Milk Allergy Clinical Trial
Official title:
A Prospective Randomized Controlled Trial to Evaluate the Effect of Infant Formula on the Resolution of Cow's Milk Allergy of Infancy
Primary Endpoint
-The percentage of subjects who develop tolerance to cow's milk protein by 12 months post
randomization to study formula.
Secondary Endpoints
- Tolerance
- The transcriptional profile of milk-specific T cells by clinical outcome.
- Growth and Weight Velocity
- Stool Consistency and Frequency
- The estimated frequency of milk-specific T cells by clinical outcome.
- The TCR diversity of milk-specific T cells by clinical outcome.
- The milk allergen component-specific IgE, IgG4 and IgA by clinical outcome.
- Safety
- The rate of reported adverse events by treatment group.
Cow's Milk Allergy (CMA) is prevalent and most often presents during infancy. Disease
manifestations vary through a range of immediate and delayed inflammatory responses to milk
protein from anaphylaxis to enterocolitis. The natural history is also highly variable; most
children will achieve clinical tolerance early in life, while a minority will have disease
persisting to adulthood for reasons that are not known. Most presentations are mild and are
managed by restriction or reduction of immunologically intact milk protein with
reintroduction sometime after a year of age; however, there are data to suggest that some
level of antigenic stimulation may be beneficial. Furthermore, recent data suggest that oral
probiotic exposure may also promote tolerance, though the kinetics of tolerance acquisition,
the interaction between these two factors (probiotics and milk antigen exposure) and their
relationship to regulatory T cell responses are all poorly defined. Therefore, there is an
unmet need to identify dietary interventions, along with corresponding immune responses, that
favor the promotion of tolerance.
A major objective will be to measure the effect probiotics have on the development of
tolerance to milk antigen over time. By following these infants during the first year of
life, and repeatedly collecting blood and stool samples from them, we will be poised to
analyze their stool microbiome signatures, and we will estimate the frequency, phenotype and
TCR diversity of milk-specific T cells over time. By repeatedly challenging them with more
immunologically intact milk protein, we will better define the kinetics of CMA resolution and
its association to these variables. This information is likely to further elucidate CMA
disease mechanisms and identify possible biomarkers of disease resolution versus persistence.
It will be directly useful for evaluating the efficacy of probiotics and hydrolyzed formula
for promoting milk tolerance.
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