Novel Treatments for Drug-Induced Toxic Epidermal Necrolysis (Lyell’s Syndrome)

Paquet, Philippe; Pierard, Gérald; Quatresooz, Pascale

doi:10.1159/000083947

Cited by 45 publications

(56 citation statements)

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“…Conversely, treatments that only block the activities of the proinflammatory cytokines and receptors produced in TEN, without acting on the deregulation of the electron transport chain in mitochondriae will probably have a limited effect on the course of TEN. This may be the case for intravenous immunoglobulins, systemic corticosteroids, cyclosporine and anti-TNF-· agents (47). Until effective chemical treatments are developed that are able to neutralize the reactive electrophilic metabolites and to restore the electron transfer chain in TEN keratinocytes, we suggest that several blocking agents (e.g.…”

Section: Conclusion and Future Prospectsmentioning

confidence: 99%

Toxic epidermal necrolysis: Revisiting the tentative link between early apoptosis and late necrosis (Review)

Paquet

Pierard

2007

Int J Mol Med

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Abstract. Toxic epidermal necrolysis (TEN) is a dramatic drug-induced reaction that may lead to full destruction of the epidermis and epithelial mucosae. The keratinocytes themselves seem to play a major role in the pathogenic mechanism. Biochemical and morphological studies performed on early epidermal lesions demonstrated that keratinocytes undergo apoptosis, but histological and clinical data show evidence of necrosis of the epidermis later in the disease evolution. Based on the limited information currently available about TEN pathomechanism, we present a 'mitochondrial hypothesis' that may explain both early apoptosis and late necrosis in TEN epidermis. Strong electrophilic drug metabolites are generated in TEN-affected keratinocytes due to an impaired detoxication pathway. These compounds presumably disrupt the electron transfer chain in the mitochondriae resulting in a decline in ATP production, loss of electrochemical gradient across the inner membrane (Δψm), and partial reduction in O 2 with production of reactive oxygen species (ROS). The latter compounds directly damage cell membranes and act as intracellular chemical messengers stimulating proapoptotic systems such as CD95 and TNF-·, which in turn can activate nitric oxide (NO) metabolism. NO interacts with ROS to enhance their toxic effects. These proapoptotic events represent swift processes in the involved cells. The loss of Δψm and the opening of permeability transition pores in the mitochondrial membrane lead to osmotic swelling and rupture of these organelles with subsequent necrosis of the cell. The necrotic events follow apoptosis when both phenomena are present.

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Section: Conclusion and Future Prospectsmentioning

confidence: 99%

Toxic epidermal necrolysis: Revisiting the tentative link between early apoptosis and late necrosis (Review)

Paquet

Pierard

2007

Int J Mol Med

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“…To date, no cause other than drugs has been found in TEN although 5% of the cases remain ''idiopathic' ' [22]. The mortality rate, which is higher than 40% in patients with more than 30% skin detachment is mainly due to septicemia and metabolic disturbances following the loss of epidermal integrity [11].The mechanism leading to massive keratinocyte death in TEN is thought to be apoptosis [18]. Disregulations in the tumor necrosis factor-a (TNF-a) pathway, CD95 system (Fas ligand-CD95L, Fas receptor-CD95R) and calcium homeostasis in the epidermis are likely involved [18].…”

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confidence: 99%

“…Indeed, TEN keratinocytes express large amounts of active CD95L able to induce apoptosis of CD95R-positive cells. CD95R, which belongs to the TNF/NGF receptor family is over-expressed in TEN epidermis.The TEN initiation phase leading to keratinocyte apoptosis is followed by an amplification phase involving inflammatory cells [18]. An active role has been ascribed to T lymphocytes, particularly CD4+ cells in the dermis and CD8+ cells in the epidermis.…”

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confidence: 99%

“…Disregulations in the tumor necrosis factor-a (TNF-a) pathway, CD95 system (Fas ligand-CD95L, Fas receptor-CD95R) and calcium homeostasis in the epidermis are likely involved [18]. Indeed, TEN keratinocytes express large amounts of active CD95L able to induce apoptosis of CD95R-positive cells.…”

mentioning

confidence: 99%

“…The TEN initiation phase leading to keratinocyte apoptosis is followed by an amplification phase involving inflammatory cells [18]. An active role has been ascribed to T lymphocytes, particularly CD4+ cells in the dermis and CD8+ cells in the epidermis.…”

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Analytical quantification of the inflammatory cell infiltrate and CD95R expression during treatment of drug-induced toxic epidermal necrolysis

et al. 2005

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The treatment of drug-induced toxic epidermal necrolysis (TEN) remains unsatisfactory. Intravenous immunoglobulins (IVIg) and intravenous cyclosporin A (CsA) have shown some efficacy in short series of patients. We assessed the effects of IVIg and CsA on TEN lesional and apparently uninvolved skin using standard histology and immunohistochemistry. Cutaneous biopsies were taken from necrotic and clinically uninvolved TEN skin at admission (D1) before any treatment, and after a 5-day treatment (D5). Two IVIg-treated patients (0.75 g/kg/day), two CsA-treated patients (5 mg/kg/day) and two control patients only receiving supportive care were compared. Biopsies were examined by standard histology and immunohistochemistry using antibodies directed to CD68 antigen (macrophages), CD45R0 antigen (activated T lymphocytes), Factor XIIIa (dermal dendrocytes) and the CD95 receptor (apoptosis marker). The different cell densities were evaluated by computerized image analysis. The clinical outcomes with the different treatments were also recorded. There was no obvious difference in the duration of hospitalization in intensive care unit between the three groups but one patient passed away in each of the IVIg-and CsAgroups. At D5, no differences were found between the three groups in the histological and clinical rate of reepithelialization, and in the evolution of T lymphocyte, macrophage and dendrocyte densities in the epidermis and dermis. However, the expression of the CD95 receptor was similarly and strongly abated at D5 in the epidermis of IVIg-and CsA-treated patients, while it was conversely increased in the two patients under supportive care only. Such a difference was found both in necrotic and uninvolved sites. IVIg and CsA treatments thus appeared to exert no obvious effect on the inflammatory infiltrate, but both abated the expression of the CD95 receptor in the skin of TEN patients. This effect did not seem sufficient to fully reverse the clinical evolution of the disease. It is inferred that IVIg and CsA do not completely abate the TEN process.Keywords Toxic epidermal necrolysis AE Cyclosporin A AE Immunoglobulin Drug-induced toxic epidermal necrolysis (TEN) is a lifethreatening disease characterized by extensive destruction of the epidermis [5]. To date, no cause other than drugs has been found in TEN although 5% of the cases remain ''idiopathic' ' [22]. The mortality rate, which is higher than 40% in patients with more than 30% skin detachment is mainly due to septicemia and metabolic disturbances following the loss of epidermal integrity [11].The mechanism leading to massive keratinocyte death in TEN is thought to be apoptosis [18]. Disregulations in the tumor necrosis factor-a (TNF-a) pathway, CD95 system (Fas ligand-CD95L, Fas receptor-CD95R) and calcium homeostasis in the epidermis are likely involved [18]. Indeed, TEN keratinocytes express large amounts of active CD95L able to induce apoptosis of CD95R-positive cells. CD95R, which belongs to the TNF/NGF receptor family is over-expressed in TEN epid...

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Therapeutic Targets of the TNF Superfamily

Grewal¹

2009

Advances in Experimental Medicine and Biology

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Novel Treatments for Drug-Induced Toxic Epidermal Necrolysis (Lyell’s Syndrome)

Cited by 45 publications

References 210 publications

Toxic epidermal necrolysis: Revisiting the tentative link between early apoptosis and late necrosis (Review)

Toxic epidermal necrolysis: Revisiting the tentative link between early apoptosis and late necrosis (Review)

Analytical quantification of the inflammatory cell infiltrate and CD95R expression during treatment of drug-induced toxic epidermal necrolysis

Therapeutic Targets of the TNF Superfamily

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