Abstract

Erythema multiforme (EM) is a polymorphous cutaneous eruption composed of symmetrically distributed macules, papules, bullae and targetoid lesions which have a propensity for the distant extremities and oral mucosae. It is estimated that 15-63% of EM cases are secondary to infection with herpes simplex virus (HSV). Like HSV, EM is a self-limited, often recurrent disorder. In scattered reports, EM skin lesions were found to be positive for infectious virus, virus particles, or viral antigens. However, HSV cultures of EM lesions are usually negative, and the exact role of HSV in EM pathogenesis is unclear. An additional component of EM pathogenesis is cell mediated immune (CMI) reactions, but the antigenic specificity of the involved T cells and identity of the T cell receptor (TCR) are unknown. The studies proposed in this application are a continuation of our previous observation using the polymerase chain reaction (PCR), indicating that DNA sequences homologous to a 92 bp fragment of the HSV DNA polymerase gene are present in EM lesions. They seek to determine the relationship of HSV to BM and establish the potential contribution of HSV and self antigens to the EM-related CMI responses.
The specific aims are: (i) to determine, by PCR, the presence in EM tissues of DNA sequences homologous to fragments of HSV genes that map along the entire HSV genome and represent all three kinetic classes, and identify their location in the dermis or epidermis, (ii) to determine whether the HSV genes that apparently persist in EM lesions, and the latency associated transcript (LAT) that is associated with latency are expressed by using the reverse transcriptase linked PCR (RT/PCR), and establish their cellular localization by in situ hybridization, (iii) to determine, in RT/PCR, whether expression of heat shock proteins (hsp) (that can be induced by HSV infection) is increased in EM lesions as compared to normal tissues, and (iv) to determine the TCR repertoire of T cells in EM lesions as compared to peripheral blood leukocytes and establish whether they proliferate in response to HSV or hsp antigens. These studies will provide a better understanding of the immunopathogenesis of EM and its relationship to HSV (and potentially hsp) thereby allowing the development of novel therapeutic interventions based on TCR Vbeta targeting. They will generate clinically relevant information for the diagnosis and management of the patients with post-herpetic EM as well as their differentiation from those with EM caused by other pathogens or by drug sensitivity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR042647-02
Application #
2082036
Study Section
General Medicine A Subcommittee 2 (GMA)
Project Start
1994-03-10
Project End
1998-02-28
Budget Start
1995-03-01
Budget End
1996-02-29
Support Year
2
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Maryland Baltimore
Department
Pharmacology
Type
Schools of Medicine
DUNS #
003255213
City
Baltimore
State
MD
Country
United States
Zip Code
21201

  Publications

Burnett, Joseph W; Laing, Jennifer M; Aurelian, Laure (2008) Acute skin eruptions that are positive for herpes simplex virus DNA polymerase in patients with stem cell transplantation: a new manifestation within the erythema multiforme reactive dermatoses. Arch Dermatol 144:902-7
Li, B; Smith, C C; Laing, J M et al. (2007) Overload of the heat-shock protein H11/HspB8 triggers melanoma cell apoptosis through activation of transforming growth factor-beta-activated kinase 1. Oncogene 26:3521-31
Gober, Michael D; Laing, Jennifer M; Burnett, Joseph W et al. (2007) The Herpes simplex virus gene Pol expressed in herpes-associated erythema multiforme lesions upregulates/activates SP1 and inflammatory cytokines. Dermatology 215:97-106
Sharma, B K; Smith, Cynthia C; Laing, Jennifer M et al. (2006) Aberrant DNA methylation silences the novel heat shock protein H11 in melanoma but not benign melanocytic lesions. Dermatology 213:192-9
Ono, Fumitake; Sharma, Bhuvnesh K; Smith, Cynthia C et al. (2005) CD34+ cells in the peripheral blood transport herpes simplex virus DNA fragments to the skin of patients with erythema multiforme (HAEM). J Invest Dermatol 124:1215-24
Aurelian, L (2005) HSV-induced apoptosis in herpes encephalitis. Curr Top Microbiol Immunol 289:79-111
Gober, Michael D; Smith, Cynthia C; Ueda, Kaori et al. (2003) Forced expression of the H11 heat shock protein can be regulated by DNA methylation and trigger apoptosis in human cells. J Biol Chem 278:37600-9
Perkins, Dana; Gyure, Kymberly A; Pereira, Edna F R et al. (2003) Herpes simplex virus type 1-induced encephalitis has an apoptotic component associated with activation of c-Jun N-terminal kinase. J Neurovirol 9:101-11
Perkins, D; Pereira, E F R; Aurelian, L (2003) The herpes simplex virus type 2 R1 protein kinase (ICP10 PK) functions as a dominant regulator of apoptosis in hippocampal neurons involving activation of the ERK survival pathway and upregulation of the antiapoptotic protein Bag-1. J Virol 77:1292-305
Aurelian, L; Ono, F; Burnett, J (2003) Herpes simplex virus (HSV)-associated erythema multiforme (HAEM): a viral disease with an autoimmune component. Dermatol Online J 9:1

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