Downloaded from http://bjo.bmj.com/ on April 27, 2015 - Published by group.bmj.com 1186 BrJOphthalmol1999;83:1186–1189 Influence of highly active antiretroviral therapy on the development of CMV disease in HIV positive patients at high risk for CMV disease FrankDVerbraak,RenéBoom,PaulineMEWertheim-vanDillen, GerardusJvandenHorn,AizeKijlstra,MarcDdeSmet Abstract Conclusion—In HIV positive patients at Background/aims—In the pre-HAART high risk of CMV retinitis, either with a era,HIV positive patients with CD4+ cell positive CMV PCR assay in blood and/or countsbelow50cells·10 6/l,andthosewith withCD4+cellcountsbelow50cell·10 6/l, detectable cytomegalovirus (CMV) DNA HAARTcausesadramaticdecreaseinthe intheirperipheralblood,wereconsidered occurrenceofCMVdisease.Thisdecrease to be at high risk for the development of is paralleled by an increase in CD4+ cell CMV disease. With the start of highly count, and a decrease in the amount of active antiretroviral therapy (HAART), a CMV DNA in the blood,which was below restoration of immune function occurred detection levels in all patients with CD4+ in these patients, and as a consequence cellcountsabove100cells·10 6/l. patients became less vulnerable to CMV (BrJOphthalmol1999;83:1186–1189) disease.Sinceitisnotexactlyknownhow HAART influences CMV viral load in peripheral blood and the incidence of The presence of cytomegalovirus (CMV) CMV disease in high risk HIV positive DNAeitherinwholebloodorincellfreesam- patients a group of patients was followed ples has been recognised as an important risk beforeandafterinitiationofHAART. factor,inadditiontolowCD4+cellcounts,for Methods—29 HIV positive patients, seen thedevelopmentofclinicalmanifestCMVdis- in the first 3 months of 1996 at the AIDS easeinHIVpositivepatients.Studiesonserum Departmentof clinicoftheAcademicMedicalCentre,at or plasma samples reported useful statistical Ophthalmology, highriskfordevelopmentofCMVdisease variables for CMV DNA polymerase chain AcademicMedical Centre,Universityof (positiveCMVDNAassayinbloodand/or reaction(PCR)assaysinpredictingCMVdis- Amsterdam, CD4+cellcountbelow50cells·10 6/l),not ease (sensitivity between 75% and 90%; Amsterdam, receivinganti-CMVmaintenancetherapy, specificity between 60% and 85%; positive Netherlands were included in a prospective cohort predictivevaluebetween60and70%;negative FDVerbraak study. HAART was started in the second predictive value between 80 and 98%).1–6 The GJvandenHorn AKijlstra trimesterof1996.Patientswereevaluated overall incidence of CMV retinitis in these MDdeSmet for the occurrence of CMV retinitis, or studiesduringafollowupperiodof12months CMV disease elsewhere, comparing the was between 25% and 35%. Spector et al Laboratoryof incidenceofCMVeventsbeforeandafter reporteda12monthKaplan–MeierCMVdis- Microbiology, the start of HAART. Following the intro- easeeventrateof14%inPCRCMVnegative Departmentof ductionofHAART,CD4+cellcountsand patients and of 43% in the PCR positive Virology,Academic MedicalCentre, quantitative polymerase chain reaction patients,correspondingtoa3.4-foldincreased Universityof (PCR)forCMVDNAinbloodweremoni- risk of developing CMV disease.In over 90% Amsterdam, tored in all patients who remained alive of cases CMV disease manifested itself as Amsterdam, andwerenotreceivinganti-CMVmainte- retinitis.2 Netherlands nancetherapy(n=22).Followupwasper- The use of antiretroviral combination RBoom PMEWertheim-van formeduntilAugust1998;themeanfollow therapy—for example, triple threrapy consist- Dillen up after the start of HAART was 14.9 ing of two reverse transcriptase inhibitors and months(range8–22months). one protease inhibitor, often called highly Departmentof Results—In the pre-HAART period four active antiretroviral therapy (HAART), has Ophthalmo-Immunology,patientsdevelopedCMVdisease,andfour resultedinadramaticchangeinthemorbidity theNetherlands died (without clinically manifest CMV associated with HIV. A significant decline in OphthalmicResearch Institute,Amsterdam, disease). After the start of HAART no the incidence of CMV disease has been Netherlands patient developed CMV disease or died. reportedinpatientsreceivingthiscombination AKijlstra WithHAART,themeanCD4+cellcounts antiretroviral therapy.78 Van den Horn et al increased from 34 cells ·10 6/l to 194 cells reported that patients with CMV retinitis CFroarnrkesDpoVnedrebnrcaeakto,:University ·10 6/l at the end of follow up. CMV DNA treated with HAART showed no recurrences ofAmsterdam,Academic could be detected in the blood of 11 duringafollowupperiodof42–52weekspro- MedicalCentre,Department patients.Quantification showed a decline vided the CD4+ cell counts remained above oGf2O–2p4h5th,aPlOmoBloogxy2,2R7o0o0m, in the amount of detectable DNA during 100 cells ·10 6/l.9 HAART induces a rapid 1100DEAmsterdam, followup.Atthelastexaminationonlyone redistribution and eventually a restoration of Netherlands. patientshowedapositivePCRassay.This the immune system, and as a result, patients, was the only patient with a CD4+ cell normallyexpectedtobeathighriskfordevel- Acceptedforpublication 24May1999 countremainingbelow100cells·10 6/l. oping CMV retinitis or recurrences of already Downloaded from http://bjo.bmj.com/ on April 27, 2015 - Published by group.bmj.com InfluenceofHAARTonthedevelopmentofCMVdiseaseinHIVpositivepatients 1187 Table1 EVectofHAARTonoccurrenceofCMVeventsandsurvivalinHIVpositivepatientsathighriskfordeveloping CMVdisease BeforeHAART(n=29) AfterHAART(n=22) PCR+ PCR− Timetoeventor PCR+ PCR− (n=16) (n=13) death(months)* (n=10) (n=12) CMVevents(n) 4 — 0.5,2,2,3 — — Death(n) 3 1 1,2,2,4 — — Living,withoutanti-CMVmaintenancetherapy(n) 10 12 — 7 11 Meanfollowup(months) 5.0† 14.9‡ HAART=highlyactiveantiretroviraltherapy;PCR=polymerasechainreaction;+=positiveresult,−=negativeresult;*time betweenstartofstudyandoccurrenceofevent/death;†meanfollowupbetweenstartofstudyandstartofHAART;‡meanfollow upfollowingstartofHAART. present CMV retinitis, are again able to neuropathy. Additionally at each visit, the suppressactiveCMVinfection. treating physician from the department of Since it is not known exactly how HAART internalmedicinereceivedaquestionnaireand influencesCMVviralloadinperipheralblood wasexplicitlyaskedforanysignsofextraocular or the incidence of CMV disease in high risk CMV disease. CD4+ cell counts were per- HIV positive patients, we assessed a group of formedeverythirdmonth. patientsbeforeandafterthestartofHAART. PCRANALYSIS Patientsandmethods CMV DNA was purified from 50 µl EDTA PATIENTSELECTION bloodspecimenstogetherwith70moleculesof Patients were selected from a group of 100 internal control (IC) DNA as described previ- consecutive HIV positive patients seen in ously, using 20 µl of size fractionated silica MarchandApril1996attheAIDSclinicofthe particles.10DNAwaselutedin100µlTEbuVer AcademicMedicalCenteroftheUniversityof (10 mM TRIS,1 mM EDTA,pH 8.0).CMV Amsterdam. Eligible patients either tested DNA levels in blood were determined as positiveforCMVPCRinblood(n=18),orhad describedpreviously(BoomR,SolC,WeelJ,et a CD4+ count below 50 cells ·10 6/l (n=15). al. A highly sensitive assay for detection and WithtwoexceptionsallPCRpositivepatients quantificationofhumancytomegalovirusDNA hadaCD4+countbelow50cells·10 6/l.Four in serum and plasma by PCR and electro- patients refused to participate. All other chemiluminescence,submitted).Inshort,puri- patients (n=29) underwent a full ophthalmo- fied DNA (25 µl) was subjected to a 35 cycle logical examination, including funduscopy in PCRwithasingleprimerpairwhichamplifiesa mydriasisatbaseline. 578bpDNAfragmentfromexon4ofthemajor ACMVeventcouldbeeitheraCMVretini- immediateearlygeneofCMVandafragmentof tis,definedasanecrotisingretinitiswithchar- identical size and GC content from IC DNA. acteristic “cheese-like” appearance with or The amounts of CMV and IC PCR products without haemorrhages, as observed by an were subsequently determined by electro- experienced ophthalmologist, or extraocular chemiluminescence (ECL) in the QPCR Sys- CMVdisease,forwhichdiagnosisimmunohis- tem 5000 (Perkin Elmer) after hybridisation tologicalproofhadtobepresent. with (TRIS (2,2'-bipyridine) ruthenium (II) BeforethestartofHAARTfourpatientsdied chelate) (TBR) labelled probes specific for without clinically manifest CMV disease, after either CMV or IC amplimers. The viral load 4,7,9,and15weeksrespectively.Themeanfol- (expressedascopiesCMV/mlblood)wascalcu- low up period for the other patients from the latedfromtheratio(R)ofCMVoverICECL startofthestudytothestartofHAARTwas5 signals (after background correction) by the months (range 4–6 months). All patients were algorithm“copiesCMV/mlblood=R· 1400”. givenHAARTinthesecondtrimesterof1996. HAART consisted of triple therapy, using a STATISTICALANALYSIS combinationoftworeversetranscriptaseinhibi- ForstatisticalanalysiswecomparedtheCMV torsandoneproteaseinhibitor. eventrate,duringfollowupbeforethestartof ThreepatientsdevelopedCMVretinitisand HAART, with CMV event rate following the received anti-CMV maintenance therapy. start of HAART, using the Kaplan–Meier Thesepatientswereexcludedfromfurtherfol- methodandthelogranktest.11 low up. Mean follow up after the start of HAART for those patients not receiving Results anti-CMV maintenance therapy (n= 22), was Fourpatients,allbelongingtotheCMVPCR 14.9months(range8–22months). positive patient group, developed a clinically BetweenNovember1996andJuly1998the manifest CMV disease in the pre-HAART 22 patients without anti-CMV maintenance period, after 1, 7, 9, and 12 weeks. Three therapy underwent a full ophthalmological patients were diagnosed with a CMV retinitis examination,includingfunduscopyinmydria- andallwereputonmaintenancetherapyafter sis,everymonthduringthefirst6months,and successful induction therapy. One patient every other month during the remaining part developedaCMVcolitisandonlyreceiveda3 of follow up.At the same time blood samples week induction therapy. Additionally, four were taken for quantitative PCR analysis. At patientsdiedbeforethestartofHAART,with- each visit patients were asked for complaints outclinicallymanifestCMVdisease,after4,7, related to oesophagitis, colitis, pneumonia, or 8,and17weeksrespectively(Table1). Downloaded from http://bjo.bmj.com/ on April 27, 2015 - Published by group.bmj.com 1188 Verbraak,Boom,Wertheim-vanDillen,etal Table2 EVectofHAARTonCD4+cellcountsandCMVviralloadin22HIVpositivepatients,withoutanti-CMVmaintenancetherapy,athighrisk fordevelopingCMVdisease BeforeHAART AfterHAART Lastexam Exam0 Exam1 Exam2 Exam3 Exam4 Exam5 Exam6 Exam7 Patient Aftern No CD4+ PCR CD4+ PCR PCR PCR CD4+ PCR PCR PCR CD4+ PCR months PCR CD4+ 1 10 1469 70 — — — 110 — — — 230 — 18 — 130 2 150 914 150 — — — 140 — — — 180 — 18 — 150 3 20 1136 210 — — — 250 — — — 250 — 12 — 170 4 20 562 90 — — — 220 — — — ND — 9 — 460 5 40 1529 160 — — — 130 — — 171 140 — 18 — 170 6 40 382 30 2071 1474 ND ND ND ND ND 100 — 12 — 100 7 40 2355 100 — — 376 150 584 — — 170 — 16# — 180 8 90 1259 170 384 — — 200 — — — 190 — 22 — 200 9* 30 1423 90 — — 947 100 — ND ND ND ND 13 — 100 10* 20 604 140 133 — — 200 — — — 200 — 16 — 200 11 30 — 10 — — 237 ND ND — — ND ND 12 — 180 12 20 — 60 6488 1464 — 130 534 602 — 140 — 13 — 120 13 20 — 30 — 186 875 40 — 346 — 20 — 16 727 60 14 10 — 110 — — — 260 — — — 170 — 16* — 340 15 20 — 60 — — — 90 — — — 80 — 17 — 250 16 50 — 190 — ND ND 130 — ND ND ND ND 9 — 130 17 30 — 70 — — — 150 — — — 170 — 16 — 110 18 10 — 230 — — — 60 — — — 170 — 18 — 250 19 10 — 80 — — ND 100 — — — 130 — 13 — 190 20 30 — 140 — — ND ND ND ND ND ND 8 — 140 21 30 — 50 — — — 80 — — — ND — 14 — 130 22* 30 — 120 — — — 190 — 148 — 400 — 22 — 500 CD4+=CD4+cellcount(cells· 106/l);HAART=highlyactiveantiretroviraltherapy;PCR=quantitativepolymerasechainreaction,incopiesCMV·10 6/ml;−= negativeresult;ND=notdone;exam0=firstexamination,atintake,beforethestartofHAART;exam1–7=examinations,monthly,afterthestartofHAART.After the7thexamination,followupscheduledeveryothermonth,resultsnotshown.*Patient9,10,and22previousdiagnosisofextraocularCMVdisease.;†patient7one positivetest12monthsafterstartHAART(280copies/ml);‡patient14onepositivetest14monthsafterstartHAART(98copies/ml);lastexamafternmonths= lastexaminationofthepatientatnmonthsafterthestartofHAART. Following the start of HAART none of the Discussion 22 patients not receiving anti-CMV mainte- In this study we present data showing that in nance treatment developed clinically manifest 22 patients, previously considered to be at CMVdiseaseduringameanfollowupof14.9 extremely high risk for developing CMV months (range 8–22 months), and none of disease, not one new case of CMV disease thesepatientsdied. manifested itself during a mean follow up of Statistical analysis comparing the incidence 14.9months(range8–22months). ofCMVdiseaseinpatientsbeforeandafterthe HAARTresultedinagradualriseinCD4+ start of HAART using the Kaplan–Meier lymphocyte counts and a gradual drop in method and the log rank test resulted in a p CMVviralloadintheperipheralblood.Atthe valueof0.05. lastexaminationCMVDNAbecameundetec- MostpatientsrespondedtoHAARTwitha table,withtheexceptionofonepatientwhose steady increase in their CD4+ cell counts CD4+cellcountremainedlessthan100cells (Table 2). The mean CD4 positive count ·10 6/l.Nopatientdiedduringfollowup. increased from 32 cells ·10 6/l (range 10–150) ComparingtheincidenceofCMVdiseasein at the start of follow up, through 144 cells the patients before and after the start of ·10 6/l (range 40 to 260) halfway, to 194 cells HAART,usingtheKaplan–Meiermethodwith ·10 6/l (range 60–500) at the last examination. the log rank test, we found a statistically With the exception of one patient (patient significant, albeit weak, diVerence between number 13), all CD4+ cell counts were over bothobservationperiods(p=0.05).Aplacebo 100cells·10 6/latthelastexamination. controlledtrial(withholdingHAARTtothese In eight patients a positive CMV PCR test patients)wasconsideredtobeunethical. wasobtainedduringfollowupafterthestartof Patients with a history of extraocular CMV HAART(Table2).QuantificationofthePCR disease have been reported to be especially testshowedadecreaseoftheamountofCMV pronetothesubsequentdevelopmentofCMV DNA detectable in the peripheral blood of all retinitis.Over85%ofthesepatientsdeveloped these patients. At the seventh examination, a CMV retinitis after a mean follow up of 6.4 longest follow up 10 months after the start of months.12Notoneofthethreepatients(patient HAART, none of the tested patients had nos 9,10,and 22,Table 2) in this study with detectable CMV DNA in their blood. How- gastrointestinalCMVdiseasedevelopedCMV ever,inpatient7,12monthsfollowingstartof retinitis during follow up after the start of HAART, 280 CMV copies/ml could be HAART. measured, and in patient 14, 14 months The fact that no clinically manifest CMV following the start of HAART, 98 CMV diseaseoccurredinourgroupofHIVpositive copies/ml could be detected (not shown in patientscanonlybeexplainedbythesuccessof Table2).Atthelastexamination,afteramean the HAART treatment. Others have also follow up of 14.9 months, only one patient reportedthedecreasedincidenceofCMVdis- (number13)testedpositive,withaCMVviral ease in HIV positive patients with favourable load of 727 copies/ml.This was also the only responses to HAART treatment.7–9 The de- patient with a CD4+ cell count less than 100 crease of CMV viral load found in this study cells·10 6/l. confirmstherestorationoftheimmunesystem, Downloaded from http://bjo.bmj.com/ on April 27, 2015 - Published by group.bmj.com InfluenceofHAARTonthedevelopmentofCMVdiseaseinHIVpositivepatients 1189 enabling the patients to successfully suppress This decrease is paralleled by an increase in reactivationfromtheirlatentCMVinfection. CD4+lymphocytecount,andadecreaseinthe All four patients with clinically manifest amount of CMV DNA in the blood, which CMV disease in the pre-HAART period becomes undetectable in all patients with belongedtothegroupofpatientswithaCMV CD4+cellcountsabove100cells·10 6/l. 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Downloaded from http://bjo.bmj.com/ on April 27, 2015 - Published by group.bmj.com Influence of highly active antiretroviral therapy on the development of CMV disease in HIV positive patients at high risk for CMV disease Frank D Verbraak, René Boom, Pauline M E Wertheim-van Dillen, Gerardus J van den Horn, Aize Kijlstra and Marc D de Smet Br J Ophthalmol 1999 83: 1186-1189 doi: 10.1136/bjo.83.10.1186 Updated information and services can be found at: http://bjo.bmj.com/content/83/10/1186 These include: References This article cites 13 articles, 6 of which you can access for free at: http://bjo.bmj.com/content/83/10/1186#BIBL Email alerting Receive free email alerts when new articles cite this article. Sign up in the service box at the top right corner of the online article. 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