A Critical Role for the Proapoptotic Protein Bid in Ultraviolet-Induced Immune Suppression and Cutaneous Apoptosis

Pradhan, Sanjay; Kim, Hee Kyung; Thrash, Christopher; Cox, Maureen A.; Mantena, Sudheer K.; Wu, Jianghong; Athar, Mohammad; Katiyar, Säntosh K.; Elmets, Craig A.; Timares, Laura

doi:10.4049/jimmunol.181.5.3077

Cited by 26 publications

(17 citation statements)

References 46 publications

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“…Specifically, it was not possible to detect the presence of the typical Birbeck granule in lesional skin. After nb-UVB exposure, in fact, there is a replacement of Langerhans cells, which have migrated to the dermis, by immature precursors [15]. This CD83 expression reduction, on the other hand, was not observed in the lesional dermis of vitiligo skin where there is an increase of 25%.…”

Section: Discussionmentioning

confidence: 92%

Dendritic cells: ultrastructural and immunophenotypical changes upon nb-UVB in vitiligo skin

et al. 2010

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The role of dendritic cells in vitiligo is still unclear. Few studies have provided contradictory results about their quantitative variation and no data exist concerning their immunophenotypical distribution in diseased skin. The purpose of our study was to analyze the presence, the distribution, the immunophenotypical markers and the effects of nb-UVB therapy on dendritic cells in nonlesional, perilesional, and lesional vitiligo skin. Punchbiopsies of 6 mm were taken from lesional, perilesional, and non-lesional skin of 12 patients affected by nonsegmental vitiligo, treated with nb-UVB. An immunohistochemical and an ultrastructural analysis were performed. Immunohistochemical and ultrastructural analysis showed both quantitative and qualitative modifications of Langerhans cells. Nb-UVB therapy, one of the most effective treatments for the disease, was able to reduce the Langerhans cells number and to redistribute main dendritic subsets. This study underlines the importance of dendritic cells, Langerhans cells in particular, in non-segmental vitiligo, in its pathogenesis and in its better therapeutical approach.

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Section: Discussionmentioning

confidence: 92%

Dendritic cells: ultrastructural and immunophenotypical changes upon nb-UVB in vitiligo skin

et al. 2010

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“…Immature DCs (both human and mouse) are highly susceptible to UVB radiation, whereas mature DCs upregulate c-FLIP and Bcl-2 and are less susceptible to UV-induced apoptosis (52). Prevention of apoptosis of Langerhans cells blocks UV-induced immunosuppression, suggesting that UVinduced DC apoptosis makes viable DCs tolerogenic; however, the mechanism remains unclear (53).…”

Section: Regulation Of DC Apoptosismentioning

confidence: 99%

Dendritic Cell Apoptosis: Regulation of Tolerance versus Immunity

Kushwah

2010

The Journal of Immunology

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Dendritic cell (DC) apoptosis is an important event that regulates the balance between tolerance and immunity through multiple pathways, and defects in DC apoptosis can trigger autoimmunity. DC apoptosis is also associated with immunosuppression and has been observed under several pathologies and infections. Recent studies indicate that apoptotic DCs can also play an active role in induction of tolerance. This review discusses the regulatory pathways of DC apoptosis, stimuli inducing DC apoptosis, and the implications of DC apoptosis in the induction of immunosuppression and/or tolerance.

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“…The former is activated under oxidative stress conditions, after exposure to ultraviolet rays, and under physical stress conditions such as heat shock [13][14][15][16], and the latter is activated by physiological ligands such as TNF-a, TNF-related apoptosis inducing ligand, and Fas ligand [17,18]. The activation of any of the two pathways results in the apoptosis of tumor cells and unwanted cells.…”

Section: Introductionmentioning

confidence: 99%

Mouse 3T3-L1 cells acquire resistance against oxidative stress as the adipocytes differentiate via the transcription factor FoxO

et al. 2009

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Repression of excessive increase and enlargement of adipocytes that is closely associated with obesity is effective in the prevention and treatment of metabolic syndrome. Generally, apoptosis is induced in cells via a wide variety of intracellular or extracellular substances, and recently, it has been suggested that the FoxO subfamily is involved in the induction of apoptosis. We aimed to elucidate the mechanism of FoxO-mediated apoptosis-induction in the adipocytes under the reactive oxygen species (ROS) stimulus. The treatment of differentiated and undifferentiated 3T3-L1 cells with glucose oxidase (GOD), an enzyme that generates H(2)O(2), induced apoptosis and led to the accumulation of 8-OHdG. Apoptosis analysis revealed that GOD treatment induced apoptosis in differentiated 3T3-L1 cells less efficiently than in undifferentiated preadipocytes. GOD remarkably increased the levels of Bad, Bax, and Bim-the genes that are actively involved in cell apoptosis. GOD treatment also increased the expression of FoxO3a mRNA and protein. The introduction of FoxO3a-siRNA into 3T3-L1 cells suppressed the oxidative stress-induced expression of Bim mRNA, as well as the GOD-induced apoptosis. Furthermore, the expression of MnSOD, Cu/ZnSOD, and catalase, as well as of FoxO, increased significantly along with the progression of adipocyte differentiation. These results indicated that ROS-induced apoptosis in undifferentiated 3T3-L1 cells via the expression of FoxO3a, whereas FoxO expression suppressed the ROS-induced apoptosis in differentiated 3T3-L1 cells via the expression of ROS-scavenging enzymes.

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A Critical Role for the Proapoptotic Protein Bid in Ultraviolet-Induced Immune Suppression and Cutaneous Apoptosis

Cited by 26 publications

References 46 publications

Dendritic cells: ultrastructural and immunophenotypical changes upon nb-UVB in vitiligo skin

Dendritic cells: ultrastructural and immunophenotypical changes upon nb-UVB in vitiligo skin

Dendritic Cell Apoptosis: Regulation of Tolerance versus Immunity

Mouse 3T3-L1 cells acquire resistance against oxidative stress as the adipocytes differentiate via the transcription factor FoxO

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