
Ordering Information
| Product Name | Catalog # | UNIT | Price | Qty | FAVORITES | |
VDAC3 CRISPR/Cas9 KO Plasmid (h) | sc-404240 | 20 µg | $397.00 | |||
VDAC3 HDR Plasmid (h) | sc-404240-HDR | 20 µg | $445.00 |
VDAC3 (voltage-dependent anion channel 3) is a mitochondrial outer membrane porin that contributes to metabolite and ion exchange between the cytosol and the intermembrane space, influencing oxidative phosphorylation, mitochondrial membrane potential, and redox homeostasis. As part of the VDAC family, VDAC3 interfaces with pathways governing mitochondrial permeability, apoptosis-related signaling, and cellular stress responses, and it has been linked to regulation of reactive oxygen species and mitochondrial quality control. Altered VDAC3 expression or function has been associated with mitochondrial dysfunction phenotypes, including impacts on energy metabolism and sperm motility, and has been explored in contexts of neurodegeneration and cancer-associated metabolic remodeling. These features make VDAC3 a useful target for dissecting mitochondria-driven signaling and bioenergetic adaptations in human cell models.
VDAC3 CRISPR/Cas9 KO Plasmid (h) is a pool of plasmids designed for targeted disruption of the VDAC3 gene in human cell lines. Each plasmid in the pool co-expresses a unique sgRNA, targeting a distinct site within the VDAC3 locus, alongside the Streptococcus pyogenes Cas9 nuclease, and encodes GFP to enable fluorescent identification and enrichment of successfully transfected cells. This multi-guide strategy increases the likelihood of inducing frameshifts or deletions that produce a functional knockout, offering a more robust alternative to single-guide approaches. DSBs induced at multiple sites are resolved through non-homologous end joining (NHEJ) or, when used with the included HDR donor template, homology-directed repair (HDR) at a defined target site within the locus.
When used in conjunction with the RFP-expressing HDR donor, GFP and RFP fluorescence can be used together to distinguish transfected from edited cell populations, streamlining flow cytometry-based sorting and clone selection workflows.
For applications requiring confirmed, selectable knockout clones, VDAC3 HDR Plasmid (h) includes an HDR donor construct containing a puromycin resistance cassette (PuroR) and a red fluorescent protein (RFP) reporter, flanked by homology arms specific to a defined VDAC3 target site.
When co-transfected with VDAC3 CRISPR/Cas9 KO Plasmid (h):
The HDR donor construct features loxP sites flanking the PuroR-RFP selection cassette to allow clean marker removal following clone confirmation. Transient expression of Cre recombinase via the included Cre Vector: sc-418923 excises the cassette, leaving a minimal residual loxP site within the VDAC3 locus and eliminating potential confounding effects on downstream assays.
This two-step approach:
For Research Use Only. Not Intended for Diagnostic or Therapeutic Use.