Mouse epithelium
Summary
The house mouse is found everywhere in the world as a commensal of humans. Its allergens are present in workplaces, especially in mouse-handling laboratories, homes, and community settings, such as schools, where they are the most commonly detected allergen. Mouse urine is the main source of allergens, which become airborne on dust particles as the urine dries in the environment, but they are also found in mouse saliva, and on hair and epithelial fragments. Exposure to mouse allergens has been associated with asthma in adults and children. Laboratory animal workers are at risk of sensitization, and up to one-third will have symptomatic asthma. In inner-city children with asthma, risk factors for sensitization to mouse include allergen exposure, a history of atopy, and sensitization to cockroach allergen. One study showed that in a city preschool population, one-quarter of children had evidence of IgE sensitization to mouse. Exposure to greater than 0.5µg mouse allergen in home dust samples was associated with more symptomatic days, cough without a cold, exercise-related symptoms and use of short-acting ß-agonists than in children with either lower exposure or a non-sensitized state. Risk of hospitalization was greatly increased, while risk of an unscheduled physician or emergency department visit for asthma also increased two- to threefold in the sensitized and exposed children, compared with the less-exposed or non-sensitized children. Other symptoms of mouse allergy include rhinoconjunctivitis, eczema, and urticaria. For asthma patients with IgE sensitization to mouse, reduction of mouse allergen in the environment is critical, and implementation of comprehensive pest management strategies are effective in achieving this. The major mouse allergen is the pheromone-binding protein, Mus m 1. As a lipocalin, Mus m 1 demonstrates a degree of cross-reactivity with those of other animals, such as horse, dog, cow, and cockroach. In most rodent-sensitized patients, rat and mouse sensitization is coexistent.
Epidemiology
Worldwide distribution
Native to the Indian subcontinent, the house mouse has now colonized all regions of the world. It survives in all climates and may be found indoors and out.
Although mice can be kept as pets, they are normally considered to be pests on account of their ability to establish themselves in buildings such as homes and schools. Their chewing can cause structural damage and their feces and continual dribble of urine lead to contamination.
Risk factors
Rodent contact in general has long been identified as a risk factor for IgE sensitization to rodents. The exact nature of the relationship between exposure and the risk of becoming sensitized has been explored in greater depth in recent studies.
Laboratory animal workers are at risk of sensitization and up to one-third will have symptomatic asthma. An atopic background and the intensity of exposure are further risk factors.
The National Cooperative Inner-City Asthma Study demonstrated that an increase of Mouse skin test sensitivity was associated with a Mus m 1 level of greater than 1.6 µg/g.
One study investigating the relationship between exposure and risk of IgE sensitization showed that prevalence rates of skin test sensitivity to mouse in a population of suburban children increased as exposure to mouse allergens in bedroom dust increased.
In an inner-city population with mouse allergens 100- to 1000-fold higher than those in the suburban population, an increasing risk of sensitization throughout the first three quartiles of exposure was demonstrated. At the highest levels of exposure, however, sensitization was attenuated, suggesting that at very high levels of exposure, some measure of protection may be conveyed.
Among inner-city children with asthma, allergen exposure, a history of atopy, and sensitization to cockroach allergen have been shown to be significant risk factors for mouse sensitization.
Pediatric issues
The School Inner-City Asthma Study demonstrated that, not only are mouse allergens the most commonly detected allergen in schools, but levels are significantly higher than in homes.
Route Of Exposure
Main
Early studies examining mouse allergen exposure in occupational settings sampled airborne particles and analyzed their size distribution and density in the environment. Mouse allergen is carried predominantly on particles measuring less than 10μm. At this size, particles may be easily deposited in airways.
Clinical Relevance
Asthma
In occupational settings, the association between laboratory animal allergy or occupational asthma and rodent exposure is well documented. Symptoms may include rhinoconjunctivitis, eczema, urticaria, and asthma. Cases are often identified using disease surveillance methods, and exposure reduction may be achieved by the use of respiratory protection or by reassignment to a job where exposure is minimized. Medication may also be required.
It is estimated that between 11% and 44% of people working with laboratory animals will develop allergies related to their occupation. Of those, between 4% and 33% will go on to develop occupational asthma or other lower airway symptoms.
The clinical relevance of mouse allergen exposure and sensitization outside of the laboratory setting has also been demonstrated. Exposure to mouse allergen has been associated with a diagnosis of asthma in adult populations. Furthermore, mouse allergen sensitization has been associated with more severe asthma in women. Sensitization to mouse allergen alone has been shown to be a risk factor for young children with allergic airway disease. A birth cohort study in New York City showed that mouse allergen-sensitized, two- to three-year-old children were at greater risk than were non-sensitized children, of developing rhinitis, wheeze and eczema.
Worse asthma outcomes have been associated with the combination of mouse sensitization with exposure, as opposed to just exposure or sensitization alone. Two recent studies measured morbidity in mouse-sensitized inner-city children who were exposed to high levels of mouse allergen. One-quarter of children in a Baltimore City preschool population demonstrated evidence of IgE sensitization to mouse. Bedroom settled dust samples were analyzed and those children exposed to greater than 0.5 µg/g mouse allergen had more symptomatic days, cough without a cold, exercise-related symptoms and use of short-acting ß-agonists, than either children who were non-sensitized or those who were exposed to lower exposure levels. Risk of hospitalization was greatly increased, while risk of an unscheduled physician or emergency department visit for asthma also increased two- to threefold in the sensitized and exposed children, compared with the less-exposed or non-sensitized children.
Allergic rhinitis
In occupational settings, the association between laboratory animal allergy or occupational asthma and rodent exposure is well documented. It is estimated that between 11% and 44% of people working with laboratory animals will develop allergies related to their occupation. Symptoms may include rhinoconjunctivitis, eczema, urticaria, and asthma. Cases are often identified using disease surveillance methods, and exposure reduction may be achieved by the use of respiratory protection or by reassignment to a job where exposure is minimized. Medication may also be required.
The clinical relevance of mouse allergen exposure and sensitization outside of the laboratory setting has also been demonstrated. Sensitization to mouse allergen alone has been shown to be a risk factor for young children with allergic airway disease. A birth cohort study in New York City showed that mouse allergen-sensitized, two- to three-year-old children were at greater risk than were non-sensitized children, of developing rhinitis, wheeze and eczema.
Atopic dermatitis
In occupational settings, the association between laboratory animal allergy or occupational asthma and rodent exposure is well documented. It is estimated that between 11% and 44% of people working with laboratory animals will develop allergies related to their occupation. Symptoms may include rhinoconjunctivitis, eczema, urticaria, and asthma. Cases are often identified using disease surveillance methods, and exposure reduction may be achieved by the use of respiratory protection or by reassignment to a job where exposure is minimized. Medication may also be required.
Sensitization to mouse allergen alone has been shown to be a risk factor for young children with allergic airway disease. A birth cohort study in New York City showed that mouse allergen-sensitized, two- to three-year-old children were at greater risk than were non-sensitized children, of developing rhinitis, wheeze and eczema.
Diagnostics
Environmental source
In occupational settings, mouse ‘load’, a function of mouse density and room ventilation, has been shown to be directly related to higher airborne mouse allergen levels.
In a home setting, it is generally not possible for the clinician to obtain settled dust samples. However, collection of a history, including reports of recent mouse sightings, can be a strong predictor of higher levels of mouse allergen exposure. In one study, parent reports of having seen mice had a 90% positive predictive value for mouse allergen levels greater than 0.5 μg/g. The absence of mouse sightings, however, cannot be relied upon to rule out clinically relevant mouse exposure.
Main methods
Vacuum pumps are used to collect samples by drawing air through a filter. The captured airborne particles are analyzed for Mus m 1 content.
Measures
Mus m 1 exposure is expressed as mass per volume of air, normally using units ng/. It is derived from a known flow rate of the sampling pump (in liters per minute) and duration of sampling time (in minutes).
Prevention And Therapy
Prevention strategies
For asthma patients demonstrating evidence of IgE sensitization of mouse, environmental interventions that will reduce mouse allergen levels in the home should be recommended. Integrated pest management involves using multiple strategies that will reduce food sources for mice, eliminate them from the home, and prevent them from regaining access. Examples of such strategies include clearing away exposed food and storing foods in containers through which mice cannot chew, setting traps and repairing structural damage, such as cracks and holes, in the home. One pilot study demonstrated a 75% reduction in mouse allergen levels in the home.
Cross-Reactivity
Practically all respiratory allergens originating from animals, including mouse, belong to the lipocalin family of proteins. The major allergens of horse, cow, dog, mouse and cockroach are all examples of these, along with beta-lactoglobulin, from cow’s milk. Thus, there may be a certain degree of cross-reactivity.
The major rat allergen is Rat n 1. Excreted in the urine, Rat n 1 is also a lipocalin and a pheromone-binding protein. Rat n 1 shares 60-80% homology with Mus m 1, which means that in most, if not all, rodent-sensitized patients, rat and mouse sensitization is coexistent.
References
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