KC-6194

TMD8-PLCG2-R665W-KI Cell Line

61306

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Background of TMD8-PLCG2-R665W-KI Cell Line

PLCG2-R665W is a gain-of-function missense mutation in the phospholipase C gamma 2 (PLCG2) gene. This mutation substitutes arginine with tryptophan at position 665, located in the autoinhibitory SH2 domain of the PLCγ2 enzyme, which normally represses basal catalytic activity. The substitution disrupts this autoinhibition, leading to constitutive activation of PLCγ2. This results in sustained intracellular calcium flux, hyperactive downstream signaling (e.g., via NF-κB and MAPK pathways), and aberrant B-cell and myeloid cell activation. The PLCG2-R665W mutation is a primary genetic cause of *autoinflammation and PLCγ2-associated antibody deficiency and immune dysregulation* (APLAID), a rare autosomal dominant syndrome. Clinical manifestations include early-onset systemic autoinflammation (e.g., erythematous plaques, arthralgia), recurrent infections, and antibody deficiency. Unlike the related PLCG2-L845F mutation, APLAID driven by R665W typically lacks cold-induced urticaria. The mutation highlights the critical role of PLCγ2 autoinhibition in immune homeostasis and presents a target for developing specific kinase or PLCγ2 inhibitors.

Specifications

Catalog Number	KC-6194
Cell Line Name	TMD8-PLCG2-R665W-KI Cell Line
Clone Number	1A2
Host Cell Line	TMD8
Description	Stable TMD8 clone expressing endogenous PLCG2 gene bearing R665W mutations, No.1A2
Quantity	Two vials of frozen cells (≥2-10⁶/vial)
Stability	Stable in culture over a minimum of 10 passages
Application	Drug screening and biological assays
Freezing Medium	70% RPMI1640+20% FBS+10% DMSO
Propagation Medium	RPMI1640+10% FBS
Selection Marker	NA
Morphology	Lymphoblast
Subculture	Split saturated culture 1:3-1:6 every 2-3 days; seed out at about 1-3 × 10⁵ cells/mL
Incubation	37 °C with 5% CO₂
Storage	Liquid nitrogen immediately upon receiving
Doubling Time	Approximately 30 hours
Mycoplasma Status	Negative

Cell Line Generation

TMD8-PLCG2-R665W-KI cell line was generated using the CRISPR method.

Characterization

Figure 1: Characterization of TMD8-PLCG2-R665W-KI cell line stable clone using PCR sequencing.

Figure 2: Characterization of TMD8-PLCG2-R665W-KI cell line stable clone using RT-PCR sequencing.

Figure 3. Characterization of dose-response curves for PLCG2 inhibitors on TMD8 and TMD8-PLCG2-R665W-KI cells.

Cell Resuscitation

Prewarm culture medium (RPMI1640 + 10% FBS)in a 37°C water bath.
Thaw the frozen vial in a 37°C water bath for 1-2 minutes.
Transfer the vial into biosafety cabinet, and wipe the surface with 70% ethanol.
Unscrew the top of the vial and transfer the cell suspension gently into a sterile centrifuge tube containing 9.0mL complete culture medium.
Spin at ~ 125 × g for 5-7 minutes at room temperature, and discard the supernatant without disturbing the pellet.
Resuspend cell pellet with the appropriate volume of complete medium and transfer the cell suspension into a T25 culture flask.
Incubate the flask at 37°C, 5% CO₂ incubator.
Split saturated culture 1:3-1:6 every 2-3 days; seed out at about 1-3 × 10⁵ cells/mL.

Cell Freezing

Prepare the freezing medium (70% RPMI1640 + 20% FBS + 10% DMSO) fresh immediately before use.
Keep the freezing medium on ice and label cryovials.
Transfer cells to a sterile, conical centrifuge tube, and count the cells.
Centrifuge the cells at 250×g for 5 minutes at room temperature and carefully aspirate off the medium.
Resuspend the cells at a density of at least 3×10⁶ cells/mL in chilled freezing medium.
Aliquot 1 mL of the cell suspension into each cryovial.
Freeze cells in the CoolCell freezing container overnight in a -80°C freezer.
Transfer vials to liquid nitrogen for long-term storage

References

Neves, J.F., et al. (2018). "The PLCG2-R665W mutation causes a unique autoinflammatory disease distinct from PLAID." Journal of Allergy and Clinical Immunology, 141(3), 1052-1055.
Zhou, Q., et al. (2012). "A hypermorphic missense mutation in PLCG2, encoding phospholipase Cγ2, causes a dominantly inherited autoinflammatory disease with immunodeficiency." American Journal of Human Genetics, 91(4), 713-720.
Hoxha, V., et al. (2023). "PLCG2-associated diseases: from genetics to targeted therapy." Journal of Clinical Immunology, 43(6), 1097-1110.