TINO: T Cells in the Nose of Older Adults

Recruiting

• Conditions: Respiratory Tract Infections; Aging

• Registration Number: NCT06039527
• Lead Sponsor: Leiden University Medical Center

Brief Summary

Rationale: Individuals with advanced age are at a progressively increasing risk of acquiring lower respiratory tract infections. Besides calendar age, the degree of frailty also associates with increased susceptibility to pneumonia requiring hospitalization. How alterations in the mucosal immune system with advanced age predispose to infections remains unclear as access to relevant tissue samples is limited. With minimally-invasive nasal sampling methods, it was recently observed that in vital older adults, both CD4+ T cells and CD8+ T cells are selectively lost from the nasal mucosa. However, the exact phenotype, underlying mechanisms, key molecules and consequences of this have not yet been investigated.

Objective:

Elucidate the mechanisms underlying the loss of nasal T cells and characterize in depth the differences of T cells in young and older adults and associate this loss with susceptibility to infections.

Study design: Prospective cohort study

Study population: Participants will be recruited from 3 groups:

* healthy young adults (18-30 years, n=50)

* vital older adults (\>65 years, n=60)

* frail elderly (\>65 years, n=60). This group includes individuals without a history of recurrent respiratory infections or with \>2 self-reported episodes of respiratory infection in the past year.

Main study parameters/endpoints: Frequency of nasal CD8+ T cells in young adults and frail older adults.

Secondary study parameters/endpoints:

* Phenotype (subsets, activation status), functionality, transcriptomic state, clonality and frequency of nasal and blood T cell populations

* Stability of T cells and other immune parameters, as described for main study parameter, during a second sample after 3 months.

* Analysis of other immune populations as for main study parameter

* Concentration of nasal and systemic factors (e.g. cytokines and metabolites) and their association with T cells and other immune populations

* Respiratory tract microbiota profiles and presence of asymptomatic viral infections and their association with T cells and other immune parameters

* Chronological and biological age, sex, and other immunologically relevant parameters with T cell populations and other immune parameters

* Alteration of T cell phenotype, during and following respiratory tract infections. Levels of antigen-specific T cells and other immune parameters in nose and blood post infection.

Detailed Description

Not available

Study Timeline

• Study Start: 2021-01-24
• Study First Submitted: 2023-09-01
• Study First Submitted QC: 2023-09-08
• Study First Posted: 2023-09-15
• Status Verified: 2024-06
• Last Update Submitted: 2024-06-17
• Last Update Posted: 2024-06-18
• Primary Completion: 2025-05
• Study Completion: 2025-05

Recruitment & Eligibility

• Status: RECRUITING
• Sex: All
• Target Recruitment: 170

Inclusion Criteria

•Adults able and willing to provide informed consent.

Specific inclusion criteria per group:

• Young adults aged 18-30 years old
• Healthy elderly aged >65 years old
• Frail elderly >65 years old
• Clinical Frailty score healthy elderly 1-3
• Clinical Frailty score frail elderly >3
• Self-reported respiratory tract infection in previous year healthy elderly 0-1
• Self-reported respiratory tract infection in previous year frail elderly 0-1 or >1

Exclusion Criteria

• Incompetence to provide informed consent prior or during study
• Current smoker or >40 pack year history
• History of severe nose bleedings
• Diagnosed with asthma, COPD or chronic rhinosinusitis
• Use of inhalation corticosteroids or antibiotics in the past 6 weeks
• Current use of anti-coagulants (to prevent nosebleeds). Platelet inhibitors like acetylsalicylzuur (Ascal) are allowed.
• Respiratory tract infection or common cold in the past 2 weeks
• Immunocompromised individuals (with primary immune deficiency or secondary immune deficiency)
• Life expectancy <28 days in the opinion of study physician
• Vaccination in the 2 months prior to study start. A potential subject that is only excluded from participation based on a recent vaccination will be asked to re-participate 2 months post vaccination.

Study & Design

• Study Type: OBSERVATIONAL
• Study Design: Not specified

Primary Outcome Measures

Name	Time	Method
Frequency of nasal CD8+ T cells in young adults and frail older adults.	baseline sample or month 3 sample	CD8 T cells relative to nasal epithelial cells (ratio)

Secondary Outcome Measures

Name	Time	Method
Effect of sex on aging effects of nasal immune populations	baseline sample or month 3 sample	ratio to nasal epithelial cells
Effect of sex on aging effects of blood immune populations	baseline sample or month 3 sample	percentage of CD45+ cells
Clonality of nasal and blood T cell populations in young adults, healthy older adults and frail older adults that suffer from recurrent respiratory tract infections or not.	baseline sample or month 3 sample	Number and proportion of TCR clones
Concentration of nasal and systemic metabolitesother immune populations	baseline sample or month 3 sample	concentrations
Respiratory tract microbiota profiles and their association with T cells and other immune parameters	baseline sample or month 3 sample	microbiota abundance (total sum scaling)
Presence of asymptomatic viral infections and their association with T cells and other immune parameters	baseline sample or month 3 sample	viral of loads (Ct)
Stability of nasal immune populations, during a second sample after 3 months.	baseline sample versus month 3 sample	immune cell populations relative to nasal epithelial cells (ratio)
Comparison of peripheral immune cell populations between young adults, vital and frail elderly	baseline sample or month 3 sample	percentage of total CD45+ cells
Concentration of nasal and systemic cytokines	baseline sample or month 3 sample	concentrations
Frequencies of antigen-specific T cells in nose post infection.	symptom onset and 1, 3 and 5 months later	antigen-specific T cells as percentage of T cells
Frequencies of antigen-specific T cells in blood post infection.	symptom onset and 1, 3 and 5 months later	antigen-specific T cells as percentage of T cells
Phenotype of nasal and blood T cell populations in young adults, healthy older adults and frail older adults that suffer from recurrent respiratory tract infections or not.	baseline sample or month 3 sample	percentage of T cells and T cell subsets
Functionality of nasal and blood T cell populations in young adults, healthy older adults and frail older adults that suffer from recurrent respiratory tract infections or not.	baseline sample or month 3 sample	percentage of T cells responding to in vitro stimulations
Transcriptomic cluster composition of nasal and blood T cell populations in young adults, healthy older adults and frail older adults that suffer from recurrent respiratory tract infections or not, as frequency of T cell subsets.	baseline sample or month 3 sample	T cell clusters based on gene expression patterns
Stability of nasal T cells, as described for main study parameter, during a second sample after 3 months.	baseline sample versus month 3 sample	CD8 T cells relative to nasal epithelial cells (ratio)
Comparison of nasal immune cell populations between young adults, vital and frail elderly	baseline sample or month 3 sample	ratio to epithelial cells

Trial Locations

Locations (1)

Leiden University Medical Center; 🇳🇱 Leiden, Zuid Holland, Netherlands