<?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>0212-7199</journal-id>
<journal-title><![CDATA[Anales de Medicina Interna]]></journal-title>
<abbrev-journal-title><![CDATA[An. Med. Interna (Madrid)]]></abbrev-journal-title>
<issn>0212-7199</issn>
<publisher>
<publisher-name><![CDATA[Arán Ediciones, S. L.]]></publisher-name>
</publisher>
</journal-meta>
<article-meta>
<article-id>S0212-71992005000100005</article-id>
<title-group>
<article-title xml:lang="es"><![CDATA[Lamivudina en el tratamiento de la hepatopatía crónica por virus hepatitis B AgHbe minus]]></article-title>
<article-title xml:lang="en"><![CDATA[Lamivudine for the treatment of patients with hepatitis B AgHbe minus]]></article-title>
</title-group>
<contrib-group>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Carneros Martín]]></surname>
<given-names><![CDATA[J. A.]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Coba Ortiz]]></surname>
<given-names><![CDATA[C. de la]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Martínez Núñez]]></surname>
<given-names><![CDATA[E.]]></given-names>
</name>
<xref ref-type="aff" rid="A02"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Fradejas Salazar]]></surname>
<given-names><![CDATA[P.]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Álvarez Delgado]]></surname>
<given-names><![CDATA[A.]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Sánchez Martín]]></surname>
<given-names><![CDATA[F.]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Rodrigo Rodríguez]]></surname>
<given-names><![CDATA[M.]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[González San Martín]]></surname>
<given-names><![CDATA[F.]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
</contrib-group>
<aff id="A01">
<institution><![CDATA[,Hospital Universitario de Salamanca Servicio de Aparato Digestivo ]]></institution>
<addr-line><![CDATA[Salamanca ]]></addr-line>
</aff>
<aff id="A02">
<institution><![CDATA[,CAP Emigrantes II Área 4 de Atención Primaria ]]></institution>
<addr-line><![CDATA[Madrid ]]></addr-line>
</aff>
<pub-date pub-type="pub">
<day>00</day>
<month>01</month>
<year>2005</year>
</pub-date>
<pub-date pub-type="epub">
<day>00</day>
<month>01</month>
<year>2005</year>
</pub-date>
<volume>22</volume>
<numero>1</numero>
<fpage>21</fpage>
<lpage>23</lpage>
<copyright-statement/>
<copyright-year/>
<self-uri xlink:href="http://scielo.isciii.es/scielo.php?script=sci_arttext&amp;pid=S0212-71992005000100005&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://scielo.isciii.es/scielo.php?script=sci_abstract&amp;pid=S0212-71992005000100005&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://scielo.isciii.es/scielo.php?script=sci_pdf&amp;pid=S0212-71992005000100005&amp;lng=en&amp;nrm=iso"></self-uri><abstract abstract-type="short" xml:lang="es"><p><![CDATA[Introducción: Se estima que la hepatopatía crónica por virus de la hepatitis B afecta a más de 350 millones de personas en todo el mundo. Los pacientes AgHbe minus representan en algunas áreas entre el 50-80% del total. En estos pacientes la remisión espontánea es rara, la respuesta a interferón menor y la probabilidad de evolución a cirrosis y hepatocarcinoma mayor que en la cepa salvaje. Objetivo: Analizar la respuesta al tratamiento con Lamivudina en pacientes con hepatopatía crónica VHB AgHBe negativos. Resultados: De los nueve pacientes tratados en nuestro servicio durante más de 3 meses, 7 eran AgHbe negativos. De ellos 6 pacientes respondieron al tratamiento, en un tiempo medio de 3,5 meses (rango 1-6). Se han producido dos recidivas a los 18 y 24 meses que han sido tratadas con Adefovir. Cuatro pacientes persisten con ADN negativo y transaminasas normales tras un tiempo medio de tratamiento de 25 meses. Conclusiones: En nuestra serie, la mayoría de los pacientes (77,7%) eran AgHbe negativos al inicio del tratamiento. La eficacia del tratamiento con Lamivudina en ellos es alta (85,7%) y precoz (media de 3,5 meses). En un tercio de los pacientes tratados se produce recidiva viral, al menos tras 1 año y medio de tratamiento.]]></p></abstract>
<abstract abstract-type="short" xml:lang="en"><p><![CDATA[Introduction: It is estimated that chronic hepatitis B affects to than 350 million people around the world. Patients with eAgHB- minus account, in some areas, for between 50-80% of the total of the population with chronic hepatitis B. Spontaneous clearance is rare within these patients, the response to interferon is low and the probability of developing cirrhosis and hepatocarcinoma is higher than in the wild type. Aim: To analyze the response to lamivudine treatment in patients with chronic hepatitis B which are eAgHB negative. Results: Seven of the 9 patients which were treated in our department for more than 3 months were eAgHB negative. Six of them responded to the treatment in an average time of 3.5 months (range 1-6 months). There were two patients that relapsed at 18 and 24 months and they were treated with adefovir. Four patients remained DNA negative and had normal aminotransferases values after an average treatment time of 25 months. Conclusion: In our series, the majority of the patients (77.7%) were eAgHB negative at the beginning of treatment. The efficacy of the treatment with lamivudine in these cases is high (85.7%) and with an early response (average 3,5 months). One third of patients treated relapsed after one and a half years of treatment.]]></p></abstract>
<kwd-group>
<kwd lng="es"><![CDATA[Virus de la Hepatitis B]]></kwd>
<kwd lng="es"><![CDATA[Antígeno e de la hepatitis B]]></kwd>
<kwd lng="es"><![CDATA[Lamivudina]]></kwd>
<kwd lng="en"><![CDATA[Hepatitis B virus]]></kwd>
<kwd lng="en"><![CDATA[Antigen e]]></kwd>
<kwd lng="en"><![CDATA[Lamivudine]]></kwd>
</kwd-group>
</article-meta>
</front><body><![CDATA[ <p>&nbsp;</p> <table border="0" width="100%"> <tr> <td width="15%" valign="top"></td> <td width="85%" valign="top">     <p><b><font size=5>Lamivudina en el tratamiento de la hepatopat&iacute;a cr&oacute;nica por virus hepatitis B AgHbe minus</font></b></p>     <p>J. A. CARNEROS MART&Iacute;N, C. DE LA COBA ORTIZ, E. MART&Iacute;NEZ N&Uacute;&Ntilde;EZ<sup>1</sup>, P. FRADEJAS SALAZAR, A. &Aacute;LVAREZ DELGADO, F. S&Aacute;NCHEZ MART&Iacute;N, M. RODRIGO RODRIGUEZ, F. GONZ&Aacute;LEZ SAN MART&Iacute;N</p>     <p><i>Servicio de Aparato Digestivo. Hospital Universitario. Salamanca. <sup>1</sup>CAP Emigrantes II. &Aacute;rea 4 de Atenci&oacute;n Primaria. Madrid</i></p>     <p></p> </td> </tr> </table> <table border="0" width="100%"> <tr> <td width="48%" valign="top"></td> <td width="4%" valign="top"></td> <td width="48%" valign="top">     <p><i><font size="2">LAMIVUDINE FOR THE TEATMENT OF PATIENTS WITH HEPATITIS B AGHBE MINUS</font></i></p>     <p>&nbsp;</p> </td> </tr> <tr> <td width="48%" valign="top">     <p>RESUMEN</p>     <p><i>Introducci&oacute;n:</i> Se estima que la hepatopat&iacute;a cr&oacute;nica por virus de la hepatitis B afecta a m&aacute;s de 350 millones de personas en todo el mundo. Los pacientes AgHbe minus representan en algunas &aacute;reas entre el 50-80% del total. En estos pacientes la remisi&oacute;n espont&aacute;nea es rara, la respuesta a interfer&oacute;n menor y la probabilidad de evoluci&oacute;n a cirrosis y hepatocarcinoma mayor que en la cepa salvaje.</p>     <p><i>Objetivo:</i> Analizar la respuesta al tratamiento con Lamivudina en pacientes con hepatopat&iacute;a cr&oacute;nica VHB AgHBe negativos.</p>     ]]></body>
<body><![CDATA[<p><i>Resultados:</i> De los nueve pacientes tratados en nuestro servicio durante m&aacute;s de 3 meses, 7 eran AgHbe negativos. De ellos 6 pacientes respondieron al tratamiento, en un tiempo medio de 3,5 meses (rango 1-6). Se han producido dos recidivas a los 18 y 24 meses que han sido tratadas con Adefovir. Cuatro pacientes persisten con ADN negativo y transaminasas normales tras un tiempo medio de tratamiento de 25 meses.</p>     <p><i>Conclusiones: </i>En nuestra serie, la mayor&iacute;a de los pacientes (77,7%) eran AgHbe negativos al inicio del tratamiento. La eficacia del tratamiento con Lamivudina en ellos es alta (85,7%) y precoz (media de 3,5 meses). En un tercio de los pacientes tratados se produce recidiva viral, al menos tras 1 a&ntilde;o y medio de tratamiento.</p>     <p>PALABRAS CLAVE<b>:</b> Virus de la Hepatitis B. Ant&iacute;geno e de la hepatitis B. Lamivudina.</p> </td> <td width="4%" valign="top"></td> <td width="48%" valign="top">     <p>ABSTRACT</p>     <p>Introduction:<i>It is estimated that chronic hepatitis B affects to than 350 million people around the world. Patients with eAgHB- minus account, in some areas, for between 50-80% of the total of the population with chronic hepatitis B. Spontaneous clearance is rare within these patients, the response to interferon is low and the probability of developing cirrhosis and hepatocarcinoma is higher than in the wild type. </i></p>     <p>Aim: <i>To analyze the response to lamivudine treatment in patients with chronic hepatitis B which are eAgHB negative.</i></p>     <p>Results: <i>Seven of the 9 patients which were treated in our department for more than 3 months were eAgHB negative. Six of them responded to the treatment in an average time of 3.5 months (range 1-6 months). There were two patients that relapsed at 18 and 24 months and they were treated with adefovir. Four patients remained DNA negative and had normal aminotransferases values after an average treatment time of 25 months.</i></p>     <p>Conclusion: <i>In our series, the majority of the patients (77.7%) were eAgHB negative at the beginning of treatment. The efficacy of the treatment with lamivudine in these cases is high (85.7%) and with an early response (average 3,5 months). One third of patients treated relapsed after one and a half years of treatment.</i></p>     <p>KEY WORDS: <i>Hepatitis B virus. Antigen e. Lamivudine.</i></p> </td> </tr> </table>     <p><i>Carneros Martín JA, De la Coba Ortiz C, Martínez Núñez E, Fradejas Salazar P, Álvarez Delgado A, Rodrigo Rodríguez M, González San Martín F. Lamivudina en el tratamiento de la hepatopat&iacute;a cr&oacute;nica por virus hepatitis B AgHbe minus. An Med Interna (Madrid) 2005; 22: 21-23.</i></p> <hr width="30%" align="left">     ]]></body>
<body><![CDATA[<p><font size="2"><i>Trabajo aceptado</i>: 14 de octubre de 2004</font></p>     <p><font size="2"><i>Correspondencia</i>: José Antonio Carneros Martín. C/ Transversal Sexta, 10-5, 2ºd. 28021 Madrid. e-mail: <a href="mailto:jcarneros.hflr@salud.madrid.org">jcarneros.hflr@salud.madrid.org</a></font></p> <hr>     <p>INTRODUCCI&Oacute;N</p>     <p>La hepatopat&iacute;a cr&oacute;nica por el virus de la hepatitis B (VHB) afecta a m&aacute;s de 350 millones de personas en todo el mundo (1). El &aacute;rea de distribuci&oacute;n del virus es mundial aunque existen zonas especialmente end&eacute;micas como Asia, &Aacute;frica subsahariana, Australia, Nueva Zelanda y Sudam&eacute;rica (2). En Estados Unidos se estima que hay 1,25 millones de portadores cr&oacute;nicos, definidos como positivos para el ant&iacute;geno de superficie AgHbs durante m&aacute;s de 6 meses. Espa&ntilde;a es un pa&iacute;s con una incidencia intermedia y pese a que los casos de infecciones agudas est&aacute;n disminuyendo, debido a la mejora de las condiciones higi&eacute;nico sanitarias y a la generalizaci&oacute;n de la vacunaci&oacute;n, existe todav&iacute;a un n&uacute;mero importante de personas con infecci&oacute;n cr&oacute;nica (3). De ellos entre el 15 y 40% desarrollar&aacute;n complicaciones en relaci&oacute;n con una hepatopat&iacute;a cr&oacute;nica progresiva (cirrosis hep&aacute;tica y hepatocarcinoma) (4, 5).</p>     <p>La afectaci&oacute;n hep&aacute;tica es m&aacute;s severa y r&aacute;pidamente progresiva en pacientes con hepatopat&iacute;a cr&oacute;nica VHB con el AgHbe negativo y el AcHbe positivo, que representan en algunas &aacute;reas el 50-80% del total (6). Estos pacientes se caracterizan por la presencia de hepatopat&iacute;a cr&oacute;nica VHB (con niveles de ADN viral detectables en suero y actividad necroinflamatoria en la biopsia hep&aacute;tica) pero con AgHbe negativo debido a la presencia de mutaciones en la regi&oacute;n precore o core (7). La m&aacute;s frecuente, G1896A, crea un cod&oacute;n de parada prematura en la regi&oacute;n precore que impide la producci&oacute;n de AgHbe (8). La tasas de respuesta sostenida en pacientes con hepatopat&iacute;a cr&oacute;nica VHB con mutante precore tratados con interfer&oacute;n son menores que en los pacientes con la cepa salvaje (9) lo que obliga a la b&uacute;squeda de alternativas en el tratamiento de estos pacientes.</p>     <p>El objetivo de nuestro estudio es analizar la eficacia del tratamiento con Lamivudina en pacientes con hepatopat&iacute;a cr&oacute;nica VHB AgHbe negativos (mutante precore).</p>    <br>     <p>PACIENTES Y M&Eacute;TODOS</p>     <p>En el Servicio de Aparato Digestivo del Hospital Universitario de Salamanca han sido tratados 12 pacientes con hepatopat&iacute;a cr&oacute;nica por VHB con Lamivudina 100 mg/d&iacute;a por v&iacute;a oral. Nueve llevan m&aacute;s de 3 meses de tratamiento, y, de ellos, 7 (77,7%) eran AgHbe negativo al inicio del tratamiento. Tres pacientes hab&iacute;an sido previamente tratados con interfer&oacute;n alfa 2b durante un tiempo medio de 10 meses. En dos de ellos no hab&iacute;a existido respuesta y el tercero present&oacute; recidiva tras retirar el tratamiento.</p>     <p>Todos los pacientes fueron evaluados en consultas externas como m&iacute;nimo una vez cada 3 meses con anamnesis y determinaciones de laboratorio que inclu&iacute;an, entre otras, transaminasas, AgHbs y DNA viral. Definimos la respuesta al tratamiento como la normalizaci&oacute;n de las transaminasas y la negativizaci&oacute;n del ADN viral (determinado en nuestro caso por t&eacute;cnicas de PCR). La recidiva implicaba la elevaci&oacute;n de transaminasas acompa&ntilde;ada de positivizaci&oacute;n de ADN de VHB.</p>    ]]></body>
<body><![CDATA[<br>     <p>RESULTADOS</p>     <p>Cuatro pacientes eran varones. La edad media al inicio del tratamiento era de 46,5 a&ntilde;os (rango 31-64).</p>     <p>De los 7 pacientes con hepatopat&iacute;a cr&oacute;nica VHB AgHbe negativo tratados con Lamivudina, 6 (85,7%) han presentado respuesta al tratamiento. El tiempo medio de respuesta fue de 3,5 meses (rango 1-6).</p>     <p>Dos pacientes de los 6 con respuesta al tratamiento (33,3%) han recidivado con aumento de transaminasas y ADN viral positivo a los 18 y 24 meses de iniciado el mismo.</p>     <p>En ambos se administr&oacute; posteriormente Adefovir con respuesta en uno de ellos (en el otro paciente se suspendi&oacute; el tratamiento en el primer mes por intolerancia digestiva).</p>    <br>     <p>Cuatro pacientes (66,6%) persisten con ADN negativo y transaminasas normales tras un tiempo medio de 25 meses de tratamiento (rango 16-48). En ning&uacute;n paciente se ha producido la negativizaci&oacute;n del AgHbs.</p>    <br>     <p>DISCUSI&Oacute;N</p>     ]]></body>
<body><![CDATA[<p>El diagn&oacute;stico de pacientes con hepatopat&iacute;a cr&oacute;nica por VHB AgHbe negativo se basa en la presencia de AgHbs durante m&aacute;s de 6 meses, AgHbe indetectable con presencia de AcHbe, ADN del VHB, elevaci&oacute;n de ALT y actividad necroinflamatoria en la biopsia hep&aacute;tica (10). La distribuci&oacute;n de esta variante e minus es mayor de lo que se cre&iacute;a inicialmente, encontr&aacute;ndose casos en pr&aacute;cticamente todo el mundo y no &uacute;nicamente en el &aacute;rea mediterr&aacute;nea y Asia como se hab&iacute;a descrito (11). En nuestra serie representan el 77,7% del total de pacientes con hepatopat&iacute;a cr&oacute;nica VHB.</p>     <p>Los pacientes AgHbe negativos tienen habitualmente una edad mayor que los AgHbe positivos y existe un mayor predominio de varones (10). Adem&aacute;s, en estos pacientes la enfermedad suele tener mayor actividad y ser m&aacute;s avanzada. De esta forma hasta el 38% de los pacientes tienen cirrosis en el momento del diagn&oacute;stico (12). Estos datos (edad mas avanzada y mayor grado de da&ntilde;o hep&aacute;tico) han hecho suponer que representa un estadio m&aacute;s avanzado en la historia natural de la hepatopat&iacute;a por VHB (10).</p>     <p>La Lamivudina es un an&aacute;logo de nucle&oacute;sidos que se administra por v&iacute;a oral y, tras su fosforilaci&oacute;n, compite por la incorporaci&oacute;n en la cadena de ADN del VHB provocando su terminaci&oacute;n prematura (13) sin interferir con la s&iacute;ntesis de ADN humano. En pacientes con hepatopat&iacute;a cr&oacute;nica por virus hepatitis B AgHbe negativos la Lamivudina consigue tasas de repuesta bioqu&iacute;mica y virol&oacute;gica del 70-96% tras 48 semanas de tratamiento frente a &lt;10% en los pacientes en los que se administr&oacute; un placebo (14, 15). Las tasas de mejor&iacute;a histol&oacute;gica var&iacute;an ampliamente entre el 20 y 95% (16).</p>     <p>Sin embargo, la mayor&iacute;a de los pacientes (90%) recidivan, con elevaci&oacute;n de las transaminasas y reaparici&oacute;n del ADN viral, en cuanto se suspende el tratamiento (16, 17). La administraci&oacute;n indefinida del f&aacute;rmaco tampoco es la soluci&oacute;n debido a la aparici&oacute;n de mutaciones en el dominio YMDD de la ADN polimerasa viral que confieren resistencia al f&aacute;rmaco (18-20). De esta forma al final del primer a&ntilde;o de tratamiento el 19% de los pacientes han desarrollado mutaciones, cifra que se eleva al 44% al final del segundo a&ntilde;o (21). El mantenimiento del tratamiento con Lamivudina tras la aparici&oacute;n de mutaciones no ha demostrado ser de utilidad por lo que en la actualidad se recomienda su suspensi&oacute;n o sustituci&oacute;n (22).</p>     <p>La &uacute;nica alternativa actual al tratamiento con Interfer&oacute;n o Lamivudina es el Adefovir Dipivoxil. Este f&aacute;rmaco, que ha sido recientemente aprobado para el tratamiento de la hepatopat&iacute;a cr&oacute;nica VHB, es un prof&aacute;rmaco del Adefovir, un an&aacute;logo sint&eacute;tico del deoxiadenos&iacute;n-monofosfato. Presenta una potente actividad antiviral frente a la ADN polimerasa de hepadnavirus, retrovirus y herpesvirus y tiene las ventajas de su administraci&oacute;n oral, la pr&aacute;ctica ausencia de efectos adversos y la hasta ahora inusual aparici&oacute;n de mutaciones que condicionen la resistencia al f&aacute;rmaco (23,24). Este &uacute;ltimo aspecto puede influir en que se convierta en la primera opci&oacute;n de tratamiento en pacientes con mutante precore, en los que la necesidad de tratamiento a largo plazo con Lamivudina puede favorecer la aparici&oacute;n de mutaciones.</p>     <p>En conclusi&oacute;n, en nuestra serie la mayor&iacute;a de los pacientes con hepatopat&iacute;a cr&oacute;nica VHB tienen la variante e minus (77,7%), en ellos la eficacia del tratamiento con Lamivudina 100 mgs/d&iacute;a por v&iacute;a oral es alta (85,7%), consigui&eacute;ndose de forma precoz (media de 3,5 meses) la normalizaci&oacute;n de las transaminasas y la negativizaci&oacute;n del ADN viral. En un tercio de los pacientes se produce recidiva viral al menos tras 1 a&ntilde;o de tratamiento, en ellos el Adefovir es una alternativa de tratamiento.</p>     <p>&nbsp;</p>     <p><i><font size="4">Bibliograf&iacute;a</font></i></p>     <!-- ref --><p>1. Lee W. Hepatitis B virus infection. N Engl J Med 1997; 337: 1733-1745.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568612&pid=S0212-7199200500010000500001&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     ]]></body>
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<body><![CDATA[<!-- ref --><p>7. Hunt CM, McGill JM, Allen MI, Condreay LD. Clinical relevance of hepatitis B viral mutations. Hepatology 2000; 31: 1037-44.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568624&pid=S0212-7199200500010000500007&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>8. Okamoto H, Tsuda F, Akahane Y, Sugai Y , Yoshiba M, Moriyama K, Tanaka T, et al. Hepatitis B virus with mutations in the core promoter for an e antigen-negative phenotype in carriers with antibody to e antigen. J Virol 1994; 68: 8102-8110.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568626&pid=S0212-7199200500010000500008&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>9. Lampertico P, Del Ninno E, Manzin A, Donato MF, Rumi MG, Lunghi G, Morabito A, et al. A randomized, controlled trial of a 24-month course of interferon alfa 2b in patients with chronic hepatitis B who had hepatitis B virus DNA without hepatitis B e antigen in serum. Heptology 1997; 26: 1621-1625.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568628&pid=S0212-7199200500010000500009&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>10. Fattovich G. Natural history and prognosis of hepatitis B. Semin Liver Dis 2003; 23: 47-58.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568630&pid=S0212-7199200500010000500010&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>11. Funk ML; Rosenberg DM, Lok ASF. World-wide epidemiology of HbeAg-negative chronic hepatitis B and associated precore and core promoter variants. J Viral Hepatol 2002; 9: 52-61.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568632&pid=S0212-7199200500010000500011&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     ]]></body>
<body><![CDATA[<!-- ref --><p>12. Zarski JP, Marcellin P, Cohard M, et al. Comparison of antiHBe-positive and Hbe-antigen-positive chronic hepatitis B in France. J Hepatol 1994; 20: 636-640.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568634&pid=S0212-7199200500010000500012&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>13. Doong SL, Tsai CH, Schinazi RF, Liotta DC, Cheng YC. Inhibition of the replication of hepatitis B virus in vitro by 2',3'-dideoxy-3'-thiacytidine and related analogues. Proc Natl Acad Sci U S A 1991; 88: 8495-8499.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568636&pid=S0212-7199200500010000500013&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>14. Rizzetto M. Efficacy of lamivudine in HbeAg-negative chronic hepatitis B. J Med Viral 2002; 66: 435-451.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568638&pid=S0212-7199200500010000500014&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>15. Gaia S, Volpes R, Smedile A, Paganin S, Actis GC, Rizzetto M. Lamivudine in anti-HbeAg positive chronic hepatitis B: response after one year of treatment. J Hepatol 2000; 32 (Supl. 2): 112.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568640&pid=S0212-7199200500010000500015&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>16. Tassopoulos NC, Volpes R, Pastore G, Heathcote J, Buti M, Goldin RD, et al. Efficacy of lamivudine in patients with hepatitis B e antigen negative/hepatitis B virus DNA-positive (precore mutant) chronic hepatitis B. Lamivudine Precore Mutant Study Group. Hepatology 1999; 29: 889-896.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568642&pid=S0212-7199200500010000500016&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     ]]></body>
<body><![CDATA[<!-- ref --><p>17. Santantonio T, Mazzola M, Iacovazzi T, Miglietta A, Guastadisegni A, Pastore G. Long-tterm follow-up of patients with anti-Hbe/HBV DNA-positive chronic hepatitis B treated for 12 months with lamivudine. J Hepatol 2000; 32: 300-6.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568644&pid=S0212-7199200500010000500017&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>18. Lai CL, Chien RN, Leung NWY, Chang TT, Guan R, Tai DI, et al. A one-year trial of lamivudine for chronic hepatitis B. N Engl J Med 1998; 339: 61-68.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568646&pid=S0212-7199200500010000500018&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>19. Liaw YF, Leung NW, Chang TT, Guan R, Tai DI, Ng KY, et al. Effects of extended lamivudine therapy in asian patients with chronic hepatitis B. Gastroenterology 2000; 119: 172-180.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568648&pid=S0212-7199200500010000500019&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>20. Dienstag JL, Schiff ER, Wright TL, Perrillo RP, Hann HW, Goodman Z, et al. Lamivudine as initial treatment for chronic hepatitis B in the United States. N Engl J Med 1999; 341: 1256-1263.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568650&pid=S0212-7199200500010000500020&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>21. Buti M, Cotrina M, Jardi R, de Castro EC, Rodr&iacute;guez-Fr&iacute;as F, S&aacute;nchez-&Aacute;vila F, et al. Two years of lamivudine therapy in anti-Hbe-positive patients with chronic hepatitis B. J Viral Hepatol 2001; 8: 270-5.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568652&pid=S0212-7199200500010000500021&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     ]]></body>
<body><![CDATA[<!-- ref --><p>22. Liaw YF, Chien RN, Yeh CT. No benefit to continue lamivudine therapy after emergence of YMDD mutations. Antivir Ther 2004; 9: 257-262.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568654&pid=S0212-7199200500010000500022&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>23. Marcellin P, Chang T-T, Lim SG, Tong MJ, Sievert W, Shiffman MI, et al. Adefovir Dipivoxil for the treatment of hepatitis B e antigen-positive chronic hepatitis B. N Engl J Med 2003; 348: 808-816.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568656&pid=S0212-7199200500010000500023&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>     <!-- ref --><p>24. Hadziyannis S, Tassopoulos N, Heathcote E, Chang TT, Kitis G, Rizzetto M, et al. Adefovir Dipivoxil for the treatment of hepatitis B e antigen-negative chronic hepatitis B. N Engl J Med 2003; 348:800-807.    &nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;&nbsp;[&#160;<a href="javascript:void(0);" onclick="javascript: window.open('/scielo.php?script=sci_nlinks&ref=568658&pid=S0212-7199200500010000500024&lng=','','width=640,height=500,resizable=yes,scrollbars=1,menubar=yes,');">Links</a>&#160;]<!-- end-ref --></p>       ]]></body><back>
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