SIRT6 enhances oxidative phosphorylation in breast cancer and promotes mammary tumorigenesis in mice

Pamela Becherini; Irene Caffa; Francesco Piacente; Patrizia Damonte; Valerio G Vellone; Mario Passalacqua; Andrea Benzi; Tommaso Bonfiglio; Daniele Reverberi; Amr Khalifa; Moustafa Ghanem; Ana Guijarro; Luca Tagliafico; Marzia Sucameli; Angelica Persia; Fiammetta Monacelli; Michele Cea; Santina Bruzzone; Silvia Ravera; Alessio Nencioni

doi:10.1186/s40170-021-00240-1

SIRT6 enhances oxidative phosphorylation in breast cancer and promotes mammary tumorigenesis in mice

Cancer Metab. 2021 Jan 22;9(1):6. doi: 10.1186/s40170-021-00240-1.

Authors

Pamela Becherini^#^{1

2}, Irene Caffa^#^{1

2}, Francesco Piacente^#^{1

2

3}, Patrizia Damonte¹, Valerio G Vellone^{2

4}, Mario Passalacqua³, Andrea Benzi³, Tommaso Bonfiglio¹, Daniele Reverberi², Amr Khalifa¹, Moustafa Ghanem¹, Ana Guijarro², Luca Tagliafico¹, Marzia Sucameli¹, Angelica Persia¹, Fiammetta Monacelli^{1

2}, Michele Cea^{1

2}, Santina Bruzzone³, Silvia Ravera⁵, Alessio Nencioni^{6

7}

Affiliations

¹ Department of Internal Medicine and Medical Specialties (DIMI), University of Genoa, V.le Benedetto XV 6, 16132, Genoa, Italy.
² Ospedale Policlinico San Martino IRCCS, Largo Rosanna Benzi 10, 16132, Genoa, Italy.
³ Department of Experimental Medicine (DIMES), University of Genoa, V.le Benedetto XV 1, 16132, Genoa, Italy.
⁴ Department of Integrated, Surgical and Diagnostic Sciences (DISC), University of Genoa, L.go Rosanna Benzi 8, 16132, Genoa, Italy.
⁵ Department of Experimental Medicine (DIMES), University of Genoa, V.le Benedetto XV 1, 16132, Genoa, Italy. silvia.ravera@unige.it.
⁶ Department of Internal Medicine and Medical Specialties (DIMI), University of Genoa, V.le Benedetto XV 6, 16132, Genoa, Italy. alessio.nencioni@unige.it.
⁷ Ospedale Policlinico San Martino IRCCS, Largo Rosanna Benzi 10, 16132, Genoa, Italy. alessio.nencioni@unige.it.

^# Contributed equally.

Abstract

Background: Sirtuin 6 (SIRT6) is a NAD⁺-dependent deacetylase with key roles in cell metabolism. High SIRT6 expression is associated with adverse prognosis in breast cancer (BC) patients. However, the mechanisms through which SIRT6 exerts its pro-oncogenic effects in BC remain unclear. Here, we sought to define the role of SIRT6 in BC cell metabolism and in mouse polyoma middle T antigen (PyMT)-driven mammary tumors.

Methods: We evaluated the effect of a heterozygous deletion of Sirt6 on tumor latency and survival of mouse mammary tumor virus (MMTV)-PyMT mice. The effect of SIRT6 silencing on human BC cell growth was assessed in MDA-MB-231 xenografts. We also analyzed the effect of Sirt6 heterozygous deletion, of SIRT6 silencing, and of the overexpression of either wild-type (WT) or catalytically inactive (H133Y) SIRT6 on BC cell pyruvate dehydrogenase (PDH) expression and activity and oxidative phosphorylation (OXPHOS), including respiratory complex activity, ATP/AMP ratio, AMPK activation, and intracellular calcium concentration.

Results: The heterozygous Sirt6 deletion extended tumor latency and mouse survival in the MMTV-PyMT mouse BC model, while SIRT6 silencing slowed the growth of MDA-MB-231 BC cell xenografts. WT, but not catalytically inactive, SIRT6 enhanced PDH expression and activity, OXPHOS, and ATP/AMP ratio in MDA-MB-231 and MCF7 BC cells. Opposite effects were obtained by SIRT6 silencing, which also blunted the expression of genes encoding for respiratory chain proteins, such as UQCRFS1, COX5B, NDUFB8, and UQCRC2, and increased AMPK activation in BC cells. In addition, SIRT6 overexpression increased, while SIRT6 silencing reduced, intracellular calcium concentration in MDA-MB-231 cells. Consistent with these findings, the heterozygous Sirt6 deletion reduced the expression of OXPHOS-related genes, the activity of respiratory complexes, and the ATP/AMP ratio in tumors isolated from MMTV-PyMT mice.

Conclusions: Via its enzymatic activity, SIRT6 enhances PDH expression and activity, OXPHOS, ATP/AMP ratio, and intracellular calcium concentration, while reducing AMPK activation, in BC cells. Thus, overall, SIRT6 inhibition appears as a viable strategy for preventing or treating BC.

Keywords: Breast cancer; Cancer metabolism; Mammary tumorigenesis; Oxidative phosphorylation; SIRT6.

Abstract

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