Mutations in superoxide dismutase-1 (SOD1) cause familial amyotrophic lateral sclerosis (fALS). Recent evidence implicates adaptive responses to endoplasmic reticulum (ER) stress in the disease process via a pathway known as the unfolded protein response (UPR). Here, we investigated the contribution to fALS of X-box-binding protein-1 (XBP-1), a key UPR transcription factor that regulates genes involved in protein folding and quality control. Despite expectations that XBP-1 deficiency would enhance the pathogenesis of mutant SOD1, we observed a dramatic decrease in its toxicity due to an enhanced clearance of mutant SOD1 aggregates by macroautophagy, a cellular pathway involved in lysosome-mediated protein degradation. To validate these observations in vivo, we generated mutant SOD1 transgenic mice with specific deletion of XBP-1 in the nervous system. XBP-1-deficient mice were more resistant to developing disease, correlating with increased levels of autophagy in motoneurons and reduced accumulation of mutant SOD1 aggregates in the spinal cord. Post-mortem spinal cord samples from patients with sporadic ALS and fALS displayed a marked activation of both the UPR and autophagy. Our results reveal a new function of XBP-1 in the control of autophagy and indicate critical cross-talk between these two signaling pathways that can provide protection against neurodegeneration.[Keywords: Amyotrophic lateral sclerosis; unfolded protein response; endoplasmic reticulum stress; XBP-1; autophagy] Supplemental material is available at http://www.genesdev.org. Received June 10, 2009; revised version accepted August 19, 2009. Most neurodegenerative disorders-such as amyotrophic lateral sclerosis (ALS), Alzheimer's, and Parkinson's and Huntington's diseases-share a common pathology characterized by abnormal protein inclusions containing specific misfolded proteins (Matus et al. 2008). ALS is a progressive and deadly adult-onset motor neuron disease characterized by muscle weakness, spasticity, atrophy, paralysis, and premature death. The pathological hallmark of ALS is the selective degeneration of motoneurons in the spinal ventral horn, most brainstem nuclei, and the cerebral cortex (Boillee et al. 2006;Pasinelli and Brown 2006). ALS is more frequent in males, and the disease lacks a defined genetic component in a majority of ALS patients, so-called sporadic ALS (sALS), while ;10% of cases are familial (fALS). More than 100 mutations in the gene encoding superoxide dismutase-1 (SOD1) are linked to fALS and trigger its misfolding and abnormal aggregation, resulting in motoneuron dysfunction (Pasinelli and Brown 2006). Overexpression of human fALS-linked SOD1 mutations in transgenic mice recapitulates essential features of the human pathology, provoking agedependent protein aggregation, paralysis, and motor neuron degeneration. Since sALS and fALS affect the same neurons with similar pathology, therapeutics effective in mutant SOD1 mouse models may translate to sALS.The pathogenesis of mutant SOD1 toxicity remains unclear, and m...
