UV-induced DNA damage is an intermediate step in UV-induced expression of human immunodeficiency virus type 1, collagenase, c-fos, and metallothionein.

Stein, Bernd; Rahmsdorf, Hans J.; Steffen, Anȷa; Litfin, Margarethe; Herrlich, Peter

doi:10.1128/mcb.9.11.5169

Cited by 534 publications

(337 citation statements)

References 73 publications

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“…This induction response includes transcriptional activation, repression of a speci®c expression of some genes, and induction of endogenous virus (Ronai et al, 1990;Angel, 1995). Based on studies with DNA repairde®cient Xeroderma pigmentosum cells (Schorpp et al, 1984;Stein et al, 1989) DNA damage or by-products have been hypothesized to provide the primary signal transduction pathways mediating u.v. response.…”

Section: Discussionmentioning

confidence: 99%

“…The exposure of mammalian cells to u.v. irradiation, including short (UVC, 200 ± 280 nM) and long (UVA, 320 ± 400 nM) wavelengths, as well as mid-wavelengths (UVB, 280 ± 320 nM), leads to a large number of changes in cells, such as activation of transcription factor AP-1 and NFkB and P53 (Stein et al, 1989;Devary, 1991;Ronai and Weinstein, 1988;. AP-1 (and another transcription factor, NFkB) has served to detect one of the decisive DNA binding motifs required for gene regulation by tumor promoters, such as 12-O-tetradecanoylphorbol-13-acetate (TPA), 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) and u.v.…”

Section: Introductionmentioning

confidence: 99%

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Signal transduction through atypical PKCs, but not the EGF receptor, is necessary for UVC-induced AP-1 activation in immortal murine cells

Huang

Dong

1997

Oncogene

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The exposure of mammalian cells to ultraviolet (u.v.) irradiation leads to activation of transcription factors, such as AP-1 and NFkB. It is postulated that the EGF receptor but not protein kinase C (PKC) is the major membrane mediator in UVC-induced signal transduction. We demonstrate here that the antisense oligonucleotides of PKCz and the dominant negative mutant of PKCl/i as well as dominant negative PKCz markedly blocked UVC-induced AP-1 activity. In contrast, UVC-induced AP-1 activity in cells devoid of the EGF receptor (B82), is not signi®cantly di erent from that of the stable transfectants with a kinase-de®cient EGF receptor (B82M721), or wild-type EGF receptor (B82L). This was found at all UVC irradiation doses and time courses studied, while high levels of EGF-induced AP-1 activity were observed in B82L cells but not in B82 cells. This evidence strongly suggests that atypical PKCs, but not the EGF receptor, is necessary for UVC-induced AP-1 activation in JB6 and B82 cells.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Signal transduction through atypical PKCs, but not the EGF receptor, is necessary for UVC-induced AP-1 activation in immortal murine cells

Huang

Dong

1997

Oncogene

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“…Reporter plasmids containing di erent deletions of the QR1 5'-¯anking sequences up to +55 with respect to the transcription start site, were transfected into tsPA101 infected QNR cells. CAT5 empty vector (Stein et al, 1989) and RSV/CAT (Gorman et al, 1982) were used as controls. CAT activity was measured at the permissive (378C: v-Src induced proliferation) and nonpermissive (418C: growth arrest) temperature.…”

Section: The C Box Is a Transcriptional Enhancermentioning

confidence: 99%

“…C7 mutation was introduced into 71173/+55; 71265/+55 and 71265A7/+55 plasmids by PCR mediated mutagenesis. The 768/+55 minimal promoter sequence (mp) was obtained by PCR and inserted into the CAT5 vector (Stein et al, 1989) upstream from the CAT gene to give rise to mpCAT5 plasmid. To generate 71265/ 7935mpCAT5 constructs carrying A7 and/or C7 mutations, HindIII/BamHI fragments corresponding to the 71265/7935 region of QR1 promoter were excised from the appropriate 71265/+55 reporters and inserted into the mpCAT5 vector upstream from the minimal promoter.…”

Section: Plasmid Constructionsmentioning

confidence: 99%

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Characterization of a novel quiescence responsive element downregulated by v-Src in the promoter of the neuroretina specific QR1 gene

et al. 2000

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The neuroretina is a functional unit of the central nervous system which arises through successive steps of division, growth arrest and di erentiation of neuroectodermal precursors. Postmitotic quail neuroretina (QNR) cells are conditionally induced to divide upon infection with temperature sensitive mutants of Rous sarcoma virus (RSV), since QNR cell division can be arrested by either inactivating p60v-Src at the nonpermissive temperature (418C) or by serum deprivation at 378C. We are studying the transcriptional control of QR1, a neuroretina speci®c gene, whose expression is downregulated in proliferating cells at 378C and is fully restored when these cells are made quiescent. We previously showed that this quiescence speci®c upregulation implicates a promoter region named A box, which binds Maf transcription factors. We report the identi®-cation of the C box, a second promoter sequence that activates QR1 transcription in non dividing cells. This sequence is able to form two DNA-protein complexes, one of which (C4) is predominantly detected in growth arrested NR cells. We identi®ed the DNA binding site for C4 and described mutations that abolish both C4 binding and promoter activity in quiescent cells. Moreover, we show that a multimerized C box is able to stimulate a heterologous promoter in non dividing cells and constitutes, therefore, a novel quiescence responsive enhancer. Finally, we report that QR1 transcriptional response to cell quiescence requires cooperation between the C box and A box. Oncogene (2000) 19, 4736 ± 4745.

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Clinical Manifestations of Photosensitivity in Patients With Human Immunodeficiency Virus Infection

Gregory¹

1994

Arch Dermatol

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UV-induced DNA damage is an intermediate step in UV-induced expression of human immunodeficiency virus type 1, collagenase, c-fos, and metallothionein.

Cited by 534 publications

References 73 publications

Signal transduction through atypical PKCs, but not the EGF receptor, is necessary for UVC-induced AP-1 activation in immortal murine cells

Signal transduction through atypical PKCs, but not the EGF receptor, is necessary for UVC-induced AP-1 activation in immortal murine cells

Characterization of a novel quiescence responsive element downregulated by v-Src in the promoter of the neuroretina specific QR1 gene

Clinical Manifestations of Photosensitivity in Patients With Human Immunodeficiency Virus Infection

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