Literature DB >> 21914785

PGC1α promotes tumor growth by inducing gene expression programs supporting lipogenesis.

Kavita Bhalla1, Bor Jang Hwang, Ruby E Dewi, Lihui Ou, William Twaddel, Hong-Bin Fang, Scott B Vafai, Francesca Vazquez, Pere Puigserver, Laszlo Boros, Geoffrey D Girnun.   

Abstract

Despite the role of aerobic glycolysis in cancer, recent studies highlight the importance of the mitochondria and biosynthetic pathways as well. PPARγ coactivator 1α (PGC1α) is a key transcriptional regulator of several metabolic pathways including oxidative metabolism and lipogenesis. Initial studies suggested that PGC1α expression is reduced in tumors compared with adjacent normal tissue. Paradoxically, other studies show that PGC1α is associated with cancer cell proliferation. Therefore, the role of PGC1α in cancer and especially carcinogenesis is unclear. Using Pgc1α(-/-) and Pgc1α(+/+) mice, we show that loss of PGC1α protects mice from azoxymethane-induced colon carcinogenesis. Similarly, diethylnitrosamine-induced liver carcinogenesis is reduced in Pgc1α(-/-) mice as compared with Pgc1α(+/+) mice. Xenograft studies using gain and loss of PGC1α expression showed that PGC1α also promotes tumor growth. Interestingly, while PGC1α induced oxidative phosphorylation and tricarboxylic acid cycle gene expression, we also observed an increase in the expression of two genes required for de novo fatty acid synthesis, ACC and FASN. In addition, SLC25A1 and ACLY, which are required for the conversion of glucose into acetyl-CoA for fatty acid synthesis, were also increased by PGC1α, thus linking the oxidative and lipogenic functions of PGC1α. Indeed, using stable (13)C isotope tracer analysis, we show that PGC1α increased de novo lipogenesis. Importantly, inhibition of fatty acid synthesis blunted these progrowth effects of PGC1α. In conclusion, these studies show for the first time that loss of PGC1α protects against carcinogenesis and that PGC1α coordinately regulates mitochondrial and fatty acid metabolism to promote tumor growth. ©2011 AACR.

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Year:  2011        PMID: 21914785      PMCID: PMC3282487          DOI: 10.1158/0008-5472.CAN-11-1011

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  50 in total

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9.  PGC-1alpha-responsive genes involved in oxidative phosphorylation are coordinately downregulated in human diabetes.

Authors:  Vamsi K Mootha; Cecilia M Lindgren; Karl-Fredrik Eriksson; Aravind Subramanian; Smita Sihag; Joseph Lehar; Pere Puigserver; Emma Carlsson; Martin Ridderstråle; Esa Laurila; Nicholas Houstis; Mark J Daly; Nick Patterson; Jill P Mesirov; Todd R Golub; Pablo Tamayo; Bruce Spiegelman; Eric S Lander; Joel N Hirschhorn; David Altshuler; Leif C Groop
Journal:  Nat Genet       Date:  2003-07       Impact factor: 38.330

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Review 2.  The diverse role of the PPARγ coactivator 1 family of transcriptional coactivators in cancer.

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Journal:  Semin Cell Dev Biol       Date:  2012-01-21       Impact factor: 7.727

3.  B7-H4 downregulation induces mitochondrial dysfunction and enhances doxorubicin sensitivity via the cAMP/CREB/PGC1-α signaling pathway in HeLa cells.

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Journal:  Pflugers Arch       Date:  2014-12       Impact factor: 3.657

4.  Sleeping Beauty screen reveals Pparg activation in metastatic prostate cancer.

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5.  Loss of SETD2 Induces a Metabolic Switch in Renal Cell Carcinoma Cell Lines toward Enhanced Oxidative Phosphorylation.

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6.  PPARγ Regulates Mitochondrial Structure and Function and Human Pulmonary Artery Smooth Muscle Cell Proliferation.

Authors:  Samantha M Yeligar; Bum-Yong Kang; Kaiser M Bijli; Jennifer M Kleinhenz; Tamara C Murphy; Gloria Torres; Alejandra San Martin; Roy L Sutliff; C Michael Hart
Journal:  Am J Respir Cell Mol Biol       Date:  2018-05       Impact factor: 6.914

7.  De novo lipogenesis represents a therapeutic target in mutant Kras non-small cell lung cancer.

Authors:  Anju Singh; Christian Ruiz; Kavita Bhalla; John A Haley; Qing Kay Li; George Acquaah-Mensah; Emily Montal; Kuladeep R Sudini; Ferdinandos Skoulidis; Ignacio I Wistuba; Vassiliki Papadimitrakopoulou; John V Heymach; Laszlo G Boros; Edward Gabrielson; Julian Carretero; Kwok-Kin Wong; John D Haley; Shyam Biswal; Geoffrey D Girnun
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8.  Distinct Metabolic Signature of Human Bladder Cancer Cells Carrying an Impaired Fanconi Anemia Tumor-Suppressor Signaling Pathway.

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