Developmental responses to nutrient stress reflect systems-level regulation -- the entire animal and its progeny can be affected. But how developmental physiology is coordinated across the animal and over generations is not well understood. The long-term goal of this project is to understand the molecular basis of persistent effects of nutrient stress in the roundworm C. elegans. The worm is an ideal model since it has evolved to thrive in feast and famine and its short generation time facilitates multigenerational studies. Preliminary results show that larval starvation causes germline tumors to develop during early adulthood (intragenerational effect), but that reduction of insulin/IGF signaling suppresses tumors by promoting ferroptosis. They also show that mater- nal dietary restriction protects progeny from starvation-induced tumors by reducing insulin/IGF signaling (inter- generational effect). Our studies also demonstrate epigenetic inheritance of increased starvation resistance and lifespan as well as altered gene expression following dauer arrest (transgenerational effect), and they sug- gest that small RNAs in the germ line mediate these effects. These preliminary results lay the foundation for mechanistic analysis of persistent effects of nutrient stress during development and across generations. The premise of this proposal is that early-life starvation compromises developmental integrity, but parental or an- cestral nutrient stress buffers progeny from starvation. The central hypothesis is that early-life starvation leads to development of adult germline tumors, but maternal provisioning and epigenetic inheritance protect progeny from such pathological effects of starvation. The objectives are to identify signaling and gene regulatory mech- anisms that mediate adaptation to nutrient stress across generations. The central hypothesis is supported by strong preliminary data as well as the literature. It will be tested with the following three aims: 1) Identify mech- anisms by which reduction of insulin/IGF signaling suppresses starvation-induced germline tumors, 2) Identify mechanisms by which maternal dietary restriction buffers progeny from pathological effects of early-life starva- tion, and 3) Identify regulatory mechanisms that mediate epigenetic inheritance of starvation resistance. Genet- ic, genomic, pharmacological and biochemical approaches will be used to complete these aims. This work is innovative for developing models that facilitate mechanistic analysis of intra-, inter- and transgenerational ef- fects of nutrient stress and for investigating ferroptosis as a tumor suppressor mechanism regulated by a FoxO transcription factor and insulin/IGF signaling. The contributions of the proposed work will be identification of regulatory mechanisms that mediate adaptation to nutrient stress across generations. These include mecha- nisms by which FoxO transcription factors suppress tumors as well as mechanisms for inheritance of starvation resistance. These contributions will be significant because they will fill critical gaps in understanding of how nutrient stress affects development, maternal provisioning, and epigenetic inheritance. The deeply conserved function of insulin/IGF signaling and FoxO factors suggests that mechanisms discovered will be conserved.

Public Health Relevance

The proposed research is relevant to public health given the paramount importance of nutrition on health and disease. Dysregulation of nutrient sensing pathways causes cancer and diabetes, and there is mounting evidence that diet affects disease risk across generations. This work will increase fundamental understanding of how animals adapt to nutrient stress, suggesting preventive strategies and therapeutic interventions to reduce public health burden.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM117408-06
Application #
9993538
Study Section
Cellular Mechanisms in Aging and Development Study Section (CMAD)
Program Officer
Gaillard, Shawn R
Project Start
2015-09-18
Project End
2023-08-31
Budget Start
2020-09-01
Budget End
2021-08-31
Support Year
6
Fiscal Year
2020
Total Cost
Indirect Cost
Name
Duke University
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
044387793
City
Durham
State
NC
Country
United States
Zip Code
27705
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Webster, Amy K; Jordan, James M; Hibshman, Jonathan D et al. (2018) Transgenerational Effects of Extended Dauer Diapause on Starvation Survival and Gene Expression Plasticity in Caenorhabditis elegans. Genetics 210:263-274
Burton, Nicholas O; Dwivedi, Vivek K; Burkhart, Kirk B et al. (2018) Neurohormonal signaling via a sulfotransferase antagonizes insulin-like signaling to regulate a Caenorhabditis elegans stress response. Nat Commun 9:5152
Burton, Nicholas O; Furuta, Tokiko; Webster, Amy K et al. (2017) Insulin-like signalling to the maternal germline controls progeny response to osmotic stress. Nat Cell Biol 19:252-257
Hibshman, Jonathan D; Doan, Alexander E; Moore, Brad T et al. (2017) daf-16/FoxO promotes gluconeogenesis and trehalose synthesis during starvation to support survival. Elife 6:
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Hibshman, Jonathan D; Hung, Anthony; Baugh, L Ryan (2016) Maternal Diet and Insulin-Like Signaling Control Intergenerational Plasticity of Progeny Size and Starvation Resistance. PLoS Genet 12:e1006396
Kaplan, Rebecca E W; Chen, Yutao; Moore, Brad T et al. (2015) dbl-1/TGF-? and daf-12/NHR Signaling Mediate Cell-Nonautonomous Effects of daf-16/FOXO on Starvation-Induced Developmental Arrest. PLoS Genet 11:e1005731