The Herpes Simplex Virus Gene Pol Expressed in Herpes-Associated Erythema Multiforme Lesions Upregulates/Activates SP1 and Inflammatory Cytokines

Gober, Michael D.; Laing, Jennifer M.; Burnett, Joseph W.; Aurelian, Laure

doi:10.1159/000104259

Cited by 19 publications

(21 citation statements)

References 88 publications

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“…The Pol-induced upregulation of the transcription factor SP1 and SP1-regulated genes in HAEM lesional skin are associated with the inflammatory and autoreactive components of HAEM. 7,17 …”

Section: Commentmentioning

confidence: 99%

Acute Skin Eruptions That Are Positive for Herpes Simplex Virus DNA Polymerase in Patients With Stem Cell Transplantation

Burnett

Laing²,

Aurelian³

2008

Arch Dermatol

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“…The Pol-induced upregulation of the transcription factor SP1 and SP1-regulated genes in HAEM lesional skin are associated with the inflammatory and autoreactive components of HAEM. 7,17 …”

Section: Commentmentioning

confidence: 99%

Acute Skin Eruptions That Are Positive for Herpes Simplex Virus DNA Polymerase in Patients With Stem Cell Transplantation

Burnett

Laing²,

Aurelian³

2008

Arch Dermatol

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“…The lesions are free of infectious virus, but they contain viral DNA fragments and express a limited number of viral proteins that are associated with lesion development, notably Pol [6,7,8,9,10,11,12]. The viral DNA fragments are transported to the skin by CD1a+ Langerhans cells that develop through E-cadherin-facilitated differentiation of CD34+ cells infected with HSV while in circulation [6,7,8].…”

Section: Discussionmentioning

confidence: 99%

“…Also, constraints imposed by the limited availability of tissues and PBMC have restricted our studies to the use of immunofluorescent staining. However, the specificity of the Pol antibody is established [6,7,8,9,10,11,12]. The PBMC from normal subjects are known to be Pol negative [11], and the absence of Pol staining in the pre-HSCT samples suggests that the Pol+CD34+ and Pol+CD1a+ cells in the skin tissues are of donor origin, having been infected while in circulation.…”

Section: Discussionmentioning

confidence: 99%

“…This is supported by the known histological similarity of GVHD to drug and viral exanthems [5] and the rather diverse clinical presentation of erythematous lesions that fall under the EM umbrella. We still do not know whether the skin GVHD-diagnosed lesions express the markers [IFN-γ, SP1, TGF-β, p21 (waf1) and Hsp27], which differentiate HAEM from other GVHD-like skin diseases such as Stevens-Johnson syndrome [10,12] and we do not exclude the possibility that reactivated HSV increases the risk of GVHD through its ability to stimulate T cell proliferation and induce DC maturation and IL-12 secretion [1,6,11]. Also still unclear is the potential contribution of other herpesviruses that are reactivated from latency by the immunosuppressive drugs used during allogeneic transplantation [2].…”

Section: Discussionmentioning

confidence: 99%

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Acute Skin Graft-versus-Host Disease with Molecular Features Mimicking Herpes Simplex Virus-Associated Erythema Multiforme: Report of Three Cases

Joseph

Shvartsbeyn²,

Günay³

et al. 2013

Dermatology

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Background: Acute skin erythematous lesions that follow allogeneic hematopoietic stem cell transplantation (HSCT) and are histologically diagnosed as graft-versus-host disease (GVHD) are often associated with reactivation of latent herpes simplex virus (HSV). Objective: To further examine the relationship between reactivated HSV and GVHD development. Methods: We present 3 patients with acute skin GVHD after allogeneic HSCT who were studied prospectively for expression of the HSV antigen Pol, which is involved in HSV-associated erythema multiforme. Results: Pol was expressed in the GVHD lesions but not the pre-HSCT normal skin or peripheral blood mononuclear cells. Lesion severity correlated with the Pol levels but not the histopathologically defined GVHD grade. Lesion development was accompanied by increased numbers of Pol+ circulating/skin-infiltrating CD34+ stem cells and CD1a+ and other dermal dendritic cells. Conclusions: Subclinical HSV infection of circulating CD34+ cells can contribute to some post-HSCT skin lesions histologically diagnosed as GVHD, with potential preventive and therapeutic implications.

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“…Plus tard, des cellules progénitrices hématopoïétiques CD34+ ont été mises en évidence dans le transport de fragments d'ADN viral (notamment d'ADN polymérase) vers les sites cutanés lésionnels [11] expliquant que des traces d'ADN viral soient parfois retrouvées au sein des lésions d'EP. D'autres travaux ont été réalisés pour mieux comprendre les mécanismes intervenant dans cette pathologie, notamment sur les liens existant entre la présence de fragments d'ADN, la production de TGF-β et le rôle tenu par la molécule p21 waf1 et le facteur de transcription SP1 qui semblent tous augmentés au sein des lésions présentant des fragments d'ADN viraux mais dont les rôles ne sont pas encore bien définis [12]. Des études récentes laissent supposer qu'il pourrait exister un rôle des lymphocytes Th17, sous-population effectrice de lymphocytes T CD4+, dans la pathogenèse de l'EP [13] et certains auteurs ont mis en évidence une augmentation des lymphocytes B périphériques chez des patients atteints d'EP [14].…”

Section: Fig 3 Case Report Number 3 Oral Mucosal Damages During Emunclassified

Manifestations orales de l’érythème polymorphe : présentation de cas cliniques

Rochefort

Hervé²,

Agbo-Godeau

2016

Med Buccale Chir Buccale

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Résumé -Introduction : L'érythème polymorphe (EP) est une maladie caractérisée par une atteinte bulleuse cutanéo-muqueuse aiguë. Les infections sont les principales causes déclenchantes connues, en particulier l'herpès, dans plus de 50 % des cas. Deux formes d'EP sont à distinguer : l'une mineure, dont les symptômes sont peu invalidants, l'autre majeure, comporte une atteinte cutanée et muqueuse buccale et/ou génitale, et peut entraîner une altération de l'état général. Observations : Trois cas d'EP récurrents sont décrits. Le premiers cas concerne un EP muqueux et les deux derniers un EP cutanéo-muqueux. Discussion : L'atteinte buccale d'EP se présente sous la forme de lésions bulleuses laissant rapidement place à des érosions plus ou moins étendues. Des croûtes sanguinolentes sont généralement situées sur les lèvres. L'atteinte cutanée en cocardes est caractéristique mais inconstante. L'analyse anatomopathologique des lésions trouve un décollement situé entre la lame basale et les kératinocytes basaux. Les stratégies thérapeutiques sont à visée symptomatique avec un traitement antalgique et antiseptique local et pour les formes récidivantes, un traitement préventif des récurrences, si le facteur déclenchant est connu, aciclovir ou valaciclovir quand il s'agit de l'herpès. Conclusion : Le diagnostic d'EP doit être évoqué devant des ulcérations buccales récidivantes associées à une atteinte des autres muqueuses. La présence de cocarde sur la peau est caractéristique de l'EP. Abstract -Oral manifestations of erythema multiforme: case reports. Introduction: Erythema multiforme (EM)is characterised by acute cutaneous and mucous bullous lesions. Infections are the most common cause. The herpes virus is associated with 50% of cases of erythema multiforme. There are two clinical aspects, the minor and the major forms. Erythema multiforme minor represents a localised eruption of the skin. The major form presents with cutaneous and mucous (oral and/or genital) lesions and general symptoms. Observation: Three cases of recurrent EM are described. The first case involves mucous EM and the other two mucocutaneous EM. Discussion: Oral mucosal involvement consists of multiple bullous lesions and post-bullous erosions. The skin is affected by the typical target lesions, but this sign is inconsistent. Histology shows a detachment between the epithelium and basal lamina. Treatment is symptomatic with analgesics and local antiseptic. Topical corticosteroids may be prescribed for recurrent cases. Conclusion: The diagnosis of EM should be considered for recurrent oral ulcers associated with other mucous membranes. Target lesions on the skin are characteristic of EM.

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The Herpes Simplex Virus Gene Pol Expressed in Herpes-Associated Erythema Multiforme Lesions Upregulates/Activates SP1 and Inflammatory Cytokines

Cited by 19 publications

References 88 publications

Acute Skin Eruptions That Are Positive for Herpes Simplex Virus DNA Polymerase in Patients With Stem Cell Transplantation

Acute Skin Eruptions That Are Positive for Herpes Simplex Virus DNA Polymerase in Patients With Stem Cell Transplantation

Acute Skin Graft-versus-Host Disease with Molecular Features Mimicking Herpes Simplex Virus-Associated Erythema Multiforme: Report of Three Cases

Manifestations orales de l’érythème polymorphe : présentation de cas cliniques

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