Psychoneuroendocrinology71(2016)102–109 ContentslistsavailableatScienceDirect Psychoneuroendocrinology journal homepage: www.elsevier.com/locate/psyneuen Executive functioning and diabetes: The role of anxious arousal and inflammation KyleW.Murdocka,AngieS.LeRoya,b,TamaraE.Lacourtc,DannyC.Duked, Cobi J.H eijnenc,Ch ristop he rP.Fagun desa,c,e, ∗ aDepartmentofPsychology,RiceUniversity,BioscienceResearchCollaborativeRoom773,6100MainStreet,Houston,TX77005,UnitedStates bDepartment of Psychology, Univ ersityofHo uston,369 5CullenB oulevardRoo m126 ,Hou ston, TX77 204,Un itedState s cDepartment of SymptomRe search,The U niversity ofTex asMD Anderson Cancer Cen ter,1515 Hol combe Bouleva rd,Unit1450,Houston,TX77030,United States dDivisionofPsychology,InstituteonDevelopmentandDisability,OregonHealthandScienceUniversity,707SWGainesStreet,Portland,OR97239,United States eDepartmentofPsychiatry,BaylorCollegeofMedicine,OneBaylorPlaza–BCM350,Houston,TX77030,UnitedStates a r t i c l e i n f o a b s t r a c t Articlehistory: Individualswhoperformpoorlyonmeasuresoftheexecutivefunctionofinhibitionhavehigheranx- Receiv ed28January2016 iousarousa linc ompariso ntoth ose withbett er perf ormance. Highanx iou sarousali sasso ciated with RAeccceepivteedd i3n Mr eavyis2e0d1 f 6orm 2 May 2016 a pro -inflam ma tory respon se. Chron ically high anxious arous al and inflamm ation i nc rease one’s risk ofdevelopingtype2diabetes.Wesoughttoevaluateanxiousarousalandinflammationasunderlying mechanismslinkinginhibitionwithdiabetesincidence.Participants(N=835)completedmeasuresof Keywords: cognitiveabi lities,a self-report meas ureofan xiousarou sal,anddona ted blood toassessi nterleukin -6 Executivefunctioning (IL-6)andglycatedhemoglobin(HbA1c).Individualswithlowinhibitionweremorelikelytohavedia- Inhibition betesthanthosewithhighinhibitionduetotheserialpathwayfromhighanxiousarousaltoIL-6.Findings Anxiousarousal Inflamm ation remained when entering other indicators of cognitive abilities as covariates, suggesting that inhibition Diabetes isauniquecognitiveabilityassociatedwithdiabetesincidence.Onthebasisofourresults,wepropose severalavenuestoexploreforimprovedpreventionandtreatmenteffortsfortype2diabetes. ©2016ElsevierLtd.Allrightsreserved. 1. Introduction tions.Thepresentstudydrawsfromthepsychoneuroimmunology literaturetoexaminehowcognitiveprocessesandimmunefunc- Emotionalstressisariskfactorforpoorphysicalhealth.Indeed, tioning underlie the association between anxious arousal and highanxietyisassociatedwithdiabetesincidence(Lietal.,2008). glycated hemoglobin (HbA1c), a well-known biomarker used to A better understanding of the association between anxiety and estimatebloodglucoseduringthepreceding2–3months. bloodglucoseisimportantgiventhatapproximately347million Theexecutivefunctionofinhibition(alsoknownasattentional people worldwide have diabetes, which has imposed a growing controlorinhibitorycontrol)isassociatedwiththeexperienceof economicstrainonhealthcaresystems(Zhangetal.,2010).More- stressfulemotionssuchasanxiety.Inhibitionistheabilitytorefrain over, approximately 90% of all diabetes is type 2, which can be fromrespondingorattendingtotempting/distractinginformation, preventedordelayedvialifestylechanges(e.g.,physicalactivity, objects,thoughts,oractivities.Indeed,thosewhohavelowinhi- diet;TuomilehtoandWolf,1987;WHO,2014)thataremorediffi- bition are more likely to attend to anxious thoughts, and have culttoachievewhenstressedoranxious(Stults-Kolehmainenand greaterdifficultyshiftingtheirattentionawayfromsuchthoughts, Sinha,2014).Therefore,afurtherunderstandingoftheassociation thanthosewithhighinhibition(DeGutisetal.,2015;Joormannand betweenanxietyandbloodglucoseisneededtoimproveinterven- Gotlib,2010;SchmeichelandTang,2015).Othershavearguedthat betterinhibitionisassociatedwithlessanxietyviatheabilityto flexiblyandadaptivelyrespondtoone’senvironmentusingopti- malcopingstrategies(e.g.,Marteletal.,2007).Indeed,inflexibility ∗ inthinkingisassociatedwithincreasedanxiety(e.g.,Brittonetal., Correspondingauthorat:BioscienceResearchCollaborative,Rm773MS-142, 6100MainStreet,H ouston ,Un itedStates . 20 10),whic h mayexplai nwh ythosewi thbette rinh ibitionr ep ort E-mailaddresses:[email protected],[email protected] lessanxietythanthosewithpoorinhibition.Theneurovisceralinte- (C.P.Fagun des). http://dx.doi.org/10.1016/j.psyneuen.2016.05.006 0306-4530/©2016ElsevierLtd.Allrightsreserved. K.W.Murdocketal./Psychoneuroendocrinology71(2016)102–109 103 .09* (.02, .16) Anxious Arousal Interleukin-6 -.12* (-.05, -.18) .26* (.03, .50) .08 (-.16, .31) -.08* (-.02, -.15) -.01 (-.23, .21) Inhibition Diabetes Incidence Fig.1. Amediationmodelofassociationsbetweeninhibition,anxiousarousal,interleukin-6,anddiabetesincidence.Standardizedregressioncoefficientsarerepresented whenpredictinganxiousarousalandinterleukin-6,whilelogisticregressioncoefficientsarerepresentedwhenpredictingdiabetesincidence.95%confidenceintervalsare depict edinparen theses.I ndirecte ffec tsusing5000b ootstr apsamp les:anxiou sarousal(0 .008 9,SE=0.0144 ,95% CI=−0.018 1,0.0407 ),interleuk in-6 (0.0220,SE= 0.0142,9 5% CI=0.0023,0.0616),andserialmediation(i.e.,mediationinsequence;0.0028,SE=0.0022,95%CI=0.0003,0.0103).Controlvariablesincludedparticipantage,sex,ethnicity, bodymassindex,useofinsulin,andsmokinghistory,aswellthetimelagbetweenassessments.*p<0.05. grationmodel(e.g.,ThayerandLane,2009)alsoindicatesthatthose raldeclineofcognitiveskillsandincreaseininflammationnearthe withpoorinhibitionarelessphysiologicallycapableofresponding endofhumanlife(Magakietal.,2007;Simenetal.,2011).Further- and adapting to their environment in comparison to those with more,inhibitionistypicallycombinedwithothercognitiveabilities betterinhibition.Asaresult,thosewithpoorinhibitionaremore instatisticalanalyses,limitingtheabilitytounderstandtheunique likelytohaveapre-attentivebiastothreatinformationthanthose effectsofinhibition(Marslandetal.,2015).Specifically,indicators withbetterinhibitionduetoaninabilitytoflexiblyrespond,and ofexecutivefunctioning(i.e.,workingmemory,cognitiveflexibil- aremorelikelytoreportincreasedarousalduetothisbias(Thayer ity,andinhibition)areoftencombinedintoalatentconstructof andFriedman,2004).Therefore,bothcognitiveandphysiological executive functioning as opposed to being evaluated as individ- processes may link poor inhibition with increased anxiety. High ualpredictorsoftargetedoutcomes.Accordingly,itisimportantto anxiety is associated with poor overall physical health in adults determineifinhibitionisassociatedwithdiabetesthroughanxious (Needham et al., 2015), which is notable given that those with arousalandinflammation. lowinhibitionaschildrenexhibitpoorphysicalhealthoutcomes Weexpectedthatlowinhibitionwouldbeassociatedwithhigh inadulthood(Moffittetal.,2011). anxiousarousaland,inturn,highinflammation.Itwaspredicted The underlying mechanisms linking low inhibition and poor that the serial pathway from anxious arousal to inflammation healthhavenotbeenadequatelystudied.Inadditiontoincreased wouldexplaintheassociationbetweeninhibitionanddiabetesinci- anxiety(SchmeichelandTang,2015),lowinhibitionisalsoarisk dence(i.e.,serialmediation).Furthermore,weexpectedthatthis factor for poor diabetes management because of an inability to pathwaywouldremainsignificantaboveandbeyondotherindica- consistentlyadheretoandcompletediabetesmanagementtasks torsofcognitiveabilities(i.e.,performanceondigitspan,backwards (Wassermanetal.,2015).Therefore,itisimportanttogeneratea counting,andnumberseriesmeasures). further understanding of how inhibition is linked to diabetes to improvepreventionandinterventionefforts. Inflammation may play an important role in linking inhibi- tion and diabete s. Tho se w ith high stress dem on strate a greater 2. Materialandmethods inflammatoryresponsethanindividualswhoarelessstressedat themoderate effectsize level (i.e.,r=0.42 to0 .57; Fagu ndeseta l., 2.1. Participantsandprocedure 2013).Anxiety,aswellasstressmoregenerally,leadstoinflam- mation viaactiv ati onof nu clearfa ctor-k appaB(N F-KB). Ac tivation DatawereobtainedfromtheMidlifeDevelopmentintheUnited ofNF-K Bin creasespr od uctiono fpro-inflamm a torycyto kinessuch States (M IDU S) study in wh ich menta l and physica l h ealt h out- as interle ukin-6(B ierhauseta l.,2 003).Further,chro nicinflam ma- comes wereexa mined am ongan ationall yrep resentati vesamp leof tio n is a reliabl e predicto r o f d iabete s onset a t the s mall effect middle aged adults.Da tafrom t wotimepo intswereutili zedinth e size le ve l (i.e., r= 0.28–0.33 ; C hen et a l., 200 9; Pert icone et al., present stud y.Speci ficall y,me asur esof cogniti veab ilitydesc ri bed 2008 ;We nget a l., 2010),asw ellas m orbi dityan dmortalit yw ith beloww ereco mpleteddur ingabase lin evisit.Al lother measures smallt omod era tee ffectsi zes typi cal lyidentifie d(i.e .,r=0.10– 0.40; werec ompl etedatthe follow- up visit,wh icho ccu rreda naverage Kieco lt- Glasereta l.,201 0).In addition toinflamm atio n b eingapre- of 23 .39 months (S D= 14.28) afte r par ticipan ts comple ted cogni- dictor of diabe te s o nset, d ia betes pro gr ession is asso ciated w ith tiv e mea sures. A tota l of 451 2 pa rticipants co mpleted co gnitive increa sed inflamm ationo vertime( Stehouwere ta l.,2002).Ch ronic asse ssments.O ft hose wh ocom pletedtheco gnitiveass essments, elevated i nflammation is ass ociat ed with inc re ase d risk of heart 1255agreed top artici patea ndwereid enti fiedasbe ingmedically disease ( OR=1.45; Han ss on, 2005), a maj or complic ation o f dia- safet otravel to Madison,W I,L osAn geles,CA,o rW ashi ngton,DC, betes(G rund y etal. ,1999).Ind icators o fanxio usarousal(e.g .,ra cing fort he follow -u passessm ent. Com pleteda taw as obtainedfro ma heart, chestpa in) ar estron gerpredict or sofinfla mmatio ntha ncog- tot alof 835partic ipants(Mage= 57.62,SD =11. 60).S ignifican tmea n nitive anxie ty(e.g .,fe arfulof dyingorlo sin gcontrol)at thes mall differ en ces were not id entified amo ng th ose w ith comple te vs. effects sizelev el(r= 0.12;D ui viset al., 2013), possibly du eto acti- incomplete dataf orth evastmaj orityof study variab les(i.e.,in hi- vation ofth esym p at hetic nervou ss yst em(Jan ig,2014 ). bition,anxio usa rou sal, inter leukin-6, dia betes incidence ,age ,sex, Asl ow inh ibitionisass ociatedw ithhig hanxio usarousalatthe ethnici ty, body mass in dex, and time lag betw een asses smen ts); mediu me ffectsizele ve l(r=0.38; DeGu tiset al.,201 5),lowi nh ibi- however, partic ipant s with inco mplet e d ata were older (t=2.34, tionmay alsob eass ociat ed w ithh ighinfla mm at ion;ho wev er,itis p=0.02) a nd more lik ely to have a his tory of sm oking (t = 2.84, uncl earif inhi bit ionisassoc iated with inflammation inthegen er al p = 0.01) in c ompar ison to th ose w i th comp let e data, co n si stent populat io nasthelite ra turehaspr imar ilybeenfocuse do nth enatu- w it hthe ne edtobemedi cal lysafe totra veltothef ollow -upassess- ment . 104 K.W.Murdocketal./Psychoneuroendocrinology71(2016)102–109 Table1 Participantcharacteristics. Variable Metcriteriafordiabetes(n=103)Mean(SD)or Didnotmeetcriteriafordiabetes(n=737) number(%) Mean(SD)ornumber(%) Participantageatbiologicalassessment 62.55(10.88) 57(11.58) Participantsex Male 54(52.4) 319(43.6) Female 49(47.6) 413(56.4) Participantethnicity White 93(90.3) 686(93.8) Non-white 10(9.7) 46(6.2) Bodymassindex 32.51(7.57) 28.69(5.65) Eversmokedcigarettesregularly? Yes 51(49.5) 428(58.4) No 52(50.5) 304(41.6) Inhib ition −0 .21(2. 02) 0.35 (1.94) Logtransformedinterleukin-6 0.45(0.31) 0.30(0.32) HemoglobinA1cpercentage 7.53(1.35) 5.73(0.36) Fastingglucosemg/dL 133.22(49.19) 95.16(10.40) Digitspan 4.71(1.27) 5.08(1.42) Backwardscounting 36.51(11.45) 39.80(10.82) Numberseries 2.01(1.40) 2.64(1.50) Note.Inhibitionreflectsthez-standardizationandcombinationofaveragereactiontimeandnumberoferrorsonthereversedandmixedconditionsofthego-nogotask. Allcognitivetestswereadministeredoverthetelephoneinthe conditionoftheSGSTwasmoderatelycorrelated(i.e.,r=0.52)with MIDUSstudy(TunandLachman,2006).Thereliabilityandvalidity TaskSwitchingfromtheBostonCognitiveBattery,a90mininper- ofconductingthecognitivemeasuresoverthephoneintheMIDUS sonassessment,usingasubsampleofMIDUSparticipants(n=299) study was recently evaluated and excellent test-retest reliability who also participated in the Boston Longitudinal Study (BOLOS; wasidentified(Lachmanetal.,2014).Moreover,moderatetolarge Miller and Lachman, 2000). The SGST was also tested in person correlations ranging from 0.55 to 0.95 were identified between among a subsample (n=30) of participants who had also com- atelephoneadministrationandanin-personadministrationina pletedthemeasureoverthetelephone.Thecorrelationbetween subsampleof30participants.Inaddition,moderatetolargecorre- thetelephoneandinpersonadministrationsoftheSGSTwas0.71 lationsrangingfrom0.42to0.54wereidentifiedbetweenmeasures (Lachmanetal.,2014). onthetelephoneadministrationandparticipantperformancefor similarmeasuresontheBostonCognitiveBattery(Lachmanetal., 2.2.2. Anxiousarousal 2014)w hichisad mi niste redin person. Th e62item versionoftheMoodandAnxietySymptomQues- tionnaire(MASQ;ClarkandWatson,1991)wasutilizedtomeasure 2.2. Measures anxiousarousal.OntheMASQ,individualsreportedthedegreeto whichth eyexpe rien ced variou sfeelingso rsensatio ns( e.g.,“w as 2.2.1. Inhibition shortofbreath”)duringthepreviousweekonascalerangingfrom1 Th estopandgoswitchtask(SGST)wasdesignedtomeasure (very sli ghtlyorn otata ll)to 5(extre mely) .A to talof 16item scom - inhibiti on an d a tten tion sh ifting (Lachm an et al., 201 4; Tun and prise theanxi ou sar ou sals ca le ,withtherem a ining it em sasse ssing Lachman, 2006 ,2008)an dconsis tsofthree con dit ions.In the first gener ald istressa ndanhe donia .Inth epr esentstud y,the reliability condition (i.e.,n ormal) ,par ticipants w ereas kedtorespo nd bys tat- coefficie ntforth ean xiousarous al sca lewasac ceptab le( (cid:2)=0.75). ing“stop”whenpresentedwiththestimulusword“red”or“go” wh enpres entedw iththesti mulus wo rd“green ”acros s20tr ials .For 2.2.3. Interleukin-6 these condcond ition (i.e. ,reverse) ,part icipants werei nst ructed to Se rumIL-6levelswereevaluatedviahigh-sensitivityenzyme- stat ethew ord“go”w hen presente dwiththest imulu sword“re d” linked im mun osorbe nt as say (ELISA ) (Q uantikine, R&D Systems, and“ stop ”whe npre sente dwiththe stimu lus word“gr een”a cross Minne apolis,MN)witha sensi tivityof detectionat0 .16pg .mL.Val- 20t rials.In thet hirdandfin alco ndi tion(i.e., mixed ),partic ipants ueswerelog trans form e dtonorma liz ethedist rib utio nofsco res. we re pro vid ed with a cu e of e ither “nor mal” or “rev erse” before IL-6 was sele cted as an in dic ator of infl am mation as it ha s been being presente dwith astim u luswo rdacross 32 trials.For exam- linke dwi thanxiou sa rou sal(O’Don ov anetal.,2010) an dt ype 2dia- ple,if aparticipa ntwa s provided witht hecue of “norm al”a ndthe betes( Doyl eetal.,2 013).Se rumIL-6is als oa mark erof acut e and stim u lu s word “gre en,” the corre ct re spo nse wa s “go”; h owe ver, chron icstres s( Kiec olt-Gla sereta l.,2 00 3).M o reover, an imalw ork iftheyw erepr esentedw ith thecue of“rever se”a ndthe stimulus hasdem onstr atedthatvagus ne rve stimu lation,wh ichisas soci- w ord“ green ,”thecorre ctres pon sew as “stop.”Res pon sela tencyfor ated with improve d in hibitio n (Tha yer and Lane , 2009 ), r educes theSG STinth ep resents tudyrefl ects theave ragetime ittook to prod uction of tumor necrosis f actor (TN F)-a lpha a nd IL-6 (Wang corr ectly res pon dtoeach stimu lusinth ere versean dmix ed cond i- etal.,2004) .O therim munebio marke rsthatwere anal yzed during tion.Inth enorma lc ondit ion,inhib iti ons killsare not utilize d,and th eM IDUSs tudy(i .e.,C-Rea ctiveprotei n,IL- 6rece ptor,E-se lectin, assu ch ,res ponsela tencyinth enormalc ondit ionw as notinclu ded inte rcellula radhe sion molecule1 (ICAM-1 ))ar enotstron glylinked in prese ntstudya nalyses .D urin gfollow -upanaly ses, we included with vagus n erve stim ulation a n d stress r egu latio n, two i mpor- th enumbe rofer rorsfrom eachc onditiona saddition alin dicators tant mecha nisms fortheassoc iatio nbetw eeninhibit iona ndIL-6 ofin hibition to determ ine ifthe rewerean ys peed/error tradeoffs. (Step toeetal.,200 7; Wan getal.,200 4). Indicatorsofinhibitionwerereversecodedsuchthathigherscores indicatedbetterinhibition. 2.2.4. HemoglobinHbA1c Usingresponselatencyastheprimaryindicatorofinhibition, AnHbA1cassaywasperformedbyMeriterLabsinMadison,WI Lachman etal.(201 4)dem ons trat edexcell entpsych om etricchar- using theCob asInt egra ®analyzer (Ro cheDia gnost ic s,Indiana po- acteristicsfortheSGST.Forinstance,responselatencyforthemixed lis, IN). Percent HbA1c, which is represented in the descriptions K.W.Murdocketal./Psychoneuroendocrinology71(2016)102–109 105 Table2 Bivariatecorrelationsbetweenstudyvariables. Variable 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 1.Inhibition-reverse – 2.Inhibition-mixed 0.61* – 3. AA −0.11 * −0.13* – 4. IL-6 −0.14* −0.13* 0.14* – 5. Diab etes −0.08* −0.08 0.10* 0.16* – 6. HbA1c −0.09 −0.14 * 0.12* 0.17* 0.57* – 7. Age −0.19 * −0.25* 0.02 0.25* 0.16* 0.18* – 8. Sex 0.04 −0.07 0.10 * 0.04 −0.06 0.01 −0.03 – 9. Ethn icity 0.03 −0.06 0.04 0.04 0.05 0.07 −0.11 * 0.02 – 10 .Bodymassindex −0.0 1 −0.06 0.12 * 0.31 * 0.18 * 0.19 * −0.05 −0.0 7* 0.06 – 11. Smok ingH istory −0.04 −0.05 0.11* 0.07 0.05 0.03 0.11* −0.08* 0.03 0.02 – 12. Currenti nsulinu se −0.10 * −0.11 * 0.10* 0.10 * 0.59 * 0.38 * 0.09* −0.06 0.02 0.20 * −0.01 – 13. Timelag 0.07* 0.13* −0.03 0.09* −0.11 * −0.12 * −0.04 0.12* 0.01 −0.09 * −0.06 −0.11* – 14. Digit spa n 0.23* 0.18* −0.08 * −0.07 * −0.09* −0.06 −0.15 * 0.05 −0.0 3 −0.08* 0.07* −0.08* 0.09* – 15. Backw ards counting 0.37* 0.41* −0.06 −0.13* −0.11* −0.09 * −0.38* −0.1 1* −0.06 −0.05 −0.07 * −0.07 0.08* 0.28* – 16. Numberse ries 0.24* 0.27* −0.15 * −0.10* −0.13* −0.13* −0.21* −0.09* −0.11 * −0.02 −0.05 −0.09 * 0.05 0.32* 0.40* Note.Pearsoncorrelationsarepresentedforcorrelationsbetweencontinuousvariables;Spearman’scoefficientsarepresentedforcategoricalvariables.AA=anxiousarousal; IL–6=interleukin6.Participantgendercodedas1=maleand2=female.Participantethnicitycodedas0=non-whiteand1=white.Smokinghistorycodedas0=neversmoked cigarettesregularlyand1=havesmokedcigarettesregularly.Currentinsulinusecodedas0=noand1=yes.*p<0.05. and analyses below, is determined by the quotient of HA1C by oncognitivemeasuresassociatedwithagingthatisseparate,but totalhemoglobin.Higherscoresrepresentworseglycemiccontrol. related,toinhibition(e.g.,Baudouinetal.,2009). ConsistentwiththeInternationalExpertCommittee’ssuggestions for using HbA1c to diagnose diabetes (The International Expert 2.2.8. Numberseriestask Committee,2009),scoresabove6.5%wereconsideredtobecon- Participantscompletedanumberseriestask(SalthouseandPrill, sistent with a diagnosis of diabetes; however, the committee 1987)whichwasutilizedasacovariate.Forthistask,participants suggestedthatarepeatmeasurementofHbA1cisneededfordiag- werepresentedfive-numberseries,oneatatime,andwereasked nosis of diabetes if clinical symptoms and blood glucose levels toindicatethecorrectnumberthatshouldappearnextintheseries. below200mg/dl(11.1mmol/l)areidentified.Asecondmeasure- Total scores reflected the number of series completed correctly mentwasnotconductedforsuchindividualsinthepresentstudy. after a five trials. It has been argued that measures of fluid rea- In the analyses described below, diabetes incidence was defined soning,suchasnumberseriestasks,arerelatedtothemajorityof aswhetherornotparticipantsdemonstratedHbA1clevelsgreater measuresofexecutivefunctioningandintelligence(e.g.,Unsworth than 6.5% and/or self-reported using medication to manage dia- etal.,2009).Asaresult,thismeasurewaschosenasacovariate betes. todetermineifbroadcognitiveskillsexplainhypothesizedassoci- ations.Thisisimportantgiventhatanxietysymptomsassociated 2.2.5. Demographics withpost-traumaticstresshavebeenfoundtobespecifictoinhi- Participantsprovidedself-reportedage,sex,ethnicity,smoking bitionasopposedtogeneralexecutivedysfunction(DeGutisetal., history,andcurrentuseofinsulin.Participantheightandweight 2015). wasmeasuredinordertocalculatebodymassindex(BMI). 2.3. Analyticstrategy 2.2.6. Digitspan ThebackwarddigitspantaskfromtheWechslerAdultIntelli- SPSSstatisticalsoftware(IBM,2012)wasutilizedforallanal- genceScale,ThirdEdition(WAIS-III;Wechsler,1997)wasalsoused yses.Moreover,themodelrepresentedinFig.1wastestedusing asacovariateinthepresentstudy.Thedigitspantaskinvolvedthe thePROCESSmacroforSPSS(Hayes,2013)whichallowsforeval- participant listening to a series of numbers ranging from two to uation of serial mediation. Indirect effects were evaluated using eight digits that increased in length as they progressed through 5000bootstrapsamples.Anindirecteffectissignificantifthe95% thetrials.Afterlisteningtotheseriesofnumbers,theparticipants confidence interval does not contain zero (Hayes, 2013). Media- wereaskedtorepeateachseriesinthereverseorder.Participants tionmodelsreflectthatonevariable(i.e.,themediator)explains, weregiventwoseparateopportunities,usingadifferentorderof orpartiallyexplains,anassociationbetweenanindependentand digits,toprovidethecorrectresponseforagivenserieslength.The dependent variable. Of note, mediation models can be tested taskwasdiscontinuediftheparticipantdidnotprovidethecorrect without longitudinal data if hypotheses are theoretically driven responsetoatrialaftertwoattemptsforagivenserieslength.The (MacKinnon,2008).Furthermore,inserialmediationmodels,itis numberofdigitsinthelongestseriescorrectlyrecalledwasuti- hypothesizedthatonemediatorisseriallyassociatedwithanother lizedasanindicatorofdigitspanability.Thebackwarddigitspan taskwaschosenasacovariateinthepresentstudyasitisrelated Table3 totheexecutivefunctionofupdating/monitoringofinformationin Logist icregressionanalysespredictingdiabetesincidence. wo rki ngmemor y(Hilber te tal.,2015). Variable Model1 Model2 Model3 2.2.7. Backwardscountingtask Inhibition −0.11 −0.01 −0.04 AnxiousArousal 0.08 0.07 0.04 For30s,participantswereaskedtocountbackwardsfrom100 Interleukin-6 0.44* 0.26* 0.42* asquicklyaspossible.Thenumberofcorrectresponseswasuti- liz edasan ind icatorof proc essingsp ee d,acova riateinthe pre sent Note. Values represent logistic regression coefficients (i.e., odds ratios). Model 1=unadjusted.Model2=adjustedforage,sex,ethnicity,bodymassindex,smok- study.Thenumberoferrorsduetorepeatingorskippingnumbers wassu btra ctedfrom t hetota lsco re .Thismea su rewasch osenasa i3n=g ahdijsutostreyd, afonrd ptehref otirmmea nlacge boentwdiegeitns cpoagnn,ibtaivcek wanadrd bsiocloougnictianl gasasnedssnmuemnbtse.r Mseordieesl covariategiventhatprocessingspeedisapredictorofperformance tasks.*p<0.05 106 K.W.Murdocketal./Psychoneuroendocrinology71(2016)102–109 .10* (.03, .17) Anxious Arousal Interleukin-6 -.12* (-.05, -.18) .06* (.01, .12) -.01 (-.07, .04) -.08* (-.01, -.15) .02 (-.03, .08) Inhibition HbA1c Percentage Fig.2. Amediationmodelofassociationsbetweeninhibition,anxiousarousal,interleukin-6,andHbA1c.Valuesrepresentstandardizedregressioncoefficientsand95% confi de nc eintervals aredep ict edinparenth eses.Ind irecteffects using50 00boots trapsamples: anxi ousarou sal(−0 .0015,SE= 0.0038,95%CI =−0.0111, 0.0047),inte rleu kin- 6(.0049,SE=0.0034,95%CI=0.0005,0.0154),andserialmediation(i.e.,mediationinsequence;0.0007,SE=0.0006,95%CI=0.0001,0.0028).Controlvariablesincluded participantage,sex,ethnicity,bodymassindex,smokinghistory,insulinuse,aswellthetimelagbetweenassessments.*p<0.05. mediator, and that this chain explains, or partially explains, an inhibition.Allsignificantpaths,aswellasindirecteffects,remained. associationbetweenanindependentanddependentvariable(e.g., Moreover,betternumberseriesperformancewasassociatedwith Hayes,2012 ).Import ant ly,thePROCE SSm acroautom aticallyi den- lower anx ious ar ousal ((cid:3) =−0.1 3, p<0.05) a nd d ecreased l ikeli- tifiesd ichotom ousdepend ent variables, sucha sdiabetesincid ence hoodo fmeetin gcriteria for diabete s (B =−0. 35,p <0.05);ho wever, in the present study, and utilizes logistic regression. Participant further analysis revealed that number series performance was age,sex,ethnicity,BMI,smokinghistory,andthetimelagbetween not associated with diabetes incidence through anxious arousal asse ssme ntswere utiliz edasco variates. Add itio nally ,pa rticipant (−0 .0082,SE=0 .0163 ;95%CI= −0.0434, 0.0224)o rIL-6(− 0.0113, performance onth ecognit ive tasksrepre sentingdigit span,back- SE=0.0122 ;9 5 %CI=−0 .045 2, 0. 0051).Mo reover,i nh ibitio nwasthe wardscounting,andnumberserieswereenteredascovariatesin onlycognitiveskilldirectlyassociatedwithIL-6. follow-upanalyses. 4. Discussion 3. Results Ourfindingsindicatethatthosewithbetterinhibitionevidence Descriptive statistics are presented in Table 1 and bivariate lower anxious arousal, IL-6, and HbA1c, in addition to a lower correlations are presented in Table 2. As expected, better inhi- likelihood of meeting criteria for diabetes, than those with poor bition was associated with less anxious arousal, IL-6, diabetes inhibition. Additionally, those with higher anxious arousal had incidence,andHbA1c.Moreover,allindicatorsofcognitiveability higher IL-6. As expected, higher IL-6 was associated with higher weresignificantlypositivelyassociated.Furthermore,inlinewith HbA1candlikelihoodofdiabetesincidence.Inthefullmodel(see hypotheses,higheranxiousarousalwasassociatedwithgreaterIL- Fig. 1), poor inhibition was associated with increased diabetes 6.Asexpected,higherIL-6wasassociatedwithagreaterlikelihood incidencethroughtheserialpathwayfromanxiousarousaltoIl- of diabetes incidence and higher HbA1c. Interestingly, increased 6 as hypothesized. These findings were unique to inhibition as anxiousarousalwasassociatedwithahigherBMIandlikelihood outcomesdidnotchangewhenotherindicatorsofcognitiveabil- of reporting a history of regular cigarette use. Moreover, greater itywereincludedinthemodel.Findingsextendtheliteratureby IL-6wasassociatedwithhigherBMI,andworseperformanceonall demonstratingthatlowinhibitionisariskfactorfordiabetesinci- measuresofcognitiveability. dence as opposed to being a consequence of disease processes AsseeninFig.1,lowerinhibitionwasassociatedwithgreater (e.g.,Bottirolietal.,2014;Tranetal.,2014).Betternumberseries anxious arousal and plasma IL-6. Higher anxious arousal was performance was independently associated with lower anxious also associated with greater IL-6. Furthermore, serial mediation arousalanddecreasedlikelihoodofmeetingcriteriafordiabetes, wassupported,indicatingthatthesequentialpathwayfromanx- suggestingthatnumberseriesperformanceandinhibitionshould iousarousaltoIL-6explainedtheassociationbetweeninhibition bedifferentiatedwithinmodelsofdiabetesincidence. and diabete s i ncide nce. Logis tic regression analyses predicting Parasympathe tic ner vous sy st em and NF-(cid:4)B activation are diabetes incidence are presented in Table 3. Covariates signifi- potentialmechanismslinkinginhibitionwithanxiousarousaland cantlyassociatedwithdiabetesincidenceincludedparticipantage inflammation.Indeed,thosewithpoorinhibitionaremorelikely (B=0.53,p<0.05)andBMI(B=0.54,p<0.05),aswellasthetime tohavestressfulthoughtsenterandcontinuetooccupyworking lag betw ee n asses sme nttim e p oints (B =−0.2 8,p <0.0 5) .Pri mary me mory thantho sewithb etteri nhib ition(Joo rm an,2010 ).More- findingsremainedconsistentwhenexaminingHbA1casacontin- over, those with poor inhibition are more likely to demonstrate uousdependentvariablewithinsulinuseincludedasacovariate maladaptivephysiologicalandpsychologicalresponsestostress- (Fig. 2), in addition to when adding the number of errors made orsthanthosewithbetterinhibition(Lackschewitzetal.,2008). duringthereverseandmixedtasksasadditionalindicatorsofinhi- Therefore,asaresultofbeingunabletoblockstressfulthoughts bition.Furthermore,serialmediationwasnotsupportedwhenthe frombeingattendedto,andaninabilitytoshiftattentionawayfrom sequencewasreversedsuchthatIL-6ledtoanxiousarousal(.0013, distressingthoughts,thosewithpoorinhibitionmaybemorelikely SE=0.001 3;95 %CI=−0 .0005 ,0.00 54) .We al soexam inedifd iabetes toexperien ceanxious arous alan ddem onstrate heigh te nedin flam- incidencewasassociatedwithinflammationthroughthepathway mationwhenexposedtostressorsthanthosewithbetterinhibition. fromanxiousarousaltoinhibitiongiventhatmanagementofdia- Althoughinhibitionisahypothesizedprecursortoanxiousarousal betes is associated with potentially anxiety providing situations andinflammation,furtherresearchisneededtoevaluateifinhi- (DukeandHarris,2014).Resultsdidnotsupportthisserialmedia- bitionisassociatedwithageneralarousalsystemasopposedto tional path way(0 .0004,S E=0.00 06; 95% CI=−0. 0001 ,0.00 27). being ap recursorto anxi ou sarousa landin flamma tio ngiventh is Infollow-upanalyses,digitspan,backwardscountingandnum- speculativehypothesis. berseriesperformancewereexaminedascovariatesinthemodel Maladaptive health behaviors associated with poor inhibition depictedinFig.1todetermineifprimaryfindingswereuniqueto mayalsoexplaintheassociationbetweeninhibitionanddiabetes. K.W.Murdocketal./Psychoneuroendocrinology71(2016)102–109 107 Indeed,individualswithpoorinhibitionarelesslikelytoeathealthy etal.,2014),supportingpresentstudyfindings.Moreover,asstudy foods (Limbers and Young, 2015; Segerstrom and Nes, 2007) or variableswerenotassessedovermultipletimepoints,directional- engage in healthy amounts of physical activity than those with ityofassociationscannotbedetermined.Longitudinaldesignscan highinhibition,evenwhentheyhavetheintentionofdoingso(Hall addressthislimitationinfuturework. etal.,2008).Thosewithpoorinhibitionarelesslikelytoconsume fruits/vegetables(AllomandMullan,2014),adheretoaweightloss 5. Conclusions plan(Pauli-Pottetal.,2010),utilizesunscreen(Allometal.,2013), or demonstrate adaptive sleeping habits than those with better Consistent with theoretical models linking inhibition, stress, inhibition(KorandMullan,2011).Impairedinhibitionalsoleads andhealth,poorinhibitionisassociatedwithincreaseddiabetes to alcohol relapse following treatment (Garland et al., 2012). As incidencethroughtheserialpathwayfromhighanxiousarousalto highanxietyandpoorhealthbehaviorsareknownriskfactorsfor highinflammation.Thesefindingshaveimportantimplicationsfor type2diabetes(Lietal.,2008;WHO,2014),futureworkshouldtar- thepreventionandtreatmentofdiabetesbyidentifyingunderlying gethealthbehaviorsasanunderlyingmechanismlinkinginhibition mechanismscontributingtoelevatedbloodglucose. withtype2diabetes. Findings point to several intervention opportunities that Contributors may reduce diabetes incidence. Mindfulness-based therapeutic techniquescanimproveneuralnetworksassociatedwithpoorinhi- K.W.M was involved in data analysis and manuscript writing bition, such as in the an terior cingulate cortex (AC C; G ard e t al., forthepre sent study.A. S.L ,T.E.L .,D.C.D, C.J.H ,andC.P.F.p rovided 2012) which fa cil itate sexecuti veattenti onbyd etecti ngand m it- crit ical feedbac kande dited them anuscr ipt. igating distra cting tho ughts (Van Veen an d Carter, 20 02). Low inhibitionisalsoimprovedviastimulantmedication(Roschetal., Roleofthefundingsource 2015). Anxious arousal is reduced through cognitive behavioral therapy,andinparticular,exposureandresponseprevention(Arch DatacollectionforthepresentstudywasfundedbytheNational etal.,2013).Useofanti-inflammatorymedicationmayalsoreduce InstituteonAging(P01-AG020166).Preparationofthemanuscript riskofdiabetesgivenpresentstudyfindings(Serhanetal.,2008). wassupportedbyagrantfromtheNationalHeart,Lung,andBlood Further research is needed to determine if implementing such Institute(1R01HL127260-01)toC.P.F. interventions can reduce diabetes incidence among at risk indi- viduals. References Inhibition,anxiousarousal,andinflammationarealsoimpor- tantfordiabetesmanagement.Individualswithlowinhibitionare Allom,V.,Mullan,B.,2014.Individualdifferencesinexecutivefunctionpredict at ri sk f or poor glycemic cont rol leading to en hanc ed inhibit ion dis tin cteating be havio urs.Appeti te80,123–1 30 ,http://dx .doi.org/ 10.1016/j. di fficul ties (Duk e and Ha rris, 201 4; Gailli ot et al., 2007 ). 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