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Cat. No. ARG44124

SORCS2 Knockout HGC-27 Cell Line

  • Product Type:

    In Stock Cell Lines

  • Species:

    Homo sapiens (Human)

  • Tissue Source:

    Stomach

  • Disease:

    Carcinoma

The SORCS2 Knockout HGC-27 Cell Line is a CRISPR/Cas9-edited knockout cell line enabling targeted disruption of SORCS2, a VPS10 domain sorting receptor that regulates cell adhesion and migration. Derived from a human gastric carcinoma cell line of lymph node metastasis origin, this model is ideal for studying epithelial-mesenchymal transition (EMT) and metastatic mechanisms. SORCS2 loss promotes ??-catenin and STAT3 signaling, enhancing invasiveness. This cell line supports applications in gastric cancer research, protein trafficking studies, and drug target validation through assays such as Transwell migration, Western blotting, and co-immunoprecipitation.

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Shipping Info:

Cryopreserved in vials and shipped on dry ice


Disclaimer:

For Research Use Only

  • Characteristics

    Host Cell

    HGC-27

    Sex of Donor

    Unknown

    Age

    Unknown

    Derived From Site

    Metastatic; Lymph node

    Gene Name

    SORCS2

    Gene Identifier

    NCBI Gene ID 57537

    Morphology

    Epithelial-like

    Growth Mode

    Adherent

    Storage

    Liquid nitrogen (LN2)

  • Culture Conditions

    Temperature

    37°C

    Atmosphere

    5% CO₂

  • Quality Control

    Sterility testing

    The bacterial, yeast, and fungi are not detected in these cells by daily monitor.

    Mycoplasma testing

    Negative for mycoplasma through PCR analysis

  • Disclaimer

    Intended Use

    This product is intended for laboratory in vitro use only. lt is not intended for diagnostic, therapeutic, or clinical applications.

    Disclaimer

    Ascent Research endeavors to provide accurate and up-to-date product information. However, no warranties or representations are made regarding its completeness or reliability. References to scientific literature and patents are for informational purposes only, and the customer assumes sole responsibility for verifying their accuracy.

    By accepting this product, the customer acknowledges and agrees to assume all risks associated with its receipt, handling, storage, disposal, and use, including compliance with all applicable safety and environmental regulations and precautions. Relevant laws, regulations, and ethical guidelines must be followed in conducting any research, modifications, or derivatives derived from this product.

    This product is provided "AS IS", and except as expressly stated herein, Ascent Research disclaims all other warranties, express or implied. Under no circumstances shall Ascent Research, its affiliates, or representatives be liable for indirect, incidental, consequential, or punitive damages arising from the use of this material. While Ascent Research employs rigorous quality control measures, we shall not be held responsible for damages resulting from misidentification or misinterpretation of the provided materials.

Description

The SORCS2 Knockout HGC-27 Cell Line is a CRISPR/Cas9-edited knockout cell line that provides targeted disruption of SORCS2 in the HGC-27 background. This stable loss-of-function model enables precise investigation of SORCS2-dependent cellular processes without the introduction of exogenous reporters or selection markers that could confound phenotypic interpretation. As a gene-edited tool, it serves as a critical resource for dissecting the molecular mechanisms controlled by SORCS2 in gastric cancer biology.

The HGC-27 cell line is a widely used human gastric carcinoma model derived from a lymph node metastasis, exhibiting an undifferentiated and aggressive phenotype. These cells display robust in vitro migration, invasion, and altered cell adhesion properties, recapitulating key features of metastatic disease. This background is inherently suited for studying epithelial-mesenchymal transition (EMT) and provides a physiologically relevant context for evaluating SORCS2 function in advanced gastric cancer.

SORCS2 encodes a VPS10 domain-containing sorting receptor that mediates intracellular trafficking of cell adhesion molecules and signaling receptors. It interacts with APP, p75NTR, and SORT1, and is recruited to membranes by GGA1 and GGA2 adaptor proteins. SORCS2 functions downstream of ligands such as BDNF, NGF, pro-neurotrophins, EGF, and TGF-??, and its activity impacts multiple pathways. Notably, SORCS2 regulates E-cadherin and ??-catenin stability, Rho GTPase function, and STAT3 phosphorylation. SORCS2 also associates with BACE1 and influences JNK and NF-??B signaling, linking neurotrophin pathways to cell adhesion dynamics. Loss of SORCS2 disrupts this balance, leading to enhanced ??-catenin/TCF/LEF transcriptional activity and STAT3 signaling, which together promote EMT and cell migration.

SORCS2 knockout in HGC-27 cells enhances the mesenchymal and invasive traits characteristic of metastatic gastric cancer, offering a model to study how loss of this sorting receptor accelerates EMT and tumor dissemination. This system allows dissection of the signaling rewiring that drives metastasis, including aberrant protein trafficking and transcriptional reprogramming. The cell line thus provides a controlled platform for evaluating the role of SORCS2 in maintaining epithelial integrity and the consequences of its loss during tumor progression.

This knockout model is suited for a broad spectrum of applications, including gene function studies, metastatic mechanism analysis, protein trafficking dissection, and drug target validation. Representative assays encompass Western blotting, RT-qPCR, Transwell migration/invasion, cell adhesion, co-immunoprecipitation, immunofluorescence, ??-catenin/TCF reporter assays, STAT3 phosphorylation analysis, RNA-seq, and apoptosis assays. Researchers can employ these techniques to interrogate signaling pathways and test therapeutic hypotheses. For further technical information or support, please contact Ascent Research.

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