Joseph W. Burnett scite author profile

Scanning tunneling microscopy shows that large two-dimensional Ag clusters on Ag(100) can diffuse. The value of the diffusion coefficient at room temperature is of order 10-17 cm2s-1 and varies little, if at all, with cluster size in the range studied, 100 to 720 atoms per cluster. This weak variation rules out periphery diffusion as the main mechanism of cluster diffusion, suggesting instead two-dimensional evaporationcondensation. This conclusion is compatible with the energetics of atomic-scale events within the cluster and with the dissolution of small clusters observed at low coverages. Keywords Ames Laboratory, Mathematics Disciplines Mathematics | Physical Chemistry CommentsThis article is from Physical Review Letters 73, no. 19 (1994) .- (a) . (

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Coarsening Mechanisms in a Metal Film: From Cluster Diffusion to Vacancy Ripening

Wen

et al. 1996

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Herpes Simplex Virus Associated Erythema Multiforme (HAEM) is Mechanistically Distinct from Drug-Induced Erythema Multiforme: Interferon-γ is Expressed in HAEM Lesions and Tumor Necrosis Factor-α in Drug-Induced Erythema Multiforme Lesions

Kokuba

Aurelian

Burnett

1999

Journal of Investigative Dermatology

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Erythema multiforme follows administration of several drugs or infection with various agents, including herpes simplex virus, a syndrome designated herpes simplex virus associated erythema multiforme. Lesional skin from 21 of 26 (81%) herpes simplex virus associated erythema multiforme patients was positive for herpes simplex virus gene expression as evidenced by reverse transcriptase-polymerase chain reaction with primers for DNA polymerase and/or immunohistochemistry with DNA polymerase antibody. Reverse transcriptase-polymerase chain reaction and immunohistochemistry studies indicated that herpes simplex virus associated erythema multiforme lesional skin from 16 of 21 (76%) DNA polymerase positive herpes simplex virus associated erythema multiforme patients was also positive for interferon-gamma, a product of T cells involved in delayed-type hypersensitivity (p < 0. 0001 by Pearson correlation coefficient). Interferon-gamma signals were in infiltrating mononuclear cells and in intercellular spaces within inflammatory sites in the epidermis and at the epidermis/dermis junction. Herpes simplex virus lesional skin was also positive for DNA polymerase [five of five (100%)] and interferon-gamma [four of five (80%)], but lesional skin from drug-induced erythema multiforme patients was negative. Lesional herpes simplex virus associated erythema multiforme keratinocytes also stained with antibody to transforming growth factor-beta [14 of 23 (61%)] and cyclin-dependent kinase inhibitor waf [12 of 18 (67%)]. Staining was also seen in keratinocytes from herpes simplex virus lesions [five of five (100%)], but not in normal skin. By contrast, staining with antibody to tumor necrosis factor-alpha, another pro-inflammatory cytokine, was seen in seven of 11 (64%) drug-induced erythema multiforme patients, but not in herpes simplex virus or herpes simplex virus associated erythema multiforme patients, and lesional keratinocytes from drug-induced erythema multiforme patients were negative for transforming growth factor-beta and cyclin-dependent kinase inhibitor waf. We interpret the data to indicate that herpes simplex virus associated erythema multiforme pathology includes a delayed-type hypersensitivity component and is mechanistically distinct from drug-induced erythema multiforme.

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Erythema multiforme lesions are associated with expression of a herpes simplex virus (HSV) gene and qualitative alterations in the HSV-specific T-cell response

et al. 1998

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A common form of erythema multiforme, herpes-associated erythema multiforme (HAEM), occurs following infection with herpes simplex virus (HSV). Here we report that HSV gene expression and the qualitative nature of the virus-specific T-cell responses are related to HAEM lesion development. Skin from HAEM lesions and 1-3 months healed HAEM lesional skin were positive for the viral DNA polymerase gene (Pol) by polymerase chain reaction. However, gene expression as determined by immunohistochemistry with Pol-specific antibody was seen only in HAEM lesions, suggesting that lesion development is associated with Pol gene expression. Similar HSV-specific T-cell lymphoproliferative responses were seen in peripheral blood mononuclear cells (PBMCs) from patients with acute or healed HAEM lesions or HSV lesions and from HSV-seropositive patients with unrelated inflammatory diseases. However, the T-cell receptor variable (V beta) chain repertoire of HSV-stimulated PBMCs obtained from HAEM lesions was altered; the prevalence of some families of variable chain (namely V beta 16 and V beta 19) was reduced, whereas the prevalence of others was increased (namely V beta 2 and V beta 7). V beta 2 cells were found in HAEM lesional skin positive for Pol antigen, suggesting that these cells home to viral antigen-positive skin.

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Partial purification of box jellyfish (Chironex fleckeri) nematocyst venom isolated at the beachside

Bloom

Burnett

Alderslade³

1998

Toxicon

147

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Teledermatology and In-Person Examinations

Lowitt¹,

Kessler²,

Kauffman³

et al. 1998

Arch Dermatol

153

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Jellyfish envenomation syndromes

Burnett

Calton

Burnett

1986

Journal of the American Academy of Dermatology

107

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Treatment of Atlantic cnidarian envenomations

Burnett

2009

Toxicon

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Joseph W. Burnett

Diffusion of Large Two-Dimensional Ag Clusters on Ag(100)

Coarsening Mechanisms in a Metal Film: From Cluster Diffusion to Vacancy Ripening

Herpes Simplex Virus Associated Erythema Multiforme (HAEM) is Mechanistically Distinct from Drug-Induced Erythema Multiforme: Interferon-γ is Expressed in HAEM Lesions and Tumor Necrosis Factor-α in Drug-Induced Erythema Multiforme Lesions

Erythema multiforme lesions are associated with expression of a herpes simplex virus (HSV) gene and qualitative alterations in the HSV-specific T-cell response

Partial purification of box jellyfish (Chironex fleckeri) nematocyst venom isolated at the beachside

Teledermatology and In-Person Examinations

Jellyfish envenomation syndromes

Treatment of Atlantic cnidarian envenomations

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