Eine Mutation namens Magellan steuert Nervenzellen vom Kurs ab

21. November 2007

Eine Mutation namens Magellan steuert Nervenzellen vom Kurs ab

21. November 2007

La Jolla, CA – Frisch geschlüpfte Nervenzellen in einem wachsenden Embryo müssen ihren Weg zu entfernten Zielen finden, und viele der Mittel, die sie zur Navigation einsetzen, sind noch nicht aufgetaucht. In einer Studie, die in der aktuellen Ausgabe der Zeitschrift veröffentlicht wurde Neuron, Wissenschaftler am Salk Institute for Biological Studies haben ein wichtiges Signal identifiziert, das die Motoneuronen steuert – die entstehenden Zellen, die sich vom Rückenmark aus erstrecken und ihren Weg über die Gliedmaßen wie Arme, Flügel und Beine finden müssen.

The Salk study, led by Samuel Pfaff, Ph.D, a professor in the Gene Expression Laboratory, identifies a mutation they christened Magellan, after the Portuguese mariner whose ship Victoria was first to circumnavigate the globe. The Magellan mutation occurs in a gene that normally pilots motor neurons on the correct course employing a newly discovered mechanism, their results demonstrate.

In the mutants, growing neurons can be seen leaving the spinal cord normally but then appear to lose direction. The elongating cells develop “kinks” and sometimes fold back on themselves or become entwined in a spiral, forming coils outside the spinal cord. “They appear to become lost in a traffic roundabout,” described Pfaff, who observed the growing neurons with fluorescent technology.

Understanding how motor neurons reach the appropriate targets is necessary for the implementation of novel therapies, including embryonic stem cell replacement for the treatment of presently incurable disorders such as Lou Gehrig’s disease, in which motor neurons undergo irreversible decay.

“Embryonic studies provide useful insights on how to replicate the system in an adult,” said Pfaff. And, as he also pointed out, the mechanisms used by motor neurons are likely to be similar to those used in other parts of the central nervous system, such as the brain. The Magellan mutation discovered by Pfaff’s group was found in mice, but the affected gene, called Phr1, has also been identified in other model systems, including fruit flies and the worm species C. elegans.

A growing nerve bears at its bow a structure called the growth cone, a region rich in the receptor molecules whose job is to receive cues from the environment, much as ancient mariners who observed the stars and set their course accordingly. During development, the growth cone continuously pushes forward, while the lengthening neuron behind it matures into the part of the cell called the axon. Once the growing cell “lands” at its target in a muscle cell, it is the axon that will relay the messages that allow an animal to control and move its limbs at will.

In Magellan mutants, Pfaff’s team discovered that the growth cone becomes disordered. Rather than forming a distinct “cap” on the developing neuron, the cone is dispersed in pieces along both the forward end and the axon extending behind it.

“The defect is found in the structure of the neuron itself,” said Pfaff, noting that the fundamental pieces, such as the receptors capable of reading cues, all seem to be present. Without the correct orientation of receptors, however, signals cannot be read accurately, resulting in growth going off course.

“A precise gradient normally exists across the cone,” said Pfaff, “which is disrupted in the Magellan mutants.” As a result, cells lose their polarity. They literally do not know the front end from the back end, according to Pfaff. This sense of polarity is a universal feature common to all growing neurons. Therefore, “Phr1 is likely to play a role in most growing neurons to ensure their structure is retained at the same time they are growing larger,” he said.

Pfaff and his group identified Magellan using a novel system they had developed, in which individual motor neurons and axons can be visualized fluorescently. They were able to screen more than a quarter of a million mutations, and the mutations of interest were rapidly mapped to known genes as a result of the availability of the sequenced mouse genome – a byproduct of the effort to sequence entire genomes such as that in the human.

Die Magellan mutation is located in a gene known as Phr1, which is also active in other parts of the nervous system, indicating that it most likely functions to steer other types of neurons, such as those that enervate sensory organs or connect different regions of the brain. Studies of Magellan may therefore shed light on how a variety of neurological disorders might be treated with cell replacement strategies.

Lead author on the study is Joseph W. Lewcock, formerly a postdoctoral fellow in Pfaff’s laboratory and currently at Genentech, Inc. Additional Salk authors include postdoctoral fellow Nicolas Genoud and senior research assistant Karen Lettieri.

The study, titled “The ubiquitin ligase Phr1 regulates axon outgrowth through modulation of microtubule dynamics,” was supported by the National Institute for Neurological Disorders and Stroke.

Das Salk Institute for Biological Studies in La Jolla, Kalifornien, ist eine unabhängige gemeinnützige Organisation, die sich grundlegenden Entdeckungen in den Biowissenschaften, der Verbesserung der menschlichen Gesundheit und der Ausbildung zukünftiger Forschergenerationen widmet. Jonas Salk, M.D., dessen Polio-Impfstoff die lähmende Kinderlähmung im Jahr 1955 fast ausgerottet hat, eröffnete das Institut 1965 mit einer Landschenkung der Stadt San Diego und der finanziellen Unterstützung der March of Dimes.