CellOnco™ CHO-K1-Tg(Human Gαqi5//Human S1P1 Receptor) Division-Arrested Cell, Single Clone (CAT#: ITS-0624-HMM608)

Creative Biolabs offers CHO-K1-Tg(Human Gαqi5//Human S1P1 Receptor) Division-Arrested Cell which S1P1 receptor stably expressed in CHO-K1 cells which overexpress Gαqi5.

CHO-K1-Tg(Human Gαqi5//Human S1P1 Receptor) Division-Arrested Cell was engineered to express the receptor human S1P1 (NM_001400) and Gαqi5 gene. This cell line can be used to study S1P1 receptor function, signaling pathways, and potential therapeutic interventions. Dividing-arrest cells are cells that are normally kept under specific culture conditions or treated with agents that prevent cell division from being held in a non-dividing state. This can be achieved through methods such as serum starvation, chemical inhibitors of cell cycle progression, or genetic modification.

Well-characterized stable cell lines;
for cell-based high-throughput screening;
Low-cost evaluation of stable cell lines or limited quantities of compounds.

S1P1 receptor function, signaling pathways, and potential therapeutic interventions.

GPCR

S1P1

Lysophospholipid

Human

CHO-K1 Gαqi5

Expression vector containing full-length human S1P1 cDNA (GenBank Accession Number NM_001400) with FLAG tag sequence at N-terminus

NM_001400

S1P1 (or EDG1) is a widely distributed G-protein-coupled receptor for sphingosine-1-phosphate (S1P), a blood-borne bioactive lipid. Stimulation of the S1P1 receptor triggers a Gi-linked pathway, leading to growth, survival, migration, and morphogenesis. Disruption of the S1P1 gene in mice results in embryonic lethality because of its key role within endothelial cells in regulating the coverage of blood vessels by vascular smooth muscle cells. S1P1 also mediates activation of Rac and functions as a typical chemotactic receptor.