Literature DB >> 29121854

Monitoring Interactions Inside Cells by Advanced Spectroscopies: Overview of Copper Transporters and Cisplatin.

Alessia Lasorsa1, Giovanni Natile2, Antonio Rosato2, Francesco Tadini-Buoninsegni3, Fabio Arnesano2.   

Abstract

BACKGROUND: Resistance, either at the onset of the treatment or developed after an initial positive response, is a major limitation of antitumor therapy. In the case of platinum- based drugs, copper transporters have been found to interfere with drug trafficking by facilitating the import or favoring the platinum export and inactivation.
METHODS: The use of powerful spectroscopic, spectrometric and computational methods has allowed a deep structural insight into the mode of interaction of platinum drugs with the metal-binding domains of the transporter proteins.
RESULTS: This review article focuses on the mode in which platinum drugs can compete with copper ion for binding to transport proteins and consequent structural and biological effects. Three types of transporters are discussed in detail: copper transporter 1 (Ctr1), the major responsible for Cu+ uptake; antioxidant-1 copper chaperone (Atox1), responsible for copper transfer within the cytoplasm; and copper ATPases (ATP7A/B), responsible for copper export into specific subcellular compartments and outside the cell.
CONCLUSION: The body of knowledge summarized in this review can help in shaping current chemotherapy to optimize the efficacy of platinum drugs (particularly in relation to resistance) and to mitigate adverse effects on copper metabolism. Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.

Entities:  

Keywords:  NMR spectroscopy; Platinum anticancer drugs; copper ATPases; copper chaperones; drug resistance; mass spectrometry.

Mesh:

Substances:

Year:  2018        PMID: 29121854     DOI: 10.2174/0929867324666171110141311

Source DB:  PubMed          Journal:  Curr Med Chem        ISSN: 0929-8673            Impact factor:   4.530


  8 in total

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Authors:  Renan Vieira de Brito; Marília Wellichan Mancini; Marcel das Neves Palumbo; Luis Henrique Oliveira de Moraes; Gerson Jhonatan Rodrigues; Onivaldo Cervantes; Joel Avram Sercarz; Marcos Bandiera Paiva
Journal:  Int J Mol Sci       Date:  2022-05-25       Impact factor: 6.208

3.  Relevance of Copper and Organic Cation Transporters in the Activity and Transport Mechanisms of an Anticancer Cyclometallated Gold(III) Compound in Comparison to Cisplatin.

Authors:  Sarah Spreckelmeyer; Margot van der Zee; Benoît Bertrand; Ewen Bodio; Stefan Stürup; Angela Casini
Journal:  Front Chem       Date:  2018-09-04       Impact factor: 5.221

4.  CRISP-R/Cas9 Mediated Deletion of Copper Transport Genes CTR1 and DMT1 in NSCLC Cell Line H1299. Biological and Pharmacological Consequences.

Authors:  Ekaterina Y Ilyechova; Elisa Bonaldi; Iurii A Orlov; Ekaterina A Skomorokhova; Ludmila V Puchkova; Massimo Broggini
Journal:  Cells       Date:  2019-04-06       Impact factor: 6.600

5.  Cisplatin and beyond: molecular mechanisms of action and drug resistance development in cancer chemotherapy.

Authors:  Tomaz Makovec
Journal:  Radiol Oncol       Date:  2019-03-28       Impact factor: 2.991

Review 6.  Cellular Dynamics of Transition Metal Exchange on Proteins: A Challenge but a Bonanza for Coordination Chemistry.

Authors:  Jean-Marc Moulis
Journal:  Biomolecules       Date:  2020-11-21

7.  Interaction of Copper Trafficking Proteins with the Platinum Anticancer Drug Kiteplatin.

Authors:  Alessandra Barbanente; Angela Galliani; Rosa Maria Iacobazzi; Alessia Lasorsa; Maria Incoronata Nardella; Antonio Pennetta; Nicola Margiotta; Fabio Arnesano
Journal:  ChemMedChem       Date:  2021-11-15       Impact factor: 3.540

8.  PTBP1 modulates osteosarcoma chemoresistance to cisplatin by regulating the expression of the copper transporter SLC31A1.

Authors:  Cheng Cheng; Qiuyue Ding; Zhicai Zhang; Shangyu Wang; Binlong Zhong; Xin Huang; Zengwu Shao
Journal:  J Cell Mol Med       Date:  2020-03-24       Impact factor: 5.310

  8 in total

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