Pneumococcal Vaccination in Adults: A Narrative Review of Considerations for Individualized Decision-Making
Abstract
:1. Introduction
2. Methods
3. Risk of Severe Pneumococcal Disease in Adults
4. Pneumococcal Vaccines and Serotype Coverage
- PCV13 serotype coverage: 1, 3, 4, 5, 6A, 6B, 7F, 9V, 14, 18C, 19A, 19F, 23F
- PCV15 serotype coverage: 22F and 33F, in addition to PCV13 serotypes
- PCV21 serotype coverage (not yet commercially available): 3, 6A, 7F, 8, 9N, 10A, 11A, 12F, 15A, 15C, 16F, 17F, 19A, 20, 22F, 23A, 23B, 24F, 31, 33F, 35B. These serotypes contribute to 74–94% of invasive pneumococcal disease in adults aged ≥65 years [27]. Eight of these pathogenic pneumococcal polysaccharides (15A, 15C, 16F, 23A, 23B, 24F, 31, and 35B) are not included in any currently licensed pneumococcal vaccines. Among 508 adults in a Phase 2 study (71% 50–64 years and 29% ≥65 years of age), PCV21 was non-inferior to PPSV23 for 12 shared serotypes and superior to PPSV23 for 9 unique serotypes in PCV21 [27]
- PCV23 serotype coverage (not yet commercially available): 2, 8, 9N, 10A, 11A, 12F, 15B, 17F, 20, 22F, and 33F, in addition to PCV13 serotypes (except for 6A). Serotypes 9N, 17F, and 20 are included in PPSV23 and are absent from PCV20
- PCV24 serotype coverage (not yet commercially available): 1, 3, 4, 5, 6A, 6B, 7F, 9V, 14, 18C, 19A, 19F, 23F (shared PCV13 serotypes) plus 2, 8, 9N, 10A, 11A, 12F, 15B, 17F, 22F, and 33F (shared PPSV23 serotypes) and 20B. This vaccine also incorporates a fusion protein consisting of two highly conserved pneumococcal proteins (sp1500 and sp0785) that may help protect against both vaccine and nonvaccine serotypes [28]
5. Immunogenicity and Clinical Efficacy of Pneumococcal Vaccination
6. Mucosal Immunity and Indirect Effect
7. Coadministration of Pneumococcal Vaccine with Other Vaccines
8. Waning Immunity and Replacement Strains
9. Future Directions
10. Conclusions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
References
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Vaccine [Ref] | Brand Name | Serotype Coverage | Recommended Age Groups | Dosing Schedules |
---|---|---|---|---|
PCV13 [31] | Prevnar 13 (Pfizer, Inc., New York, NY, US) | 1, 3, 4, 5, 6A, 6B, 7F, 9V, 14, 18C, 19A, 19F, 23F | All infants and children 2–59 months of age Children * and adults ** ≥ 60 months of age with underlying medical conditions Adults ≥ 65 years of age | Infants ≥ 6 weeks and children ≤ 15 months: IM 0.5 mL per dose given at 2, 4, 6, and 12 through 15 months of age (for a total of 4 doses) Adults IM 0.5 mL as a single dose |
PCV15 [10,32] | Vaxneuvance (Merck and Co, Inc., Rahway, NJ, US) | 22F and 33F, in addition to PCV13 serotypes | All infants and children 2–59 months of age Children * and adults ** ≥60 months of age with underlying medical conditions Adults ≥65 years of age | Infants ≥6 weeks and children ≤15 months: IM 0.5 mL per dose given at 2, 4, 6, and 12 through 15 months of age (for a total of 4 doses) Adults IM 0.5 mL as a single dose |
PCV20 [10] | Prevnar 20 (Pfizer, Inc., New York, NY, US) | 8, 10A, 11A, 12F, 15B, 22F, and 33F, in addition to PCV13 serotypes | Adults 19–64 years of age with underlying medical conditions ** Adults ≥ 65 years of age | Adults IM 0.5 mL as a single dose If PCV20 is given, then PPSV23 is not required |
PPSV23 [31] | Pneumovax 23 (Merck and Co, Inc., Rahway, NJ, US) | 2, 8, 9N, 10A, 11A, 12F, 15B, 17F, 20, 22F, 33F, in addition to PCV13 serotypes, less 6A | Children * and adults ** ≥ 60 months of age with underlying medical conditions Adults ≥65 years of age | IM or SC 0.5 mL as a single dose Administer PPSV23 ≥ 1 year after PCV13 or PCV15 Administer a final dose of PPSV23 ≥ 5 years after the previous dose of PPSV23 once the patient turns 65 years of age |
Author (Year) [Ref] | Population | Intervention | Comparison | Outcome |
---|---|---|---|---|
Ermlich (2018) [39] | 691 adults aged ≥ 50 years | PCV15 | PCV13 or PPSV23 | Compared to PCV13 and PPSV23, PCV15 had better immunogenicity for shared serotypes and similar safety at 1-month post-vaccination |
Kishino (2022) [40] | 245 Japanese adults ≥ 65 years of age | PCV15 (includes PCV13 serotypes, and serotypes 22F and 33F) | PCV13 | Higher proportion of participants with a ≥4-fold increase in serotype-specific opsonophagocytic activity responses for PCV15 than for PCV13 for serotypes 3, 22F, and 33F |
Peterson (2019) [41] | 250 adults ≥ 65 years of age with prior PPSV23 ≥ 1 year before | PCV15 | PCV13 | Good safety and immunogenicity in both trial groups |
Platt (2022) [42] | 1202 adults (about 30% aged 50–64 years) | PCV15 | PCV13 | PCV15 non-inferior to PCV13 for 13 shared serotypes, and superior immunogenicity for the 2 unique serotypes |
Simon (2022) [43] | 1299 healthy adults ≥ 65 years of age | PCV15, then PPSV23 6 months later | PCV13, then PPSV23 6 months later | Similar immunogenicity and safety |
Song (2021) [44] | 652 adults (about 50% aged ≥ 65 years) | PCV15, then PPSV23 12 months later | PCV13, then PPSV23 12 months later | Similar immunogenicity and safety |
Stacey (2019) [45] | 690 adults ≥ 50 years of age | PCV15 | PCV13 | Similar immunogenicity and safety |
Cannon (2021) [46] | 875 adults ≥ 65 years of age, with prior pneumococcal vaccination | PCV20 | PCV13 (if prior PPSV23); PPSV23 (if prior PCV13) | PCV20 was immunogenic 1 month after PCV20, regardless of prior PCV13 or PPSV23 |
Essink (2022) [47] | 893 generally healthy pneumococcal vaccine-naïve adults 18–59 years of age | PCV20 | PCV13 | PCV20 was safe and well tolerated. Immunogenicity of PCV20 comparable to that of PCV13 |
Essink (2022) [47] | 3009 generally healthy pneumococcal vaccine-naïve adults ≥ 60 years of age | PCV20, then PPSV23 1 month later | PCV13, then PPSV23 1 month later | PCV20 was safe and well tolerated. Immunogenicity of PCV20 comparable to that of PCV13 or PPSV23 |
Fitz-Patrick (2021) [48] | 104 healthy Japanese adults 18–49 years of age residing in the United States for ≤5 years | PCV20, or complementary 7-valent PCV (cPCV7) (containing non-PCV13 serotypes) | PCV13 | Good opsonophagocytic activity at 1-month post-vaccination |
Klein (2021) [49] | 1710 adults 18–49 years of age | PCV20 | PCV13 | Similar immunogenicity and safety |
Hurley (2021) [26] | 444 adults 60–64 years of age | PCV20, then placebo 1 month later | PCV13, then PPSV23 1 month later | Similar immunogenicity and safety |
Chichili (2022) [28] | 126 pneumococcal vaccine-naïve adults 18–64 years of age. 390 pneumococcal vaccine-naïve adults 65–85 years of age | PCV24 | PCV13 | Higher proportion of participants with opsonophagocytic activity responses at day 30 for PCV24 than for PCV13 for both PCV13 and non-PCV13 serotypes |
Author (Year) [Ref] | Population | Intervention | Comparison | Outcome |
---|---|---|---|---|
Eriksson (2020) [50] | 74 adult kidney transplant recipients, mean age 52.4–55.9 years | PPSV23 before transplant | PCV13 before transplant, with repeat PCV13 6 months after | Similar immunogenicity and safety. Waning sero-response post-transplant restored with repeat PCV13 |
Eriksson (2021) [51] | 47 adult liver transplant recipients, mean age 54.9–56.1 years | PPSV23 before transplant | PCV13 before transplant, with repeat PCV13 6 months after | Similar immunogenicity and safety. Waning sero-response post-transplant restored with repeat PCV13 |
Kantso (2019) [52] | 82 Crohn’s disease patients with or without immunosuppressive therapy, mean age 44 ± 14 years | PPSV23 | PCV13 | Similar persistence of induced antibodies in both trial groups, with similarly reduced persistence when patients were on combination thiopurines and TNF-α antagonists |
Hammit (2022) [53] (2023) [54] | 1131 at-risk adults * and 381 adults without risk factors 18–49 years of age | PCV15, then PPSV23 6 months later | PCV13, then PPSV23 6 months later | Similar immunogenicity, safety, and tolerability across risk factor groups |
Mohapi (2022) [55] | 302 adults living with HIV and receiving antiretroviral therapy, mean age 41.3–42.4 years (range 21–74 years) | PCV15, then PPSV23 8 weeks later | PCV13, then PPSV23 8 weeks later | Similar opsonophagocytic activity geometric mean titers for shared serotypes at day 30 and week 12 |
Clinical Question | Considerations | Details |
---|---|---|
Should the patient receive pneumococcal vaccination? | Risk of severe pneumococcal disease | Yes, for patients at risk of severe invasive or non-invasive pneumococcal disease, which is in turn dependent on patient factors (age, comorbid conditions), and on exposure risk (epidemiology) |
Which pneumococcal vaccine or vaccines should be used? | Immunogenicity Clinical efficacy Mucosal immunity Indirect effect Herd protection | Chosen vaccine should be immunogenic and safe, with as broad protection as possible to cover pathogenic serotypes. Chosen vaccine should have demonstrated reduction of adverse health outcomes such as hospitalization or mortality. Immunocompromised patients benefit despite having lower vaccine immune responses. Consider an additional pneumococcal vaccine if broadened serotype coverage can help prevent severe invasive or non-invasive pneumococcal disease, especially when herd protection is insufficient |
Can pneumococcal vaccine be co-administered with other vaccines? | Immunologic interference Safety and tolerability | Yes, if immunogenicity of both vaccines is not affected and if adverse events are not significantly increased, e.g., with inactivated influenza vaccines |
Should pneumococcal vaccination be repeated? | Waning immunity Replacement strains | Yes, if waning immunity is expected. Immunocompromised patients may benefit from repeated vaccination due to lower vaccine immunogenicity. Emergence of replacement strains may necessitate broadened serotype cover by administering a different vaccine, one that may already be existing or a new vaccine that becomes available to cover additional pathogenic serotypes |
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See, K.C. Pneumococcal Vaccination in Adults: A Narrative Review of Considerations for Individualized Decision-Making. Vaccines 2023, 11, 908. https://doi.org/10.3390/vaccines11050908
See KC. Pneumococcal Vaccination in Adults: A Narrative Review of Considerations for Individualized Decision-Making. Vaccines. 2023; 11(5):908. https://doi.org/10.3390/vaccines11050908
Chicago/Turabian StyleSee, Kay Choong. 2023. "Pneumococcal Vaccination in Adults: A Narrative Review of Considerations for Individualized Decision-Making" Vaccines 11, no. 5: 908. https://doi.org/10.3390/vaccines11050908
APA StyleSee, K. C. (2023). Pneumococcal Vaccination in Adults: A Narrative Review of Considerations for Individualized Decision-Making. Vaccines, 11(5), 908. https://doi.org/10.3390/vaccines11050908