Riding the neural crest

During the fourth week of human embryonic development, in the ridges of the closing neural tube, a remarkable group of cells emerges.

Named for their birthplace, these “neural crest” cells journey to sites near and far in the developing embryo, where they form a wide array of tissues, including the peripheral nervous system, facial skeleton and melanocytes in the skin.

The fate of an individual neural crest cell – what it becomes – relates to both its starting position (top-to-bottom) along the neural tube and to its migration path, explains Michelle Southard-Smith, Ph.D.

She’s interested in the cells that trek from the neural tube ridges into the future gut and along the length of the developing intestine. There, they form the neurons and glia of the enteric nervous system – the “brain” of the gut that controls motility, mucosal transport, tissue defense and vascular perfusion of the gastrointestinal tract.

“These cells have the longest neural crest migration that occurs in the developing embryo,” says Southard-Smith, assistant professor of Medicine and Cell & Developmental Biology at Vanderbilt. “Variations that impair the ability of those neural crest cells to complete the migration or to survive and become functional neurons and glia in the gut wall can cause gastrointestinal disorders like Hirschsprung’s disease.”

Patients with Hirschsprung’s disease are missing enteric ganglia (nerve bundles) in the intestine, causing constipation and blockages and requiring surgical intervention. Hirschsprung’s occurs in one out of every 5,000 live births in the United States and can be fatal.

The severity of the disease depends on how much of the large intestine is affected – how successful, or not, the neural crest cells were in migrating through and populating the gut, Southard-Smith explains.

The migration of neural crest-derived cells in the developing gut is revealed in a transgenic mouse embryo by the Cerulean Fluorescent Protein, a marker of Phox2b expression. The transcription factor Phox2b, a “master regulator,” guides development of the enteric nervous system, which controls motility and other functions of the gut. By tracking the migration of early nerve progenitors that express Phox2b, scientists hope to be able to identify, and eventually correct, abnormalities that can cause disorders in GI function in humans.

This image, magnified 48.5 times, was captured by research assistant Ashley Cantrell using a confocal microscope. Courtesy of Michelle Southard-Smith, Ph.D.

Reprinted from Developmental Dynamics, Vol. 237, No. 4, 2008, pages 1119-1132. Copyright 2008, John Wiley & Sons, Inc.
Reprinted with permission of Wiley-Liss, Inc., a subsidiary of John Wiley & Sons, Inc.

To explore how neural crest cells migrate and make decisions about their fate, Southard-Smith and colleagues have developed genetically engineered mice using two genes important for enteric nervous system development, Sox10 and Phox2b, to drive the expression of fluorescent proteins. In these mice, the neural crest cells that populate the enteric nervous system “glow” a vibrant blue-green.

Following the glowing cells with imaging technologies has already revealed a surprise: differences between neurons and glia are evident when the neural crest cells are just starting their journey to the gut, suggesting that cells make fate decisions earlier than scientists believed, Southard-Smith says.

In addition to tracking cells as they migrate, the researchers are capturing the glowing cells and culturing them in the laboratory. The aim is to understand how the cells respond to various growth factors and to evaluate their ability to form enteric nerves and glia after transplantation into a mouse model of Hirschsprung’s disease.

Ultimately, the research could offer treatment options for patients with the disease, Southard-Smith says.

“There are neural crest cells in skin – we’re hoping to take them out and reprogram them with cues to make them become enteric neurons and glia,” she says. “That’s where we’re going with this.”