Jun proteins and AP-1 in tumorigenesis

doi:10.1017/CBO9781139046947.028

27 - Jun proteins and AP-1 in tumorigenesis

from Part 2.1 - Molecular pathways underlying carcinogenesis: signal transduction

Published online by Cambridge University Press: 05 February 2015

Shira Anzi and

Eitan Shaulian

Edited by

Edward P. Gelmann ,

Charles L. Sawyers and

Frank J. Rauscher, III

Show author details

Shira Anzi: Affiliation:
Department of Developmental Biology and Cancer Research, IMRIC, he Hebrew University - Hadassah Medical School, Jerusalem, Israel
Eitan Shaulian: Affiliation:
Department of Biochemistry and Molecular Biology, IMRIC, The Hebrew University - Hadassah Medical School, Jerusalem, Israel
Edward P. Gelmann: Affiliation:
Columbia University, New York
Charles L. Sawyers: Affiliation:
Memorial Sloan-Kettering Cancer Center, New York
Frank J. Rauscher, III: Affiliation:
The Wistar Institute Cancer Centre, Philadelphia

Book contents

Get access

Summary

AP-1

Activating protein 1 (AP-1) is a dimeric transcription factor which serves as an integrator of numerous signals to regulate gene expression affecting cellular proliferation, differentiation, apoptosis, autophagy, inflammation, cellular migration, and neoplastic transformation. AP-1 is composed of proteins from several families whose common denominator is the possession of basic leucine-zipper (bZIP) domains that are essential for dimerization and DNA binding. Jun (c-Jun, JunB, and JunD) and Fos (c-Fos, FosB, Fra1, and Fra2) subfamilies are the major AP-1 proteins. ATF proteins ATF2, LRF1/ATF3, B-ATF, JDP1, and JDP2 are also components of AP-1, and the Maf subfamily, which includes c-Maf, MafB, MafA, MafG/F/K, and Nrl are considered to be close relatives which form heterodimers with Fos and Jun, and occupy AP-1 binding sites. Jun–Fos heterodimers bind preferentially to a heptamer consensus sequence known as the TPA responsive element (TRE; 5ʹ-TGA(C/G)TCA-3ʹ), whereas Jun-ATF dimers bind with higher affinity to another consensus sequence known as the cyclic AMP responsive element (CRE; 5ʹ- TGACGTCA -3ʹ). The seven Fos-Jun family members can form 18 different homo- and heterodimers. The composition of the dimers varies among different tissues, regulated by exposure to different stimuli, and determines specificity of the binding site and consequently the identity of activated genes (1). Increased diversity of AP-1 and consequently increased complexity, is also generated by the ability of “core AP-1 proteins” Jun and Fos to interact with other leucine-zipper-containing proteins, sometimes resulting in binding to novel DNA elements (2). Additional layers of complexity may stem from interactions of AP-1 components with structurally unrelated proteins which recruit them to other divergent binding sites on the DNA in order to regulate gene transcription (1).

Type: Chapter
Information: Molecular Oncology
Causes of Cancer and Targets for Treatment
, pp. 319 - 327

DOI: https://doi.org/10.1017/CBO9781139046947.028 [Opens in a new window]

Publisher: Cambridge University Press

Print publication year: 2013

Access options

Get access to the full version of this content by using one of the access options below. (Log in options will check for institutional or personal access. Content may require purchase if you do not have access.)

Book purchase

Temporarily unavailable

References

Chinenov, Y, Kerppola, TK. Close encounters of many kinds: Fos-Jun interactions that mediate transcription regulatory specificity. Oncogene 2001;20:2438–52.CrossRef

Cai, DH, Wang, D, Keefer, J, et al. C/EBP alpha: AP-1 leucine zipper heterodimers bind novel DNA elements, activate the PU.1 promoter and direct monocyte lineage commitment more potently than C/EBP alpha homodimers or AP-1. Oncogene 2008;27:2772–9.CrossRef

Kouzarides, T, Ziff, E. The role of the leucine zipper in the fos-jun interaction. Nature 1988;336:646–51.CrossRef

Kallunki, T, Deng, T, Hibi, M, Karin, M. c-Jun can recruit JNK to phosphorylate dimerization partners via specific docking interactions. Cell 1996;87:929–39.CrossRef

Adler, J, Reuven, N, Kahana, C, Shaul, Y. c-Fos proteasomal degradation by default and its regulation by NQO1 determines c-Fos serum response kinetics. Molecular and Cellular Biology 2010;30:3767–78.CrossRef

Hibi, M, Lin, A, Smeal, T, Minden, A, Karin, M. Identification of an oncoprotein- and UV-responsive protein kinase that binds and potentiates the c-Jun activation domain. Genes and Development 1993;7:2135–48.CrossRef

Derijard, B, Hibi, M, Wu, IH, et al. JNK1: a protein kinase stimulated by UV light and Ha-Ras that binds and phosphorylates the c-Jun activation domain. Cell 1994;76:1025–37.CrossRef

Morton, S, Davis, RJ, McLaren, A, Cohen, P. A reinvestigation of the multisite phosphorylation of the transcription factor c-Jun. EMBO Journal 2003;22:3876–86.CrossRef

Lin, A, Frost, J, Deng, T, et al. Casein kinase II is a negative regulator of c-Jun DNA binding and AP-1 activity. Cell 1992;70:777–89.CrossRef

Boyle, WJ, Smeal, T, Defize, LH, et al. Activation of protein kinase C decreases phosphorylation of c-Jun at sites that negatively regulate its DNA-binding activity. Cell 1991;64:573–84.CrossRef

Barila, D, Mangano, R, Gonfloni, S, et al. A nuclear tyrosine phosphorylation circuit: c-Jun as an activator and substrate of c-Abl and JNK. EMBO Journal 2000;19:273–81.CrossRef

Zhu, F, Choi, BY, Ma, WY, et al. COOH-terminal Src kinase-mediated c-Jun phosphorylation promotes c-Jun degradation and inhibits cell transformation. Cancer Research 2006;66:5729–36.CrossRef

Weiss, C, Schneider, S, Wagner, EF, et al. JNK phosphorylation relieves HDAC3-dependent suppression of the transcriptional activity of c-Jun. EMBO Journal 2003;22:3686–95.CrossRef

Angel, P, Hattori, K, Smeal, T, Karin, M. The jun proto-oncogene is positively autoregulated by its product, Jun/AP-1. Cell 1988;55:875–85.CrossRef

Stein, B, Angel, P, van Dam, H, et al. Ultraviolet-radiation induced c-jun gene transcription: two AP-1 like binding sites mediate the response. Photochemistry and Photobiology 1992;55:409–15.CrossRef

Abate, C, Patel, L, Rauscher, FJ, 3rd, Curran T. Redox regulation of fos and jun DNA-binding activity in vitro. Science 1990;249:1157–61.CrossRef

Xanthoudakis, S, Curran, T. Redox regulation of AP-1: a link between transcription factor signaling and DNA repair. Advances in Experimental Medical Biology 1996;387:69–75.CrossRef

Fuchs, SY, Dolan, L, Davis, RJ, Ronai, Z. Phosphorylation-dependent targeting of c-Jun ubiquitination by Jun N-kinase. Oncogene 1996;13:1531–5.

Musti, AM, Treier, M, Bohmann, D. Reduced ubiquitin-dependent degradation of c-Jun after phosphorylation by MAP kinases. Science 1997;275:400–2.CrossRef

Wei, W, Jin, J, Schlisio, S, Harper, JW, Kaelin, WG The v-Jun point mutation allows c-Jun to escape GSK3-dependent recognition and destruction by the Fbw7 ubiquitin ligase. Cancer Cell 2005;8:25–33.CrossRef

Yogev, O, Saadon, K, Anzi, S, Inoue, K, Shaulian, E. DNA damage-dependent translocation of B23 and p19 ARF is regulated by the Jun N-terminal kinase pathway. Cancer Research 2008;68:1398–406.CrossRef

Shaulian, E, Karin, M. AP-1 as a regulator of cell life and death. Nature Cell Biology 2002;4:E131–6.

Greenberg, ME, Ziff EB. Stimulation of 3T3 cells induces transcription of the c-fos proto-oncogene. Nature 1984;311:433–8.CrossRef

Angel, P, Karin, M. The role of Jun, Fos and the AP-1 complex in cell-proliferation and transformation. Biochimica et Biophysica Acta 1991;1072:129–57.

Piette, J, Hirai, S, Yaniv, M. Constitutive synthesis of activator protein 1 transcription factor after viral transformation of mouse fibroblasts. Proceedings of the National Academy of Sciences USA 1988;85:3401–5.CrossRef

Smeal, T, Binetruy, B, Mercola, DA, Birrer, M, Karin, M. Oncogenic and transcriptional cooperation with Ha-Ras requires phosphorylation of c-Jun on serines 63 and 73. Nature 1991;354:494–6.CrossRef

Hernandez, JM, Floyd, DH, Weilbaecher, KN, Green, PL, Boris-Lawrie, K. Multiple facets of junD gene expression are atypical among AP-1 family members. Oncogene 2008;27:4757–67.CrossRef

Shaulian, E, Schreiber, M, Piu F, et al. The mammalian UV response: c-Jun induction is required for exit from p53-imposed growth arrest. Cell 2000;103:897–907.CrossRef

Devary, Y, Gottlieb, RA, Lau, LF, Karin, M. Rapid and preferential activation of the c-jun gene during the mammalian UV response. Molecular and Cellular Biology 1991;11:2804–11.CrossRef

Gupta, S, Campbell, D, Derijard, B, Davis, RJ. Transcription factor ATF2 regulation by the JNK signal transduction pathway. Science 1995;267:389–93.CrossRef

Yogev, O, Anzi, S, Inoue, K, Shaulian, E.Induction of transcriptionally active Jun proteins regulates drug-induced senescence. Journal of Biological Chemistry 2006;281:34 475–83.CrossRef Google Scholar PubMed

Macian, F, Lopez-Rodriguez, C, Rao, A. Partners in transcription: NFAT and AP-1. Oncogene 2001;20:2476–89.CrossRef

Shaulian, E, Karin, M. AP-1 in cell proliferation and survival. Oncogene 2001;20:2390–400.CrossRef

Schreiber, M, Kolbus, A, Piu, F, et al. Control of cell cycle progression by c-Jun is p53 dependent. Genes and Development 1999;13:607–19.CrossRef

Johnson, RS, van Lingen, B, Papaioannou, VE, Spiegelman, BM. A null mutation at the c-jun locus causes embryonic lethality and retarded cell growth in culture. Genes and Development 1993;7:1309–17.CrossRef

Weitzman, JB, Fiette, L, Matsuo, K, Yaniv, M. JunD protects cells from p53-dependent senescence and apoptosis. Molecular Cell 2000;6:1109–19.CrossRef

Johnson, AC, Murphy, BA, Matelis, CM, et al. Activator protein-1 mediates induced but not basal epidermal growth factor receptor gene expression. Molecular Medicine 2000;6:17–27.

Zenz, R, Scheuch, H, Martin, P, et al. c-Jun regulates eyelid closure and skin tumor development through EGFR signaling. Developmental Cell 2003;4:879–89.CrossRef

MacLaren, A, Black, EJ, Clark, W, Gillespie, DA. c-Jun-deficient cells undergo premature senescence as a result of spontaneous DNA damage accumulation. Molecular and Cellular Biology 2004;24:9006–18.CrossRef

Passegue, E, Wagner, EF. JunB suppresses cell proliferation by transcriptional activation of p16(INK4a) expression. EMBO Journal 2000;19:2969–79.CrossRef

Andrecht, S, Kolbus, A, Hartenstein, B, Angel, P, Schorpp-Kistner M. Cell cycle promoting activity of JunB through cyclin A activation. Journal of Biological Chemistry 2002;277:35 961–8.CrossRef Google Scholar PubMed

Passegue, E, Jochum, W, Behrens, A, Ricci, R, Wagner, EF. JunB can substitute for Jun in mouse development and cell proliferation. Nature Genetics 2002;30:158–66.CrossRef

Brown, JR, Nigh, E, Lee, RJ, et al. Fos family members induce cell cycle entry by activating cyclin D1. Molecular and Cellular Biology 1998;18:5609–19.CrossRef

Brusselbach, S, Mohle-Steinlein, U, Wang, ZQ, et al. Cell proliferation and cell cycle progression are not impaired in fibroblasts and ES cells lacking c-Fos. Oncogene 1995;10:79–86.

Eferl, R, Wagner, EF. AP-1: a double-edged sword in tumorigenesis. Nature Reviews Cancer 2003;3:859–68.CrossRef

Shaulian, E. AP-1–The Jun proteins: oncogenes or tumor suppressors in disguise? Cellular Signaling 2010;22:894–9.

Hilberg, F, Aguzzi, A, Howells, N, Wagner, EF. c-Jun is essential for normal mouse development and hepatogenesis. Nature 1993;365:179–81 [published erratum appears in Nature 1993;366:368].

Eferl, R, Ricci, R, Kenner, L, et al. Liver tumor development. c-Jun antagonizes the proapoptotic activity of p53. Cell 2003;112:181–92.

Le-Niculescu, H, Bonfoco, E, Kasuya, Y, et al. Withdrawal of survival factors results in activation of the JNK pathway in neuronal cells leading to Fas ligand induction and cell death. Molecular and Cellular Biology 1999;19:751–63.CrossRef

Behrens, A, Sibilia, M, Wagner, EF. Amino-terminal phosphorylation of c-Jun regulates stress-induced apoptosis and cellular proliferation. Nature Genetics 1999;21:326–9.CrossRef

Gurzov, EN, Ortis, F, Bakiri, L, Wagner, EF, Eizirik, DL. JunB inhibits ER stress and apoptosis in pancreatic beta cells. PLoS ONE 2008;3:e3030.

Yogev, O, Goldberg, R, Anzi, S, Shaulian, E. Jun proteins are starvation-regulated inhibitors of autophagy. Cancer Research 2010;70:2318–27.CrossRef

Yogev, O, Shaulian, E. Jun proteins inhibit autophagy and induce cell death. Autophagy 2010;6(4):566–7.CrossRef

Saez, E, Rutberg, SE, Mueller, E, et al. c-fos is required for malignant progression of skin tumors. Cell 1995;82:721–32.CrossRef

Ozanne, BW, Spence, HJ, McGarry, LC, Hennigan, RF. Transcription factors control invasion: AP-1 the first among equals. Oncogene 2007;26:1–10.CrossRef

Reichmann, E, Schwarz, H, Deiner, EM, et al. Activation of an inducible c-FosER fusion protein causes loss of epithelial polarity and triggers epithelial-fibroblastoid cell conversion. Cell 1992;71:1103–16.CrossRef

Fialka, I, Schwarz, H, Reichmann, E, et al. The estrogen-dependent c-JunER protein causes a reversible loss of mammary epithelial cell polarity involving a destabilization of adherens junctions. Journal of Cell Biology 1996;132:1115–32.CrossRef Google Scholar PubMed

Vleugel, MM, Greijer, AE, Bos, R, van der Wall, E, van Diest, PJ. c-Jun activation is associated with proliferation and angiogenesis in invasive breast cancer. Human Pathology 2006;37:668–74.CrossRef

Zhang, G, Dass, CR, Sumithran, E, et al. Effect of deoxyribozymes targeting c-Jun on solid tumor growth and angiogenesis in rodents. Journal of the National Cancer Institute 2004;96:683–96.CrossRef Google Scholar PubMed

Damert, A, Ikeda, E, Risau, W. Activator-protein-1 binding potentiates the hypoxia-inducible factor-1-mediated hypoxia-induced transcriptional activation of vascular-endothelial growth factor expression in C6 glioma cells. Biochemical Journal 1997;327:419–23.CrossRef

Schmidt, D, Textor, B, Pein, OT, et al. Critical role for NF-kappaB-induced JunB in VEGF regulation and tumor angiogenesis. EMBO Journal 2007;26:710–19.CrossRef

Gerald, D, Berra, E, Frapart, YM, et al. JunD reduces tumor angiogenesis by protecting cells from oxidative stress. Cell 2004;118:781–94.CrossRef

Ruther, U, Garber, C, Komitowski, D, Muller, R, Wagner, EF. Deregulated c-Fos expression interferes with normal bone development in transgenic mice. Nature 1987;325:412–16.CrossRef

Ruther, U, Komitowski, D, Schubert, FR, Wagner, EF. c-Fos expression induces bone tumors in transgenic mice. Oncogene 1989;4:861–5.

Young, MR, Li, JJ, Rincon, M, et al. Transgenic mice demonstrate AP-1 (activator protein-1) transactivation is required for tumor promotion. Proceedings of the National Academy of Sciences USA 1999;96:9827–32.CrossRef

Behrens, A, Jochum, W, Sibilia, M, Wagner, EF. Oncogenic transformation by ras and fos is mediated by c-Jun N-terminal phosphorylation. Oncogene 2000;19:2657–63.CrossRef

Chang, Q, Zhang, Y, Beezhold, KJ, et al. Sustained JNK1 activation is associated with altered histone H3 methylations in human liver cancer. Journal of Hepatology 2009;50:323–33.CrossRef Google Scholar PubMed

Hui, L, Zatloukal, K, Scheuch, H, Stepniak, E, Wagner, EF. Proliferation of human HCC cells and chemically induced mouse liver cancers requires JNK1-dependent p21 downregulation. Journal of Clinical Investigation 2008;118:3943–53.CrossRef Google Scholar PubMed

Toualbi, K, Guller, MC, Mauriz, JL, et al. Physical and functional cooperation between AP-1 and beta-catenin for the regulation of TCF-dependent genes. Oncogene 2007;26:3492–502.CrossRef

Sancho, R, Nateri, AS, de Vinuesa, AG, et al. JNK signalling modulates intestinal homeostasis and tumourigenesis in mice. EMBO Journal 2009;28:1843–54.CrossRef

Nateri, AS, Spencer-Dene, B, Behrens, A. Interaction of phosphorylated c-Jun with TCF4 regulates intestinal cancer development. Nature 2005;437:281–5.CrossRef

Passegue, E, Jochum, W, Schorpp-Kistner, M, Mohle-Steinlein, U, Wagner, EF. Chronic myeloid leukemia with increased granulocyte progenitors in mice lacking junB expression in the myeloid lineage. Cell 2001;104:21–32.CrossRef

Passegue, E, Wagner, EF, Weissman, IL. JunB deficiency leads to a myeloproliferative disorder arising from hematopoietic stem cells. Cell 2004;119:431–43.CrossRef

Santaguida, M, Schepers, K, King, B, et al. JunB protects against myeloid malignancies by limiting hematopoietic stem cell proliferation and differentiation without affecting self-renewal. Cancer Cell 2009;15:341–52.CrossRef

Milde-Langosch, K. The Fos family of transcription factors and their role in tumourigenesis. European Journal of Cancer 2005;41:2449–61.CrossRef Google Scholar PubMed

Verde, P, Casalino, L, Talotta, F, Yaniv, M, Weitzman, JB. Deciphering AP-1 function in tumorigenesis: fra-ternizing on target promoters. Cell Cycle 2007;6:2633–9.CrossRef

Mariani, O, Brennetot, C, Coindre, JM, et al. JUN oncogene amplification and overexpression block adipocytic differentiation in highly aggressive sarcomas. Cancer Cell 2007;11:361–74.CrossRef

Mathas, S, Hinz, M, Anagnostopoulos, I, et al. Aberrantly expressed c-Jun and JunB are a hallmark of Hodgkin lymphoma cells, stimulate proliferation and synergize with NF-kappa B. EMBO Journal 2002;21:4104–13.CrossRef

Rassidakis, GZ, Thomaides, A, Atwell, C, et al. JunB expression is a common feature of CD30+ lymphomas and lymphomatoid papulosis. Modern Pathology 2005;18:1365–70.CrossRef

Mao, X, Orchard, G, Lillington, DM, et al. BCL2 and JUNB abnormalities in primary cutaneous lymphomas. British Journal of Dermatology 2004;151:546–56.CrossRef Google Scholar PubMed

Mao, X, Orchard, G, Lillington, DM, et al. Amplification and overexpression of JUNB is associated with primary cutaneous T-cell lymphomas. Blood 2003;101:1513–19.CrossRef

Staber, PB, Vesely, P, Haq, N, et al. The oncoprotein NPM-ALK of anaplastic large-cell lymphoma induces JUNB transcription via ERK1/2 and JunB translation via mTOR signaling. Blood 2007;110:3374–83.CrossRef

Yang, MY, Liu, TC, Chang, JG, Lin, PM, Lin, SF. JunB gene expression is inactivated by methylation in chronic myeloid leukemia. Blood 2003;101:3205–11.CrossRef

Steidl, U, Rosenbauer, F, Verhaak, RG, et al. Essential role of Jun family transcription factors in PU.1 knockdown-induced leukemic stem cells. Nature Genetics 2006;38:1269–77.CrossRef