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. 2022 Jun 15;40(27):3746-3751.
doi: 10.1016/j.vaccine.2022.04.086. Epub 2022 May 11.

Decay of anti-Bordetella pertussis antibodies in women of childbearing age following COVID-19 non-pharmaceutical measures

Affiliations

Decay of anti-Bordetella pertussis antibodies in women of childbearing age following COVID-19 non-pharmaceutical measures

Frederic Reicherz et al. Vaccine. .

Abstract

Background: Immunization against Bordetella pertussis during pregnancy reduces morbidity from severe pertussis in young infants via trans-placental transfer of anti-B. pertussis Immunoglobulin G (IgG). Studies have reported a near disappearance of respiratory pathogens including B. pertussis following implementation of mitigation strategies to control Coronavirus disease 2019 (COVID-19). We explored how immunity against B. pertussis changed in women of childbearing-age through the COVID-19 pandemic.

Methods: Paired blood samples from females of childbearing-age collected at the beginning (May-June 2020) and nearly one year into the COVID-19 pandemic (February-May 2021) in British Columbia (BC), Canada were tested for anti-B. pertussis IgG levels. To ascertain whether early-pandemic IgG levels in 2020 reflected levels in pregnant women early in gestation, 1st trimester sera collected from age-matched healthy pregnant women in 2018 and 2019 were tested for anti-B. pertussis IgG. Levels were compared by t tests. P-value of 0.05 was assigned and statistical significance was set as p < 0.016 using Bonferroni correction.

Results: Annual provincial B. pertussis incidences per 100,000 in BC in 2020 (3/100,000) and 2021 (<1/100,000) approximated the lowest levels since 1990. In 2021 vs. 2020, anti-pertussis toxin (PT), filamentous hemagglutinin (FHA) and pertactin (PRN) IgG levels declined in women of childbearing-age: 6.8 IU/ml (95 %CI, 4.2-10.9) vs. 8.4 IU/ml (5.1-13.9; p = 0.004); 18.8 IU/ml (10.9-32.2) vs. 23.6 IU/ml (13.2-42.1; p < 0.001); and 37.1 IU/ml (18.1-75.9) vs. 47.2 IU/ml (24.8-89.9; p = 0.092), respectively. Although all values were slightly higher, anti-PT, FHA and PRN IgG levels in women of childbearing age did not significantly differ in 2020 compared with early-gestation pregnant women in 2018-2019, 8.4 IU/ml (95% CI, 5.1-13.9) vs. 5.4 IU/ml (95% CI, 3.8-7.7; p = 0.166), 23.6 IU/ml (95% CI, 13.2-42.1) vs. 20.1 IU/ml (95% CI, 13.4-30.2; p = 0.656), and 47.2 IU/ml (24.8-89.9) vs. 17.3 IU/ml (95% CI, 10.5-28.7; p = 0.021), respectively.

Discussion: B. pertussis infections should be closely monitored during the relaxing of mitigation measures for COVID-19.

Keywords: Antenatal immunization; COVID-19; Immunity; Pertussis.

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Conflict of interest statement

Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper.

Figures

Fig. 1
Fig. 1
Incidence of laboratory-confirmed and epidemiology-linked Bordetella pertussis cases reported to the British Columbia Centre for Disease Control during the years 2015–2021. *Incidence in 2021 was < 1/100,000 overall, as well as stratified by age among infants < 1 year as well as adults 18–50 and > 50 years. Case definition of a laboratory-confirmed case was isolation of B. pertussis from nasopharyngeal swab or nasopharyngeal wash or detection of B. pertussis DNA using a polymerase chain reaction assay from an appropriate clinical specimen, and one or more of the following: Cough lasting 2 weeks or longer; Paroxysmal cough of any duration; Cough with inspiratory “whoop”; Cough ending in vomiting or gagging, or associated with apnea. Epidemiology-linked case was defined as epidemiological link to a laboratory-confirmed case and one or more of the following for which there is no other etiology: Paroxysmal cough of any duration; Cough with inspiratory “whoop”; Cough ending in vomiting or gagging, or associated with apnea (Source: British Columbia Centre for Disease Control [28]).
Fig. 2
Fig. 2
Geometric mean concentration of serum immunoglobulin (Ig) G to pertussis toxin (A), filamentous hemagglutinin (B), and pertactin (C) in paired samples of women of childbearing age early in the COVID-19 pandemic (2020 in blue dots; n = 18 [for filamentous hemagglutinin n = 17]) and one year after non-pharmaceutical measures (2021 in red dots; n = 18 [for filamentous hemagglutinin n = 17]). Dot-line plot of serum IgG to pertussis toxin (D), filamentous hemagglutinin (E), and pertactin (F) in paired samples of women of childbearing age early in the COVID-19 pandemic (2020 in blue dots; n = 18 [for filamentous hemagglutinin n = 17]) and one year after non-pharmaceutical measures (2021 in red dots; n = 18 [for filamentous hemagglutinin n = 17])).

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