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Size | List Price | Price | Cart |
---|---|---|---|
100 ul | $329.00 | Add to Cart |
The heat shock proteins were discovered since they are heavily upregulated when cells are stressed by temperatures above the normal physiological range. They are expressed in unstressed cells also and have a normal function as chaperones, helping other proteins to fold correctly, but are required in much greater amounts if the cell or tissue is stressed by heat. Heat shock protein 27 (HSP27) is an abundant protein which functions as a chaperone but has many other functions. Upregulation of this protein is protective against neurodegenerative diseases at least in certain mouse models. Point mutations in the HSP27 gene are associated with two neurological diseases, Charcot-Marie-Tooth disease type 2F and distal hereditary motor neuropathy IIB. These diseases are associated with axonal loss apparently following defects in the transport of neurofilaments. HSP27 may bind cytoplamsic cytochrome c released from mitochondria which would otherwise normally activate the caspase apoptotic cascade. HSP27 is a major phosphoprotein of cells primarily under the influence of the p38/SAP kinase and JNK pathways. The central region of the HSP27 molecule corresponds to a crystallin domain, a compact module found in many chaperones and heat shock proteins. HSP27 is implicated in several other aspects of cell signaling and response to cancer and other diseases. The amino acid sequence of HSP27 is relatively poorly conserved across species boundaries, so there are 159 amino acids identities between human, cow, rat and mouse HSP27, out of 204-209 amino acids. This variability results in some antibodies being species specific while others work across many species. CH22133 was made against full length recombinant HSP27 expressed in and purified from E. coli. This antibody binds to an epitope on the human molecule missing from the rat and mouse homologue, likely variable peptides in the N and C terminal of human HSP27. Product Highlights: |
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