The Notch signaling pathway is remarkably important for the development and maintenance of most complex tissues in multicellular organisms and defective Notch signaling has been implicated in severe developmental defects and cancer. Understanding the basic mechanisms and functions of Notch is imperative to developing therapies for Notch-related diseases. Notch is a single-pass transmembrane receptor that, upon activation by a ligand, is cleaved in the transmembrane domain to release the intracellular domain into the cytoplasm. The free intracellular domain translocates to the nucleus where it forms a ternary protein complex to promote target gene transcription and influence cell fate and function. The Notch intracellular domain is difficult to visualize directly because the free intracellular domain is rapidly degraded, but manipulations affecting the stability or level of the intracellular domain cause cell fate transformations, complicating studies of signaling onset, duration, and dynamics. Thus, Notch activity has been assessed using target gene transcriptional reporters, which are limited by time lags due to transcription, translation, and fluorescent protein maturation, as well as perdurance of reporter proteins after signaling has ceased. Preliminary data shows that a Sensor Able to detect Lateral Signaling Activity, or SALSA, is a promising novel, rapid-response, in vivo biosensor of Notch activity. SALSA is a bipartite system consisting of a ?switch? in which the Notch locus is endogenously tagged with a protease, and a cleavable, dual-fluorescent protein reporter. When Notch is activated, the protease- tagged intracellular domain translocates to the nucleus where the protease cleaves the reporter and that allows the individual fluorescent proteins to be localized to different cellular compartments. This project will 1) establish a protocol for quantifying the level of Notch activity using SALSA. This protocol will be established in model organism C. elegans because of the speed of generating transgenic lines, the ability to image the entire organism in vivo throughout its lifecycle, and the well conserved and characterized Notch signaling events. This project will then 2) use SALSA to determine how the timing and levels of Notch activity influence cell fate decisions in two paradigms for Notch signaling in C. elegans: the Vulval Precursor Cells and the Anchor Cell/Ventral Uterine precursor cell decision in the somatic gonad. Results from this project will establish a useful tool for studying many aspects of Notch signaling in a variety of contexts, and provide insight into a universal relationship between the timing and levels of Notch activity with cell fate decisions.

Public Health Relevance

Notch signaling is essential for human development and aberrant Notch signaling has been implicated in a multitude of diseases including ocular diseases, cardiovascular diseases, and cancer. Understanding the basic mechanisms and functions of Notch signaling can reveal potential avenues to develop therapeutics for these diseases. This project will develop a novel, genetically-encoded, rapid-response Notch biosensor to study Notch signaling and use it to explore the relationship between signaling dynamics and cell fate outcomes.

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Predoctoral Individual National Research Service Award (F31)
Project #
1F31EY030331-01A1
Application #
9910619
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Agarwal, Neeraj
Project Start
2019-12-16
Project End
2021-12-15
Budget Start
2019-12-16
Budget End
2020-12-15
Support Year
1
Fiscal Year
2020
Total Cost
Indirect Cost
Name
Columbia University (N.Y.)
Department
Biology
Type
Graduate Schools
DUNS #
049179401
City
New York
State
NY
Country
United States
Zip Code
10027