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Kinetics of immune responses to nasal challenge with meningococcal polysaccharide one year after serogroup-C glycoconjugate vaccination

Kinetics of immune responses to nasal challenge with meningococcal polysaccharide one year after serogroup-C glycoconjugate vaccination
Kinetics of immune responses to nasal challenge with meningococcal polysaccharide one year after serogroup-C glycoconjugate vaccination
BACKGROUND: Recipients of serogroup-C glycoconjugate meningococcal vaccine (MCC) exhibit waning of serum bactericidal antibody (SBA) titers, but the rate of decline and the speed of their immunological memory in response to new meningococcal nasopharyngeal colonization are unknown.

METHODS: In a prospective challenge study, we measured persistence of SBA and anti-Neisseria meningitidis serogroup-C (MenC) immunoglobulin (Ig) G and IgA in adults aged 18-39, 28 days and 12 months after receiving MCC. Volunteers were then challenged intranasally with 50 ?g MenC polysaccharide to mimic meningococcal colonization, and systemic and mucosal antibody responses were measured.

RESULTS: All subjects had protective SBA titers (?8) 28 days after MCC vaccination, but 12.3% and 20.2% had unprotective (<8) or low (<128) levels, respectively, after 12 months. Following rechallenge (12 months postvaccination) and measurement of antibody responses after 4, 7, and 10 days, rises in SBA titers were only observed in subjects with low (<128) or nonprotective (<8) prerechallenge SBA titers. In subjects with pre rechallenge SBA titers <8, the majority did not reach a protective SBA titer until 7 days post-rechallenge. MenC-specific IgG levels rose in both serum and saliva in correlation with SBA titers. No detectable rise in salivary IgA was observed.

CONCLUSIONS: In those individuals who fail to retain protective SBA 12 months after MCC, immunological memory fails to generate protective systemic and mucosal antibodies until 7 days post intranasal challenge with cognate meningococcal polysaccharide. This is likely too slow to protect from natural meningococcal infection. MCC vaccinees rely on persistence of antibody levels rather than immunological memory for sustained protection.
1058-4838
1317-1323
Wing, James B.
f1e7db81-a229-4386-87ea-f58dd0e8519a
Smart, Lynne
e307ff61-93e1-43a1-9b74-4344cec1796b
Borrow, Ray
45e5fda9-8300-486e-89ca-323f3ae9c9a6
Findlow, Jamie
8580c790-262c-4fc5-99bc-0beddaef98a0
Findlow, Helen
9c348bc8-0bc8-4143-b2b4-f5f29f67f9cb
Heath, Andrew W.
303a3623-9848-4b85-add7-880752386f0d
Read, Robert C.
b5caca7b-0063-438a-b703-7ecbb6fc2b51
Wing, James B.
f1e7db81-a229-4386-87ea-f58dd0e8519a
Smart, Lynne
e307ff61-93e1-43a1-9b74-4344cec1796b
Borrow, Ray
45e5fda9-8300-486e-89ca-323f3ae9c9a6
Findlow, Jamie
8580c790-262c-4fc5-99bc-0beddaef98a0
Findlow, Helen
9c348bc8-0bc8-4143-b2b4-f5f29f67f9cb
Heath, Andrew W.
303a3623-9848-4b85-add7-880752386f0d
Read, Robert C.
b5caca7b-0063-438a-b703-7ecbb6fc2b51

Wing, James B., Smart, Lynne, Borrow, Ray, Findlow, Jamie, Findlow, Helen, Heath, Andrew W. and Read, Robert C. (2011) Kinetics of immune responses to nasal challenge with meningococcal polysaccharide one year after serogroup-C glycoconjugate vaccination. Clinical Infectious Diseases, 52 (11), 1317-1323. (doi:10.1093/cid/cir198). (PMID:21596673)

Record type: Article

Abstract

BACKGROUND: Recipients of serogroup-C glycoconjugate meningococcal vaccine (MCC) exhibit waning of serum bactericidal antibody (SBA) titers, but the rate of decline and the speed of their immunological memory in response to new meningococcal nasopharyngeal colonization are unknown.

METHODS: In a prospective challenge study, we measured persistence of SBA and anti-Neisseria meningitidis serogroup-C (MenC) immunoglobulin (Ig) G and IgA in adults aged 18-39, 28 days and 12 months after receiving MCC. Volunteers were then challenged intranasally with 50 ?g MenC polysaccharide to mimic meningococcal colonization, and systemic and mucosal antibody responses were measured.

RESULTS: All subjects had protective SBA titers (?8) 28 days after MCC vaccination, but 12.3% and 20.2% had unprotective (<8) or low (<128) levels, respectively, after 12 months. Following rechallenge (12 months postvaccination) and measurement of antibody responses after 4, 7, and 10 days, rises in SBA titers were only observed in subjects with low (<128) or nonprotective (<8) prerechallenge SBA titers. In subjects with pre rechallenge SBA titers <8, the majority did not reach a protective SBA titer until 7 days post-rechallenge. MenC-specific IgG levels rose in both serum and saliva in correlation with SBA titers. No detectable rise in salivary IgA was observed.

CONCLUSIONS: In those individuals who fail to retain protective SBA 12 months after MCC, immunological memory fails to generate protective systemic and mucosal antibodies until 7 days post intranasal challenge with cognate meningococcal polysaccharide. This is likely too slow to protect from natural meningococcal infection. MCC vaccinees rely on persistence of antibody levels rather than immunological memory for sustained protection.

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Published date: June 2011
Organisations: Clinical & Experimental Sciences

Identifiers

Local EPrints ID: 341689
URI: http://eprints.soton.ac.uk/id/eprint/341689
ISSN: 1058-4838
PURE UUID: 1c85cea8-e7ca-4775-b1e2-e3ae37433416
ORCID for Robert C. Read: ORCID iD orcid.org/0000-0002-4297-6728

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Date deposited: 03 Aug 2012 10:32
Last modified: 15 Mar 2024 03:42

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Contributors

Author: James B. Wing
Author: Lynne Smart
Author: Ray Borrow
Author: Jamie Findlow
Author: Helen Findlow
Author: Andrew W. Heath
Author: Robert C. Read ORCID iD

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