<?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>0120-5633</journal-id>
<journal-title><![CDATA[Revista Colombiana de Cardiología]]></journal-title>
<abbrev-journal-title><![CDATA[Rev. Col. Cardiol.]]></abbrev-journal-title>
<issn>0120-5633</issn>
<publisher>
<publisher-name><![CDATA[Sociedad Colombiana de Cardiologia. Oficina de Publicaciones]]></publisher-name>
</publisher>
</journal-meta>
<article-meta>
<article-id>S0120-56332005000400004</article-id>
<title-group>
<article-title xml:lang="es"><![CDATA[Trasplante autólogo de células progenitoras derivadas de la médula ósea, por vía intramiocárdica, para revascularización en cardiopatía isquémica crónica]]></article-title>
<article-title xml:lang="en"><![CDATA[Autologous intramyocardial transplant of bone marrow derived stem cells for revascularization in ischemic chronic cardiopathy]]></article-title>
</title-group>
<contrib-group>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Velásquez]]></surname>
<given-names><![CDATA[Óscar]]></given-names>
</name>
<xref ref-type="aff" rid="A02"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Senior]]></surname>
<given-names><![CDATA[Juan M]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Cuéllar]]></surname>
<given-names><![CDATA[Francisco]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Velásquez]]></surname>
<given-names><![CDATA[Margarita]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[García]]></surname>
<given-names><![CDATA[Luis F]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Navas]]></surname>
<given-names><![CDATA[Claudia]]></given-names>
</name>
<xref ref-type="aff" rid="A02"/>
</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 Universitario San Vicente de Paul  ]]></institution>
<addr-line><![CDATA[Medellín ]]></addr-line>
<country>Colombia</country>
</aff>
<pub-date pub-type="pub">
<day>00</day>
<month>08</month>
<year>2005</year>
</pub-date>
<pub-date pub-type="epub">
<day>00</day>
<month>08</month>
<year>2005</year>
</pub-date>
<volume>12</volume>
<numero>2</numero>
<fpage>80</fpage>
<lpage>84</lpage>
<copyright-statement/>
<copyright-year/>
<self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_arttext&amp;pid=S0120-56332005000400004&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_abstract&amp;pid=S0120-56332005000400004&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_pdf&amp;pid=S0120-56332005000400004&amp;lng=en&amp;nrm=iso"></self-uri><abstract abstract-type="short" xml:lang="es"><p><![CDATA[Introducción: estudios experimentales y clínicos demuestran que la implantación intramiocárdica de células progenitoras derivadas de la médula ósea, produce angiogénesis y mejora la función cardiaca en pacientes con cardiopatía isquémica crónica. Metodología: este es el reporte del seguimiento a dos meses de un paciente con cardiopatía isquémica crónica no susceptible de revascularización quirúrgica o percutánea, a quien se le realizó ,por vía epicárdica, un implánte de células progenitoras derivadas de médula ósea movilizadas con factor de crecimiento granulocito-macrófago. Resultados: se demostró mejoría significativa en la sintomatología, en la capacidad funcional (1.8 MET a 10 MET), en el estado funcional (IV a I), en el tamaño del defecto de perfusión miocárdica por medicina nuclear, en la fracción de eyección y en la disminución del volumen sistólico final del ventrículo izquierdo, sin observar complicaciones relacionadas con el procedimiento. Conclusión: el trasplante de células progenitoras derivadas de la médula ósea es una terapia efectiva y segura para promover neovascularización y para mejorar la contractilidad y la perfusión miocárdica en los pacientes con cardiopatía isquémica crónica pobres candidatos a cirugía.]]></p></abstract>
<abstract abstract-type="short" xml:lang="en"><p><![CDATA[Introduction: experimental and clinical studies have demonstrated that intramyocardial bone marrow derived stem cells implantation produce angiogenesis and improvement of cardiac function in patients with chronic ischemic cardiopathy. Methodology: this is a two months follow-up report of a patient with chronic ischemic cardiopathy not susceptible of surgical or percutaneous revascularization, to whom bone marrow stem cells mobilized with granulocyte - macrophage growth factor was implanted. Results: significant improvement was demonstrated in symptomatology, functional capacity (1.8 Mets to 10 Mets), functional state (IV to I), size of the myocardial perfusion defect by nuclear medicine, in the ejection fraction and diminution of the final left ventricular systolic volume, without complications related to the procedure. Conclusion: bone marrow derived stem cells transplant is an effective and safe therapy in order to promote neo-vascularization and improve contractility and myocardic perfusion in patients with chronic ischemic cardiopathy considered poor surgical candidates.]]></p></abstract>
<kwd-group>
<kwd lng="es"><![CDATA[cardiopatía isquémica]]></kwd>
<kwd lng="es"><![CDATA[células madre]]></kwd>
<kwd lng="es"><![CDATA[intramiocárdico]]></kwd>
<kwd lng="es"><![CDATA[angiogénesis]]></kwd>
<kwd lng="es"><![CDATA[médula ósea]]></kwd>
<kwd lng="en"><![CDATA[ischemic cardiopathy]]></kwd>
<kwd lng="en"><![CDATA[stem cells]]></kwd>
<kwd lng="en"><![CDATA[intramyocardic]]></kwd>
<kwd lng="en"><![CDATA[angiogenesis]]></kwd>
<kwd lng="en"><![CDATA[bone marrow]]></kwd>
</kwd-group>
</article-meta>
</front><body><![CDATA[ <P align="center"><strong><font size="4" face="Times New Roman, Times, serif">Trasplante    aut&oacute;logo de c&eacute;lulas progenitoras derivadas de la m&eacute;dula    &oacute;sea, por v&iacute;a intramioc&aacute;rdica, para revascularizaci&oacute;n    en cardiopat&iacute;a isqu&eacute;mica cr&oacute;nica</font></strong></P> <B>     <P ALIGN="CENTER"><font face="Times New Roman, Times, serif">Autologous intramyocardial    transplant of bone marrow derived stem cells for revascularization in ischemic    chronic cardiopathy</font></P> </B>      <P ALIGN="CENTER"><font face="Times New Roman, Times, serif">&Oacute;scar Vel&aacute;squez,    MD.(2); Juan M. Senior, MD.(1, 2); Francisco Cu&eacute;llar, MD.(1, 2); Margarita    Vel&aacute;squez, MD.(1); Luis F. Garc&iacute;a, MD., MSc.(1); Claudia Navas,    MD.(2)</font></P>     <P ALIGN="CENTER"><font face="Times New Roman, Times, serif">(1) Universidad de    Antioquia, Medell&iacute;n, Colombia.    <BR>   (2) Hospital Universitario San Vicente de Paul, Medell&iacute;n, Colombia.    <BR>   Correspondencia: &Oacute;scar Vel&aacute;squez Uribe, MD. Grupo de Terapia Celular    Regenerativa. Hospital Universitario San Vicente de Paul, Universidad de Antioquia.    Calle 64, carrera 51D. Tel&eacute;fono: 516-23-53 ext. 230. Medell&iacute;n,    Colombia. Correo electr&oacute;nico: <a href="mailto:ooavelasquez@epm.net.co">ooavelasquez@epm.net.co</a></font></P>     <P> <HR WIDTH="64%"> <font face="Times New Roman, Times, serif">      <P ALIGN="JUSTIFY">Introducci&oacute;n: estudios experimentales y cl&iacute;nicos    demuestran que la implantaci&oacute;n intramioc&aacute;rdica de c&eacute;lulas    progenitoras derivadas de la m&eacute;dula &oacute;sea, produce angiog&eacute;nesis    y mejora la funci&oacute;n cardiaca en pacientes con cardiopat&iacute;a isqu&eacute;mica    cr&oacute;nica.</P>     <P ALIGN="JUSTIFY">Metodolog&iacute;a: este es el reporte del seguimiento a dos    meses de un paciente con cardiopat&iacute;a isqu&eacute;mica cr&oacute;nica    no susceptible de revascularizaci&oacute;n quir&uacute;rgica o percut&aacute;nea,    a quien se le realiz&oacute; ,por v&iacute;a epic&aacute;rdica, un impl&aacute;nte    de c&eacute;lulas progenitoras derivadas de m&eacute;dula &oacute;sea movilizadas    con factor de crecimiento granulocito-macr&oacute;fago.</P>     <P ALIGN="JUSTIFY">Resultados: se demostr&oacute; mejor&iacute;a significativa    en la sintomatolog&iacute;a, en la capacidad funcional (1.8 MET a 10 MET), en    el estado funcional (IV a I), en el tama&ntilde;o del defecto de perfusi&oacute;n    mioc&aacute;rdica por medicina nuclear, en la fracci&oacute;n de eyecci&oacute;n    y en la disminuci&oacute;n del volumen sist&oacute;lico final del ventr&iacute;culo    izquierdo, sin observar complicaciones relacionadas con el procedimiento.</P>     ]]></body>
<body><![CDATA[<P ALIGN="JUSTIFY">Conclusi&oacute;n: el trasplante de c&eacute;lulas progenitoras    derivadas de la m&eacute;dula &oacute;sea es una terapia efectiva y segura para    promover neovascularizaci&oacute;n y para mejorar la contractilidad y la perfusi&oacute;n    mioc&aacute;rdica en los pacientes con cardiopat&iacute;a isqu&eacute;mica cr&oacute;nica    pobres candidatos a cirug&iacute;a.</P>     <P ALIGN="JUSTIFY">Palabras clave: cardiopat&iacute;a isqu&eacute;mica, c&eacute;lulas    madre, intramioc&aacute;rdico, angiog&eacute;nesis, m&eacute;dula &oacute;sea.</P> </font>     <P> <HR WIDTH="64%"> <font face="Times New Roman, Times, serif">     <P ALIGN="JUSTIFY">Introduction: experimental and clinical studies have demonstrated    that intramyocardial bone marrow derived stem cells implantation produce angiogenesis    and improvement of cardiac function in patients with chronic ischemic cardiopathy.</P>     <P ALIGN="JUSTIFY">Methodology: this is a two months follow-up report of a patient    with chronic ischemic cardiopathy not susceptible of surgical or percutaneous    revascularization, to whom bone marrow stem cells mobilized with granulocyte    - macrophage growth factor was implanted. </P>     <P ALIGN="JUSTIFY">Results: significant improvement was demonstrated in symptomatology,    functional capacity (1.8 Mets to 10 Mets), functional state (IV to I), size    of the myocardial perfusion defect by nuclear medicine, in the ejection fraction    and diminution of the final left ventricular systolic volume, without complications    related to the procedure. </P>     <P ALIGN="JUSTIFY">Conclusion: bone marrow derived stem cells transplant is an    effective and safe therapy in order to promote neo-vascularization and improve    contractility and myocardic perfusion in patients with chronic ischemic cardiopathy    considered poor surgical candidates. </P>     <P ALIGN="JUSTIFY">Key words: ischemic cardiopathy, stem cells, intramyocardic,    angiogenesis, bone marrow. </P> </font>     <P> <HR WIDTH="64%"> <font face="Times New Roman, Times, serif"><STRONG>      <P ALIGN="CENTER">Introducci&oacute;n</P> </STRONG>     ]]></body>
<body><![CDATA[<P ALIGN="JUSTIFY">El tratamiento de la enfermedad coronaria ha variado sustancialmente    en la &uacute;ltima d&eacute;cada debido a la modificaci&oacute;n de los factores    de riesgo, la utilizaci&oacute;n de nuevos y m&aacute;s potentes medicamentos    tales como: antiagregantes, betabloqueadores e inhibidores de la enzima convertidora    de angiotensina y bloqueadores de los receptores de angiotensina II, y al avance    significativo en las t&eacute;cnicas de revascularizaci&oacute;n tanto percut&aacute;nea    como quir&uacute;rgica, las cuales han reducido en forma significativa la morbimortalidad    por cardiopat&iacute;a isqu&eacute;mica y falla cardiaca secundaria. </P>     <P ALIGN="JUSTIFY">Es posible ofrecer un trasplante cardiaco ortot&oacute;pico    (1), y actualmente para una mayor poblaci&oacute;n, el trasplante de c&eacute;lulas    progenitoras (2, 3), a un porcentaje de pacientes que no se beneficia de los    procesos de revascularizaci&oacute;n descritos inicialmente (quir&uacute;rgico    y/o percut&aacute;neo), por la presencia de lechos arteriales coronarios distales    deficientes, oclusiones arteriales cr&oacute;nicas y comorbilidades (31); adicionalmente,    las oclusiones tard&iacute;as de los puentes coronarios o con restenosis intrastent,    tambi&eacute;n hacen parte de este grupo, el cual se caracteriza por deterioro    en la calidad de vida debido al desarrollo de angina refractaria y falla cardiaca    a pesar de efectuar un tratamiento m&eacute;dico &oacute;ptimo. </P>     <P ALIGN="JUSTIFY">Cl&aacute;sicamente, se ha considerado que durante la etapa    embrionaria y fetal hay replicaci&oacute;n activa de cardiomiocitos por la presencia    de reguladores positivos del ciclo celular permitiendo la carioquinesis (4).    Antes del nacimiento, la actividad disminuye y se produce duplicaci&oacute;n    gen&oacute;mica con cardiomiocitos binucleados con posterior aumento de reguladores    negativos que detienen el ciclo celular en un estado postmit&oacute;tico, sin    replicaci&oacute;n celular activa significativa en la edad adulta (4-6). Lo    anterior explica por qu&eacute; despu&eacute;s de la lesi&oacute;n producida    por un evento isqu&eacute;mico mioc&aacute;rdico, se pierde un n&uacute;mero    significativo de cardiomiocitos y hay deterioro de la funci&oacute;n ventricular    por el proceso de remodelaci&oacute;n a largo plazo (7). Las c&eacute;lulas    progenitoras, pueden tener origen en el embri&oacute;n o en estructuras adultas,    como las c&eacute;lulas sat&eacute;lites o mioblastos esquel&eacute;ticos y    c&eacute;lulas derivadas de la m&eacute;dula &oacute;sea. Resultados de estudios    experimentales y cl&iacute;nicos demuestran que las c&eacute;lulas progenitoras    derivadas de la m&eacute;dula &oacute;sea pueden utilizarse no s&oacute;lo para    regenerar cardiomiocitos sino para producir angiog&eacute;nesis, debido a su    plasticidad a trav&eacute;s de mecanismos como transdiferenciaci&oacute;n y    fusi&oacute;n (8-10).</P>     <P ALIGN="JUSTIFY">El objetivo de este reporte es demostrar la seguridad y efectividad    del trasplante aut&oacute;logo de c&eacute;lulas progenitoras derivadas de la    m&eacute;dula &oacute;sea (TCPDMO) movilizadas con factor de crecimiento granulocito-macr&oacute;fago    en un paciente con cardiopat&iacute;a isqu&eacute;mica cr&oacute;nica.</P> <STRONG>     <P ALIGN="CENTER">Paciente y m&eacute;todos</P> </STRONG>     <P ALIGN="JUSTIFY">Este es un reporte del seguimiento a dos meses, de un paciente    con cardiopat&iacute;a isqu&eacute;mica cr&oacute;nica, pobre candidato para    revascularizaci&oacute;n quir&uacute;rgica o percut&aacute;nea, atendido en    la Unidad Cardiovascular y de Trasplantes del Hospital Universitario San Vicente    de Paul, a quien se le realiz&oacute; TCPDMO por v&iacute;a epic&aacute;rdica.</P>     <P ALIGN="JUSTIFY">El caso se discuti&oacute; en consenso m&eacute;dico-quir&uacute;rgico    de la instituci&oacute;n y se suministr&oacute; el consentimiento informado    evaluado por el Comit&eacute; de &Eacute;tica M&eacute;dica al paciente y a    la familia acerca de la patolog&iacute;a y el procedimiento. Se obtuvo historia    cl&iacute;nica completa y paracl&iacute;nicos de base como: hemoleucograma y    sedimentaci&oacute;n, PCR, BUN, creatinina, ionograma, CK MB, troponina I, LDH,    &aacute;cido &uacute;rico, perfil lip&iacute;dico y glicemia, electrocardiograma    de doce derivaciones, angiograf&iacute;a coronaria, ecocardiograma M, 2D, Doppler    color, viabilidad e isquemia mioc&aacute;rdica con talio reposo-redistribuci&oacute;n-reinyecci&oacute;n    y monitoreo Holter. El paciente se monitoriz&oacute; en la unidad de cuidado    intensivo cardiovascular por 48 horas, y se realiz&oacute; manejo convencional    posquir&uacute;rgico. Luego del alta se reevalu&oacute; a los dos meses post-procedimiento    con una evaluaci&oacute;n cl&iacute;nica completa, hemoleucograma y sedimentaci&oacute;n,    PCR, BUN, creatinina, troponina I, CPK MB, qu&iacute;mica sangu&iacute;nea,    ecocardiograma, electrocardiograma, viabilidad mioc&aacute;rdica e isquemia    por medicina nuclear y monitoreo Holter.</P>     <P ALIGN="JUSTIFY">Las c&eacute;lulas progenitoras derivadas de la m&eacute;dula    &oacute;sea se obtuvieron por la estimulaci&oacute;n del paciente (aut&oacute;logas)    con factor estimulante de colonias granulocito-macr&oacute;fago por v&iacute;a    subcut&aacute;nea 10 mcg/kg/d&iacute;a, en los 5 d&iacute;as previos a su implantaci&oacute;n.    El d&iacute;a del procedimiento se lleva al paciente a la sala de cirug&iacute;a    y bajo anestesia local se extraen 50 mL de m&eacute;dula &oacute;sea por aspiraci&oacute;n    en la cresta il&iacute;aca. Las c&eacute;lulas mononucleares se a&iacute;slan    por gradiente de densidad en Ficoll-Paque Plus en el laboratorio de Inmunolog&iacute;a    de la Facultad de Medicina de la Universidad de Antioquia, por citometr&iacute;a    de flujo el conteo de las CD34, CD4, CD8, CD20, CD 19, CD14 y CD 56 y cultivos    para hongos y bacterias (11). </P>     <P ALIGN="JUSTIFY">La suspensi&oacute;n celular contiene 726 x 106 de c&eacute;lulas    mononucleares, 24,7 x 106 CD34+, la viabilidad celular fue del 100% por azul    de tripano, CD34+CD45LOW 1%, CD34+ICAM1+ 3,4% y los cultivos microbiol&oacute;gicos    fueron negativos.</P>     <P ALIGN="JUSTIFY">La implantaci&oacute;n se realiz&oacute; en la sala de cirug&iacute;a.    Luego de la esternotom&iacute;a convencional se visualiz&oacute; la zona de    necrosis y el &aacute;rea isqu&eacute;mica, y se procedi&oacute; a la implantaci&oacute;n    de la suspensi&oacute;n celular inyectando en forma directa 0,2 mL en 10 oportunidades,    con aguja fina a lo largo de toda la circunferencia del borde de la lesi&oacute;n.</P>     ]]></body>
<body><![CDATA[<P ALIGN="CENTER"><strong>Resultados </strong></P> <STRONG>     <P ALIGN="JUSTIFY">Caso cl&iacute;nico</P> </STRONG>     <P ALIGN="JUSTIFY">Paciente de 59 a&ntilde;os, hipertenso y dislipid&eacute;mico,    con enfermedad coronaria severa de tres vasos, revascularizado en 1996 en forma    quir&uacute;rgica, con adecuada evoluci&oacute;n. Asintom&aacute;tico hasta    agosto de 2003, cuando consult&oacute; por angina estable de dos meses de evoluci&oacute;n    progresiva estado funcional II Clasificaci&oacute;n Canadiense (CCS); se optimiz&oacute;    el manejo m&eacute;dico adicionando nitratos orales y sublinguales a su tratamiento    con &aacute;cido acetilsalic&iacute;lico, metoprolol, lovastatina y captopril.    Se realiz&oacute; angiograf&iacute;a coronaria y de puentes, con lo que se demostr&oacute;    oclusi&oacute;n del puente de la arteria mamaria a la descendente anterior y    del puente venoso a la coronaria derecha, permeabilidad del puente venoso a    la primera obtusa marginal, oclusi&oacute;n cr&oacute;nica del lecho nativo    (CD-DA) y p&eacute;simos lechos distales; la medicina nuclear demostr&oacute;    un gran territorio isqu&eacute;mico en la cara anterior e inferior y una peque&ntilde;a    zona de necrosis apical. Se consider&oacute; pobre candidato para nueva revascularizaci&oacute;n    quir&uacute;rgica o percut&aacute;nea, por lo cual se optimiz&oacute; el manejo    m&eacute;dico con el aumento de la dosis de nitratos orales y la adici&oacute;n    de un calcioantagonista. El paciente persisti&oacute; en estado funcional II,    hasta septiembre de 2003 en el que progres&oacute; a estado funcional IV, con    gran compromiso de su calidad de vida a pesar de la utilizaci&oacute;n de 120    mg/d&iacute;a de nitrato oral, m&aacute;s 30 mg de nitrato por v&iacute;a sublingual    cada d&iacute;a, betabloqueadores, calcioantagonistas, inhibidores de la enzima    convertidora de angiotensina y estatinas. Se discuti&oacute; en consenso m&eacute;dico-quir&uacute;rgico    en el cual se recomend&oacute; revascularizaci&oacute;n percut&aacute;nea de    la arteria descendente anterior, con intento fallido de angioplastia el 30 de    septiembre de 2003. Posterior a esto, se decidi&oacute; realizar TCPDMO por    v&iacute;a epic&aacute;rdica. </P>     <P ALIGN="JUSTIFY">El d&iacute;a del trasplante el paciente fue trasladado a la    sala de cirug&iacute;a donde se realiz&oacute; el aspirado de m&eacute;dula    &oacute;sea. Se inici&oacute; el procedimiento quir&uacute;rgico en forma convencional    a trav&eacute;s de una esternotom&iacute;a media, extensa liberaci&oacute;n    de m&uacute;ltiples adherencias secundarias a la revascularizaci&oacute;n quir&uacute;rgica    previa, y posteriormente se realiz&oacute; la implantaci&oacute;n de las c&eacute;lulas    en la forma descrita. Durante el procedimiento present&oacute; hipotensi&oacute;n    al luxar el coraz&oacute;n para la implantaci&oacute;n de las c&eacute;lulas    en la cara inferior, la cual se recuper&oacute; r&aacute;pidamente con la administraci&oacute;n    de cristaloides y la suspensi&oacute;n de la maniobra. No se encontr&oacute;    ninguna arteria susceptible de revascularizaci&oacute;n por puentes aortocoronarios.    Se termin&oacute; el procedimiento en forma convencional y el paciente fue extubado    y trasladado a la unidad de cuidados intensivos. No se presentaron complicaciones    en el postrasplante inmediato tales como arritmias, sangrado en el sitio de    la implantaci&oacute;n, elevaci&oacute;n de marcadores s&eacute;ricos de injuria    mioc&aacute;rdica, derrame peric&aacute;rdico o aumento de la efusi&oacute;n    pleural atribuibles al procedimiento, y fue dado de alta en el cuarto d&iacute;a.  </P>     <P ALIGN="JUSTIFY">En el seguimiento a dos meses en el programa de rehabilitaci&oacute;n    cardiaca, se demostr&oacute; mejor&iacute;a significativa en los par&aacute;metros    evaluados (<A HREF="/img/revistas/rcca/v12n2/a4t1.jpg">Tabla 1</A>), pasando    a estado funcional I, sin episodios anginosos con actividades de la vida diaria,    disminuci&oacute;n en el consumo de nitratos (30 mg/d&iacute;a oral y 0 mg/d&iacute;a    sublingual), sin cambios en la dosis de las otras medicaciones y con disminuci&oacute;n    significativa en el defecto de perfusi&oacute;n durante el ejercicio en la medicina    nuclear (Figuras <A HREF="#figura1">1</A> y <A HREF="#figura2">2</A>). Despu&eacute;s    de dos meses no se detectaron alteraciones del ritmo cardiaco en el Holter de    control. </P>     <P ALIGN="JUSTIFY"><A HREF="/img/revistas/rcca/v12n2/a4t1.jpg"><I>Tabla 1</I></A>.    Par&aacute;metros de respuesta A DOS meses de seguimiento</P> </font>     <P ALIGN="CENTER">&nbsp;</P>     <P ALIGN="CENTER"><font face="Times New Roman, Times, serif"><A NAME="figura1"></A></font></P>     <P ALIGN="CENTER"><font face="Times New Roman, Times, serif"><IMG SRC="/img/revistas/rcca/v12n2/a4fig1.jpg" WIDTH=370 HEIGHT=376></font></P>     <P ALIGN="JUSTIFY">&nbsp;</P>     ]]></body>
<body><![CDATA[<P ALIGN="CENTER"><font face="Times New Roman, Times, serif"><A NAME="figura2"></A></font></P>     <P ALIGN="CENTER"><font face="Times New Roman, Times, serif"><IMG SRC="/img/revistas/rcca/v12n2/a4fig2.jpg" WIDTH=370 HEIGHT=396></font></P>     <P ALIGN="CENTER">&nbsp;</P> <STRONG>     <P ALIGN="CENTER"><font face="Times New Roman, Times, serif">Discusi&oacute;n</font></P> </STRONG>     <P ALIGN="JUSTIFY"><font face="Times New Roman, Times, serif">Nuestros resultados    demuestran que la implantaci&oacute;n epic&aacute;rdica de c&eacute;lulas progenitoras    derivadas de la m&eacute;dula &oacute;sea movilizadas con factor de crecimiento    granulocito-macr&oacute;fago en pacientes con cardiopat&iacute;a isqu&eacute;mica    cr&oacute;nica es segura y eficaz. Orlic y colaboradores (8) y otros grupos    de investigaci&oacute;n han demostrado en forma fehaciente la posibilidad de    diferenciaci&oacute;n de las c&eacute;lulas progenitoras derivadas de la m&eacute;dula    &oacute;sea Lin– cKit+ en cardiomiocitos, c&eacute;lulas endoteliales y de m&uacute;sculo    liso vascular, lo que permite no s&oacute;lo regenerar tejido mioc&aacute;rdico    sino revascularizar el tejido isqu&eacute;mico (12 -15). La utilizaci&oacute;n    de factor estimulante de crecimiento de colonias de granulocito-macr&oacute;fago    aumenta el n&uacute;mero de c&eacute;lulas progenitoras endoteliales en la m&eacute;dula    &oacute;sea y circulantes, asegurando una mayor concentraci&oacute;n de &eacute;stas    y menor volumen de la suspensi&oacute;n celular para la implantaci&oacute;n    (16,17) lo cual es crucial cuando se realizan inyecciones intramioc&aacute;rdicas    como en este caso; adem&aacute;s, estimula la maduraci&oacute;n y activaci&oacute;n    de las c&eacute;lulas progenitoras (18), posiblemente del subgrupo que se requiere    para regeneraci&oacute;n y revascularizaci&oacute;n, y promueve el crecimiento    de colaterales arteriales cardiacas (19). Sin embargo, no se pueden pasar por    alto los efectos secundarios protromb&oacute;ticos reportados en dos casos relacionados    con la administraci&oacute;n del factor y leucocitosis (20, 21) no confirmados    en otros estudios (16, 22-26).</font></P>     <P ALIGN="JUSTIFY"><font face="Times New Roman, Times, serif">La mejor&iacute;a    dram&aacute;tica experimentada por este paciente luego de dos meses, evidenciada    por la mejor&iacute;a en la perfusi&oacute;n mioc&aacute;rdica y adem&aacute;s    por el cambio en el estado funcional de IV a I CCS, el aumento significativo    en el n&uacute;mero de metros caminados en el test de los seis minutos, el cambio    de su capacidad de ejercicio de 1,8 MET a 10 MET, la disminuci&oacute;n de los    episodios anginosos y la dosis de vasodilatadores consumidos tanto por v&iacute;a    oral como sublingual, concuerda con lo reportado en la literatura (9-10,27-29)    y constituye una base firme para recomendar el TCPDMO en pacientes con cardiopat&iacute;a    isqu&eacute;mica cr&oacute;nica, pobres candidatos a revascularizaci&oacute;n    quir&uacute;rgica o percut&aacute;nea, sin esperanza de mejor&iacute;a (30).    El cambio en la funci&oacute;n ventricular con aumento en la fracci&oacute;n    de eyecci&oacute;n, disminuci&oacute;n del volumen de fin de s&iacute;stole    del ventr&iacute;culo izquierdo y la disminuci&oacute;n del defecto de perfusi&oacute;n    demuestran la bondad de esta terapia (29) y la ausencia de efectos secundarios.    Persisten interrogantes acerca de la carga celular &amp;laquo;ideal&amp;raquo;,    as&iacute; como de la v&iacute;a de implantaci&oacute;n en los diferentes tipos    de cardiopat&iacute;as, que pueden beneficiar en mayor grado a los pacientes.    </font></P> <STRONG>     <P ALIGN="CENTER"><font face="Times New Roman, Times, serif">Bibliograf&iacute;a</font></P> </STRONG>     <!-- ref --><P ALIGN="JUSTIFY"><font face="Times New Roman, Times, serif">1. Kirklin JK, Young    JB, McGiffin D. Recipient evaluation and selection. In: Kirklin JB, Young JB,    McGiffin DC eds. Heart Transplantation. 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