Hindawi Publishing Corporation BioMed Research International Volume 2014, Article ID 925840, 13 pages http://dx.doi.org/10.1155/2014/925840 Review Article Novel Biomarkers of Abdominal Aortic Aneurysm Disease: Identifying Gaps and Dispelling Misperceptions DemetriosMoris,1EleftheriosMantonakis,1EfthymiosAvgerinos,2MarinosMakris,3 ChrisBakoyiannis,1EmmanuelPikoulis,1andSotiriosGeorgopoulos1 1FirstDepartmentofSurgery,VascularUnit,“Laiko”GeneralHospital,NationalandKapodistrianUniversityofAthens, AgiouThoma17,11527Athens,Greece 2DivisionofVascularSurgery,UniversityofPittsburgh,Pittsburgh,PA15213-2582,USA 3ImperialCollege,LondonSW72AZ,UK CorrespondenceshouldbeaddressedtoEleftheriosMantonakis;[email protected] Received6March2014;Revised29April2014;Accepted4May2014;Published20May2014 AcademicEditor:ThomasSchmitz-Rixen Copyright©2014DemetriosMorisetal. This is an open access article distributed under the Creative Commons Attribution License,whichpermitsunrestricteduse,distribution,andreproductioninanymedium,providedtheoriginalworkisproperly cited. Abdominalaorticaneurysm(AAA)isaprevalentandpotentiallylife-threateningdisease.Earlydetectionbyscreeningprograms andsubsequentsurveillancehasbeenshowntobeeffectiveatreducingtheriskofmortalityduetoaneurysmrupture.Theaimofthis reviewistosummarizethedevelopmentsintheliteratureconcerningthelatestbiomarkers(from2008todate)andtheirpotential screeningandtherapeuticvalues.OursearchincludedhumanstudiesinEnglishandfoundnumerousnovelbiomarkersunder research,whichwerecategorizedin6groups.Mostofthesestudiesareeitherexperimentalorhamperedbytheirlownumbersof patients.Weconcludedthatcurrentlynospecificlaboratorymarkersallowscreeingforthediseaseandmonitoringitsprogression ortheresultsoftreatment.Furtherstudiesandstudiesinlargerpatientgroupsarerequiredinordertovalidatebiomarkersas cost-effectivetoolsintheAAAdisease. 1.Introduction countries such as UK [5]. Current guidelines recommend electiverepairforaneurysmsofmorethan5.5cmindiameter, Abdominal aortic aneurysm (AAA) is a relatively common whileincreasedriskgroups(women,smokers,andvascular and potentially life-threatening disease, with a prevalence hypertensionandchronicairwaypatients)maybenefitbya rangingfrom4.1%to11.5%inEuropeanpopulations[1].The lowerthresholdof5cm[6]. mostfearedcomplicationofAAAdiseaseisrupture,which Advances in the endovascular aneurysm repair (EVAR) often leads to the patient’s death. While small aneurysms technique over the last two decades have led to a major may rupture too, the risk is greater for bigger aneurysms, paradigmshiftinsurgicalapproachforaorticaneurysms[7, soearlydiagnosisthroughscreeningandpromptevaluation 8].Byprovidinglowerperioperativemortalityandmorbidity, of which aneurysms are likely to rupture are key points in endovasculartechniquesareincreasinglybeingpreferredin the management and research around AAA. No effective the elective setting [8, 9]. However, late complications of conservativetreatmentexistsand,whendecidedtointervene, EVAR, such as endoleaks, may result in progression of the surgical correction remains the only effective and “finite” underlyinganeurysm,evendelayedrupture,thusmandating treatment of AAA, with the optimal timing for surgery alifelongsurveillanceprogram[10]. beingthemaindebatablepoint.Existingevidenceindicates TraditionalAAAscreening,evaluation,andsurveillance betteroveralloutcomewhenrepairofAAAisperformedon programsemploytheuseofimagingtechniquessuchasCT electivebasiscomparedtotheemergencyrepair[2–4].Thus angiogram(CTA),ultrasoundsonography(US),ormagnetic screeningprogramsofAAAhavebeeninitiatedindeveloped resonance imaging (MRI). Despite the proven efficacy of 2 BioMedResearchInternational these imaging techniques, the cost associated with such 3.1.BiomarkersRelatedtoExtracellularMatrix programscanincursignificantfinancialburdenstothehealth HomeostasisorProteolysis caresystems[11–14],soalternativemethodsarecontinuously being 3.1.1.CystatinCandCathepsin. CystatinCistheendogenous researched. inhibitor of the elastolytic enzymes cathepsins, which are Biomarkershaveattractedmuchattentioninthefieldof strongly expressed in the aneurysmatic wall. Cystatin C aneurysmresearchandaredefinedasmeasurablemolecules expressionisfoundreducedinAAAdisease,leadingtolack (peptides, proteins, and metabolic products) that express of inhibition of the elastolytic properties of cathepsins. In a specific biological process in the organism at a given a prospective study [18], a negative correlation of serum time [15]. In order for a biomarker to be useful, it should cystatinCvalueswithAAAsizeandannualexpansionrate be able either to detect the disease itself or to express its wasfound,butwithoutmentionablepotentialforpredicting progression.Soausefulbiomarkershoulddetectthepresence casesrequiringsurgery. of a subclinical aneurysm or be a measure of its size and In another large study [19], plasma cathepsin S levels expansionrate,thuspredictingtheriskofrupture.Itisknown correlatedpositivelywithaorticdiametersbutnegativelywith that this risk increases when the observed expansion rate lowestankle-branchialindex(ABI).PlasmacathepsinSlevels isgreaterthantheexpected[16].Furthermore,abiomarker showed no correlation with AAA annual expansion rate, a coulddefinetheoptimalsurveillanceintervalsandpossibly finding mentioned as inexplicable. After logistic regression identifypathogenicpathwayswhichcouldguidemonitoring analysis, the study also reflected reduced cystatin C in and treatment [17]. We should not fail to mention that, in humans with AAA lesions, while no association was found orderforabiomarkertobeemployedinmodernhealthcare between cystatin C and AAA annual growth rate, likely system,itsuseshouldbecost-effective.Someofthepatients becauseoftherelativelyshortAAAobservationtime. selected through this process should be pointed towards more focused screening by specialized imaging techniques. 3.1.2. Circulating Basement-Membrane (BM) Fragments. Circulatingbiomarkersthuspresentasattractivealternatives Types IV and XVIII of collagen are components of the forscreeningandmonitoringpurposesparticularlyinhealth- basement membrane. Ramazani et al. [20] have recently care systems which lack the infrastructure to support other shown that AAA patients had significantly increased levels primary or secondary screening programs. In this review, oftypes IV andXVIII collagen comparedwiththecontrols we aim to provide a summary of the emerging biomarkers (𝑃 = 0.005and𝑃 < 0.001,resp.).Moreover,AAApatients implicatedinAAApathophysiology. had significantly increased level of type XVIII collagen (𝑃 < 0.01) when compared with the peripheral arterial disease(PAD)group[20]. 2.MaterialsandMethods Thisstudywasconductedinasmallnumberofpatients, indicating that further studies are required to establish the The MEDLINE/PubMed database was searched for pub- potentialroleofBMfragmentsasbiomarkersforAAA. lications with the medical subject heading “biomarkers in abdominal aortic aneurysms (AAA).” Two independent 3.1.3. Osteoprotegerin (OPG). It has been suggested that reviewers (D.M. and E.M.) performed the literature search, serum osteoprotegerin (OPG) levels are associated with thestudyselection,andthedataextraction.Allthereferences growth of AAAs while in vitro experiments showed that fromtheidentifiedarticlesweresearchedforrelevantinfor- OPGpromotesmatrixmetalloprotease(MMP)releasefrom mation.ThestartingdatewasJanuary2008,since,previously, monocytes and vascular smooth muscle cells [21, 22]. In bibliography was covered by the review of Urbonavicius et a recent study [23], the concentration of aortic wall OPG al. [17] and the end date of the review was April 2014. We was positively associated with established markers of AAA focused on human studies that reported the presence of severity(cathepsinsA,B,andSandtheactivityofMMP-2and aneurysm,size,expansionrates,andriskofruptureandon MMP-9),whileitappearedtobeassociatedwithlymphocytes new biomarkers and their potential value relevant to the andplasmacells.Thesenewerdatainhumansreinforcethe management of AAA. We excluded articles that were not olderfindingsofaroleforOPGinAAApathogenesis. writteninEnglishorarticlesofwhichfull-textsandabstracts werenotaccessibleorcomprehensive. 3.1.4. Tenascin-C (TN-C). TN-C is a matricellular (extra- cellular matrix) protein that is synthesized by various cell 3.Results types including vascular smooth muscle cells (VSMC) in response to inflammatory cytokines and mechanical stress Numerousstudieswerefoundandcategorizedinthefollow- [24].TN-Cistypicallysynthesizedinpathologicalconditions ingcategories:biomarkersrelatedtotheextracellularmatrix like wounds, inflammation, and tumorigenesis [25]. No homeostasis or proteolysis, biomarkers related to cellular biomarkerisavailableforindicatingthepathologicalstatusof signaling pathways, proteins releases by the intraluminal VSMCandinterstitialcellsandTN-Cmaybeusefulforthis thrombus,biomarkersrelatedtocirculatingcellsandinflam- purpose, possibly in combination with other inflammatory mation, metabolomics, and genetic biomarkers. These are markers and ECM degradation products. TN-C has the describedseparatelyinthefollowingsection. advantage of being deposited locally in the inflammatory BioMedResearchInternational 3 lesion (AAA) and it is also released in stable forms into correlationamongPRX-1andAAAdiameterandexpansion circulation[26]. rate were also found. The combination of PRX-1 and AAA Further studies are required to elucidate the complete sizeseemstobesignificantlypredictiveofAAAgrowth[36], function of TN-C and to evaluate whether serum levels or establishingPRX-1asapromisingbiomarker. bioimaging of TN-C is better suited for the assessment of diseaseactivityinhumanAAA. 3.3.2. Neutrophil Gelatinase-Associated Lipocalin (NGAL). NGALplasmaconcentrationshavebeenassociatedwithcar- 3.2.BiomarkersRelatedtoCellularSignalingPathways diovascular diseases [37]. Polymorphonuclear cells (PMNs) isolated from AAA patients secreted significantly greater 3.2.1.C-ReactiveProtein. ItisknownthatC-reactiveprotein amountsofNGALthanPMNsfromcontrolsandcorrelated (CRP)isanindependentriskfactorforarteriosclerosis. with retrospective AAA growth [38]. The ILT releases large In a cohort study in men with small AAAs [27], CRP amountsofNGALcomparedtotheabluminalthrombus,the levelswerefoundhigherinlargerAAAs,butnoassociation aneurysm wall, and the healthy aortic media [38]. Further wasfoundwiththeaneurysmexpansionrate.Asapossible studies in larger subjects groups are needed to confirm the explanation,itwassuggestedthatinflammation,asdepicted association between NGAL and AAA presence and growth bythelevelsofinflammatorymarkers,ismorearesponseto [38]. expansionratherthantheprimarycause. It has been suggested that the ILT ofAAAs predisposes Inanotherstudy[28],nocorrelationwasfoundbetween for enlargement and rupture. The growth of the AAA is levels of circulating CRP and other inflammatory markers dependentonproteolyticdegradationofelastin.NGALcan and the expansion of small-diameter AAAs, indicating no bindtoMMP-9andinhibititsdegradation,therebypreserv- clinicaluseofthesemarkersinAAAsurveillance. ingenzymaticactivity[39].ComplexesofNGALandactive A recent cohort study [29] investigated the association MMP-9werepresentinthrombus,theinterfacefluid,andthe betweenplasmaCRPlevelsandAAAdiameterandassessed aneurysmwall.Still,theimportanceoftheseobservationsis the relationship between the gradient of CRP levels and unknownandthecontributionofthecomplexNGAL/MMP- rates of expansion in asymptomatic AAAs. A statistical 9totheAAAgrowthshouldbefurtherevaluated[39]. association was confirmed between the AAA diameter and highsensitive-CRP(hs-CRP)plasmalevels,showingapos- 3.3.3.Insulin-LikeGrowthFactorsandTheirBindingProteins siblecausalassociationandsuggestinghs-CRPplasmalevel (IGFs and IGFBPs). Lindholt et al. [40] have evaluated the gradient as a marker of disease progression and rate of potential role of IGF-I and IGF-II as biomarkers in 115 expansion. patients with AAA, kept under annual surveillance for 10 Sincetheseresultsareconflicting,further,largerstudies years.SerumIGF-IcorrelatedpositivelywithAAAsizeand arerequiredtodrawsafeconclusions. growthrate(𝑃 = 0.016and𝑃 = 0.004,resp.),findingsthat persist after adjustment for potential confounders. Serum 3.2.2. Diminished Soluble Tumor Necrosis Factor-Like Weak IGF-Ilevelpredictedcasesneedinglatersurgery(95%con- InducerofApoptosis(sTWEAK). sTWEAKisatypeIItrans- fidenceinterval(CI):0.52–0.73)[40]. membrane glycoprotein of the TNF superfamily that circu- IGFBP-1waslocalizedintheluminalpartofAAAthrom- latesinplasma[30]andisexpressedinSMCsandleukocytes bus and IGFBP-1 levels were increased in AAA thrombus inarterialwall[31].sTWEAKwasfoundreducedinpatients conditioned media, compared to media layer and healthy withcoronaryarterydisease[32],carotidatherosclerosis[33], media [41]. It seemed to facilitate the potentiation of ADP- orPAD[34].Mart´ın-Venturaetal.[35]measuredsTWEAK inducedplateletaggregationtriggeredbyIGF-1,whileitscon- plasmalevelsinpatientswithAAAandfoundthatsTWEAK centrations were significantly higher in large AAA patients concentrationsweredecreasedinsmall(≤5cm,𝑃 = 0.03)as compared with control subjects (normal aortic size) (𝑃 < wellaslargeAAAs(>5cm,𝑃=0.004)comparedwithhealthy 0.01). Moreover, IGFBP-1 levels correlated with AAA size subjects.Moreover,sTWEAKconcentrationswerenegatively (𝑃 < 0.001), which remained significant after adjusting for associatedwithAAAsize(𝑃 = 0.008)andAAAexpansion riskfactors[41]. ratewith5yearsoffollow-up(𝑃=0.031)[35]. These results show that sTWEAK is strongly associated 3.4.BiomarkersRelatedtoCirculatingCellsandInflammation with the presence of an aneurysm but fails to differentiate amongsmallandlargeaneurysms[35]. 3.4.1. Lymphocytes. Increasing evidence shows that the autoimmuneresponsecontributesimportantlytothepatho- 3.3.ProteinsReleasedbyIntraluminalThrombus(ILT) genesis of AAA. More specifically, CD4(+), CD25(+), and FOXP3(+) Tregulatorycells(Tregs)werefoundsignificantly 3.3.1. Peroxiredoxin-1 (PRX-1). Martinez-Pinna et al. [36] decreased in AAA patients compared to the control group analyzed proteins released by intraluminal thrombus (ILT) (𝑃<0.01),indicatingimpairedimmunoregulation[42]. with proteomic approach and found that PRX-1 was more Additionally,thelossoftheinhibitoryreceptorCD31on released by the luminal layer compared with the abluminal peripheralTlymphocytesisfoundtobeassociatedwiththe layer of the ILT. Increased PRX-1 serum levels in AAA incidence of atherosclerotic complications such as AAA in patients compared with healthy subjects and a positive patients [43]. These findings should be further researched 4 BioMedResearchInternational in order to establish potential biomarkers of the natural macrophages infiltrating in the adventitia. With the intra- historyofAAA,aswellaspotentialtherapeutictargetsforthe operative use of indocyanine green lymphography, lymph inhibitionofthecreationandprogressionofaneurysms. stasis was revealed in the intima/medial in AAA patients, In another study, increased plasma levels of sCD28 and while fluorescence microscopy confirmed the accumula- sCD86(𝑃 = 0.0001)anddecreasedplasmalevelsofsCTLA- tion of lymph in the intima/media but not in adventitia. 4 (𝑃 = 0.0018) were found in AAA patients compared These results demonstrate that infiltration of macrophages with normal individuals. These levels were not related to in intima/media is associated with lymphangiogenesis and the patient’s age or the size of aneurysm, but there was a angiogenesisinAAA,whilethereisevidenceofinadequate significantinverserelationshipbetweentheconcentrationsof lymph-drainageintheAAAwall. sCTLA-4andsCD80withmatrixmetalloproteinase-9[44]. 3.4.5. Catalase. PMNs play a key role in AAA progression. Diminishedcatalaseexpressionandactivitywereobservedin 3.4.2. Monocytes. In a more recent study [45], CD16(+) PMNsfromAAApatientscomparedwithcontrols.Catalase monocytesubsets were foundincreased in large abdominal plasma levels were also decreased in large and small AAAs aorticaneurysmsandweredifferentiallyrelatedtocirculating whencomparedwithhealthyindividuals.Thisstudywasalso and cell-associated (CD143) biochemical and inflammatory conductedinaverysmallnumberofpatients[49]. biomarkers. A clinical implication of this study is that, by taking common blood measurements (plasma D-dimer, creatinine, and age to derive eGFR, uric acid, total white 3.4.6.Pathogens. Onestudy[50]showedthatP.gingivalis,a blood,andneutrophilcounts),onecoulddiscriminateAAA commonpathogeninvolvedinchronicperiodontitis,acceler- patients with different monocyte-dependent inflammatory atesAAAprogressionviarecruitmentandactivationofneu- profiles.Thisstudywashamperedbycross-sectionaldesign trophils,leadingtoproductionofNETswhicharedetectable and the relatively small number of patients, while it was intheplasmaofAAAsubjects.Theseresultswereconfirmed unable to find a clear relation of the size of AAA and the byanexperimentinrats.Sincerepeatedsubclinicalepisodes valuesofcirculatingmonocytesubsetsinpatientsatdifferent ofbacteremiaaresystematicallyassociatedwithperiodontal stagesofexpansionofaorticdamage. diseases, P. gingivalis could be therefore a key factor in human AAA progression. Still, more epidemiological and observational studies in humans should be made before 3.4.3.ProgenitorCells. CD34(+)levelsareaknownmarkerof organizing therapeutic strategies based on the treatment circulatingprogenitorcells.VanSpyketal.[46]investigated of periodontal disease to prevent AAA evolution towards the role and compared the percentage of CD34(+) cells in rupture. AAA disease and peripheral vascular disease (PVD). This smallstudyrevealedalowerpercentageofCD34(+)cellsin 3.5.Metabolomics. Metabolomicsstandsforsensitiveanalyt- AAA patients, compared to PVD patients, concluding that icaltechniquessuchasmetabolicfingerprintingwithmulti- AAAisalessseverevasculardiseasethanPVD.Furtherstudy variateanalysis.Metabolomicsseemstobeagoodapproach isneededinordertoestablishCD34(+)cellsasabiomarker tofindbiomarkersofAAA[51]. forriskstratification. Guanidinosuccinicacid(GSA),whichismainlyreleased from the ILT, is highly increased in the plasma of AAA 3.4.4. Lymphangiogenesis. A study by Scott et al. [47] patientswhencomparedtocontrols.GSAbehaves likenitric attemptedtoresearchtherelationshipbetweeninflammation oxide(NO),duetoitsvasodilatoryactionsanditsabilityto and neovascularization in AAA tissue. The results showed activatetheNOgeneratingN-methyl-D-aspartate(NMDA) thattheaneurysmwallcontainedhighlevelsofinflammatory receptor.AfterbeinggeneratedintheILT,GSAissecretedto infiltrate, while microvascular densities of blood (𝑃 < bloodstream,andtheamountofsecretedGSAisrelatedto 0.001)andlymphatic(𝑃 = 0.003)vesselsweresignificantly thestageofAAA[52]. increased in AAA samples compared with controls. Vascu- Hippuricacidissecretedonlybytheluminalpartofthe larity as expressed by positive staining for CD31, CD105, ILT and was found significantly decreased in the plasma of and D2-40 correlated positively with inflammation, while AAApatients.Thisobservationcorrelateswiththehyperex- increased VEGFR-3 and VEGF-A expression was observed cretionofhippuricacidinatheroscleroticstate[51]. within inflammatory areas of AAAs. These results suggest Long-chainacylcarnitinesweredecreasedintheplasma lymphaticvesselinvolvementinAAAdisease,associatedwith of AAA patients compared to controls. There was a clear theextentofinflammation[47]. decreasingtrendwithincreasingsizeofaneurysmwhichmay In a recent study [48], infiltration of lymphatic ves- indicatealteredfattyacid𝛽-oxidationordeficiencyofcarni- sel endothelial hyaluronan receptor- (LYVE-) 1, vascu- tine[51].Additionally,asignificantdecreaseinsphingosine- lar endothelial growth factor- (VEGF-) C, and matrix 1-phosphate (S1P) and sphinganine-1-phosphate in AAA metalloproteinase- (MMP-) 9-positive macrophages and patients was also found. Both molecules are sphingolipids; podoplanin and Prox-1-positive microvessels were identi- sphinganine-1-phosphateisaparentofsphingosineandS1P. fied by immunohistochemistry in the intima/media in the S1P is a lysophospholipid and significant changes in other AAA wall, where hypoxia-inducible factors- (HIF-) 1𝛼 was lysophospholipidslikeLysoPEsandLysoPCsarereportedin expressed. VEGF-C and MMP-9 were not expressed in thisinvestigation.Apossibleexplanationfordecreaseinthe BioMedResearchInternational 5 amount of LysoPCs/PEs in plasma of AAA patients, with a AAA [60]. The serum HDL concentrations were lower in trendrelatedtothesizeofaneurysm,istheiraccumulation patientswithAAAsandwereindependentlyassociatedwith intheILT[51]. a reduced risk of having an AAA, in men not receiving current lipid-modifying therapy (95% CI 0.56–0.93 per 0.4-mM increase) and in the total cohort (95% CI 0.63– 3.5.1. Vitamin D Binding Protein (DBP) and Vitamin D. 0.91 per 0.4-mM increase). The concentrations of LDL During last decades, there has been a surge of interest in and triglycerides were not associated with the presence of vitaminDanditswiderangeofhealthbenefits,partiallydue AAAs[61]. tothemanyassociationstudieslinkingvitaminDstatuswith Past studies [62] have revealed decreased low-density commonhumandiseases.DBPisthemainserumcarrierof lipoprotein receptor-related protein 5 (LRP5) gene expres- vitaminDmetabolites,withalbuminactingasanalternative sion in peripheral blood cells of AAA patients and an lower affinity binder [53]. Gamberi et al. [54] showed a association between decreased expression of LRP5 and negativecorrelationbetweenDBPandthepresenceofAAA. increased lipoprotein (a) [Lp(a)] levels in AAA patients. In Evenifitsvalueisnotwellestablishedyet,DBPispivotalfor a recent study [63], LRP5 gene polymorphisms rs4988300 vascularremodelinganditmayhaveanimportantroleinthe and rs3781590 were found independent genetic markers protectionofvascularwalls. of AAA, even after adjusting for age, sex, dyslipidemia, In a more recent observational study [55], 4233 older hypertension, smoking habit, and chronic obstructive pul- men (70–88 years old) participated in a randomized con- monarydisease.AAApatientshadsignificantlyhigherLp(a) trolledtrialofscreeningforAAA.Thestudymeasuredtheir levels than control subjects (𝑃 < 0.0001). Further study- infrarenalaorticdiameterbyultrasoundandtheir25(OH)D ing of the role of these markers in AAA and of LRP5 plasma levels by immunoassay. An inverse relationship gene in Lp(a) catabolism and AAA pathophysiology is between vitamin D status and the presence of larger AAA necessary. wasfound,alongwithaninversedose-responseassociation between 25(OH)D concentrations and the size of AAA, suggestingaroleofvitaminDintheseverityofaneurysmal 3.5.4. Phospholipases. Wallinder et al. [64] showed that arterial disease. Further research is needed to clarify the patientswithsmallAAAshadincreasedlevelsoftheenzyme mechanismsunderlyingtheseassociations. glycosylphosphatidylinositol-specificphospholipaseD(GPI- PLD)comparedwithcontrolswithoutaneurysmbyusinga 3.5.2.Homocysteine. Wongetal.[56]investigatedinacross- proteomic approach, providing some evidence of the value sectional study the relationship of homocysteine and the of GPI-PLD as a novel potential plasma biomarker for presence and diameter of AAAs in older men (70–88 years the detection of AAAs [64]. In the same tone, Golledge old). Plasma total homocysteine (tHcy) was found to be et al. found [65] that serum secretory phospholipase A(2) associated with the presence of AAA, while there was also (sPLA(2)) activity is elevated in men with small AAAs but a positive dose-response relationship between tHcy and isnotassociatedwithAAAprogression. abdominalaorticdiameter.Theinvestigatorsconcludedthat further, longitudinal studies and clinical trials of lowering 3.5.5. Iron. A recent study by Martinez-Pinna et al. [66] tHcyarerequiredinordertoassessiftheserelationshipsare foundincreasedredbloodcell-(RBC-)borneironretention causal. andtransferrin,transferrinreceptor,andferritinexpression in AAAtissue comparedto controls.In contrast,decreased 3.5.3.LipoproteinsandLipoprotein-RelatedReceptors. Results circulatingiron,transferrin,meancorpuscularhaemoglobin ofameta-analysissuggestthatcirculatinglipoproteinalpha concentration (MCHC), and haemoglobin concentration, (Lp(a))concentrationsmaybehigherinpatientswithAAA along with circulating RBC count, were observed in AAA than those in subjects without AAA, thus playing a role in patients compared to controls, whereas hepcidin concen- thediagnosisofAAA[57].Low-densitylipoproteinreceptor- trations were increased in AAA subjects. Moreover, iron, relatedprotein1(LRP1)demonstratedsignificantassociation transferrin, and haemoglobin levels were negatively, and with AAA size (𝑃 = 0.0042) [58]. In a small pilot study in hepcidinpositively,correlatedwithaorticdiameterinAAA 12 patients by Chan et al. [59], lipoprotein receptor-related patients. MCHC negatively correlated with thrombus area protein1(LRP1)expressionwasfoundsignificantlylowerin in another cohort of AAA patients. Anemia was signifi- AAApatientsthanincontrols,whilenosignificantcorrela- cantly more prevalent in AAA patients compared to that tionwasshownbetweenLRP1expressionandthesizeofAAA in patients with atherosclerotic aortoiliac occlusive disease. (𝑃 > 0.05). These results suggest that a reduction in LRP1 Finally,themortalityriskamongAAApatientswithanemia expressioncouldbeassociatedwithaneurysmprogression. was increased by almost 30 as compared to AAA subjects Other metabolites used to discriminate the natural with normal hemoglobin levels. This study showed that history of patients with large aneurysm, small aneurysm, local iron retention and altered iron recycling associated and controls are the metabolites of cholesterol. Decreased with high hepcidin and low transferrin systemic concen- plasmalevelsofthosemetaboliteswereobservedinpatients trationscouldleadtoreducedcirculatinghaemoglobinlev- with large and small aneurysms in comparison to con- els in AAA patients and that low haemoglobin levels are trols [51]. Lower serum HDL cholesterol and higher serum independently associated with AAA presence and clinical LDL cholesterol may be associated with the presence of outcome. 6 BioMedResearchInternational 3.6.GeneticBiomarkers 4.Discussion 3.6.1. Telomere Length. Telomeres are specialized DNA In this review article, we aimed to give a description of sequences at the ends of linear chromosomes. Telomere the emerging biomarkers that can correlate with biological attritionisthephenomenonoftelomerelength“shortening” processesassociatedwiththeexistence(presence/diagnosis) with each successive cell division, eventually leading to and progression (size/risk of rupture) of abdominal aortic cell senescence and/or apoptosis. These observations can aneurysms(AAAs).Ourmaingoalwastoenrichthecurrent contribute to the estimation of the cellular biological age knowledgeonbiomarkersinAAAdisease,asitwaspresented [67]. In humans, reduced telomere length in circulating by Urbonavicius et al. [17] in their review at 2008, and leucocytes is associated with premature vascular disease, analyze the progress made in this scientific field from 2008 withthetelomere:genomicDNAcontentbeingsignificantly to date. As stated earlier, the clinical value of biomarkers reducedinwallbiopsiesofAAAcomparedtonormalaortas is based on their properties to satisfy the goals of early (𝑃 < 0.001) [67]. This decreased telomerase endothelial detection(screening),surveillanceintermsofearlyandlater expression implies a protective role of telomerase against progression,andmonitoringofthebiologicperformanceof AAA formation [68]. Lowest telomere restriction fragment anAAAaftersurgicaltreatment.Anidealbiomarkershould (TRF)lengthvaluesdoubletheriskofhavingAAAcompared be able to be applied in all of the above. Early detection with a mean TRF length in the highest values (𝑃 = 0.005) andclosesurveillancecangreatlybenefitpatients,sincethey [69]. are referred for elective repair with a lower risk, compared with the emergency setting [2–4]. The mortality of elective 3.6.2. AAA1 Locus on Chromosome 19q13. Several single- AAA repair has been 5% or less, but, once rupture occurs, nucleotidepolymorphisms(SNPs)werenominallyassociated operative mortality is as high as 48% [77]. Studies have with AAAs (𝑃 < 0.05) [70, 71]. The SNPs with most alsoshownincreasedcostofopenrepairofrupturedAAAs significant𝑃valueswerepeptidaseD(PEPD)andCD22[71]. (rAAAs) compared to elective open repair; some are even Immunohistochemical staining for CD22 revealed protein as high as five times more per life saved per year, with the expressioninlymphocytespresentintheaneurysmalaortic costsfromemergencyrepairofrAAAviaEVARtobeeven wallonlyandnodetectableexpressionincontrolaortas[71]. higher[78,79].ManydevelopedcountriesliketheUSA,UK, PEPDproteinwasexpressedinfibroblastsandmyofibroblasts and Sweden have established national screening programs in the media-adventitia border in both aneurysmal and for AAA based mostly on ultrasonography with important nonaneurysmaltissuesamples[71]. resultsinthefieldofearlydetectionandfollow-up[11–14,80]. Unfortunately,thisisnotthecaseinothercountries,which cannot afford such high cost of implementing such a wide 3.6.3.9p21. AAAisamonganumberofvasculardisordersto screeningprogram[80].Morespecifically,inarecentstudy berecentlyassociatedwithacommonallelicvariantsituated [81],itwasshownthattheindividualcostperinvitedsubject on chromosome 9p21 [72, 73]. A significant association wasC60(US$83.2)and0.011additionalqualityadjustedlife betweenrs10757278-GandthepresenceofAAAwasfound years(QALY)weregainedperpatientinthescreenedcohort, (𝑃 = 0.03), an effect size completely consistent with that corresponding to an incremental cost-effectiveness ratio originally reported [73]. rs10757278 was not significantly (ICER) of C5673/QALY (US $7870/QALY). These numbers associated with altered AAA growth rate [73]. In a newer areunlikelytobefeasibleinaperiodofworldeconomiccrisis. study[74],single-nucleotidepolymorphismsrs10757278and Taking into account the relatively high prevalence of the rs1333049 of chromosome 9p21-3 region were significantly diseaseandthehighmortalityratesincasesofrupture,along associatedwithincreasedriskofAAA.Thisstudyrevealedno withthehighICUandhospitalcosts[82],evenafterEVAR, associationbetweenpolymorphismsandaorticdiametersin itseemsimperativetoestablishandstandardizebiomarkers AAApatients,whileaspecificgenotype(GGofrs10757278) thatcanbeappliedindailypracticeandbe was suggested to interact with the homocysteine biological cost-effective. pathwaytostimulatethepresenceofAAA.Thisdataempha- Aspresented,numerousbiomarkers,relatedtotheAAA sizedtheneedtofurtherstudytheroleofthesebiomarkers. disease,arecurrentlybeingresearched.Mostofthesestudies areeitherexperimentalorhamperedbytheirlownumbersof 3.6.4. Chemokine Receptors (CCRs). Chronic inflammation patients.Still,onecansaythatbiomarkersreflectbiological plays an important role in AAA formation. The chemokine processesassociatedwithadisease,makingthemmoreinter- receptors CCR2, CCR5, and CXCR3 are associated with estingforpersonalizedmedicineratherthanforastatistical pathways implicated previously in aneurysm pathogenesis. pointofview. Chemokinereceptor-2(CCR2)isinvolvedintheregulation sTWEAKisstronglycorrelatedwithaneurysmexistence oftheinflammatoryresponse[75].CCR2heterozygoteV64I or expansion rate but fails to differentiate small to large polymorphism and allele frequency were more frequently aneurysms [35]. TN-C contributes in stratifying risk in observedintheAAAgroup(𝑃 = 0.01,𝑃 = 0.004)[75],but patientswithAAAbeforeinterventionorafterEVAR[2],but therewasnosignificantdifferencewiththecontrolgroupin further study is required to elucidate the function of TN-C relationtotheDelta32allelefrequency[76]. andtoevaluatewhetherserumlevelsorbioimagingofTN- Table1summarizesthepublishedstudiesonbiomarkers C would be suited for the assessment of disease activity in inAAAandtheirclinicalvalue. humanAAAs. BioMedResearchInternational 7 d d d n n n n Clinicalvalue Aneurysmprogressio neurysmdetectionaprogression Aneurysmdetection Aneurysmsize Aneurysmdetection Aneurysmgenesis Aneurysmdetection Aneurysmgeneris Aneurysmsizeandprogression Aneurysmsizeandthrombusexistence neurysmdetectionaprogression neurysmdetectionaprogression A A A rs(2008–2014)inAAAandtheirclinicalvalue. FindingsAstatisticalassociationwasconfirmedbetweentheAAAdiameterandhighsensitive-CRP(hs-CRP)plasmalevels.Otherstudiesshowcontroversialresults[27,28]sTWEAKplasmalevelsinpatientswithAAAcomparedwithhealthysubjects.sTWEAKconcentrationswerenegativelyassociatedwithAAAsizeandAAAexpansionrateCD4(+),CD25(+),andFOXP3(+)TcellsinAAApatientsarefoundsignificantlylowerthanthoseofthecontrolgroup CD16(+)monocytesubsetswerefoundincreasedinlargeabdominalaorticaneurysmsandweredifferentiallyrelatedtocirculatingandcell-associated(CD143)biochemicalandinflammatorybiomarkers AlowerpercentageofCD34(+)cellsinAAApatients,comparedtoPVDpatients,wasfound LymphaticvesselinvolvementinAAAdisease,associatedwiththeextentofinflammation Infiltrationofmacrophagesinintima/mediaisassociatedwithlymphangiogenesisandangiogenesisinAAA,whilethereisevidenceofinadequatelymph-drainageintheAAAwallDiminishedcatalaseexpressionandactivitywereobservedinPMNsfromAAApatientscomparedwithcontrolsP.gingivalisacceleratesAAAprogressionviarecruitmentandactivationofneutrophils,leadingtoproductionofNETs SerumIGF-IcorrelatedpositivelywithAAAsizeandgrowthrate IGFBP-1concentrationsweresignificantlyhigherinlargeAAApatientscomparedwithcontrolsubjects AAApatientssecretedsignificantlygreateramountsofNGALthanPMNsfromcontrolsandcorrelatedwithretrospectiveAAAgrowthIncreasedPRX-1serumlevelsinAAApatientscomparedwithhealthysubjectsandpositivecorrelationamongPRX-1andAAAdiameterandexpansionratewerealsofound e nnovelbiomark Studydesign Cohortstudy secontrolstudy ospectivestudy secontrolstudy secontrolstudy secontrolstudy secontrolstudy secontrolstudy Experimentalstudy ospectivestudy secontrolstudy secontrolstudy ospectivestudy o Ca Pr Ca Ca Ca Ca Ca Pr Ca Ca Pr s e di u anst Year 2012 2011 2010 2013 2013 2013 2014 2011 2011 2011 2012 2012 2011 m u h yofthepublished Author DeHaroetal.[29] ´Martın-Venturaetal.[35] Yinetal.[42] Ghigliottietal.[45] VanSpyketal.[46] Scottetal.[47] Sanoetal.[48] Ramos-Mozoetal.[49] Delboscetal.[50] Lindholtetal.[40] Ramos-Mozoetal.[41] Ramos-Mozoetal.[38] Martinez-Pinnaetal.[36] r a m s r Table1:Sum Biomarker CRP sTWEAK Lymphocytecorrelatedbiomarke Monocyte-relatedbiomarkers ProgenitorCells Lymphangiogenesis Catalase(PMNs) Pathogens IGFs NGAL Peroxiredoxin-1 s y a w s dtopath dtond bymbu Category Biomarkersrelatecellularsignaling Biomarkersrelatecirculatingcellsainflammation Proteinsreleasedintraluminalthro(ILT) 8 BioMedResearchInternational ClinicalvalueAneurysmsizeandprogressionAneurysmsizeandprogression Aneurysmdetection neurysmgenesisandgrowth neurysmprogressionndtreatmentefficacy Aneurysmdetection Aneurysmdetection Aneurysmdetection Aneurysmgenesis Aneurysmdetection A Aa FindingsNegativecorrelationwithaneurysmsizeandexpansion,nopotentialforpredictingsurgeryPositivecorrelationwithaorticdiameters,nocorrelationwithAAAannualexpansionrate AAApatientshadsignificantlyincreasedlevelsoftypesIVandXVIIIcollagencomparedwiththecontrols AorticwallOPGwaspositivelyassociatedwithestablishedmarkersofAAAseverity,whileitappearedtobeassociatedwithlymphocytesandplasmacellsTN-CisusedtostratifyriskinpatientswithAAAbeforeinterventionandalsoafterendovascularrepairTelomere:genomicDNAcontentbeingsignificantlyreducedinwallbiopsiesofAAAcomparedtonormalaortas CD22revealedproteinexpressioninlymphocytespresentintheaneurysmalaorticwallonlyandnotincontrolaorta.PEPDproteinwasexpressedinfibroblastsandmyofibroblastsinthemedia-adventitiaborderinbothaneurysmalandnonaneurysmaltissuesamples Asignificantassociationbetweenrs10757278-Gandthe𝑃=0.030presenceofAAAwasfound().rs10757278wasnotsignificantlyassociatedwithalteredAAAgrowthrate SNPrs10757278andrs1333049ofchromosome9p21-3regionweresignificantlyassociatedwithincreasedriskofAAA.ThisstudyrevealednoassociationbetweenpolymorphismsandaorticdiametersinAAApatientsCCR2heterozygoteV64IpolymorphismandallelefrequencyweremorefrequentlyobservedintheAAAgroup able1:Continued. Studydesign Prospectivestudy Prospectivestudy Casecontrolstudy Retrospectivestudy Follow-upstudy Casecontrolstudy GWAS Cohortstudy Casecontrolstudy Casecontrolstudy T Year 2001 2012 2011 2012 2010 2008 2011 2009 2014 2011 Author Lindholtetal.[18] Lvetal.[19] Ramazanietal.[20] Kooleetal.[23] Greenhalghetal.[2] Wilsonetal.[67] Lillvisetal.[71] Thompsonetal.[73] Weietal.[74] Katranciogluetal.[75] e n a 3 Biomarker CystatinC CathepsinS Circulatingbasement-membrfragments OPG Tenascin-C(TN-C) Telomerelength AAA1locusonchromosome19q1 9p21 CCRs s si y elatedtomatrixorproteol Category Biomarkersrextracellularhomeostasis Genomicbiomarkers BioMedResearchInternational 9 Clinicalvalue Aneurysmdetection Aneurysmdetection Aneurysmdetection Aneurysmdetection Aneurysmdetection Aneurysmdetection Aneurysmsize Aneurysmdetectionandsize Aneurysmsizeanddetection Aneurysmdetectionandprogression nsitive;Se:selenium;Lp(a): e s FindingsLp(a)concentrationsmaybehigherinpatientswithAAAthanthoseinsubjectswithoutAAA LowerserumHDLcholesterolandhigherserumLDLcholesterolmaybeassociatedwithAAApresenceLipoproteinreceptor-relatedprotein1(LRP1)expressionwasfoundsignificantlylowerinAAApatientsthancontrols,whilenosignificantcorrelationwasshownbetweenLRP1expressionandthesizeof𝑃>0.05AAA()AssociationbetweendecreasedexpressionlevelsofLRP5geneinAAApatientsLRP5genepolymorphismsrs4988300andrs3781590werefoundindependentgeneticmarkersofAAA.AAApatientshadsignificantlyhigherLp(a)levelsthan𝑃<0.0001controlsubjects() NegativecorrelationbetweenDBPandAAApresence AninverserelationshipbetweenvitaminDstatusandthepresenceoflargerAAAwasfound,alongwithaninversedose-responseassociationbetween25(OH)DconcentrationsandthesizeofAAA Plasmatotalhomocysteine(tHcy)wasfoundtobeassociatedwiththepresenceofAAA,whiletherewasalsoapositivedose-responserelationshipbetweentHcyandabdominalaorticdiameterSmallAAAhadincreasedlevelsoftheenzymeglycosylphosphatidylinositol-specificphospholipaseD(GPI-PLD)comparedwiththecontrolswithoutaneurysmLocalironretentionandalteredironrecyclingassociatedwithhighhepcidinandlowtransferrinsystemicconcentrationscouldleadtoreducedcirculatinghaemoglobinlevelsinAAApatients.LowhaemoglobinlevelsareindependentlyassociatedwithAAApresenceandclinicaloutcome or-alpha;IL-6:interleukin-6;CRP:Creactiveprotein;hs:highlyors. Table1:Continued. Studydesign Meta-analysis Meta-analysis Casecontrolstudy Casecontrolstudy Casecontrolstudy Proteomics Randomizedclinicalstudy Cross-sectionalstudy Casecontrolstudy ha:tumornecrosisfactCRs:chemokinerecept pC Year 2009 2010 2013 2009 2013 2011 2013 2013 2012 2014 TNF-alocalin; ator;dlip Author Takagietal.[57] Takagietal.[60] Chanetal.[59] Giustietal.[62] Galoraetal.[63] ngGamberietal.[54] Wongetal.[55] Wongetal.[56] Wallinderetal.[64] Martinez-Pinnaetal.[66] tissue-likeplasminogenactiveutrophilgelatinase-associate ndi e es PA:L:n Biomarker Lps VitaminDbiprotein Homocystein Phospholipas Iron metalloproteinases;ta1antitrypsin;NGA dingalph graAT: Category Metabolomics MMPs:matrix-delipoprotein(a);a1- 10 BioMedResearchInternational As far as biomarkers related to ILT are concerned, IGF reviewingthepaper.SotiriosGeorgopouloswasresponsible and PRX-1 seem to be the most promising due to their forthecriticalandthoughtfulreviewandthesupervisionof statistically established correlation with AAA diameter and thecompositionofthepaper. growth[36,40]. 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