关于安卓健的学术论文安卓健对乳腺癌细胞的诱导作用.docx
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关于安卓健的学术论文安卓健对乳腺癌细胞的诱导作用.docx
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关于安卓健的学术论文安卓健对乳腺癌细胞的诱导作用
论文标题:
安卓健对乳腺癌细胞的诱导作用
论文摘要:
乳腺癌是全世界最流行的妇科癌症,同时乳腺癌也是全球第二大(除肺癌)造成妇女死亡的癌症。
本研究,我们通过老鼠实验证实萃取自牛樟芝的环乙烯酮化合物—安卓健对乳腺癌细胞具有明显的抑制其成长,促使其凋亡的作用。
我们将80只雌性大白鼠分为五组,分别为AC低剂量组(喂食0.25g牛樟芝菌丝体每千克体重)、AC高剂量组(喂食0.5g牛樟芝菌丝体每千克体重)、安卓健低剂量组(喂食15mg安卓健每千克体重)、安卓健高剂量组(喂食30mg安安卓健每千克体重)、紫杉醇组(喂食5mg紫杉醇每千克体重)。
实验结果显示,无论是牛樟芝组、安卓健组还是紫杉醇组,小于10mm的乳腺肿瘤均显著地缩小。
但是,大于10mm的乳腺肿瘤只在安卓健组观察到显著缩小。
同时发现,高剂量的牛樟芝组比低剂量的牛樟芝组,乳腺肿瘤的缩小程度更显著,并且在高剂量的牛樟芝组,小于10mm的乳腺肿瘤在17周内没有出现复发现象。
英文版本论文全文如下:
Name:
Antrodiacamphorateextractanditspurifiedcompound-Antroquinonolorally
treatsN-methyl-N-nitrosourea-inducedbreastcancer
Summary:
Antrodiacamphoratepossessesanti-breastcanceractivity
TheGoldenBiotechnologyCorp..camphoratainitiatedbythecompany,manyexpertsinvolvedinthestudythemechanismforthetreatmentofbreastcancer
Relatedresearch.StudieshaveshownthatA.camphoratawithanti-canceractivity.
Li-HsuenChen1,Wei-ChihYang1,Gain-HeFang1,Mao-TienKuo2,Wu-CheWen2,PeiniChen3,Ching-FengWeng1*1
DepartmentofLifeScienceandtheInstituteofBiotechnology,National
Dong–HwaUniversity,Hualien974,Taiwan.
2
GoldenBiotechnologyCorp.,DanshueiTownship,TaipeiCounty251,Taiwan.
3
DepartmentofRadiology,TaipeiVeteransGeneralHospital,Taipei112,
Taiwan.
*Towhomcorrespondenceandreprintrequestsshouldbemade
Runningtitle:
Antrodiacamphoratepossessesanti-breastcanceractivity
____________________________________________________________
*Correspondingauthor.Tel.:
+88638633637;fax:
+88638630255.
E-mailaddress:
cfweng@mail.ndhu.edu.tw(Ching-FengWeng).
Abstract
Breastcanceristhemostprevalentcancerinwomenworldwide,excluding
non-melanomaskincancer,andisthesecondleadingcauseofcancerdeathsin
women(followinglungcancer).Inthisstudy,Antrodiacamphoratemyceliumwith
mediumextract(AC)anditspurifiedcompound-Antroquinonolwereappliedtotreat
insitubreastcancerinanN-methyl-N-nitrosourea(MNU)-inducedratmodelto
evaluatethetherapeuticpotentialofA.camphorate.EightyfemaleSprague-Dawley
rats(21daysold)werefedadlibitumwithstandardratchowandwereinjected
intraperitoneallythreetimeswith25mgMNU/kgBwt.Ratswerepalpatedevery
weektocheckthesizeofthetumorsandthetumordimensionsweremeasuredusinga
caliper.Breastcancerratsweredividedintothreegroups.Fourgroupswereorally
treatedwith
(1)low(0.25g/kgBwt)and
(2)high(0.5g/kgBwt)dosesofAC;(3)low
(15mg/kgBwt)and(4)high(30mg/kgBwt)dosesofAntroquinonolfor5weeks,
whiletheothergroupwasgiven5mgPaclitaxel/kgBwtintraperitoneallyfivetimes.
Theresultsshowedthatratbreasttumorssmallerthan10mmweremarkedly
diminishedinthePaclitaxel-,Antroquinonol-andAC-treatedgroups,however,
tumorslargerthan10mmwerenotreducedamongthePaclitaxelandACgroups.
Examinationsofthetumorssmallerthan10mmshowedthatthehighdoseACgroup
hadmoretumorshrinkagecomparedtothelowdosegroup.Moreover,lessthan10
mmindimensionafterhighdoseACtreatmentexhibitednorecurrencewithin17
weeks.Inconclusion,Antrodiacamphorateanditspurifiedcompound-Antroquinonol
possessesanti-tumoractivityfortreatingtheearlystagesofbreastcancer.
Keywords:
Antrodiacamphorate,Antroquinonol,Paclitaxel,N-methyl-N-nitrosourea,
insitubreastcancer
Introduction
EdiblemushroomsincludingGanodermalucidum(Reishi),Lentinula.edodes
(shiitake),Antrodiacamphorate(niu-chang-chih,Chang-chih)havebeenwidelyused
asamedicinalfungus.G.lucidumhasalsobeenusedtosuppresscelladhesionand
cellmigrationofhighlyinvasivebreastandprostatecancercells,suggestingits
potencytoreducetumorinvasiveness(reviewedinThyagarajanetal.,2007).
Recently,onereportdemonstratedthatcombinationsofgreenteawithG.lucidum
extractsshowpotentialforthesuppressionofgrowthandinvasivenessofmetastatic
breastcancer(MDA-MB-231)cells(Thyagarajanetal.,2007).Moreover,structurally
relatedlanostane-typetriterpenes,includingganodericacidA,FandH(GA-A,GA-F,
GA-H),havebeenidentifiedinanorientalmedicinalmushroomG.lucidum.GA-A
andGA-Hexerttheirbiologicaleffectsthroughinhibitionofthetranscriptionfactors
AP-1andNF-ĸB,resultinginthedown-regulationofexpressionofCdk4and
suppressionofsecretionofuPA,respectively(Jiangetal.,2008).Lentinulaedodes
(shiitake)aqueousextractshavedemonstrateddirectinhibitionoftheproliferationof
humanbreastcancercellsinvitroandimmuno-stimulatorypropertiesintermsof
mitogenicandco-mitogenicactivityinvitro(Israilidesetal.,2008).
A.camphorata,oneoftheextensivelyusedmedicinalmushrooms,iswellknown
inTaiwanasatraditionalChinesemedicineandhasrecentlybeenidentifiedas
belongingtothenewgenusoftheAntrodiaspecies(Taiwanofungus).Itsfruitingbody
hasbeenutilizedintraditionalChinesemedicineforthetreatmentoffoodanddrug
intoxication,diarrhea,abdominalpain,hypertension,skinitches,livercancer,
anti-inflammatory,anti-oxidation,inducedvasorelaxation,decreasedhepatitisBvirus,
andhypotriglyceride(reviewedinSuketal.,2008).However,theA.camphorata
fruitingbodiesareveryrareandexpensive,andlittlehasbeenreportedaboutits
biologicalactivity,especiallyintreatingthebreastcancer.Breastcanceristhemost
prevalentcancerinwomenworldwide,excludingnon-melanomaskincancer,andis
thesecondleadingcauseofcancerdeathinwomen(followinglungcancer).Breast
cancerremainsaglobalpublichealthproblemwithsome1.1millionwomennewly
diagnosedwithbreastcancerin2002(Ferlayetal.,2002),withapproximately
185,000newcasesandover40,000deathsestimatedintheUSAin
2008(Jemaletal.,2008).Therefore,developingasuitableanimalmodelfortesting
theanti-breastcancerpotencyofA.camphoratabecomesahighpriority.
N-methyl-N-nitrosourea(MNU)isanalkylatingagentthatmethylatesDNAbasesat
nucleophilicsites(generatingN7andN3alkylpurines).Theprimarymutageniclesion
isO6methylguanine.MNU-inducedmammarytumorigenesisinratsisoneofthe
mostbroadlyusedrodentmammarytumorigenesismodelsforstudyinghumanbreast
cancer(Russoetal.,1990;Gould,1995;Nandietal.,1995).MNU-inducedrat
mammarytumorigenesisandhumanbreastcancerdevelopmentsharemany
similaritiesinhormonedependency,pathogenesis,histologicalclassification,and
immunocytochemicalmarkers.Basedonthesesimilarities,MNU-inducedrat
mammarytumorigenesisappearstobeausefulexperimentalmodelforthestudyof
humanbreastcancerdevelopment(Thordarsonetal.,2001).Antroquinonol
(1),an
ubiquinonederivative,isisolatedfromthesolid-statefermentedmyceliumofA.
camphorate,aparasiticfungusindigenoustoTaiwan.Thestructureofcompound1is
elucidatedbytheanalysisoftheirspectroscopicdata.Itcontainsanti-tumoractivity
(Leeetal.,2007).Recently,A.camphorateextracthasbeenprovenforthetreatment
ofsystemiclupuserythematosus(SLE)inSLE-proneNZB/WF1mice(Changetal.,
2008).Theaimofthisstudywastoproducebreastcancerinratstoevaluatethe
anti-tumoractivityofA.camphorateextractanditspurifiedcompound-
Antroquinonolfortreatinginsitubreastcancer.
Materialsandmethods
Chemicals
N-methyl-N-nitrosourea(MNU,N4766)andPaclitaxel(Taxol
TM
T7191)were
purchasedfromSigma-aldrich(St.Louis,CA,USA).ThepureAntroquinonol
compoundandA.camphorataextract(ACE)wereobtainedfromGolden
BiotechnologyCompany,Taiwan.
PreparationofA.camphorataextract
TheA.camphorata(strainno.486bp)usedinthisstudywasauthenticatedbyDr
TzeanShang-Shong,DepartmentofPlantPathologyandMicrobiology,National
TaiwanUniversity,Taiwan.ThemyceliaofA.camphoratawereculturedin1000mL
ofgrowthmediumcontaining0.1gNaCl,10gpeptone,2gyeastextract,10gagar
and10gcerealmixture(rice,wheatorcorn),pH7.5at25
o
Cfor12–14weeks.After
cultivation,500goflyophilizedA.camphoratamyceliumwasextractedwith2500
mLofn-hexanefor6h.Then-hexanefraction,definedasA.camphorateextract
(GD-66,productnameandGD-AIDT7,batchname),wasconcentratedto20–30mL
viavacuumevaporation.A.camphorateextracthasbeenapprovedasahealthfoodby
TaiwanFDA(HealthyFoodNo.A00124).ThepurifiedprocedureofAntroquinonol
wasdescribedinourpreviousstudy(Leeetal.,2007).Briefly,Antroquinonolwas
purifiedfromA.camphorateextractbysilicagelchromatography(column=45cm,5
cmi.d.)(ASTMsilicagel,MerckCo.,Germany)andelutedwithn-hexane:
ethyl
acetate(10:
3v/v).Theresultingeluatewasfurthersubjectedtosizeexclusion
chromatographyusingSephadexLH20column(70cmlong,5cmi.d.)(ABgel,GE
HealthcareBio-Science,USA).Theantroquinonol(98%purity)waselutedwith95%
ethanol;theA.camphorateextractfractionwasdeterminedtohave0.01%
antroquinonol.
Animalsandtreatments
Twenty-one-day-oldfemaleSprague-Dawleyratswereobtainedfromthe
BioLASCOTaiwanCo.,Ltd(Taipei,Taiwan)andwerekeptina
temperature-controlledenvironment(23
o
C)with70%relativehumidityundera12-h
light/darkcycle.Theanimalexperimentswereperformedaccordingtothe‘‘Guidefor
theCareandUseofLaboratoryAnimals’’ofNationalDong-HwaUniversity.Rats
werefedstandardratchow(LabDietTM-500lRodentDiet;TestDiet,Richmond,IN,
USA).Afteroneweekadaptation,allratsre
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