5-aza-2',2'-Difluoro Deoxycytidine (NUC013): A Novel Nucleoside DNA Methyl Transferase Inhibitor and Ribonucleotide Reductase Inhibitor for the Treatment of Cancer.

Richard Daifuku,Zhenbo Hu,Yogen Saunthararajah

doi:10.3390/ph10030065

Abstract

Tumor suppressor genes can be silenced genetically as well as epigenetically. One approach to reversing epigenetic suppression of tumor suppressor genes is to inhibit DNA methyl transferase. 5-aza-2′,2′-diflurorodeoxycytidine (NUC013) is a novel DNA methyl transferase and ribonucleotide reductase inhibitor that is a more potent inhibitor of growth than decitabine in the NCI 60 cancer cell line panel. NUC013 is more active than decitabine against p53-null/mutant cancer cell lines (p = 0.027) but is even more so against p53 wild-type (WT) cell lines (p = 0.0025). The maximum tolerated dose in mice of NUC013 is greater than 120 mg/kg administered intravenously for three consecutive days a week for three weeks. With this regimen and a dose of 20 mg/kg in a human leukemia HL-60 (p53-null) NCr-nu/nu mouse xenograft model (n = 10/group), NUC013 demonstrated a survival benefit (saline median survival (MS) = 26.5 days, NUC013 MS = 32 days and hazard ratio (HR) = 0.26 (p = 0.032)). In a colon cancer LoVo (TP53 WT) xenograft, mice treated with decitabine at 5 mg/kg had worse survival than saline controls (decitabine MS = 31 days, saline MS > 60 days and HR = 26.89 (p < 0.0001)). At a dose of 20 mg/kg NUC013, mean tumor volume in the LoVo xenografts was lower than controls by 50.9% and at 40 mg/kg by 53.7% (both p < 0.0001).

Highlights

An aberrant gain of DNA methylation at the promoter CpG islands and enhancer regions of critical tumor suppressors is observed in most cancers and leads to the inactivation of the expression of genes that suppress tumorigenesis [1]
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Summary

Introduction

An aberrant gain of DNA methylation at the promoter CpG islands and enhancer regions of critical tumor suppressors is observed in most cancers and leads to the inactivation of the expression of genes that suppress tumorigenesis [1]. 5-aza-2 ,2 -difluoro deoxycytidine (NUC013) is a novel nucleoside analog designed to be a DNA methyl transferase inhibitor (DNMTI) and ribonucleotide reductase inhibitor (RNRI). NUC013 consists of the base of 5-azacytidine (Vidaza®, Celgene, Summit, NJ, USA) or 5-aza-2 -deoxycytidine, known as decitabine, (Dacogen®, Otsuka America Pharmaceutical, Rockville, MD, USA) conjugated with the sugar moiety of gemcitabine (Gemzar®, Eli Lilly, Indianapolis, IN, USA) (see Figure 1). Pharmaceuticals 2017, 10, 65 Pharmaceuticals 2017, 10, 65 2 of 14 2 of 14 Decitabine Gemcitabine NUC013. Both 5-azacytidine and decitabine are approved in the United States for the treatment of myBelootdhys5p-laazsaticcystiydnidnreomaned(MdDecSi)t.aMbionree arreeceanptlpy,rodveecditaibnintehheaUs bneiteendaSptpartoevsedforinththee tEreuarotmpeeannt of mUyenlioodnyfsopr ltahsetitcresaytnmdernotmofe a(cMutDeSm).yMelooirde lreeuckeenmtliya, [d3e].cTithaebsienenuhcalesobseideens awpeprreofviresdt siynntthheesEizuerdoipnean U1n9io64n [f4o,r5]t.hTehterelaactkmoefnatpopfraocvuetde nmoyveellomidolleecuukleesminiat[h3e].inTthereisme natutecsletsotsoidtehse wdieffriecufilrtsytisnydnethsiegsniiznegd in 19s6a4fe[4a,n5d]. Both 5-azacytidine and decitabine are approved in the United States for the treatment of myBelootdhys5p-laazsaticcystiydnidnreomaned(MdDecSi)t.aMbionree arreeceanptlpy,rodveecditaibnintehheaUs bneiteendaSptpartoevsedforinththee tEreuarotmpeeannt of mUyenlioodnyfsopr ltahsetitcresaytnmdernotmofe a(cMutDeSm).yMelooirde lreeuckeenmtliya, [d3e].cTithaebsienenuhcalesobseideens awpeprreofviresdt siynntthheesEizuerdoipnean U1n9io64n [f4o,r5]t.hTehterelaactkmoefnatpopfraocvuetde nmoyveellomidolleecuukleesminiat[h3e].inTthereisme natutecsletsotsoidtehse wdieffriecufilrtsytisnydnethsiegsniiznegd in 19s6a4fe[4a,n5d]. eTffheectliavcekmooflaecpuplreosvoefdthnisocvlealssm. olecules in the interim attests to the difficulty in designing safe anTdoebffeecatcitvievemaosleacuDleNsMofTtIh, i5s-aczlaascsy.tidine must first be reduced in vivo to the deoxy-analog, decTitoabbineea. cDteivcietaabsinae mDNusMt tThIe,n5b-eazpahcoystpidhionreylamteudsttofidrsetcibtaebirneedturcipehdosinphvaivteoantod tihnecodrpeoorxayte-adnianlog, deDcNitaAbinbee.foDrecitinabhibnietimngusDt tNhAen bmeepthhyolsaptihoonry[l6a]t.edBotothdedcrituagbsineprtoridpuhcoesprhematiessainodnsinocor rpcolirnaicteadl in DNimAprboevfeomreeinnthsibinitimngorDeNthAanmhetahlfyloaftitohne [t6r]e.aBteodthpdartuiegnstsprwoidthucMe DreSm. iOsspiotinmsiozartciolinniocafltihmerparpoyvehmasents ininmcoluredethdan(1h) alrfedofutchinegtrethateeddpoasetietnots fwavitohr MhDypSo. mOpetthimyliaztaiotinonoovfetrhecryatpotyohxiacsitiyn;cl(u2d) epdr(o1l)onregdinugcing thaeddmoisneisttoraftaivoonr hscyhpeodmuleetshyalantdion(3o)veirncyretaostionxgicitdyo;s(e2) ipnrtoelnosnitgyingwaitdhmouitnisrteraacthioingschcyedtoutolexsicaitnyd. (3) inCcroenassiidnegridnogsethianttebnostihtyhwavitehothuet rceoamchmionng csyidtoetoefxfieccittyo. fCmonyseildoesuripnpgrethssaitobnotthhaht alvimeitthsedcoosminmg oanndside effdeucrtaotifomnyoefltorseuatpmperenst,siiot nis tchleaatrlitmhaittsbdetotseirnignhainbditodrusroaftiDoNn Aofmtreetahtymlaetniot,nitairsecnleeeadr ethdaftobr ectltinericianlhuisbei,tors ofpDarNtiAcumlareltyhyolnaetsiotnhaatrehanveeedleesds fcoyrtoctloinxiiccaitlyuasned, pmarotriecualcatrivlyitoynaegsatihnsatt shoalvide tluesmsocrysto[7to,8x].icDitaytaanfrdommore actthiveittywaogaciunrsrtensotllyidatpupmroovresd[7d,8r]u. gDsatsaugfrgoemst tthheattwmoyceulorirdenmtlyalaigpnparnocvieesd adrreugthsesungegoepsltasthmast mmyoestloid msaelnigsnitaivneciteos ianrheitbhiteonrseoopf lDasNmAs mmeotshtysleantisoitni;vheotwo ienvheirb, itthoerrseoifsDnNo Aknmowetnhyrelaatsioonn;whhoywseovleidr, tthuemreoriss no knsohwounldrenaostorneswphonydsoalsidwteullm[9o,1rs0]s.hould not respond as well [9,10].

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