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Colorectalcancer12ColorectalcanceroccursinthecolonandtherectumRiskfactors
3Riskfactorsforcolorectalcancerincludelifestyle,olderage,andinheritedgeneticdisorders.Otherriskfactorsincludediet,smoking,alcohol,lackofphysicalactivity,familyhistoryofcoloncancerandcolonpolyps,presenceofcolonpolyps,race,exposuretoradiation,andevenotherdiabetes,obesity.4Physicalactivity5meat6Smokingalcohol7diabetes,obesity
AccordingtoWHO,Morethan30%Americanaretroublingwithobesityproblem.It’ssimilarinotherdevelopedcountrieswithhighrateofcolorectalcancer.8Otherriskfactors
suchasinflammatoryboweldisease,whichincludesCrohn'sdiseaseandulcerativecolitis,canincreasetheriskofcolorectalcancer.Someoftheinheritedconditionsthatcancausecolorectalcancerinclude:familialadenomatouspolyposisandhereditarynon-polyposiscoloncancer;however,theserepresentlessthan5%ofcases.Ittypicallystartsasabenigntumor,oftenintheformofapolyp,whichovertimebecomescancerous.Epidemiology910Age-standardizeddeathfromcolorectalcancerper100,000inhabitantsin2004.Globally,
Highest
incidenceratesintheAustralia,NewZealand,EuropeandtheUSandlowestratesinAfricaandSouth-CentralAsia.11Signsandsymptoms12abdominalpain,diarrhea….Thesymptomsandsignsofcolorectalcancerdependonthelocationofthetumorinthebowel,
andwhetherithasspreadelsewhereinthebody(metastasis).Signsandsymptoms1314RectumCheckingBecauseofhavingthesamesymptomwithbloodinthestoolandhavingnotclearlyrectumchecking,Inclinic,lotsofrectumcancerpatientsusuallymisdiagnosedashemorrhoids(痔瘡)
andundergonesomeincorrecttreatments.15ThebodypostureforrectumcheckingLateralpostureKnee-chestpostureLithotomypostureCrouchpostureBendposture16AbdominaldistensionTumorwithbigmass,seriousascites,intestineobstruction…..17IntestinalObstruction1819CauseLocationandappearanceoftwoexamplecolorectaltumorsMorethan75-95%ofcoloncanceroccursinpeoplewithlittleornogeneticrisk.Otherriskfactorsincludeolderage,malegender,
highintakeoffat,alcohol
orredmeat,obesity,smoking,
andalackofphysicalexercise.20Inflammatoryboweldisease21Peoplewithinflammatoryboweldisease(ulcerativecolitis
andCrohn'sdisease)areatincreasedriskofcoloncancer.
Peoplewithinflammatoryboweldiseaseaccountforlessthan2%ofcoloncancercasesyearly.InthosewithCrohn'sdisease2%getcolorectalcancerafter10
years,8%after20
years,and18%after
30years.
Inthosewithulcerativecolitisabout16%developeitheracancerprecursororcancerofthecolonover30
years.
22ulcerativecolitisandCrohn'sdisease23Thosewithafamilyhistoryintwoormorefirst-degreerelatives(suchasaparentorsibling)haveariskofdiseaseandthisgroupaccountsforabout20%ofallcases.
Anumberofgeneticsyndromesarealsoassociatedwithhigherratesofcolorectalcancer.Themostcommonoftheseishereditarynonpolyposiscolorectalcancer(HNPCCorLynchsyndrome)whichispresentinabout3%ofpeoplewithcolorectalcancer.
24PathogenesisColorectalcancerisadiseaseoriginatingfromtheepithelialcellsliningthecolonorrectumofthegastrointestinaltract,mostfrequentlyasaresultofmutationsintheWntsignalingpathwaythatincreasesignalingactivity.Themutationscanbeinheritedoracquired,andmostprobablyoccurintheintestinalcryptstemcell(隱窩干細胞).
25ThemostcommonlymutatedgeneinallcolorectalcanceristheAPCgene,whichproducestheAPCprotein.TheAPCproteinpreventstheaccumulationofβ-cateninprotein.WithoutAPC,β-cateninaccumulatestohighlevelsandtranslocates(moves)intothenucleus,bindstoDNA,andactivatesthetranscriptionofproto-oncogenes.Thesegenesarenormallyimportantforstemcellrenewal(重建、重生)
anddifferentiation,butwheninappropriatelyexpressedathighlevels,theycancausecancer.26P53proteinBeyondthedefectsintheWntsignalingpathway,othermutationsmustoccurforthecelltobecomecancerous.Thep53protein,producedbytheTP53gene,normallymonitorscelldivisionandkills
cellsiftheyhaveWntpathwaydefects.27DiagnosisSignsandsymptomsRadiologicaltechniquesEndoscopyTumormarkers(CEA,CA199…)Pathologicassessment28TheextentofthediseaseisusuallydeterminedbyaCTscanofthechest,abdomenandpelvis.ThereareotherpotentialimagingtestsuchasPETandMRIwhichmaybeusedincertaincases.ColoncancerstagingisdonenextandbasedontheTNMsystemwhichisdeterminedbyhowmuchtheinitialtumorhasspread,ifandwherelymphnodesareinvolved,andtheextentofmetastaticdisease.29Diagnosisofcolorectalcancerisviasamplingofareasofthecolonsuspiciousforpossibletumordevelopmenttypicallydoneduringcolonoscopyorsigmoidoscopy,dependingonthelocationofthelesion.30Pathologicassessmentmicroscopymacroscopy31Cancersontherightsideofthelargeintestine(ascendingcolonandcecum)tendtobeexophytic(外生的),thatis,thetumorgrowsoutwardsfromonelocationinthebowelwall.Thisveryrarelycausesobstructionoffeces,andpresentswithsymptomssuchasanemia.Left-sidedtumorstendtobecircumferential(環(huán)周的),andcanobstructthebowellumen
andresultsinthinnercaliberstools.
macroscopy32macroscopyAppearanceoftheinsideofthecolonshowingoneinvasivecolorectalcarcinoma(thecrater-like,reddish,irregularlyshapedtumor).Grossappearanceofacolectomyspecimencontainingtwoadenomatouspolyps(thebrownishovaltumorsabovethelabels,attachedtothenormalbeigeliningbyastalk)andoneinvasivecolorectalcarcinoma(thecrater-like,reddish,irregularlyshapedtumorlocatedabovethelabel).33macroscopyEndoscopicimageofcoloncanceridentifiedinsigmoidcolon
onscreeningcolonoscopyinthesettingofCrohn'sdisease.???PET/CTofastagingexamofcoloncarcinoma.Besidestheprimarytumoralotoflesionscanbeseen.Oncursorposition:lungnodule.
34Themicroscopecellularcharacteristicsofthetumorareusuallyreportedfromtheanalysisofthetissuetakenfromabiopsyorsurgery.Apathologyreportwillusuallycontainadescriptionofcelltypeandgrade.Themostcommoncoloncancercelltypeisadenocarcinomawhichaccountsfor98%ofcases.Other,rarertypesincludelymphomaandsquamouscellcarcinoma.microscopy35micrographsCancer—Invasiveadenocarcinoma(themostcommontypeofcolorectalcancer).Thecancerouscellsareseeninthecenterandatthebottomrightoftheimage(blue).Nearnormalcolon-liningcellsareseenatthetoprightoftheimage.Cancer—Histopathologicimageofcoloniccarcinoid.36micrographsPrecancer—Tubularadenoma(管狀腺瘤)
(leftofimage),atypeofcolonicpolypandaprecursorofcolorectalcancer.Normalcolorectalmucosaisseenontheright.Precancer—Colorectalvillousadenoma(絨毛腺瘤)37ThecoloncancerstagingcanbemadeaccordingtotheTNMstagingsystemfromtheWHOorganization,theUICCandtheAJCC.TheAstler-Collerclassification(1954)ortheDukesclassification(1932)arenowlessused.Staging38TheTstagesofbowelcancerDukesstageAbowelcancer;thecancerisonlyintheinnerliningofthebowel.DukesstageBbowelcancer;thecancerhasinvadedthemuscleDukesstageCbowelcancer;thecancerhasinvadedthenearbylymphnodesDukesstageDbowelcancer;thecancerhasmetastasizedtheDukesclassification(1932)arenowlessused.39AJCC(TNM)StagingSystem:ThemostcommonlyusedstagingsystemforcolorectalcanceristhatoftheAmericanJointCommitteeonCancer(AJCC),sometimesalsoknownastheTNMsystem.40TheTNMsystemdescribes3keypiecesofinformation:T
describeshowfarthemain(primary)tumorhasgrownintothewalloftheintestineandwhetherithasgrownintonearbyareas.N
describestheextentofspreadtonearby(regional)lymphnodes.Lymphnodesaresmallbean-shapedcollectionsofimmunesystemcellsthatareimportantinfightinginfections.M
indicateswhetherthecancerhasspread(metastasized)tootherorgansofthebody.(Colorectalcancercanspreadalmostanywhereinthebody,butthemostcommonsitesofspreadaretheliverandlungs)41NumbersorlettersappearafterT,NandMtoprovidemoredetailsabouteachofthesefactors.Thenumbers0through4indicatedincreasingseverity.TheletterXmeans“cannotbeassessedbecausetheinformationisnotavailable.”42T
categories
for
colorectal
cancer
the
extent
of
spread
through
the
layers
thatform
the
wall
of
the
colon
and
rectum.
These
layers,
from
the
inner
to
the
outer,
include:
?The
inner
lining
(mucosa)
?A
thin
muscle
layer
(muscularis
mucosa)
?The
fibrous
tissue
beneath
this
muscle
layer
(submucosa)
?A
thick
muscle
layer
(muscularis
propria)
that
contracts
to
force
the
contents
of
the
intestines
along
?The
thin,
outermost
layers
of
connective
tissue
(subserosa
and
serosa)
that
cover
most
of
the
colon
but
not
the
rectum43Tx:No
description
of
the
tumor's
extent
is
possible
because
of
incomplete
information.
Tis:The
cancer
is
in
the
earliest
stage
(in
situ).
It
involves
only
the
mucosa.
It
has
not
grown
beyond
the
muscularis
mucosa
(inner
muscle
layer).
T1:The
cancer
has
grown
through
the
muscularis
mucosa
and
extends
into
the
submucosa.
T2:The
cancer
has
grown
through
the
submucosa
and
extends
into
the
muscularis
propria
(thick
outer
muscle
layer).
T3:The
cancer
has
grown
through
the
muscularis
propria
and
into
the
outermost
layers
of
the
colon
or
rectum
but
not
through
them.
It
has
not
reached
any
nearby
organs
or
tissues.
T4a:The
cancer
has
grown
through
the
serosa
(also
known
as
the
visceral
peritoneum),
the
outermost
lining
of
the
intestines.
T4b:The
cancer
has
grown
through
the
wall
of
the
colon
or
rectum
and
is
attached
to
or
invades
into
nearby
tissues
or
organs.
44N
categories
for
colorectal
cancer
N
categories
indicate
whether
or
not
the
cancer
has
spread
to
nearby
lymph
nodes
and,
if
so,
how
many
lymph
nodes
are
involved.
To
get
an
accurate
idea
about
lymph
node
involvement,
most
doctors
recommend
that
at
least
12
lymph
nodes
be
removed
during
surgery
and
looked
at
under
a
microscope.45Nx:No
description
of
lymph
node
involvement
is
possible
because
of
incomplete
information.
N0:
No
cancer
in
nearby
lymph
nodes.
N1a:
Cancer
cells
are
found
in
1
nearby
lymph
node.
N1b:Cancer
cells
are
found
in
2
to
3
nearby
lymph
nodes.
N1c:
Small
deposits
of
cancer
cells
are
found
in
areas
of
fat
near
lymph
nodes,
but
not
in
the
lymph
nodes
themselves.
N2a:Cancer
cells
are
found
in
4
to
6
nearby
lymph
nodes.
N2b:Cancer
cells
are
found
in
7
or
more
nearby
lymph
nodes.
46Mcategories
indicate
whether
or
not
the
cancer
has
spread
(metastasized)
to
distant
organs,
such
as
the
liver,
lungs,
or
distant
lymph
nodes.
M0:No
distant
spread
is
seen.
M1a:
The
cancer
has
spread
to
1
distant
organ
or
set
of
distant
lymph
nodes.
M1b:
The
cancer
has
spread
to
more
than
1
distant
organ
or
set
of
distant
lymph
nodes,
or
it
has
spread
to
distant
parts
of
the
peritoneum
(the
lining
of
the
abdominal
cavity).47Stage
0
:Tis,
N0,
M0Stage
I
:T1-T2,
N0,
M0Stage
IIA
:T3,
N0,
M0Stage
IIA
:T3,
N0,
M0Stage
IIC
:T4b,
N0,
M0Stage
IIIA
:T1-T2,
N1,
M0;T1,
N2a,
M0:Stage
IIIB
:T3-T4a,
N1,
M0;T2-T3,
N2a,
M0;T1-T2,
N2b,
M0Stage
IIIC
:T4a,
N2a,
M0;T3-T4a,
N2b,
M0;T4b,
N1-N2,
M0Stage
IVA
:Any
T,
Any
N,
M1aStage
IVB
:Any
T,
Any
N,
M1b:Stage
grouping
4849Mostcolorectalcancersshouldbepreventable,throughincreasedsurveillanceandlifestylechanges.Prevention50LifestyleCurrentdietaryrecommendationstopreventcolorectalcancerincludeincreasingtheconsumptionofwholegrains,fruitsandvegetables,andreducingtheintakeofredmeat.Theevidenceforfiberandfruitsandvegetableshoweverispoor.Physicalexerciseisassociatedwithamodestreductionincolonbutnotrectalcancerrisk.Sittingregularlyforprolongedperiodsisassociatedwithhighermortalityfromcoloncancer.Theriskisnotnegatedbyregularexercise,thoughitislowered.51MedicationAspirinandcelecoxib(希樂葆)
appeartodecreasetheriskofcolorectalcancerinthoseathighrisk.However,itisnotrecommendedinthoseataveragerisk.
Thereistentativeevidenceforcalciumsupplementationbutitisnotsufficienttomakearecommendation.VitaminDintakeandbloodlevelsareassociatedwithalowerriskofcoloncancer.52ScreeningAsmorethan80%ofcolorectalcancersarisefromadenomatouspolyps,screeningforthiscanceriseffectivenotonlyforearlydetectionbutalsoforprevention.
Diagnosisofcasesofcolorectalcancerthroughscreeningtendstooccur2–3yearsbeforediagnosisofcaseswithsymptoms.
Anypolypsthataredetectedcanberemoved,usuallybycolonoscopy,andthuspreventedfromturningcancerous.Screeninghasthepotentialtoreducecolorectalcancerdeathsby60%.53Thethreemainscreeningtestsarefecaloccultbloodtesting(大便潛血試驗),flexiblesigmoidoscopy,andcolonoscopy.
Ofthethree,onlysigmoidoscopycannotscreentherightsideofthecolonwhere42%ofmalignanciesarefound.
VirtualcolonoscopyviaaCTscanappearsasgoodasstandardcolonoscopyfordetectingcancersandlargeadenomasbutisexpensive,associatedwithradiationexposure,andcannotremoveanydetectedabnormalgrowthslikestandardcolonoscopycan.54Fecaloccultbloodtesting(FOBT)ofthestoolistypicallyrecommendedeverytwoyears.
IfabnormalFOBTresultsarefound,participantsaretypicallyreferredforafollow-upcolonoscopyexamination.AnnualtobiennialFOBTscreeningreducecolorectalcancermortalityby16%andamongthoseparticipatinginscreeningcolorectalcancermortalitycanbereducedupto23%,althoughithasnotbeenproventoreduceall-causemortality.
Immunochemicaltestsarehighlyaccurateanddonotrequiredietaryormedicationchangesbeforetesting.55SomecountrieshavenationalcolorectalscreeningprogramswhichofferFOBTscreeningforalladultswithinacertainagegroup,typicallystartingbetweenage50and60.ExamplesofcountrieswithorganizedscreeningincludetheUnitedKingdom,
AustraliaandtheNetherlands.56MedicalsocietiesintheUnitedStatestypicallyrecommendscreeningbetweentheageof50and75
yearswithsigmoidoscopyevery5yearsandcolonoscopyevery10years.Forthoseathighrisk,screeningsusuallybeginataround40.Itisunclearwhichofthesetwomethodsisbetter.
Colonoscopymayfindmorecancersinthefirstpartofthecolonbutisassociatedwithgreatercostandmorecomplications.Forpeoplewithaverageriskwhohavehadahigh-qualitycolonoscopywithnormalresults,theAmericanGastroenterologicalAssociationdoesnotrecommendanytypeofscreeninginthe10yearsfollowingthecolonoscopy.
Forpeopleover75orthosewithalifeexpectancyoflessthan10
years,screeningisnotrecommended.57Thetreatmentofcolorectalcancercanbeaimedatcureorpalliation.Thedecisiononwhichaimtoadoptdependsonvariousfactors,includingtheperson'shealthandpreferences,aswellasthestageofthetumor.
Whencolorectalcancerbefoundatearlystages,surgerycanbecurative.However,whenitisdetectedatadvancedstages(forwhichmetastasesarepresent),thisislesslikelyandtreatmentisoftendirectedatpalliation,torelievesymptomscausedbythetumourandkeepthepersonascomfortableaspossible.Treatment58SurgeryLaparotomyLaparoscopicoperationPalliativeoperation59SurgeryAdiagramofalocalresectionofearlystagecoloncancerAdiagramoflocalsurgeryforrectalcancer60D1,2,3DissectionCentralgroupMiddlegroupNearbygroup61CME
(completemesocolicexcision)forcoloncancerTME(totalmesorectalexcision)forrectumcancerTwoconceptsoftheoperationforcolorectalcancer:62TheprinciplesofCMEandTME:Withthevisualizingandthesharpdissection,totallyremovethemesocolicorthemesorectalbetweentheviscerallayerandwalllayeroffascia.Exposingandcuttingoffcentrallyatthemesentericvesselroot.Completelyremovetheregionallymphnodesandtopreventthespreadingandmetastasesofcancercells.63CME
(completemesocolicexcision)forcoloncancer64CME
(completemesocolicexcision)forcoloncancer65TME(totalmesorectalexcision)forrectumcancer----Coronalsection66-----sagittalsection----CoronalsectionTME(totalmesorectalexcision)forrectumcancer67ChemotherapyInbothcancerofthecolonandrectum,chemotherapymaybeusedinadditiontosurgeryincertaincases.Thedecisiontoaddchemotherapyintreatmentofcolonandrectalcancerdependsonthestageofthedisease.68InStageIcoloncancer,nochemotherapyisoffered,andsurgeryisthedefinitivetreatment.TheroleofchemotherapyinStageIIcoloncancerisdebatable,andisusuallynotofferedunlessriskfactorssuchasT4tumororinadequatelymphnodesamplingisidentified.Itisalsoknownthatthepatientswhocarryabnormalitiesofthemismatchrepairgenesdonotbenefitfromchemotherapy.ForstageIIIandStageIVcoloncancer,chemotherapyisanintegralpartoftreatment.69Ifcancerhasspreadtothelymphnodesordistantorgans,whichisthecasewithstageIIIandstageIVcoloncancerrespectively,addingchemotherapyagentsfluorouracil,capecitabineoroxaliplatinincreaseslifeexpectancy.
Ifthelymphnodesdonotcontaincancer,thebenefitsofchemotherapyarecontroversial.Ifthecanceriswidelymetastaticorunresectable,treatmentisthenpalliative.Typicallyinthissetting,anumberofdifferentchemotherapymedicationsmaybeused.Chemotherapydrugsforthisconditionmayincludecapecitabine,fluorouracil,irinotecan,oxaliplatinandUFT.70Antiangiogenicdrugssuchasbevacizumabareoftenaddedinfirstlinetherapy.Anotherclassofdrugsusedinthesecondlinesettingareepidermalgrowthfactorreceptor(EGFR)inhibitors,ofwhichthetwoFDAapprovedonesarecetuximabandpanitumumab.71Theprimarydifferenceintheapproachtolowstagerectalcanceristheincorporationofradiationtherapy.Often,itisusedinconjunctionwithchemotherapyinaneoadjuvantfashiontoenablesurgicalresection,sothatultimatelyascolostomyisnotrequired.However,itmaynotbepossibleinlowlyingtumors,inwhichcase,apermanentcolostomymayberequired.StageIVrectalcanceristreatedsimilartostageIVcoloncancer.72RadiationtherapyWhileacombinationofradiationandchemotherapymaybeusefulforrectalcancer,itsuseincoloncancerisnotroutineduetothesensitivityofthebowelstoradiation.
Justasforchemotherapy,radiotherapycanbeusedintheneoadjuvantandadjuvantsettingforsomestagesofrectalcancer.73PalliativecarePalliativecareismedicalcarewhichfocusesontreatmentofsymptomsfromseriousillness,likecancer,andimprovingqualityoflife.
Palliativecareisrecommendedforanypersonwhohasadvancedcoloncancerorhassignificantsymptoms.Involvementofpalliativecaremaybebeneficialtoimprovethequalityoflifeforboththepersonandhisorherfamily,byimprovingsymptoms,anxietyandpreventingadmissionstothehospital.74Palliativecarecanconsistofproceduresthatrelievesymptomsorcomplicationsfromthecancerbutdonotattempttocuretheunderlyingcancer,therebyimprovingqualityoflife.Surgicaloptionsmayincludenon-curativesurgicalremovalofsomeofthecancertissue,bypassingpartoftheintestines,orstentplacement.Theseprocedurescanbeconsideredtoimprovesymptomsandreducecomplicationssuchasbleedingfromthetumor,abdominalpainandintestinalobstruction.
Non-operativemethodsofsymptomatictreatmentincluderadiationtherapytodecreasetumorsizeaswellaspainmedications.Follow-up75Theaimsoffollow-uparetodiagnose,intheearliestpossiblestage,anymetastasisortumorsthatdeveloplater,butdidnotoriginatefromtheoriginalcancer.76TheU.S.NationalComprehensiveCancerNetwork(NCCN)andAmericanSocietyofClinicalOncology(ASCO)provideguidelinesforthefollow-upofcoloncancer.
Amedicalhistoryandphysicalexaminationarerecommendedevery3to6monthsfor2years,thenevery6monthsfor5years.
Carcinoembryonicantigenbloodlevelmeasurementsfollowthesametiming,butareonlyadvisedforpeoplewithT2orgreaterlesionswhoarecandidatesforintervention.77ACT-scanofthechest,abdomenandpelviscanbeconsideredannuallyforthefirst3yearsforpatientswhoareathighriskofrecurrence(forexample,thosewhohadpoorlydifferentiatedtumorsorvenousorlymphaticinvasion)andarecandidatesforcurativesurgery(withtheaimtocure).Acolonoscopycanbedoneafter1year,exceptifitcouldnotbedoneduringtheinitialstagingbecauseofanobstructingmass,inwhichcaseitshouldbeperformedafter3to6months.Ifavillouspolyp,apolyp>1centimeterorhighgradedysplasiaisfound,itcanberepeatedafter3years,thenevery5years.Forotherabnormalities,thecolonoscopycanberepeatedafter1year.78RoutinePETorultrasoundscanning,chestX-rays,completebloodcountorliverfunctiontestsarenotrecommended.
Theseguidelinesarebasedonrecentmeta-analysesshowingintensivesurveillanceandclosefollow-upcanreducethe5-yearmortalityratefrom37%to30%.79Exercisemayberecommendedinthefutureassecondarytherapytocancersurvivors.
Inepidemiologicalstudies,exercisemaydecreasecolorectalcancer-specificmortalityandall-causemortality.Resultsforthespecificamountsofexerciseneededtoobserveabenefitwereconflicting.Thesedifferencesmayreflectdifferencesintumourbiologyandexpressionofbiomarkers.Themechanismofhowexercisebenefitssurvivalmaybeinvolvedinimmunesurveillanceandinflammationpathways.Exercise80Inclinicalstudies,apro-inflammatoryresponsewasfoundinpatientswithstageII-IIIcolorectalcancerwhounderwent2weeksofmoderateexerciseaftercompletingtheirprimarytherapy.Oxidativebalancemaybeanotherpossiblemechanismforbenefitsobserved.Otherpossiblemechanismsmayinvolvemetabolichormoneandsex-steroidhormones,althoughthesepathwaysmaybeinvolvedinothertypesofcancers.81InEuropethefive-yearsurvivalrateforcolorectalcancerislessthan60%.Inthedevelopedworldaboutathirdofpeoplewhogetthediseasedie
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