Abstract

During development, tissues are sculpted into organs with precise forms and functions in a process called tissue morphogenesis. Tissue morphogenesis results from cellular forces that are transmitted across the tissue. Improper generation or coordination of forces leads to defects in organ formation, such as spina bifida. Therefore, it is critical to both our understanding of development and human disease to determine the mechanisms that control tissue morphogenesis at the molecular, cellular, and tissue level. Tissue invagination during gastrulation and neural tube closure is driven by apical constriction of epithelial cells. This causes columnar cells to adopt a wedge shape, which promotes folding of the epithelial sheet. We made the surprising discovery that apical constriction during Drosophila gastrulation is driven by pulsed contractions of the actin-myosin cytoskeleton. Contraction pulses have now been observed to promote many different morphogenetic processes, including tissue folding, contraction, and axis elongation. Our work has shown that the dynamic turnover of actomyosin that accompanies pulsing is critical to stably transmit force between cells. Furthermore, mutants in Cofilin, a gene involved in actin turnover, are associated with neural tube defects in mice and humans. The mechanisms that regulate actin turnover and enable forces to be transmitted across a tissue are unknown. We will investigate the mechanisms that enable forces to propagate across a tissue. First, we will determine the spatial and temporal function of actin cytoskeletal genes we have determined are important for force transmission. Second, we will examine how the apical contractile cortex is radially organized, which enables forces to be transmitted across a cell. Third, we will examine the supracellular actomyosin network that drives Drosophila gastrulation and determine how its organization contributes to developmental robustness. The availability of live imaging, quantitative image analysis, genetics (mutants, RNAi), cell biology (drugs), biophysics (laser cutting), and biochemistry makes Drosophila gastrulation a powerful system to address these questions. This multidisciplinary and multiscale approach is essential to understand how dynamic molecular and cellular behaviors collectively result in precise changes in tissue morphology. Members of my lab have backgrounds in cell biology, genetics, physics, and computer science. In addition, we have established collaborations with Mathematicians and experts in Mass Spectrometry to expand our research capabilities. We are poised to make important discoveries regarding forces are passed between cells to drive robust tissue morphogenesis.

Public Health Relevance

Understanding mechanisms of tissue morphogenesis is fundamental to understand birth defects. We will undertake a interdisciplinary approach to examine how mechanical forces are transmitted between cells to sculpt tissues during development. These studies promise to provide insight into how molecular and cellular behaviors are regulated and coordinated during the development of tissue shape.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM105984-07
Application #
9841942
Study Section
Development - 2 Study Section (DEV2)
Program Officer
Hoodbhoy, Tanya
Project Start
2013-05-01
Project End
2022-12-31
Budget Start
2020-01-01
Budget End
2020-12-31
Support Year
7
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Massachusetts Institute of Technology
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
001425594
City
Cambridge
State
MA
Country
United States
Zip Code
02142

  Publications

Coravos, Jonathan S; Mason, Frank M; Martin, Adam C (2017) Actomyosin Pulsing in Tissue Integrity Maintenance during Morphogenesis. Trends Cell Biol 27:276-283
Chanet, Soline; Miller, Callie J; Vaishnav, Eeshit Dhaval et al. (2017) Actomyosin meshwork mechanosensing enables tissue shape to orient cell force. Nat Commun 8:15014
Heer, Natalie C; Miller, Pearson W; Chanet, Soline et al. (2017) Actomyosin-based tissue folding requires a multicellular myosin gradient. Development 144:1876-1886
Heer, Natalie C; Martin, Adam C (2017) Tension, contraction and tissue morphogenesis. Development 144:4249-4260
Vasquez, Claudia G; Martin, Adam C (2016) Force transmission in epithelial tissues. Dev Dyn 245:361-71
Xie, Shicong; Mason, Frank M; Martin, Adam C (2016) Loss of G?12/13 exacerbates apical area dependence of actomyosin contractility. Mol Biol Cell 27:3526-3536
Jodoin, Jeanne N; Martin, Adam C (2016) Abl suppresses cell extrusion and intercalation during epithelium folding. Mol Biol Cell 27:2822-32
Vasquez, Claudia G; Heissler, Sarah M; Billington, Neil et al. (2016) Drosophila non-muscle myosin II motor activity determines the rate of tissue folding. Elife 5:
Coravos, Jonathan S; Martin, Adam C (2016) Apical Sarcomere-like Actomyosin Contracts Nonmuscle Drosophila Epithelial Cells. Dev Cell 39:346-358
Rodal, Avital A; Del Signore, Steven J; Martin, Adam C (2015) Drosophila comes of age as a model system for understanding the function of cytoskeletal proteins in cells, tissues, and organisms. Cytoskeleton (Hoboken) 72:207-24

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