Human c-MET (Luc) HEK293 Reporter Cell

描述（Description）

The Human c-MET (Luc) HEK293 Reporter Cell was engineered to express signaling response element driving luciferase expressing systems and human c-MET (Gene ID: 4233). When stimulated with human HGF protein, the HGF/c-MET interaction drives RE-mediated luminescence. Neutralization of biological effect of human HGF protein by corresponding antibody results in a decrease in luminescence.

應(yīng)用說(shuō)明（Application）

Screen for neutralizing antibodies blocking the stimulation of human HGF protein.

生長(zhǎng)特性（Growth Properties）

Adherent

篩選標(biāo)記（Selection Marker）

Puromycin (2 μg/mL)

培養(yǎng)基（Culture Medium）

DMEM + 10% FBS

凍存液（Freeze Medium）

Serum-free cell cryopreservation medium

裝量（Quantity）

1 vial contains at least 5×10^6 cells in 1 mL serum-free cryopreservation medium

存儲(chǔ)（Storage）

Frozen in liquid nitrogen.

支原體檢測(cè)（Mycoplasma Testing）

Negative

無(wú)菌檢測(cè)（Sterility Testing）

Negative

使用說(shuō)明（Instructions for Use）

See data sheet for detailed culturing and assay protocol.

背景（Background）

Hepatocyte growth factor receptor (HGFR) is also known as mesenchymal-epithelial transition factor (MET), c-Met, and is a glycosylated receptor tyrosine kinase that plays a central role in epithelial morphogenesis and cancer development. HGFR protein possesses tyrosine-kinase activity. The primary single chain precursor protein is post-translationally cleaved to produce the alpha and beta subunits, which are disulfide linked to form the mature receptor. HGFR is normally expressed by cells of epithelial origin, while expression of HGF is restricted to cells of mesenchymal origin. Upon HGF stimulation, HGFR induces several biological responses that collectively give rise to a program known as invasive growth. Abnormal HGFR activation in cancer correlates with poor prognosis, where aberrantly active HGFR triggers tumor growth, formation of new blood vessels (angiogenesis) that supply the tumor with nutrients, and cancer spread to other organs (metastasis). HGFR is deregulated in many types of human malignancies, including cancers of kidney, liver, stomach, breast, and brain. Normally, only stem cells and progenitor cells express HGFR, However, cancer stem cells are thought to hijack the ability of normal stem cells to express HGFR, and thus become the cause of cancer persistence and spread to other sites in the body. Various mutations in the HGFR gene are associated with papillary renal carcinoma. HGFR mediates a complex program known as invasive growth. Activation of HGFR triggers mitogenesis, and morphogenesis.

Permits & Restrictions

This cell line is provided for research use only. It is not intended for any animal or human therapeutic use, any human or animal consumption, or any diagnostic use. You are not allowed to share, distribute, sell, modify, sublicense, or otherwise make this cell line available for use to other laboratories, departments, research institutions, hospitals, universities, or biotech companies. AcroBiosystems does not warrant the suitability of this cell line for any particular use, and does not accept any liability in connection with the handling or use of this cell line.