<?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>0121-0793</journal-id>
<journal-title><![CDATA[Iatreia]]></journal-title>
<abbrev-journal-title><![CDATA[Iatreia]]></abbrev-journal-title>
<issn>0121-0793</issn>
<publisher>
<publisher-name><![CDATA[Universidad de Antioquia]]></publisher-name>
</publisher>
</journal-meta>
<article-meta>
<article-id>S0121-07932016000200005</article-id>
<article-id pub-id-type="doi">10.17533/udea.iatreia.v29n2a05</article-id>
<title-group>
<article-title xml:lang="es"><![CDATA[Insuficiencia renal aguda inducida por rabdomiolisis]]></article-title>
<article-title xml:lang="en"><![CDATA[Acute renal failure due to rhabdomyolyisis]]></article-title>
<article-title xml:lang="es"><![CDATA[Insuficiência renal aguda induzida por rabdomiólise]]></article-title>
</title-group>
<contrib-group>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Nieto-Ríos]]></surname>
<given-names><![CDATA[John Fredy]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Vega-Miranda]]></surname>
<given-names><![CDATA[Juliana]]></given-names>
</name>
<xref ref-type="aff" rid="A02"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Serna-Higuita]]></surname>
<given-names><![CDATA[Lina María]]></given-names>
</name>
<xref ref-type="aff" rid="A03"/>
</contrib>
</contrib-group>
<aff id="A01">
<institution><![CDATA[,Universidad de Antioquia  ]]></institution>
<addr-line><![CDATA[Medellín ]]></addr-line>
<country>Colombia</country>
</aff>
<aff id="A02">
<institution><![CDATA[,Hospital Pablo Tobón Uribe  ]]></institution>
<addr-line><![CDATA[Medellín ]]></addr-line>
<country>Colombia</country>
</aff>
<aff id="A03">
<institution><![CDATA[,Universidad de Antioquia  ]]></institution>
<addr-line><![CDATA[Medellín ]]></addr-line>
<country>Colombia</country>
</aff>
<pub-date pub-type="pub">
<day>00</day>
<month>06</month>
<year>2016</year>
</pub-date>
<pub-date pub-type="epub">
<day>00</day>
<month>06</month>
<year>2016</year>
</pub-date>
<volume>29</volume>
<numero>2</numero>
<fpage>157</fpage>
<lpage>169</lpage>
<copyright-statement/>
<copyright-year/>
<self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_arttext&amp;pid=S0121-07932016000200005&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_abstract&amp;pid=S0121-07932016000200005&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_pdf&amp;pid=S0121-07932016000200005&amp;lng=en&amp;nrm=iso"></self-uri><abstract abstract-type="short" xml:lang="es"><p><![CDATA[La insuficiencia renal aguda (IRA) es una causa frecuente de morbilidad y mortalidad en los servicios de urgencias, hospitalización y cuidado crítico, siendo la rabdomiolisis responsable del 15 % de los casos en los centros hospitalarios de alta complejidad. La rabdomiolisis consiste en daño muscular con necrosis y liberación a la circulación de componentes intracelulares, y puede tener múltiples causas. El daño renal por rabdomiolisis es multifactorial e incluye obstrucción tubular, vasoconstricción y daño oxidativo. El tratamiento principal de la IRA por rabdomiolisis es la hidratación, forzar la diuresis y evitar los fármacos nefrotóxicos. Cuando el daño es lo suficientemente grave para causar uremia, acidosis metabólica, hiperpotasemia y sobrecarga de volumen se debe recurrir a la terapia de reemplazo renal. Aunque la regla es que se recupere la función renal, estos pacientes tienen mayor riesgo futuro de desarrollar enfermedad renal crónica.]]></p></abstract>
<abstract abstract-type="short" xml:lang="en"><p><![CDATA[Acute renal failure is a frequent cause of morbidity and mortality in emergency, hospitalization and critical care services. In 15 % of cases it is due to rhabdomyolysis, in which there is breakdown of skeletal muscle with massive necrosis and leakage of muscle cell contents into the circulation. It has many different etiologies. The rhabdomyolysis-induced acute kidney injury results from the combination of several mechanisms, including tubular obstruction, vasoconstriction and oxidative stress. The most important therapeutic measures are: Aggressive repletion of fluids, forced diuresis and avoidance of exposure to nephrotoxic substances. In cases of severe uremia, metabolic acidosis, hiperkalemia or fluid overload it is necessary to start renal replacement therapy. As a rule, kidney function is completely recovered, but these patients have higher risk of future chronic kidney disease.]]></p></abstract>
<abstract abstract-type="short" xml:lang="pt"><p><![CDATA[A insuficiência renal aguda (IRA) é uma causa frequente de morbidade e mortalidade entre os serviços de emergência, internação e cuidados críticos. A rabdomiólise é responsável por 15 % dos casos. Consiste de dano muscular com necrose e liberação à circulação de componentes intercelulares, e pode ter várias causas. O dano renal por rabdomiólise é multifatorial e inclui obstrução tubular, vasoconstrição e dano oxidativo. O principal tratamento da IRA por rabdomiólise é a hidratação, forçar a diurese e evitar fármacos nefrotóxicos. Quando o dano é suficientemente grave para causar uremia, acidose metabólica, hiperpotassemia e sobrecarga de volume se deve recorrer à terapia de substituição renal. Embora a regra é que se recupera a função renal, esses pacientes têm um maior risco futuro de desenvolver doença renal crônica.]]></p></abstract>
<kwd-group>
<kwd lng="es"><![CDATA[Insuficiencia Renal Aguda]]></kwd>
<kwd lng="es"><![CDATA[Mioglobina]]></kwd>
<kwd lng="es"><![CDATA[Músculo Esquelético]]></kwd>
<kwd lng="es"><![CDATA[Necrosis]]></kwd>
<kwd lng="es"><![CDATA[Rabdomiolisis]]></kwd>
<kwd lng="en"><![CDATA[Acute Renal Failure]]></kwd>
<kwd lng="en"><![CDATA[Myoglobin]]></kwd>
<kwd lng="en"><![CDATA[Necrosis]]></kwd>
<kwd lng="en"><![CDATA[Rhabdomyolysis]]></kwd>
<kwd lng="en"><![CDATA[Skeletal Muscles]]></kwd>
<kwd lng="pt"><![CDATA[Insuficiência Renal Aguda, Mioglobina]]></kwd>
<kwd lng="pt"><![CDATA[Músculo Esquelético]]></kwd>
<kwd lng="pt"><![CDATA[Necrose]]></kwd>
<kwd lng="pt"><![CDATA[Rabdomiólise]]></kwd>
</kwd-group>
</article-meta>
</front><body><![CDATA[ <font size="2" face="Verdana, Arial, Helvetica, sans-serif">     <p align="right">DOI <a href="http://dx.doi.org/10.17533/udea.iatreia.v29n2a05" target="_blank">10.17533/udea.iatreia.v29n2a05</a></p>     <p align="right">&nbsp;</p>     <p align="right">&nbsp;</p>     <p align="right"><b>ART&Iacute;CULO DE REVISI&Oacute;N</b></p>     <p>&nbsp;</p>    <p align="center"><font size="4"><b>Insuficiencia renal aguda inducida por rabdomiolisis</b></font></p>     <p>&nbsp;</p>    <p align="center"><font size="3"><b>Acute renal failure due to rhabdomyolyisis</b></font></p>     <p>&nbsp;</p>    ]]></body>
<body><![CDATA[<p align="center"><font size="3"><b>Insufici&ecirc;ncia renal aguda induzida por rabdomi&oacute;lise</b></font></p>     <p align="center">&nbsp;</p>     <p align="center">&nbsp;</p>     <p><b>John Fredy Nieto-R&iacute;os<sup>1</sup>; Juliana Vega-Miranda<sup>2</sup>; Lina Mar&iacute;a Serna-Higuita<sup>3</sup></b></p>     <p>&nbsp;</p>     <p>1 Nefr&oacute;logo, Hospital Pablo Tob&oacute;n Uribe, Universidad de Antioquia, Medell&iacute;n, Colombia.</p>     <p>2 M&eacute;dica Internista, Hospital Pablo Tob&oacute;n Uribe, Medell&iacute;n, Colombia.</p>     <p>3 Nefr&oacute;loga Pediatra, Hospital Pablo Tob&oacute;n Uribe, Universidad de Antioquia, Medell&iacute;n, Colombia. <a href="mailto:lm.serna@hotmail.com">lm.serna@hotmail.com</a></p>     <p>&nbsp;</p>     <p>&nbsp;</p>     ]]></body>
<body><![CDATA[<p>Recibido: marzo 18 de 2015    <br>   Aceptado: agosto 19 de 2015</p>     <p>&nbsp;</p>     <p>&nbsp;</p> <hr size="1" />     <p><b>RESUMEN</b></p>     <p>La insuficiencia renal aguda &#40;IRA&#41; es una causa frecuente de morbilidad y mortalidad en los   servicios de urgencias, hospitalizaci&oacute;n y cuidado cr&iacute;tico, siendo la rabdomiolisis responsable   del 15 &#37; de los casos en los centros hospitalarios de alta complejidad. La rabdomiolisis consiste   en da&ntilde;o muscular con necrosis y liberaci&oacute;n a la circulaci&oacute;n de componentes intracelulares,   y puede tener m&uacute;ltiples causas. El da&ntilde;o renal por rabdomiolisis es multifactorial e incluye   obstrucci&oacute;n tubular, vasoconstricci&oacute;n y da&ntilde;o oxidativo. El tratamiento principal de la IRA por   rabdomiolisis es la hidrataci&oacute;n, forzar la diuresis y evitar los f&aacute;rmacos nefrot&oacute;xicos. Cuando   el da&ntilde;o es lo suficientemente grave para causar uremia, acidosis metab&oacute;lica, hiperpotasemia   y sobrecarga de volumen se debe recurrir a la terapia de reemplazo renal. Aunque la regla es   que se recupere la funci&oacute;n renal, estos pacientes tienen mayor riesgo futuro de desarrollar   enfermedad renal cr&oacute;nica.</p>     <p><b>PALABRAS CLAVE  </b></p>     <p><i>Insuficiencia Renal Aguda, Mioglobina, M&uacute;sculo Esquel&eacute;tico, Necrosis, Rabdomiolisis</i></p> <hr size="1" />     <p><b>SUMMARY</b></p>     <p>Acute renal failure is a frequent cause of morbidity and mortality in emergency, hospitalization   and critical care services. In 15 &#37; of cases it is due to rhabdomyolysis, in which there is breakdown   of skeletal muscle with massive necrosis and leakage of muscle cell contents into the   circulation. It has many different etiologies. The rhabdomyolysis-induced acute kidney injury   results from the combination of several mechanisms, including tubular obstruction, vasoconstriction   and oxidative stress. The most important therapeutic measures are: Aggressive repletion of fluids, forced diuresis and avoidance of exposure to nephrotoxic substances. In cases of severe uremia, metabolic acidosis, hiperkalemia or fluid overload it is necessary to start renal replacement therapy. As a rule, kidney function is completely recovered, but these patients have higher risk of future chronic kidney disease.</p>     ]]></body>
<body><![CDATA[<p> <b>PALABRAS CLAVE  </b></p>     <p><i>Acute Renal Failure, Myoglobin, Necrosis, Rhabdomyolysis,   Skeletal Muscles </i></p>   <hr size="1" />     <p><b>RESUMO</b></p>     <p>A insufici&ecirc;ncia renal aguda &#40;IRA&#41; &eacute; uma causa frequente   de morbidade e mortalidade entre os servi&ccedil;os   de emerg&ecirc;ncia, interna&ccedil;&atilde;o e cuidados cr&iacute;ticos. A rabdomi&oacute;lise   &eacute; respons&aacute;vel por 15 &#37; dos casos. Consiste   de dano muscular com necrose e libera&ccedil;&atilde;o &agrave; circula&ccedil;&atilde;o   de componentes intercelulares, e pode ter v&aacute;rias   causas. O dano renal por rabdomi&oacute;lise &eacute; multifatorial   e inclui obstru&ccedil;&atilde;o tubular, vasoconstri&ccedil;&atilde;o e   dano oxidativo. O principal tratamento da IRA por   rabdomi&oacute;lise &eacute; a hidrata&ccedil;&atilde;o, for&ccedil;ar a diurese e evitar   f&aacute;rmacos nefrot&oacute;xicos. Quando o dano &eacute; suficientemente   grave para causar uremia, acidose metab&oacute;lica,   hiperpotassemia e sobrecarga de volume se deve recorrer   &agrave; terapia de substitui&ccedil;&atilde;o renal. Embora a regra   &eacute; que se recupera a fun&ccedil;&atilde;o renal, esses pacientes t&ecirc;m   um maior risco futuro de desenvolver doen&ccedil;a renal cr&ocirc;nica.</p>     <p> <b>PALAVRAS CHAVE</b></p>     <p> <i>Insufici&ecirc;ncia Renal Aguda, Mioglobina, M&uacute;sculo Esquel&eacute;tico,   Necrose, Rabdomi&oacute;lise</i> </p>       <p>&nbsp;</p>     <p><b>C&oacute;mo citar:</b> Nieto-R&iacute;os JF, Vega-Miranda J, Serna-Higuita LM. Insuficiencia renal aguda inducida por rabdomiolisis. Iatreia. 2016 Abr-Jun;29&#40;2&#41;:157-169. DOI <a href="http://dx.doi.org/10.17533/udea.iatreia.v29n2a05" target="_blank">10.17533/udea.iatreia.v29n2a05</a>.</p> <hr size="1" />     <p>&nbsp;</p>     <p>&nbsp;</p>     ]]></body>
<body><![CDATA[<p><font size="3"><b>INTRODUCCI&Oacute;N</b></font></p>       <p>La rabdomiolisis es un s&iacute;ndrome producido por la lesi&oacute;n   del m&uacute;sculo estriado con liberaci&oacute;n al torrente   sangu&iacute;neo de gran cantidad de productos intracelulares   que pueden afectar varios &oacute;rganos, entre ellos   el coraz&oacute;n y los ri&ntilde;ones &#40;1-4&#41;; aproximadamente 1 de   cada 10.000 personas en EE. UU. puede tener un episodio   de rabdomiolisis en su vida. Su espectro cl&iacute;nico es muy amplio, desde pasar inadvertida hasta tener complicaciones graves, entre ellas arritmias card&iacute;acas, s&iacute;ndrome compartimental, coagulaci&oacute;n intravascular diseminada e insuficiencia renal aguda &#40;IRA&#41; &#40;5&#41;. La asociaci&oacute;n de rabdomiolisis con IRA la describieron por primera vez Bywaters y Beall en la Segunda Guerra Mundial &#40;5,6&#41; y en la actualidad se presenta en 10 &#37; a 40 &#37; de los casos &#40;7&#41;, con prevalencia mayor en hombres &#40;relaci&oacute;n 2:1&#41;. Este art&iacute;culo presenta una revisi&oacute;n de la IRA secundaria a rabdomiolisis.</p>     <p>&nbsp;</p>       <p><font size="3"><b>FISIOPATOLOG&Iacute;A</b></font></p>       <p>Los principales mecanismos fisiopatol&oacute;gicos que explican     la rabdomiolisis son el trauma directo de la     fibra muscular y la depleci&oacute;n del ATP muscular. En     estado fisiol&oacute;gico la concentraci&oacute;n de Na<sup>+</sup> extracelular     se mantiene por el funcionamiento adecuado     de la bomba Na<sup>+</sup> K<sup>+</sup> ATP-asa, que extrae sodio de la     c&eacute;lula &#40;5,8&#41;; secundario a ello aumentan las cargas     negativas en el espacio intracelular &#40;recu&eacute;rdese que     el recambio es de 3 mol&eacute;culas de Na<sup>+</sup> por 2 mol&eacute;culas     de K<sup>+</sup>&#41;. Durante el proceso de contracci&oacute;n muscular,     el sodio entra a la c&eacute;lula intercambi&aacute;ndose     luego por calcio &#40;Ca<sup>++</sup>&#41; mediante otro cotransportador     de la membrana celular que tambi&eacute;n depende     de ATP; de igual manera, la c&eacute;lula mantiene bajas     concentraciones de Ca<sup>++</sup> &#40;0,12 mmol/L&#41; gracias a     transportadores que introducen este cati&oacute;n al ret&iacute;culo     sarcopl&aacute;smico y a la mitocondria &#40;9&#41;. Cuando     hay una lesi&oacute;n muscular se presenta isquemia tisular,     que se explica por la disminuci&oacute;n del flujo sangu&iacute;neo     o porque las demandas de ox&iacute;geno superan     los suministros; como consecuencia, se reduce considerablemente     la producci&oacute;n de ATP lo que lleva al     mal funcionamiento de los transportadores i&oacute;nicos,     con aumento de la concentraci&oacute;n de sodio y calcio     intracelular e intramitocondrial &#40;1,27 mml/L&#41; &#40;9&#41;. El     calcio, por su parte, activa la fosfolipasa A2 y las     proteasas; adem&aacute;s, ocasiona contracci&oacute;n muscular     prolongada y disfunci&oacute;n mitocondrial &#40;7&#41;; finalmente,     hay ruptura del sarcolema &#40;membrana celular     muscular&#41; y liberaci&oacute;n de gran cantidad de componentes     celulares al torrente sangu&iacute;neo &#40;iones, mioglobina,     tromboplastina&#41;, sustancias responsables de     las manifestaciones cl&iacute;nicas de la rabdomiolisis &#40;8&#41;   &#40;<a href="img/revistas/iat/v29n2/v29n2a05f1.jpg" target="_blank">figuras 1</a> y <a href="#f2">2</a>&#41;. </p>       <p align="center"><a name="f2"></a><img src="/img/revistas/iat/v29n2/v29n2a05f2.jpg"></p>       <p>El da&ntilde;o renal secundario a rabdomiolisis se explica     por tres mecanismos fisiopatol&oacute;gicos &#40;10&#41;: constricci&oacute;n     de vasos renales, lesi&oacute;n oxidativa mediada por la     mioglobina y obstrucci&oacute;n tubular.    </p>       <p><b>Vasoconstricci&oacute;n </b></p>       <p>Durante la rabdomiolisis hay una disminuci&oacute;n multifactorial     del flujo sangu&iacute;neo renal; el m&uacute;sculo lesionado     se convierte en un tercer espacio al atrapar     grandes cantidades de l&iacute;quido, ocasionando hipoperfusi&oacute;n     sist&eacute;mica, que a su vez lleva a la activaci&oacute;n     adren&eacute;rgica y del sistema renina angiotensina aldosterona   &#40;RAAS&#41; &#40;11&#41;; por otro lado, la mioglobina, al     actuar sobre el &aacute;cido araquid&oacute;nico, libera sustancias     como F2-isoprostanos, endotelina-1 y tromboxano-     A2 que promueven la vasoconstricci&oacute;n; finalmente,     hay disminuci&oacute;n generalizada del &oacute;xido n&iacute;trico &#40;vasodilatador     natural&#41; &#40;1,10-12&#41;.    </p>       <p><b>Lesi&oacute;n oxidativa</b> </p>       ]]></body>
<body><![CDATA[<p>Esta lesi&oacute;n se presenta por un aumento en la filtraci&oacute;n     de mioglobina que supera la capacidad de reabsorberla     en el t&uacute;bulo proximal &#40;7&#41;; esto lleva a acumulaci&oacute;n tanto     de la mioglobina como de sus componentes, entre     ellos el hierro. La liberaci&oacute;n de hierro genera radicales     libres &#40;reacci&oacute;n de Fenton&#41; que causan peroxidaci&oacute;n lip&iacute;dica,     da&ntilde;o de las membranas celulares &#40;10&#41; y muerte     celular; por otro lado, hay quimiotaxis de neutr&oacute;filos     con presencia de inflamaci&oacute;n local y perpetuaci&oacute;n del     da&ntilde;o y posteriormente da&ntilde;o por reperfusi&oacute;n &#40;11&#41;.</p>       <p> <b>Obstrucci&oacute;n tubular </b></p>       <p>La acidez es una condici&oacute;n obligada para el dep&oacute;sito y     toxicidad tubular por mioglobina. Un individuo hipoperfundido     es un paciente acid&oacute;tico que l&oacute;gicamente     produce orina &aacute;cida como medida salvadora para liberarse     de las altas cargas de hidrogeniones. Una vez     la mioglobina alcanza los t&uacute;bulos renales, su concentraci&oacute;n     intraluminal es cada vez mayor; esto, sumado     a un pH urinario &aacute;cido, lleva a una interacci&oacute;n entre     la mioglobina y las prote&iacute;nas de Tamm Horsfall, y a la     producci&oacute;n de cilindros intraluminales que obstruyen     el flujo urinario &#40;7&#41;.</p> 	    <p>&nbsp;</p>       <p><font size="3"><b>ETIOLOG&Iacute;A DE LA RABDOMIOLISIS</b></font></p>       <p>Para facilitar el estudio y enfoque de un paciente     con rabdomiolisis se han establecido 8 categor&iacute;as de     causas o eventos iniciadores que se deben buscar minuciosamente     para establecer un tratamiento oportuno;     son las siguientes: trauma, ejercicio, hipoxia     muscular, defectos gen&eacute;ticos, temperaturas extremas,     infecciones, trastornos metab&oacute;licos o electrol&iacute;ticos,     drogas y toxinas &#40;1,7,10-13&#41; &#40;<a href="img/revistas/iat/v29n2/v29n2a05t1.jpg" target="_blank">tabla 1</a>&#41;. Entre ellas, las     toxinas ex&oacute;genas son la principal causa con repercusi&oacute;n     cl&iacute;nica, responsables de hasta 46 &#37; de los casos     que requieren hospitalizaci&oacute;n &#40;drogas il&iacute;citas, alcohol y medicamentos prescritos&#41; &#40;4&#41;. Entre los medicamentos,     los m&aacute;s a menudo implicados son las estatinas,     los antipsic&oacute;ticos, los inhibidores de la recaptaci&oacute;n de     serotonina y los antihistam&iacute;nicos; con frecuencia la     interacci&oacute;n de varios medicamentos es lo que desencadena     el problema, como por ejemplo la combinaci&oacute;n     de estatinas con fibratos. Los defectos metab&oacute;licos     del m&uacute;sculo son responsables del 10 &#37; de los casos     de rabdomiolisis y los pacientes portadores de estos     defectos son los que m&aacute;s riesgo tienen de recurrencia     o de que ciertos medicamentos o toxinas la desencadenen.     Para tener en cuenta, en el 60 &#37; de los casos     interviene m&aacute;s de una causa y hasta en el 10 &#37; no se     encuentran factores de riesgo asociados. </p>       <p><b>Trauma    </b></p>       <p>La mayor parte de la evidencia disponible acerca     de IRA inducida por rabdomiolisis se ha desarrollado     a partir de pacientes traumatizados &#40;14&#41;. Durante     los grandes desastres naturales, como por ejemplo     los terremotos, aparece la rabdomiolisis como una     pandemia. El otro escenario relacionado son los accidentes     de tr&aacute;nsito. Sin embargo, tambi&eacute;n debe sospecharse     rabdomiolisis en los pacientes con quemaduras     el&eacute;ctricas y con picaduras extensas. Durante todos     los procesos hay una ruptura mec&aacute;nica del sarcolema     con liberaci&oacute;n subsecuente de sustancias al torrente     sangu&iacute;neo &#40;15,16&#41;. </p>       <p><b>Ejercicio excesivo y aumento de la actividad     muscular &#40;17&#41;    </b></p>       <p>Se presenta en los pacientes cuya tasa de metabolismo     de glucosa excede la capacidad oxidativa, lo que lleva     a acumulaci&oacute;n de piruvato y a acidosis l&aacute;ctica &#40;18&#41;.     Normalmente se desarrolla en pacientes con desacondicionamiento     f&iacute;sico basal incluso con esfuerzos     aer&oacute;bicos peque&ntilde;os, o en individuos entrenados que     hacen actividad f&iacute;sica bajo condiciones extremas de     calor y humedad &#40;19-22&#41;.    </p>       ]]></body>
<body><![CDATA[<p><b>Hipoxia muscular    </b></p>       <p>Se produce cuando hay desequilibrio entre el aporte     de ox&iacute;geno y la demanda muscular del mismo,     como en la isquemia arterial, enfermedad en la que     hay poco suministro de ox&iacute;geno por la hipoperfusi&oacute;n;     en estos casos se desarrolla una lesi&oacute;n muscular con     edema intersticial que en condiciones extremas puede     terminar en un s&iacute;ndrome compartimental. En los     procedimientos quir&uacute;rgicos puede operar el mismo     mecanismo pues la hipotensi&oacute;n desencadena hipoperfusi&oacute;n     tisular; hay mayor riesgo en las cirug&iacute;as de     larga duraci&oacute;n, en posiciones inc&oacute;modas y con uso     prolongado del torniquete &#40;23&#41;.    </p>       <p><b>D&eacute;ficits enzim&aacute;ticos musculares</b> </p>       <p>Las llamadas miopat&iacute;as metab&oacute;licas &#40;1&#41; ocurren en     pacientes con alteraci&oacute;n en la v&iacute;a del gluc&oacute;geno, l&iacute;pidos     u otras v&iacute;as metab&oacute;licas. Se caracterizan porque     los pacientes desde la infancia presentan intolerancia     al ejercicio, mialgias y episodios repetidos de     rabdomiolisis. Las principales causas son el d&eacute;ficit de     carnitil-palmitoil-transferasa y el de miofosforilasa   &#40;enfermedad de McArdle&#41;.    </p>       <p><b>Infecciones</b> </p>       <p>Existen informes de casos de rabdomiolisis asociados a     infecciones: influenza A y B, virus Coxsackie, virus de     Epstein-Barr, VIH, <i>Legionella, Streptococcus pyogenes,     Staphylococcus aureus </i>y citomegalovirus &#40;24&#41;. En la     reciente pandemia de influenza H1N1 se publicaron     art&iacute;culos seg&uacute;n los cuales 62 &#37; de los pacientes con     neumon&iacute;a y falla respiratoria ten&iacute;an elevaci&oacute;n de la     creatina-fosfoquinasa &#40;CPK&#41; &#40;18,23&#41;. Al parecer, existe     da&ntilde;o de los dominios nucleares inducido por prote&iacute;nas     virales. Se han encontrado otros casos asociados a dengue     hemorr&aacute;gico &#40;25-27&#41; y a picaduras de avispas &#40;28&#41;.    </p>       <p><b>Cambios en la temperatura corporal    </b></p>       <p>En los pacientes con quemaduras se combinan varios     factores de riego asociados a rabdomiolisis tales     como sepsis, acidosis, hiperpotasemia y formaci&oacute;n de     terceros espacios. La rabdomiolisis secundaria a lesiones     t&eacute;rmicas se asocia con alta mortalidad. En unidades     de cuidados intensivos la tasa de mortalidad es     del 22 &#37; en los pacientes sin IRA asociada, pero puede     llegar hasta el 59 &#37; cuando s&iacute; la hay &#40;25&#41;.    </p>       <p><b>Trastornos electrol&iacute;ticos y endocrinos</b></p>       <p> En general, estos trastornos alteran el funcionamiento     de las bombas dependientes de ATP y generan variaci&oacute;n     en las concentraciones intracelulares y extracelulares     de cada uno de los iones. En condiciones como     la hiperglicemia y la osmolaridad alta, se altera el     metabolismo aer&oacute;bico de la fibra muscular y a su vez     el estado de deshidrataci&oacute;n lleva a disminuci&oacute;n de la     volemia y a la alteraci&oacute;n subsecuente de la perfusi&oacute;n.    </p>       ]]></body>
<body><![CDATA[<p><b>Medicamentos    </b></p>       <p>En la actualidad existen m&aacute;s de 150 medicamentos     relacionados con la aparici&oacute;n de rabdomiolisis; de     ellos las estatinas son los implicados con mayor frecuencia   &#40;29&#41;; se calcula que hasta 0,1 &#37; de los pacientes     que usan estatinas presentan rabdomiolisis, especialmente     aquellos con enfermedad hep&aacute;tica o renal,     hipotiroidismo, diabetes mellitus y polimedicaci&oacute;n   &#40;11&#41;; al parecer, las estatinas inducen rabdiomiolisis     por el bloqueo de la s&iacute;ntesis de colesterol lo que a su     vez disminuye el colesterol en el sarcolema &#40;5&#41;; otros     autores proponen que estos medicamentos inducen     apoptosis de la fibra muscular. Los s&iacute;ntomas aparecen     de 1 a 4 semanas despu&eacute;s de iniciada la medicaci&oacute;n y     mejoran entre 1 y 30 d&iacute;as despu&eacute;s de suspenderla &#40;30&#41;.     La daptomicina, antibi&oacute;tico utilizado con frecuencia     en pacientes con disfunci&oacute;n renal, es otro de los medicamentos     relacionados con rabdomiolisis; un estudio     Fase I encontr&oacute; elevaci&oacute;n de la CPK hasta en 2,8 &#37; de los pacientes y miopat&iacute;a establecida en 0,2 &#37;; los     autores sugieren una dosis de 6 mg/kg administrada     una sola vez al d&iacute;a para evitar ese efecto indeseable   &#40;31&#41;. Se ha reportado adem&aacute;s la presencia de rabdomiolisis     con el uso de ciprofloxacina, con toxicidad     proporcional al tiempo de exposici&oacute;n &#40;31,32&#41;; otros     medicamentos asociados a esta enfermedad son: salicilatos,     teofilina, antidepresivos y fibratos especialmente     cuando se asocian a estatinas &#40;5,33-40&#41;.</p>       <p> <b>Drogas y toxinas </b></p>       <p>Sustancias como el etanol y la coca&iacute;na causan lesi&oacute;n     muscular directa que se potencia con la inmovilizaci&oacute;n     prolongada; cabe tener en cuenta que el consumo     de estas sustancias generalmente se hace de     manera concomitante &#40;5&#41;. La hero&iacute;na es otra de las     sustancias asociadas con la rabdomiolisis &#40;4&#41;.    </p>       <p><b>Enfermedades autoinmunes</b> </p>       <p>Se presenta rabdomiolisis por la destrucci&oacute;n de prote&iacute;nas     del sarcolema secundaria a la formaci&oacute;n de     autoanticuerpos.    </p> 	    <p>&nbsp;</p>       <p><font size="3"><b>MANIFESTACIONES CL&Iacute;NICAS</b></font></p>       <p>En el paciente con IRA secundaria a rabdomiolisis     predominan los s&iacute;ntomas debidos a la destrucci&oacute;n     muscular como mialgias, edema, rigidez, orina color     de t&eacute;, deshidrataci&oacute;n, hipovolemia y s&iacute;ntomas generales   &#40;5&#41;, sin embargo, hasta el 50 &#37; de los pacientes     son asintom&aacute;ticos o cursan con s&iacute;ntomas inespec&iacute;ficos   &#40;11&#41;. En cuanto al da&ntilde;o renal, puede presentarse     3-7 d&iacute;as despu&eacute;s de la lesi&oacute;n muscular, pero los trastornos     electrol&iacute;ticos pueden preceder a la oliguria y la     elevaci&oacute;n de los compuestos azoados.</p>       <p> Los siguientes son los principales factores de riesgo para     desarrollar da&ntilde;o renal por rabdomiolisis: da&ntilde;o muscular     grave, edad avanzada, diabetes mellitus, deshidrataci&oacute;n,     hiperuricemia, acidosis, sepsis, enfermedad renal     cr&oacute;nica, polimedicaci&oacute;n y estado hiperosmolar &#40;11&#41;.    </p>       ]]></body>
<body><![CDATA[<p>Se debe tener en cuenta que cuando un paciente     desarrolla da&ntilde;o renal por rabdomiolisis es porque el     da&ntilde;o muscular es extenso y, por tanto, generalmente     hay compromiso de otros &oacute;rganos y sistemas lo     que causa, por ejemplo: s&iacute;ndrome compartimental,     coagulaci&oacute;n intravascular diseminada &#40;liberaci&oacute;n de     tromboplastina&#41; y arritmias card&iacute;acas &#40;1,5,7,10-12&#41;.    </p> 	    <p>&nbsp;</p>       <p><font size="3"><b>DIAGN&Oacute;STICO</b></font></p>       <p>Para el diagn&oacute;stico de rabdomiolisis se recomiendan     las siguientes pruebas de laboratorio:    </p>       <p><b>Enzimas musculares    </b></p>       <p><i>Creatina fosfoquinasa &#40;CPK&#41;</i>: se eleva 2 a 12 horas despu&eacute;s     de la lesi&oacute;n muscular, con un pico m&aacute;ximo entre     las 24 y 72 horas. El diagn&oacute;stico de rabdomiolisis     se hace al elevarse la CPK 5 veces sobre su nivel normal   &#40;41&#41; y dicho nivel se relaciona con la presencia de     IRA. En 1994, Veenstra-Smith estudiaron 93 pacientes     con rabdomiolisis con el fin de definir la incidencia,     la mortalidad y el comportamiento de la insuficiencia     renal; encontraron que un valor de CPK mayor de     15.000 UI/L versus uno entre 5000-15.000 UI/L se asociaba     con mayor riesgo de desarrollar IRA &#40;42&#41;. En 2003     Meijer y Fikkers hicieron un estudio de cohorte para     observar los factores de riesgo para desarrollar insuficiencia     renal en rabdomiolisis; encontraron, de igual     manera, que niveles de CPK por encima de 10.000 UI/L     se asociaban a un mayor riesgo de desarrollarla &#40;43&#41;.     Rodr&iacute;guez y colaboradores hicieron un estudio de cohorte     retrospectiva en 126 pacientes que presentaron     rabdomiolisis, en ellos se encontr&oacute; que un punto de     corte de CPK mayor de 12.750 UI/L ten&iacute;a un OR de 4,9     de presentar IRA &#40;IC95 &#37;: 1,4-16,8; p &#60; 0,01&#41; &#40;4&#41;    </p>       <p><b>Mioglobina</b></p>       <p> Prote&iacute;na de 17,8 kDa cuya concentraci&oacute;n s&eacute;rica normal     oscila entre 0 y 0,003 mg/dL &#40;5&#41;; su funci&oacute;n es el     transporte de ox&iacute;geno en el m&uacute;sculo; se reabsorbe     en el t&uacute;bulo proximal por endocitosis &#40;44&#41;; posteriormente     es metabolizada y sus componentes se degradan     y el hierro se almacena en forma de ferritina &#40;12&#41;.     Debido a que el tejido muscular representa el 40 &#37; del     peso total &#40;45&#41;, cuando se presenta una destrucci&oacute;n     muscular mayor de 100 gramos se libera una gran     cantidad de mioglobina que supera la capacidad de     uni&oacute;n a prote&iacute;nas plasm&aacute;ticas y esto hace que se filtre     en el glom&eacute;rulo &#40;5&#41;, pero sin que se logre su reabsorci&oacute;n completa en el t&uacute;bulo proximal &#40;supera el dintel renal     de 0,5 a 1,5 mg/dL&#41; &#40;12&#41;.</p>       <p> La mioglobina aumenta m&aacute;s r&aacute;pido que la CPK, pero     disminuye en 1 a 24 horas &#40;46&#41;. Por lo anterior la mioglobina     es menos sensible y si es negativa no excluye     el diagn&oacute;stico de rabdomiolisis. Idealmente debe medirse     por radioinmunoensayo, pero el resultado tarda     m&aacute;s de 24 horas lo que limita su uso en la pr&aacute;ctica     cl&iacute;nica. La mioglobina parece tener un papel en determinar     el pron&oacute;stico de la lesi&oacute;n renal asociada a     rabdomiolisis, pero este beneficio no est&aacute; muy bien     establecido &#40;42,43,45,47-49&#41;.    </p>       <p><b>Otras enzimas    </b></p>       ]]></body>
<body><![CDATA[<p>Tambi&eacute;n se puede encontrar elevaci&oacute;n de lactato deshidrogenasa   &#40;LDH&#41;, aspartato aminotransferasa &#40;AST&#41;,     aldolasa y troponina T hasta en 50 &#37; de los casos &#40;5&#41;.    </p>       <p><b>Productos nitrogenados </b></p>       <p>Los principales criterios para evidenciar el da&ntilde;o renal     por rabdomiolisis son los valores elevados de nitr&oacute;geno     ureico &#40;BUN&#41; y creatinina s&eacute;rica. En los estadios     iniciales la relaci&oacute;n BUN/creatinina se encuentra baja     por aumento de la creatinina en sangre secundaria al     catabolismo muscular; en los estadios tard&iacute;os la mioglobina     se metaboliza a urea por lo cual la relaci&oacute;n     BUN/creatinina aumenta en forma desproporcionada     con respecto a las lesiones renales por otras causas   &#40;15,16,18,23,25,30-33,42,43,45,47-49&#41;.    </p>       <p><b>Citoqu&iacute;mico de orina </b></p>       <p>La orina presenta una coloraci&oacute;n oscura denominada     ''coloraci&oacute;n t&eacute;''. La tirilla es positiva para sangre, pero     en el estudio microsc&oacute;pico no se observan eritrocitos.     Adem&aacute;s, se observan cilindros granulosos, pigmentados     y epiteliales.    </p>       <p><b>Fracci&oacute;n excretada de sodio &#40;FeNa&#41;    </b></p>       <p>Inicialmente es menor del 1 &#37;, con sodio urinario menor     de 20 mEq/L en la etapa de vasoconstricci&oacute;n &#40;50&#41;.     Posteriormente, por el da&ntilde;o tubular, la FeNA es mayor     del 2 &#37; y el sodio urinario sobrepasa los 30 mEq/L.    </p>       <p><b>Electr&oacute;litos, gasometr&iacute;a y &aacute;cido &uacute;rico </b></p>       <p><i>Potasio:</i> se observa hiperpotasemia que es la principal     responsable de la toxicidad card&iacute;aca &#40;con cada     100 gramos de m&uacute;sculo lesionado aumenta 1 mEq el     potasio&#41; y que se potencia por la IRA.    </p>       <p><i>F&oacute;sforo:</i> se libera a la circulaci&oacute;n por la destrucci&oacute;n     muscular y genera hiperfosfatemia; esto a su vez favorece     la hipocalcemia por precipitaci&oacute;n.  </p>       ]]></body>
<body><![CDATA[<p><i>&Aacute;cido &uacute;rico:</i> se encuentra elevado por la destrucci&oacute;n     muscular.</p>       <p> <i>Calcio:</i> generalmente hay hipocalcemia en los estadios     iniciales lo que potencia la cardiotoxicidad.    </p>       <p><i>Gasometr&iacute;a arterial: </i>se observa acidosis metab&oacute;lica     con ani&oacute;n gap elevado.    </p>       <p>&nbsp;</p>       <p><font size="3"><b>TRATAMIENTO Y PREVENCION DE LA IRA INDUCIDA     POR RABDOMIOLISIS</b></font></p>       <p>Tiene 4 pilares fundamentales:    </p>       <p>1. Identificaci&oacute;n y tratamiento de la causa espec&iacute;fica,     lo que incluye la suspensi&oacute;n de los medicamentos     o toxinas implicados para evitar la perpetuaci&oacute;n     del da&ntilde;o renal.    </p>       <p>2. Hidrataci&oacute;n y manejo de las complicaciones electrol&iacute;ticas     y del desequilibrio &aacute;cido base.    </p>       <p>3. Evitar cualquier tipo de f&aacute;rmaco nefrot&oacute;xico y     ajustar las dosis de los medicamentos de acuerdo     con la funci&oacute;n renal del paciente.    </p>       <p>4. Terapias de soporte renal cuando haya da&ntilde;o renal     grave.</p>       ]]></body>
<body><![CDATA[<p> A continuaci&oacute;n se hace &eacute;nfasis en las intervenciones     espec&iacute;ficas:    </p>       <p><b>Hidrataci&oacute;n</b></p>       <p> Es indudable el beneficio de la expansi&oacute;n del volumen     en la prevenci&oacute;n y tratamiento de la nefropat&iacute;a     inducida por pigmentos, entre ellos el aumento del     flujo sangu&iacute;neo tubular, la disminuci&oacute;n de la acidez     plasm&aacute;tica y urinaria y la mejor&iacute;a de la perfusi&oacute;n     muscular. En los primeros d&iacute;as se requieren vol&uacute;menes     tan altos como de 10 litros de soluci&oacute;n salina al d&iacute;a &#40;12&#41;; por este motivo es muy importante tener     en cuenta el estado cardiovascular del paciente, en     especial si se encuentra en la fase olig&uacute;rica de la lesi&oacute;n     renal; el objetivo de la hidrataci&oacute;n es mantener     un gasto urinario de 200 a 300 mL/hora &#40;2 a 3 mL/kg/     hora&#41; &#40;12&#41;. Los l&iacute;quidos endovenosos &#40;LEV&#41; se deben     suministrar hasta lograr valores de CPK por debajo de     1000 &#40;5&#41;; se recomienda no usar soluciones con potasio     ni lactato &#40;5&#41;.    </p>       <p><b>Manejo de la hiperpotasemia    </b></p>       <p>Se deben detectar precozmente las alteraciones del     ritmo card&iacute;aco secundarias a la hiperpotasemia; si est&aacute;n     presentes, es necesario administrar calcio intravenoso.     Otras medidas utilizadas son las siguientes:  </p>       <p>&#8226; Redistribuci&oacute;n del potasio: para lograr esto se utilizan     agonistas de los receptores B2 e infusi&oacute;n de     insulina + dextrosa.</p>       <p> &#8226; Eliminaci&oacute;n gastrointestinal de potasio: para esto     se utilizan resinas de intercambio i&oacute;nico como el     poliestireno; administrar concomitantemente un     laxante que facilite su eliminaci&oacute;n.  </p>       <p>&#8226; Ver adelante indicaciones de uso de diur&eacute;ticos y     terapia de reemplazo renal &#40;9,10,12&#41;.    </p>       <p><b>Diur&eacute;ticos </b></p>       <p><i>Furosemida:</i> se utiliza para forzar la diuresis, pero hay     controversia acerca de su empleo porque puede disminuir     a&uacute;n m&aacute;s el pH en los t&uacute;bulos renales distales     potenciando la nefrotoxicidad de la mioglobina. Otros     autores sugieren utilizar dosis tituladas una vez que el     paciente alcance un estado adecuado de hidrataci&oacute;n.     Aunque todav&iacute;a no est&aacute; claro, parece existir un beneficio     con el uso de la acetazolamida porque este medicamento     disminuye la reabsorci&oacute;n proximal del bicarbonato     aumentando el pH intraluminal; sin embargo,     a&uacute;n no hay evidencia concluyente al respecto &#40;51&#41;.    </p>       ]]></body>
<body><![CDATA[<p><b>Alcalinizaci&oacute;n de la orina </b></p>       <p><i>Bicarbonato:</i> se utiliza con el fin de mantener el pH     urinario por encima de 6,5 para as&iacute; aumentar la solubilidad     de la mioglobina y el &aacute;cido &uacute;rico y evitar     las lesiones renales secundarias a la acumulaci&oacute;n     de ambas sustancias; sin embargo, los estudios no     son concluyentes en los desenlaces cl&iacute;nicamente     importantes como mortalidad o necesidad de terapia     de reemplazo renal &#40;1,7,9-12,15,16,18,23,25,30-     33,42,43,45,47-52&#41;. Antes de usarlo se debe verificar     que el paciente no tenga alcalosis metab&oacute;lica o hipocalcemia     significativa y se recomienda obtener una     concentraci&oacute;n de bicarbonato de 130 mEq/L mezclado     en dextrosa al 5 &#37; o en agua destilada. Se inicia     con una infusi&oacute;n de 200 mL/hora y se ajusta con el     fin de alcanzar un pH urinario mayor de 6,5. Se debe     suspender este tratamiento si hay hipocalcemia sintom&aacute;tica     o alcalosis metab&oacute;lica con pH por encima de     7,5 o HCO<sub>3</sub> mayor de 30 mmol/L.    </p>       <p><b>Manitol    </b></p>       <p>Su beneficio te&oacute;rico radica en la capacidad de inducir     vasodilataci&oacute;n en el par&eacute;nquima renal y actuar como     antioxidante al atrapar radicales libres, pero los estudios     no son concluyentes; posiblemente los pacientes     que m&aacute;s se benefician son los que tienen valores de     CPK por encima de 30.000 UI/L &#40;7&#41;. Se utiliza a la dosis     de 1 a 2 gramos por kilogramo d&iacute;a, con una velocidad     de infusi&oacute;n de 5 gramos por hora. Est&aacute; contraindicado     en los pacientes deshidratados, hipovol&eacute;micos o     que cursen con oliguria.    </p>       <p><b>Alopurinol</b> </p>       <p>En caso de hiperuricemia por encima de 8 mg/dL en     el contexto de IRA por rabdomiolisis se recomienda     usar alopurinol, aunque no hay estudios que avalen     tal conducta en estos pacientes.    </p>       <p><b>Otros medicamentos</b></p>       <p> De acuerdo con los mecanismos fisiopatol&oacute;gicos descritos,     se estudian m&uacute;ltiples v&iacute;as para intervenir, por     ejemplo:  </p>       <p>&#8226; L arginina para contrarrestar la deficiencia relativa     de &oacute;xido n&iacute;trico &#40;9&#41;.</p>       <p> &#8226; Fasudil como inhibidor de la apoptosis de c&eacute;lulas     renales &#40;53&#41;.  </p>       ]]></body>
<body><![CDATA[<p>&#8226; Esteroides en la rabdomiolisis inducida por alcohol   &#40;54&#41;.</p>       <p> &#8226; Vitamina C como antioxidante &#40;55&#41;.  </p>       <p>&#8226; Eritropoyetina &#40;56&#41;.    </p>       <p><b>Terapia de reemplazo renal    </b></p>       <p>Es necesaria en pacientes olig&uacute;ricos &#40;85 &#37; de los pacientes     olig&uacute;ricos requieren terapia de reemplazo renal     frente a 30 &#37; de los no olig&uacute;ricos&#41; &#40;7&#41;; otras indicaciones     para iniciarla son las siguientes:  </p>       <p>&#8226; Hiperpotasemia mayor de 6,5 mEq/L resistente al     tratamiento m&eacute;dico, con cambios en el electrocardiograma.</p>       <p> &#8226; Oliguria persistente o anuria.  </p>       <p>&#8226; Uremia marcada, en general BUN por encima de     80 mg/dL y creatinina mayor de 5 mg/dL.  </p>       <p>&#8226; Complicaciones ur&eacute;micas como sangrado, encefalopat&iacute;a,     pericarditis o polineuropat&iacute;a.</p>       <p> &#8226; Sobrecarga de volumen con afectaci&oacute;n pulmonar.  </p>       ]]></body>
<body><![CDATA[<p>&#8226; Acidosis metab&oacute;lica &#40;pH menor de 7,1&#41;, resistente     al tratamineto m&eacute;dico.    </p>       <p>Debe tenerse en cuenta que la hemodi&aacute;lisis convencional     no remueve la mioglobina por el tama&ntilde;o de     la part&iacute;cula; esto solo puede lograrse con di&aacute;lisis con     filtros de alta permeabilidad &#40;57,58&#41;. Se recomienda     suspender la terapia de reemplazo renal cuando el     paciente inicie la recuperaci&oacute;n de la funci&oacute;n renal,     con una depuraci&oacute;n adecuada de productos nitrogenados   &#40;45&#41; y una vez comience la fase poli&uacute;rica.    </p>       <p>&nbsp;</p>       <p><font size="3"><b>PRON&Oacute;STICO</b></font></p>       <p>La regla es la recuperaci&oacute;n de la funci&oacute;n renal. Entre     1980 y 1993 se llev&oacute; a cabo un estudio de seguimiento     a 14 a&ntilde;os de estos pacientes y se encontr&oacute; una tasa de     supervivencia del 78,6 &#37; &#40;8&#41;. La mayor&iacute;a de los pacientes     recuperan la funci&oacute;n renal en un tiempo promedio     de 3 semanas, pero es importante tener en cuenta el     contexto cl&iacute;nico ya que no es lo mismo un paciente     con rabdomiolisis aislada, que uno con rabdomiolisis     en el marco de una falla org&aacute;nica multisist&eacute;mica en la     unidad de cuidados intensivos &#40;59&#41;. Adem&aacute;s, est&aacute; demostrado     que la IRA es un factor de riesgo independiente     para desarrollar falla renal cr&oacute;nica en el futuro.</p> 	    <p>&nbsp;</p>       <p> <font size="3"><b>NUEVOS MARCADORES DE FALLA RENAL Y     RABDOMIOLISIS</b></font></p>       <p><b>Factor de crecimiento fibrobl&aacute;stico 23 &#40;FGF-23&#41;    </b></p>       <p>La IRA por rabdomiolisis cursa con hiperfosfatemia e     hipocalcemia con elevaci&oacute;n secundaria de la hormona     paratiroidea &#40;PTH&#41;. Sin embargo, parece existir resistencia     a la acci&oacute;n tisular de esta hormona mediada     por una deficiencia de vitamina D.</p>       <p> El FGF-23 es fosfat&uacute;rico, se eleva al aumentar la concentraci&oacute;n     s&eacute;rica de fosfato, y aumenta la excreci&oacute;n     renal de este ion. Paralelamente este factor inhibe la     25-hidroxivitamina D, disminuyendo por ende los niveles     de vitamina D. Parece que el FGF-23 est&aacute; elevado     en este tipo de falla renal &#40;a diferencia de otros     tipos de lesiones&#41;, independientemente de la tasa de     filtraci&oacute;n glomerular &#40;60&#41;.    </p>       ]]></body>
<body><![CDATA[<p><b>Cistatina C</b></p>       <p> Al parecer la cistatina C mide con mayor precisi&oacute;n la     tasa de filtraci&oacute;n glomerular &#40;61&#41;.    </p> 	    <p>&nbsp;</p>       <p><font size="3"><b>CONCLUSI&Oacute;N</b></font></p>       <p> La rabdomiolisis es una complicaci&oacute;n frecuente, no     exclusiva de pacientes con trauma o quemaduras.     Aunque la IRA secundaria a rabdomiolisis generalmente     tiene un curso benigno, son importantes su     prevenci&oacute;n y el diagn&oacute;stico precoz, puesto que est&aacute;     bien establecido que la IRA es un factor de riesgo para     enfermedad renal cr&oacute;nica. En la actualidad la medida     terap&eacute;utica con mayor evidencia e impacto en la IRA     por rabdomiolisis es la administraci&oacute;n de l&iacute;quidos endovenosos     y forzar la diuresis pues esto interviene en     los mecanismos fisiopatol&oacute;gicos iniciales de la lesi&oacute;n     renal. Aunque existen muchos estudios experimentales     acerca de otras posibilidades terap&eacute;uticas, a&uacute;n no     hay suficiente evidencia para hacer otras recomendaciones.    </p> 	    <p>&nbsp;</p>       <p><font size="3"><b>REFERENCIAS BIBLIOGR&Aacute;FICAS</b></font></p>       <!-- ref --><p>1. Toledo Rojas R, L&oacute;pez Jim&eacute;nez V, Mart&iacute;n-Reyes G,     Torres Rueda A, de Frutos Sanz MA. Rabdomi&oacute;lisis 2009;29&#40;1&#41;:77-80.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=1612474&pid=S0121-0793201600020000500001&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>       <!-- ref --><p> 2. Zimmerman JL, Shen MC. Rhabdomyolysis. 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