Atopy


Atopy is the tendency to produce an exaggerated IgE immune response to otherwise harmless environmental substances, while an allergic disease can be defined as the clinical manifestation of this inappropriate IgE immune response.
Atopy may have a hereditary component, although contact with the allergen or irritant must occur before the hypersensitivity reaction can develop. Maternal psychological trauma in utero may also be a strong indicator for development of atopy.
The term atopy was coined by Coca and Cooke in 1923. Many physicians and scientists use the term "atopy" for any IgE-mediated reaction, but many pediatricians reserve the word "atopy" for a genetically mediated predisposition to an excessive IgE reaction. The term is from Greek ἀτοπία meaning "the state of being out of place", "absurdity".

Signs and symptoms

Atopic sensitization is considered IgE positivity or prick test positivity to any common food or air born allergen. Atopic conditions are considered: atopic dermatitis, allergic rhinitis, allergic asthma. The likelihood of having asthma, rhinitis and atopic dermatitis together is 10 times higher than could be expected by chance. Atopy is more common among individuals with a number of different conditions, such as eosinophilic esophagitis, non-celiac gluten sensitivity.
Allergic reactions can range from sneezing and rhinorrhoea to anaphylaxis and even death.

Pathophysiology

In an allergic reaction, initial exposure to an otherwise harmless exogenous substance triggers the production of specific IgE antibodies by activated B cells. These IgE antibodies bind to the surface of mast cells via high-affinity IgE receptors, a step that is not itself associated with a clinical response. However, upon re-exposure, the allergen binds to membrane-bound IgE which activates the mast cells, releasing a variety of mediators. This type I hypersensitivity reaction is the basis of the symptoms of allergic reactions, which range from sneezing and rhinorrhoea to anaphylaxis. Allergens can be a number of different substances, for example pollen, dander, dust mites, foods.

Causes

Atopic reactions are caused by localized hypersensitivity reactions to an allergen. Atopy appears to show a strong hereditary component. One study concludes that the risk of developing atopic dermatitis or atopy in general "increases by a factor of two with each first-degree family member already suffering from atopy". As well, maternal stress and perinatal programming is increasingly understood as a root cause of atopy, finding that "...trauma may be a particularly robust potentiator of the cascade of biological events that increase vulnerability to atopy and may help explain the increased risk found in low-income urban populations.”
Environmental factors are also thought to play a role in the development of atopy, and the 'hygiene hypothesis' is one of the models that may explain the steep rise in the incidence of atopic diseases, though this hypothesis is incomplete and in some cases, contradictory to findings. This hypothesis proposes that excess 'cleanliness' in an infant's or child's environment can lead to a decline in the number of infectious stimuli that are necessary for the proper development of the immune system. The decrease in exposure to infectious stimuli may result in an imbalance between the infectious-response elements and the allergic-response elements within the immune system.
Some studies also suggest that the maternal diet during pregnancy may be a causal factor in atopic diseases in offspring, suggesting that consumption of antioxidants, certain lipids, and/or a Mediterranean diet may help to prevent atopic diseases.
An epidemiological study, "Measles and Atopy,in Guinea-Bissau, published by NCBI defined a 2.8% higher risk of developing an atopic allergy after receiving a Measles vaccine, than of those who had Meastudy titles
The multicenter PARSIFAL study in 2006, involving 6630 children age 5 to 13 in 5 European countries, suggested that reduced use of antibiotics and antipyretics is associated with a reduced risk of allergic disease in children.

Genetics

There is a strong genetic predisposition toward atopic allergies, especially on the maternal side. Because of the strong familial evidence, investigators have tried to map susceptibility genes for atopy. Genes for atopy tend to be involved in allergic responses or other components of the immune system. C11orf30 seems to be the most relevant for atopy as it may increase susceptibility to poly-sensitization.

''Staphylococcus aureus''

Bleach baths provide temporary control of eczema. Ciprofloxacin is an allergen that may cause contact dermatitis, symptoms of which are indistinguishable from eczema. Filaggrin mutations are associated with atopic eczema and may contribute to the excessive dryness of the skin and the loss of the barrier function of normal skin. It may be possible that the filaggrin mutations and the loss of the normal skin barrier expose crevices that make it possible for Staphylococcus aureus to colonize the skin. Atopic eczema is often associated with genetic defects in genes that control allergic responses. Thus, some investigators have proposed that atopic eczema is an allergic response to increased Staphylococcus aureus colonization of the skin. A hallmark indicator of atopic eczema is a positive “wheal-and-flare” reaction to a skin test of S. aureus antigens. In addition, several studies have documented that an IgE-mediated response to S. aureus is present in people with atopic eczema.

Changes in prevalence

In adults, the prevalence of IgE sensitization to allergens from house dust mite and cat, but not grass, seem to decrease over time as people age. However, the biological reasons for these changes are not fully understood.

Treatments

The treatment of atopic disorders depends on the organ involved. It can vary from local treatment options, often topical corticosteroids, to systemic treatment options with oral corticosteroids, biological treatments or allergen immunotherapy. An anaphylactic reaction on the other hand is treated with adrenaline, given as an intramuscular injection.