011;60:1-4. (D). This therapeutic resource was only cleared for the elderly with chronic diseases in 2011²⁶26 Centers for Disease Control and Prevention (CDC). Updated recommendations for use of tetanus toxoid, reduced diphtheria toxoid and acellular pertussis (Tdap) vaccine from the Advisory Committee on Immunization Practices, 2010. MMWR 2011;60:13-15..²⁸28 Centers for Disease Control and Prevention (CDC). FDA approval of expanded age indication for a tetanus toxoid reduced diphitheria and acellular pertussis vaccine. MMWR Morb Mortal Wkly Rep 2011;60:1279-80. (D), and preliminary results demonstrate better immunological response for adults between 55 and 64 years²⁹29 Van Damme P, McIntyre P, Grimprel E, Kuriyakose S, Jacquet JM, Hardt K, et al. Immunogenicity of the reducedantigen-content dTpa vaccine (Boostrix(®) in adults 55 years of age and over: a sub-analysis of four trials. Vaccine 2011;29:5932-9. (B). It should be remembered that Brazil has maintained the eradication of the poliomyelitis disease for years1.6(D) and, as the effective clinical protection of anti-pertussis vaccines is against whooping cough³²32 Halperin SA, Smith B, Russel M, Scheifele D, Mills E, Hasselbach P, et al. Adult formulation of a five component acellular pertussis vaccine combined with diphtheria and tetanus toxoids and inactivated poliovirus vaccine is safe and immunogenic in adolescents and adults. Pediatr Infect Dis J 2000;19:276-83. (A) ²⁵25 Grimprel E, von Sonnenburg F, Sänger R, Abitbol V, Wolter JM, Schuerman LM, et al. Combined reduced-antigen content diphtheria-tetanus-acellular pertussis and polio vaccine (dTpa-IPV) for booster vaccination of adults. Vaccine 2005;23:3657-67. (B), it is recommended to use dTpa¹⁹19 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular). Booster.. (D), as there would be no greater benefit in using the combined vaccine with inactivated poliomyelitis (dTpa-IPV)²⁰20 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated).²¹21 Package insert for adsorbed vaccine against diphtheria, tetanus, pertussis (acellular) and Polio I, II and III (inactivated). (D). They are contraindicated in the case of previous anaphylactic allergic reaction to the vaccination or any component of the vaccine37(D).

Is there a benefit to the use of BCG vaccines?

The BCG (Bacille de Calmette et Guérin) vaccine originates from attenuated and avirulent strains of Mycobacterium bovis, which through immunogenic properties are able to stimulate protection against serious infection and illness caused by Mycobacterium tuberculosis, such as tuberculous meningitis and miliary tuberculosis. It has been used since 1921³⁸38 Barreto ML, Pereira SM, Ferreira AA. BCG vaccine: efficacy and indications for vaccination and revaccination. J Pediatr 2006;82:S45-54. (B).

The existing recommendation is for newborns up to the first month old. The loss of the protective effect of the BCG vaccine over time has led to some countries adopting revaccination³⁹39 Leung CC, Tam CM, Chan SL, Chan-Yeung M, Chan CK, Chang KC. Efficacy of the BCG revaccination programme in a cohort given BCG vaccination at birth in Hong Kong. Int J Tuberc Lung Dis 2001;5:717-23..⁴⁰40 Rahman M, Sekimoto M, Hira K, Koyama H, Imanaka Y, Fukui T. Is Bacillus Calmette-Guerin revaccination necessary for Japanese children? Prev Med 2002;35:70-7. (B). In Brazil, the Ministry of Health has recommended the BCG revaccination of the 6- to 14-year population since 1994. Nevertheless, studies on BCG revaccination (including in Brazil) has not shown protection by the second dose against tuberculosis in revaccinated adolescents³⁸38 Barreto ML, Pereira SM, Ferreira AA. BCG vaccine: efficacy and indications for vaccination and revaccination. J Pediatr 2006;82:S45-54..⁴¹41 Rodrigues LC, Pereira SM, Cunha SS, Genser B, Ichihara MY, Brito SC, et al. Effect of BCG revaccination on incidence of tuberculosis in school-aged children in Brazil: the BCG-REVAC cluster-randomised trial. Lancet 2005;366:1290-5.,⁴²42 Barreto ML, Pereira SM, Pilger D, Cruz AA, Cunha SS, Sant’Anna C, et al. Evidence of an effect of BCG revaccination on incidence of tuberculosis in school-aged children in Brazil: second report of the BCG-REVAC cluster-randomised trial. Vaccine 2011;29:4875-7.,⁴³43 Roth AE, Benn CS, Ravn H, Rodrigues A, Lisse IM, Yazdanbakhsh M, et al. Effect of revaccination with BCG in early childhood on mortality: randomised trial in Guinea-Bissau. BMJ 2010;340:c671.,⁴⁴44 von Reyn CF, Mtei L, Arbeit RD, Waddell R, Cole B, Mackenzie T, et al. Prevention of tuberculosis in Bacille Calmette-Guérin-primed, HIV-infected adults boosted with an inactivated whole-cell mycobacterial vaccine. AIDS 2010;24:675-85. (B) ⁴⁵45 Dantas OM, Ximenes RA, Albuquerque MF, Silva NL, Montarroyos UR, Souza WV, et al. A case-control study of protection against tuberculosis by BCG revaccination in Recife, Brazil. Int J Tuberc Lung Dis 2006;10:536-41. (C).

BCG revaccination has been studies both in populations with persistent protective effects as well as those where the protective effects was lost, with no differences between the groups. The incidence of tuberculosis was 16.5 and 12.9 per 100,000 people/year in vaccinated and revaccinated people respectively, without significant differences, as the reduction of the risk upon revaccination had RR = 1.28 with CI 95% 0.92-1.77³⁹39 Leung CC, Tam CM, Chan SL, Chan-Yeung M, Chan CK, Chang KC. Efficacy of the BCG revaccination programme in a cohort given BCG vaccination at birth in Hong Kong. Int J Tuberc Lung Dis 2001;5:717-23. (B). In Brazil, the incidence of tuberculosis between those vaccinated according to the usual calendar and those revaccinated is greater without the booster, but maintains the absence of benefit, with 29.3 versus 30.2 per 100,000 people/year, with RR=0.94 and CI 95% 0.76-1.2841(B). It would be necessary to immunize 4963 people to avoid the development of one case of tuberculosis, therefore, there is no adequate cost-benefit relationship⁴⁰40 Rahman M, Sekimoto M, Hira K, Koyama H, Imanaka Y, Fukui T. Is Bacillus Calmette-Guerin revaccination necessary for Japanese children? Prev Med 2002;35:70-7. (B).

Thus, in 2006, the Ministry of Health recommended the suspension of BCG revaccination. It is also not recommended to revaccinate the indigenous population. Therefore, in adults, only those in contact with leprosy should be revaccinated, and, even then, only once1(D). Currently in Brazil, the only recommendation in adults relates to household contact with leprosy patients³⁸38 Barreto ML, Pereira SM, Ferreira AA. BCG vaccine: efficacy and indications for vaccination and revaccination. J Pediatr 2006;82:S45-54. (B).

The possibility of a secondary vaccination of BCG for those with HIV is still being evaluated, with the benefits yet to be proven⁴²42 Barreto ML, Pereira SM, Pilger D, Cruz AA, Cunha SS, Sant’Anna C, et al. Evidence of an effect of BCG revaccination on incidence of tuberculosis in school-aged children in Brazil: second report of the BCG-REVAC cluster-randomised trial. Vaccine 2011;29:4875-7..⁴⁴44 von Reyn CF, Mtei L, Arbeit RD, Waddell R, Cole B, Mackenzie T, et al. Prevention of tuberculosis in Bacille Calmette-Guérin-primed, HIV-infected adults boosted with an inactivated whole-cell mycobacterial vaccine. AIDS 2010;24:675-85. (B).

The dose and frequency of application is two doses of 0.1 mL each, with a 6 month interval between them.

Each 0.1 mL dose of reconstituted intradermic BCG vaccine contains:

The adverse effects of the application of BCG vaccine are rare and generally occur due to incorrect application, such as too deep or using an excessive dose of the immunobiological component. In up to 10% of people vaccinated the formation of an ulcerate lesion occurs, which may take months to heal completely. Other presentations include abscess at the injection site and floating nodes with fistulization, osteitis, osteomyelitis, and generalized infection may possibly occur. Serious allergic reactions (anaphylaxis) are rare.

Recommendations

The BCG is recommended for newborns and infants aged up to one month at two doses of 01. mL, at 6 months intervals.

The BCG vaccine has few adverse effects, generally resulting from incorrect application. Currently in Brazil, the only recommendation for adults relates to household contact with leprosy patients³⁸38 Barreto ML, Pereira SM, Ferreira AA. BCG vaccine: efficacy and indications for vaccination and revaccination. J Pediatr 2006;82:S45-54. (B).

Which pneumococcal vaccines are available in Brazil?

There are currently two types of vaccine employing different technologies. The first type of vaccine is the 23-valent polysaccharide (VPPS-23) vaccine, an unconjugated formulation that has antigens to the walls of 23 serotypes. These are responsible for around 90% of the strains implicated in invasive pneumococcal disease (IPD), and the vaccine was developed primarily for use in adults⁴⁶46 Package insert of the pneumococcal polysaccharide vaccine Pneumovax – Merck http://www.merck.com/product/usa/pi_circulars/p/pneumovax_23/pneumova_pi.pdf (D).

The second type available uses a carrier protein conjugated to the vaccine’s polysaccharide antigens, and is therefore denominated a conjugate vaccine. This combination increases the immunogenic effect and duration of the immunological memory, providing longer lasting protection. Two new formulations conjugated with antigens of 10 (PCV10)⁴⁷47 Package insert of the pneumococcal polysaccharide vaccine Pneumovax – Merck http://www.merck.com/product/usa/pi_circulars/p/pneumovax_23/pneumova_pi.pdf (D) and 13 (PCV13)⁴⁸48 Package insert for conjugate pneumococcal vaccine – Prevenar13 – Pfizer. www.pfizer.com.br/arquivoPDF.aspx?200,pdf (D) serotypes were approved in Brazil for the prevention of IPD in children aged up to two years of age (PCV10) and children aged between two months and six years (PCV13). PCV13 has already been approved for use in adults in the European Community and some countries in Latin America, and was cleared by the FDA in September 2011, and by the ANVISA, in Brazil, in 2013.

The polysaccharide vaccine is widely used in adults and the elderly. It produces a short immune response with low permanence for the production of antibodies, mainly after 65 years of age⁴⁹49 Park S, Nahm MH. Older adults have a low capacity to opsonize pneumococci due to low IgM antibody response to pneumococcal vaccinations. Infect Immun 2011;79:314-20. (B). In some specific populations, revaccination was attempted five years after the first dose, without satisfactory results, as the improvement in the level of antibodies is transitory, with possible hyporesponsiveness⁵⁰50 Jackson LA, Baxter R, Naleway AL, Belongia EA, Baggs J. Patterns of pneumococcal vaccination and revaccination in elderly and non-elderly adults: a Vaccine Safety Datalink study. BMC Infect Dis 2009;09:37.⁵¹51 Crum-Cianflone NF, Huppler Hullsiek K, Roediger M, Ganesan A, Patel S, Landrum ML, et al. A randomized clinical trial comparing revaccination with pneumococcal conjugate vaccine to polysaccharide vaccine among HIV-infected adults. J Infect Dis 2010;202:1114-25. (B). While conjugate vaccines are habitually used in children less than 2 years old, they may also be applied in adults, stimulating the immune response with the production of antibodies with better memory effects.

Recomendation

In Brazil, there are two types of pneumococcal vaccines: the polysaccharide vaccine⁴⁶46 Package insert of the pneumococcal polysaccharide vaccine Pneumovax – Merck http://www.merck.com/product/usa/pi_circulars/p/pneumovax_23/pneumova_pi.pdf (D), and the conjugate vaccines⁴⁷47 Package insert of the pneumococcal polysaccharide vaccine Pneumovax – Merck http://www.merck.com/product/usa/pi_circulars/p/pneumovax_23/pneumova_pi.pdf.⁴⁸48 Package insert for conjugate pneumococcal vaccine – Prevenar13 – Pfizer. www.pfizer.com.br/arquivoPDF.aspx?200,pdf (D).

What is the importance of S. pneumoniae as a cause of serious respiratory disease?

S. pneumoniae or pneumococcus is a Gram positive bacterium, generally encapsulated, that is present in pairs or short chains in the form of a spear. There are approximately 92 immunologically distinct serotypes capable of leading to various diseases. Of these 92 serotypes, 20 are responsible for 75% of invasive infections.

Pneumococcal infection is classified either as carrier state, noninvasive disease (NID) - localized purulent infection, such as sinusitis, otitis media, conjunctivitis and nonbacteremic pneumonia – or Invasive Pneumococcus Disease (IPD) - pneumonia with bacteremia, bacteremia, meningitis, and endocarditis, which also constitute the forms of presentation in adults and the elderly⁵²52 Center for Disease Control and Prevention. Pneumococcal disease. Epidemiology and prevention of vaccine-preventable diseases. The pink book: course textbook. 11a ed. Atkinson W, Wolfe S, Hamborsky J, McIntyre L, editores. Washington: Public Health Foundation; 2009. p.217-30. (B).

S. pneumoniae is the most frequent agent in community-acquired pneumonia (CAP), varying between 35 and 50% of the cases, ahead of H. influenzae, M. pneumoniae, C. pneumoniae, Legionella sp, respiratory viruses and enterobacteria. As in other parts of the world, S. pneumoniae is also the most common agent for CAP in Latin America (35%). The mortality rate for CAP increases progressively from the age of 60 years, reaching levels 10 times higher than for children less than one year old among individuals aged over 80 years⁵³53 Corrêa RA, Lundgren FL, Pereira-Silva JL, Frare e Silva RL, Cardoso AP, Lemos AC, et al. Brazilian guidelines for community-acquired pneumonia in immunocompetent adults - 2009. J Bras Pneumol 2009;35:574-601. (D).

IPD has a high morbidity and high mortality rate. Even with pneumococcus vaccination administered to the elderly, there are cases of pneumonia, sometimes complicated with empyema, bacteremia without a defined focus, meningitis, spontaneous bacterial peritonitis, septic arthritis, endocarditis and osteomyelitis. There is also the possibility of a patient having associations with the aforesaid conditions. Mortality within 30 days is 16% and does not depend on the person being vaccinated or not⁵⁴54 Rueda AM, Serpa JA, Matloobi M, Mushtaq M, Musher DM. The spectrumof invasive pneumococcal disease at an adult tertiary care hospital in the early 21st century. Medicine 2010;89:331-6. (B).

The IPD rate changed significantly after the use of conjugate vaccine 7 (PCV7) in children under 5, falling from 252 cases per 100,000 people/year (1991-1997) to 87 cases per 100,000 people/year ^{(2001-2006) 55}55 Lacapa R, Bliss SJ, Larzelere-Hinton F, Eagle KJ, McGinty DJ, Parkinson AJ, et al. Changing epidemiology of invasive pneumococcal disease among White Mountain Apache persons in the era of the pneumococcal conjugate vaccine. Clin Infect Dis 2008;47:476-84. (B) or 19-29.9 cases per 100,000 people/year (1998-1999) to 11.2-18 cases per 100,000 people/year⁵⁶56 Rosen JB, Thomas AR, Lexau CA, Reingold A, Hadler JL, Harrison LH, et al; CDC Emerging Infections Program Network. Geographic variation in invasive pneumococcal disease following pneumococcal conjugate vaccine introduction in the United States. Clin Infect Dis 2011;53:137-43. (B). However, the same fact did not occur with the use of pneumococcus vaccine (VPPS-23) in adults, remaining at 60 cases per 100,000 people/year in the first period and 78.9 cases per 100,000 people/year in the second period⁵⁵55 Lacapa R, Bliss SJ, Larzelere-Hinton F, Eagle KJ, McGinty DJ, Parkinson AJ, et al. Changing epidemiology of invasive pneumococcal disease among White Mountain Apache persons in the era of the pneumococcal conjugate vaccine. Clin Infect Dis 2008;47:476-84. (B).

The IPD rate in those aged over 65 years is estimated at 23 cases per 100,000 people/year; however, this increases to 460 cases per 100,000 people/year if the elderly present neoplasms as comorbidity⁵⁷57 Ripoll ME, Valenzuela BMT, Vergara FR, Abarca VK, Muñoz MA, Jiménez de la Jara J, et al. 23-valent pneumococcal vaccine. Statement of the Consultive Committee of Immunizations on behalf of the Chilean Infectious Diseases Society: February 2010. Rev Chilena Infectol 2010;27:133-7. (B).

Considering the substantial morbidity and high rate of early mortality from IPD in adults, work evaluating pneumococcus vaccination defines it as cost effective⁵⁸58 Ogilvie I, Khoury AE, Cui Y, Dasbach E, Grabenstein JD, Goetghebeur M. Costeffectiveness of pneumococcal polysaccharide vaccination in adults: a systematic review of conclusions and assumptions. Vaccine 2009;27:4891-904..⁵⁹59 Smith KJ, Zimmerman RK, Lin CJ, Nowalk MP, Ko FS, McEllistrem MC, et al. Alternative strategies for adult pneumococcal polysaccharide vaccination: a cost-effectiveness analysis. Vaccine 2008;26:1420-31. (B).

Recomendation

S. pneumoniae causes disease in the respiratory tract, such as high infections (sinusitis and otitis) and pneumonia. It can also lead to meningitis, bacteremia and sepsis. Its capacity for invasiveness produces IPD, which has high morbidity and mortality⁵⁴54 Rueda AM, Serpa JA, Matloobi M, Mushtaq M, Musher DM. The spectrumof invasive pneumococcal disease at an adult tertiary care hospital in the early 21st century. Medicine 2010;89:331-6..⁵⁸58 Ogilvie I, Khoury AE, Cui Y, Dasbach E, Grabenstein JD, Goetghebeur M. Costeffectiveness of pneumococcal polysaccharide vaccination in adults: a systematic review of conclusions and assumptions. Vaccine 2009;27:4891-904.,⁵⁹59 Smith KJ, Zimmerman RK, Lin CJ, Nowalk MP, Ko FS, McEllistrem MC, et al. Alternative strategies for adult pneumococcal polysaccharide vaccination: a cost-effectiveness analysis. Vaccine 2008;26:1420-31. (B).

What are the recommendations for the pneumococcus vaccine?

The current recommendation for pneumococcus vaccination by the CDC includes⁶⁰60 World Health Organization. 23-valent pneumococcal polysaccharide vaccine. WHO position paper. Wkly Epidemiol Rec 2008;83:373-84..⁶¹61 Centers for Disease Control and Prevention (CDC); Advisory Committee on Immunization Practices. Updated recommendations for prevention of invasive pneumococcal disease among adults using the 23-valent pneumococcal polysaccharide vaccine (PPSV23). MMWR Morb Mortal Wkly Rep 2010;59:1102-6. (D):

• all adults aged 65 years or older;

• any person aged from 2 to 64 years with a chronic diseases, such as cardiac or pulmonary diseases, sickle cell anemia, diabetes, alcoholism, cirrhosis of the liver, cerebrospinal fistula, or cochlear implants;

• any person between 2 and 64 years of age with immunosuppression conditions such as Hodgkin’s disease, lymphoma or leukemia, kidney failure, multiple myeloma, nephrotic syndrome, HIV infection or AIDS, asplenia or splenic disease and organ transplant;

• any person between 2 and 64 years of age that uses immunosuppressant drugs, such as long term corticosteroid, drugs used in the treatment of cancer, and radiotherapy;

• adults between 19 and 64 years that are smokers or have asthma;

• long-term residents of nursing homes and institutions.

In April, 2013, a new indication of the 13 valent conjugate vaccine was released in Brazil for healthy adults over 50 years. In Brazil, as well as in other locations in the world, vaccine coverage against pneumococcus is still not widely used in clinical practice⁶²62 Martins WA, Ribeiro MD, Oliveira LB, Barros LS, Jorge AC, Santos CM, et al. Influenza and pneumococcal vaccination in heart failure: a little applied recommendation. Arq Bras Cardiol 2011;96:240-5.,⁶³63 Bratzler DW, Houck PM, Jiang H, Nsa W, Shook C, Moore L, et al. Failure to vaccinate Medicare inpatients: a missed opportunity. Arch Intern Med 2002;162:2349-56.,⁶⁴64 Jones LG, Zhang Y, Ahmed MI, Ekundayo OJ, Akhter S, Sawyer P, et al. Understanding the reasons for the underuse of pneumococcal vaccination by community-dwelling older African Americans. J Am Geriatr Soc 2010;58:2323-8., ⁶⁵65 Jacups SP, Cheng A. The epidemiology of community acquired bacteremic pneumonia, due to Streptococcus pneumoniae, in the top end of the northern territory, Australia: over 22 years. Vaccine 2011;29:5386-92.,⁶⁶66 Martinelli D, Tafuri S, Caputi G, Fortunato F, Reggio P, Germinario C, et al. Eight years of active proposal of pneumococcal 23-valent polysaccharide vaccine: survey on coverage rate among elderly and chronic patients. Am J Infect Control 2010;38:e8-e15.,⁶⁷67 Lu PJ, Nuorti JP. Pneumococcal polysaccharide vaccination among adults aged 65 years and older, U.S., 1989-2008. Am J Prev Med 2010;39:287-95. (B).

The use of electronic reminders for all patients over 65 years could increase the prescription of the pneumococcus vaccine from 13.1 to 19.5%⁶⁸68 Loo TS, Davis RB, Lipsitz LA, Irish J, Bates CK, Agarwal K, et al. Electronic medical record reminders and panel management to improve primary care of elderly patients. Arch Intern Med 2011;171:1552-8. (B). Another way of increasing the prescription of the vaccine is not to miss the opportunity to vaccinate patients hospitalized for chronic diseases⁶³63 Bratzler DW, Houck PM, Jiang H, Nsa W, Shook C, Moore L, et al. Failure to vaccinate Medicare inpatients: a missed opportunity. Arch Intern Med 2002;162:2349-56. (B).

Recomendation

Pneumococcus vaccines are recommended for the prevention of pneumococcal diseases, especially IPD, in specific groups of adults⁶⁰60 World Health Organization. 23-valent pneumococcal polysaccharide vaccine. WHO position paper. Wkly Epidemiol Rec 2008;83:373-84..⁶¹61 Centers for Disease Control and Prevention (CDC); Advisory Committee on Immunization Practices. Updated recommendations for prevention of invasive pneumococcal disease among adults using the 23-valent pneumococcal polysaccharide vaccine (PPSV23). MMWR Morb Mortal Wkly Rep 2010;59:1102-6. (D). Programs are required to clarify the importance of the uses of these therapeutic resources to increase the coverage of the vaccine in the population⁶³63 Bratzler DW, Houck PM, Jiang H, Nsa W, Shook C, Moore L, et al. Failure to vaccinate Medicare inpatients: a missed opportunity. Arch Intern Med 2002;162:2349-56..⁶⁸68 Loo TS, Davis RB, Lipsitz LA, Irish J, Bates CK, Agarwal K, et al. Electronic medical record reminders and panel management to improve primary care of elderly patients. Arch Intern Med 2011;171:1552-8. (B).

Are there differences between polysaccharide and conjugate pneumococcus vaccines?

The 23-valent polysaccharide vaccine (VPPS-23) presents low immunogenicity in children less than two years old, and does not induce immunological memory as a result of not sensitizing the T cell (T-cell independent activation)⁶⁹69 O’Brien KL, Hochman M, Goldblatt D. Combined schedules of pneumococcal conjugate and polysaccharide vaccines: is hyporesponsiveness an issue? Lancet Infect Dis 2007;7:597-606. (D). Conjugate vaccines include polysaccharides conjugated to a carrier protein and therefore have greater immunogenic effect, longer immunological memory and provide longer lasting protection. However, having used a polysaccharide vaccine previously reduces the benefits achieved with the conjugate vaccine⁷⁰70 Lazarus R, Clutterbuck E, Yu LM, Bowman J, Bateman EA, Diggle L, et al. A randomized study comparing combined pneumococcal conjugate and polysaccharide vaccination schedules in adults. Clin Infect Dis 2011;52:736-42. (B). For example, as of 2000, the use of the PCV7 vaccine in children less than nine years old resulted in a significant reduction of IPD among vaccinated (direct effect) and unvaccinated individuals of all ages, particularly patients aged over 65 years (herd effect). Two new formulations conjugated with antigens for 10 (PCV10) and 13 (PCV13) serotypes were recently approved in the USA and Brazil for the prevention of IPD in children aged up to two years (PCV10) and children between two months and six years old (PCV13)⁶⁹69 O’Brien KL, Hochman M, Goldblatt D. Combined schedules of pneumococcal conjugate and polysaccharide vaccines: is hyporesponsiveness an issue? Lancet Infect Dis 2007;7:597-606. (D). The PCV13 was also approved for adults over 50 years.

The general effectiveness of VPPS-23 is 74% (CI 95%, 56%-85%), according to randomized studies, and 52% (CI 95%, 39%-63%), according to observational studies⁷¹71 Jackson LA, Janoff EN. Pneumococcal vaccination of elderly adults: new paradigms for protection. Clin Infect Dis 2008;47:1328-38. (D). However, its effectiveness in elderly individuals is inferior to that observed in healthy adults⁷²72 Pilishvili T, Lexau C, Farley MM, Hadler J, Harrison LH, Bennett NM, et al. Sustained reductions in invasive pneumococcal disease in the era of conjugate vaccine. J Infect Dis 2010;201:32-41. (B). Also, it enables a significant reduction in IPD (OR=0.26; CI 95% 0.15-0.46)⁷³73 Moberley SA, Holden J, Tatham DP, Andrews RM. Vaccines for preventing pneumococcal infection in adults. Cochrane Database Syst Rev 2008;(1):CD000422. (A).

The effectiveness against all-cause pneumonia has not yet been demonstrated⁷³73 Moberley SA, Holden J, Tatham DP, Andrews RM. Vaccines for preventing pneumococcal infection in adults. Cochrane Database Syst Rev 2008;(1):CD000422. (A) ⁷⁴74 Huss A, Scott P, Stuck AE, Trotter C, Egger M. Efficacy of pneumococcal vaccination in adults: a meta-analysis. CMAJ 2009;180:48-58. (B) and the use of VPPS-23 has not been associated with a lower mortality rate in the vaccinated group (OR=0.87 with CI 95% 0.69-1.10)⁷³73 Moberley SA, Holden J, Tatham DP, Andrews RM. Vaccines for preventing pneumococcal infection in adults. Cochrane Database Syst Rev 2008;(1):CD000422. (A). The duration of the immune response to VPPS-23 declines with time and age (over 65 years), with the levels of antibodies reaching pre-vaccination levels after 4 to 7 years⁵⁰50 Jackson LA, Baxter R, Naleway AL, Belongia EA, Baggs J. Patterns of pneumococcal vaccination and revaccination in elderly and non-elderly adults: a Vaccine Safety Datalink study. BMC Infect Dis 2009;09:37.⁵¹51 Crum-Cianflone NF, Huppler Hullsiek K, Roediger M, Ganesan A, Patel S, Landrum ML, et al. A randomized clinical trial comparing revaccination with pneumococcal conjugate vaccine to polysaccharide vaccine among HIV-infected adults. J Infect Dis 2010;202:1114-25. (B). The benefit of revaccination was demonstrated in adults under 65 years, with tolerance or hyporesponsiveness possibly occurring⁵⁰50 Jackson LA, Baxter R, Naleway AL, Belongia EA, Baggs J. Patterns of pneumococcal vaccination and revaccination in elderly and non-elderly adults: a Vaccine Safety Datalink study. BMC Infect Dis 2009;09:37.⁵¹51 Crum-Cianflone NF, Huppler Hullsiek K, Roediger M, Ganesan A, Patel S, Landrum ML, et al. A randomized clinical trial comparing revaccination with pneumococcal conjugate vaccine to polysaccharide vaccine among HIV-infected adults. J Infect Dis 2010;202:1114-25.,⁷⁵75 Törling J, Hedlund J, Konradsen HB, Ortqvist A. Revaccination with the 23-valent pneumococcal polysaccharide vaccine in middle-aged and elderly persons previously treated for pneumonia. Vaccine 2003;22:96-103. (B).

We still need robust trials that define the benefits of new conjugate vaccines for adults and the elderly⁷¹71 Jackson LA, Janoff EN. Pneumococcal vaccination of elderly adults: new paradigms for protection. Clin Infect Dis 2008;47:1328-38.,⁷²72 Pilishvili T, Lexau C, Farley MM, Hadler J, Harrison LH, Bennett NM, et al. Sustained reductions in invasive pneumococcal disease in the era of conjugate vaccine. J Infect Dis 2010;201:32-41.,⁷³73 Moberley SA, Holden J, Tatham DP, Andrews RM. Vaccines for preventing pneumococcal infection in adults. Cochrane Database Syst Rev 2008;(1):CD000422.,⁷⁴74 Huss A, Scott P, Stuck AE, Trotter C, Egger M. Efficacy of pneumococcal vaccination in adults: a meta-analysis. CMAJ 2009;180:48-58.,⁷⁵75 Törling J, Hedlund J, Konradsen HB, Ortqvist A. Revaccination with the 23-valent pneumococcal polysaccharide vaccine in middle-aged and elderly persons previously treated for pneumonia. Vaccine 2003;22:96-103.,⁷⁶76 Musher DM, Sampath R, Rodriguez-Barradas MC. The potential role for protein-conjugate pneumococcal vaccine in adults: what is the supporting evidence? Clin Infect Dis 2011;52:633-40. (D).

Pneumococcal vaccination in adults is safe, with few reports of adverse events associated with the injection (transitory pain and redness) and light systemic symptoms such as fever and myalgia, which persist for less than 48 hours. It is not recommended for pregnant women⁵⁷57 Ripoll ME, Valenzuela BMT, Vergara FR, Abarca VK, Muñoz MA, Jiménez de la Jara J, et al. 23-valent pneumococcal vaccine. Statement of the Consultive Committee of Immunizations on behalf of the Chilean Infectious Diseases Society: February 2010. Rev Chilena Infectol 2010;27:133-7. (B).

Recomendation

There are differences between polysaccharide and conjugate pneumococcus vaccines. Conjugate vaccines produce a longer lasting and more intense immunological response than non conjugate vaccines⁷⁰70 Lazarus R, Clutterbuck E, Yu LM, Bowman J, Bateman EA, Diggle L, et al. A randomized study comparing combined pneumococcal conjugate and polysaccharide vaccination schedules in adults. Clin Infect Dis 2011;52:736-42. (B). VPPS-23 significantly reduces IPD, but up to now, it has not demonstrated a reduction in the amount of pneumonia or mortality⁷³73 Moberley SA, Holden J, Tatham DP, Andrews RM. Vaccines for preventing pneumococcal infection in adults. Cochrane Database Syst Rev 2008;(1):CD000422. (A) ⁷⁴74 Huss A, Scott P, Stuck AE, Trotter C, Egger M. Efficacy of pneumococcal vaccination in adults: a meta-analysis. CMAJ 2009;180:48-58. (B), with less benefits for patients over 65 years old⁷¹71 Jackson LA, Janoff EN. Pneumococcal vaccination of elderly adults: new paradigms for protection. Clin Infect Dis 2008;47:1328-38..⁷⁶76 Musher DM, Sampath R, Rodriguez-Barradas MC. The potential role for protein-conjugate pneumococcal vaccine in adults: what is the supporting evidence? Clin Infect Dis 2011;52:633-40. (D). There is no benefit in revaccinating adults less than 65 years old, as this may cause tolerance or hyporesponsiveness. There is also discussion about the recommendation fro patients with reduced immunity⁵⁰50 Jackson LA, Baxter R, Naleway AL, Belongia EA, Baggs J. Patterns of pneumococcal vaccination and revaccination in elderly and non-elderly adults: a Vaccine Safety Datalink study. BMC Infect Dis 2009;09:37.⁵¹51 Crum-Cianflone NF, Huppler Hullsiek K, Roediger M, Ganesan A, Patel S, Landrum ML, et al. A randomized clinical trial comparing revaccination with pneumococcal conjugate vaccine to polysaccharide vaccine among HIV-infected adults. J Infect Dis 2010;202:1114-25.,⁷⁴74 Huss A, Scott P, Stuck AE, Trotter C, Egger M. Efficacy of pneumococcal vaccination in adults: a meta-analysis. CMAJ 2009;180:48-58. (B). Pneumococcus vaccination in adults is safe, with few reports of adverse events, but is not recommended for pregnant women⁵⁷57 Ripoll ME, Valenzuela BMT, Vergara FR, Abarca VK, Muñoz MA, Jiménez de la Jara J, et al. 23-valent pneumococcal vaccine. Statement of the Consultive Committee of Immunizations on behalf of the Chilean Infectious Diseases Society: February 2010. Rev Chilena Infectol 2010;27:133-7. (B).

What is the dose and application method of the pneumococcus vaccine?

The polysaccharide vaccine should be applied in a single dose of 0.5 mL intramuscularly or subcutaneously⁴⁶46 Package insert of the pneumococcal polysaccharide vaccine Pneumovax – Merck http://www.merck.com/product/usa/pi_circulars/p/pneumovax_23/pneumova_pi.pdf (D). A booster after five years is suggested in patients with reduced immunity, but there is discussion about this recommendation, as studies show a lower antigenic effect after use of the booster dose. The conjugate vaccine PCV13 for adults should be applied in a single dose of 0.5 mL, intramuscularly⁴⁸48 Package insert for conjugate pneumococcal vaccine – Prevenar13 – Pfizer. www.pfizer.com.br/arquivoPDF.aspx?200,pdf (D).

Is there a benefit to combined vaccinations for the prevention of infectious respiratory diseases in adults?

Studies on the combine used of flu and pneumococcus vaccines in patients with chronic diseases are common.

Flu and pneumococcus vaccinations are recommended in the Brazilian and global guidelines for heart failure⁷⁷77 Bocchi EA, Marcondes-Braga FG, Ayub-Ferreira SM, Rohde LE, Oliveira WA, Almeida DR, et al. Sociedade Brasileira de Cardiologia. III Diretriz brasileira de insuficiência cardíaca crônica. Arq Bras Cardiol 2009;92 (6 supl 1):1-71.,⁷⁸78 Jessup M, Abraham WT, Casey DE, Feldman AM, Francis GS, Ganiats TG, et al. 2009 Focused Update: ACCF/AHA guidelines for the diagnosis and management of heart failure in adults. Circulation 2009;119:1977-2016.,⁷⁹79 Dickstein K , Cohen-Solal A, Filippatos G, McMurray JJ, Ponikowski P, Poole-Wilson PA, et al. ESC guidelines for the diagnosis and treatment of acute and chronic heart failure 2008. Eur Heart J 2008;29:2388-442. (D), as respiratory infections are the third main cause of hospitalization for decompensated heart failure⁷⁷77 Bocchi EA, Marcondes-Braga FG, Ayub-Ferreira SM, Rohde LE, Oliveira WA, Almeida DR, et al. Sociedade Brasileira de Cardiologia. III Diretriz brasileira de insuficiência cardíaca crônica. Arq Bras Cardiol 2009;92 (6 supl 1):1-71..⁷⁸78 Jessup M, Abraham WT, Casey DE, Feldman AM, Francis GS, Ganiats TG, et al. 2009 Focused Update: ACCF/AHA guidelines for the diagnosis and management of heart failure in adults. Circulation 2009;119:1977-2016. (D). Also, there is an association between respiratory infections and increased risk of cardiac ischemia⁸⁰80 Smeeth L, Thomas SL, Hall AJ, Hubbard R, Farrington P, Vallance P. Risk of myocardial infarction and stroke after acute infection or vaccination. N Engl J Med 2004;351:2611-8..⁸¹81 Spodick DH, Flessas AP, Johnson MM. Association of acute respiratory symptoms with onset of acute myocardial infarction: prospective investigation of 150 consecutive patients and matched control patients. Am J Cardiol 1984;53:481-2. (B) and strokes⁸²82 Hung IF, Leung AY, Chu DW, Leung D, Cheung T, Chan CK, et al. Prevention of acute myocardialinfarction and stroke among elderly persons by dual pneumococcal and influenza vaccination: a prospective cohort study. Clin Infect Dis 2010;51:1007-16. (B). These two vaccinations reduce respiratory infections, hospitalizations and acute cardiovascular events⁶³63 Bratzler DW, Houck PM, Jiang H, Nsa W, Shook C, Moore L, et al. Failure to vaccinate Medicare inpatients: a missed opportunity. Arch Intern Med 2002;162:2349-56. (B).

In order to assess the benefit of 23 polyvalent pneumococcal vaccine in patients with chronic obstructive pulmonary disease (COPD), the number of exacerbations and pneumonia as well as mortality was assessed. There were no significant differences in the number of exacerbations between those vaccinated and unvaccinated (OR=0.58 with CI 95% 0.30-1.13), as well as the number of events of pneumonia (OR=0.72 with CI 95% 0.51-1.01). The evaluation of mortality for all causes within 48 months of vaccination or mortality due to cardiorespiratory causes had no significant differences, either (OR=0.94 with CI 95% 0.67-1.33 and OR=1.07 with CI 95% 0.69-1.66, respectively)⁸³83 Walters JA, Smith S, Poole P, Granger RH, Wood-Baker R. Injectable vaccines for preventing pneumococcal infection in patients with chronic obstructive pulmonary disease. Cochrane Database Syst Rev 2010;(11):CD001390. (A). The 23 polyvalent pneumococcus vaccine does not change the frequency and severity of infectious exacerbations in patients with bronchiectasis⁸⁴84 Chang CC, Singleton RJ, Morris PS, Chang AB. Pneumococcal vaccines for children and adults with bronchiectasis. Cochrane Database Syst Rev 2009;(2):CD006316. (B). Asthmatic patients present a lower number of specific antibodies after vaccination in relation to non-asthmatics, which keeps them at a high risk of developing IPD, mainly if they depend on corticoids⁸⁵85 Jung JA, Kita H, Dhillon R, Jacobson RM, Nahm MH, Park M, et al. Influence of asthma status on serotype-specific pneumococcal antibody levels. Postgrad Med 2010;122:116-24. (B). Using flu vaccine in patients with COPD does not cause adverse reactions, does not lead to exacerbation, does not worsen pulmonary function and the symptoms of dyspnea, and does not increase the restriction on exercise, regardless of any level of obstruction in the air flow⁸⁶86 Wongsurakiat P, Maranetra KN, Gulprasutdilog P, Aksornint M, Srilum W, Ruengjam C, et al. Adverse effects associated with influenza vaccination in patients with COPD: a randomized controlled study. Respirology 2004;9:550-6. (B). Patients with COPD should receive vaccination against influenza⁸⁷87 Vu T, Farish S, Jenkins M, Kelly H. A meta-analysis of effectiveness of influenza vaccine in persons aged 65 years and over living in the community. Vaccine 2002;20:1831-6.,⁸⁸88 Mullooly JP, Bennett MD, Hornbrook MC, Barker WH, Williams WW, Patriarca PA, et al. Influenza vaccination programs for elderly persons: cost-effectiveness in a health maintenance organization. Ann Intern Med 1994;121:947-52.,⁸⁹89 Schembri S, Morant S, Winter JH, MacDonald TM. Influenza but not pneumococcal vaccination protects against allcause mortality in patients with COPD. Thorax 2009;64:567-72. (B), which reduces mortality in 41% of cases⁸⁹89 Schembri S, Morant S, Winter JH, MacDonald TM. Influenza but not pneumococcal vaccination protects against allcause mortality in patients with COPD. Thorax 2009;64:567-72. (B). There is a benefit to the combined use of flu and pneumococcus vaccines with the reduction of hospitalizations, pneumonia and mortality⁹⁰90 Nichol KL. The additive benefits of influenza and pneumococcal vaccinations during influenza seasons among elderly persons with chronic lung disease. Vaccine 1999;17(Suppl 1):S91-3., ⁹¹91 Nichol KL, Baken L, Wuorenma J, Nelson A. The health and economic benefits associated with pneumococcal vaccination of elderly persons with chronic lung disease. Arch Intern Med 1999;159:2437-42., ⁹²92 Furumoto A, Ohkusa Y, Chen M, Kawakami K, Masaki H, Sueyasu Y, et al. Additive effect of pneumococcal vaccine and influenza vaccine on acute exacerbation in patients with chronic lung disease. Vaccine 2008;26:4284-9. (B), though the reduction in mortality is influenced more by the protection of the flu vaccine⁸⁹89 Schembri S, Morant S, Winter JH, MacDonald TM. Influenza but not pneumococcal vaccination protects against allcause mortality in patients with COPD. Thorax 2009;64:567-72..⁹³93 Dear K, Holden J, Andrews R, Tatham D. Vaccines for preventing pneumococcal infection in adults. Cochrane Database Syst Rev 2003;(4):CD000422. (B).

The use of PCV7 has led to a reduction in the IPD rate in children under 5 with sickle cell anemia, with a reduction in IPD in 93.4% of cases. Before this vaccine (1995 -1999) there were 2044 cases per 100,000 people/year and, after the introduction of the vaccine ^(2001-2004), this number fell to only 134 cases per 100,000 people/year. This benefit was not found for age ranges other than that described, as there were no significant differences in the IPD rate in patients over 5 after use of the conjugate vaccine (161 to 99 cases in 100,000 people/year, with p=0.36)⁹⁴94 Halasa NB, Shankar SM, Talbot TR, Arbogast PG, Mitchel EF, Wang WC, et al. Incidence of invasive pneumococcal disease among individuals with sickle cell disease before and after the introduction of the pneumococcal conjugate vaccine. Clin Infect Dis 2007;44:1428-33. (B).

Patients with asplenia or splenectomy should receive vaccines for Haemophilus influenzae B and pneumococcus vaccine for the increased risk of infection by encapsulated microorganisms, particularly S. pneumoniae, Haemophilus influenzae tipo B and Neisseria meningitidis. Special care is necessary in this population, as vaccine coverage might not reach 50% of applicable cases⁹⁵95 Fuentes-Ferrer ME, Cano-Escudero S, Mato-Chaín G, Mariano-Lázaro A, Fereres-Castiel J. Vaccination coverage against Streptococcus pneumoniae in splenectomized patients in a fourth-level hospital (1999-2004). Enferm Infecc Microbiol Clin 2008;26:194-8. (B). Splenectomized adults with an average age of 29.6 years already vaccinated with 23 polyvalent polysaccharide vaccine had 5% less cases of IPD in the clinical follow-up, without clinical benefits when adding another PCV7 conjugate vaccination, though with an increase in immunogenic response⁹⁶96 Stanford E, Print F, Falconer M, Lamden K, Ghebrehewet S, Phin N, et al. Immune response to pneumococcal conjugate vaccination in asplenic individuals. Hum Vaccin 2009;5:85-91. (B). Patients splenectomized due to hematologic malignancies respond worse to the polysaccharide pneumococcus vaccines compared to those splenectomized due to trauma, and require closer monitoring⁹⁷97 Eigenberger K, Sillaber C, Greitbauer M, Herkner H, Wolf H, Graninger W, et al. Antibody responses to pneumococcal and hemophilus vaccinations in splenectomized patients with hematological malignancies or trauma. Wien Klin Wochenschr 2007;119:228-34. (B).

Given that smoking is associated with an increased risk of respiratory infections, with populations of smokers, former smokers and nonsmokers have been studied to evaluate adherence to the use of flu and pneumococcus vaccines. Former smokers have a 17% greater change of using flu vaccines than nonsmokers (OR=1.17 with CI 95% 1.12-1.22) and a 32% greater chance of using pneumococcus vaccine than nonsmokers (OR=1.32 with CI 95% 1.24-1.41). Current smokers use these therapeutic resources less (OR=0.75 with CI 95% 0.71-0.80), but should be encouraged to receive the prevention of vaccines and stop using tobacco⁹⁸98 Pearson WS, Dube SR, Ford ES, Mokdad AH. Influenza and pneumococcal vaccination rates among smokers: data from the 2006 Behavioral Risk Factor Surveillance System. Prev Med 2009;48:180-3. (B).

The real benefit of using the pneumococcus vaccine in those with acquired immunodeficiency syndrome is no yet known⁹⁹99 Pedersen RH, Lohse N, Østergaard L, Søgaard OS. The effectiveness of pneumococcal polysaccharide vaccination in HIV-infected adults: a systematic review. HIV Med 2011;12:323-33. (B), as the only randomized clinical trial demonstrated that there was no increase in antibodies after vaccination, whether polysaccharide or conjugate¹⁰⁰100 Peñaranda M, Payeras A, Cambra A, Mila J, Riera M; Majorcan Pneumococcal Study Group. Conjugate and polysaccharide pneumococcal vaccines do not improve initial response of the polysaccharide vaccine in HIV-infected adults. AIDS 2010;24:1226-8. (A). Likewise, there is debate regarding the use of the vaccine in alcoholics, as there are reported cases of death from streptococcal sepsis after vaccination¹⁰¹101 McMahon BJ, Parkinson AJ, Rudolph K, Davidson M, Grabman J. Sepsis due to Streptococcus pneumoniae in a patient with alcoholism who received pneumococcal vaccine. Clin Infect Dis 1999;28:1162-3..¹⁰²102 Hanna JN, Wenck DJ, Murphy DN. Three fatal pneumococcal polysaccharide vaccine failures. Med J Aust 2000;173:305-7. (C).

There are no studies in adults using pneumococcus vaccines in those with CFS leak syndrome, only in children¹⁰³103 Shurtleff DB, Loeser JD, Avellino AM, Duguay S, Englund JA, Marcuse EK, et al. Haemophilus influenzae and Streptococcus pneumoniae infections in children with cerebrospinal fluid shunts. Pediatr Neurosurg 2009;45:276-80. (B).

Recomendation

There are benefits in using combined vaccines, as immunization with flu and pneumococcus vaccines reduces hospitalizations, respiratory infections and cardiovascular events in patients with heart disease⁶³63 Bratzler DW, Houck PM, Jiang H, Nsa W, Shook C, Moore L, et al. Failure to vaccinate Medicare inpatients: a missed opportunity. Arch Intern Med 2002;162:2349-56. (B); and hospitalizations, pneumonia and mortality in those with COPD⁹⁰90 Nichol KL. The additive benefits of influenza and pneumococcal vaccinations during influenza seasons among elderly persons with chronic lung disease. Vaccine 1999;17(Suppl 1):S91-3., ⁹¹91 Nichol KL, Baken L, Wuorenma J, Nelson A. The health and economic benefits associated with pneumococcal vaccination of elderly persons with chronic lung disease. Arch Intern Med 1999;159:2437-42., ⁹²92 Furumoto A, Ohkusa Y, Chen M, Kawakami K, Masaki H, Sueyasu Y, et al. Additive effect of pneumococcal vaccine and influenza vaccine on acute exacerbation in patients with chronic lung disease. Vaccine 2008;26:4284-9. (B). The association between vaccines for Haemophius influenzae B and and pneumococcus reduces the cases of IPD by 5% in patients with asplenia or those splenectomized for all reasons⁹⁶96 Stanford E, Print F, Falconer M, Lamden K, Ghebrehewet S, Phin N, et al. Immune response to pneumococcal conjugate vaccination in asplenic individuals. Hum Vaccin 2009;5:85-91. (B), with a worse response for those splenectomized due to hematologic malignancies⁹⁷97 Eigenberger K, Sillaber C, Greitbauer M, Herkner H, Wolf H, Graninger W, et al. Antibody responses to pneumococcal and hemophilus vaccinations in splenectomized patients with hematological malignancies or trauma. Wien Klin Wochenschr 2007;119:228-34. (B). The 93.4% reduction in IPD cases in children less than 5 years old with sickle cell anemia was not confirmed in adult and elderly populations⁹⁴94 Halasa NB, Shankar SM, Talbot TR, Arbogast PG, Mitchel EF, Wang WC, et al. Incidence of invasive pneumococcal disease among individuals with sickle cell disease before and after the introduction of the pneumococcal conjugate vaccine. Clin Infect Dis 2007;44:1428-33. (B).

Conflict of interest

Lundgren F: Received fees for presenting lectures sponsored by Pfizer. He has received medical consultancy fees sponsored by Pfizer.

Chatkin JM: Received reimbursement for appearing at congresses sponsored by the Wyeth and Pfizer. He has received fees for presenting lectures sponsored by the Wyeth and Pfizer.

Corrêa RA: Received reimbursement for appearing at congresses sponsored by Pfizer. He has received fees for the presentation of lectures and

medical consultancy sponsored by Pfizer.

Figueiredo MRF: Received reimbursement for medical consultancy and lectures sponsored by Pfizer

Stirbulov R: Received reimbursement for participating in congresses by GSK, Boehering-Ingelheim and Aché. He has received fees for presentations at symposiums sponsored by Takeda, Pfizer, GSK and Boehering-Ingelheim. He has received fees for medical consultancy sponsored by Boehering-Ingelheim, GSK, Novartis and Aché. He has received fees for clinical research sponsored by Takeda and Novartis.

References

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