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Molecular and Cellular Biology Volume 25, 2005 - Issue 4
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Gene Expression

Control of Mitochondrial Transcription Specificity Factors (TFB1M and TFB2M) by Nuclear Respiratory Factors (NRF-1 and NRF-2) and PGC-1 Family Coactivators

Natalie GleyzerDepartment of Cell and Molecular Biology, Northwestern University Medical School, Chicago, Illinois
,
Kristel VercauterenDepartment of Cell and Molecular Biology, Northwestern University Medical School, Chicago, Illinois
&
Richard C. ScarpullaDepartment of Cell and Molecular Biology, Northwestern University Medical School, Chicago, IllinoisCorrespondence[email protected]
Pages 1354-1366 | Received 18 Jun 2004, Accepted 19 Nov 2004, Published online: 27 Mar 2023
 
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Abstract

In vertebrates, mitochondrial DNA (mtDNA) transcription is initiated bidirectionally from closely spaced promoters, HSP and LSP, within the D-loop regulatory region. Early studies demonstrated that mtDNA transcription requires mitochondrial RNA polymerase and Tfam, a DNA binding stimulatory factor that is required for mtDNA maintenance. Recently, mitochondrial transcription specificity factors (TFB1M and TFB2M), which markedly enhance mtDNA transcription in the presence of Tfam and mitochondrial RNA polymerase, have been identified in mammalian cells. Here, we establish that the expression of human TFB1M and TFB2M promoters is governed by nuclear respiratory factors (NRF-1 and NRF-2), key transcription factors implicated in mitochondrial biogenesis. In addition, we show that NRF recognition sites within both TFB promoters are required for maximal trans activation by the PGC-1 family coactivators, PGC-1α and PRC. The physiological induction of these coactivators has been associated with the integration of NRFs and other transcription factors in a program of mitochondrial biogenesis. Finally, we demonstrate that the TFB genes are up-regulated along with Tfam and either PGC-1α or PRC in cellular systems where mitochondrial biogenesis is induced. Moreover, ectopic expression of PGC-1α is sufficient to induce the coordinate expression of all three nucleus-encoded mitochondrial transcription factors along with nuclear and mitochondrial respiratory subunits. These results support the conclusion that the coordinate regulation of nucleus-encoded mitochondrial transcription factors by NRFs and PGC-1 family coactivators is essential to the control of mitochondrial biogenesis.

ACKNOWLEDGMENTS

We thank Daniel P. Kelly of Washington University School of Medicine for the PGC-1α-expressing adenovirus vector and antibodies.

This work was supported by United States Public Health Service grant GM32525-22.

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