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- 文献和实验
- 技术资料
- 保存条件:
常温
- 保质期:
根据瓶身LOT号查询
- 英文名:
Glycerol
- 库存:
有现货
- 供应商:
浙江羽翔生物科技有限公司
- CAS号:
56-81-5
- 规格:
100ml
属性
生物来源
synthetic (organic)
质量水平
200
蒸汽密度
3.1 (vs air)
蒸汽压
<1 mmHg ( 20 °C)
方案
≥99.5%
表单
viscous liquid
自燃温度
698 °F
技术
immunofluorescence: suitable
杂质
≤0.20% Water (Karl Fischer)
颜色
colorless
折射率
n20/D 1.474 (lit.)
沸点
182 °C/20 mmHg (lit.)
mp
20 °C (lit.)
溶解性
water: 1 mL/mL, clear, colorless to faintly yellow
密度
1.25 g/mL (lit.)
痕量阳离子
heavy metals (as Pb): ≤5 ppm
λ
1 cm path
紫外吸收
λ: 205 nm Amax: 1.0
λ: 225 nm Amax: 0.40
λ: 280 nm Amax: 0.10
λ: 320 nm Amax: 0.04
λ: 340 nm Amax: 0.01
λ: 400 nm Amax: 0.01
适用性
suitable for component for culture media
应用
lipidomics
liquid formulation
sample preservation
储存温度
room temp
SMILES字符串
OCC(O)CO
InChI
1S/C3H8O3/c4-1-3(6)2-5/h3-6H,1-2H2
InChI key
PEDCQBHIVMGVHV-UHFFFAOYSA-N
一般描述
应用
生化/生理作用
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文献和实验Inhibition of DHFR targets the self-renewing potential of brain tumor initiating cells.
Brain tumors are a heterogeneous group of benign and malignant tumors arising from the brain parenchyma and its surrounding structures, with in general a poor clinical outcome due to high recurrence. One of the underlying causes for this somber prognostic is the presence of brain tumor initiating cells (BTIC) endowed with self-renewal potential, multi-lineage differentiation and resistance to treatment. One promising therapeutic avenue for brain tumors is targeting BTIC self-renewal potential and forcing their differentiation. A compelling candidate is one-carbon metabolism shown to play a key role in maintaining stem cell self-renewal in several lineages. Here, we focus on dihydrofolate reductase (DHFR), a key enzyme in one-carbon metabolism, and demonstrate this enzyme's overexpression in several human brain tumors and its expression in human BTIC. We show that DHFR inhibition, either by Methotrexate (MTX) or EphB activation with synthetic ligands, reduces the tumorigenic potential of 4 human BTIC lines, by reducing their self-renewal capacities both in vitro and in a cerebral organoid glioma (GLICO) model. Our data indicate that driving BTIC differentiation by inhibiting DHFR may provide a new therapeutic approach to treating highly refractory aggressive tumors.
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