Neuronal Pentraxins Mediate Synaptic Refinement in the Developing Visual System

Lisa Bjartmar(University of California, San Francisco), Andrew D. Huberman(University of California, San Francisco), E. M. Ullian(Stanford University), René C. Renterı́a(Johns Hopkins University), Jason Liu(Cleveland Clinic), Wei Xu(Louis Stokes Cleveland VA Medical Center), J. Prezioso(Johns Hopkins University), Michael W. Susman(Stanford University), David Stellwagen(Johns Hopkins University), Caleb Stokes(Cleveland Clinic), R. Cho(Stanford University), Paul Worley(Johns Hopkins University), Robert C. Malenka(Johns Hopkins University), Sherry L. Ball(Louis Stokes Cleveland VA Medical Center), Neal S. Peachey(University of California, Davis), David R. Copenhagen(Louis Stokes Cleveland VA Medical Center), B. Chapman(University of California, Davis), Masaru Nakamoto(Cleveland Clinic), Barbara A. Barres(University of California, Davis), M S Perin(Cleveland Clinic)
Journal of Neuroscience
June 7, 2006
Cited by 175Open Access
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Abstract

Neuronal pentraxins (NPs) define a family of proteins that are homologous to C-reactive and acute-phase proteins in the immune system and have been hypothesized to be involved in activity-dependent synaptic plasticity. To investigate the role of NPs in vivo, we generated mice that lack one, two, or all three NPs. NP1/2 knock-out mice exhibited defects in the segregation of eye-specific retinal ganglion cell (RGC) projections to the dorsal lateral geniculate nucleus, a process that involves activity-dependent synapse formation and elimination. Retinas from mice lacking NP1 and NP2 had cholinergically driven waves of activity that occurred at a frequency similar to that of wild-type mice, but several other parameters of retinal activity were altered. RGCs cultured from these mice exhibited a significant delay in functional maturation of glutamatergic synapses. Other developmental processes, such as pathfinding of RGCs at the optic chiasm and hippocampal long-term potentiation and long-term depression, appeared normal in NP-deficient mice. These data indicate that NPs are necessary for early synaptic refinements in the mammalian retina and dorsal lateral geniculate nucleus. We speculate that NPs exert their effects through mechanisms that parallel the known role of short pentraxins outside the CNS.


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