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Cat. No. ARG0252

Mapk1 Knockout H9C2 Cell Line

  • Product Type:

    Genome-edited Cells

  • Disease:

    Normal

  • Gene Species:

    Rattus norvegicus (Rat)

The Mapk1 Knockout H9C2 Cell Line is a CRISPR/Cas9-edited loss-of-function model in rat H9C2 cardiomyoblasts. Mapk1 encodes ERK2, the terminal kinase of the MAPK/ERK cascade, which is activated by MEK1/2 and phosphorylates Elk-1 and RSK to control proliferation and survival. This knockout cell line supports studies of cardiac hypertrophy, heart failure, and ERK-dependent gene expression. Applications include drug screening, growth factor signaling analysis, and reporter assays. Key techniques are phospho-ERK western blotting and Elk-1 luciferase reporters.

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Shipping Info:

Cryopreserved in vials and shipped on dry ice


Disclaimer:

For Research Use Only

  • Characteristics

    Host Cell

    H9C2

    Age

    Embryo

    Gene Name

    Mapk1

    Gene Alias

    mitogen-activated protein kinase 1; ERK; ERK2; p41mapk; MAPK2

    Gene Species

    Rattus norvegicus (Rat)

    Gene Identifier

    NCBI Gene ID 116590

    Gene Type

    protein coding gene

  • 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 Mapk1 Knockout H9C2 Cell Line is a CRISPR/Cas9-edited knockout cell line generated from the H9C2 rat embryonic ventricular cardiomyocyte line (Rattus norvegicus). CRISPR/Cas9-mediated gene disruption of Mapk1 abolishes expression of the encoded ERK2 serine/threonine kinase, establishing a stable loss-of-function model for investigating mitogen-activated protein kinase (MAPK) signaling. This engineered cell line provides a defined genetic background for dissecting ERK2-dependent processes without the complexity of pharmacological inhibition.

The H9C2 host cell line is a well-characterized cardiac myoblast line originally derived from embryonic rat ventricular tissue. These cells exhibit many properties of developing cardiomyocytes, including expression of cardiac-specific markers and the capacity for myotube formation under appropriate conditions. As a widely adopted in vitro model for cardiac biology, H9C2 cells enable reproducible studies of cardiac hypertrophy, apoptosis, and metabolic responses. Its robust, homogenous nature suits high-throughput and mechanistic analyses.

Mapk1, encoding ERK2, functions as a terminal kinase in the classical MAPK/ERK cascade. It is activated by MEK1/2 downstream of receptors including those for EGF, FGF, and PDGF, following Ras- and Raf-mediated signal transduction. Activated ERK2 phosphorylates a broad array of cytoplasmic and nuclear substrates, such as the transcription factors Elk-1, c-Fos, c-Jun, and c-Myc, and the kinases RSK, MNK, and MSK. ERK2 also interacts with scaffold proteins like KSR and IQGAP1 that modulate pathway fidelity, and its activity is attenuated by DUSP6. Thus, ERK2 coordinates cell proliferation, differentiation, and survival.

Mapk1 ablation in H9C2 cardiomyoblasts disrupts growth factor-induced ERK signaling, impairing downstream phosphorylation and cardiac gene expression programs. This knockout model is particularly relevant for studying ERK2 roles in cardiac hypertrophy and heart failure, where ERK1/2 signaling transduces hypertrophic agonists. Additionally, as ERK2 is implicated in cancer and RASopathies like Noonan syndrome, this cell line enables investigation of disease-relevant signaling in a cardiac environment.

Applications of the Mapk1 Knockout H9C2 Cell Line include cardiac hypertrophy signaling studies, MAPK pathway functional analyses, and drug screening for heart disease. It supports western blotting for phospho-ERK1/2, RT-qPCR of immediate early genes (e.g., c-Fos), immunofluorescence for ERK translocation, cell proliferation and apoptosis assays, and luciferase reporter assays for Elk-1 activity. These assays enable precise quantification of ERK2-dependent signaling outputs and therapeutic responses. For additional information or technical support, please contact Ascent Research.

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