位置:成果数据库 > 期刊 > 期刊详情页
Binomial distribution-based quantitative measurement of multiple-acceptors fluorescence resonance e
  • 期刊名称:APPLIED PHYSICS LETTERS
  • 时间:2014.8.20
  • 页码:-
  • 相关项目:活细胞中蛋白质寡聚化动态过程实时荧光成像与定量分析技术研究
作者: Huaina Yu|Jianwei Zhang|Xiaoping Wang|Tongsheng Chen|
同期刊论文项目
活细胞中蛋白质寡聚化动态过程实时荧光成像与定量分析技术研究
期刊论文 33 会议论文 1
同项目期刊论文
Intratumoral injection of taxol in vivo suppresses A549 tumor showing cytoplasmic vacuolization
Potent proapoptotic actions of dihydroartemisinin in gemcitabine-resistant A549 cells
Binomial distribution-based quantitative measurement of multiple-acceptors fluorescence resonance en
Dihydroarteminsin (DHA) induced apoptosis is not dependent on the translocation of Bim to the endopl
One-step Reduction and PEGylation of Graphene Oxide for Photothermally Controlled Drug Delivery.
Potent proapoptotic actions of dihydroartemisinin in gemcitabine-resistant A549 cells.
Facile and green reduction of covalently PEGylated nano-graphene oxide via a “water-only” route for
Resveratrol protects rabbit articular chondrocyte against sodium nitroprusside-induced apoptosis via
Spectral measurement of acceptor-to-donor extinction coefficient ratio in living cells
Quantitative FRET measurement via unmixing emission spectra with independent cross excitation correc
Synergistic induction of apoptosis in A549 cells by dihydroartemisinin and gemcitabine
One-step reduction and PEGylation of graphene oxide for photothermally controlled drug delivery
Facile and green reduction of covalently PEGylated nanographene oxide via a 'water-only' r
Resveratrol Protects Chondrocytes from Apoptosis via Altering the Ultrastructural and Biomechanical
Maximum Entropy Method-based Acceptor Triplet-State Fluorescence Correlation Spectroscopy Analysis f
Miniature fiber optic spectrometer-based quantitative fluorescence resonance energy transfer measure
Dihydroartemisinin induces apoptosis preferentially via a Bim/Bak-mediated intrinsic pathway in hepa
Artesunate induces apoptosis via a ROS-independent Bax-mediated intrinsic pathway in HepG2 cells.