EF1a-mCherry AAV (Serotype AAV-BI30)

The EF1a-mCherry AAV vector utilizes an engineered AAV-BI30 serotype for pseudotyping, combining the strong transcriptional activity of the elongation factor 1α (EF1α) promoter with the bright and photostable mCherry fluorescent reporter gene. This system offers numerous advantages in gene delivery, such as efficient transduction of various cell types (e.g., neurons, glial cells, and stem cells) due to AAV-BI30''s enhanced tissue tropism and ability to evade pre-existing neutralizing antibodies. The EF1α promoter ensures sustained and widespread expression in both dividing and non-dividing cells, while mCherry''s far-red emission allows for multiplexing with GFP/YFP-based markers and deeper tissue imaging. Compared to traditional serotypes (e.g., AAV2/9), the AAV-BI30 capsid further improves biodistribution and cellular uptake, making it ideal for challenging in vivo applications.

This vector is widely used in neuroscience research for labeling neural circuits, tracking transplanted cells, and validating CRISPR editing through fluorescent co-expression. In developmental biology, its long-term expression stability facilitates lineage tracing and organoid studies. The mCherry reporter gene also serves as a transduction control in co-delivery experiments (e.g., Cre-Lox or optogenetic tools) and allows for quantitative analysis via flow cytometry or histology. Furthermore, AAV-BI30''s reduced immunogenicity and improved CNS/retinal targeting support preclinical gene therapy studies, where mCherry can serve as a visual tracer for vector distribution. Its compatibility with live-cell microscopy and non-invasive imaging techniques further supports longitudinal studies in areas such as cancer metastasis or regenerative medicine.