论文信息 - Increased proteasome activity in human embryonic stem cells is regulated by PSMD11 - 字舞流文

Increased proteasome activity in human embryonic stem cells is regulated by PSMD11

Embryonic stem cells can replicate continuously in the absence of senescence and, therefore, are immortal in culture. Although genome stability is essential for the survival of stem cells, proteome stability may have an equally important role in stem-cell identity and function. Furthermore, with the asymmetric divisions invoked by stem cells, the passage of damaged proteins to daughter cells could potentially destroy the resulting lineage of cells. Therefore, a firm understanding of how stem cells maintain their proteome is of central importance. Here we show that human embryonic stem cells (hESCs) exhibit high proteasome activity that is correlated with increased levels of the 19S proteasome subunit PSMD11 (known as RPN-6 in Caenorhabditis elegans) and a corresponding increased assembly of the 26S/30S proteasome. Ectopic expression of PSMD11 is sufficient to increase proteasome assembly and activity. FOXO4, an insulin/insulin-like growth factor-I (IGF-I) responsive transcription factor associated with long lifespan in invertebrates, regulates proteasome activity by modulating the expression of PSMD11 in hESCs. Proteasome inhibition in hESCs affects the expression of pluripotency markers and the levels of specific markers of the distinct germ layers. Our results suggest a new regulation of proteostasis in hESCs that links longevity and stress resistance in invertebrates to hESC function and identity.

Lesley Page | Fred H. Gage | Brian Spencer | F. Gage | Leah Boyer | E. Masliah | Ianessa Morantte | F. Gage | B. Spencer | A. Dillin | W. Berggren | D. Vilchez | Eliezer Masliah | Andrew Dillin | Margaret K. Lutz | Margaret Lutz | W. Travis Berggren | David Vilchez | Leah Boyer | Carsten Merkwirth | Ianessa Morantte | Derek Joyce | Carsten Merkwirth | D. Joyce | Lesley Page

[1] J. Ballesta,et al. Rpn6p, a Proteasome Subunit from Saccharomyces cerevisiae, Is Essential for the Assembly and Activity of the 26 S Proteasome* , 2003, The Journal of Biological Chemistry.

[2] A. Goldberg,et al. The axial channel of the proteasome core particle is gated by the Rpt2 ATPase and controls both substrate entry and product release. , 2001, Molecular cell.

[3] I. Verma,et al. Design and cloning of lentiviral vectors expressing small interfering RNAs , 2006, Nature Protocols.

[4] H. van Attikum,et al. Yeast (Saccharomyces cerevisiae). , 2006, Methods in molecular biology.

[5] A. Goldberg,et al. Monitoring activity and inhibition of 26S proteasomes with fluorogenic peptide substrates. , 2005, Methods in enzymology.

[6] Richard I. Morimoto,et al. Adapting Proteostasis for Disease Intervention , 2008, Science.

[7] R. Morimoto,et al. Biological and chemical approaches to diseases of proteostasis deficiency. , 2009, Annual review of biochemistry.

[8] J. Thomson,et al. Embryonic stem cell lines derived from human blastocysts. , 1998, Science.

[9] J. I. Izpisúa Belmonte,et al. iPSCs: induced back to controversy. , 2011, Cell stem cell.

[10] A. Christiano,et al. Generation of keratinocytes from normal and recessive dystrophic epidermolysis bullosa-induced pluripotent stem cells , 2011, Proceedings of the National Academy of Sciences.

[11] B. Thiers. Induction of Pluripotent Stem Cells from Adult Human Fibroblasts by Defined Factors , 2008 .

[12] J. Thomson,et al. BMP4 initiates human embryonic stem cell differentiation to trophoblast , 2002, Nature Biotechnology.

[13] Y. Saeki,et al. Functional Analysis of Rpn6p, a Lid Component of the 26 S Proteasome, Using Temperature-sensitive rpn6 Mutants of the Yeast Saccharomyces cerevisiae* , 2005, Journal of Biological Chemistry.

[14] D. Finley,et al. Recognition and processing of ubiquitin-protein conjugates by the proteasome. , 2009, Annual review of biochemistry.

[15] Shulan Tian,et al. Induced Pluripotent Stem Cell Lines Derived from Human Somatic Cells , 2007, Science.

[16] K Tanaka,et al. Structure and functions of the 20S and 26S proteasomes. , 1996, Annual review of biochemistry.

[17] A. Sali,et al. The proteasomal subunit Rpn6 is a molecular clamp holding the core and regulatory subcomplexes together , 2011, Proceedings of the National Academy of Sciences.

[18] T. Graf. Faculty Opinions recommendation of Induction of pluripotent stem cells from adult human fibroblasts by defined factors. , 2007 .

[19] S. Yamanaka,et al. Induction of Pluripotent Stem Cells from Mouse Embryonic and Adult Fibroblast Cultures by Defined Factors , 2006, Cell.

[20] 長船健二. Marked differences in differentiation propensity among human embryonic stem cell lines , 2009 .

[21] Krishanu Saha,et al. Pluripotency and Cellular Reprogramming: Facts, Hypotheses, Unresolved Issues , 2010, Cell.

[22] Geert J. P. L. Kops,et al. Direct control of the Forkhead transcription factor AFX by protein kinase B , 1999, Nature.

[23] M. Kaufman,et al. Establishment in culture of pluripotential cells from mouse embryos , 1981, Nature.

[24] M. Tatar,et al. A Mutant Drosophila Insulin Receptor Homolog That Extends Life-Span and Impairs Neuroendocrine Function , 2001, Science.

[25] H. Schägger. Tricine–SDS-PAGE , 2006, Nature Protocols.

[26] C. Kenyon,et al. A C. elegans mutant that lives twice as long as wild type , 1993, Nature.

[27] H. Matsuzaki,et al. Regulation of intracellular localization and transcriptional activity of FOXO4 by protein kinase B through phosphorylation at the motif sites conserved among the FOXO family. , 2005, Journal of biochemistry.

[28] Fred H. Gage,et al. Modelling schizophrenia using human induced pluripotent stem cells , 2011, Nature.