CellOnco™ HEK293T-Tg(Human BB3 Receptor) Division-Arrested Cell, Single Clone (CAT#: ITS-0624-HMM523)

Creative Biolabs offers HEK293T-Tg(Human BB3 Receptor) Division-Arrested Cell which BB3 receptor stably expressed in HEK293T cells.

HEK293T-Tg(Human BB3 Receptor) Division-Arrested Cell was engineered to express the receptor human BB3 (NM_001727). This cell line can be used to study BB3 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.

BB3 receptor function, signaling pathways, and potential therapeutic interventions.

GPCR

BB3

Bombesin

Human

HEK293T

Expression vector containing full-length human BRS3 cDNA (GenBank Accession Number NM_001727) with FLAG tag sequence at N-terminus

NM_001727

The bombesin-like peptides mediate a diverse spectrum of biological activities and have been implicated as autocrine growth factors in the pathogenesis and progression of cancer. The bombesin receptor subtype 3 (BB3 or BRS3) is expressed in the lung (normal and cancer), nasal mucosa, placenta, and uterus. Mice lacking BB3 receptor develop metabolic defects and obesity phenotype, suggesting that BB3 may be an important target for obesity research. In addition, BB3 may be involved in diabetes and hypertension.