Abstract

Cellular damage caused by oxidative stress is central to the pathology of a wide variety of diseases. Mammalian cells defend against oxidative stress through a conserved transcriptional response in which the Nrf proteins induce expression of Phase II detoxification enzyme genes. Much remains to be learned about how this oxidative stress defense is controlled, and might be harnessed therapeutically. In the nematode C. elegans, we have shown that this oxidative stress response is orchestrated by the SKN-1 transcription factor, which is related to Nrf proteins. In the embryo, maternally provided SKN-1 initiates development of the feeding/digestive system. We have found that during postembryonic stages SKN-1 is expressed in the intestine and ASI chemosensory neurons, and is required for resistance to oxidative stress and for normal longevity. We have also obtained the novel and exciting observation that in the intestine SKN-1 localization is regulated by p38, GSK-3, and insulin-like signaling, apparently through direct SKN-1 phosphorylation. Our findings indicate that SKN-1 integrates multiple stress and metabolic inputs, and provide a valuable whole-organism model for studying this stress response. In the new project, we will investigate how these signals regulate SKN-1 and its functions, and employ advantages of C. elegans to identify additional mechanisms that control this stress response.
In Aim 1, we will determine how expression of SKN-1 in different tissues contributes to its functions, and we will test models for how SKN-1 is regulated in the intestine, including the exciting hypothesis that one SKN-1 form responds to mitochondrial stress.
In Aim 2 we will study how insulin-like signaling regulates SKN-1, and how SKN-1 influences biological effects of insulin-like signaling.
In Aim 3, we will use microarrays to identify additional SKN-1 target genes and functions, and RNA interference screening to identify novel mechanisms that regulate SKN-1. This work will greatly expand our understanding of how this oxidative stress response is regulated, and of the biological functions of the protein that orchestrates this response. Lay Summary: Oxidative stress (excessive levels of cellular free radicals) is important in many diseases, including diabetes, atherosclerosis, and cancer. A new means of combating oxidative stress would be to harness innate cellular mechanisms that can defend against it. In this project, we will use a simple nematode model to identify and study mechanisms that control this stress defense, and to investigate how this stress defense contributes to important biological processes that include responses to insulin.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
3R01GM062891-08S1
Application #
7675490
Study Section
Molecular Genetics B Study Section (MGB)
Program Officer
Anderson, James J
Project Start
2001-09-03
Project End
2009-11-30
Budget Start
2007-12-01
Budget End
2008-11-30
Support Year
8
Fiscal Year
2008
Total Cost
$29,489
Indirect Cost

  Institution

Name
Joslin Diabetes Center
Department
Type
DUNS #
071723084
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Ewald, Collin Yvès; Castillo-Quan, Jorge Iván; Blackwell, T Keith (2018) Untangling Longevity, Dauer, and Healthspan in Caenorhabditis elegans Insulin/IGF-1-Signalling. Gerontology 64:96-104
Yoon, Dong Suk; Choi, Yoorim; Cha, Dong Seok et al. (2017) Triclosan Disrupts SKN-1/Nrf2-Mediated Oxidative Stress Response in C. elegans and Human Mesenchymal Stem Cells. Sci Rep 7:12592
Ewald, Collin Yvès; Hourihan, John M; Bland, Monet S et al. (2017) NADPH oxidase-mediated redox signaling promotes oxidative stress resistance and longevity through memo-1 in C. elegans. Elife 6:
Lee, Gina; Zheng, Yuxiang; Cho, Sungyun et al. (2017) Post-transcriptional Regulation of De Novo Lipogenesis by mTORC1-S6K1-SRPK2 Signaling. Cell 171:1545-1558.e18
Ogawa, Takahiro; Kodera, Yukihiro; Hirata, Dai et al. (2016) Natural thioallyl compounds increase oxidative stress resistance and lifespan in Caenorhabditis elegans by modulating SKN-1/Nrf. Sci Rep 6:21611
Isik, Meltem; Blackwell, T Keith; Berezikov, Eugene (2016) MicroRNA mir-34 provides robustness to environmental stress response via the DAF-16 network in C. elegans. Sci Rep 6:36766
Steinbaugh, Michael J; Narasimhan, Sri Devi; Robida-Stubbs, Stacey et al. (2015) Lipid-mediated regulation of SKN-1/Nrf in response to germ cell absence. Elife 4:
Blackwell, T Keith; Steinbaugh, Michael J; Hourihan, John M et al. (2015) SKN-1/Nrf, stress responses, and aging in Caenorhabditis elegans. Free Radic Biol Med 88:290-301
Ewald, Collin Y; Landis, Jess N; Porter Abate, Jess et al. (2015) Dauer-independent insulin/IGF-1-signalling implicates collagen remodelling in longevity. Nature 519:97-101
Moroz, Natalie; Carmona, Juan J; Anderson, Edward et al. (2014) Dietary restriction involves NAD? -dependent mechanisms and a shift toward oxidative metabolism. Aging Cell 13:1075-85

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