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Journal of Cancer Research and Clinical Oncology

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24.04.2020 | Original Article – Cancer Research

Selected ellipticine derivatives, known to target topoisomerase II, suppress the alternative lengthening of telomere (ALT) pathway in telomerase–negative cells

verfasst von: Sevil Zencir, Meng-Hsun Hsieh, Joel-Sean Hsu, Yavuz Ergun, Guan-Ling Chou, Tsai-Kun Li, Shu-Chun Teng, Zeki Topcu

Erschienen in: Journal of Cancer Research and Clinical Oncology | Ausgabe 7/2020

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Abstract

Background

DNA topoisomerase and telomerase enzymes are popular targets of several anti-tumor drugs. Smooth proceeding of telomeric recombination requires Topoisomerase II (Top2), which is involved in telomere-telomere recombination through functioning in relaxation of positive supercoils among the cells adopting telomerase-independent Alternative lengthening of telomere (ALT) pathway. Most of the inhibitors reported so far have been designed to targetsolely telomerase-positive cells, which can potentially lead to therapeutic failure because tumor cells treated with telomerase inhibitors can activate the ALT pathway for telomere maintenance. Knowing that ALT cells are more sensitive against a Top2 inhibitor, ICRF-93 agent, compared to telomerase-positive cells, we analyzed two selected ellipticine derivatives that we recently reported as TopII-targeting compounds, to assess their effects on the formation of DNA breaks and suppression of ALT pathway.

Methods

Cell viability, Comet, C-Circle assays, dot blot, immunofluorescence staining, and telomere fluorescence in situ hybridization (FISH) staining were used for determining the effect of the compounds on ALT status of tumor cells.

Results and conclusions

Treatment of ALT cells with ellipticine derivatives resulted in the formation of DNA breaks and suppression of ALT-associated phenotypes in vitro. Our results will contribute to the development of therapeutic strategies combining telomerase and ALT pathway inhibitors.

Basenko E, Topcu Z, McEachern MJ (2011) Recombination can either help maintain very short telomeres or generate longer telomeres via a roll-and-spread mechanism in yeast cells with weak telomerase activity. Eukaryot Cell 10:1131–1142CrossRef

Blackburn EH (1992) Telomerases. Annu Rev Biochem 61:113–129CrossRef

Blackburn EH, Epel ES, Lin J (2015) Human telomere biology: a contributory and interactive factor in aging, disease risks, and protection. Science 350:1193–1198CrossRef

Blackburn EH, Greider CW, Szostak JW (2006) Telomeres and telomerase: the path from maize, Tetrahymena and yeast to human cancer and aging. Nat Med 12:1133–1138CrossRef

Bryan TM, Englezou A, Dalla-Pozza L, Dunham MA, Reddel RR (1997) Evidence for an alternative mechanism for maintaining telomere length in human tumors and tumor-derived cell lines. Nat Med 3:1271–1274CrossRef

Cesare AJ, Reddel RR (2010) Alternative lengthening of telomeres: models, mechanisms and implications. Nat Rev Genet 11:319–330CrossRef

Dar AM, Uzzaman S, Ahmad MS (2017) Steroidal imidazoles: synthesis, characterization, molecular docking studies with DNA and in vitro cytotoxicity. Med Chem Res 26:2372–2383CrossRef

Dunham MA, Neumann AA, Fasching CL, Reddel RR (2000) Telomere maintenance by recombination in human cells. Nat Genet 26:447–450CrossRef

Ghosh S, Kar A, Chowdhury S, Dasgupta D (2013) Ellipticine binds to a human telomere sequence: an additional mode of action as a putative anticancer agent? Biochemistry 52:4127–4137CrossRef

Henson JD, Reddel RR (2010) Assaying and investigating alternative lengthening of telomeres activity in human cells and cancers. FEBS Lett 584:3800–3811CrossRef

Henson JD, Cao Y, Huschtscha LI, Chang AC, Au AY, Pickett HA, Reddel RR (2009) DNA C-circles are specific and quantifiable markers of alternative-lengthening-of-telomeres activity. Nat Biotechnol 27:1181–1185CrossRef

Henson JD, Lau LM, Koch S, Martin La Rotta N, Dagg RA, Reddel RR (2017) The C-circle assay for alternative-lenghtening-of-telomeres activity. Methods 114:74–84CrossRef

Hsieh MH, Tsai CH, Lin CC, Li TK, Hung TW, Chang LT, Hsin LW, Teng SC (2015) Topoisomerase II inhibition suppresses the proliferation of telomerase-negative cancers. Cell Mol Life Sci 72:1825–1837CrossRef

Huang TH, Chen HC, Chou SM, Yang YC, Fan JR, Li TK (2010) Cellular processing determinants for the activation of damage signals in response to topoisomerase I-linked DNA breakage. Cell Res 20:1060–1075CrossRef

Isloor AM, Sunil D, Prakash Shetty P, Malladi S, Pai KSR, Maliyakkl N (2013) Synthesis, characterization, anticancer, and antioxidant activity of some new thiazolidin-4-ones in MCF-7 cells. Med Chem Res 22:758–767CrossRef

Itoh T, Hatae N, Nishiyama T, Choshi T, Hibino S, Yoshimura T, Ishikura M (2018) Synthesis and cytotoxicity of pyrido[4,3-b]carbazole alkaloids against HCT-116 and HL-60 cells. Med Chem Res 27:412–419CrossRef

Kuskucu AV, Kulmány Á, Ergün Y, Zencir S, Zupko I, Durdagi S, Kader S, Zaka M, Orhan H, Topcu Z (2020) Structural modification of ellipticine derivatives with alkyl groups of varying length is influential on their effects on human DNA topoisomerase II: a combined experimental and computational study. Med Chem Res 29:189–198CrossRef

Lee CH, Hsieh MY, Hsin LW, Chen HC, Lo SC, Fan JR, Chen WR, Chen HW, Chan NL, Li TK (2012) Anthracenedione-methionine conjugates are novel topoisomerase II-targeting anticancer agents with favorable drug resistance profiles. Biochem Pharmacol 83:1208–1216CrossRef

Lin CC, Hsieh MH, Teng SC (2016) Genistein suppresses the proliferation of telomerase-negative cells. Food Sci Nutr 5:197–204CrossRef

Lu Y, Leong W, Guerin O, Gilson E, Ye J (2013) Telomeric impact of conventional chemotherapy. Front Med 7:41–417

Martines P, Blasco MA (2015) Replicating through telomeres: a means to an end. Trends Biochem Sci 40:504–515CrossRef

McClendon AK, Osheroff N (2007) DNA topoisomerase II, genotoxicity, and cancer. Mut Res 623:83–97CrossRef

Miller CM, McCarthy FO (2012) Isolation, biological activity and synthesis of the natural product ellipticine and related pyridocarbazoles. RSC Adv 2:8883–8918CrossRef

Reddel RR, Bryan TM, Colgin LM, Perrem KT, Yeager TR (2001) Alternative lengthening of telomeres in human cells. Radiat Res 155:194–200CrossRef

Sarikaya BB, Zencir S, Somer NU, Kaya GI, Onur MA, Bastida J, Zupko I, Topcu Z (2012) The effects of arolycoricidine and narciprimine on tumor cell killing and topoisomerase activity. Rec Nat Prod 6:381–385

Sassano MF, Schlesinger AP, Jarstfer MB (2012) Identification of G quadruplex inducers using a simple, inexpensive and rapid high throughput assay, and their inhibition of human telomerase. Open Med Chem J 6:20–28CrossRef

Shay JW, Reddel RR, Wright WE (2012) Cancer and telomeres–an ALTernative to telomerase. Science 336:1388–1390CrossRef

Stiborova M, Frei E (2014) Ellipticines as DNA-targeted chemotherapeutics. Curr Med Chem 21:575–591CrossRef

Teng SC, Chang J, McCowan B, Zakian VA (2000) Telomerase independent lengthening of yeast telomeres occurs by an abrupt Rad50p-dependent, Rif-inhibited recombinational process. Mol Cell 6:947–952CrossRef

Topcu Z, Nickles K, Davis C, McEachern M (2005) Abrupt disruption of capping and a single source for recombinationally elongated telomeres in K. Lactis Proc Natl Acad Sci 102:3348–3353CrossRef

Vann KR, Ergun Y, Zencir S, Oncuoglu S, Osheroff N, Topcu Z (2016) Inhibition of human DNA topoisomerase IIα by two novel ellipticine derivatives. Bioorganic Med Chem Lett 26:1809–1812CrossRef

Wang JC (1996) DNA topoisomerases. Annu Rev Biochem 65:635–692CrossRef

Yasuhara S, Zhu Y, Matsui T, Tipirneni N, Yasuhara Y, Kaneki M, Rosenzweig A, Martyn JAJ (2003) Comparison of comet assay, electron microscopy, and flow cytometry for detection of apoptosis. J Histochem Cytochem 51:873–885CrossRef

Yeager TR, Neumann AA, Englezou A, Huschtscha LI, Noble JR, Reddel RR (1999) Telomerase-negative immortalized human cells contain a novel type of promyelocytic leukemia (PML) body. Cancer Res 59:4175–4179PubMed

Yu Y, Zhu W, Diao H, Zhou C, Chen FF, Yang J (2006) A comparative study of using comet assay and γH2AX foci formation in the detection of N-methyl-N′-nitro-N-nitrosoguanidine-induced DNA damage. Toxicol In Vitro 20:959–965CrossRef

Titel: Selected ellipticine derivatives, known to target topoisomerase II, suppress the alternative lengthening of telomere (ALT) pathway in telomerase–negative cells
verfasst von: Sevil Zencir
Meng-Hsun Hsieh
Joel-Sean Hsu
Yavuz Ergun
Guan-Ling Chou
Tsai-Kun Li
Shu-Chun Teng
Zeki Topcu
Publikationsdatum: 24.04.2020
Verlag: Springer Berlin Heidelberg
Erschienen in: Journal of Cancer Research and Clinical Oncology / Ausgabe 7/2020
Print ISSN: 0171-5216
Elektronische ISSN: 1432-1335
DOI: https://doi.org/10.1007/s00432-020-03213-x

Springer Medizin

Selected ellipticine derivatives, known to target topoisomerase II, suppress the alternative lengthening of telomere (ALT) pathway in telomerase–negative cells