Onset and Progression in Inherited ALS Determined by Motor Neurons and Microglia

Séverine Boillée; Koji Yamanaka; Christian S. Lobsiger; Neal G. Copeland; Nancy A. Jenkins; George Kassiotis; George Kollias; Don W. Cleveland

doi:10.1126/science.1123511

Onset and Progression in Inherited ALS Determined by Motor Neurons and Microglia

Séverine Boillée(University of California San Diego), Koji Yamanaka(University of California San Diego), Christian S. Lobsiger(University of California San Diego), Neal G. Copeland(University of California San Diego), Nancy A. Jenkins(University of California San Diego), George Kassiotis(University of California San Diego), George Kollias(University of California San Diego), Don W. Cleveland(University of California San Diego)

Science

June 1, 2006

10.1126/science.1123511

Cited by 1,593

Abstract

Dominant mutations in superoxide dismutase cause amyotrophic lateral sclerosis (ALS), a progressive paralytic disease characterized by loss of motor neurons. With the use of mice carrying a deletable mutant gene, expression within motor neurons was shown to be a primary determinant of disease onset and of an early phase of disease progression. Diminishing the mutant levels in microglia had little effect on the early disease phase but sharply slowed later disease progression. Onset and progression thus represent distinct disease phases defined by mutant action within different cell types to generate non-cell-autonomous killing of motor neurons; these findings validate therapies, including cell replacement, targeted to the non-neuronal cells.

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