Alternol eliminates excessive ATP production by disturbing Krebs cycle in prostate cancer

Changlin Li; Chenchen He; Ying Xu; Haixia Xu; Yuzhe Tang; Hemantkumar Chavan; Shaofeng Duan; Antonio Artigues; Marcus Laird Forrest; Partha Krishnamurthy; Suxia Han; Jeffrey M Holzbeierlein; Benyi Li

doi:10.1002/pros.23767

Alternol eliminates excessive ATP production by disturbing Krebs cycle in prostate cancer

Prostate. 2019 May;79(6):628-639. doi: 10.1002/pros.23767. Epub 2019 Jan 20.

Authors

Changlin Li^{1

2}, Chenchen He^{2

3}, Ying Xu², Haixia Xu², Yuzhe Tang², Hemantkumar Chavan⁴, Shaofeng Duan⁵, Antonio Artigues⁶, Marcus Laird Forrest⁵, Partha Krishnamurthy⁴, Suxia Han³, Jeffrey M Holzbeierlein², Benyi Li²

Affiliations

¹ Institute of Precision Medicine, Jining Medical University, Jining, China.
² Department of Urology, The University of Kansas Medical Center, Kansas City, Kansas.
³ Department of Radiation Oncology, The First Affiliated Hospital, Xi'An Jiaotong University School of Medicine, Xi'An, China.
⁴ Department of Pharmacology, Toxicology & Therapeutics, The University of Kansas Medical Center, Kansas City, Kansas.
⁵ Department of Pharmaceutical Chemistry, The University of Kansas, Lawrence, Kansas.
⁶ Department of Biochemistry & Molecular Biology, The University of Kansas Medical Center, Kansas City, Kansas.

Abstract

Background: Alternol is a natural compound isolated from fermentation products of a mutant fungus. Our previous studies demonstrated that Alternol specifically kills cancer cells but spares benign cells.

Methods: To investigate the mechanism underlying alternol-induced cancer cell-specific killing effect, we took a comprehensive strategy to identify Alternol's protein targets in prostate cancer cells, including PC-3, C4-2, and 22RV1, plus benign BPH1 cell lines. Major experimental techniques included biotin-streptavidin pulldown assay coupled with mass-spectrometry, in vitro enzyme activity assay for Krebs cycle enzymes and gas chromatography-mass spectrometry (GC-MS) for metabolomic analysis.

Results: Among 14 verified protein targets, four were Krebs cycle enzymes, fumarate hydratase (FH), malate dehydrogenase-2 (MDH2), dihydrolipoamide acetyltransferase (DLAT) in pyruvate dehydrogenase complex (PDHC) and dihydrolipoamide S-succinyltransferase (DLST) in a-ketoglutarate dehydrogenase complex (KGDHC). Functional assays revealed that PDHC and KGDHC activities at the basal level were significantly higher in prostate cancer cells compared to benign prostate BPH1 cells, while alternol treatment reduced their activities in cancer cells close to the levels in BPH1 cells. Although FH and MDH2 activities were comparable among prostate cancer and benign cell lines at the basal level, Alternol treatment largely increased their activities in cancer cells. Metabolomic analysis revealed that Alternol treatment remarkably reduced the levels of malic acid, fumaric acid, and isocitric acid and mitochondrial respiration in prostate cancer cells. Alternol also drastically reduced mitochondrial respiration and ATP production in PC-3 cells in vitro or in xenograft tissues but not in BPH1 cells or host liver tissues.

Conclusions: Alternol interacts with multiple Krebs cycle enzymes, resulting in reduced mitochondrial respiration and ATP production in prostate cancer cells and xenograft tissues, providing a novel therapeutic strategy for prostate cancer treatment.

Keywords: Krebs cycle; alternol; cellular energy; metabolic enzymes; mitochondria.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adenosine Triphosphate / metabolism
Animals
Antineoplastic Agents / pharmacology
Apoptosis / drug effects*
Cell Line, Tumor
Cell Proliferation / drug effects*
Citric Acid Cycle / drug effects*
Drug Screening Assays, Antitumor / methods
Heterocyclic Compounds, 4 or More Rings / pharmacology*
Humans
Male
Mitochondria / metabolism
Prostate / metabolism*
Prostatic Neoplasms / metabolism*

Substances

Alternol
Antineoplastic Agents
Heterocyclic Compounds, 4 or More Rings
Adenosine Triphosphate

Grants and funding

R01 CA173292/CA/NCI NIH HHS/United States