Targeting the Transcriptional Machinery with Unique Artificial Transcriptional Activators

Zhiqian (James) Wu; Garrette Belanger; Brian B Brennan; Jenifer K Lum; Aaron R Minter; Steven P Rowe; Annette Plachetka; Chinmay Y Majmudar; Anna K Mapp

doi:10.1021/ja036685v

Targeting the Transcriptional Machinery with Unique Artificial Transcriptional Activators

Zhiqian (James) Wu, Garrette Belanger, Brian B Brennan, Jenifer K Lum, Aaron R Minter, Steven P Rowe, Annette Plachetka, Chinmay Y Majmudar, Anna K Mapp

Research output: Contribution to journal › Article › peer-review

Abstract

The link between a growing number of human diseases and misregulation of gene expression has spurred intense interest in artificial transcriptional activators that could be used to restore controlled expression of affected genes. To expand the repertoire of activation domains available for the construction of artificial transcriptional regulators, a selection strategy was used to identify two unique activation domain motifs. These activation domains bear little sequence homology to endogenous counterparts and bind to unique sites within the transcriptional machinery. A comparison with two well-characterized activation domains, VP2 and P201, demonstrated for the first time that functional potency is not solely dictated by binding affinity. Finally, the selection strategy described is readily applicable to the identification of small molecule activation domains.

Original language	American English
Journal	Journal of the American Chemical Society
Volume	125
DOIs	https://doi.org/10.1021/ja036685v
State	Published - 2003

Disciplines

Medicine and Health Sciences
Pharmacy and Pharmaceutical Sciences

Access to Document

10.1021/ja036685vLicense: Unspecified

Cite this

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title = "Targeting the Transcriptional Machinery with Unique Artificial Transcriptional Activators",

abstract = " The link between a growing number of human diseases and misregulation of gene expression has spurred intense interest in artificial transcriptional activators that could be used to restore controlled expression of affected genes. To expand the repertoire of activation domains available for the construction of artificial transcriptional regulators, a selection strategy was used to identify two unique activation domain motifs. These activation domains bear little sequence homology to endogenous counterparts and bind to unique sites within the transcriptional machinery. A comparison with two well-characterized activation domains, VP2 and P201, demonstrated for the first time that functional potency is not solely dictated by binding affinity. Finally, the selection strategy described is readily applicable to the identification of small molecule activation domains. ",

author = "Wu, {Zhiqian (James)} and Garrette Belanger and Brennan, {Brian B} and Lum, {Jenifer K} and Minter, {Aaron R} and Rowe, {Steven P} and Annette Plachetka and Majmudar, {Chinmay Y} and Mapp, {Anna K}",

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journal = "Journal of the American Chemical Society",

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AU - Wu, Zhiqian (James)

AU - Belanger, Garrette

AU - Brennan, Brian B

AU - Lum, Jenifer K

AU - Minter, Aaron R

AU - Rowe, Steven P

AU - Plachetka, Annette

AU - Majmudar, Chinmay Y

AU - Mapp, Anna K

PY - 2003

Y1 - 2003

N2 - The link between a growing number of human diseases and misregulation of gene expression has spurred intense interest in artificial transcriptional activators that could be used to restore controlled expression of affected genes. To expand the repertoire of activation domains available for the construction of artificial transcriptional regulators, a selection strategy was used to identify two unique activation domain motifs. These activation domains bear little sequence homology to endogenous counterparts and bind to unique sites within the transcriptional machinery. A comparison with two well-characterized activation domains, VP2 and P201, demonstrated for the first time that functional potency is not solely dictated by binding affinity. Finally, the selection strategy described is readily applicable to the identification of small molecule activation domains.

AB - The link between a growing number of human diseases and misregulation of gene expression has spurred intense interest in artificial transcriptional activators that could be used to restore controlled expression of affected genes. To expand the repertoire of activation domains available for the construction of artificial transcriptional regulators, a selection strategy was used to identify two unique activation domain motifs. These activation domains bear little sequence homology to endogenous counterparts and bind to unique sites within the transcriptional machinery. A comparison with two well-characterized activation domains, VP2 and P201, demonstrated for the first time that functional potency is not solely dictated by binding affinity. Finally, the selection strategy described is readily applicable to the identification of small molecule activation domains.

U2 - 10.1021/ja036685v

DO - 10.1021/ja036685v

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VL - 125

JO - Journal of the American Chemical Society

JF - Journal of the American Chemical Society

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