Your search keyword '"Dorothy M. Dickson"' showing total 16 results

1. Network analysis of patterns and relevance of enteric pathogen co-infections among infants in a diarrhea-endemic setting

Author

E. Ross Colgate, Connor Klopfer, Dorothy M. Dickson, Benjamin Lee, Matthew J. Wargo, Ashraful Alam, Beth D. Kirkpatrick, and Laurent Hébert-Dufresne

Subjects

Biology (General), QH301-705.5

Published

2023

2. Infant Non-Secretor Histoblood Group Antigen Phenotype Reduces Susceptibility to Both Symptomatic and Asymptomatic Rotavirus Infection

Author

Benjamin Lee, Md Abdul Kader, Masud Alam, Dorothy M. Dickson, Patrick Harvey, E. Ross Colgate, Mami Taniuchi, William A. Petri, Rashidul Haque, and Beth D. Kirkpatrick

Subjects

rotavirus, diarrhea, gastroenteritis, secretor, FUT2, histoblood group antigen, Medicine

Abstract

The infant non-secretor histoblood group antigen phenotype is associated with reduced risk of symptomatic rotavirus diarrhea, one of the leading global causes of severe pediatric diarrheal disease and mortality. However, little is known regarding the role of secretor status in asymptomatic rotavirus infections. Therefore, we performed a nested case–control study within a birth cohort study previously conducted in Dhaka, Bangladesh, to determine the association between infant secretor phenotype and the odds of asymptomatic rotavirus infection, in addition to the risk of rotavirus diarrhea, in unvaccinated infants. In the parent cohort, infants were enrolled in the first week of life and followed through the first two years of life with multiple clinic visits and active surveillance for diarrheal illness. Secretor phenotyping was performed on saliva. Eleven surveillance stools collected over the first year of life were tested for rotavirus by real-time RT-PCR, followed by conventional PCR and amplicon sequencing to identify the infecting P-type of positive specimens. Similar to findings for symptomatic diarrhea, infant non-secretors experienced significantly fewer primary episodes of asymptomatic rotavirus infection through the first year of life in a likely rotavirus P-genotype-dependent manner. These data suggest that non-secretors experienced reduced risk from rotavirus due to decreased susceptibility to infection rather than reduced infection severity.

Published

2024

3. Oral rotavirus vaccine shedding as a marker of mucosal immunity

Author

Benjamin Lee, Md Abdul Kader, E. Ross Colgate, Marya Carmolli, Dorothy M. Dickson, Sean A. Diehl, Masud Alam, Sajia Afreen, Josyf C. Mychaleckyj, Uma Nayak, William A. Petri, Rashidul Haque, and Beth D. Kirkpatrick

Subjects

Medicine, Science

Abstract

Abstract Group A rotaviruses (RVA) remain a leading cause of pediatric diarrhea worldwide, in part due to underperformance of currently approved live-attenuated, oral vaccines in low-and-middle income countries. Improved immune correlates of protection (CoP) for existing oral vaccines and novel strategies to evaluate the performance of next-generation vaccines are needed. Use of oral vaccines as challenge agents in controlled human infection models is a potential approach to CoP discovery that remains underexplored. In a live-attenuated, oral rotavirus vaccine (Rotarix, GlaxoSmithKline) efficacy trial conducted among infants in Dhaka, Bangladesh, we explored the potential for the second dose of the two-dose series to be considered a challenge agent through which RVA immunity could be explored, using fecal virus shedding post-dose 2 as a marker of mucosal immunity. Among 180 vaccinated infants who completed the parent study per protocol, the absence of fecal vaccine shedding following the second dose of Rotarix suggested intestinal mucosal immunity generated by the first dose and a decreased risk of RVA diarrhea through 2 years of life (RR 0.616, 95% CI 0.392–0.968). Further development of controlled human infection models for group A rotaviruses, especially in prospective studies with larger sample sizes, may be a promising tool to assess rotavirus vaccine efficacy and CoPs.

Published

2021

4. Immunotranscriptomic profiling the acute and clearance phases of a human challenge dengue virus serotype 2 infection model

Author

John P. Hanley, Huy A. Tu, Julie A. Dragon, Dorothy M. Dickson, Roxana del Rio-Guerra, Scott W. Tighe, Korin M. Eckstrom, Nicholas Selig, Samuel V. Scarpino, Stephen S. Whitehead, Anna P. Durbin, Kristen K. Pierce, Beth D. Kirkpatrick, Donna M. Rizzo, Seth Frietze, and Sean A. Diehl

Subjects

Science

Abstract

Dengue virus causes a range of inflammatory pathology but understanding critical phases of the infection during human infection has been challenging. Here the author’s present immunotranscriptomic changes during the acute and clearance phases of a dengue virus serotype 2 human challenge model.

Published

2021

5. In a randomized trial, the live attenuated tetravalent dengue vaccine TV003 is well-tolerated and highly immunogenic in subjects with flavivirus exposure prior to vaccination.

Author

Stephen S Whitehead, Anna P Durbin, Kristen K Pierce, Dan Elwood, Benjamin D McElvany, Ellen A Fraser, Marya P Carmolli, Cecilia M Tibery, Noreen A Hynes, Matthew Jo, Janece M Lovchik, Catherine J Larsson, Elena A Doty, Dorothy M Dickson, Catherine J Luke, Kanta Subbarao, Sean A Diehl, and Beth D Kirkpatrick

Subjects

Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270

Abstract

Infection caused by the four serotypes of dengue virus (DENV-1-4) is a leading cause of mosquito-borne disease. Clinically-severe dengue disease is more common when secondary dengue infection occurs following prior infection with a heterologous dengue serotype. Other flaviviruses such as yellow fever virus, Japanese encephalitis virus, and Zika virus, can also elicit antibodies which are cross-reactive to DENV. As candidate dengue vaccines become available in endemic settings and for individuals who have received other flavivirus vaccines, it is important to examine vaccine safety and immunogenicity in these flavivirus-experienced populations. We performed a randomized, controlled trial of the National Institutes of Health live attenuated tetravalent dengue vaccine candidate (TV003) in fifty-eight individuals with prior exposure to flavivirus infection or vaccine. As in prior studies of this vaccine in flavivirus-naive volunteers, flavivirus-experienced subjects received two doses of vaccine six months apart and were followed closely for clinical events, laboratory changes, viremia, and neutralizing antibody titers. TV003 was well tolerated with few adverse events other than rash, which was predominately mild. Following one dose, 87% of vaccinees had an antibody response to all four serotypes (tetravalent response), suggesting a robust immune response. In addition, 76% of vaccinees were viremic; mean peak titers ranged from 0.68–1.1 log10 PFU/mL and did not differ by serotype. The second dose of TV003 was not associated with viremia, rash, or a sustained boost in antibody titers indicating that a single dose of the vaccine is likely sufficient to prevent viral replication and thus protect against disease. In comparison to the viremia and neutralizing antibody response elicited by TV003 in flavivirus-naïve subjects from prior studies, we found that subjects who were flavivirus-exposed prior to vaccination exhibited slightly higher DENV-3 viremia, higher neutralizing antibody titers to DENV-2, -3, and -4, and a higher tetravalent response frequency after TV003 administration. In summary, we demonstrate that the NIH tetravalent dengue vaccine TV003 is well-tolerated in flavivirus-experienced individuals and elicits robust post-vaccination neutralizing antibody titers.ClinicalTrials.gov NCT01506570.

Published

2017

6. Intradermal fractional-dose inactivated polio vaccine (fIPV) adjuvanted with double mutant Enterotoxigenic Escherichia coli heat labile toxin (dmLT) is well-tolerated and augments a systemic immune response to all three poliovirus serotypes in a randomized placebo-controlled trial

Author

Jessica W. Crothers, Elizabeth Ross Colgate, Kelly J. Cowan, Dorothy M. Dickson, MaryClaire Walsh, Marya Carmolli, Peter F. Wright, Elizabeth B. Norton, and Beth D. Kirkpatrick

Subjects

Hot Temperature, General Veterinary, General Immunology and Microbiology, Public Health, Environmental and Occupational Health, Infant, Antibodies, Viral, Serogroup, Antibodies, Neutralizing, Poliovirus, Poliovirus Vaccine, Inactivated, Infectious Diseases, Adjuvants, Immunologic, Poliovirus Vaccine, Oral, Molecular Medicine, Enterotoxigenic Escherichia coli, Humans, Child, Immunity, Mucosal, Poliomyelitis

Abstract

Eradication of poliomyelitis globally is constrained by fecal shedding of live polioviruses, both wild-type and vaccine-derived strains, into the environment. Although inactivated polio vaccines (IPV) effectively protect the recipient from clinical poliomyelitis, fecal shedding of live virus still occurs following infection with either wildtype or vaccine-derived strains of poliovirus. In the drive to eliminate the last cases of polio globally, improvements in both oral polio vaccines (OPV) (to prevent reversion to virulence) and injectable polio vaccines (to improve mucosal immunity and prevent viral shedding) are underway. The E. coli labile toxin with two or "double" attenuating mutations (dmLT) may boost immunologic responses to IPV, including at mucosal sites. We performed a double-blinded phase I controlled clinical trial to evaluate safety, tolerability, as well as systemic and mucosal immunogenicity of IPV adjuvanted with dmLT, given as a fractional (1/5th) dose intradermally (fIPV-dmLT). Twenty-nine volunteers with no past exposure to OPV were randomized to a single dose of fIPV-dmLT or fIPV alone. fIPV-dmLT was well tolerated, although three subjects had mild but persistent induration and hyperpigmentation at the injection site. A ≥ 4-fold rise in serotype-specific neutralizing antibody (SNA) titers to all three serotypes was seen in 84% of subjects receiving fIPV-dmLT vs. 50% of volunteers receiving IPV alone. SNA titers were higher in the dmLT-adjuvanted group, but only differences in serotype 1 were significant. Mucosal immune responses, as measured by polio serotype specific fecal IgA were minimal in both groups and differences were not seen. fIPV-dmLT may offer a benefit over IPV alone. Beyond NAB responses protecting the individual, studies demonstrating the ability of fIPV-dmLT to prevent viral shedding are necessary. Studies employing controlled human infection models, using monovalent OPV post-vaccine are ongoing. Studies specifically in children may also be necessary and additional biomarkers of mucosal immune responses in this population are needed. Clinicaltrials.gov Identifer: NCT03922061.

Published

2022

7. The effect of increased inoculum on oral rotavirus vaccine take among infants in Dhaka, Bangladesh: A double-blind, parallel group, randomized, controlled trial

Author

Abdul Kader, Faria Afrin, Daniel M. Bak, Mona Tolba, Rashidul Haque, Benjamin Lee, Mami Taniuchi, Monica M. McNeal, Sajia Afreen, Soyeon K. Gullickson, Marya P. Carmolli, Masud Alam, Dorothy M. Dickson, Beth D. Kirkpatrick, Tania Ferdousi, and Christina F. Damon

Subjects

Male, Pediatrics, medicine.medical_specialty, 030231 tropical medicine, Immunization, Secondary, Administration, Oral, Vaccines, Attenuated, medicine.disease_cause, Rotavirus Infections, Article, law.invention, Double blind, 03 medical and health sciences, 0302 clinical medicine, Primary outcome, Double-Blind Method, Randomized controlled trial, law, Rotavirus, medicine, Humans, 030212 general & internal medicine, Adverse effect, Bangladesh, Dose-Response Relationship, Drug, General Veterinary, General Immunology and Microbiology, business.industry, Immunogenicity, Rotavirus Vaccines, Public Health, Environmental and Occupational Health, Infant, Congenital malformations, Rotavirus vaccine, Treatment Outcome, Infectious Diseases, Molecular Medicine, Female, business

Abstract

BACKGROUND: Oral, live-attenuated rotavirus vaccines suffer from impaired immunogenicity and efficacy in low-income countries. Increasing the inoculum of vaccine might improve vaccine response, but this approach has been inadequately explored in low-income countries. METHODS: We performed a double-blind, parallel group, randomized controlled trial from June 2017 through June 2018 in the urban Mirpur slum of Dhaka, Bangladesh to compare vaccine take (primary outcome) among healthy infants randomized to receive either the standard dose or double the standard dose of oral Rotarix (GlaxoSmithKline) vaccine at 6 and 10 weeks of life. Infants with congenital malformations, birth or enrollment weight

Published

2020

8. Corrigendum to 'Intradermal fractional-dose inactivated polio vaccine (fIPV) adjuvanted with double mutant Enterotoxigenic Escherichia coli heat labile toxin (dmLT) is well-tolerated and augments a systemic immune response to all three poliovirus serotypes in a randomized active-controlled trial' [Vaccine 40(19) (2022) 2705–2713]

Author

Jessica W. Crothers, Elizabeth Ross Colgate, Kelly J. Cowan, Dorothy M. Dickson, MaryClaire Walsh, Marya Carmolli, Peter F. Wright, Elizabeth B. Norton, and Beth D. Kirkpatrick

Subjects

Infectious Diseases, General Veterinary, General Immunology and Microbiology, Public Health, Environmental and Occupational Health, Molecular Medicine

Published

2022

9. Histo–Blood Group Antigen Phenotype Determines Susceptibility to Genotype-Specific Rotavirus Infections and Impacts Measures of Rotavirus Vaccine Efficacy

Author

Benjamin, Lee, Dorothy M, Dickson, Allan C, deCamp, E, Ross Colgate, Sean A, Diehl, Muhammad Ikhtear, Uddin, Salma, Sharmin, Shahidul, Islam, Taufiqur Rahman, Bhuiyan, Masud, Alam, Uma, Nayak, Josyf C, Mychaleckyj, Mami, Taniuchi, William A, Petri, Rashidul, Haque, Firdausi, Qadri, and Beth D, Kirkpatrick

Subjects

Diarrhea, Bangladesh, Genotype, Errata, Rotavirus Vaccines, Infant, vaccine efficacy, Vaccines, Attenuated, vaccination, Rotavirus Infections, secretor, Major Articles and Brief Reports, fluids and secretions, rotavirus, Lewis, Viruses, Blood Group Antigens, Humans

Abstract

Background Lewis and secretor histo–blood group antigens (HBGAs) have been associated with decreased susceptibility to P[8] genotype rotavirus (RV) infections. Efficacy of vaccines containing attenuated P[8] strains is decreased in low-income countries. Host phenotype might impact vaccine efficacy (VE) by altering susceptibility to vaccination or RV diarrhea (RVD). We performed a substudy in a monovalent RV vaccine (RV1) efficacy trial in Bangladesh to determine the impact of Lewis and secretor status on risk of RVD and VE. Methods In infants randomized to receive RV1 or no RV1 at 10 and 17 weeks with 1 year of complete active diarrheal surveillance, we performed Lewis and secretor phenotyping and genotyped the infecting strain of each episode of RVD. Results A vaccine containing P[8] RV protected secretors and nonsecretors similarly. However, unvaccinated nonsecretors had a reduced risk of RVD (relative risk, 0.53 [95% confidence interval, .36–.79]) mediated by complete protection from P[4] but not P[8] RVs. This effect reduced VE in nonsecretors to 31.7%, compared to 56.2% among secretors, and decreased VE for the overall cohort. Conclusions Host HBGA status may impact VE estimates by altering susceptibility to RV in unvaccinated children; future trials should therefore account for HBGA status. Clinical Trials Registration NCT01375647., Histo–blood group antigens were associated with genotype-specific susceptibility to rotavirus infections. Nonsecretors were at decreased risk of P[4] infections, while Lewis-negative children were at increased risk of P[6] infections. These effects may impact oral rotavirus vaccine efficacy estimates.

Published

2018

10. SARS CoV-2 seroprevalence in a US school district during COVID-19

Author

Dorothy M. Dickson, Sally Cook, Marya P. Carmolli, Nancy R. Graham, Sean A. Diehl, Benjamin Lee, Beth D. Kirkpatrick, Benjamin K. Grebber, and Sean S M Bullis

Subjects

2019-20 coronavirus outbreak, Schools, Coronavirus disease 2019 (COVID-19), SARS-CoV-2, business.industry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), education, Original Research Letter, COVID-19, School district, Pediatrics, RJ1-570, Seroepidemiologic Studies, Environmental health, Pediatrics, Perinatology and Child Health, Humans, Seroprevalence, Medicine, Child, Students, business

Abstract

Reduced symptomatology and access to testing in children have led to underestimates of paediatric COVID-19 prevalence and raised concerns about school safety. To explore COVID-19 prevalence and risk factors in school settings, we conducted a SARS-CoV-2 serosurvey in a Vermont, USA school district in December 2020. Among 336 students (63%) and 196 teachers/staff (37%), adjusted seroprevalence was 4.7% (95% CI 2.9 to 7.2) and was lowest in preK-5 students (4–10 Years). Seroprevalence was 10-fold higher than corresponding state PCR data but was low overall with no evidence of onward transmissions. These results further support feasibility of in-person learning during COVID-19 with appropriate mitigation measures.

Published

2021

11. Impact of enterovirus and other enteric pathogens on oral polio and rotavirus vaccine performance in Bangladeshi infants

Author

William A. Petri, Jashim Uddin, Dorothy M. Dickson, Sharmin Begum, E. Ross Colgate, Rashidul Haque, Mami Taniuchi, Eric R. Houpt, Beth D. Kirkpatrick, Uma Nayak, Marya P. Carmolli, Shihab U. Sobuz, James A Platts-Mills, and Jie Liu

Subjects

Male, Enteric infections, viruses, Vaccine efficacy, Antibodies, Viral, medicine.disease_cause, TAC, TaqMan Array Card, NPEV, non-polio enterovirus, Feces, 0302 clinical medicine, Rotavirus, Campylobacter Infections, EPEC, enteropathogenic E. coli, ETEC, enterotoxigenic E. coli, 030212 general & internal medicine, PROVIDE, Performance of Rotavirus and Oral Polio Vaccines in Developing Countries, Oral polio vaccine, Enterovirus, Bangladesh, EIEC, enteroinvasive E. coli, Poliovirus, virus diseases, Rotavirus vaccine, 3. Good health, Poliomyelitis, Titer, Diarrhea, PCR, Infectious Diseases, Child, Preschool, Vaccine immunogenicity, Molecular Medicine, Female, medicine.symptom, EAEC, enteroaggregative E. coli, 030231 tropical medicine, chemical and pharmacologic phenomena, EV, enterovirus, Vaccines, Attenuated, complex mixtures, Article, 03 medical and health sciences, Immunology and Microbiology(all), Enterovirus Infections, medicine, Humans, General Veterinary, General Immunology and Microbiology, business.industry, IPV, inactivated poliovirus vaccine, STEC, Shiga-toxin producing E. coli, Rotavirus Vaccines, Public Health, Environmental and Occupational Health, Infant, OPV, oral polio vaccine, Campylobacter, medicine.disease, Antibodies, Neutralizing, veterinary(all), Virology, Immunoglobulin A, RV, rotavirus vaccine, Poliovirus Vaccine, Oral, Immunology, business

Abstract

Highlights • Oral vaccines exhibit poor performance in low-income settings. • Enterovirus and Campylobacter carriage are associated with lower OPV immunogenicity. • Enterovirus carriage is associated with lower Rotarix immunogenicity and efficacy., Background Oral polio vaccine (OPV) and rotavirus vaccine (RV) exhibit poorer performance in low-income settings compared to high-income settings. Prior studies have suggested an inhibitory effect of concurrent non-polio enterovirus (NPEV) infection, but the impact of other enteric infections has not been comprehensively evaluated. Methods In urban Bangladesh, we tested stools for a broad range of enteric viruses, bacteria, parasites, and fungi by quantitative PCR from infants at weeks 6 and 10 of life, coincident with the first OPV and RV administration respectively, and examined the association between enteropathogen quantity and subsequent OPV serum neutralizing titers, serum rotavirus IgA, and rotavirus diarrhea. Results Campylobacter and enterovirus (EV) quantity at the time of administration of the first dose of OPV was associated with lower OPV1-2 serum neutralizing titers, while enterovirus quantity was also associated with diminished rotavirus IgA (−0.08 change in log titer per tenfold increase in quantity; P = 0.037), failure to seroconvert (OR 0.78, 95% CI: 0.64–0.96; P = 0.022), and breakthrough rotavirus diarrhea (OR 1.34, 95% CI: 1.05–1.71; P = 0.020) after adjusting for potential confounders. These associations were not observed for Sabin strain poliovirus quantity. Conclusion In this broad survey of enteropathogens and oral vaccine performance we find a particular association between EV carriage, particularly NPEV, and OPV immunogenicity and RV protection. Strategies to reduce EV infections may improve oral vaccine responses. ClinicalTrials.gov Identifier: NCT01375647.

Published

2016

12. Delayed Dosing of Oral Rotavirus Vaccine Demonstrates Decreased Risk of Rotavirus Gastroenteritis Associated With Serum Zinc: A Randomized Controlled Trial

Author

Dorothy M. Dickson, Marya P. Carmolli, Uma Nayak, Beth D. Kirkpatrick, E. Ross Colgate, Firdausi Qadri, Josyf C. Mychaleckyj, K. Zaman, Sean A. Diehl, Masud Alam, William A. Petri, Mary Claire Walsh, and Rashidul Haque

Subjects

Male, Rotavirus, 0301 basic medicine, Microbiology (medical), medicine.medical_specialty, Administration, Oral, medicine.disease_cause, Rotavirus Infections, 03 medical and health sciences, 0302 clinical medicine, Risk Factors, Internal medicine, medicine, Humans, 030212 general & internal medicine, Seroconversion, Bangladesh, business.industry, Incidence, Incidence (epidemiology), Infant, Newborn, Rotavirus Vaccines, Odds ratio, Rotavirus vaccine, Gastroenteritis, Vaccination, Zinc, Diarrhea, 030104 developmental biology, Infectious Diseases, Immunology, Female, medicine.symptom, business, Breast feeding

Abstract

Background Rotavirus is the world's leading cause of childhood diarrheal death. Despite successes, oral rotavirus vaccines are less effective in developing countries. In an urban slum of Dhaka, we performed active diarrhea surveillance to evaluate monovalent G1P[8] rotavirus vaccine (RV1) efficacy and understand variables contributing to risk of rotavirus diarrhea (RVD). Methods We performed a randomized controlled trial of monovalent oral rotavirus vaccine (RV1). Seven hundred healthy infants received RV1 or no RV1 (1:1) using delayed dosing (10 and 17 weeks) and were followed for 1 year. Intensive diarrhea surveillance was performed. The primary outcome was ≥1 episode of RVD. Nutritional, socioeconomic, and immunologic factors were assessed by logistic regression best-subsets analysis for association with risk of RVD and interactions with vaccine arm. Results Incidence of all RVD was 38.3 cases per 100 person-years. Per-protocol RV1 efficacy was 73.5% (95% confidence interval [CI], 45.8%-87.0%) against severe RVD and 51% (95% CI, 33.8%-63.7%) against all RVD. Serum zinc level (odds ratio [OR], 0.77; P = .002) and lack of rotavirus immunoglobulin A (IgA) seroconversion (OR, 1.95; P = .018) were associated with risk of RVD, independent of vaccination status. Water treatment and exclusive breastfeeding were of borderline significance. Factors not associated with RVD included height for age at 10 weeks, vitamin D, retinol binding protein, maternal education, household income, and sex. Conclusions In an urban slum with high incidence of RVD, the efficacy of RV1 against severe RVD was higher than anticipated in the setting of delayed dosing. Lower serum zinc level and lack of IgA seroconversion were associated with increased risk of RVD independent of vaccination. Clinical trials registration NCT01375647.

Published

2016

13. Rotavirus-Specific Immunoglobulin A Responses Are Impaired and Serve as a Suboptimal Correlate of Protection Among Infants in Bangladesh

Author

Benjamin, Lee, Marya, Carmolli, Dorothy M, Dickson, E Ross, Colgate, Sean A, Diehl, Muhammad Ikhtear, Uddin, Shahidul, Islam, Motaher, Hossain, Tanzeem Ahmed, Rafique, Taufiqur Rahman, Bhuiyan, Masud, Alam, Uma, Nayak, Josyf C, Mychaleckyj, Monica M, McNeal, William A, Petri, Firdausi, Qadri, Rashidul, Haque, and Beth D, Kirkpatrick

Subjects

Diarrhea, Rotavirus, Bangladesh, Vaccination, Rotavirus Vaccines, Administration, Oral, Infant, Antibodies, Viral, Vaccines, Attenuated, Rotavirus Infections, Immunoglobulin A, Prentice criteria, Immunogenicity, Vaccine, Seroconversion, Humans, correlate of protection, Immunity, Maternally-Acquired, Articles and Commentaries, IgA

Abstract

Background Rotavirus (RV)–specific immunoglobulin A (IgA) responses following oral RV vaccination are impaired in low-income countries, where the utility of RV-IgA as a correlate of protection (CoP) remains unclear. In a monovalent oral RV vaccine (Rotarix) efficacy trial among infants in Dhaka, Bangladesh, we identified factors associated with poor RV-IgA responses and explored the utility of RV-IgA as a CoP. Methods Infants were randomized to receive Rotarix or no Rotarix at 10 and 17 weeks of life and followed with active diarrheal surveillance. RV-IgA concentration, seroconversion, and seropositivity were determined at 18 weeks of life and analyzed for correlation(s) with rotavirus diarrhea (RVD) and for contribution to Rotarix vaccine effect. Results Among vaccinated infants, overall RV-IgA geometric mean concentration was 21 U/mL; only 27% seroconverted and 32% were seropositive after vaccination. Increased RV-specific maternal antibodies significantly impaired immunogenicity. Seroconversion was associated with reduced risk of RVD through 1 year of life, but RV-IgA seropositivity only explained 7.8% of the vaccine effect demonstrated by the clinical endpoint (RVD). Conclusions RV-IgA responses were low among infants in Bangladesh and were significantly impaired by maternal antibodies. RV-IgA is a suboptimal CoP in this setting; an improved CoP for RV in low-income countries is needed. Clinical Trials Registration NCT01375647., Monovalent oral rotavirus vaccine was poorly immunogenic among infants in Bangladesh. The standard measure of vaccine immunogenicity, rotavirus-specific immunoglobulin A, appeared to be a suboptimal correlate of protection (CoP) in this population, suggesting that improved CoPs are needed.

Published

2017

14. The 'Performance of Rotavirus and Oral Polio Vaccines in Developing Countries' (PROVIDE) study: description of methods of an interventional study designed to explore complex biologic problems

Author

Mary Claire Walsh, Mami Taniuchi, Marya P. Carmolli, Uma Nayak, Dorothy M. Dickson, E. Ross Colgate, R. Haque, Masud Alam, Jennie Z. Ma, Firdausi Qadri, Beth D. Kirkpatrick, Josyf C. Mychaleckyj, William A. Petri, Sean A. Diehl, and Caitlin Naylor

Subjects

Male, Rotavirus, medicine.medical_specialty, Developing country, Administration, Oral, medicine.disease_cause, Antibodies, Viral, Vaccines, Attenuated, Rotavirus Infections, law.invention, Cohort Studies, Polio vaccine, Randomized controlled trial, law, Virology, medicine, Humans, Intensive care medicine, Child, Developing Countries, Bangladesh, business.industry, Rotavirus Vaccines, Infant, Articles, medicine.disease, Rotavirus vaccine, Poliomyelitis, Clinical trial, Poliovirus Vaccines, Poliovirus, Infectious Diseases, Child, Preschool, Poliovirus Vaccine, Oral, Immunology, Parasitology, Female, business, Cohort study

Abstract

Oral vaccines appear less effective in children in the developing world. Proposed biologic reasons include concurrent enteric infections, malnutrition, breast milk interference, and environmental enteropathy (EE). Rigorous study design and careful data management are essential to begin to understand this complex problem while assuring research subject safety. Herein, we describe the methodology and lessons learned in the PROVIDE study (Dhaka, Bangladesh). A randomized clinical trial platform evaluated the efficacy of delayed-dose oral rotavirus vaccine as well as the benefit of an injectable polio vaccine replacing one dose of oral polio vaccine. This rigorous infrastructure supported the additional examination of hypotheses of vaccine underperformance. Primary and secondary efficacy and immunogenicity measures for rotavirus and polio vaccines were measured, as well as the impact of EE and additional exploratory variables. Methods for the enrollment and 2-year follow-up of a 700 child birth cohort are described, including core laboratory, safety, regulatory, and data management practices. Intense efforts to standardize clinical, laboratory, and data management procedures in a developing world setting provide clinical trials rigor to all outcomes. Although this study infrastructure requires extensive time and effort, it allows optimized safety and confidence in the validity of data gathered in complex, developing country settings.

Published

2014

15. Environmental Enteropathy, Oral Vaccine Failure and Growth Faltering in Infants in Bangladesh

Author

Josyf C. Mychaleckyj, William C. Weldon, Fiona R. M. van der Klis, Jennie Z. Ma, Dinesh Mondal, Erica L. Buonomo, Marya P. Carmolli, Beth D. Kirkpatrick, M. Steven Oberste, Dorothy M. Dickson, William A. Petri, Ross Colgate, Rashidul Haque, Caitlin Naylor, Miao Lu, and Uma Nayak

Subjects

Male, Environmental enteropathy, Pediatrics, medicine.medical_specialty, Urban Population, Population, Administration, Oral, lcsh:Medicine, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Intestinal absorption, Infant nutrition disorder, Cohort Studies, Rotavirus, Oral vaccine failure, Outcome Assessment, Health Care, medicine, Cluster Analysis, Humans, Public Health Surveillance, education, Subclinical infection, 2. Zero hunger, education.field_of_study, Bangladesh, Vaccines, lcsh:R5-920, business.industry, Vaccination, lcsh:R, Malnutrition, Infant, Newborn, Infant, General Medicine, medicine.disease, Infant Nutrition Disorders, 3. Good health, Intestinal Diseases, Socioeconomic Factors, Female, business, lcsh:Medicine (General), Vaccine failure, Biomarkers, Research Article

Abstract

Background Environmental enteropathy (EE) is a subclinical enteric condition found in low-income countries that is characterized by intestinal inflammation, reduced intestinal absorption, and gut barrier dysfunction. We aimed to assess if EE impairs the success of oral polio and rotavirus vaccines in infants in Bangladesh. Methods We conducted a prospective observational study of 700 infants from an urban slum of Dhaka, Bangladesh from May 2011 to November 2014. Infants were enrolled in the first week of life and followed to age one year through biweekly home visits with EPI vaccines administered and growth monitored. EE was operationally defied as enteric inflammation measured by any one of the fecal biomarkers reg1B, alpha-1-antitrypsin, MPO, calprotectin, or neopterin. Oral polio vaccine success was evaluated by immunogenicity, and rotavirus vaccine response was evaluated by immunogenicity and protection from disease. This study is registered with ClinicalTrials.gov, number NCT01375647. Findings EE was present in greater than 80% of infants by 12 weeks of age. Oral poliovirus and rotavirus vaccines failed in 20.2% and 68.5% of the infants respectively, and 28.6% were malnourished (HAZ, Highlights • Environmental enteropathy was present in the majority of Dhaka slum children at 12 weeks of age. • Growth in the first year of life was negatively impacted by environmental enteropathy • Oral vaccine response, but not parenteral vaccine response, was negatively impacted by environmental enteropathy • Biomarkers predictive of malnutrition and vaccine failure fell into three clusters: gut inflammation, systemic inflammation and maternal factors. Malnutrition and oral vaccine failure are common in infants living in unsanitary conditions in low income countries. We hypothesized that exposure to infections of the gut at an early age could result in an inflammatory condition of the intestine termed Environmental Enteropathy (EE), and that this in turn could contribute to malnutrition and vaccine response. Children from an urban slum in Dhaka Bangladesh were enrolled within the first week of life, and vaccine response and growth measured to age one year. Most children were infected by two or more enteric infections and had the characteristic inflammation of EE. Both malnutrition and oral vaccine failure were associated with EE. We concluded that improvement in child health in low income countries will likely require prevention or treatment of gut damage due to infection.

16. Effect of substituting IPV for tOPV on immunity to poliovirus in Bangladeshi infants: An open-label randomized controlled trial

Author

Dorothy M. Dickson, M. Steven Oberste, K. Zaman, Masud Alam, Uma Nayak, Marya P. Carmolli, Mami Taniuchi, William A. Petri, Eric R. Houpt, William C. Weldon, E. Ross Colgate, Rashidul Haque, Dadong Zhang, Beth D. Kirkpatrick, and Josyf C. Mychaleckyj

Subjects

Pediatrics, medicine.medical_specialty, Oral poliovirus vaccine, Serum neutralizing antibody, ClinicalTrials.gov NCT01375647, 030231 tropical medicine, medicine.disease_cause, Herd immunity, 03 medical and health sciences, Feces, 0302 clinical medicine, Immunology and Microbiology(all), medicine, Humans, 030212 general & internal medicine, Seroconversion, Viral shedding, Immunity, Mucosal, Shedding, Bangladesh, General Veterinary, General Immunology and Microbiology, business.industry, Poliovirus, Public Health, Environmental and Occupational Health, Infant, social sciences, medicine.disease, veterinary(all), Poliomyelitis, Virus Shedding, Vaccination, Regimen, Poliovirus Vaccine, Inactivated, Infectious Diseases, Immunology, Inactivated Poliovirus Vaccine, Molecular Medicine, Inactivated poliovirus vaccine, Intestinal immunity, business

Abstract

Background The Polio Endgame strategy includes phased withdrawal of oral poliovirus vaccines (OPV) coordinated with introduction of inactivated poliovirus vaccine (IPV) to ensure population immunity. The impact of IPV introduction into a primary OPV series of immunizations in a developing country is uncertain. Methods Between May 2011 and November 2012, we enrolled 700 Bangladeshi infant-mother dyads from Dhaka slums into an open-label randomized controlled trial to test whether substituting an injected IPV dose for the standard Expanded Program on Immunization (EPI) fourth tOPV dose at infant age 39 weeks would reduce fecal shedding and enhance systemic immunity. The primary endpoint was mucosal immunity to poliovirus at age one year, measured by fecal excretion of any Sabin virus at five time points up to 25 days post-52 week tOPV challenge, analyzed by the intention to treat principle. Findings We randomized 350 families to the tOPV and IPV vaccination arms. Neither study arm resulted in superior intestinal protection at 52 weeks measured by the prevalence of infants shedding any of three poliovirus serotypes, but the IPV dose induced significantly higher seroprevalence and seroconversion rates. This result was identical for poliovirus detection by cell culture or RT-qPCR. The non-significant estimated culture-based shedding risk difference was −3% favoring IPV, and the two vaccination schedules were inferred to be equivalent within a 95% confidence margin of −10% to +4%. Results for shedding analyses stratified by poliovirus type were similar. Conclusions Neither of the vaccination regimens is superior to the other in enhancing intestinal immunity as measured by poliovirus shedding at 52 weeks of age and the IPV regimen provides similar intestinal immunity to the four tOPV series, although the IPV regimen strongly enhances humoral immunity. The IPV-modified regimen may be considered for vaccination programs without loss of intestinal protection.