Functional activity of myogenic HLH proteins requires hetero-oligomerization with E12/E47-like proteins in vivo

Andrew B. Lassar; Robert L. Davis; Woodring E. Wright; Tom Kadesch; Cornelis Murre; Anna Voronova; David Baltimore; Harold Weintraub

doi:10.1016/0092-8674(91)90620-E

Functional activity of myogenic HLH proteins requires hetero-oligomerization with E12/E47-like proteins in vivo

Andrew B. Lassar, Robert L. Davis, Woodring E. Wright, Tom Kadesch, Cornelis Murre, Anna Voronova, David Baltimore, Harold Weintraub

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

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Abstract

In this report we provide four lines of evidence indicating that E12/E47-like proteins interact in vivo with the myogenic HLH proteins MyoD and myogenin. First, cotransfection of MyoD and E47 in COS cells indicates that these factors synergistically enhance transcription of a reporter gene containing an oligomerized MyoD-binding site. Second, mobility-shift assays of muscle cell nuclear extracts, "double shifted" with specific antisera, have identified complexes binding to the MEF1 site that contain either MyoD or myogenin in association with El 2/E47-like proteins. Third, association with E47 alters the phosphorylation state of MyoD. Fourth, C3H10T1/2 cells expressing antisense E2A transcripts contain low levels of E2A gene products and display less terminal muscle differentiation when infected with retroviral MyoD or when challenged to differentiate with 5-azacytidine treatment. In addition we demonstrate that MyoD, in conjunction with E12/E47-like proteins, is functioning as a regulatory nodal point for activation of several other downstream muscle regulators.

Original language	English (US)
Pages (from-to)	305-315
Number of pages	11
Journal	Cell
Volume	66
Issue number	2
DOIs	https://doi.org/10.1016/0092-8674(91)90620-E
State	Published - Jul 26 1991

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

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10.1016/0092-8674(91)90620-E

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@article{bd21309983be4a499a29c2ae4724ec9d,

title = "Functional activity of myogenic HLH proteins requires hetero-oligomerization with E12/E47-like proteins in vivo",

abstract = "In this report we provide four lines of evidence indicating that E12/E47-like proteins interact in vivo with the myogenic HLH proteins MyoD and myogenin. First, cotransfection of MyoD and E47 in COS cells indicates that these factors synergistically enhance transcription of a reporter gene containing an oligomerized MyoD-binding site. Second, mobility-shift assays of muscle cell nuclear extracts, {"}double shifted{"} with specific antisera, have identified complexes binding to the MEF1 site that contain either MyoD or myogenin in association with El 2/E47-like proteins. Third, association with E47 alters the phosphorylation state of MyoD. Fourth, C3H10T1/2 cells expressing antisense E2A transcripts contain low levels of E2A gene products and display less terminal muscle differentiation when infected with retroviral MyoD or when challenged to differentiate with 5-azacytidine treatment. In addition we demonstrate that MyoD, in conjunction with E12/E47-like proteins, is functioning as a regulatory nodal point for activation of several other downstream muscle regulators.",

author = "Lassar, {Andrew B.} and Davis, {Robert L.} and Wright, {Woodring E.} and Tom Kadesch and Cornelis Murre and Anna Voronova and David Baltimore and Harold Weintraub",

note = "Funding Information: We thank Bruce Paterson for SV2-chicken MyoD, Janet Mar and Charles Ordahl for M-CAT oligonucleotides, and our colleagues at the Hutchinson Center for their thoughtful comments and suggestions. This work was supported by grants from the NIH, Howard Hughes Medical Institute, and the Lucille P. Markey Charitable Trust; a portion of this work was supported by Public Health Service grant GM39456 (D. B.). A. 6. L. is a Lucille P. Markey Scholar.",

year = "1991",

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doi = "10.1016/0092-8674(91)90620-E",

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T1 - Functional activity of myogenic HLH proteins requires hetero-oligomerization with E12/E47-like proteins in vivo

AU - Lassar, Andrew B.

AU - Davis, Robert L.

AU - Wright, Woodring E.

AU - Kadesch, Tom

AU - Murre, Cornelis

AU - Voronova, Anna

AU - Baltimore, David

AU - Weintraub, Harold

N1 - Funding Information: We thank Bruce Paterson for SV2-chicken MyoD, Janet Mar and Charles Ordahl for M-CAT oligonucleotides, and our colleagues at the Hutchinson Center for their thoughtful comments and suggestions. This work was supported by grants from the NIH, Howard Hughes Medical Institute, and the Lucille P. Markey Charitable Trust; a portion of this work was supported by Public Health Service grant GM39456 (D. B.). A. 6. L. is a Lucille P. Markey Scholar.

PY - 1991/7/26

Y1 - 1991/7/26

N2 - In this report we provide four lines of evidence indicating that E12/E47-like proteins interact in vivo with the myogenic HLH proteins MyoD and myogenin. First, cotransfection of MyoD and E47 in COS cells indicates that these factors synergistically enhance transcription of a reporter gene containing an oligomerized MyoD-binding site. Second, mobility-shift assays of muscle cell nuclear extracts, "double shifted" with specific antisera, have identified complexes binding to the MEF1 site that contain either MyoD or myogenin in association with El 2/E47-like proteins. Third, association with E47 alters the phosphorylation state of MyoD. Fourth, C3H10T1/2 cells expressing antisense E2A transcripts contain low levels of E2A gene products and display less terminal muscle differentiation when infected with retroviral MyoD or when challenged to differentiate with 5-azacytidine treatment. In addition we demonstrate that MyoD, in conjunction with E12/E47-like proteins, is functioning as a regulatory nodal point for activation of several other downstream muscle regulators.

AB - In this report we provide four lines of evidence indicating that E12/E47-like proteins interact in vivo with the myogenic HLH proteins MyoD and myogenin. First, cotransfection of MyoD and E47 in COS cells indicates that these factors synergistically enhance transcription of a reporter gene containing an oligomerized MyoD-binding site. Second, mobility-shift assays of muscle cell nuclear extracts, "double shifted" with specific antisera, have identified complexes binding to the MEF1 site that contain either MyoD or myogenin in association with El 2/E47-like proteins. Third, association with E47 alters the phosphorylation state of MyoD. Fourth, C3H10T1/2 cells expressing antisense E2A transcripts contain low levels of E2A gene products and display less terminal muscle differentiation when infected with retroviral MyoD or when challenged to differentiate with 5-azacytidine treatment. In addition we demonstrate that MyoD, in conjunction with E12/E47-like proteins, is functioning as a regulatory nodal point for activation of several other downstream muscle regulators.

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Functional activity of myogenic HLH proteins requires hetero-oligomerization with E12/E47-like proteins in vivo

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