Chronic dermatophyte infections. I. Clinical and mycological features

Hay, Roderick J.

doi:10.1111/j.1365-2133.1982.tb00895.x

Cited by 92 publications

(57 citation statements)

References 14 publications

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“…Nucleotide and deduced amino acid sequences of recombinant Tri r 4. The NH 2 -terminal amino acid residues (positions [1][2][3][4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19] contain the conserved features of a signal peptide with a predicted cleavage site between Ala 19 and Phe 20 . Underlined regions represent amino acid sequences previously obtained for the NH 2 terminus and for six enzymatically generated peptides of natural Tri t 4.…”

Section: Methodsmentioning

confidence: 99%

Trichophyton Antigens Associated with IgE Antibodies and Delayed Type Hypersensitivity

Woodfolk¹,

Wheatley²,

Piyasena³

et al. 1998

Journal of Biological Chemistry

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The dermatophyte fungus Trichophyton exhibits unique immunologic properties by its ability to cause both immediate and delayed type hypersensitivity. An 83-kDa Trichophyton tonsurans allergen (Tri t 4) was previously shown to elicit distinct T lymphocyte cytokine profiles in vitro. The homologous protein, Tri r 4, was cloned from a Trichophyton rubrum cDNA library, and the recombinant protein was expressed in Pichia pastoris. This 726-amino acid protein contained an arrangement of catalytic triad residues characteristic of the prolyl oligopeptidase family of serine proteinases (Ser-Asp-His). In addition, a novel Trichophyton allergen, encoding 412 amino acids, was identified by its human IgE antibody-binding activity. Sequence similarity searches showed that this allergen, designated Tri r 2, contained all of the conserved residues characteristic of the class D subtilase subfamily (41-58% overall sequence identity). Forty-two percent of subjects with immediate hypersensitivity skin test reactions to a Trichophyton extract exhibited IgE antibody binding to a recombinant glutathione S-transferase fusion protein containing the carboxyl-terminal 289 amino acids of Tri r 2. Furthermore, this antigen was capable of inducing delayed type hypersensitivity skin test reactions. Our results define two distinct antigens derived from the dermatophyte Trichophyton that serve as targets for diverse immune responses in humans.Dermatophyte fungi of the genus Trichophyton colonize keratinized tissues in humans including nails, hair shafts, and the stratum corneum of the skin. Trichophyton tonsurans, Trichophyton mentagrophytes, and Trichophyton rubrum are common causes worldwide of tinea capitis, athlete's foot, and onychomycosis (infection of the nail beds) (1). An estimated 30 -70% of adults are asymptomatic carriers of these pathogens, and the incidence of symptomatic disease increases with age (2). The immune response to antigens derived from Trichophyton is unique in that both immediate hypersensitivity (IH) 1 and delayed type hypersensitivity (DTH) skin test reactions are induced. Studies suggest that the nature of the underlying immune response to Trichophyton antigens is related to the severity of dermatophytosis; IH skin tests are associated with chronic recurrent infections characterized by low-grade inflammatory lesions and the presence of IgE antibodies (Ab) (4 -7). In contrast, DTH reactions are associated with highly inflamed lesions that resolve spontaneously and a resistance to re-infection (4, 8 -13). The implication of these findings is that cellmediated immune responses to Trichophyton are more effective at eradicating infection and may confer protection. Chronic dermatophytosis has been associated with allergic disease in the respiratory tract in individuals with immediate hypersensitivity (14 -17). Furthermore, exposure to Trichophyton proteins may result in bronchial sensitization and symptomatic asthma that can be controlled with systemic antifungal therapy (7,18,19).Experimental mouse models support a role...

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Section: Methodsmentioning

confidence: 99%

Trichophyton Antigens Associated with IgE Antibodies and Delayed Type Hypersensitivity

Woodfolk¹,

Wheatley²,

Piyasena³

et al. 1998

Journal of Biological Chemistry

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“…They further obtained evi dence that type I hypersensitivity in atopic subjects antag onizes the effect of cellular immunity locally [21]. They concluded that deficient or compromised cellular immuni ty is a correlate of susceptibility to dermatophyte infec tions from a study of experimental dermatophytosis in naturally infected subjects [22], In vitro assays of T lym phocyte functions also demonstrated a deficiency of cellu lar immunity as well as a high incidence of atopy in indi viduals with chronic dermatophytosis [23][24][25], Another interesting point about the chronicity is the high incidence of palmoplantar infections [25] and that of T.rubrum infections [26]. both of which are associated with low in vitro T lymphocyte reactivity.…”

Section: Chronic Dermatophyte Infectionsmentioning

confidence: 95%

Inflammation and Immunity in Dermatophytosis

Tagami¹,

Kudoh²,

Takematsu³

1989

Dermatology

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Infections by dermatophytes (dermatophytosis) naturally stimulate the immune system as in those by other microorganisms to induce various immunological phenomena. However, differing from other infections, the infecting organisms cannot become a direct target of antibody response or phagocytosis because they reside only in the barrier membrane of the body surface, i.e. in the stratum corneum.Thus, the immunity against dermatophytes is relative as compared with the absolute one noted in other infections such as measles and mumps. In dermatophytosis, a unique behavior of the epidermis as noted in contact dermatitis plays an important role in the defense against infection. Dermatitic changes induced by fungal products, particularly those due to contact sensitivity to a fungal antigen, trichophytin, enhance epidermopoiesis, which leads to increased turnover of the epidermis with their resultant elimination from the skin surface. Furthermore, the dermatophytes in the stratum corneum provoke transepidermal leukocyte chemotaxis by generating chemotactic C5a anaphylatoxin in exudating serum via alternative complement pathway activation in addition to a release of low molecular weight chemotactic factors. Such neutrophilic migration with the formation of subcorneal pustules also enhances epidermal proliferation as in psoriasis.

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“…As early as 1949, a high incidence of allergic history in patients with chronic dermatophytosis was reported (48,61,63). Although elevated total IgE levels in the serum of patients with chronic dermatophytosis have been reported (7), normal IgE levels have also been observed among individuals with athlete's foot, irrespective of atopic history (87).…”

Section: Background: Historical Perspectivementioning

confidence: 99%

Allergy and Dermatophytes

Woodfolk

2005

Clin Microbiol Rev

147

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Tinea pedis (athlete's foot) and onychomycosis (infection of the toenails) caused by the dermatophyte fungus Trichophyton are highly prevalent in adults. Several Trichophyton allergens have been identified based on elicitation of immunoglobulin E antibody-mediated immediate-hypersensitivity (IH) responses. Evidence of an etiologic role for Trichophyton in asthma in some subjects with IH and chronic dermatophytosis is provided by bronchial reactivity to Trichophyton. Improvement of asthma after systemic antifungal treatment corroborates this link. A unique feature of Trichophyton allergens is the ability of the same antigen to elicit delayed-type hypersensitivity (DTH) in individuals who lack IH reactivity. Delayed responses appear to confer protection, while IH responses do not, based on the association with acute versus chronic skin infection. The amino acid sequence identity of Trichophyton allergens with diverse enzyme families supports a dual role for these proteins in fungal pathogenesis and allergic disease. Characterizing the immunologic properties of Trichophyton allergens and defining immune mechanisms which drive dichotomous responses are pivotal to understanding the dermatophyte-allergy relationship. Recent studies have identified DTH-associated major T-cell epitopes which could facilitate the development of peptide vaccines. Characterization of additional molecular targets by using new techniques may aid not only in the eradication of infection but also in the resolution of allergic symptoms

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Chronic dermatophyte infections. I. Clinical and mycological features

Cited by 92 publications

References 14 publications

Trichophyton Antigens Associated with IgE Antibodies and Delayed Type Hypersensitivity

Trichophyton Antigens Associated with IgE Antibodies and Delayed Type Hypersensitivity

Inflammation and Immunity in Dermatophytosis

Allergy and Dermatophytes

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