This clinical study will investigate the relationships between sequential respiratory viral infections, patterns of intestinal and respiratory bacterial colonization, and adaptive cellular immune phenotypes which are associated with increased susceptibility to respiratory infections and long term respiratory morbidity in preterm and full term infants. This is a prospective, cohort study, enrolling at a single center via two sites (URMC and URMC-affiliated Highland Hospital and Rochester General Hospital). Enrollment will be accomplished in approximately 15 - 36 months. The study will enroll 280 subjects, 150 pre-term and 130 full-term.
This clinical study will investigate the relationships between sequential respiratory viral infections, patterns of intestinal and respiratory bacterial colonization, and adaptive cellular immune phenotypes which are associated with increased susceptibility to respiratory infections and long term respiratory morbidity in preterm and full term infants. This is a prospective, cohort study, enrolling at a single center via two sites (URMC and URMC-affiliated Highland Hospital and Rochester General Hospital). Enrollment will be accomplished in approximately 15 - 36 months. The study will enroll 280 subjects, 150 pre-term and 130 full-term. This protocol does not study an agent or intervention. However, the bronchodilator, albuterol, a beta 2 agonist, will be administered as part of the Respiratory Inductive Plethysmography (RIP) pulmonary function assessments. All infants will remain in the study up to 3 years plus 17 weeks, depending on gestational age at birth. The full-term infants are expected to be typically developing newborns and generally healthy. Enrolled newborns will have a sample of cord blood (CB) for evaluation of lymphocyte phenotype and baseline neutralizing antibody titers. Maternal saliva samples will be collected to test exposure to environmental tobacco smoke. A nose, throat and rectal swab will be obtained for the assessment of the respiratory and gut microbiome and testing for known respiratory pathogens and pathogen discovery. Prior to hospital discharge, infants will have an evaluation of lymphocyte phenotype and function, and will undergo a respiratory assessment via RIP prior to and after a bronchodilator. Co-morbidities, familial and environmental risk factors for atopy, asthma and respiratory symptoms will be assessed. Following hospital discharge, all babies (full-term and former preterm infants) will be followed longitudinally through 3 years CGA as outpatients. During the first year of follow-up, all infants will have rectal and nose, throat swabs obtained monthly. Screening for symptomatic respiratory dysfunction and illnesses will also occur during the time of follow-up as per schedule.
Study Type
Respiratory Inductive Plethysmography (RIP) will be used to document thoracoabdominal motion, relative minute ventilation, and apnea during the minimally invasive respiratory assessments (NIRAs). Both Full and Preterm Infants will undergo a respiratory assessment via RIP prior to and after a bronchodilator (albuterol)
University of Rochester Medical Center - Strong Memorial Hospital - Infectious Diseases
Rochester, New York, United States
Calculate presence of at/near term gestation cellular immune response to mitogen and antigen specific responses to > /=1 viral pathogens isolated over 1st 2yrs CGA via lymphocyte assessment
Time frame: 2 years CGA
Degree of adaptive immune system maturation utilizing flow cytometric analysis of lymphocytes in blood
Assess blood lymphocyte subsets at birth (cord blood), discharge and at 1 year of age
Time frame: From 41 weeks gestation through 3 years CGA
Degree of immune system maturation utilizing flow cytometric analysis of lymphocytes in umbilical cord blood and peripheral blood
Time frame: From 41 weeks gestation through 3 years CGA
Etiology of symptomatic viral respiratory infections as assessed by TLDA PCR Assays of biospecimens
Time frame: 2 years CGA
Number of respiratory tract symptomatic and asymptomatic viral infections weekly.
Time frame: 41weeks gestation
Number of symptomatic viral respiratory infections
Time frame: 2 years CGA
Occurrence of respiratory tract viral infections (asymptomatic and symptomatic)
Time frame: From 37- 41 weeks gestation, through the first 1 and 2 years CGA, respectively
Patterns of respiratory and gut bacterial microbiome as they develop weekly
Time frame: 41 weeks gestation
Pulmonary function via Respiratory Inductive Plethysmography (RIP) with Bronchodilator Response (BDR)
Time frame: 41 weeks gestation
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OBSERVATIONAL
Enrollment
267
Rate of adaptive immune system maturation utilizing flow cytometric analysis of lymphocytes in blood
Time frame: From 37- 41 weeks, through the first 1 and 3 years CGA
Rate of immune system maturation utilizing flow cytometric analysis of lymphocytes in umbilical cord blood and peripheral blood
Time frame: 41 weeks gestation
Severity of illness due to viral respiratory tract infections
Time frame: 2 years CGA
Severity of respiratory tract viral infections (asymptomatic and symptomatic) as assessed by the COAST Respiratory Symptom Scale.
Time frame: 2 years CGA
Viral load of respiratory pathogens in the nasopharynx of infants with symptomatic RTIs
Time frame: 2 years CGA
Patterns of respiratory and gut bacterial microbiome as they change monthly from hospital discharge at term or near term gestation
Time frame: Through the first 1 year CGA
Presence of cord blood antigen-neutralizing antibodies correlates with the presence of specific antigen responses in lymphocytes
Time frame: At term or near term gestation
Pulmonary function via RIP with BDR
Time frame: At 1 year CGA and 3 years CGA
Titers of neutralizing antibodies in cord blood to isolated viral pathogens
Time frame: Through the first 2 years CGA