In Vitro Evaluation of Oxoplatin: An Oral Platinum(IV) Anticancer Agent

Olszewski, Ulrike; Ach, Florian; Ulsperger, Ernst; Baumgartner, Gerhard; Zeillinger, Robert; Bednarski, Patrick J.; Hamilton, Gerhard

doi:10.1155/2009/348916

Cited by 30 publications

(46 citation statements)

References 34 publications

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“…Cell cycle arrest induced by titanocene C is clearly distinct from that of platinum-based drugs, which points to different mechanisms of action [17]. Our present findings identify expression of helicases such as topoisomerase I, IIα and MCM4 as main targets of titanocene C leading to cell cycle arrest and downregulation of HIST1H4 core histones.…”

Section: Discussionmentioning

confidence: 55%

“…Thus, in the present study, NCI-H526 cells were treated with titanocene C, and alterations in gene expression were analyzed using a human gene survey microarray system. Although these data need to be confirmed by PCR and/or immunochemistry, they provide an insight into the cellular pathways affected by the test compound [17]. Treatment of NCI-H526 cells resulted in significant changes in gene expression, affecting a host of transcripts involved in different cellular pathways.…”

Section: Discussionmentioning

confidence: 92%

“…Therefore, alternative drugs distinct from cisplatin in respect to their modes of action and resistance are urgently needed, especially for SCLC patients. Titanocene C induced accumulation of cells in G1/0 for HL-60 and NCI-H526 cells and in S phase for a SCLC line, clearly distinct from the G2M arrest characteristic of platinum compounds [17,18]. Cross-resistance of titanocene C to the platinum compounds cisplatin and oxoplatin was investigated using highly resistant HL-60 variant cell lines, namely HL-60cis and HL-60oxo, in chemosensitivity assays [19].…”

Section: Discussionmentioning

confidence: 99%

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Anticancer activity and mode of action of titanocene C

et al. 2010

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Titanocenes constitute a class of metal-based anticancer agents that seem to display a mode of action distinct from that of platinum complexes and to be more tolerable with a differing spectrum of activity. In the present study, titanocene C (bis-(N,N-dimethylamino-2(N-methylpyrrolyl)-methyl-cyclopentadienyl) titanium(IV) dichloride) was shown to exhibit antiproliferative activity against human tumor cell lines with a mean IC₅₀ value of 48.3 ± 32.5 µM. In particular, high activity was found against small cell lung cancer (SCLC) cell lines with a profile different from cisplatin. Titanocene C induced cell cycle arrest at the G1/0-S interphase. Cross-resistance to either cisplatin or oxoplatin, respectively, was low for titanocene C and absent for titanocene Y in variant HL-60 cell lines. Alterations in gene expression of NCI-H526 SCLC cells induced by titanocene C were investigated using genome-wide expression arrays. Downregulation was found for genes coding for topoisomerases I and IIα, histones of the HIST1H4 cluster, enzymes involved in glycolysis, components of the cytoskeleton and vesicular transport, among others. In contrast, expression of genes involved in apoptosis, stress response, particularly members of the metallothionein gene cluster 1, DNA damage and growth factors was upregulated following exposure to titanocene C. Approximately 50% of those genes downregulated by titanocene C and cisplatin were concordant, including the previously identified markers of cisplatin-sensitivity, tubulin and stathmin, indicating partial overlap of the pathways affected by these metal complexes. The present findings point helicases/topoisomerases and HIST1H4 core histones out as targets of titanocene C and metallothioneins as putative main effectors of drug resistance.

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Section: Discussionmentioning

confidence: 55%

Section: Discussionmentioning

confidence: 92%

Section: Discussionmentioning

confidence: 99%

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Anticancer activity and mode of action of titanocene C

et al. 2010

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“…However, despite enormous promise and anticancer activity reported to date, none of the HSP90 inhibitors in development has been approved for cancer therapy [12]. Since platinum-based combinations are frequently used for the treatment of metastatic gastric cancer we tested cisplatin and a platinum (IV) derivative, namely oxoplatin, in combination with ganetespib for cytotoxic activity against the gastric cancer cell lines and normal IEC6 cells [9]. Combinational treatment of ganetespib with platinum substances, cis-/oxoplatin, resulted in a marked synergistic cytotoxic effect, except for the normal intestinal epithelial cell lines IEC6.…”

Section: Mkn1mentioning

confidence: 99%

2208 In vitro cytotoxic activities of the oral platinum(IV) prodrug oxoplatin and HSP90 inhibitor ganetespib against a panel of gastric cancer cell lines

Klameth¹,

Rath²,

Kriwanek³

et al. 2015

European Journal of Cancer

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“…d,l-1,2-Diamino-cyclohexane-tetrachloro-Pt(IV) has been reported that the reduction mechanism is as follows: the Pt(IV) complex binds to guanine base in DNA and subsequently induces direct-electron transfer between Pt(IV) and guanine base, in which oxidized guanine was observed [19][20][21]. In addition, several researchers have reported that the reduction of Pt(IV) compounds can be accomplished by intracellular reductants such as ascorbic acid (AsA) or thiol-containing species like glutathione (GSH), cysteine and metallothioneins [2,[22][23][24][25]. However, the mechanisms of Pt(IV) reduction and reactivity with DNA in the presence of reductants have not yet been elucidated.…”

Section: Introductionmentioning

confidence: 99%