<?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>0034-7434</journal-id>
<journal-title><![CDATA[Revista Colombiana de Obstetricia y Ginecología]]></journal-title>
<abbrev-journal-title><![CDATA[Rev Colomb Obstet Ginecol]]></abbrev-journal-title>
<issn>0034-7434</issn>
<publisher>
<publisher-name><![CDATA[Federación Colombiana de Obstetricia y GinecologíaRevista Colombiana de Obstetricia y Ginecología]]></publisher-name>
</publisher>
</journal-meta>
<article-meta>
<article-id>S0034-74342011000400005</article-id>
<title-group>
<article-title xml:lang="es"><![CDATA[Sellantes de fibrina en ginecología laparoscópica: Aspectos moleculares y mecanismo de acción: revisión de la literatura]]></article-title>
<article-title xml:lang="en"><![CDATA[Molecular aspects and mechanism of action regarding the use of fibrin sealants in laparoscopic gynecology: a literature review]]></article-title>
</title-group>
<contrib-group>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Navarro-Newball]]></surname>
<given-names><![CDATA[Hernando]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[García-Gutiérrez]]></surname>
<given-names><![CDATA[William]]></given-names>
</name>
<xref ref-type="aff" rid="A02"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Paredes-Becerra]]></surname>
<given-names><![CDATA[Eliana]]></given-names>
</name>
<xref ref-type="aff" rid="A02"/>
</contrib>
</contrib-group>
<aff id="A01">
<institution><![CDATA[,Universidad Libre Ginecología y Laparoscopia ]]></institution>
<addr-line><![CDATA[Cali ]]></addr-line>
<country>Colombia</country>
</aff>
<aff id="A02">
<institution><![CDATA[,Universidad Libre Ginecología y Obstetricia Residencia de IV año]]></institution>
<addr-line><![CDATA[Cali ]]></addr-line>
<country>Colombia</country>
</aff>
<pub-date pub-type="pub">
<day>00</day>
<month>12</month>
<year>2011</year>
</pub-date>
<pub-date pub-type="epub">
<day>00</day>
<month>12</month>
<year>2011</year>
</pub-date>
<volume>62</volume>
<numero>4</numero>
<fpage>321</fpage>
<lpage>325</lpage>
<copyright-statement/>
<copyright-year/>
<self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_arttext&amp;pid=S0034-74342011000400005&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_abstract&amp;pid=S0034-74342011000400005&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_pdf&amp;pid=S0034-74342011000400005&amp;lng=en&amp;nrm=iso"></self-uri><abstract abstract-type="short" xml:lang="es"><p><![CDATA[Objetivo: hacer una revisión sobre la actividad biológica y mecanismo de acción de los sellantes de fibrina en ginecología laparoscópica. Materiales y métodos: se realizó una búsqueda de la literatura publicada tanto en inglés como en español a través de Medline vía PubMed, Ovid y Cochrane, desde 1993 a 2010. Se analizaron los artículos que incluían el uso de los sellantes en ginecología laparoscópica y se agruparon por temáticas tales como antecedentes, actividad biológica, composición, administración y características biofísicas. Resultados: se encontraron entre 1993 y 2010, 200 artículos de los cuales 49 correspondían a los criterios establecidos siendo objeto de análisis. Los sellantes de fibrina contribuyen al logro de la hemostasia aumentando la expresión en las células peritoneales de los activadores e inhibidores del plasminógeno, afectando el proceso de curación, que puede ser de beneficio en la reducción de las adherencias posoperatorias. Conclusión: el desarrollo de los sellantes de fibrina surge como una alternativa práctica para la reducción de la hemorragia y control de la hemostasia, además de la reducción de las adherencias posoperatorias en la cirugía laparoscópica ginecológica.]]></p></abstract>
<abstract abstract-type="short" xml:lang="en"><p><![CDATA[Objective: reviewing fibrin sealants&rsquo; biological activity and mechanism of action related to laparoscopic gynecology. Materials and methods: a search was made of the literature published in both English and Spanish via PubMed/Medline, OVID and Cochrane from 1993 to 2010. Articles involving the use of sealants in laparoscopic gynecology were analyzed and grouped by topic, such as background, biological activity, composition, administration and biophysical characteristics. Results: 200 articles were found which had been published from 1993 to 2010, 49 of them complied with the established analysis criteria. Fibrin sealants contributed towards achieving hemostasis, increasing plasminogen activator and inhibitor expression in peritoneal cells, thereby affecting curing, which could be beneficial in reducing post-operative adhesion. Conclusion: developing fibrin sealants emerges as a practical alternative for reducing hemorrhage and controlling hemostasia, as well as reducing postoperative adhesion in surgery involving laparoscopic gynecology.]]></p></abstract>
<kwd-group>
<kwd lng="es"><![CDATA[sellante de fibrina]]></kwd>
<kwd lng="es"><![CDATA[hemostático]]></kwd>
<kwd lng="es"><![CDATA[adhesivo]]></kwd>
<kwd lng="es"><![CDATA[ginecología]]></kwd>
<kwd lng="es"><![CDATA[laparoscopia]]></kwd>
<kwd lng="en"><![CDATA[fibrin sealant]]></kwd>
<kwd lng="en"><![CDATA[haemostatic]]></kwd>
<kwd lng="en"><![CDATA[adhesive]]></kwd>
<kwd lng="en"><![CDATA[gynecology]]></kwd>
</kwd-group>
</article-meta>
</front><body><![CDATA[  <font face="verdana" size="2"> <font size="4">    <center>   <b>Sellantes de fibrina en ginecolog&iacute;a laparosc&oacute;pica. Aspectos moleculares y mecanismo de acci&oacute;n: revisi&oacute;n de la literatura</b> </center></font>     <p>    <center>     <p>Hernando Navarro-Newball, M.D.*, William Garc&iacute;a-Guti&eacute;rrez**, Eliana Paredes-Becerra** </p></center></p>     <p>    <center>    <p>Recibido: mayo 4/11 &ndash; Aceptado: diciembre 19/11</p></center></p>     <p>* Ginec&oacute;logo Laparoscopista. Docente Universidad Libre, Cali (Colombia). Correo electr&oacute;nico: <a href="mailto:hnavarro_newball@hotmail.com">hnavarro_newball@hotmail.com</a> </p>     <p>** Residente de IV a&ntilde;o Ginecolog&iacute;a y Obstetricia Universidad Libre. Cali, (Colombia). </p>     ]]></body>
<body><![CDATA[<p><b>RESUMEN</b></p>     <p><b>Objetivo:</b> hacer una revisi&oacute;n sobre la actividad biol&oacute;gica y mecanismo de acci&oacute;n de los sellantes de fibrina en ginecolog&iacute;a laparosc&oacute;pica. </p>     <p><b>Materiales y m&eacute;todos: </b>se realiz&oacute; una b&uacute;squeda de la literatura publicada tanto en ingl&eacute;s como en espa&ntilde;ol a trav&eacute;s de Medline v&iacute;a PubMed, Ovid y Cochrane, desde 1993 a 2010. Se analizaron los art&iacute;culos que inclu&iacute;an el uso de los sellantes en ginecolog&iacute;a laparosc&oacute;pica y se agruparon por tem&aacute;ticas tales como antecedentes, actividad biol&oacute;gica, composici&oacute;n, administraci&oacute;n y caracter&iacute;sticas biof&iacute;sicas. </p>     <p><b>Resultados: </b>se encontraron entre 1993 y 2010, 200 art&iacute;culos de los cuales 49 correspond&iacute;an a los criterios establecidos siendo objeto de an&aacute;lisis. Los sellantes de fibrina contribuyen al logro de la hemostasia aumentando la expresi&oacute;n en las c&eacute;lulas peritoneales de los activadores e inhibidores del plasmin&oacute;geno, afectando el proceso de curaci&oacute;n, que puede ser de beneficio en la reducci&oacute;n de las adherencias posoperatorias. </p>     <p><b>Conclusi&oacute;n: </b>el desarrollo de los sellantes de fibrina surge como una alternativa pr&aacute;ctica para la reducci&oacute;n de la hemorragia y control de la hemostasia, adem&aacute;s de la reducci&oacute;n de las adherencias posoperatorias en la cirug&iacute;a laparosc&oacute;pica ginecol&oacute;gica. </p>     <p><b>Palabras clave: </b>sellante de fibrina, hemost&aacute;tico, adhesivo, ginecolog&iacute;a, laparoscopia. </p> <font size="4">    <center><b>Molecular aspects and mechanism of action regarding the use of fibrin sealants in laparoscopic gynecology: a literature review</b></center></font>     <p><b>SUMMARY</b></p>     <p><b>Objective: </b>reviewing fibrin sealants&rsquo; biological activity and mechanism of action related to laparoscopic gynecology. </p>     <p><b>Materials and methods:</b> a search was made of the literature published in both English and Spanish via PubMed/Medline, OVID and Cochrane from 1993 to 2010. Articles involving the use of sealants in laparoscopic gynecology were analyzed and grouped by topic, such as background, biological activity, composition, administration and biophysical characteristics. </p>     ]]></body>
<body><![CDATA[<p><b>Results:</b> 200 articles were found which had been published from 1993 to 2010, 49 of them complied with the established analysis criteria. Fibrin sealants contributed towards achieving hemostasis, increasing plasminogen activator and inhibitor expression in peritoneal cells, thereby affecting curing, which could be beneficial in reducing post-operative adhesion. </p>     <p><b>Conclusion:</b> developing fibrin sealants emerges as a practical alternative for reducing hemorrhage and controlling hemostasia, as well as reducing postoperative adhesion in surgery involving laparoscopic gynecology. </p>     <p><b>Key words: </b>fibrin sealant, haemostatic, adhesive, gynecology, laparoscopy. </p>     <p><b>INTRODUCCI&Oacute;N</b></p>      <p>Con el auge de la laparoscopia se han incorporado nuevas t&eacute;cnicas y m&eacute;todos de hemostasia dentro de los cuales los sellantes de fibrina ocupan un lugar muy importante por su facilidad de aplicaci&oacute;n y resultados.<sup>1,2 </sup>Los sellantes de fibrina pertenecen al grupo de productos con propiedades adhesivas y hemost&aacute;ticas derivados principalmente del plasma humano, contienen fibrin&oacute;geno, trombina, factor XIII, fibronectina, aprotinina y cloruro de calcio.<sup>3 </sup>Estos productos reproducen los pasos finales de la cascada de coagulaci&oacute;n, formando un co&aacute;gulo de fibrina estable, deteniendo la p&eacute;rdida sangu&iacute;nea y ayudando en el proceso normal de cicatrizaci&oacute;n.<sup>3 </sup></p>      <p>Con el prop&oacute;sito de brindar informaci&oacute;n al ginec&oacute;logo laparoscopista y a otros profesionales de la salud, que facilite el conocimiento y aplicaci&oacute;n de estos productos se presenta esta revisi&oacute;n sobre la farmacolog&iacute;a, el mecanismo acci&oacute;n y la actividad biol&oacute;gica de los sellantes de fibrina. </p>      <p><b>MATERIALES Y M&Eacute;TODOS </b></p>      <p>Con las palabras clave &ldquo;sellantes de fibrina&rdquo;, &ldquo;hemostasia&rdquo;, &ldquo;ginecolog&iacute;a&rdquo; y &ldquo;laparoscopia&rdquo; se realiz&oacute; una b&uacute;squeda en las bases de datos Medline v&iacute;a PubMed, Ovid y Cochrane desde 1993 hasta 2010, en idiomas ingl&eacute;s y espa&ntilde;ol. </p>      <p>Se analizaron los art&iacute;culos relacionados con las caracter&iacute;sticas biof&iacute;sicas y bioqu&iacute;micas de los sellantes, administraci&oacute;n, actividad biol&oacute;gica y del uso del dispositivo m&eacute;dico en laparoscopia ginecol&oacute;gica. Se clasificaron las revisiones bibliogr&aacute;ficas de acuerdo con las variables mencionadas y se condens&oacute; la informaci&oacute;n en forma ordenada y secuencial. </p>      <p><b>RESULTADOS</b></p>      ]]></body>
<body><![CDATA[<p>Se encontraron 200 referencias de los cuales se analizaron 49 art&iacute;culos porque se relacionaban con uso en humanos y laparoscopia ginecol&oacute;gica. Respecto al uso de sellantes en ginecolog&iacute;a fueron incluidas 11 referencias. </p>      <p><b>Caracter&iacute;sticas farmacol&oacute;gicas y mecanismo de acci&oacute;n </b></p>     <p>El primer sellante de fibrina aprobado por la FDA en 1998 y el m&aacute;s estudiado en los Estados Unidos fue Tisseel o Tissucol<sup>&reg;</sup> (Baxter), contiene aprotinina bovina que es un agente antifibrinol&iacute;tico que frena la disoluci&oacute;n natural del co&aacute;gulo.<sup>1,4</sup> Este sistema hemost&aacute;tico est&aacute; constituido por dos componentes de origen humano: el concentrado proteico liofilizado, para disolver con soluci&oacute;n de aprotinina, y la trombina liofilizada para reconstituir con soluci&oacute;n de cloruro de calcio. Ambos componentes se elaboran a partir de una mezcla de plasma humano.<sup>5-7</sup> El mecanismo de acci&oacute;n de los sellantes de fibrina corresponde a la &uacute;ltima fase de la coagulaci&oacute;n sangu&iacute;nea. La mol&eacute;cula de fibrin&oacute;geno humana es una glicoprote&iacute;na compuesta de tres pares de cadenas polipept&iacute;dicas (&prop;, &beta;, &gamma;) que forman una mol&eacute;cula con dos mitades sim&eacute;tricas.<sup>8 </sup>El fibrin&oacute;geno bajo la acci&oacute;n de la trombina se transforma en fibrina (&prop;, &beta;, &gamma;) con liberaci&oacute;n de dos mol&eacute;culas de fibrinop&eacute;ptido A y B. Los mon&oacute;meros de fibrina formados se polimerizan en d&iacute;meros y posteriormente se unen entre s&iacute; mediante enlaces covalentes, por acci&oacute;n del factor XIII previamente activado por la trombina y en presencia de iones de calcio.<sup>8,9</sup> La fibrina producida se adhiere a los tejidos que resultan expuestos tras la lesi&oacute;n tisular, con especial afinidad por las fibras de col&aacute;geno.<sup>2 </sup>La malla de fibrina formada sirve de soporte para la proliferaci&oacute;n de fibroblastos y capilares que se producen en el proceso de cicatrizaci&oacute;n.<sup>10</sup> La &uacute;ltima fase del proceso es la degradaci&oacute;n por prote&oacute;lisis y fagocitosis de la malla de fibrina, en la que intervienen los sellantes de fibrina. La fibrin&oacute;lisis, entre otros factores, depende de la presencia de los activadores tisulares del plasmin&oacute;geno, cuya concentraci&oacute;n puede variar de un tejido a otro. As&iacute;, la etapa final es la sustituci&oacute;n de la malla de fibrina por tejido conjuntivo y la posterior formaci&oacute;n de un tejido de cicatrizaci&oacute;n.<sup>6,7</sup> Es en este punto en el que el tipo de sellante juega un papel relevante de acuerdo con la cantidad de fibrin&oacute;geno, plasmin&oacute;geno y activador del plasmin&oacute;geno tisular (t-PA).<sup>7 </sup></p>     <p><b>Composici&oacute;n </b></p>      <p>El liofilizado necesario para obtener 1 ml de soluci&oacute;n sellante de fibrina contiene los siguientes principios activos: prote&iacute;na coagulable 75-115 mg; fibrin&oacute;geno 70-110 mg; plasmafibronectina 2-9 mg; plasmin&oacute;geno 40-120 mcg; factor XIII 10-50 UI; soluci&oacute;n de aprotinina bovina we3.000 UIC/ml; trombina humana liofilizada; trombina 4: 1 ml de la soluci&oacute;n reconstituida contiene 4 UI; trombina 500: 1 ml de la soluci&oacute;n reconstituida contiene 500 UI; soluci&oacute;n de cloruro de calcio 40 &micro;mol CaCI<Sub>2</Sub>/m.<sup>5,11-14 </sup></p>      <p><b>Caracter&iacute;sticas biof&iacute;sicas </b></p>      <p>Las formas de fibrin&oacute;geno fotoqu&iacute;micamente reticulado de los sellantes de tejidos son al menos 5 veces m&aacute;s fuertes (presi&oacute;n), (95,9 +/-4,5 kilopascales (kPa) o 19,501 g) que un sellador de fibrina convencional (17,9 +/-9,3 kPa o 3,640 g); con una fuerza tensil de 125 g/cm&sup2;.<sup>15-18 </sup>Cuando se comparan las caracter&iacute;sticas de varios agentes hemost&aacute;ticos, se encuentra que las suturas son las que ofrecen mayor presi&oacute;n y pueden ser utilizadas en vasos de mayor calibre (900 mmHg y 7 mm, respectivamente), seguidos por los clips de pol&iacute;mero (854 mmHg y 4 mm), bipolar (601 mmHg y 4 mm), endograpadora (310 mmHg y 17 mm) y luego los sellantes de fibrina en par&eacute;nquima (378 mmHg), superiores al uso de monopolar (230 mmHg) bistur&iacute; arm&oacute;nico (204 mmHg y 4 mm).<sup>15,19-25 </sup></p>      <p><b>Actividad biol&oacute;gica </b></p>      <p>Para evaluar la actividad del sellador de fibrina se realiz&oacute; un ensayo cl&iacute;nico en el laboratorio de la Universidad de Detroit (Michigan) divisi&oacute;n de Ginecolog&iacute;a y Obstetricia en el 2004, en donde se midi&oacute; la expresi&oacute;n del &aacute;cido ribonucleico mensajero (ARNm) de factores reguladores de la coagulaci&oacute;n como el activador del plasmin&oacute;geno en las c&eacute;lulas peritoneales.<sup>8</sup> La actividad del plasmin&oacute;geno y del activador del plasmin&oacute;geno tisular t-PA, se cree que juegan un papel fundamental en la degradaci&oacute;n de la malla de fibrina que se desarrolla despu&eacute;s de procedimientos quir&uacute;rgicos. La reducci&oacute;n de estos compuestos, como ocurre con el trauma de los tejidos, se traduce en un mayor desarrollo de adherencias posoperatorias.<sup>8</sup> Se utiliz&oacute; transcriptasa reversa (RT) y cambios en la reacci&oacute;n de polimerasa (PCR) para determinar los cambios de t-PA y del inhibidor del activador del plasmin&oacute;geno 1 (PAI-1, por sus siglas en ingl&eacute;s) en seis condiciones, a las 6, 12, 24 y 48 horas. El sellante de fibrina usado fue Tissucol, un sellante de fibrina en dos componentes en diluci&oacute;n 1 a 2, y cultivo control. No hubo cambios en los niveles de ARNm de t-PA y PAI-1 a las 48 horas. Se observ&oacute; un aumento selectivo en los fibroblastos peritoneales normales; aumentos similares fueron identificados en los cultivos de fibroblastos. Los autores concluyen que la aprotinina utilizada como antifibrinol&iacute;tico no aumenta la expresi&oacute;n en las c&eacute;lulas peritoneales tanto de la t-PA como del PAI-1, los cambios no se ven en concentraciones fisiol&oacute;gicas del sellante de fibrina. Estas observaciones sugieren que, adem&aacute;s de su capacidad para contribuir al logro de la hemostasia, el sellante de fibrina afecta el proceso de curaci&oacute;n mediante la alteraci&oacute;n de los componentes del sistema activador del plasmin&oacute;geno, que puede ser de beneficio en la reducci&oacute;n de las adherencias posoperatorias.<sup>8 </sup></p>      <p>En otro estudio realizado por la Universidad de Sao Paulo (Brasil), y publicado en el 2009, al realizar histerectom&iacute;a abdominal en conejas, utilizaron sutura de &aacute;cido poliglic&oacute;lico y sellantes de fibrina, se encontr&oacute; mejor adherencia a la c&uacute;pula, con mejor tejido de granulaci&oacute;n con el &aacute;cido poliglic&oacute;lico, pero una mejor malla de fibrina y mayor presi&oacute;n de ruptura con los sellantes de fibrina, con lo que concluyen que el cierre de la c&uacute;pula vaginal utilizando la cola de fibrina es un procedimiento seguro y fiable despu&eacute;s de la histerectom&iacute;a abdominal en el modelo de conejas.<sup>11 </sup></p>      ]]></body>
<body><![CDATA[<p><b>Administraci&oacute;n </b></p>      <p>Deben administrarse &uacute;nicamente por v&iacute;a t&oacute;pica. La dosis requerida depende del tama&ntilde;o de la superficie que debe cubrirse, con la presentaci&oacute;n de 1 ml - 2 ml de soluci&oacute;n, se cubre un &aacute;rea de unos 10 cm&sup2; si se utiliza en c&aacute;nula, y de 25 cm&sup2; a 100 cm&sup2;, utilizando un equipo pulverizador.<sup>5,14-16,26 </sup>El sellante de fibrina se adhiere firmemente al tejido circundante entre 3 a 5 minutos, a los 10 minutos adquiere el 70% de resistencia, la cual es m&aacute;xima a las dos horas.<sup>5,17 </sup></p>      <p><b>Usos en ginecolog&iacute;a laparosc&oacute;pica </b></p>      <p>El uso de sellantes de fibrina durante la miomectom&iacute;a laparosc&oacute;pica podr&iacute;a reducir considerablemente el riesgo de adherencias.<sup>26,27</sup> Los sellantes han aumentado su popularidad en las intervenciones para mejorar la hemostasia perioperatoria. Existen revisiones sistem&aacute;ticas de ensayos controlados en los que pacientes adultos llevados a cirug&iacute;a electiva se asignan al azar a manejo con sellantes o grupo sin tratamiento, en los que se encuentra que en el abordaje laparosc&oacute;pico durante la miomectom&iacute;a se disminuye un 36% el riesgo de adherencias, en comparaci&oacute;n con la laparotom&iacute;a.<sup>13,15,26,28-30 </sup>Cuando se adiciona sellante de fibrina se disminuye el riesgo de adherencias de 6,5% a 3%, observado en la laparoscopia de control; adem&aacute;s, hay una disminuci&oacute;n del riesgo de hemorragia perioperatoria (340 ml frente a 110 ml).<sup>17,31,32 </sup></p>      <p><b>CONCLUSI&Oacute;N</b>     <p>Los sellantes de fibrina contribuyen al logro de la hemostasia aumentando tanto la expresi&oacute;n en las c&eacute;lulas del t-PA como del PAI-1, afectan el proceso de curaci&oacute;n mediante la alteraci&oacute;n de los componentes del sistema activador del plasmin&oacute;geno, que puede ser de beneficio en la reducci&oacute;n de las adherencias posoperatorias. </p>      <p><b>REFERENCIAS</b>     <!-- ref --><p>1. 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