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Cat. No. ARG0391

NUP188 Knockout Hep-G2 Cell Line

  • Product Type:

    Genome-edited Cells

  • Tissue Source:

    Liver

  • Disease:

    Hepatoblastoma

  • Gene Species:

    Homo sapiens (Human)

The NUP188 Knockout Hep-G2 Cell Line is a CRISPR/Cas9-edited Hep-G2 hepatocarcinoma cell line with targeted disruption of the NUP188 gene, encoding a key scaffold nucleoporin of the nuclear pore complex. This model facilitates research on nucleocytoplasmic transport, nuclear envelope integrity, and mitotic progression. NUP188 is regulated by Cyclin B/CDK1 and Aurora A kinases and interacts with nucleoporins Nup93 and Nup155, as well as Lamin B, to control nuclear import of cargoes like ??-catenin and STAT3. The line is suited for studying nuclear transport dysfunction in hepatocellular carcinoma, cell cycle checkpoints, and screening nucleocytoplasmic transport inhibitors.

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Shipping Info:

Cryopreserved in vials and shipped on dry ice


Disclaimer:

For Research Use Only

  • Characteristics

    Host Cell

    Hep-G2

    Morphology

    Epithelial-like

    Age

    15 years

    Sex of Donor

    Male

    Gene Name

    NUP188

    Gene Species

    Homo sapiens (Human)

    Gene Identifier

    NCBI Gene ID 23511

  • Culture Conditions

    Temperature

    37°C

    Atmosphere

    5% CO₂

  • Quality Control

    Sterility testing

    Daily monitoring confirms that the cells are free from bacterial, yeast, and fungal contamination.

    Mycoplasma testing

    Negative for mycoplasma through PCR analysis

    Pathogens

    Cells tested negative for HIV-1, HBV, and HCV.

  • 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 NUP188 Knockout Hep-G2 Cell Line is a CRISPR/Cas9-edited knockout cell line derived from the Hep-G2 human hepatocellular carcinoma line, engineered for loss-of-function studies of the NUP188 gene. This product provides a genetically defined model in which CRISPR/Cas9-mediated gene disruption eliminates NUP188 expression, enabling dissection of this scaffold nucleoporin’s roles in a liver cancer context. The edited cell population provides a stable loss-of-function model for rigorous investigation of nuclear pore complex integrity, nucleocytoplasmic transport, and cell cycle progression.

Hep-G2 is a human hepatocellular carcinoma cell line with epithelial morphology, widely used in liver metabolism, toxicity testing, and hepatocarcinoma research. It retains hepatocyte-like metabolic functions and offers a consistent genetic background for comparing wild-type and NUP188-deficient states, making it an appropriate host for studying nuclear transport in cancer.

NUP188 encodes a scaffold nucleoporin integral to the nuclear pore complex (NPC), interacting with Nup93, Nup205, Nup155, Ndc1, and Lamin B. It functions downstream of Cyclin B/CDK1 and Aurora A kinases, regulated by Ran GTPase. NUP188 facilitates nuclear import of signal transducers such as STAT3 and ??-catenin and is essential for mitotic spindle assembly and nuclear envelope reorganization. These molecular interactions are critical for maintaining the selective permeability barrier and orchestrating cargo translocation. Knockout of NUP188 disrupts these processes, impairing nucleocytoplasmic trafficking and mitotic progression.

In hepatocellular carcinoma, efficient nucleocytoplasmic transport is vital for oncogenic signaling and proliferation. Loss of NUP188 in Hep-G2 cells allows investigation of how NPC dysfunction impacts ??-catenin-driven transcription and cell cycle checkpoints, potentially uncovering vulnerabilities in NPC-dependent pathways for liver cancer. This model probes the intersection of nuclear transport, mitosis, and cancer cell fitness.

Applications include Western blot and immunofluorescence to verify NUP188 ablation and assess NPC composition, nuclear import assays using fluorescent reporters, cell cycle analysis by flow cytometry, and proliferation assays (MTT/BrdU). Transcriptomic profiling via RNA-seq and co-immunoprecipitation reveal downstream pathways and altered protein interactions. The line is suited for studying nucleoporin roles in hepatocellular carcinoma, drug screening for transport inhibitors, and mitotic regulation research. Contact Ascent Research for more information.

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