<?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>0121-8123</journal-id>
<journal-title><![CDATA[Revista Colombiana de Reumatología]]></journal-title>
<abbrev-journal-title><![CDATA[Rev.Colomb.Reumatol.]]></abbrev-journal-title>
<issn>0121-8123</issn>
<publisher>
<publisher-name><![CDATA[Asociación Colombiana de Reumatología]]></publisher-name>
</publisher>
</journal-meta>
<article-meta>
<article-id>S0121-81232011000400003</article-id>
<title-group>
<article-title xml:lang="es"><![CDATA[Historia de la enfermedad de Devic]]></article-title>
<article-title xml:lang="en"><![CDATA[History of Devic's disease]]></article-title>
</title-group>
<contrib-group>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Iglesias Rodríguez]]></surname>
<given-names><![CDATA[Antonio]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Gil]]></surname>
<given-names><![CDATA[Diana]]></given-names>
</name>
<xref ref-type="aff" rid="A02"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Restrepo]]></surname>
<given-names><![CDATA[José Félix]]></given-names>
</name>
<xref ref-type="aff" rid="A03"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Iglesias Gamarra]]></surname>
<given-names><![CDATA[Antonio]]></given-names>
</name>
<xref ref-type="aff" rid="A03"/>
</contrib>
</contrib-group>
<aff id="A01">
<institution><![CDATA[,Hospital San Ignacio de Loyola  ]]></institution>
<addr-line><![CDATA[ ]]></addr-line>
</aff>
<aff id="A02">
<institution><![CDATA[,Universidad Nacional de Colombia Unidad de Reumatología ]]></institution>
<addr-line><![CDATA[ ]]></addr-line>
</aff>
<aff id="A03">
<institution><![CDATA[,Universidad Nacional de Colombia Facultad de Medicina ]]></institution>
<addr-line><![CDATA[ ]]></addr-line>
</aff>
<pub-date pub-type="pub">
<day>00</day>
<month>10</month>
<year>2011</year>
</pub-date>
<pub-date pub-type="epub">
<day>00</day>
<month>10</month>
<year>2011</year>
</pub-date>
<volume>18</volume>
<numero>4</numero>
<fpage>271</fpage>
<lpage>284</lpage>
<copyright-statement/>
<copyright-year/>
<self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_arttext&amp;pid=S0121-81232011000400003&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_abstract&amp;pid=S0121-81232011000400003&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_pdf&amp;pid=S0121-81232011000400003&amp;lng=en&amp;nrm=iso"></self-uri><abstract abstract-type="short" xml:lang="es"><p><![CDATA[En este escrito hacemos una completa revisión de la enfermedad de Devic, desde sus primeras descripciones por Eugene Devic, hasta el concepto actual, donde es considerada una neuromielitis óptica. Exponemos las diferentes formas de presentación de la neuromielitis óptica así como los hallazgos clínicos y de laboratorio que permiten diferenciar esta entidad de la esclerosis múltiple, tarea que muchas veces no es fácil de realizar por la semejanza en la presentación clínica. Sin embargo es importante su diferenciación porque el tratamiento y el pronóstico difieren entre estas dos enfermedades. No obstante, el descubrimiento de los anticuerpos IgG anti NMO, dirigidos contra los canales de agua de acuaporina 4 fueron fundamentales en tal diferenciación. Realizamos una mención especial sobre la enfermedad de Devic y el lupus y finalmente hacemos unas notas sobre el tratamiento disponible para esta patología.]]></p></abstract>
<abstract abstract-type="short" xml:lang="en"><p><![CDATA[In this paper we do a complete review of Devic's disease, from its first descriptions by Eugene Devic, to the current concept, which is considered a neuromyelitis optica (NMO). We present the different forms of presentation of NMO as well as clinical and laboratory findings that distinguish this entity from multiple sclerosis, a task that frequently is not easy to perform because of the similarity in clinical presentation. Its differentiation is important because the treatment and prognosis differ between these two diseases. However the discovery of NMO IgG antibodies directed against aquaporin-4 water channels was a critical step in such differentiation. We made special mention of Devic's disease and lupus, and finally make some notes on the available treatment for this pathology.]]></p></abstract>
<kwd-group>
<kwd lng="es"><![CDATA[enfermedad de Devic]]></kwd>
<kwd lng="es"><![CDATA[lupus eritematoso sistémico]]></kwd>
<kwd lng="es"><![CDATA[neuromielitis óptica]]></kwd>
<kwd lng="es"><![CDATA[esclerosis múltiple]]></kwd>
<kwd lng="en"><![CDATA[Devic'disease]]></kwd>
<kwd lng="en"><![CDATA[systemic lupus erythematosus]]></kwd>
<kwd lng="en"><![CDATA[neuromyelitis optica]]></kwd>
<kwd lng="en"><![CDATA[multiple sclerosis]]></kwd>
</kwd-group>
</article-meta>
</front><body><![CDATA[  <font face="Verdana" size="2">      <p><b>HISTORIA</b></p>     <p><font size="4"><b>    <center>Historia de la enfermedad de Devic</center></b></font></p>     <p><font size="3"><b>    <center>History of Devic's disease</center></b></font></p>     <p>    <center>Antonio Iglesias Rodr&iacute;guez<sup>1</sup>, Diana Gil<sup>2</sup>, Jos&eacute; F&eacute;lix Restrepo<sup>3</sup>, Antonio Iglesias Gamarra<sup>3</sup></center></p>     <br>     <p><sup>1</sup>Fellow de Neurolog&iacute;a, Hospital San Ignacio de Loyola. Chicago. EUA.    ]]></body>
<body><![CDATA[<br> <sup>2</sup>Reumatolog&iacute;a. Unidad de Reumatolog&iacute;a, Universidad Nacional de Colombia.    <br> <sup>3</sup>Profesor titular de Medicina Interna y Reumatolog&iacute;a, Facultad de Medicina, Universidad Nacional de Colombia.    <br> Correspondencia, Dr. Antonio Iglesias G.: <a href="mailto:iglesias.antonio1@gmail.com">iglesias.antonio1@gmail.com</a></p>     <p>Los autores declaran no presentar ning&uacute;n conflicto de inter&eacute;s al momento de la redacci&oacute;n del manuscrito.</p>     <p>Recibido: 13 de junio de 2011 Aceptado: 11 de octubre de 2011</p>  <hr>     <p><font size="3"><b>Resumen</b></font></p>     <p>En este escrito hacemos una completa revisi&oacute;n de la enfermedad de Devic, desde sus primeras descripciones por Eugene Devic, hasta el concepto actual, donde es considerada una neuromielitis &oacute;ptica. Exponemos las diferentes formas de presentaci&oacute;n de la neuromielitis &oacute;ptica as&iacute; como los hallazgos cl&iacute;nicos y de laboratorio que permiten diferenciar esta entidad de la esclerosis m&uacute;ltiple, tarea que muchas veces no es f&aacute;cil de realizar por la semejanza en la presentaci&oacute;n cl&iacute;nica. Sin embargo es importante su diferenciaci&oacute;n porque el tratamiento y el pron&oacute;stico difieren entre estas dos enfermedades. No obstante, el descubrimiento de los anticuerpos IgG anti NMO, dirigidos contra los canales de agua de acuaporina 4 fueron fundamentales en tal diferenciaci&oacute;n. Realizamos una menci&oacute;n especial sobre la enfermedad de Devic y el lupus y finalmente hacemos unas notas sobre el tratamiento disponible para esta patolog&iacute;a.</p>     <p><b>Palabras clave</b>: enfermedad de Devic, lupus eritematoso sist&eacute;mico, neuromielitis &oacute;ptica, esclerosis m&uacute;ltiple.</p> <hr>     <p><font size="3"><b>Summary</b></font></p>     <p>In this paper we do a complete review of Devic's disease, from its first descriptions by Eugene Devic, to the current concept, which is considered a neuromyelitis optica (NMO). We present the different forms of presentation of NMO as well as clinical and laboratory findings that distinguish this entity from multiple sclerosis, a task that frequently is not easy to perform because of the similarity in clinical presentation. Its differentiation is important because the treatment and prognosis differ between these two diseases. However the discovery of NMO IgG antibodies directed against aquaporin-4 water channels was a critical step in such differentiation. We made special mention of Devic's disease and lupus, and finally make some notes on the available treatment for this pathology.</p>     ]]></body>
<body><![CDATA[<p><b>Key words</b>: Devic'disease, systemic lupus erythematosus, neuromyelitis optica, multiple sclerosis.</p> <hr>     <p><font size="3"><b>Introducci&oacute;n</b></font></p>     <p>La neuromielitis &oacute;ptica, tambi&eacute;n conocida como enfermedad de Devic, es una enfermedad desmielinizante inflamatoria idiop&aacute;tica del sistema nervioso central que afecta preferencialmente los nervios &oacute;pticos y la medula espinal, t&iacute;picamente respeta el cerebro y tiene un curso con reca&iacute;das.</p>     <p>En 1870, Sir Thomas Clifford Allbut<sup>1</sup> expres&oacute; el inter&eacute;s de la ciencia al analizar la asociaci&oacute;n de dos alteraciones neurol&oacute;gicas que se iniciaban en la m&eacute;dula espinal (mielitis), en cinco pacientes. Doce a trece semanas despu&eacute;s los pacientes presentaron el compromiso ocular (neuritis). En 1889, Achard y Guinon<sup>2</sup> describieron un estudio cl&iacute;nico-patol&oacute;gico de esta nueva entidad. Posteriormente Eugene Devic fue el primero en utilizar los t&eacute;rminos de "neuromielitis &oacute;ptica".</p>      <p>    <center><img src="img/revistas/rcre/v18n4/v18n4a03f1.jpg" width="214" height="257"> </center></p>     <p><font size="3"><b>&iquest;Qui&eacute;n fue Eugene Devic?</b></font></p>     <p>Despu&eacute;s de describir la neuromielitis &oacute;ptica, poco se sab&iacute;a de este investigador de origen franc&eacute;s, hasta que Dar&iacute;o Giorgi<sup>3</sup>, m&eacute;dico del Departamento de Ciencias Oftalmol&oacute;gicas "La Sapienza" de la Universidad de Roma, averigu&oacute; la vida de este investigador.</p>     <p>Eugene Devic naci&oacute; en Lyon el 24 de octubre de 1858<sup>3</sup>; fue disc&iacute;pulo y colaborador del profesor Bouveret en Lyon. Se gradu&oacute; de m&eacute;dico en 1886 con la tesis titulada "Des rachutes de la fi&egrave;vre typh&ouml;de"<sup>3</sup>. En 1888, Devic empez&oacute; a trabajar como cl&iacute;nico en el Hospital de Antiquaille y posteriormente continu&oacute; su carrera en el servicio de Anatom&iacute;a patol&oacute;gica entre 1892 y 1894 y luego trabaj&oacute; en el Hospital de Lyon, donde le interes&oacute; la pediatr&iacute;a<sup>3</sup>.</p>     <p>Entre 1888 y 1891, public&oacute; una serie de art&iacute;culos en la revista m&eacute;dica de Lyon Province medicale sobre varias enfermedades de la infancia, como reumatismo nodoso, corea, varicela, tosferina, ros&eacute;ola, enuresis, tuberculosis del h&iacute;gado y fiebre tifoidea. Con el doctor Bouveret public&oacute; algunos art&iacute;culos sobre gastroenterolog&iacute;a (ver <a href="#tab1">tabla 1</a>, sobre las diferentes publicaciones desde 1892 a 1917)<sup>3</sup>.</p>     ]]></body>
<body><![CDATA[<p>    <center><a name="tab1"><img src="img/revistas/rcre/v18n4/v18n4a03t1.jpg"></a></center></p>     <p><font size="3"><b>Descripci&oacute;n de la neuromielitis &oacute;ptica</b></font></p>     <p>De su producci&oacute;n cient&iacute;fica, la neuromielitis &oacute;ptica (NMO) fue su trabajo seminal; public&oacute; dos art&iacute;culos y con su estudiante Fernand Gault describieron diecisiete casos de neuromielitis &oacute;ptica, que para esa &eacute;poca era un serie excelente<sup>4-6</sup>. Para el Congreso Franc&eacute;s de Medicina, en 1894 Devic escrib&iacute;a lo siguiente: "<i>Ils repr&eacute;sent une des nombreuses modalit&eacute;s cliniques constitu&eacute;es par les localisations multiples d'unm&ecirc;me temps divers points du syst&egrave;me nerveux central et p&eacute;riph&eacute;rique</i>"<sup>5</sup>.</p>     <p>Esta hip&oacute;tesis de Devic a&uacute;n persiste. En 1897, Devic logr&oacute; trabajar en cardiolog&iacute;a y con el profesor Tripier escribi&oacute; un cap&iacute;tulo sobre "S&eacute;m&eacute;iologie da coeur et des vaisseaux" para el libro de patolog&iacute;a del profesor Bouchard. Finalmente, un estudiante an&oacute;nimo, el 23 de febrero de 1930, en la revista <i>Lyon medicale</i>, n&uacute;mero 8, escribi&oacute; lo siguiente:</p>     <p><i>Those who knew Dr. Devic only through his studies did not really know him. He was mostly himself while teaching the basic elements of the service he provided, first of all at the Red Cross Hospital and then at the Hospital of Lyon where he stayed until after World War I. There he educated an elite, an elite which has now dispersed, an elite which despite all still bears the imprint left by its master. He showed how to examine a patient, the patience needed and the method involved, the modesty, honesty and precision called for when making a diagnosis. He had a refined clinical sense and clarity of judgment which he made appears simple but that masked a broad education and culture. He was also highly conscientious, the greatest quality any worker can have and the worst vice of the ambitious. Eug&egrave;n&egrave; Devic helped form a talented group of doctors, and had a major impact on medical training during his day. His greatest contribution was to have made clinical medicine into a school. It follows that for men like Eug&egrave;n&egrave; Devic, who avoided all pomp, honors and awards that any judgment made of them mirrored their modest way of life. However, it is only right that they are remembered for standing out. Dr. Devic is dead. He requested a simple funeral. Throughout his life he avoided ostentation; I, more than anyone else, know he would have detested all this pomp and ceremony surrounding his name. Nonetheless, I do not feel I have betrayed his memory by recounting his life's work. He loved his science too much not to pardon one of his pupils, bound to him by numerous ties, for writing a brief summary in a medical journal o fall that he has left us</i><sup>3</sup>.</p>     <p>En 1914, Holden<sup>7</sup> informa sobre cinco casos en los cuales la mielitis se complic&oacute; por una ceguera completa. En 1936, Balser<sup>8</sup>, despu&eacute;s de estudiar a varios pacientes, pensaba que era parte de la esclerosis m&uacute;ltiple. Desde 1936, muchos observadores de diferentes continentes consideraban que la neuritis de Devic pudiese ser una forma de la esclerosis m&uacute;ltiple aguda, o de una encefalomielitis, y que era dif&iacute;cil establecer una diferenciaci&oacute;n entres los tres grupos de entidades de acuerdo con los estudios de Russel Brain<sup>9</sup> en 1929.</p>     <p>Desde 1936, el s&iacute;ndrome de Devic se asoci&oacute; con una variante de la esclerosis m&uacute;ltiple, tratando de buscar una causa de la etiolog&iacute;a de esta enfermedad.</p>     <p>As&iacute;, de esta manera, desde la descripci&oacute;n de Devic<sup>4-5</sup> en 1894, y la tesis de Gault<sup>6</sup> en 1894, la b&uacute;squeda de la etiolog&iacute;a tuvo un gran inter&eacute;s en los diferentes investigadores como Goulden<sup>10</sup> en 1914, Beck<sup>11</sup> en 1927, Stansbury<sup>12</sup> en 1949, y Mandler y cols.<sup>13</sup> en 1993. En unos pocos casos la neuritis &oacute;ptica y la mielitis se han asociado aisladamente a enfermedades como el lupus eritematoso sist&eacute;mico<sup>14-16</sup>, neuro-Behcet<sup>17</sup>, miasteniagravis<sup>18</sup>, s&iacute;ndrome de Sj&ouml;gren primario<sup>19,</sup> <sup>20</sup>, tiroiditis de Hashimoto<sup>20</sup> y varicela<sup>21</sup>, pero en la mayor&iacute;a de los pacientes con enfermedad de Devic no se ha demostrado una asociaci&oacute;n, y en muchos de estos casos se ha comprobado la presencia de anticuerpos antinucleares y anticuerpos dirigidos contra ant&iacute;genos extra&iacute;bles, lo que sugiere una etiolog&iacute;a autoinmune contra los &oacute;rganos (nervio &oacute;ptico y medula espinal). En algunas publicaciones interesantes como las de Beck<sup>11</sup> en 1927, Stansbury<sup>12</sup> en 1949, Ortiz de Zarate y cols.<sup>22</sup> en 1968, Fukazawa y cols.<sup>23</sup> en 1990, Mandler y cols.<sup>13</sup> en 1993 y otras se planteaba que la enfermedad de Devic era una variante de la esclerosis m&uacute;ltiple. Uno de los trabajos seminales fue el de Leonardi y cols.<sup>24</sup> en 1987, en el que realizaron un estudio neuropatol&oacute;gico donde observaron necrosis, cavitaci&oacute;n y engrosamiento de la pared vascular a nivel del cord&oacute;n espinal, adem&aacute;s estudiaron el l&iacute;quido c&eacute;faloraqu&iacute;deo, y observaron que estos hallazgos no se observaban en la esclerosis m&uacute;ltiple; igual conclusi&oacute;n realizaron Mandler y cols.<sup>13</sup>. Otros estudios efectuados en el Reino Unido por Swingler y Compston en 1986 y 1990<sup>25,</sup> <sup>26</sup> observaron que la enfermedad de Devic no era frecuente en el grupo &eacute;tnico cauc&aacute;sico, como s&iacute; se observa en la esclerosis m&uacute;ltiple. A partir de los estudios de Miller y cols.<sup>27</sup>en 1987, Tashiro y cols.<sup>28</sup> en 1987, Paty y cols.<sup>29</sup> en 1988, Thompson y cols.<sup>30</sup> en 1990 y Fasekas y cols. <sup>31</sup> en 1994 se demostr&oacute; que la resonancia magn&eacute;tica del cord&oacute;n espinal y el an&aacute;lisis del l&iacute;quido c&eacute;faloraqu&iacute;deo en los pacientes con enfermedad de Devic eran diferentes a lo observado en la esclerosis m&uacute;ltiple, y la banda oligoclonal que se advierte en el 90% de los pacientes con esclerosis m&uacute;ltiple se ha descrito solo en algunos pacientes con enfermedad de Devic.</p>      <p>Muchos pacientes con NMO pueden diagnosticarse como esclerosis m&uacute;ltiple, pero los estudios comparativos de Seze y cols.<sup>32,</sup> <sup>33</sup> en 2001 y 2003 plantean la posibilidad de que son dos enfermedades diferentes. Bergamaschi y Ghezzi<sup>34</sup> un a&ntilde;o despu&eacute;s demuestran que la NMO puede asociarse con enfermedades autoinmunes y con la presencia de anticuerpos antinucleares, extractables, anticardiolipinas y antic&eacute;lulas parietales.</p>     ]]></body>
<body><![CDATA[<p>Como muchas de las enfermedades autoinmunes no &oacute;rgano-espec&iacute;ficas y &oacute;rgano-espec&iacute;ficas, las infecciones y las alteraciones autoinmunitarias pueden estar comprometidas en la patog&eacute;nesis de la NMO.</p>     <p>El nervio &oacute;ptico y los cordones espinales pueden contener ant&iacute;genos que son blancos por los procesos mediados por una respuesta inmunitaria, mediada por mecanismos humorales<sup>34-37</sup>. Al inicio del cuadro cl&iacute;nico, los eventos que comprometen los nervios &oacute;pticos y el cord&oacute;n espinal suelen ocurrir en un mes o la crisis puede presentarse 120 meses despu&eacute;s.</p>     <p>Ochenta a noventa por ciento de los pacientes con neuromielitis &oacute;ptica tienen episodios de reca&iacute;das y se comprometen simult&aacute;neamente los nervios &oacute;pticos y la mielitis, m&aacute;s que un curso monof&aacute;sico<sup>13,32,33,</sup> <sup>37,38-43</sup>. Las reca&iacute;das suelen presentarse un a&ntilde;o despu&eacute;s en un 60% de los pacientes o al tercer a&ntilde;o en el 90% de los pacientes.</p>     <p><font size="3"><b>Acuaporinas</b></font></p>     <p>En 1992, Preston y cols.<sup>44</sup> identificaron el primer miembro de la familia de las acuaporinas. Actualmente se conocen once miembros en los mam&iacute;feros. Los canales de agua se han postulado como estructuras que permiten el paso del agua a trav&eacute;s de ciertas membranas, y este es uno de los mecanismos para explicar la difusi&oacute;n plasm&aacute;tica<sup>41,44-46</sup>. Las acuaporinas se distribuyen ampliamente en el cuerpo, especialmente en los ri&ntilde;ones, los eritrocitos, los pulmones y los epitelios secretorios como las gl&aacute;ndulas salivares<sup>41,44-48</sup>. La acuaporina 4 (AQP4) se expresa en el sistema nervioso central, m&uacute;sculo esquel&eacute;tico, pulmones, ri&ntilde;ones, est&oacute;mago y gl&aacute;ndulas exocrinas<sup>41,44-48</sup>.</p>     <p>La acuaporina-4 es la principal en los canales de agua del sistema nervioso central y se expresa en la membrana plasm&aacute;tica de los astrocitos; envuelven los capilares de sus alrededores, especialmente en los pies de los astrocitos. Tambi&eacute;n se localiza en las membranas basolaterales de las c&eacute;lulas ependimarias ventriculares y en los n&uacute;cleos hipotal&aacute;micos<sup>41,44-,47,48</sup>. La localizaci&oacute;n de la AQP4 permite la interacci&oacute;n con la distrofina, que incluye el alfa, sintrofina<sup>40,41,44-48</sup>. El papel importante de la AQP4 es la regulaci&oacute;n de la distribuci&oacute;n del agua a trav&eacute;s del cerebro. La AQP4 participa en la manipulaci&oacute;n del agua cerebral, por ello su papel en el edema cerebral secundario a tumores, trauma cerebral, abscesos cerebrales y accidentes cerebro-vasculares; esto se ha podido demostrar en ratones nulos para AQP4 (AQP4- null mice) sometidos a edema cerebral vasog&eacute;nico<sup>48-51</sup>.</p>     <p>El nervio &oacute;ptico y los cordones espinales tienen ant&iacute;geno o autoant&iacute;geno de AQP4, que son blancos para los procesos inmunitarios mediados por v&iacute;a humoral<sup>44,</sup> <sup>47,</sup> <sup>52-54</sup>. Estudios recientes demuestran que la AQP4 genera una respuesta celular T, que a la vez induce una activaci&oacute;n de los linfocitos B espec&iacute;ficos para AQP4, y una gran producci&oacute;n de anticuerpos anti-AQP4 y estos anticuerpos son los que se encuentran en los pacientes con neuromielitis &oacute;ptica<sup>53,54-59</sup> (<a href="#tab2">ver espectro de la neuromielitis &oacute;ptica</a>). Experimentos recientes demuestran que los anticuerpos dirigidos contra la AQP4 son de la subclase IgG1 y tienen la capacidad de activar el complemento<sup>45,57,58</sup>. La transferencia pasiva de AQP4 intratecal de pacientes con NMO puede inducir lesiones como NMO en animales de experimentaci&oacute;n<sup>45,58</sup>. Con los experimentos mencionados previamente, se explica el mecanismo humoral de la NMO, como una enfermedad &oacute;rgano-espec&iacute;fica y por ello se ha descrito en el lupus eritematoso sist&eacute;mico, en el s&iacute;ndrome de Sj&ouml;gren, en la miastenia gravis, en la tiroiditis de Haschimoto y adem&aacute;s tambi&eacute;n se observa la presencia de otros anticuerpos como los ANAS, ENAS, anticar-diolipinas y anticuerpos anti-parietales<sup>44,47,52-59</sup>. Pero la AQP4 no se expresa en los oligoden-drocitos. Lennon y cols. <sup>52,53</sup> en 2004 y 2005 mostraron que los anticuerpos IgG anti- NMO se observan en pacientes con neuromielitis &oacute;ptica y este anticuerpo podr&iacute;a ayudar a diferenciar a los pacientes con s&iacute;ndrome de Devic de las otras alteraciones desmielinizantes<sup>41-42,45,52-55,59-61</sup>.</p>     <p>Los anticuerpos anti-NMO-IgG se unen a la acuaporina-4 en los principales canales que regulan la homeostasis del agua en el sistema nervioso central<sup>44-47,52,53-63</sup>. Los anticuerpos IgG anti-NMO se pueden detectar en el suero de pacientes con algunos des&oacute;rdenes relacionados a la neuromielitis, que incluye la esclerosis m&uacute;ltiple &oacute;ptica-espinal de origen asi&aacute;tico; mielitis recurrente, asociada con mielitis longitudinal extensa (compromete m&aacute;s de tres cuerpos vertebrales); neuritis &oacute;ptica aislada recurrente; neuritis &oacute;ptica o mielitis en el contexto de ciertas enfermedades &oacute;rgano-espec&iacute;ficas (tiroiditis de Haschi-moto) y enfermedades no &oacute;rgano-espec&iacute;ficas como el lupus y el s&iacute;ndrome de Sj&ouml;gren primario, lo que hoy en d&iacute;a se conoce como el espectro de patolog&iacute;as que producen la neuromielitis &oacute;ptica<sup>44,52-63</sup>.</p>     <p>Un papel efector del anticuerpo IgG anti-NMO en la neuromielitis &oacute;ptica no se ha podido documentar, aunado a una carencia de modelos en animales como s&iacute; ocurre con otras patolog&iacute;as neurol&oacute;gicas como la epilepsia y la enfermedad de Parkinson, lo cual pudiera explicar mejor los mecanismos informados (vida supra).</p>     <p><font size="3"><b>Criterios diagn&oacute;sticos de la enfermedad de Devic</b></font></p>     ]]></body>
<body><![CDATA[<p>Las primeras propuestas elaboradas para el diagn&oacute;stico de la neuromielitis &oacute;ptica fueron las de Mandler y cols.<sup>13</sup> en 1993, en las que aplican los criterios cl&iacute;nicos y por primera vez se utilizan las neuroim&aacute;genes como la resonancia de la m&eacute;dula espinal y el an&aacute;lisis del LCR.</p>     <p>O'Riordan y cols.<sup>37</sup> en 1996 utilizaron los mismos criterios para la NMO, pero incorporaron el concepto de monof&aacute;sico o multifasico o recidivante.</p>     <p>Wingerchuk y cols.<sup>41</sup> en 1999 analizaron los criterios absolutos, en los que incluyen la presencia de neuritis &oacute;ptica, mielitis y la ausencia de enfermedad en otras &aacute;reas diferentes a los nervios &oacute;pticos y la mielitis. Introducen los criterios de soportes mayores y menores. En el 2006 estos criterios se revisan y se establece un consenso en la Cl&iacute;nica Mayo<sup>41-43,64-66</sup>.</p>     <p>Los criterios desarrollados por Dean M. Wingerchuk y cols. y luego revisados por los mismos expertos para la enfermedad de Devic son las gu&iacute;as para el diagn&oacute;stico de esta patolog&iacute;a. Se requieren dos criterios absolutos y al menos otros dos o tres de soportes<sup>41-42,64-66</sup>.</p> <ol type="A">    <li>Criterios absolutos</li> <ol type="1">    <li>Neuritis &oacute;ptica</li>     <li>Mielitis aguda</li>    </ol>     <li>Criterios de soportes</li>    </ol>     ]]></body>
<body><![CDATA[<p>Incluyen:</p>     <p><b><i>1. Resonancia magn&eacute;tica cerebral</i></b>. Ausencia de esclerosis m&uacute;ltiple. En la NMO se caracteriza por la ausencia de lesiones parenquimatosas, pero pueden encontrarse algunas lesiones en la sustancia blanca que no sean caracter&iacute;sticas de la esclerosis m&uacute;ltiple.</p>     <p><b><i>2. Resonancia magn&eacute;tica del cord&oacute;n espinal</i></b>, especialmente las im&aacute;genes en T2 que comprometen m&aacute;s de tres segmentos de los cuerpos vertebrales, que corresponde a una lesi&oacute;n extensa, es decir una mielitis longitudinal<sup>27-35,37-42,64-73</sup>. La presencia de una lesi&oacute;n heterog&eacute;nea en T2 sugiere necrosis o cavitaci&oacute;n<sup>64-73</sup>.</p>     <p><b>3. Anticuerpos</b>.</p>     <p><b><i>La seropositividad de los anticuerpos IgG anti-NMO</i></b>. Estos anticuerpos eval&uacute;an la seropositividad de los anticuerpos anti-AQP4 por la t&eacute;cnica del radioinmunoensayo (ELISA)<sup>39,44,45,52,53,62</sup>.</p>     <p><i><b>Otros anticuerpos</b></i>. Es necesario analizar otros anticuerpos como los ANAS, ENAS, anti-ADN de doble cadena, cardiolipinas, anti-TPO, anti-tiroglobulinas, especialmente cuando exista la posibilidad de una enfermedad auto-inmune como el LES o el s&iacute;ndrome de Sj&ouml;gren primario. La verdadera incidencia no es conocida, pero pueden asociarse hasta en un 50% de los pacientes<sup>64-66</sup>.</p>     <p><b><i>4. L&iacute;quido c&eacute;falo raqu&iacute;deo (LCR)</i></b>. Es importante el an&aacute;lisis del LCR como soporte para el diagn&oacute;stico. Ocasionalmente los pacientes tienen una pleocitosis con un incremento de las c&eacute;lulas blancas durante el episodio agudo o durante las exacerbaciones. En pacientes con neuro-mielitis aguda por lupus, el LCR se puede confundir con una meningitis bacteriana. El grado de celularidad es muy raro en la esclerosis m&uacute;ltiple. La banda oligoclonal generalmente es negativa en pacientes con enfermedad de Devic.</p>      <p>Ocasionalmente se pueden observar m&aacute;s de 50 gl&oacute;bulos blancos/mm3 durante la exacerbaci&oacute;n de la mielitis aguda, y en el recuento diferencial revela la presencia especialmente de neutr&oacute;filos y puede asociarse con una lesi&oacute;n severa de mielitis, como necrosis. Esta celularidad por neutr&oacute;filo es raro observarla en la esclerosis m&uacute;ltiple<sup>37,41-43,64-66,74,77,78</sup>.</p>     <p>En el 85% de los pacientes con esclerosis m&uacute;ltiple se pueden detectar bandas oligoclonales en el LCR; en cambio, se puede observar solo en el 15% a 35% de las series recientes de los pacientes con NMO. Incremento en la s&iacute;ntesis de IgG casi no se observa en la NMO<sup>41-43, 64-66</sup>.</p>     <p><b><i>5. Pruebas electro-diagn&oacute;sticas</i></b>. Los potenciales evocados visuales ocasionalmente pueden detectar lesiones subcl&iacute;nicas, tienen poco poder diagn&oacute;stico en la NMO.</p>     ]]></body>
<body><![CDATA[<p><font size="3"><b>El espectro de la neuromielitis &oacute;ptica</b></font></p>     <p>Dean M. Wingerchuk y cols.<sup>42</sup> en su publicaci&oacute;n seminal de 2007, titulada <i>The spectrum of neuromyelitis &oacute;ptica</i>, informan acerca de las diferentes variantes en las que se ha informado en los diferentes continentes las formas fenot&iacute;picas de la neuromielitis &oacute;ptica.</p>     <p>    <center>  <font face="Verdana" size="2"><a name="tab2"><img src="img/revistas/rcre/v18n4/v18n4a03t2.jpg"></a></font> </center></p>      <p><font size="3"><b>Neuromielitis &oacute;ptica y el fenotipo de esclerosis m&uacute;ltiple de origen asi&aacute;tico</b></font></p>     <p>La esclerosis m&uacute;ltiple (EM) es una enfermedad inflamatoria desmielinizante del sistema nervioso central, que es desencadenada por una respuesta autoinmunitaria de tipo humoral, cuyo blanco importante es la mielina<sup>59</sup>.</p>     <p>La EM es rara en Asia, pero cuando aparece, compromete los nervios &oacute;pticos y el cord&oacute;n espinal<sup>79</sup>. La EM &oacute;ptico-espinal o EMOE tiene en su presentaci&oacute;n algunas caracter&iacute;sticas cl&iacute;nicas parecidas a la enfermedad de Devic que se observa en la poblaci&oacute;n occidental<sup>79</sup>. De acuerdo con los estudios de Lennon y cols.<sup>52</sup>, en el 2004, al demostrar como la inmunoglobulina IgG se une a algunos tejidos espec&iacute;ficos del sistema nervioso central, pero espec&iacute;ficamente en los pacientes con neuromielitis &oacute;ptica (NMO) o NMO-IgG, se considera que pudiese ser una entidad diferente a la EM. Pero esta afirmaci&oacute;n de Lennon y cols.<sup>52,53</sup> no la pudieron corroborar Nakashima y cols.<sup>70</sup> en el 2006, al estudiar pacientes japoneses con EM, pues informaron la presencia de NMO-IgG en el 60% de los pacientes con EMOE. Sin embargo, los anticuerpos contra NMO-IgG no se observan en todos los casos de NMO o de EMOE y se encuentran solamente en el 10% de los pacientes con EM cl&aacute;sica<sup>80</sup>. Esto pone de presente que establecer una dicotom&iacute;a entre EM y NMO o enfermedad de Devic es complejo y existe una plausibilidad biol&oacute;gica, &eacute;tnica y ambiental en la que puedan coexistir subgrupos de pacientes de EM y NMO que comparten algunas caracter&iacute;sticas cl&iacute;nicas, imagenol&oacute;gicas y de anticuerpos, que hagan dif&iacute;cil separar un cuadro cl&iacute;nico del otro, ya que cuando se describi&oacute; la NMO, se inform&oacute; que ten&iacute;a un curso recidivante, convulsiones jacksonianas, cefalea, hipo severo, v&oacute;mito y disartria, como lo informaron Devic<sup>3,4</sup>, Beck<sup>11</sup>, Balser y Stansbury<sup>12</sup> y otros investigadores m&aacute;s recientes<sup>37,41-43,59,64-66,71,79,81</sup>.</p>     <p><font size="3"><b>Esclerosis m&uacute;ltiple, fenotipo asi&aacute;tico</b></font></p>     <p>Antes de la d&eacute;cada de 1950, la EM se informaba espor&aacute;dicamente en los pa&iacute;ses asi&aacute;ticos. En 1958, Okinaka y cols.<sup>82</sup> informaron que estudiaron 270 pacientes de EM diagnosticada entre 1890 y 1955, y observaron que el 65% de los pacientes era NMO, 24% ten&iacute;an EM, 2% enfermedad de Schilder y otros casos no se pudieron clasificar. Entre los pacientes con NMO, 48% de los pacientes ten&iacute;an un curso recidivante y los investigadores observaron por primera vez unos pacientes que ten&iacute;an una forma intermedia entre EM y NMO<sup>82</sup>. A partir de este estudio, los japoneses denominaron NMO a la forma monof&aacute;sica, es decir, aquellos casos en los que la enfermedad aparece simult&aacute;neamente comprometiendo los nervios &oacute;pticos y la mielitis, o cuando aparece la neuromielitis con un intervalo de menos de varias semanas, mientras que a los casos recidivantes los denominaron EM<sup>82</sup>.</p>     <p>En 1972, Kuroiwa y cols.<sup>83</sup>, en el Jap&oacute;n, en un estudio epidemiol&oacute;gico, revisaron 1.084 pacientes, y encontraron una baja prevalencia de EM. Esto le permiti&oacute; a Shibasaki y cols.<sup>84</sup> estudiar a la poblaci&oacute;n japonesa y a pacientes de origen ingl&eacute;s y establecer una serie de caracter&iacute;sticas de la EM en la poblaci&oacute;n asi&aacute;tica. Estas caracter&iacute;sticas cl&iacute;nicas son: 1) un compromiso severo de los nervios &oacute;pticos y del cord&oacute;n espinal, 2) progresi&oacute;n r&aacute;pida y 3) ocurrencia familiar rara, y no encontraron asociaci&oacute;n a un HLA, pero plantearon la posibilidad de que la EM de origen asi&aacute;tico pudiese ser diferente a la que se observa en la poblaci&oacute;n occidental. Kira y cols.<sup>59,79,85</sup> tienen varias publicaciones sobre este t&oacute;pico y plantean que existe una diferencia entre el EMOE de origen asi&aacute;tico y la EM convencional que se origina en occidente. Describen que en el Jap&oacute;n, entre el 15% y el 40% de los pacientes con EM tienen algunas caracter&iacute;sticas del fenotipo EMOE y se caracterizan por: 1) iniciaci&oacute;n a una edad mayor, 2) m&aacute;s frecuencia en las mujeres, 3) muchas reca&iacute;das, 4) un compromiso severo en los nervios &oacute;pticos y en la m&eacute;dula espinal, con mucha discapacidad, 5) pocas lesiones cerebrales, 6) desarrollo de una mielitis longitudinal extensa en la resonancia magn&eacute;tica, 7) marcada pleocitosis con neutrofilia en el l&iacute;quido cefalorraqu&iacute;deo, 8) ausencia de bandas oligoclonales y 9) el HLA que se ha descrito es el HLA-DPB*0501, a diferencia de la variante occidental que tiene el HLA-DRBI*1501<sup>59,85,86</sup>.</p>     ]]></body>
<body><![CDATA[<p><font size="3"><b>Histopatolog&iacute;a</b></font></p>     <p>Desde las publicaciones de Beck<sup>17</sup> en 1927 y de Stansbury<sup>12</sup> en 1949 se empez&oacute; a describir los hallazgos anatomo-patol&oacute;gicos de la NMO y se not&oacute; la intensa desmielinizaci&oacute;n, la p&eacute;rdida axonal y la proliferaci&oacute;n de la microglia. Posteriormente los estudios de Okinaka y cols.<sup>82</sup>, Hung<sup>87</sup>, Tabira y cols.<sup>88</sup> e Ikuta y cols.<sup>89</sup>, adem&aacute;s de lo anotado m&aacute;s arriba, observaron infiltraci&oacute;n linfoc&iacute;tica perivascular, proliferaci&oacute;n vascular que se advierte en los nervios &oacute;pticos y en el cord&oacute;n espinal generando una lesi&oacute;n necrosante y cavitaciones. De acuerdo con el estudio de Tabira y cols.<sup>88</sup>, quienes practicaron 90 autopsias de EM en el Jap&oacute;n desde 1955 a 1980, se observaron 25 pacientes con la forma cl&aacute;sica, 25 pacientes con enfermedad de Devic y 43 casos con la forma mixta; en esta &uacute;ltima, notaron una severa desmielinizaci&oacute;n con necrosis tisular en los nervios &oacute;pticos y en el cord&oacute;n espinal. Sin embargo, observaron algunas lesiones en el tronco cerebral y en el cerebro. Con estas evidencias histopatol&oacute;gicas es muy dif&iacute;cil diferenciar algunos casos de EM y NMO<sup>88</sup>.</p>     <p><font size="3"><b>Resonancia magn&eacute;tica de la m&eacute;dula espinal</b></font></p>     <p>La mielitis longitudinal que se observa a nivel de la m&eacute;dula espinal puede comprometer m&aacute;s de tres segmentos vertebrales, con poco compromiso cerebral; son las se&ntilde;ales caracter&iacute;sticas que se observan en la NMO en los pa&iacute;ses occidentales, pero no se observan en la EM cl&aacute;sica, aunque s&iacute; en el fenotipo asi&aacute;tico, de acuerdo con los criterios de Barkhof<sup>90</sup>. Pittock y cols.<sup>91</sup> informaron la presencia de lesiones cerebrales asintom&aacute;ticas en la resonancia magn&eacute;tica cerebral en los pacientes con NMO. De acuerdo con estos mismos investigadores, las lesiones cerebrales se observan donde la acuaporina-4 (AQP4) es abundante, como en el dienc&eacute;falo adyacente al tercer ventr&iacute;culo, en el puente y en el cerebelo adyacente al cuarto ventr&iacute;culo<sup>79,91,92</sup>. En esta serie, el 10% de los pacientes con NMO-IgG positivos ten&iacute;an compromiso cerebral, que era indistinguible de las lesiones de la EM, lo que genera una posible sobreposici&oacute;n entre la EM y la NMO.</p>     <p><font size="3"><b>Enfermedad de Devic y lupus</b></font></p>     <p>Deodhar y cols.<sup>93</sup> informaron en 1999 el caso de un paciente que comprometi&oacute; el cord&oacute;n espinal de C3 a T2 y de T7 hasta el cono medular, que ellos describieron como el primer caso de mielitis longitudinal asociado a lupus. Posteriormente, T&eacute;llez-Zenteno y cols.<sup>94</sup> describieron la primera serie de mielopat&iacute;a asociada a lupus, que se clasific&oacute; como mielitis longitudinal. Describieron seis casos, en los que se observ&oacute; una se&ntilde;al extensa en la resonancia magn&eacute;tica a nivel de T2, que compromet&iacute;a varios segmentos del cord&oacute;n espinal y tor&aacute;cico. Cuatro de los pacientes ten&iacute;an anticuerpos anti-cardiolipinas, sugiriendo que podr&iacute;a tratarse de una caracter&iacute;stica de la mielitis longitudinal.</p>     <p>Birnbaum y Kerr<sup>95</sup>, del departamento de Neurolog&iacute;a del Johns Hopkins, en el 2007, informaron el primer caso de anticuerpos IgG anti-NMO que confirm&oacute; el diagn&oacute;stico del s&iacute;ndrome de Devic en un paciente con lupus. Es interesante que el s&iacute;ndrome fuera diagnosticado durante los episodios recurrentes de mielitis longitudinal, antes de presentar el episodio de neuritis &oacute;ptica. A este paciente con anticuerpos IgG anti-NMO con mielitis longitudinal se le administr&oacute; una terapia inmunosupresora agresiva, para evitar los riesgos de las reca&iacute;das<sup>95</sup>.</p>     <p>Paira y cols.<sup>96</sup> en el 2010 informan sobre otros dos pacientes con neuromielitis &oacute;ptica con manifestaciones autoinmunitarias que sugieren lupus con t&iacute;tulos altos de anti IgG-NMO (t&iacute;tulos de 1/ 500). Los pacientes fueron tratados con cinco bolos de metilprednisolona de 1 g y 150 mg de azatioprina/d&iacute;a.</p>     <p>Pittock y cols.<sup>54,</sup> <sup>55</sup> evaluaron la presencia de autoanticuerpos en pacientes de Estados Unidos con NMO y mielitis transversa longitudinal extensa. Se detectaron anticuerpos antinucleares en el 43,8% y anticuerpos Ro en el 15,7%. Ambos tipos de anticuerpos se encontraron m&aacute;s frecuentemente en los pacientes con anticuerpos IgG anti-NMO positivos que en los pacientes con anti-IgG-NMO negativos<sup>54,</sup> <sup>55</sup>.</p>     <p>Si no hay criterios para el diagn&oacute;stico de lupus o s&iacute;ndrome de Sj&ouml;gren primario, la seropositividad para los anticuerpos antinucleares o para los anticuerpos Ro y La no excluye el diagn&oacute;stico para NMO<sup>39,54,55</sup>.</p>     ]]></body>
<body><![CDATA[<p>La frecuencia para la detecci&oacute;n de anticuerpos IgG anti-NMO en pacientes pedi&aacute;tricos con NMO se encontr&oacute; en el 76%<sup>39,</sup> <sup>97</sup>.</p>     <p>Llama la atenci&oacute;n que en el estudio de Pittock y cols.<sup>54</sup> no se encontr&oacute; un solo caso de anticuerpos IgG anti-NMO de los 49 controles con lupus y s&iacute;ndrome de Sj&ouml;gren primario, pero ninguno de estos pacientes ten&iacute;a compromiso de los nervios &oacute;pticos y mielitis<sup>54</sup>.</p>     <p>Informes aislados de pacientes con s&iacute;ndrome antifosfolip&iacute;dico primario<sup>98,99-101</sup>, lupus<sup>95,99-107</sup>, s&iacute;ndrome de Sj&ouml;gren primario<sup>109,110</sup> y endocrinopat&iacute;as autoinmunes<sup>111-113</sup> muestran que actualmente cada vez son m&aacute;s frecuentes los casos con NMO con patolog&iacute;a autoinmune, confirmando la naturaleza autoinmune y lo complejo e interesante de la NMO.</p>     <p><font size="3"><b>Mielitis y lupus</b></font></p>     <p>La mielopat&iacute;a en el lupus es un s&iacute;ndrome inflamatorio grave que compromete el cord&oacute;n espinal lo cual genera debilidad, cuadriparesia, adormecimiento y d&eacute;ficit a nivel de los esf&iacute;nteres<sup>114</sup>. De acuerdo con Theodoridou y Settas<sup>115</sup>, la mielitis puede afectar entre el 1% y el 2% de los pacientes con LES. Este compromiso se considera mil veces m&aacute;s que la prevalencia de mielitis idiop&aacute;tica en la poblaci&oacute;n general, seg&uacute;n los informes de Kaplin y cols.<sup>116</sup>. La mayor&iacute;a de los casos de mielitis en los pacientes con lupus son informes de casos. En los estudios de cohorte sobre mielitis en las enfermedades desmielinizantes se han descrito dos fenotipos diferentes como la esclerosis m&uacute;ltiple y la neuromielitis &oacute;ptica (NMO)<sup>95,97</sup>. Birnbaum y Kerr, del Johns Hopkins, revisaron su cohorte de pacientes y analizaron 22 pacientes. Observaron que 11 pacientes ten&iacute;an compromiso a nivel de la sustancia gris y estos pacientes consultaban por flacidez e hiporeflexia, mientras los otros 11 pacientes que tuvieron una disfunci&oacute;n de la sustancia blanca consultaron por espasticidad e hiporreflexia. Los pacientes con disfunci&oacute;n de la sustancia gris presentaron paraplejia irreversible con un curso monof&aacute;sico o polif&aacute;sico, asociada con una alta actividad del lupus. En los estudios del l&iacute;quido cefalorraqu&iacute;deo era dif&iacute;cil de diferenciarlo de una meningitis bacteriana. Previo a la paraplejia irreversible, estos pacientes consultaban por fiebre y retenci&oacute;n urinaria, generalmente el cuadro cl&iacute;nico se confund&iacute;a con una infecci&oacute;n urinaria. El otro subtipo, en el que hab&iacute;a disfunci&oacute;n de la sustancia blanca, ten&iacute;a neuromielitis &oacute;ptica y se asociaba m&aacute;s con la presencia de anticuerpos anticardiolipinas y anticoagulante l&uacute;pico<sup>95,106,107</sup>.</p>     <p>El anticuerpo IgG anti-NMO fue positivo en cuatro de siete pacientes con mielitis de la sustancia blanca. En cambio en los pacientes en los que se comprometi&oacute; la sustancia gris, fue positivo en uno de ocho pacientes.</p>     <p>Ambos subtipos de mielitis recibieron una inmunosupresi&oacute;n a base de esteroides y ciclofos-famida. Pero a los pacientes en las que se observo una disfunci&oacute;n de la sustancia gris, adem&aacute;s de recibir esteroides y ciclofosfamida, necesitaron plasmaferesis y gamaglobulinas<sup>95,106,107,114</sup>.</p>     <p><font size="3"><b>Tratamiento</b></font></p>     <p>Las recomendaciones terap&eacute;uticas son solo experiencias anecd&oacute;ticas de peque&ntilde;as series de casos no controlados, debido al problema agudo que genera la neuromielitis &oacute;ptica en la forma monof&aacute;sica y en los eventos recidivantes. Los principales objetivos para el tratamiento de la NMO son controlar los ataques agudos, la prevenci&oacute;n de las complicaciones m&eacute;dicas, la rehabilitaci&oacute;n y tratar de prevenir los futuros ataques. Para los pacientes en la crisis monof&aacute;sica y durante las reca&iacute;das agudas se utilizan 1000 mg de metilprednisolona por d&iacute;a, durante cinco d&iacute;as consecutivos<sup>39,41-43,64-66,95,106,107,114</sup>.</p>     <p>En aquellos pacientes que no respondan a los bolos de metilprednisolona, el uso de la plasmaferesis est&aacute; indicado y se pueden utilizar siete recambios de 55 ml/Kg de peso<sup>117-123</sup>. El uso de las gamaglobulinas se ha practicado en algunos casos en forma anecd&oacute;tica<sup>123</sup>. El compromiso medular puede generar una falla respiratoria que requiere que el tratamiento sea realizado en las unidades de terapia intensiva, para su soporte ventilatorio y vigilar el estado de una lesi&oacute;n bulbar. Adem&aacute;s se requieren medidas m&eacute;dicas para prevenir el tromboembolismo pulmonar, la neumon&iacute;a por aspiraci&oacute;n, las infecciones urinarias y las &uacute;lceras por presi&oacute;n.</p>     ]]></body>
<body><![CDATA[<p>En la serie de Mandler y cols.<sup>13</sup>, una vez realizada la inducci&oacute;n de los casos agudos, en el mantenimiento del tratamiento, para evitar las reca&iacute;das, se utiliz&oacute; un esquema basado en prednisona oral y azatioprina 2 mg/Kg/d&iacute;a<sup>13,120,124,125</sup>. La prednisona se va disminuyendo de acuerdo con el estado cl&iacute;nico, hasta una dosis de 10 mg/d&iacute;a. Los autores utilizaron la escala <i>Expanded Disability Status</i> para analizar la mejor&iacute;a en los 18 meses de tratamiento<sup>39</sup>. Tambi&eacute;n se han utilizado bolos de ciclo-fosfamida<sup>126</sup> y mitoxantrone IV<sup>127</sup>. En pacientes con mielitis l&uacute;pica longitudinal y casos de s&iacute;ndrome de Sj&ouml;gren primario y lupus con neuromielitis que no respondan al uso de metil prednisolona en bolos, plasmaferesis y gamaglobulinas, el uso del rituximab se ha hecho en forma anecd&oacute;tica<sup>128-130</sup>.</p> <hr>     <p><font size="3"><b>Referencias</b></font></p>      <!-- ref --><p>1. Allbut TC. On the ophthalmoscopic signs of spinal disease. Lancet 1870;1:76-78.&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=000105&pid=S0121-8123201100040000300001&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --><!-- ref --><p>2. 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