
Ordering Information
| Product Name | Catalog # | UNIT | Price | Qty | FAVORITES | |
ARRDC4 Lentiviral Activation Particles (h) | sc-406413-LAC | 200 µl | $455.00 |
ARRDC4 (arrestin domain containing 4) encodes an α-arrestin family adaptor protein implicated in regulating membrane protein trafficking and signal attenuation through interactions with ubiquitin ligases and endocytic machinery. It is responsive to cellular stress cues and metabolic states, linking nutrient sensing to modulation of receptor turnover and downstream signaling pathways that influence energy homeostasis. ARRDC4 has been studied in contexts including insulin-responsive tissues and adipocyte biology, where altered expression can reshape glucose handling and lipid metabolism programs. Dysregulated ARRDC4 activity or expression is therefore relevant to mechanistic studies of metabolic dysfunction and pathway rewiring in cardiometabolic and inflammatory disease models.
ARRDC4 Lentiviral Activation Particles (h) address this need by packaging the complete synergistic activation mediator (SAM) transcriptional activation system into transduction-ready, high-titer lentiviral particles, enabling efficient ARRDC4 upregulation across a broader range of human cell types.
ARRDC4 Lentiviral Activation Particles (h) deliver all functional components of the synergistic activation mediator (SAM) system via lentiviral transduction. The system comprises three particle preparations co-transduced into target cells: one encoding catalytically inactive dCas9 (D10A and N863A mutations) fused to the VP64 transactivation domain with a blasticidin resistance gene; one encoding the MS2-p65-HSF1 fusion protein with a hygromycin resistance gene; and one encoding a target-specific 20 nt sgRNA fused to two MS2 RNA aptamers with a puromycin resistance gene. Following lentiviral transduction and genomic integration of the expression cassettes, the SAM components are stably expressed and assemble at the target locus within the proximal promoter region upstream of the ARRDC4 transcriptional start site, where VP64, p65, and HSF1 act cooperatively to recruit endogenous transcriptional machinery and drive sustained upregulation of endogenous ARRDC4 expression. The use of nuclease-inactive dCas9 avoids the introduction of double-strand DNA breaks and preserves the native ARRDC4 genomic locus and regulatory architecture.
The lentiviral format offers several practical advantages: stable genomic integration supports heritable activation across cell divisions; high-titer particle preparations eliminate the need for in-house viral production; and compatibility with primary, non-dividing, and transfection-resistant cell types expands experimental accessibility. Successful transduction can be confirmed and enriched through triple antibiotic selection using puromycin, hygromycin, and blasticidin.
For Research Use Only. Not Intended for Diagnostic or Therapeutic Use.