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薛天
( 教授 )
的个人主页 http://faculty.ustc.edu.cn/xuetian/zh_CN/index.htm
教授
电子邮箱:
af58d3d59ebb0e158b4f244d8cf0c2eb74dcfef7e7a69f8206e5d2bd830f1b8d70bd5a35f925c8cd3335c4f467a371f432db56be948f64daa30c46bb9a6f40dba055ccd0c6a905239d0e2508fc381795b9bbf4554880bedc895bcb64f92816f09fa2757c488d69e460f123dffe9d1e110b86633faa8996c68f5f82d16ec2f371
职务:
生命科学与医学部分管校领导
学位:
博士
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[1]
48. Li RA, Sato K, Kodama K, Kohno T, Xue T, Tomaselli GF, Marban E. (2002). Charge conversion enables quantification of the proximity between a normally-neutral mu-conotoxin (GIIIA) site and the Na+ channel pore. FEBS Lett. 511, 159-164..2021,
[2]
47. Xue T, Marbán E, Li RA (2002). Dominant-negative suppression of HCN1- and HCN2-encoded pacemaker currents by an engineered HCN1 construct: Insights into structure-function relationships and multimerization. Circ. Res. 90, 1267-1273..2021,
[3]
46. Xue T, Li RA (2002). An external determinant in the S5-P linker of the pacemaker (HCN) channel identified by sulfhydryl modification. J. Biol. Chem. 277, 46233-42..2021,
[4]
45. Li RA, Ennis I, Xue T, Nguyen HM, Tomaselli GF, Goldin AL, Marbán E (2003). Molecular basis of isoform-specific µ-conotoxin block of cardiac, skeletal muscle and brain Na channels. J. Biol. Chem. 278, 8717-24..2021,
[5]
44. Henrikson CA, Xue T, Dong P, Sang D, Marbán E, Li RA (2003). Identification of a surface charged residue in the S3-S4 linker of pacemaker (HCN) channel that influences activation gating. J. Biol. Chem. 278, 13647-54..2021,
[6]
43. Azene EM#, Xue T#, Li RA (2003). Molecular basis of the effects of potassium on heterologously-expressed pacemaker (HCN) channels. J. Physiol. 547, 349-356..2021,
[7]
42. Xue T, Sato K, Kodama K, Ennis I, French RJ, Li RA (2003). Novel interactions identified between µ-conotoxin and the Na+ channel Domain I P-loop: Implications for toxin-pore binding geometry. Biophys. J. 85, 2299-310..2021,
[8]
41. Xue T#, Cho H#, Akar F#, Tsang SY, Jones S, Marbán E, Tomaselli GF, Li RA (2005). Functional Integration of Electrically Active Cardiac Derivatives from Genetically Engineered Human Embryonic Stem Cells with Quiescent Recipient Ventricular Cardiomyocytes. Insights into the Development of Cell-Based Pacemakers. Circulation 11, 111-20. Issue highlights, Best Paper Award, Circulation 2005.2021,
[9]
40. Wang G#, Xue T#, Tsang SY, Wong J, Cheng L, Zhang J, Li GR, Lau CP, Li RA, Tse HF (2005). Electrophysiological properties of pluripotent human and mouse embryonic stem cells. Stem Cells 23, 1526-34. .2021,
[10]
39. Azene EM, Xue T, Marban E, Tomaselli GF, Li RA (2005). Non-equilibrium behavior of HCN channels: Insights into the role of HCN channels in native and engineered pacemakers. Cardiovasc Res. 67, 263-73..2021,
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