Using the Drosophila embryo as a model system, we have the exceptional opportunity to investigate how multiple cis-regulatory modules (CRMs) cooperate to support spatiotemporally-regulated gene expression during the course of development. In studies supported by the parent grant, we found that the Dorsal transcription factor, which is instrumental for patterning the dorsal-ventral (DV) axis, exhibits dynamics as do its target genes. Significant changes in levels of Dorsal and its target genes were observed both between as well as within each nuclear cycle, on the order of minutes. Chromatin immunoprecipitation experiments were also conducted to examine in vivo DNA occupancy by transcription factors, important for embryonic patterning. These experiments showed that many genes in the embryo are regulated by pairs of concurrently active cis-regulatory modules (CRMs) that drive expression in similar spatiotemporal patterns. The experiments proposed here aim to understand why and how multiple CRMs coordinate to control spatiotemporal gene expression in the Drosophila embryo, and, in particular, to provide insight into how transfer of activity from one CRM to the next is regulated to support developmental progression. We will capitalize on ample background information and our knowledge of DV patterning to help guide choice of particularly relevant cis-regulatory systems for study. Many molecular and genetic tools are available to support these studies in Drosophila, including ease of genetic approaches as well as the ability to manipulate large transgenes through recombineering, that facilitate functional assays of CRMs and other regulatory sequences in native context. Also, we will investigate the impact of chromatin conformation on gene expression using standard techniques (3C) as well as a novel imaging approach we are developing, to provide insight into when and how particular CRMs interact with the promoter with temporal and spatial resolution. Here in this renewal application we propose three specific aims that will significantly advance our understanding of how CRM coordinate to support developmental gene expression:
Aim 1 - To analyze how transition from one CRM to the next supports continuous gene expression.
Aim 2 - To investigate the relationship between gene expression dynamics, boundaries, and levels.
Aim 3 - To assay chromatin conformation in vivo on a cell-by-cell basis. Carefully timed and spatially controlled expression of genes is required for normal development to proceed. As roughly a third of all CRMs controlling dorsal-ventral patterning may function as 'coordinate pairs', we argue that co-regulation of gene expression by integrative function of multiple CRMs is likely a general mechanism of cis-regulatory control;one that is just beginning to come to light. Splitting cis-regulatory information across multiple modules that jointly influence gene expression may provide flexibility of output that can be advantageous, especially for the developing embryo that is presented with genetic perturbation and/or changing environmental conditions. The conservation of gene regulatory mechanisms across all animals promises that these studies will have far reaching implications.

Public Health Relevance

Understanding how gene expression is regulated is at the heart of our understanding of development and disease. Carefully timed and spatially controlled expression of genes is required for normal development to proceed. Our preliminary studies of dorsal-ventral patterning in the Drosophila early embryo have led us to investigate how cis-regulatory modules coordinate to support spatiotemporal patterning in the face of dynamic changes in transcription factor levels. The conservation of gene regulatory mechanisms across all animals promises that these studies will have far reaching implications.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM077668-07
Application #
8729585
Study Section
Development - 2 Study Section (DEV2)
Program Officer
Hoodbhoy, Tanya
Project Start
2007-03-01
Project End
2017-05-31
Budget Start
2014-06-01
Budget End
2015-05-31
Support Year
7
Fiscal Year
2014
Total Cost
$316,350
Indirect Cost
$126,350
Name
California Institute of Technology
Department
Type
Schools of Arts and Sciences
DUNS #
009584210
City
Pasadena
State
CA
Country
United States
Zip Code
91125
Koromila, Theodora; Stathopoulos, Angelike (2017) Broadly expressed repressors integrate patterning across orthogonal axes in embryos. Proc Natl Acad Sci U S A :
Sandler, Jeremy E; Stathopoulos, Angelike (2016) Stepwise Progression of Embryonic Patterning. Trends Genet 32:432-443
Sandler, Jeremy E; Stathopoulos, Angelike (2016) Quantitative Single-Embryo Profile of Drosophila Genome Activation and the Dorsal-Ventral Patterning Network. Genetics 202:1575-84
Ozdemir, Anil; Ma, Lijia; White, Kevin P et al. (2014) Su(H)-mediated repression positions gene boundaries along the dorsal-ventral axis of Drosophila embryos. Dev Cell 31:100-13
Stathopoulos, Angelike; Iber, Dagmar (2013) Studies of morphogens: keep calm and carry on. Development 140:4119-24
Dunipace, Leslie; Saunders, Abbie; Ashe, Hilary L et al. (2013) Autoregulatory feedback controls sequential action of cis-regulatory modules at the brinker locus. Dev Cell 26:536-43
Garcia, Mayra; Nahmad, Marcos; Reeves, Gregory T et al. (2013) Size-dependent regulation of dorsal-ventral patterning in the early Drosophila embryo. Dev Biol 381:286-99
Jin, Hong; Stojnic, Robert; Adryan, Boris et al. (2013) Genome-wide screens for in vivo Tinman binding sites identify cardiac enhancers with diverse functional architectures. PLoS Genet 9:e1003195
Trisnadi, Nathanie; Altinok, Alphan; Stathopoulos, Angelike et al. (2013) Image analysis and empirical modeling of gene and protein expression. Methods 62:68-78
Reeves, Gregory T; Trisnadi, Nathanie; Truong, Thai V et al. (2012) Dorsal-ventral gene expression in the Drosophila embryo reflects the dynamics and precision of the dorsal nuclear gradient. Dev Cell 22:544-57

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