e101 Can f 1 | Thermo Fisher Scientific (2024)

Summary

Canis familiarisallergen 1 (Can f 1) is a salivary lipocalin protein and one of the major allergens present in dog hair and dander extracts. Can f 1 is found in all homes with dogs and in one-third of homes without dogs, and approximately half of all dog-allergic individuals have IgE directed exclusively to Can f 1. Increasing sensitization to Can f 1 is strongly associated with increasing severity and persistence of asthma symptoms in children and adults. In molecular diagnostics, recombinant Can f 1 is immunologically concordant with the natural allergen and can be reliably used to identify dog-allergic individuals sensitized to Can f 1.

Epidemiology

Worldwide distribution

A study of 25 dog-allergic patients showed that 52% had IgE against Can f 1, while IgE reactivity was also shown to Can f 2 (28%), an 18 kDa protein (60%), a 40 kDa protein (44%), and a 70 kDa protein (48%) which was probably serum albumin, now known as Can f 3 (1). In a study of 75 patients with clinical type I allergy against dogs, sera from 96% of subjects showed IgE antibodies reactive with Can f 1 and Can f 2 from hair/dander extract (2). Several studies have demonstrated that approximately half of dog-allergic individuals have IgE directed exclusively to Can f 1 (3, 4).

Can f 1 particles can remain airborne for comparatively long periods of time with minimal disturbance, and due to their small particle size can be inhaled more easily than larger particles such as mite feces or pollen grains (5). Can f 1 is found in all homes with dogs, and in one-third of homes without dogs (5).

Environmental Characteristics

Source and tissue

Can f 1 is secreted from sebaceous glands and found in hair, dander and saliva, but not in skin, salivary gland, serum or liver extracts (2, 5, 6).

Clinical Relevance

Disease severity

IgE levels against lipocalins such as Can f 1 correlate with the severity of asthma (7, 8), and sensitization to Can f 1 in childhood was significantly associated with symptoms to dog at age 16 years (9). Progression of allergic sensitization over time has been shown to involve IgE recognition of an increasing number of components from the sensitizing allergen source, forming the basis for the concept of molecular spreading, in which sensitization to a greater number of components from the same allergen source correlates with disease severity (10). Accordingly, increased bronchial inflammation in severe asthmatics is associated with multi-sensitization towards lipocalin (including Can f 1), kallikrein and secretoglobin components (11).

Simpsonet al.investigated the relationship between sensitization to groups of specific allergen components and disease, including asthma, in children aged 11 years (12). Asthma and decreased lung function were most strongly associated with sensitization to a group of 27 components that included Can f 1, Can f 2 and Can f 3 (odds ratio 8.20; 95% CI, 3.49–19.24; p<0.001) and lower FEV1(p<0.001) (12).

Sensitization to Can f 1 was strongly associated with asthma in a population-based study of 19 year olds (13). In this study, high-titer IgE antibodies to cat and dog allergens were also strongly associated with the diagnosis, severity, and persistence of asthma (13). Similar findings have been reported for children aged 13–14 years (14).

A large cross-sectional and longitudinal population-based study demonstrated that sensitization to Can f 1 in childhood was strongly associated with symptoms to dog at age 16 years (9). Additionally, polysensitization to three or more allergen molecules from dog was a better longitudinal predictor of r dog symptoms than results of IgE tests with dog allergen extracts, respectively (9). Similar findings were reported in a large population-based study of adults aged 16–75 years, where the authors concluded sensitization to furry animal allergen components is an important predictor of asthma, rhinitis, and markers of asthma severity with increased blood eosinophils, fractional exhaled nitric oxide (FeNO), and airway hyperreactivity (15).

Molecular Aspects

Allergenic Molecules

Allergenic lipocalins have been especially identified in furry animals, and four of the seven currently-identified dog allergens are lipocalins (Can f 1, Can f2, Can f 4 and Can f 6) (5, 7). Humans mutually exchange innate immune molecules such as lipocalins with their domestic animals via skin shedding and secretions (7). Lipocalins comprise an important family of proteins that dominate the respiratory mammalian allergens and usually carry lipids (or other hydrophobic/amphiphilic compounds) within a large calyx-like cavity formed by a characteristic molecular β-barrel fold (7). Ligand specificity of lipocalins is regulated by amino acid residues that line their binding pocket (7).

Can f 1 was originally named Ag13 and shown to be identical to an allergen named Ag8 (4). Can f 1 has a molecular weight ranging from 22 kDa by HPLC-gel filtration to 25 kDa on SDS-PAGE, with an additional band at 18 kDa (4).

Cross-reactivity

All dog-sensitized patients with IgE antibodies to Can f 2 also reacted to Can f 1 (5). Can f 1 and Fel d 7 (a lipocalin allergen found in cats) share 62% sequence identity, and cross-reactivity between these proteins seems likely (5).

Diagnostic Relevance

In vitro Diagnosis

Recombinant Can f 1 (rCan f 1) is immunologically concordant with the natural allergen Can f 1 and exhibits comparable antibody-binding capacities (1). A study of 25 dog-allergic patients showed that 52% had IgE against Can f 1 (1). While rCan f 1 can be reliably used to identify dog-allergic individuals sensitized to Can f 1, sensitivity for detecting dog allergy increases if multiple allergen candidates are assayed (1). Sensitization to Can f 1, Can f 2, Can f 3 and Can f 5 identifies less than half of those with IgE to dog (12).

Compiled By

Author:RubyDuke Communications

Reviewer: Dr. Magnus Borres

Last reviewed: December 2020