NDLI: Investigation of a Recombinant Smn Protein Delivery System to Treat Spinal Muscular Atrophy

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Investigation of a Recombinant Smn Protein Delivery System to Treat Spinal Muscular Atrophy

Content Provider	Semantic Scholar
Author	Anderton, Ryan S. Meloni, Bruno P. Mastaglia, F. Boulos, Sherif
Copyright Year	2014
Abstract	Spinal muscular atrophy (SMA), the most common genetic cause of infant death, is a neurodegenerative disorder affecting motor neurons. SMA results from a loss in full-length survival of motor neuron (SMN) protein due to deletions/mutations in the SMN1 gene. In this study, we assessed the ability of cell-penetrating peptides (CPP) to deliver recombinant SMN protein to cultured neurons as a prelude for a potential therapeutic to treat SMA. Firstly, we confirmed that E. coli produced recombinant GFP protein fused to TAT (YGRKKRRQRRR; TAT-GFP) transduced rat cortical neurons in a concentration dependent manner. However, due to low yields of recombinant TATSMN protein obtainable from E. coli, we investigated the potential of a modified TAT (TATκ: YARKAARQARA) or R9 (RRRRRRRRR) peptide downstream of the fibronectin (FIB) secretory signal peptide to generate recombinant CPP-fused SMN protein. While U251 cells transduced with an adenoviral vector expressing CMV-FIB-TATκ-SMN secreted recombinant TATκ-SMN protein, we did not detect TATκ-SMN protein transduction of cortical neurons. Further, purified TATκ-SMN was unable to transduce SH-SY5Y cells, nor block apoptosis following LY294002 treatment of these cells. Our findings indicate that TATκ is not a suitable CPP to deliver SMN protein to neurons. Nonetheless, we have developed a novel method to generate full-length recombinant SMN protein using a mammalian expression system, which can be used to explore the application of other CPPs to deliver SMN protein as a treatment for SMA.
File Format	PDF HTM / HTML
Alternate Webpage(s)	http://researchrepository.murdoch.edu.au/id/eprint/25427/1/muscular%20atrophy.pdf
Language	English
Access Restriction	Open
Content Type	Text
Resource Type	Article

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