
Ordering Information
| Product Name | Catalog # | UNIT | Price | Qty | FAVORITES | |
IRS-1 CRISPR/Cas9 KO Plasmid (h2) | sc-400096-KO-2 | 20 µg | $397.00 | |||
IRS-1 HDR Plasmid (h2) | sc-400096-HDR-2 | 20 µg | $445.00 |
Insulin receptor substrate 1 (IRS-1), encoded by the human IRS1 gene, is a core adaptor protein that couples activated insulin and IGF-1 receptors to downstream signaling through PI3K–AKT–mTOR and RAS–MAPK pathways. Through phosphorylation-dependent docking of SH2-domain proteins, IRS-1 regulates glucose uptake, glycogen synthesis, protein translation, and cell growth, integrating metabolic and mitogenic cues. Altered IRS1/IRS-1 signaling has been linked to insulin resistance and metabolic dysregulation, and it is also studied in contexts where growth factor signaling contributes to aberrant proliferation and survival programs. IRS-1 therefore serves as a mechanistic node for dissecting pathway crosstalk between receptor tyrosine kinases, nutrient sensing, and cellular stress responses.
IRS-1 CRISPR/Cas9 KO Plasmid (h2) is a pool of plasmids designed for targeted disruption of the IRS1 gene in human cell lines. Each plasmid in the pool co-expresses a unique sgRNA, targeting a distinct site within the IRS1 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, IRS-1 HDR Plasmid (h2) 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 IRS1 target site.
When co-transfected with IRS-1 CRISPR/Cas9 KO Plasmid (h2):
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 IRS1 locus and eliminating potential confounding effects on downstream assays.
This two-step approach:
For Research Use Only. Not Intended for Diagnostic or Therapeutic Use.