Architectural Role of Mitochondrial Transcription Factor A in Maintenance of Human Mitochondrial DNA

Author:

Kanki Tomotake1,Ohgaki Kippei1,Gaspari Martina2,Gustafsson Claes M.2,Fukuoh Atsushi1,Sasaki Narie3,Hamasaki Naotaka1,Kang Dongchon1

Affiliation:

1. Department of Clinical Chemistry and Laboratory Medicine, Kyushu University Graduate School of Medical Sciences, Higashi-ku, Fukuoka

2. Department of Medical Nutrition, Karolinska Institute, Novum, Hudddinge, Sweden

3. Department of Biology, Faculty of Science, Ochanomizu University, Tokyo, Japan

Abstract

ABSTRACT Mitochondrial transcription factor A (TFAM), a transcription factor for mitochondrial DNA (mtDNA) that also possesses the property of nonspecific DNA binding, is essential for maintenance of mtDNA. To clarify the role of TFAM, we repressed the expression of endogenous TFAM in HeLa cells by RNA interference. The amount of TFAM decreased maximally to about 15% of the normal level at day 3 after RNA interference and then recovered gradually. The amount of mtDNA changed closely in parallel with the daily change in TFAM while in organello transcription of mtDNA at day 3 was maintained at about 50% of the normal level. TFAM lacking its C-terminal 25 amino acids (TFAM-ΔC) marginally activated transcription in vitro. When TFAM-ΔC was expressed at levels comparable to those of endogenous TFAM in HeLa cells, mtDNA increased twofold, suggesting that TFAM-ΔC is as competent in maintaining mtDNA as endogenous TFAM under these conditions. The in organello transcription of TFAM-ΔC-expressing cells was no more than that in the control. Thus, the mtDNA amount is finely correlated with the amount of TFAM but not with the transcription level. We discuss an architectural role for TFAM in the maintenance of mtDNA in addition to its role in transcription activation.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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