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<art><ui>cc10221</ui><ji>1364-8535</ji><fm>
<dochead>Letter</dochead>
<bibl>
<title>
<p>Intravenous magnesium in subarachnoid hemorrhage</p>
</title>
<aug>
<au ca="yes" id="A1"><snm>Abdo</snm><mi>F</mi><fnm>Wilson</fnm><insr iid="I1"/><email>f.abdo@neuro.umcn.nl</email></au>
<au id="A2"><snm>Hoedemaekers</snm><mi>W</mi><fnm>Cornelia</fnm><insr iid="I1"/><email>c.hoedemaekers@ic.umcn.nl</email></au>
<au id="A3"><snm>van der Hoeven</snm><mi>G</mi><fnm>Johannes</fnm><insr iid="I1"/><email>hahoe@mac.com</email></au>
</aug>
<insg>
<ins id="I1"><p>Department of Critical Care Medicine, Radboud University Nijmegen Medical Center, Geert Grooteplein 10, PO Box 9101, 6500 HB Nijmegen, The Netherlands</p></ins>
</insg>
<source>Critical Care</source>
<issn>1364-8535</issn>
<pubdate>2011</pubdate>
<volume>15</volume>
<issue>3</issue>
<fpage>427</fpage>
<url>http://ccforum.com/content/15/3/427</url>
<note>See related research by Wong <it>et al.</it>, <url>http://ccforum.com/content/15/1/R52</url></note>
<xrefbib><pubidlist><pubid idtype="pmpid">21631908</pubid><pubid idtype="doi">10.1186/cc10221</pubid></pubidlist></xrefbib>
</bibl>
<history><pub><date><day>24</day><month>5</month><year>2011</year></date></pub></history>
<cpyrt><year>2011</year><collab>BioMed Central Ltd</collab></cpyrt>
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<classification subtype="pubmedcentral-release-delay-information" type="BMC">
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</classification>
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<sec>
<st>
<p/>
</st>
<p>We would like to offer some comments on the updated meta-analysis on intravenous magnesium sulphate for aneurysmal subarachnoid hemorrhage <abbrgrp>
<abbr bid="B1">1</abbr>
</abbrgrp>, which was conducted by Wong and colleagues and published in a recent issue of <it>Critical Care</it>.</p>
<p>First, the authors did not mention a (non-blinded) randomized placebo-controlled trial conducted by Akdemir and colleagues and published in 2009 <abbrgrp>
<abbr bid="B2">2</abbr>
</abbrgrp>. Although this study would probably not pass Wong and colleagues' method of scrutiny, we believe that it should be mentioned alongside two other studies the authors described but did not include in the data analysis.</p>
<p>Second, the study by Westermaier and colleagues <abbrgrp>
<abbr bid="B3">3</abbr>
</abbrgrp> should not be included in the data analysis. These authors, in contrast to those of the other included studies in which magnesium was used as an add-on therapy, did not use nimodipine in any of the included patients. Wong and colleagues exclude the study by Schmid-Elsaesser and colleagues <abbrgrp>
<abbr bid="B4">4</abbr>
</abbrgrp> because nimodipine was not used in the magnesium group but omit doing the same for the study by Westermaier and colleagues.</p>
<p>Third, Figure 3 <abbrgrp>
<abbr bid="B1">1</abbr>
</abbrgrp> shows that the number of control subjects in 'Veyna 2002' was 20. However, in that study, the outcome data in the control group were present for only 16 patients (4 of the 20 patients were withdrawn because study requirements were not met) <abbrgrp>
<abbr bid="B5">5</abbr>
</abbrgrp>. Accordingly, the risk ratios in Figure 3 should be adjusted.</p>
<p>Fourth, given Wong and colleagues' definition of delayed cerebral ischemia, we wonder why the studies of Veyna and colleagues <abbrgrp>
<abbr bid="B5">5</abbr>
</abbrgrp>, Muroi and colleagues <abbrgrp>
<abbr bid="B6">6</abbr>
</abbrgrp>, and their own study in 2006 <abbrgrp>
<abbr bid="B7">7</abbr>
</abbrgrp> were not included in Figure <figr fid="F1">1</figr>
<abbrgrp>
<abbr bid="B1">1</abbr>
</abbrgrp>. In the study by Veyna and colleagues <abbrgrp>
<abbr bid="B5">5</abbr>
</abbrgrp>, the outcome measure 'clinical vasospasm' was defined as a 'new focal neurological deficit that could not be accounted for by other causes'. Although the time frame in which this was scored is not mentioned, this was during the patients' stay in the intensive care unit and therefore would be clinically relevant to include in Figure <figr fid="F1">1</figr>
<abbrgrp>
<abbr bid="B1">1</abbr>
</abbrgrp>. The same applies to the outcome measures 'delayed ischemic neurological deficit' in the study by Muroi and colleagues <abbrgrp>
<abbr bid="B6">6</abbr>
</abbrgrp> and 'symptomatic vasospasm' in their own study in 2006 <abbrgrp>
<abbr bid="B7">7</abbr>
</abbrgrp>.</p>
<fig id="F1"><title><p>Figure 1</p></title><caption><p>Fixed-effects model of risk ratio for a favorable outcome at 3 months</p></caption><text>
   <p><b>Fixed-effects model of risk ratio for a favorable outcome at 3 months</b>. A comparison between magnesium sulphate infusion and a placebo in patients with aneurysmal subarachnoid hemorrhage is shown. CI, confidence interval; M-H, Mantel-Haenszel.</p>
</text><graphic file="cc10221-1"/></fig>
</sec>
<sec>
<st>
<p>Authors' response</p>
</st>
<p>George KC Wong and Wai S Poon</p>
<p>We thank Abdo and colleagues for their interest in our articles <abbrgrp>
<abbr bid="B1">1</abbr>
<abbr bid="B8">8</abbr>
</abbrgrp> and for their comments. We would like to offer the following clarifications.</p>
<p>First, it is unfortunate that the article by Akdemir and colleagues <abbrgrp>
<abbr bid="B2">2</abbr>
</abbrgrp> slipped through the established search methodology for the journals. Nevertheless, the authors' results on the lack of an effect of magnesium sulphate infusion on clinical outcome echoed the conclusion of our review.</p>
<p>Second, the study by Schmid-Elsaesser and colleagues <abbrgrp>
<abbr bid="B4">4</abbr>
</abbrgrp> compared magnesium sulphate infusion with nimodipine, the latter of which has an established beneficial effect on aneurysmal subarachnoid hemorrhage. The study by Westermaier and colleagues <abbrgrp>
<abbr bid="B3">3</abbr>
</abbrgrp> was trickier in mentioning how their cohort of patients employed nimodipine in the Discussion section but not in the Results section. Westermaier and colleagues mentioned that they did not seek an alternative route of administration for oral tablet forms of nimodipine for intubated patients but did not mention that they would omit the nimodipine oral tablets in good-grade patients. This actually is the policy in some neurosurgical centers. The nature of the comparison between magnesium sulphate infusion with placebo infusion is also different from that of Schmid-Elsaesser and colleagues <abbrgrp>
<abbr bid="B4">4</abbr>
</abbrgrp>. Again, the omission of the data of Westermaier and colleagues did not alter the conclusion of the review.</p>
<p>Third, Veyna and colleagues <abbrgrp>
<abbr bid="B5">5</abbr>
</abbrgrp> exposed a problem in the earlier study report format, in which numbers of patients were not mentioned in each step. Withdrawal could mean just the study medications, and the patients were assessed for intention-to-treat analysis. If the four control patients had been excluded, the result would have been the same (Figure <figr fid="F1">1</figr>) <abbrgrp>
<abbr bid="B5">5</abbr>
<abbr bid="B6">6</abbr>
<abbr bid="B9">9</abbr>
</abbrgrp>.</p>
<p>Fourth, the new definition of delayed cerebral ischemia included the subsets of patients with asymptomatic cerebral infarction <abbrgrp>
<abbr bid="B10">10</abbr>
</abbrgrp>, which turned out to be an important prognostic factor and which earlier studies ignored. Lastly, we would like to emphasize that the detrimental effect of higher-achieved plasma magnesium concentrations further supported the results of the current meta-analysis <abbrgrp>
<abbr bid="B11">11</abbr>
</abbrgrp>.</p>
</sec>
<sec>
<st>
<p>Competing interests</p>
</st>
<p>The authors declare that they have no competing interests.</p>
</sec>
</bdy><bm>
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