Extracellular Heat Shock Protein 70: A Critical Component for Motoneuron Survival

doi:10.1523/JNEUROSCI.1912-05.2005

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The Journal of Neuroscience, October 19, 2005, 25(42):9735-9745; doi:10.1523/JNEUROSCI.1912-05.2005

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Development/Plasticity/Repair
Extracellular Heat Shock Protein 70: A Critical Component for Motoneuron Survival
Mac B. Robinson,^* J. Lille Tidwell,^* Thomas Gould, Anna R. Taylor, Jason M. Newbern, Jason Graves, Michael Tytell, and Carol E. Milligan
Department of Neurobiology and Anatomy, Wake Forest University School of Medicine, Winston-Salem, North Carolina 27157

The dependence of developing spinal motoneuron survival on asoluble factor(s) from their target, muscle tissue is well establishedboth in vivo and in vitro. Considering this apparent dependence,we examined whether a specific component of the stress responsemediates motoneuron survival in trophic factor-deprived environments.We demonstrate that, although endogenous expression of heatshock protein 70 (HSP70) did not change during trophic factordeprivation, application of e-rhHsp70 (exogenous recombinanthuman Hsp70) promoted motoneuron survival. Conversely, depletionof HSP70 from chick muscle extract (MEx) potently reduces thesurvival-promoting activity of MEx. Additionally, exogenoustreatment with or spinal cord overexpression of Hsp70 enhancesmotoneuron survival in vivo during the period of naturally occurringcell death [programmed cell death (PCD)]. Hindlimb muscle cellsand lumbar spinal astrocytes readily secrete HSP70 in vitro,suggesting potential physiological sources of extracellularHsp70 for motoneurons. However, in contrast to exogenous treatmentwith or overexpression of Hsp70 in vivo, muscle-targeted injectionsof this factor in an ex vivo preparation fail to attenuate motoneuronPCD. These data (1) suggest that motoneuron survival requirementsmay extend beyond classical trophic factors to include HSP70,(2) indicate that the source of this factor is instrumentalin determining its trophic function, and (3) may therefore influencetherapeutic strategies designed to increase motoneuron Hsp70signaling during disease or injury.

Key words: muscle extract; cell death; apoptosis; stress response; Hsp70; motoneuron; trophic

Received July 9, 2003; revised September 5, 2005; accepted September 8, 2005.

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