17-10189 Sigma-AldrichLentiBrite™ GFP-LC3 Control Mutant Lentiviral Biosensor
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Overview
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Key Spec Table
Key Applications | Detection Methods |
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TFX, IF, ICC | Fluorescent |
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Catalogue Number | 17-10189 |
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Description | LentiBrite™ GFP-LC3 Control Mutant Lentiviral Biosensor |
Overview | Read our application note in Nature Methods! http://www.nature.com/app_notes/nmeth/2012/121007/pdf/an8620.pdf (Click Here!) Learn more about the advantages of our LentiBrite Lentiviral Biosensors! Click Here Biosensors can be used to detect the presence/absence of a particular protein as well as the subcellular location of that protein within the live state of a cell. Fluorescent tags are often desired as a means to visualize the protein of interest within a cell by either fluorescent microscopy or time-lapse video capture. Visualizing live cells without disruption allows researchers to observe cellular conditions in real time. Lentiviral vector systems are a popular research tool used to introduce gene products into cells. Lentiviral transfection has advantages over non-viral methods such as chemical-based transfection including higher-efficiency transfection of dividing and non-dividing cells, long-term stable expression of the transgene, and low immunogenicity. EMD Millipore is introducing LentiBrite™ Lentiviral Biosensors, a new suite of pre-packaged lentiviral particles encoding important and foundational proteins of autophagy, apoptosis, and cell structure for visualization under different cell/disease states in live cell and in vitro analysis.
EMD Millipore’s LentiBrite™ GFP-LC3-G120A mutant lentiviral particles serve as a negative control alongside GFP-LC3 wild-type (catalog # 17-10193) for live cell analysis of autophagy. |
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Background Information | Autophagy, a degradative pathway that provides recycled nutrients to cells under stress, plays both protective and deleterious roles in many diseases, including cancer, neurodegeneration, and infections. Members of the LC3 family play a key role in the maturation of the autophagosome, the central organelle of autophagy. LC3 precursors, diffusely distributed in the cytosol, are proteolytically processed to form LC3-I. Upon initiation of autophagy, the C-terminal glycine is modified by addition of a phosphatidylethanolamine (PE) to form LC3-II, which translocates rapidly to nascent autophagosomes in a punctate distribution. DNA constructs encoding fluorescent proteins fused to LC3 are widely employed for introduction into cells for monitoring autophagosome formation by fluorescence microscopy. A mutant form of LC3 with the C-terminal glycine changed to alanine (LC3-G120A) is unable to accept the PE modification and fails to translocate to the autophagosome upon induction of autophagy. EMD Millipore’s LentiBrite™ GFP-LC3-G120A lentiviral particles serve as a negative control alongside GFP-LC3 wild-type (catalog # 17-10193) for live cell analysis of autophagy. |
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Components |
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Detection method | Fluorescent |
Quality Level | MQ100 |
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Purification Method | PEG precipitation |
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Quality Assurance | Evaluated by transduction of HT-1080 cells and fluorescent imaging performed for assessment of transduction efficiency. |
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Material Size | 1 vial (minimum of 3 x 10E8 IFU/mL) |
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Specifications |
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Catalogue Number | GTIN |
17-10189 | 04053252423642 |
Documentation
LentiBrite™ GFP-LC3 Control Mutant Lentiviral Biosensor MSDS
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LentiBrite™ GFP-LC3 Control Mutant Lentiviral Biosensor Certificates of Analysis
Brochure
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Advancing cancer research: From hallmarks & biomarkers to tumor microenvironment progression |
Hallmarks of Aging |
Technical Info
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LentiBrite™ Lentiviral Biosensors for Fluorescent Cellular Imaging: Analysis of Autophagosome Formation |
Posters
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Autophagy Signaling |