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      [Ru(phen) 2podppz] 2+ significantly inhibits glioblastoma growth in vitro and vivo with fewer side-effects than cisplatin

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          Abstract

          Ru1 could most effectively inhibit tumor growth and avoid any detectable side-effects compared with other ruthenium( ii) complexes and cisplatin, demonstrating its potential to be an exciting new drug candidate for glioblastoma treatment.

          Abstract

          To overcome the acquired resistance and the significant side-effects of the reported drugs, four new ruthenium( ii) complexes with alkynyl ( Ru1, Ru2, Ru3, Ru4) were designed and synthesized. Ru1, Ru2, Ru3 and Ru4 were characterized by ESI-MS, 1H NMR, 1H– 1H COSY NMR and elemental analysis. Compared with Ru2, Ru3, Ru4 and cisplatin, the anti-tumor experiments in vitro and vivo confirmed that Ru1 could most effectively inhibit tumor growth. In the experiments of safety evaluation in vivo, Ru1 could avoid any detectable side-effects compared with cisplatin. DNA binding experiments and cell cycle experiments showed that Ru1 exhibited the strongest DNA binding ability and interfered with the cell cycle by inserting DNA to inhibit tumor growth. The study demonstrated that Ru1 had the potential to be an exciting new drug candidate for glioblastoma treatment.

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          Author and article information

          Contributors
          Journal
          ICHBD9
          Dalton Transactions
          Dalton Trans.
          Royal Society of Chemistry (RSC)
          1477-9226
          1477-9234
          July 7 2020
          2020
          : 49
          : 26
          : 8864-8871
          Affiliations
          [1 ]Shanghai East Hospital
          [2 ]Shanghai Key Lab of Chemical Assessment and Sustainability
          [3 ]School of Chemical Science and Engineering
          [4 ]Tongji University
          [5 ]200092 Shanghai
          [6 ]Department of Pharmacy
          [7 ]Shanghai 200120
          [8 ]PR China
          Article
          10.1039/D0DT01877E
          ff0ab07d-f121-4040-a9ae-ef481fee88eb
          © 2020

          http://rsc.li/journals-terms-of-use

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