Gene knockdown by large circular antisense for high-throughput functional genomics

被引:0
|
作者
Yun-Han Lee
Ik-Jae Moon
Bin Hur
Jeong-Hoh Park
Kil-Hwan Han
Seok-Yong Uhm
Yong-Joo Kim
Koo-Jeong Kang
Jong-Wook Park
Young-Bae Seu
Young-Ho Kim
Jong-Gu Park
机构
[1] WelGENE Inc.,Department of General Surgery
[2] 71B 4L,Department of Immunology
[3] Development Sector 2-3,Department of Microbiology
[4] Sungseo Industrial Park,Department of Medical Genetic Engineering
[5] Dalseogu,undefined
[6] Dongsan Medical Center,undefined
[7] Keimyung University,undefined
[8] Kyungpook National University,undefined
[9] 1370 Sangyeokdong,undefined
[10] Bookgu,undefined
[11] Keimyung University School of Medicine,undefined
[12] Kyungpook National University,undefined
[13] 1370 Sangyeokdong,undefined
[14] Bookgu,undefined
[15] College of Natural Sciences,undefined
[16] Kyungpook National University,undefined
[17] 1370 Sangyeokdong,undefined
[18] Bookgu,undefined
[19] Keimyung University School of Medicine,undefined
[20] Dongsan Medical Center,undefined
[21] 194 Dongsandong,undefined
[22] Joonggu,undefined
来源
Nature Biotechnology | 2005年 / 23卷
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摘要
Single-stranded genomic DNA of recombinant M13 phages was tested as an antisense molecule and examined for its usefulness in high-throughput functional genomics. cDNA fragments of various genes (TNF-α, c-myc, c-myb, cdk2 and cdk4) were independently cloned into phagemid vectors. Using the life cycle of M13 bacteriophages, large circular (LC)-molecules, antisense to their respective genes, were prepared from the culture supernatant of bacterial transformants. LC-antisense molecules exhibited enhanced stability, target specificity and no need for target-site searches. High-throughput functional genomics was then attempted with an LC-antisense library, which was generated by using a phagemid vector that incorporated a unidirectional subtracted cDNA library derived from liver cancer tissue. We identified 56 genes involved in the growth of these cells. These results indicate that an antisense sequence as a part of single-stranded LC-genomic DNA of recombinant M13 phages exhibits effective antisense activity, and may have potential for high-throughput functional genomics.
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页码:591 / 599
页数:8
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