Nsg nod scid mice

Manufactured by Jackson ImmunoResearch

NSG (NOD-SCID) mice are a strain of immunodeficient mice developed for use in biomedical research. They lack mature T cells, B cells, and natural killer cells, making them suitable for engraftment of human cells and tissues.

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Lab products found in correlation

Matrigel, by BD (2 mentions)

Close spelling variants of this product

NOD-scid IL2Rγnull (NSG) mice NOD Scid gamma (NSG; NOD-SCID) mice Immunodeficient NSG (NOD/LtSz-scid/IL2Rγnull) mice Female NOD/SCID/IL-2Rγ−/− (NSG) mice NOD-scid IL2Rgnull (NSG) mice NOD-SCID-γ chain−/− (NSG) mice NOD-scid γcnull (NSG) mice NOD/LtSz-scid/IL2Rγ cnull (NSG) mice Female NOD-SCID-γc−/− (NSG) mice IL2Rcg−/−Nod.Scid (NSG) mice

2 protocols using nsg nod scid mice

Evaluating KRAS and BRAF Inhibitors in Mice

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PLX4032, AMG-510, and MRTX-1257 were dissolved in 2% DMSO + 30% PEG 300 + 5% Tween 80 + ddH2O. Tumors were engrafted in NSG (NOD-SCID) mice (The Jackson Laboratory) by subcutaneous injection of 3 × 10⁵ A375 or H2122 cells in RPMI-1640 medium supplemented with 50% Matrigel (BD Biosciences, cat. no. 354234). Seven days after the injection, animals were assigned randomly to control and various treatment groups (n = 5 for each group). Tumor bearing mice were administered by oral garvage: (1) Vehicle, 2% DMSO + 30% PEG 300 + 5% Tween 80 + ddH2O; (2) PLX4032, 1 mg/kg body weight/day; (3) Atorvastatin, 1.2 mg/kg body weight/day; (4) AMG-510, 5 mg/kg body weight/day; (5) MRTX-1257, 3 mg/kg body weight/day. The mice were treated every other day. Tumors were measured with an external caliper, and the volume was calculated as (4π/3) × (width/2)² × (length/2).

Wang X.D., Kim C., Zhang Y., Rindhe S., Cobb M.H, & Yu Y. (2021). Cholesterol Regulates the Tumor Adaptive Resistance to MAPK Pathway Inhibition. Journal of proteome research, 20(12), 5379-5391.

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Evaluating Anti-Cancer Drug Efficacy

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PLX4032, AMG-510, and MRTX-1257 were dissolved in 2% DMSO + 30% PEG 300 + 5% Tween 80 + ddH2O. Tumors were engrafted in NSG (NOD-SCID) mice (The Jackson Laboratory) by subcutaneous injection of 3 × 10 5 A375 or H2122 cells in RPMI-1640 medium supplemented with 50% Matrigel (BD Biosciences, cat. no. 354234). Seven days after the injection, animals were assigned randomly to control and various treatment groups (n = 5 for each group). Tumor bearing mice were administered by oral garvage: (1) Vehicle, 2% DMSO + 30% PEG 300 + 5% Tween 80 + ddH2O; (2) PLX4032, 1 mg/kg body weight/day; (3) Lipitor, 1.2 mg/ kg body weight/ day; (4) AMG-510, 5 mg /kg body weight/day; (5) MRTX-1257, 3 mg/ kg body weight/day. The mice were treated every other day. Tumors were measured with an external caliper, and the volume was calculated as (4π/3) × (width/2) 2 × (length/2).

Wang X., Kim C., Zhang Y., Rindhe S., Cobb M.H., & Yu Y. (2021). Quantitative Tyr Phosphoproteomic Analyses Identify Cholesterol as a Master Regulator of the Tumor Adaptive Resistance to MAPK Inhibition.

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