Abstract

An ability to sense and respond to diverse stress stimuli from the environment is a basic cellular function conserved throughout evolution. In unicellular organisms, such responses are critical for survival. In higher organisms including humans, cellular stress responses can be seen in the inflammation resulting from asthma, arthritis, or bacterial infection, as well as in the response of cancer cells to cytotoxic therapies. In order to sense stress stimuli and regulate cellular physiology, eukaryotic organisms from yeast to humans utilize a signaling module called a MAP kinase (MAPK) cascade. MAPKs dedicated for stress signaling are also known as SAPKs (Stress-Activated Protein Kinases) and play key roles in cellular responses to changes in the environmental conditions as well as responses to bacterial endotoxins, inflammatory cytokines, and chemotherapeutic drugs. The long-term objective of the research described in this proposal is to understand at a molecular level how diverse stress stimuli are sensed and transmitted to SAPK, and how activated SAPK then modulates cellular processes for stress adaptation. These studies will use the genetically tractable model system provided by the fission yeast Schizosaccharomyces pombe, whose SAPK pathway has been demonstrated to be structurally and functionally similar to those in humans. Signaling within MAPK cascades is achieved by sequential activation of a MAPK kinase kinase (MAPKKK), a MAPK kinase (MAPKK) and finally, a MAPK. In the S. pombe SAPK cascade, signaling to the Spcl SAPK is initiated by two MAPKKKs, Wis4 and Win1. We have found that Wis4 and Win1 form a complex with multiple proteins and serve as a hub for stress sensing and response via the Spc1 pathway. The three specific aims focus on this MAPKKK complex: (I) to determine how the complex is organized and discover novel proteins that interact with Wis4 and Win1; (II) to uncover how oxidative stress signaling to the SAPK cascade is mediated by a glycolytic enzyme, GAPDH, which has unexpectedly been found as a component of the MAPKKK complex; and (iii) to determine how another MAPKKK-interacting protein, Wsh3, regulates a newly discovered cellular function of the SAPK pathway, the maintenance of cell polarity under high similarity stress. It is anticipated that the proposed SAPK research in S. pombe will serve as a valuable paradigm for human SAPK, facilitating understanding of the roles of SAPKs in clinical contexts.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM059788-08
Application #
7104325
Study Section
Cell Development and Function Integrated Review Group (CDF)
Program Officer
Anderson, Richard A
Project Start
1999-08-01
Project End
2008-08-31
Budget Start
2006-09-01
Budget End
2007-08-31
Support Year
8
Fiscal Year
2006
Total Cost
$254,076
Indirect Cost

  Institution

Name
University of California Davis
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
047120084
City
Davis
State
CA
Country
United States
Zip Code
95618

  Publications

Morigasaki, Susumu; Ikner, Aminah; Tatebe, Hisashi et al. (2013) Response regulator-mediated MAPKKK heteromer promotes stress signaling to the Spc1 MAPK in fission yeast. Mol Biol Cell 24:1083-92
Morigasaki, Susumu; Shiozaki, Kazuhiro (2010) Two-component signaling to the stress MAP kinase cascade in fission yeast. Methods Enzymol 471:279-89
Tatebe, Hisashi; Shiozaki, Kazuhiro (2010) Rab small GTPase emerges as a regulator of TOR complex 2. Small GTPases 1:180-182
Tatebe, Hisashi; Morigasaki, Susumu; Murayama, Shinichi et al. (2010) Rab-family GTPase regulates TOR complex 2 signaling in fission yeast. Curr Biol 20:1975-82
Shiozaki, Kazuhiro (2009) Nutrition-minded cell cycle. Sci Signal 2:pe74
Ikeda, Kyoko; Morigasaki, Susumu; Tatebe, Hisashi et al. (2008) Fission yeast TOR complex 2 activates the AGC-family Gad8 kinase essential for stress resistance and cell cycle control. Cell Cycle 7:358-64
Tatebe, Hisashi; Nakano, Kentaro; Maximo, Rachel et al. (2008) Pom1 DYRK regulates localization of the Rga4 GAP to ensure bipolar activation of Cdc42 in fission yeast. Curr Biol 18:322-30
Morigasaki, Susumu; Shimada, Koichi; Ikner, Aminah et al. (2008) Glycolytic enzyme GAPDH promotes peroxide stress signaling through multistep phosphorelay to a MAPK cascade. Mol Cell 30:108-13
Wang, Ling-yu; Shiozaki, Kazuhiro (2006) The fission yeast stress MAPK cascade regulates the pmp3+ gene that encodes a highly conserved plasma membrane protein. FEBS Lett 580:2409-13
Tatebe, Hisashi; Shimada, Koichi; Uzawa, Satoru et al. (2005) Wsh3/Tea4 is a novel cell-end factor essential for bipolar distribution of Tea1 and protects cell polarity under environmental stress in S. pombe. Curr Biol 15:1006-15

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