Literature DB >> 25583489

Natural variations of copper and sulfur stable isotopes in blood of hepatocellular carcinoma patients.

Vincent Balter1, Andre Nogueira da Costa2, Victor Paky Bondanese3, Klervia Jaouen4, Aline Lamboux3, Suleeporn Sangrajrang5, Nicolas Vincent3, François Fourel3, Philippe Télouk3, Michelle Gigou6, Christophe Lécuyer7, Petcharin Srivatanakul5, Christian Bréchot8, Francis Albarède3, Pierre Hainaut9.   

Abstract

The widespread hypoxic conditions of the tumor microenvironment can impair the metabolism of bioessential elements such as copper and sulfur, notably by changing their redox state and, as a consequence, their ability to bind specific molecules. Because competing redox state is known to drive isotopic fractionation, we have used here the stable isotope compositions of copper ((65)Cu/(63)Cu) and sulfur ((34)S/(32)S) in the blood of patients with hepatocellular carcinoma (HCC) as a tool to explore the cancer-driven copper and sulfur imbalances. We report that copper is (63)Cu-enriched by ∼0.4‰ and sulfur is (32)S-enriched by ∼1.5‰ in the blood of patients compared with that of control subjects. As expected, HCC patients have more copper in red blood cells and serum compared with control subjects. However, the isotopic signature of this blood extra copper burden is not in favor of a dietary origin but rather suggests a reallocation in the body of copper bound to cysteine-rich proteins such as metallothioneins. The magnitude of the sulfur isotope effect is similar in red blood cells and serum of HCC patients, implying that sulfur fractionation is systemic. The (32)S-enrichment of sulfur in the blood of HCC patients is compatible with the notion that sulfur partly originates from tumor-derived sulfides. The measurement of natural variations of stable isotope compositions, using techniques developed in the field of Earth sciences, can provide new means to detect and quantify cancer metabolic changes and provide insights into underlying mechanisms.

Entities:  

Keywords:  cancer; copper; liver; stable isotopes; sulfur

Mesh:

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Year:  2015        PMID: 25583489      PMCID: PMC4313854          DOI: 10.1073/pnas.1415151112

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  24 in total

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  28 in total

1.  Evidence of isotopic fractionation of natural uranium in cultured human cells.

Authors:  Eduardo Paredes; Emilie Avazeri; Véronique Malard; Claude Vidaud; Pascal E Reiller; Richard Ortega; Anthony Nonell; Hélène Isnard; Frédéric Chartier; Carole Bresson
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Journal:  Anal Bioanal Chem       Date:  2018-11-22       Impact factor: 4.142

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Authors:  Xiaojuan Liu; Wenjing Zhang; Zhijuan Wu; Yutao Yang; Y James Kang
Journal:  J Biol Chem       Date:  2018-08-06       Impact factor: 5.157

4.  Method development for on-line species-specific sulfur isotopic analysis by means of capillary electrophoresis/multicollector ICP-mass spectrometry.

Authors:  Sebastian Faßbender; Katerina Rodiouchkina; Frank Vanhaecke; Björn Meermann
Journal:  Anal Bioanal Chem       Date:  2020-07-01       Impact factor: 4.142

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Authors:  Zhuhong Wang; Jiubin Chen; Ting Zhang
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6.  Distinct nitrogen isotopic compositions of healthy and cancerous tissue in mice brain and head&neck micro-biopsies.

Authors:  M Straub; D M Sigman; A Auderset; J Ollivier; B Petit; B Hinnenberg; F Rubach; S Oleynik; M-C Vozenin; A Martínez-García
Journal:  BMC Cancer       Date:  2021-07-13       Impact factor: 4.430

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Authors:  Illa Tea; Arnaud De Luca; Anne-Marie Schiphorst; Mathilde Grand; Sophie Barillé-Nion; Eric Mirallié; Delphine Drui; Michel Krempf; Régis Hankard; Guillaume Tcherkez
Journal:  Metabolites       Date:  2021-06-09

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Authors:  Sara Lauwens; Marta Costas-Rodríguez; Hans Van Vlierberghe; Frank Vanhaecke
Journal:  Sci Rep       Date:  2016-07-29       Impact factor: 4.379

9.  13C and 15N natural isotope abundance reflects breast cancer cell metabolism.

Authors:  Illa Tea; Estelle Martineau; Ingrid Antheaume; Julie Lalande; Caroline Mauve; Francoise Gilard; Sophie Barillé-Nion; Anneke C Blackburn; Guillaume Tcherkez
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10.  CD147 functions as the signaling receptor for extracellular divalent copper in hepatocellular carcinoma cells.

Authors:  Pengfei Ding; Xin Zhang; Shujuan Jin; Bo Duan; Pengxiang Chu; Yufei Zhang; Zhi-Nan Chen; Bin Xia; Fei Song
Journal:  Oncotarget       Date:  2017-05-09
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