Detecting Kinase Activities from Single Cell Lysate Using Concentration-Enhanced Mobility Shift Assay

被引：37

作者：

Cheow, Lih Feng ^{[1
]}

Sarkar, Aniruddh ^{[1
]}

Kolitz, Sarah ^{[2
]}

Lauffenburger, Douglas ^{[2
]}

Han, Jongyoon ^{[1
,2
]}

机构：

[1] MIT, Dept Elect Engn & Comp Sci, Cambridge, MA 02139 USA

[2] MIT, Dept Biol Engn, Cambridge, MA 02139 USA

来源：

ANALYTICAL CHEMISTRY | 2014年 / 86卷 / 15期

关键词：

CAPILLARY-ZONE-ELECTROPHORESIS; PROTEIN-KINASE; DYNAMICS; LYSIS; SENSITIVITY; DEVICE; STATES; ISOTACHOPHORESIS; PRECONCENTRATION; PHOSPHORYLATION;

D O I：

10.1021/ac502185v

中图分类号：

O65 [分析化学];

学科分类号：

070302 ; 081704 ;

摘要：

Electrokinetic preconcentration coupled with mobility shift assays can give rise to very high detection sensitivities. We describe a microfluidic device that utilizes this principle to detect cellular kinase activities by simultaneously concentrating and separating substrate peptides with different phosphorylation states. This platform is capable of reliably measuring kinase activities of single adherent cells cultured in nanoliter volume microwells. We also describe a novel method utilizing spacer peptides that significantly increase separation resolution while maintaining high concentration factors in this device. Thus, multiplexed kinase measurements can be implemented with single cell sensitivity. Multiple kinase activity profiling from single cell lysate could potentially allow us to study heterogeneous activation of signaling pathways that can lead to multiple cell fates.

引用

页码：7455 / 7462

页数：8

共 47 条

[1]

Babu CVS, 2005, ELECTROPHORESIS, V26, P3765, DOI [10.1002/elps.20050007, 10.1002/elps.200500007]

[2] Method for Analyte Identification Using Isotachophoresis and a Fluorescent Carrier Ampholyte Assay [J].

Bercovici, M. ;

Kaigala, G. V. ;

Santiago, J. G. .

ANALYTICAL CHEMISTRY, 2010, 82 (05) :2134-2138

[3]

BERENBAUM MC, 1972, CANCER CHEMOTH REP 1, V56, P563

[4] Multiplexed mass cytometry profiling of cellular states perturbed by small-molecule regulators [J].

Bodenmiller, Bernd ;

Zunder, Eli R. ;

Finck, Rachel ;

Chen, Tiffany J. ;

Savig, Erica S. ;

Bruggner, Robert V. ;

Simonds, Erin F. ;

Bendall, Sean C. ;

Sachs, Karen ;

Krutzik, Peter O. ;

Nolan, Garry P. .

NATURE BIOTECHNOLOGY, 2012, 30 (09) :858-U89

[5] Continuous Signal Enhancement for Sensitive Aptamer Affinity Probe Electrophoresis Assay Using Electrokinetic Concentration [J].

Cheow, Lih Feng ;

Han, Jongyoon .

ANALYTICAL CHEMISTRY, 2011, 83 (18) :7086-7093

[6] Increasing the Sensitivity of Enzyme-Linked Immunosorbent Assay Using Multiplexed Electrokinetic Concentrator [J].

Cheow, Lih Feng ;

Ko, Sung Hee ;

Kim, Sung Jae ;

Kang, Kwan Hyoung ;

Han, Jongyoon .

ANALYTICAL CHEMISTRY, 2010, 82 (08) :3383-3388

[7] A microchamber array for single cell isolation and analysis of intracellular biomolecules [J].

Eyer, Klaus ;

Kuhn, Phillip ;

Hanke, Conni ;

Dittrich, Petra S. .

LAB ON A CHIP, 2012, 12 (04) :765-772

[8] Tripping the switch fantastic: How a protein kinase cascade can convert graded inputs into switch-like outputs [J].

Ferrell, JE .

TRENDS IN BIOCHEMICAL SCIENCES, 1996, 21 (12) :460-466

[9] Integration of single cell injection, cell lysis, separation and detection of intracellular constituents on a microfluidic chip [J].

Gao, J ;

Yin, XF ;

Fang, ZL .

LAB ON A CHIP, 2004, 4 (01) :47-52

[10] Prediction of electrophoretic mobilities of peptides in capillary zone electrophoresis by quantitative structure-mobility relationships using the offord model and artificial neural networks [J].

Jalali-Heravi, M ;

Shen, Y ;

Hassanisadi, M ;

Khaledi, MG .

ELECTROPHORESIS, 2005, 26 (10) :1874-1885

← 1 2 3 4 5 →