JSAP1, a Novel Jun N-Terminal Protein Kinase (JNK)-Binding Protein That Functions as a Scaffold Factor in the JNK Signaling Pathway

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Molecular and Cellular Biology, November 1999, p. 7539-7548, Vol. 19, No. 11
0270-7306/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.

JSAP1, a Novel Jun N-Terminal Protein Kinase (JNK)-Binding Protein That Functions as a Scaffold Factor in the JNK Signaling Pathway

Michihiko Ito,¹ Katsuji Yoshioka,²^,^* Mizuho Akechi,¹ Shinya Yamashita,³ Nobuhiko Takamatsu,¹ Kenji Sugiyama,⁴ Masahiko Hibi,⁵ Yusaku Nakabeppu,⁶ Tadayoshi Shiba,¹ and Ken-Ichi Yamamoto²

Department of Biosciences, School of Science, Kitasato University, Kanagawa 228,¹ Department of Molecular Pathology, Cancer Research Institute, Kanazawa University, Kanazawa 920,² Central Research Laboratory, Nippon Suisan Kaisha Ltd., Tokyo 192,³ Nippon Boehringer Ingelheim Co., Ltd., Kawanishi Pharma Research Institute, Department of Molecular and Cellular Biology, Hyogo 666,⁴ Department of Molecular Oncology, Biomedical Research Center, Osaka University Medical School, Osaka 565,⁵ and Department of Biochemistry, Medical Institute of Bioregulation, Kyushu University, and CREST, Japan Science and Technology, Fukuoka 812,⁶ Japan

Received 17 June 1999/Returned for modification 28 July 1999/Accepted 12 August 1999

The major components of the mitogen-activated protein kinase (MAPK) cascades are MAPK, MAPK kinase (MAPKK), and MAPKK kinase(MAPKKK). Recent rapid progress in identifying members of MAPKcascades suggests that a number of such signaling pathways existin cells. To date, however, how the specificity and efficiencyof the MAPK cascades is maintained is poorly understood. Here,we have identified a novel mouse protein, termed Jun N-terminalprotein kinase (JNK)/stress-activated protein kinase-associatedprotein 1 (JSAP1), by a yeast two-hybrid screen, using JNK3 MAPKas the bait. Of the mammalian MAPKs tested (JNK1, JNK2, JNK3,ERK2, and p38 $alpha$ ), JSAP1 preferentially coprecipitated with theJNKs in cotransfected COS-7 cells. JNK3 showed a higher bindingaffinity for JSAP1, compared with JNK1 and JNK2. In similar cotransfectionstudies, JSAP1 also interacted with SEK1 MAPKK and MEKK1 MAPKKK,which are involved in the JNK cascades. The regions of JSAP1 thatbound JNK, SEK1, and MEKK1 were distinct from one another. JNKand MEKK1 also bound JSAP1 in vitro, suggesting that these interactionsare direct. In contrast, only the activated form of SEK1 associatedwith JSAP1 in cotransfected COS-7 cells. The unstimulated SEK1bound to MEKK1; thus, SEK1 might indirectly associate with JSAP1through MEKK1. Although JSAP1 coprecipitated with MEK1 MAPKK andRaf-1 MAPKKK, and not MKK6 or MKK7 MAPKK, in cotransfected COS-7cells, MEK1 and Raf-1 do not interfere with the binding of SEK1and MEKK1 to JSAP1, respectively. Overexpression of full-lengthJSAP1 in COS-7 cells led to a considerable enhancement of JNK3activation, and modest enhancement of JNK1 and JNK2 activation,by the MEKK1-SEK1 pathway. Deletion of the JNK- or MEKK1-bindingregions resulted in a significant reduction in the enhancementof the JNK3 activation in COS-7 cells. These results suggest thatJSAP1 functions as a scaffold protein in the JNK3 cascade. Wealso discuss a scaffolding role for JSAP1 in the JNK1 and JNK2cascades.

^* Corresponding author. Mailing address: Department of Molecular Pathology, Cancer Research Institute, Kanazawa University,13-1 Takaramachi, Kanazawa 920-0934, Japan. Phone: 81-76-265-2757.Fax: 81-76-234-4517. E-mail: katsuji{at}kenroku.kanazawa-u.ac.jp.

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