重组人 Hsp27 蛋白
产品名称: 重组人 Hsp27 蛋白
英文名称: Recombinant Human Hsp27
产品编号: SPR-105C
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产品产地: 加拿大
品牌商标: StressMarq
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SDS PAGE of Hsp27 protein.
Hsp27s  belong to an abundant and ubiquitous family of small heat shock  proteins (sHSP). It is an important HSP found in both normal human cells  and cancer cells. The basic structure of most sHsps is a homologous and  highly conserved amino acid sequence, with an α-crystallin-domain at  the C-terminus and the WD/EPF domain at the less conserved N-terminus.  This N-terminus is essential for the development of high molecular  oligomers (1, 2). Hsp27-oligomers consist of stable dimers formed by as  many as 8-40 Hsp27 protein monomers (3). The oligomerization status is  connected with the chaperone activity: aggregates of large oligomers  have high chaperone activity, whereas dimers have no chaperone activity  (4). HSP27 is localized to the cytoplasm of unstressed cells but can  redistribute to the nucleus in response to stress, where it may function  to stabilize DNA and/or the nuclear membrane. Other functions include  chaperone activity (as mentioned above), thermotolerance in vivo,  inhibition of apoptosis, and signal transduction. Specifically, in  vitro, it acts as an ATP-independent chaperone by inhibiting protein  aggregation and by stabilizing partially denatured proteins, which  ensures refolding of the HSP70 complex. Hsp27 is also involved in the  apoptotic signaling pathway because it interferes with the activation of  cytochrome c/Apaf-1/dATP complex, thereby inhibiting the activation of  procaspase-9. It is also hypothesized that hsp27 may serve some role in  cross-bridge formation between actin and myosin (5). And finally, Hsp27  is also thought to be involved in the process of cell differentiation.  The up-regulation of Hsp27 correlates with the rate of phosphorylation  and with an increase of large oligomers. It is possible that Hsp27 may  play a crucial role in termination of growth (6).
1. Kim K.K., Kim R., and Kim, S. (1998) Nature 394(6693): 595-599.
2. Van Montfort R., Slingsby C., and Vierling E. (2001) Addv Protein Chem. 59: 105-56.
3. Ehrnsperger M., Graber S., Gaestel M. and Buchner J. (1997) EMBO J. 16: 221-229.
4. Ciocca D.R., Oesterreich S., Chamness G.C., McGuire W.L., and Fugua S.A. (1993) J Natl Cancer Inst. 85 (19): 1558-70.
5. Sarto C. Binnz P.A. and Mocarelli P. (2000) Electrophoresis. 21(6): 1218-26.
6. Arrigo A.P. (2005) J Cell Biochem. 94(2): 241-6.
