跳转到主内容

非常抱歉,我们不完全支持您的浏览器。如果您可以选择,请升级到较新版本或使用 Mozilla Firefox、Microsoft Edge、Google Chrome 或 Safari 14 或更高版本。如果您无法进行此操作且需要支持,请将您的反馈发送给我们。

全新设计的官网为您带来全新体验,期待您的反馈 在新的选项卡/窗口中打开

Elsevier
通过我们出版

Conference speaker

Amy E. Shyer

AES

Amy E. Shyer

The Rockefeller University, USA

During development, cells must arrange into particular tissue patterns in order to  order to become functional organs. Shyer studies the emergence of biological form, or morphogenesis, using the chicken embryo as a model system. By focusing on physical dynamics, the lab is able to gain insight into critical symmetry-breaking events that control how tissues and organs take shape. 

As an organism develops, homogenous tissues gradually give rise to complex morphological features. Understanding this process is crucial to enhancing fundamental knowledge about development. In recent decades, the prominence of genetic models has led to an assumption that patterns of gene expression, more than any other factor, govern tissue formation. Taking an alternative course, the Shyer lab focuses on the mechanical forces that influence morphogenesis. Her team takes an integrative approach to developmental biology, melding physical and molecular perspectives.

To better understand the dynamics of morphogenesis, the lab measures and perturbs physical aspects of cells in chicken embryos. The group conducts experiments in eggs, whole tissue explants, and primary cells extracted from embryos. Using these techniques, Shyer seeks to determine whether, given the appropriate physical and chemical contexts, researchers can reconstitute tissue dynamics from cellular components. The emergence of feather follicles in birds is analogous to that of hair follicles in mammals. The Shyer lab therefore uses avian skin as a model for investigating questions about pattern formation that may be relevant in human skin. An applied goal of the lab is to uncover tactics for generating lab-grown tissues that more faithfully mimic their natural counterparts. Though scientists can already generate tissue from cultured cells, these products have limited clinical usefulness because they often fail to develop important morphological features. For example, skin grafts made from cultured cells using existing techniques do not form hair follicles or sweat glands—a shortcoming that may cause health issues if used to replace damaged skin. A lack of sweat glands, for instance, can lead to problems with thermoregulation. Previously, Shyer and co-author Alan Rodrigues showed that avian follicle morphology and gene expression patterns depend on contractility-driven cellular mechanics. These findings corroborate the scientists’ view that mechanical processes can precede and trigger gene-expression changes that are cell fate-determining. Shyer and Rodrigues ultimately aim to build unified models that integrate mechanical and molecular perspectives of morphogenesis. To test the generality of these mechanisms, they hope to explore whether other tissue types demonstrate patterning dynamics similar to those observed in skin.