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scAAV6-GFP

scAAV6-GFP

Cat.No. :  AAV00198Z

Titer: ≥1x10^12 GC/mL / ≥1x10^13 GC/mL Size: 30 ul/100 ul/500 ul/1 ml

Serotype:  AAV Serotype 6 Storage:  -80 ℃

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AAV Particle Information

Quality Control

Cat. No. AAV00198Z
Description Self-complementary AAV serotype 6 particles contain GFP under the control of CMV promoter.
Reporter GFP
Serotype AAV Serotype 6
Application

1. Determination of optimal MOI (multiplicity of infection), administration methods etc.

2. Detection of the infection efficiency of the AAV serotype against a specific cell type or tissue.

3. Using reporter genes to visualize the distribution and expression of AAV vectors in live animals, helping assess the biodistribution and persistence of gene delivery.

Titer Varies lot by lot, typically ≥1x10^12 GC/mL
Size Varies lot by lot, for example, 30 μL, 50 μL, 100 μL etc.
Storage Store at -80℃. Avoid multiple freeze/thaw cycles.
Shipping Frozen on dry ice
Creative Biogene ensures high-quality AAV particles by optimizing and standardizing production protocols and performing stringent quality control (QC). The specific QC experiments performed vary between AAV particle lots.
Endotoxin Endotoxins, primarily derived from Gram-negative bacteria, can trigger adverse immune responses. Endotoxin contamination is a significant concern in the production of AAV, especially for applications in animal studies and gene therapy. Effective endotoxin quality control is essential in the development and manufacturing of AAV particles. Creative Biogene utilizes rigorous endotoxin detection methods to monitor the endotoxin level in our produced AAV particles to ensure regulatory compliance.
Purity AAV purity is critical for ensuring the safety and efficacy of AAV-based applications.AAV capsids are composed of three main protein components, known as viral proteins: VP1, VP2, and VP3. These proteins play a critical role in the structure and functionality of the AAV capsid. Monitoring the VP1, VP2, and VP3 content in AAV preparations is essential for quality control in AAV production. Our AAV particles are tested for showing three clear bands of VP1, VP2 VP3 by SDS-PAGE.
Sterility The AAV virus samples are inoculated into the cell culture medium for about 5 days to detect bacterial and fungal growth.
Transducibility Upon requirement, Creative Biogene can perform in vitro or in vivo transduction assays to evaluate the ability of AAV to deliver genetic material into target cells or tissues, and assess gene expression and functional activities.
Empty vs. Full Capsids Based-on our proprietary AAV production and purification technology, Creative Biogene can always offer AAV particles with high ratio of full capsids. If required, we can also assess the ratio for a specifc lot of AAV particles by transmission electron microscopy (TEM) or other methods.
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Gene transfer methods are mainly divided into two categories: viral transfer and non-viral transfer. Viral gene transfer has been shown to be a more efficient cell transduction than non-viral gene transfer. It allows for more efficient protein production from transgenic cells, faster transduction, and long-term expression of the target protein. Among various viral vectors, adeno-associated virus (AAV) vector delivery has been shown to be an effective and safe method for genetically modifying both dividing and non-dividing cells. Gene transduction using traditional AAV vectors has been applied to canine myotubular myopathy, hemophilia B, glycogen storage disease type Ia, retinal degeneration, and mucopolysaccharidosis type VII. Self-complementary adeno-associated virus (scAAV) is known to be 5 to 140 times more efficient within host cells than traditional AAV vectors because scAAV vectors can bypass the rate-limiting DNA synthesis step. scAAV vector delivery has been shown to be an effective and safe method for gene delivery in humans with low immunogenicity and high efficiency. scAAV vectors have multiple serotypes with different tropisms depending on tissue type. Due to their varying levels of tissue tropism, selection of the appropriate serotype is critical for successful treatment.
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Customer Reviews
Superior Transduction Efficiency

I have been using the scAAV6-GFP vectors in my gene therapy research, and the results have been outstanding. The transduction efficiency is remarkable, providing strong and consistent GFP expression in my target cells.

Germany

06/05/2024

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