Primary sensitization to inhalant allergens

Claudia Macaubas(The Kids Research Institute Australia), Susan L. Prescott(The Kids Research Institute Australia), T. Venaille(The Kids Research Institute Australia), Barbara J. Holt(The Kids Research Institute Australia), Troy B. Smallacombe(The Kids Research Institute Australia), Peter D. Sly(The Kids Research Institute Australia), Patrick G. Holt(The Kids Research Institute Australia)
Pediatric Allergy and Immunology
October 1, 2000
Cited by 21Open Access
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Abstract

The neonatal T-cell system is capable of responding to allergens at birth, indicating the occurrence of prenatal sensitization, and the cytokine profile of these responses is skewed towards the Th-2 type. This response is further modified by postnatal exposure to different types of allergens. In relation to inhalant allergen (employed by HDM) the low level fetal Th-2 responses in non-atopics appear to be down-regulated rapidly after birth, parallel to an increase in allergen-specific IFN-gamma production. In contrast, atopics appear to consolidate their initial Th-2 responses, and around the age of 6 exhibit a cytokine response profile similar to the adult pattern. A pre-existing deficiency in IFN-gamma production may be one of the key factors determining the postnatal persistence of Th-2 responses in atopics.


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