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常温
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- 英文名:
Pluronic® F-127
- 库存:
有现货
- 供应商:
浙江羽翔生物科技有限公司
- CAS号:
9003-11-6
- 规格:
250G
属性
描述
Non-ionic
contains 100ppm BHT
质量水平
200
产品线
BioReagent
表单
powder
分子量
~12600 g/mol
技术
cell culture | mammalian: suitable
CMC
950-1000 ppm (~25°C)
转变温度
cloud point >100 °C
HLB
18 - 23
SMILES字符串
O2C(C2)C.O1CC1
InChI
1S/C3H6O.C2H4O/c1-3-2-4-3;1-2-3-1/h3H,2H2,1H3;1-2H2
InChI key
RVGRUAULSDPKGF-UHFFFAOYSA-N
一般描述
应用
- 作为肽到伤口部位的递送系统,以研究肽对小鼠伤口愈合的影响。
- 作为 PDMS(聚二甲基硅氧烷)印章的表面涂层,使其具有水凝胶排斥性。
- 制备用于测量神经活动的钙指示剂储备溶液。
- 作为磷酸盐缓冲盐水 (PBS) 的成分,可降低非特异性细胞和蛋白质对基于 PDMS 的微流体装置的粘附。
- 这种非离子共聚物表面活性剂适合作为消泡剂用于昆虫细胞培养应用。
生化/生理作用
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文献和实验Critical role of ATP-induced ATP release for Ca2+ signaling in nonsensory cell networks of the developing cochlea.
Spatially and temporally coordinated variations of the cytosolic free calcium concentration ([Ca2+]c) play a crucial role in a variety of tissues. In the developing sensory epithelium of the mammalian cochlea, elevation of extracellular adenosine trisphosphate concentration ([ATP]e) triggers [Ca2+]c oscillations and propagation of intercellular inositol 1,4,5-trisphosphate (IP3)-dependent Ca2+ waves. What remains uncertain is the relative contribution of gap junction channels and connexin hemichannels to these fundamental mechanisms, defects in which impair hearing acquisition. Another related open question is whether [Ca2+]c oscillations require oscillations of the cytosolic IP3 concentration ([IP3]c) in this system. To address these issues, we performed Ca2+ imaging experiments in the lesser epithelial ridge of the mouse cochlea around postnatal day 5 and constructed a computational model in quantitative adherence to experimental data. Our results indicate that [Ca2+]c oscillations are governed by Hopf-type bifurcations within the experimental range of [ATP]e and do not require [IP3]c oscillations. The model replicates accurately the spatial extent and propagation speed of intercellular Ca2+ waves and predicts that ATP-induced ATP release is the primary mechanism underlying intercellular propagation of Ca2+ signals. The model also uncovers a discontinuous transition from propagating regimes (intercellular Ca2+ wave speed > 11 μm⋅s-1) to propagation failure (speed = 0), which occurs upon lowering the maximal ATP release rate below a minimal threshold value. The approach presented here overcomes major limitations due to lack of specific connexin channel inhibitors and can be extended to other coupled cellular systems.
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