<?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>0864-0300</journal-id>
<journal-title><![CDATA[Revista Cubana de Investigaciones Biomédicas]]></journal-title>
<abbrev-journal-title><![CDATA[Rev Cubana Invest Bioméd]]></abbrev-journal-title>
<issn>0864-0300</issn>
<publisher>
<publisher-name><![CDATA[ECIMED]]></publisher-name>
</publisher>
</journal-meta>
<article-meta>
<article-id>S0864-03001999000300011</article-id>
<title-group>
<article-title xml:lang="es"><![CDATA[Tratamiento de la infección por Helicobacter pylori: Comentario al respecto]]></article-title>
</title-group>
<contrib-group>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Padrón Pérez]]></surname>
<given-names><![CDATA[Noel]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Fernández Vallín-Cárdenas]]></surname>
<given-names><![CDATA[Eulalia]]></given-names>
</name>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Quiñones Pérez]]></surname>
<given-names><![CDATA[Dianelys]]></given-names>
</name>
</contrib>
</contrib-group>
<aff id="A01">
<institution><![CDATA[,Hospital Clínico Quirúgico General Calixto García  ]]></institution>
<addr-line><![CDATA[Ciudad de La Habana ]]></addr-line>
<country>Cuba</country>
</aff>
<pub-date pub-type="pub">
<day>00</day>
<month>12</month>
<year>1999</year>
</pub-date>
<pub-date pub-type="epub">
<day>00</day>
<month>12</month>
<year>1999</year>
</pub-date>
<volume>18</volume>
<numero>3</numero>
<fpage>236</fpage>
<lpage>240</lpage>
<copyright-statement/>
<copyright-year/>
<self-uri xlink:href="http://scielo.sld.cu/scielo.php?script=sci_arttext&amp;pid=S0864-03001999000300011&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://scielo.sld.cu/scielo.php?script=sci_abstract&amp;pid=S0864-03001999000300011&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://scielo.sld.cu/scielo.php?script=sci_pdf&amp;pid=S0864-03001999000300011&amp;lng=en&amp;nrm=iso"></self-uri><abstract abstract-type="short" xml:lang="es"><p><![CDATA[Se realizó una revisión bibliográfica sobre las pautas de tratamiento recomendadas en la infección causada por Helicobacter pylori. Las altas tasas de erradicación logradas por los esquemas triple y cuádruple, hacen que éstos sean utilizados como primera y segunda línea de tratamiento respectivamente. Se relacionan las afecciones asociadas con la infección, en las que se debe utilizar el tratamiento erradicador. El uso de antimicrobianos, en zonas donde la resistencia era elevada, redujo la eficacia del esquema utilizado. La vacuna anti-H. pylori constituyó una novedosa opción de tratamiento. La utilización de diferentes sitios mucosos de vacunación con adyuvantes de baja toxicidad, también se trataron en este trabajo. La efectividad terapéutica de la vacuna, según los autores, resultó alta en modelos experimentales y alcanzó 100 % de protección frente a la infección por esta bacteria gramnegativa.]]></p></abstract>
<abstract abstract-type="short" xml:lang="en"><p><![CDATA[A bibliographic review on the schedules of treatment recommended in the infection caused by Helicobacter pylori was made. The high rates of erradication attained by the triple and quadruple therapies allow their use as first and second line treatment, respectively. Those affections associated with the infection, in which the erradicating treatment should be applied, are related. The utilization of antimicrobials in areas where the resistance was high reduced the efficacy of the therapy used. The anti-H. pylori vaccine became a new option of treatment. The use of different mucous sites of vaccination with adjuvants of low toxicity was also dealt with in this paper. The therapeutic effectiveness of the vaccine according to the authors proved to be high in experimental models and achieved 100 % of protection against the infection caused by this gramnegative bacterium.]]></p></abstract>
<kwd-group>
<kwd lng="es"><![CDATA[INFECCIONES POR HELICOBACTER]]></kwd>
<kwd lng="es"><![CDATA[HELICOBACTER PYLORI]]></kwd>
<kwd lng="en"><![CDATA[HELICOBACTER INFECTIONS]]></kwd>
<kwd lng="en"><![CDATA[HELICOBACTER PYLORI]]></kwd>
</kwd-group>
</article-meta>
</front><body><![CDATA[ <h3> Comunicaci&oacute;n corta</h3>Hospital Cl&iacute;nico Quir&uacute;gico "General  Calixto Garc&iacute;a" <h2> Tratamiento de la infecci&oacute;n por <i>Helicobacter  pylori</i>: Comentario al respecto</h2><i>Dr. Noel Padr&oacute;n P&eacute;rez,  Dra. Eulalia Fern&aacute;ndez Vall&iacute;n-C&aacute;rdenas y Dra. Dianelys Qui&ntilde;ones  P&eacute;rez</i> <h4> RESUMEN</h4>Se realiz&oacute; una revisi&oacute;n bibliogr&aacute;fica  sobre las pautas de tratamiento recomendadas en la infecci&oacute;n causada por  <i>Helicobacter pylori. </i>Las altas tasas de erradicaci&oacute;n logradas por  los esquemas triple y cu&aacute;druple, hacen que &eacute;stos sean utilizados  como primera y segunda l&iacute;nea de tratamiento respectivamente. Se relacionan  las afecciones asociadas con la infecci&oacute;n, en las que se debe utilizar  el tratamiento erradicador. El uso de antimicrobianos, en zonas donde la resistencia  era elevada, redujo la eficacia del esquema utilizado. La vacuna anti<i>-H. pylori  </i>constituy&oacute; una novedosa opci&oacute;n de tratamiento. La utilizaci&oacute;n  de diferentes sitios mucosos de vacunaci&oacute;n con adyuvantes de baja toxicidad,  tambi&eacute;n se trataron en este trabajo. La efectividad terap&eacute;utica  de la vacuna, seg&uacute;n los autores, result&oacute; alta en modelos experimentales  y alcanz&oacute; 100 % de protecci&oacute;n frente a la infecci&oacute;n por esta  bacteria gramnegativa.     <p><i>Descriptores DeCS: </i>INFECCIONES POR HELICOBACTER  /terapia; HELICOBACTER PYLORI.     <p>La infecci&oacute;n causada por <i>Helicobacter  pylori</i>, bacteria gramnegativa espiral, se asocia con: gastritis cr&oacute;nica  tipo B, &uacute;lcera p&eacute;ptica, carcinoma g&aacute;strico y linfoma tipo  MALT (mucosa-<i>associated lymphoid tissue</i>). Tambi&eacute;n se investiga la  posible implicaci&oacute;n de este microorganismo pat&oacute;geno como causa de  dispepsia y otros trastornos extraintestinales, entre los cuales se pueden mencionar  la enfermedad arterial coronaria, la urticaria y el retraso del crecimiento en  ni&ntilde;os.<sup>1,2</sup> Reportes epidemiol&oacute;gicos se&ntilde;alan que  la infecci&oacute;n por este microorganismo constituye una de las infecciones  m&aacute;s prevalentes en el planeta. Es pa&iacute;ses desarrollados afecta a  50 % de los adultos, pero las naciones en v&iacute;as de desarrollo alcanzan cifras  de 90 % (e incluso mayores) de habitantes infectados.<sup>3,4</sup>     <p>En el caso  de la enfermedad p&eacute;ptica ulcerosa, la erradicaci&oacute;n del microorganismo  pat&oacute;geno conduce a la curaci&oacute;n, reduce significativamente las recurrencias  posterior al tratamiento y disminuye el costo de la terapia.<sup>5,6</sup> Es  por esta raz&oacute;n que en una reuni&oacute;n de consenso de los Institutos  Nacionales de Salud de los EE.UU., celebrada en 1994, se recomend&oacute; utilizar  el tratamiento erradicador en todos los pacientes con &uacute;lceras p&eacute;pticas  asociadas con <i>H. pylori</i>.<sup>7</sup> En otra reuni&oacute;n, realizada  en 1996, pero del Grupo Europeo para el estudio del <i>Helicobacter pylori</i>,  se lleg&oacute; al consenso de administrar el tratamiento erradicador, adem&aacute;s,  a los pacientes que presentaran &uacute;lceras p&eacute;pticas sangrantes y a  los casos que se encontraran en estadio temprano del linfoma tipo MALT.<sup>8</sup>      <p>Aunque hay necesidad de erradicar la infecci&oacute;n en los pacientes con  &uacute;lceras p&eacute;pticas, existen elementos que justifican la administraci&oacute;n  del tratamiento erradicador en formas avanzadas y graves de gastritis con <i>H.  pylori</i> positivo, como: metaplasia intestinal, atrofia glandular y variedades  hipertr&oacute;ficas erosivas de gastritis. Son conocidas las m&uacute;ltiples  combinaciones de antimicrobianos y antisecretores para combatir la infecci&oacute;n  por esta bacteria gramnegativa; sin embargo, no se dispone de un esquema de tratamiento  que logre erradicar la infecci&oacute;n en 100 % de los pacientes tratados. Las  pautas utilizadas en la actualidad que alcanzan las m&aacute;s altas tasas de  erradicaci&oacute;n, en general por encima de 90 %, son las combinaciones de 3  o 4 drogas. Estas modalidades de terapia reducen las recurrencias posterior a  la culminaci&oacute;n del esquema utilizado, pero no logran la curaci&oacute;n  total y condicionan a la aparici&oacute;n de resistencias.<sup>9,10</sup> Sin  embargo, algunos autores han obtenido resultados contradictorios. Van der Hulst  demostr&oacute;, en un estudio prospectivo, que las lesiones histol&oacute;gicas,  el grado de metaplasia intestinal y la atrofia, se mantuvieron inalterables a  pesar de una erradicaci&oacute;n exitosa.<sup>11</sup>     <p>El control de la infecci&oacute;n  por este microorganismo comprende su diagn&oacute;stico, su tratamiento y el seguimiento  posterior. La confirmaci&oacute;n de la erradicaci&oacute;n de la infecci&oacute;n  por <i>H. pylori</i>, con el uso de m&eacute;todos endosc&oacute;picos, est&aacute;  indicada en los pacientes con &uacute;lceras p&eacute;pticas complicadas, &uacute;lceras  g&aacute;stricas y estadio temprano de linfoma tipo MALT. Por otra parte, los  m&eacute;todos no invasivos (<i>test</i> del aliento, pruebas serol&oacute;gicas)  son recomendados para el seguimiento de los pacientes con &uacute;lceras duodenales  no complicadas.<sup>6,12,13</sup>     <p>Se han realizado varios estudios con el empleo  de las diferentes pautas para erradicar la infecci&oacute;n por <i>H. pylori</i>.  Todas estas investigaciones buscan obtener un tratamiento erradicador que alcance  tasas de &eacute;xito superior a 90 % posterior a su culminaci&oacute;n, de f&aacute;cil  cumplimiento para el paciente, de corta duraci&oacute;n, de bajo costo y con resultados  reproducibles. Los m&uacute;ltiples ensayos cl&iacute;nicos realizados han demostrado  que la terapia triple y cu&aacute;druple proporcionan las m&aacute;s altas tasas  de erradicaci&oacute;n, en general por encima de 90 %, aunque con mayor incidencia  de efectos adversos.<sup>14-17</sup> La terapia dual, propuesta como primera l&iacute;nea  de tratamiento en 1994, disminuye la incidencia de efectos adversos, pero no es  eficaz y no logra tasas de erradicaci&oacute;n como la terapia triple y cu&aacute;druple.  Varios ensayos indican que no debe ser recomendada por las razones antes expuestas.<sup>17-19</sup>      <p>La asociaci&oacute;n de 1 inhibidor de la bomba de protones (omeprazol, lansoprazol)  y 2 antibi&oacute;ticos (generalmente amoxicilina, claritromicina o metronidazol)  constituye la estrategia terap&eacute;utica de mayor uso en la actualidad, y alcanza  tasas de erradicaci&oacute;n alrededor de 90 %. Se recomienda como segunda l&iacute;nea  de tratamiento el esquema de 4 drogas, si el anterior fracasa.<sup>13-17</sup>  Un elemento de extraordinaria importancia, que influye en la eficacia del esquema  triple y cu&aacute;druple, es la aparici&oacute;n de cepas resistentes a los derivados  imidaz&oacute;licos, y m&aacute;s reciente a la claritromicina.<sup>20-22</sup>  Si en el esquema de 3 drogas se combina un inhibidor de la bomba de protones con  metronidazol y claritromicina en un &aacute;rea de alta prevalencia de resistencia  al metronidazol, seg&uacute;n <i>Buckley </i>y otros,<sup>21</sup> esto conduce  a un incremento de la resistencia a la claritromicina, independientemente de la  reducci&oacute;n de la eficacia del tratamiento.     <p>La infecci&oacute;n por <i>H.  pylori</i> rara vez recurre despu&eacute;s de una erradicaci&oacute;n exitosa.<sup>23,24</sup><i>  Abu-Mahfouz</i> y otros,<sup>24</sup> en un per&iacute;odo de 5 a&ntilde;os posterior  a un tratamiento exitoso, demostraron que la recurrencia es baja en EE.UU., casi  de 1 % por a&ntilde;o. Es por ello que hoy d&iacute;a se utiliza la triple terapia  como primera pauta de tratamiento, basada en 1 inhibidor de la bomba de protones  y 2 antimicrobianos. Esta modalidad es recomendada en el informe del consenso  de Maastricht; se tiene en cuenta que es sencilla, bien tolerada por los pacientes,  costeable y que logra altas tasas de erradicaci&oacute;n, en general alrededor  de 90 % en rigurosos estudios.<sup>8,14-17</sup> <h4> Vacuna anti-<i>H. PYLORI</i></h4>La  inmunizaci&oacute;n, como en conocidas enfermedades infecciosas, vislumbra nuevos  horizontes en el tratamiento de la infecci&oacute;n por <i>Helicobacter pylori</i>.  Varias han sido las v&iacute;as utilizadas para administrar la vacuna anti-<i>H.  pylori</i>. Las rutas oral, intranasal, rectal e incluso intravaginal, se han  empleado en modelos animales con el uso de vacunas recombinantes con adyuvantes  mucosos.<sup>25-9</sup> <i>Kleanthous</i> y otros<sup>25</sup> emplearon una vacuna  de ureasa recombinante en ratones con el objetivo de obtener, mediante la utilizaci&oacute;n  de las 3 primeras v&iacute;as antes mencionadas, el sitio de vacunaci&oacute;n  que ofrece mayor protecci&oacute;n. Seg&uacute;n el estudio, todas las v&iacute;as  ofrecen protecci&oacute;n contra la infecci&oacute;n, sin embargo, la v&iacute;a  rectal gener&oacute; los m&aacute;s altos niveles de IgA antiureasa g&aacute;strica,  en comparaci&oacute;n con los otros sitios de vacunaci&oacute;n.     <p>La efectividad  de la inmunizaci&oacute;n oral fue comprobada por <i>G&oacute;mez-Duarte</i> y  otros,<sup>26</sup> que utilizaron una vacuna recombinante de <i>Salmonella typhimurium</i><b>  </b>(viva, atenuada), que expresa las subunidades A y B de la enzima ureasa. A  las 5 semanas despu&eacute;s los ratones inmunizados fueron infectados con cepas  de <i>H. pylori</i> adaptadas a este modelo experimental, y a las 6 semanas se  sacrificaron. Se comprob&oacute; 100 % de protecci&oacute;n en los ratones inmunizados,  por otro lado se observ&oacute; 100 % de infecci&oacute;n en los no inmunizados.  La respuesta inmune, en los niveles local y sist&eacute;mico, se demostr&oacute;  por la presencia de anticuerpos contra la subunidad A y B de la enzima ureasa.      ]]></body>
<body><![CDATA[<p>Sin dudas, las investigaciones recientes acercan m&aacute;s hacia la posibilidad  de combatir la infecci&oacute;n por <i>H. pylori</i> mediante la inmunizaci&oacute;n.  La administraci&oacute;n por v&iacute;a mucosa de subunidades proteicas recombinantes,  junto con adyuvantes mucosos, constituye una estrategia moderna de tratamiento  que previene y cura la infecci&oacute;n en modelos animales, y muestra actividad  terap&eacute;utica parcial en humanos.<sup>28,29</sup>     <p>En la b&uacute;squeda  por lograr una vacuna eficaz en 100 % se ha aislado el genoma de la bacteria para  obtener nuevos ant&iacute;genos. El aislamiento de nuevos ant&iacute;genos, en  combinaci&oacute;n con adyuvantes mucosos seguros (baja toxicidad), podr&iacute;an  ser usados en forma de vacuna oral para ser administrados en ni&ntilde;os antes  de la exposici&oacute;n al microorganismo. La administraci&oacute;n del tratamiento  erradicador con la vacuna, es una alternativa de tratamiento cuya eficacia est&aacute;  a&uacute;n en fase investigativa.<sup>30</sup> <h4> SUMMARY</h4>A bibliographic  review on the schedules of treatment recommended in the infection caused by <i>Helicobacter  pylori</i> was made. The high rates of erradication attained by the triple and  quadruple therapies allow their use as first and second line treatment, respectively.  Those affections associated with the infection, in which the erradicating treatment  should be applied, are related. The utilization of antimicrobials in areas where  the resistance was high reduced the efficacy of the therapy used. The anti-H.  pylori vaccine became a new option of treatment. The use of different mucous sites  of vaccination with adjuvants of low toxicity was also dealt with in this paper.  The therapeutic effectiveness of the vaccine according to the authors proved to  be high in experimental models and achieved 100 % of protection against the infection  caused by this gramnegative bacterium.     <p><i>Subject headings: </i>HELICOBACTER  INFECTIONS/therapy; HELICOBACTER PYLORI. <h4> REFERENCIAS BIBLIOGR&Aacute;FICAS</h4><ol>      <!-- ref --><li> Dunn BE, Cohen H, Blaser MJ. <i>Helicobacter pylori</i>. Clin Microbiol Rev  1997;10(4):720-41.</li>    <!-- ref --><li> Wisniewski RM, Peura DA. <i>Helicobacter pylori</i>:  beyond peptic ulcer disease. Gastroenterologist 1997;5(4):295--305.</li>    <!-- ref --><li> Cave  DR. Transmission and epidemiology of <i>Helicobacter pylori</i>. Am J Med 1996;100(5A):s12-s17.</li>    <!-- ref --><li>  Dunn BE, Cohen H, Blaser MJ. <i>Helicobacter pylori</i>. Clin Microbiol Rev 1997;10(4):720-41.</li>    <!-- ref --><li>  Hopkins RJ, Girardi LS, Turney EA. Relationship between <i>Helicobacter pylori</i>  erradication and reduced duodenal and gastric ulcer recurrence: a review. Gastroenterology  1996;110:1244-52.</li>    <li> Bazzoli F, Pozzato P. Therapy of <i>Helicobacter pylori</i>  infection. J Physiol Pharmacol 1997 Sep;48 suppl 4:39--46.</li>    <!-- ref --><li> NHI Consensus  Conference: <i>Helicobacter pylori</i> in peptic ulcer disease. JAMA 1994;272:65-9.</li>    <!-- ref --><li>  The European Helicobacter Study Group. Current European concepts in the management  of <i>Helicobacter pylori</i> infection. The Maastricht consensus report. Gut  1997,41:8-13.</li>    <!-- ref --><li> Van der Hulst RWM, Keller JJ, Rauws EA, Tytgat GN. Treatment  of <i>Helicobacter pylori</i>: A review of world literature. Helicobacter 1996  Mar;1(1):6-19.</li>    <li> P&eacute;rez Mota A, Alberdi JM, Pita L, Galan JL, Garc&iacute;a  Benito MD, Crespo L <i>et al</i>. <i>Helicobacter pylori</i>, efficacy of the  new triple therapy in six and twelve-day schedules. Rev Esp Enferm Dig 1997 Dec;  89(12):879--84.</li>    <!-- ref --><li> Van der Hulst RWM, van der Ende A, Dekker F, ten kate  FJW, Weel JFL, Keller JJ <i>et al</i>. Effect of <i>Helicobacter pylori</i> erradication  on gastritis in relation to cagA: a prospective one year follow up study. Gastroenterology  1997;113:25-30.</li>    <li> Goodwin CS. Antimicrobial treatment of <i>Helicobacter  pylori</i> infection. Clin Infect Dis 1997 Nov; 25(5):1023--6.</li>    <!-- ref --><li> Van der  Hulst RWM, Keller JJ, Rauws EAJ, Tytgat GN. Treatment of <i>Helicobacter pylori</i>  infection: a review of world literature. Helicobacter 1996 Mar;1(1):6-19.</li>    <li>  De Boer WA, van Etten RJ, Lai JY, Schneeberger PM, Van de Wouw BA, Driessen WM.  Effectiveness of quadruple therapy using lansoprazole, instead of omeprazole,  in curing <i>Helicobacter pylori</i> infection. Helicobacter 1996 Sep;1(3):145-50.</li>    <!-- ref --><li>  Lind T, Veldhuyzen Van Zanten S, Unge P, Spiller R, Bayerdorffer E, O&acute;Morain  C <i>et al</i>. Eradication of <i>Helicobacter pylori</i> using one-week triple  therapies combining omeprazole with two antimicrobials: The MACH I Study. Helicobacter  1996 Sep; 1(3):138-44.</li>    <li> Riff DS, kldd S, Rose P, Haber M, Weissfeld A,  Siepman N. Triple therapy with lansoprazole, clarithromycin and amoxicillin for  the cure of <i>Helicobacter pylori</i> infection: a short report. Helicobacter  1996 Dec; 1(4):238--42.</li>    <li> Pieramico O, Zanetti MV, Innerhofer M, Malfertheiner  P. Omeprazole-based dual and triple therapy for the treatment of <i>Helicobacter  pylori</i> infection in peptic ulcer disease: a randomized trial. Helicobacter  1997 Jun; 2(2):92-7.</li>    ]]></body>
<body><![CDATA[<!-- ref --><li> Thijs JC, van Zwet AA, Moolenaar W, Wolfhagen MJ,  ten Bokkel Huinink J. Triple therapy versus amoxicillin plus omeprazole for treatment  of <i>Helicobacter pylori</i>: a multicenter, prospective, randomized, controlled  study of efficacy and side effects. Am J Gastroenterol 1996;91:93-7.</li>    <li>  Gabryelewicz A, Laszewick W, Dzieniszewski J, Ciok J, Marlicz K, Bielecki D <i>et  al</i>. Multicenter evaluation of dual therapy (omeprazole and amoxicillin) for  <i>Helicobacter pylori</i> associated duodenal and gastric ulcer (two years of  the observation). J Physiol Pharmacol 1997 Sep;48 suppl 4:93-105.</li>    <!-- ref --><li> Van  del Hulst RWM, van der Ende A, Homan A, Roorda P, Dankert J, Tytgat GN <i>et al</i>.  Influence of metronidazole resistance on efficacy of quadruple therapy for <i>Helicobacter  pylori</i> eradication. Gut 1998 Feb;42(2):166-9.</li>    <li> Buckley MJ, Xia HX,  Hyde DM, Keane CT, O&acute;Morain CA. Metronidazole resistance reduces efficacy  of triple therapy and leads to secondary calrithromycin resistance. Dig Dis Sci  1997 Oct;42(10):211-5.</li>    <li> Ling TK, Cheng AF, Sung JJ, Yiu PY, Chung SS.  An increase in <i>Helicobacter pylori</i> strains resistant to metronidazole:  a five year study. Helicobacter 1996 Mar; 1(1):57-61.</li>    <!-- ref --><li> Van del Hulst RWM,  Rauws EAJ, Koyen B, Keller JJ, ten Kate FJW, Dankert J, <i>et al</i> . <i>Helicobacter  pylori</i> reinfection is virtually absent after successful eradication. J Infect  Dis 1997;76:196-200.</li>    <li> Abu Mahfouz MZ, Prasad VM, Santogade P, Cutler AF.  <i>Helicobacter pylori</i> recurrence after successful eradication: A five year  follow up in the United States. Am J Gastroenterol 1997 Nov;92(11):2025-8.</li>    <li>  Kleanthous H, Myers GA, Georgakopoulos KM, Tibbitts TJ, Ingrassia JW. Rectal and  intranasal immunizations with recombinant urease induce distinct local and serum  immune responses in mice and protect against <i>Helicobacter pylori </i>infection.  Infect Immun 1998 Jun;66(6):2879-86.</li>    <li> G&oacute;mez Duarte OG, Lucas B,  Yan ZX, Panthel K, Haas R, Meyer TF. Protection of mice against gastrict colonization  by <i>Helicobacter pylori</i> by single oral dose immunization with attenuated  <i>Salmonella typhimurium</i> producing urease subunits A and B. Vaccine 1998  Mar; 16(5):460-71.</li>    <li> Corthesy Theulaz IE, Hopkins S, Bachmann D, Saldinger  PF, Porta N, Hass R <i>et al</i>. Mice are protected from <i>Helicobacter pylori</i>  infection by nasal immunization with attenuated <i>Salmonella typhimurium</i>  PhoPc expressing urease A and B subunits. Infect Immun 1998 Feb;66(2):581-6.</li>    ]]></body>
<body><![CDATA[<!-- ref --><li>  Kleanthous H, Lec CK, Monath TP. Vaccine development against infection with <i>Helicobacter  pylori</i>. Br Med Bull 1998;54(1):229-41.</li>    <!-- ref --><li> De Magistris MT, Pizza M,  Douce G, Ghiara P, Dougan G, Rappuoli R. Adjuvant effect of non-toxic mutants  of <i>E. Coli</i> heat labile enterotoxin following intranasal, oral and intravaginal  immunization. Dev Biol Stand 1998;92:123-6.</li>    <li> Czinn SJ. What is the role  for vaccination in <i>Helicobacter pylori</i>?. Gastroenterology 1997 Dec; 113(6  suppl):s 149-53.</li>    </ol>    <p>Recibido 10 de mayo de 1999. Aprobado: 5 de noviembre  de 1999.     <br>Dr. <i>Noel Padr&oacute;n P&eacute;rez.</i> Edificio SP-21, Apartamento  23-E. Micro 10, Alamar, municipio Habana del Este, Ciudad de La Habana, Cuba.       ]]></body><back>
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