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Project Details

Viral Diversity and Pathogenicity in Mucosal Respiratory and Gastrointestinal Disease

Parent Project Number3U19AI144297-03S1

Sub-Project ID6259

Contact PI/Project LeaderESTES, MARY KOLB

Awardee OrganizationBAYLOR COLLEGE OF MEDICINE

Description

Abstract Text

PROJECT SUMMARY Human norovirus (HuNoV), a NIAID Category B pathogen, is the leading cause of acute gastroenteritis globally, and respiratory syncytial virus (RSV), a Category C pathogen, is the major global respiratory pathogen of children. HuNoV infections result in significant acute morbidity in all age groups, chronic disease in immunocompromised cancer and transplant patients, and death in young children and older adults. RSV is the leading cause of lower respiratory tract morbidity and mortality among children, and contributes significantly to illness and death in the immunocompromised, those with co-morbidities and older adults. The burden of disease and economic impact of these mucosal pathogens have stimulated extensive efforts for vaccine development. With vaccines anticipated in the next 5 years for both pathogens, this pre-licensure window, together with our recent development of a successful cultivation system for HuNoVs using stem cell-derived human intestinal organoids (HIOs) and the recent description of RSV infections in human lung organoids (HLOs) provide an ideal window to apply analytical genomics and functional studies in relevant human culture systems to address key questions about HuNoV and RSV diversity, evolution and virulence. Our proposed studies utilize carefully selected clinical specimens covering the spectrum of HuNoV and RSV illness, including: (i) acute gastroenteritis in immunocompetent children from two populations (USA and Hong Kong), (ii) acute respiratory infections in children in the CDC sponsored New Vaccine Surveillance Network, (iii) well-controlled volunteer HuNoV challenge studies, (iv) transplant and immunocompromised patients with chronic HuNoV infection or acute RSV infection, (v) the first randomized double-blind clinical trial of nitazoxanide (NTZ) for treatment of chronic HuNoV in transplant recipients, and (vi) women and infants in the first phase III trial of an RSV-F vaccine (Novavax) in healthy pregnant women for preventing disease in their infants. In addition to pathogen-targeted sequencing, we will evaluate the role of the ecological niche in viral pathogenesis using high throughput, integrated sequencing approaches to profile the bacteriome and virome of clinical samples. Full-length (FL) genomic analyses of HuNoV and functional studies in HIEs will provide critical information on virus diversity in different populations and over time in diverse hosts, the presence of intragenotypic and intergenotypic recombinants, and the appearance of mutants with treatment resistance to NTZ. FL genomic analyses of RSV and functional studies in HLOs and other cell lines will establish specific viral signatures of RSV disease severity, enable understanding the effects of immune pressure and immunotherapeutics on the viral genome including antigenic site specific motifs, and changes in B and T cell epitopes. The scientific community will benefit immensely from large databases of FL genomes for HuNoV and RSV, and functional studies in novel human cultures that comprehensively address viral genomic signatures, microbial ecology and host responses before vaccine introduction. Identifying biomarkers, viral and host targets will guide treatment and development of therapeutics.

Public Health Relevance Statement

Data not available.

NIH Spending Category

No NIH Spending Category available.

Project Terms

AcuteAcute respiratory infectionAddressAntigensAppearanceB-LymphocytesBiologicalBiological MarkersCancer PatientCategoriesCategory B pathogenCategory C pathogenCell Culture TechniquesCell LineCellsCenters for Disease Control and Prevention (U.S.)Cessation of lifeCharacteristicsChildChronicChronic DiseaseClinicalClinical TrialsCommunitiesDatabasesDevelopmentDiagnosisDiseaseDouble-Blind MethodEcologyElderlyEpidemicEpidemiologyEpithelialEvaluationEvolutionFrequenciesGastroenteritisGastrointestinal DiseasesGene Expression ProfileGeneticGenetic RecombinationGenetic TranscriptionGenomeGenomicsHong KongHumanHuman VolunteersImmuneImmune responseImmunocompetentImmunocompromised HostImmunologicsImmunotherapeutic agentIn VitroIndividualInfantInfectionIntegration Host FactorsIntestinesKnowledgeLeadLengthLicensureLower respiratory tract structureLungLung diseasesMetagenomicsMorbidity - disease rateMucous MembraneNational Institute of Allergy and Infectious DiseaseNorovirusOrganoidsPathogenesisPathogenicityPatientsPerformancePhysiologicalPluripotent Stem CellsPopulationPredispositionPregnant WomenPreventionRandomizedRecombinantsRespiratory MucosaRespiratory Syncytial Virus InfectionsRespiratory SystemRespiratory syncytial virusReverse Transcriptase Polymerase Chain ReactionRoleSamplingSeverity of illnessSiteSpecimenSystemT-Lymphocyte EpitopesTestingTherapeuticTimeTransplant RecipientsVaccinesViralViral GenomeViral PathogenesisVirulenceVirusVirus DiseasesVirus ReplicationWomanage groupaging populationbacteriomebaseburden of illnessclinical developmentclinically relevantcomorbidityeconomic impactepidemiologic datafallsgastrointestinalgenetic signaturegenomic datagenomic signaturehuman morbidityhuman mortalityimprovedinsightmetagenomic sequencingmicrobialmortalitymutantnitazoxanidenovelnovel vaccinespandemic diseasepathogenpatient subsetsphase III trialpreclinical developmentpressurepreventreconstitutionrespiratoryrespiratory pathogenresponsestem cellssurveillance networktargeted sequencingtherapeutic developmenttherapy developmenttherapy resistanttoolvaccine developmentviral genomicsviromevirus host interaction

Details

Contact PI/ Project Leader

Name

ESTES, MARY KOLB

Title

PROFESSOR

Contact

Other PIs

Not Applicable

Program Official

Name

BROWN, LILIANA L

Contact

Organization

Name

BAYLOR COLLEGE OF MEDICINE

City

HOUSTON

Country

UNITED STATES (US)

Department Type

Unavailable

Organization Type

Domestic Higher Education

State Code

Congressional District

Other Information

Opportunity Number

RFA-AI-18-004

Study Section

ZAI1-EC-M

Fiscal Year

2021

Award Notice Date

17-August-2021

Administering Institutes or Centers

National Institute of Allergy and Infectious Diseases

CFDA Code

DUNS Number

051113330

UEI

FXKMA43NTV21

Project Start Date

17-August-2021

Project End Date

31-March-2022

Budget Start Date

01-April-2021

Budget End Date

31-March-2022

Project Funding Information for 2021

Total Funding

$499,999

Direct Costs

$394,628

Indirect Costs

$105,371

Year	Funding IC	FY Total Cost by IC
2021	National Institute of Allergy and Infectious Diseases	$499,999

Sub Projects

No Sub Projects information available for 3U19AI144297-03S1 6259

Publications

Publications are associated with projects, but cannot be identified with any particular year of the project or fiscal year of funding. This is due to the continuous and cumulative nature of knowledge generation across the life of a project and the sometimes long and variable publishing timeline. Similarly, for multi-component projects, publications are associated with the parent core project and not with individual sub-projects.

No Publications available for 3U19AI144297-03S1 6259

Patents

No Patents information available for 3U19AI144297-03S1 6259

Outcomes

The Project Outcomes shown here are displayed verbatim as submitted by the Principal Investigator (PI) for this award. Any opinions, findings, and conclusions or recommendations expressed are those of the PI and do not necessarily reflect the views of the National Institutes of Health. NIH has not endorsed the content below.

No Outcomes available for 3U19AI144297-03S1 6259

Clinical Studies

No Clinical Studies information available for 3U19AI144297-03S1 6259

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