<?xml version="1.0" encoding="ISO-8859-1"?><article xmlns:mml="http://www.w3.org/1998/Math/MathML" xmlns:xlink="http://www.w3.org/1999/xlink" xmlns:xsi="http://www.w3.org/2001/XMLSchema-instance">
<front>
<journal-meta>
<journal-id>0256-9574</journal-id>
<journal-title><![CDATA[SAMJ: South African Medical Journal]]></journal-title>
<abbrev-journal-title><![CDATA[SAMJ, S. Afr. med. j.]]></abbrev-journal-title>
<issn>0256-9574</issn>
<publisher>
<publisher-name><![CDATA[Health and Medical Publishing Group]]></publisher-name>
</publisher>
</journal-meta>
<article-meta>
<article-id>S0256-95742012000800024</article-id>
<title-group>
<article-title xml:lang="en"><![CDATA[Profile of cause of death assigned to adults on antiretroviral therapy in Soweto]]></article-title>
</title-group>
<contrib-group>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Karstaedt]]></surname>
<given-names><![CDATA[A S]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
</contrib-group>
<aff id="A01">
<institution><![CDATA[,University of the Witwatersrand Chris Hani Baragwanath Hospital Department of Medicine]]></institution>
<addr-line><![CDATA[Johannesburg ]]></addr-line>
</aff>
<pub-date pub-type="pub">
<day>00</day>
<month>08</month>
<year>2012</year>
</pub-date>
<pub-date pub-type="epub">
<day>00</day>
<month>08</month>
<year>2012</year>
</pub-date>
<volume>102</volume>
<numero>8</numero>
<fpage>680</fpage>
<lpage>682</lpage>
<copyright-statement/>
<copyright-year/>
<self-uri xlink:href="http://www.scielo.org.za/scielo.php?script=sci_arttext&amp;pid=S0256-95742012000800024&amp;lng=en&amp;nrm=iso&amp;tlng=en"></self-uri><self-uri xlink:href="http://www.scielo.org.za/scielo.php?script=sci_abstract&amp;pid=S0256-95742012000800024&amp;lng=en&amp;nrm=iso&amp;tlng=en"></self-uri><self-uri xlink:href="http://www.scielo.org.za/scielo.php?script=sci_pdf&amp;pid=S0256-95742012000800024&amp;lng=en&amp;nrm=iso&amp;tlng=en"></self-uri><abstract abstract-type="short" xml:lang="en"><p><![CDATA[This retrospective cohort study describes causes of death in 305 patients (baseline median CD4 count from 2 943 adults on antiretroviral therapy. Acute sepsis (20%), tuberculosis (18%) and Mycobacterium avium complex (MAC) bacteraemia (14%) were the most common causes. Mortality owing to the disease was 66% for MAC bacteraemia and 23% for non-Hodgkin's lymphoma. In 37 patients dying beyond one year on ART, virological failure was present in 11 (30%), and non-HIV-related causes of death occurred in 10. The main causes were acute sepsis (6), tuberculosis (7) and chronic medical conditions (5). Initiating ART at higher CD4 counts should reduce early mortality.]]></p></abstract>
</article-meta>
</front><body><![CDATA[ <p align="right"><font face="Verdana, Arial, Helvetica, sans-serif" size="2"><b>RESEARCH</b></font></p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="4"><b><a name="top"></a>Profile    of cause of death assigned to adults on antiretroviral therapy in Soweto</b></font></p>     <p>&nbsp;</p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2"><b>A S Karstaedt</b></font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">MB BCh, M Med.    Division of Infectious Diseases, Department of Medicine, Chris Hani Baragwanath    Hospital and University of the Witwatersrand, Johannesburg </font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2"><a href="#back">Correspondence    to</a></font> </p>     <p>&nbsp;</p>     <p>&nbsp;</p> <hr size="1" noshade>     ]]></body>
<body><![CDATA[<p><font face="Verdana, Arial, Helvetica, sans-serif" size="2"><b>ABSTRACT</b></font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">This retrospective    cohort study describes causes of death in 305 patients (baseline median CD4    count&nbsp;from 2 943 adults on antiretroviral therapy. Acute sepsis (20%),    tuberculosis (18%) and <i>Mycobacterium avium</i> complex (MAC) bacteraemia    (14%) were the most common causes. Mortality owing to the disease was 66% for    MAC bacteraemia and 23% for non-Hodgkin's lymphoma. In 37 patients dying beyond    one year on ART, virological failure was present in 11 (30%), and non-HIV-related    causes of death occurred in 10. The main causes were acute sepsis (6), tuberculosis    (7) and chronic medical conditions (5). Initiating ART at higher CD4 counts    should reduce early mortality.</font></p> <hr size="1" noshade>     <p>&nbsp;</p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Early mortality    on antiretroviral therapy (ART) in low-income countries is substantially higher    than in high-income countries.<sup>1</sup> Mortality during the first year on    ART in sub-Saharan Africa has ranged from 8% to 26%.<sup>2</sup> Main causes    of early death in cohort studies from sub-Saharan Africa include tuberculosis,    acute sepsis, cryptococcal meningitis, malignancies and chronic diarrhoea or    wasting syndromes.<sup>2</sup> Less is known about causes of death later in    the course of ART. In high-income countries, there is increasing emphasis on    non-HIV infection-related causes of death.<sup>3</sup> This study describes    the causes of death in a large single-centre cohort on ART according to time    on treatment and, in particular, death beyond the first year on ART.</font></p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="3"><b>Methods</b></font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Chris Hani Baragwanath    Hospital is a 2 700-bed university-associated public sector hospital serving    Soweto. WHO stage 4 diseases (AIDS) or a CD4 cell count &lt;200 cells/&igrave;!    qualify patients for ART, usually comprising stavudine, lamivudine and efavirenz.    Cotrimoxazole prophylaxis was provided too. Frequent clinic visits were scheduled    for the first 6 months, after which clinically well patients were seen less    frequently.</font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">A retrospective    cohort study was conducted of the 2 943 adult patients (218 years of age) who    initiated ART between 1 April 2004 and 31 December 2005. Patients were followed    till January 2009 for a median of 2.7 years.</font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Causes of death    were assigned by attending doctors in the hospital wards and HIV clinic. For    patients who died at home, an attempt was made to differentiate sudden unexpected    death from chronic ill-health. Family members of patients who died at home were    informally asked the symptoms and cause of death as part of routine follow-up    of patients who missed appointments or if family members reported the death.    The researcher reviewed clinic records, inpatient hospital files and laboratory    investigations on all patients who died, and designated a final cause of death.    Acute sepsis included acute pneumonia, acute bacterial meningitis, septicaemia    and other severe bacterial infections. Chronic medical conditions included diabetes    mellitus, chronic cardio-respiratory diseases and renal diseases (excluding    HIV-associated nephropathy). Unmasking of an appropriate opportunistic disease    within 6 months of starting effective ART was adjudged to be immune reconstitution    disease (IRD). Patients were considered lost to follow-up if not seen in the    6 months preceding the close of the study.</font></p>     ]]></body>
<body><![CDATA[<p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">The study was approved    by the Committee for Research on Human Subjects of the University of the Witwatersrand.</font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Chi-squared test    calculations or Fisher's exact test were used for group comparisons.</font></p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="3"><b>Results</b></font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Death was known    to have occurred in 305 (10.4%) of the 2 943 patients. The median age of those    who died was 36 years (range 19 - 69 years) and the median CD4 count at baseline    was 26/&igrave;! (range 1 -479/&#956;. <a href="#t1">Table 1</a> compares baseline    characteristics of 305 patients who died with the 2 638 survivors. Comparing    the baseline characteristics of the 268 patients who died &lt;12 months on ART    with the 37 who died &gt;12 months on ART, significantly more died in the first    12 months with CD4 &lt;50 cells/&igrave; (193 (72%) v. 18 (49%) (p=0.0039))    and with WHO stage 4 disease (168 (63%) v. 12 (32%) (p=0.0004)).</font></p>     <p><a name="t1"></a></p>     <p>&nbsp;</p>     <p align="center"><img src="/img/revistas/samj/v102n8/24t01.jpg"></p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Of those who died,    165 (54%) died in the first 3 months on ART, 53 (17%) in months 4 - 6, 50 (16%)    in months 7 - 12, 22 (7%) in the second year, 9 (3%) in the third year, and    6 (2%) beyond 3 years. Over the study period, 268 (9.1%) patients were lost    to follow-up.</font></p>     ]]></body>
<body><![CDATA[<p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">A specific cause    of death was retrospectively assigned to 275 (90%) patients. There was no information    on 22 (7%) of the deaths, and 8 (3%) had a sudden unexpected death at home.    More than one cause was found in 14 patients.</font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Acute sepsis (20%),    TB (18%) and <i>Mycobacterium avium</i> complex (MAC) bacteraemia (14%) were    the most common causes of death (<a href="#f1">Fig. 1</a>). Of 64 with confirmed    MAC bacteraemia in the total cohort, 42 (66%) died from the condition. Standard    initial treatment of MAC bacteraemia included clarithromycin with ethambutol    and a third drug, usually ciprofloxacin. Lactic acidosis as a toxicity owing    predominantly to stavudine was implicated in 11 (3.6%) deaths. The 21 AIDS-defining    cancers causing death comprised Kaposi's sarcoma (12), non-Hodgkin's lymphoma    (6), Burkitt's lymphoma (1), and carcinoma of the cervix (2). Of 30 in the cohort    with non-Hodgkin's lymphoma, 7 (23%) died. The 7 non-AIDS defining malignancies    were 3 with Hodgkin's lymphoma, and 1 each with carcinoma of the lung, anus    and oesophagus, and one with acute myeloid leukaemia. Chronic medical conditions    included 9 patients with cardiac disease (4 with dilated cardiomyopathy, 2 with    rheumatic heart disease, and 1 each with atrial myxoma, third-degree heart block,    and aortic aneurysm), 5 with chronic lung disease, 3 with chronic renal failure    predating ART, and 3 with diabetes mellitus. Sepsis was microbiologically defined    in 15 (25%) patients with acute sepsis including 3 patients with bacterial meningitis    (2 with <i>Streptococcus pneumoniae</i> and 1 with non-typhoidal <i>salmonella</i>    who was also bacteraemic) and 13 with bacteraemia (5 with <i>Escherichia coli,</i>    4 with <i>Staphylococcus aureus</i> and 4 with non-typhoidal <i>salmonella).</i>    Unmasking IRD comprised 4 patients with tuberculosis and 2 with MAC infection.</font></p>     <p><a name="f1"></a></p>     <p>&nbsp;</p>     <p align="center"><img src="/img/revistas/samj/v102n8/24f01.jpg"></p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Deaths in hospital    occurred in 39 (78%) of 50 patients who died after 7 - 12 months on ART and    in 26 (70%) of 37 who died after &gt;12 months on ART. Virological failure (viral    load &gt;400 copies/ml) was noted in 9 (18%) who died in months 7 - 12, and    11 (30%) who died beyond the first year; 8 of the latter 11 died of sepsis,    tuberculosis or MAC bacteraemia. Common causes of death &gt;12 months after    starting ART were acute sepsis (16%), TB (19%; 5 cultured; 1 each with multi-drug    resistance and rifampicin monoresistance), and chronic medical conditions (14%).    Non-HIV-related causes were found in 10 patients, comprising chronic medical    conditions (5), motor vehicle accident (2), and 1 each with cancer of the anus,    pulmonary embolism (in a patient with chronic diarrhoea related to intestinal    spirochaetosis), and postoperative complications. Three patients died of lactic    acidosis in the second year.</font></p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="3"><b>Discussion</b></font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">The most striking    finding of this study among AIDS-related causes of death, in contrast with other    African studies,<sup>2,4</sup> was the importance of MAC bacteraemia. It has    been recognised as an important opportunistic infection in countries in sub-Saharan    Africa in studies employing mycobacterial blood cultures.<sup>5-6</sup> It is    associated with a high mortality in the ART era with only 30% of such patients    alive beyond 2 years.<sup>7</sup> Treatment failure is common, reasons including    drug toxicity, inadequate serum levels and development of drug resistance. Primary    prophylaxis with clarithromycin or azithromycin for patients with CD4 cell counts    &lt;50 - 100/&igrave;! might have prevented cases prior to ART.</font></p>     ]]></body>
<body><![CDATA[<p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">TB and cryptococcal    meningitis have been the leading causes of death in most other African studies.<sup>2,4</sup>    Cryptococcal meningitis was a less common cause in this study.<sup>2,4</sup>    Bacterial causes of death, other than mycobacterial infections, have not been    well-defined in ART studies. The organisms found are common in patients with    HIV infection.<sup>2</sup></font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Among non-Hodgkin's    lymphoma patients co-infected with HIV in California, 59% died within 2 years    of diagnosis compared with 30% without HIV infection.<sup>8</sup> In Uganda,    only 20 of 154 patients with non-Hodgkin lymphoma, irrespective of HIV status,    were known to be alive a year after diagnosis.<sup>9</sup> The outcome in this    study appears better but merits a dedicated study as some patients who died    might not have accessed ART. Non-AIDS-defining cancers are likely to increase    with longer duration on ART and increasing age.</font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Unmasking IRD was    an uncommon cause of death, as it was in Uganda.<sup>4</sup> Two missing causes    of death, compared with other settings,<sup>3</sup> were liver failure, possibly    owing to low rates of hepatitis C infection in this cohort and the activity    of lamivudine against hepatitis B, and ischaemic heart disease, since coronary    atherosclerosis is uncommon in this population.<sup>10</sup></font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">This study mirrored    the high first-year mortality in cohorts in sub-Saharan Africa.<sup>2,4</sup>    Mortality was low beyond 1 year on ART, as in similar studies.<sup>2,4</sup>    Beyond 12 months of ART, virological failure was a prominent finding in those    who died. This was partially responsible for the continued importance of TB,    MAC bacteraemia and acute sepsis, accounting for half of these cases. Non-HIV-related    causes, especially chronic medical conditions, acquired increased relative prominence.</font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">This study has    some potential limitations. Many patients were lost to follow-up, some of whom    probably died.<sup>11</sup> Missed deaths might have affected the ranking of    causes of death. No autopsies were performed. There was no formal verbal autopsy    for those who died at home, and not all of those had a family member interviewed.</font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">The study strength,    despite its retrospective nature, was that ascertainment of cause of death was    as accurate as could be achieved without autopsies. Those who died having received    ART for &lt;6 months were seen frequently as in- or outpatients. Of the patients    who died having been on ART &gt;6 months, 75% died in hospital. Both groups    could be investigated at a tertiary level. Studies such as this involving the    clinical record are important as death certificates and routine surveillance    data are less accurate.<sup>12</sup> There is also an inherent tension between    clinical assignment and public health coding of cause of death for the purposes    of public health planning, programmes and evaluation. Some clinical causes have    been labelled 'garbage coding', including categories such as sepsis and pulmonary    embolism since each has an underlying cause to precipitate the chain of events    leading to death.<sup>13</sup> In this study, that underlying cause was AIDS.</font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">In conclusion,    MAC bacteraemia was an important cause of death not highlighted in other African    studies. Access to treatment of malignancy may improve outcomes. Virological    failure and non-HIV-related causes were prominent beyond the first year on ART.    Initiating ART at higher CD4 counts should reduce early mortality and increase    the relative importance of non-HIV-related causes of death over time.<sup>14</sup></font></p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2"><b>Acknowledgements.</b>    I thank Salome Charalambous from the Aurum Institute, Johannesburg, for assistance    with data.</font></p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="3"><b>References</b></font></p>     ]]></body>
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S Afr Med J 2009;99: 648-652.</font>&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=549621&pid=S0256-9574201200080002400012&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --><!-- ref --><p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">13.&nbsp;Naghavi    M, Makela S, Foreman K, et al. Algorithms for enhancing public health utility    of national causes-of-death data. Population Health Metrics 2010;8:9.</font>&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=549622&pid=S0256-9574201200080002400013&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --><!-- ref --><p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">14.&nbsp;Hoffman    CJ, Fielding KL, Johnston V, et al. Changing predictors of mortality over time    from cART start: implications for care. J Acquir Immune Defic Syndr 2011;58:269-276.</font>&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=549623&pid=S0256-9574201200080002400014&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --><p>&nbsp;</p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2">Accepted 18 June    2012.</font></p>     <p>&nbsp;</p>     <p>&nbsp;</p>     <p><font face="Verdana, Arial, Helvetica, sans-serif" size="2"><b><a name="back"></a><a href="#top"><img src="/img/revistas/samj/v102n8/seta.jpg" border="0"></a>    Correspondence to:    ]]></body>
<body><![CDATA[<br>   </b> A Karstaedt    <br>   (<a href="mailto:karstaedt@mweb.co.za">karstaedt@mweb.co.za</a>)</font></p>      ]]></body>
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