<?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>0034-7450</journal-id>
<journal-title><![CDATA[Revista Colombiana de Psiquiatría]]></journal-title>
<abbrev-journal-title><![CDATA[rev.colomb.psiquiatr.]]></abbrev-journal-title>
<issn>0034-7450</issn>
<publisher>
<publisher-name><![CDATA[Asociacion Colombiana de Psiquiatria.]]></publisher-name>
</publisher>
</journal-meta>
<article-meta>
<article-id>S0034-74502014000200008</article-id>
<title-group>
<article-title xml:lang="es"><![CDATA[Factores asociados con el declive cognitivo en población menor de 65 años. Una revisión sistemática]]></article-title>
<article-title xml:lang="en"><![CDATA[Factors Associated with Cognitive Decline in a Population Less than 65 Years Old. A Systematic Review]]></article-title>
</title-group>
<contrib-group>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Aguirre-Acevedo]]></surname>
<given-names><![CDATA[Daniel Camilo]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Henao]]></surname>
<given-names><![CDATA[Eliana]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Tirado]]></surname>
<given-names><![CDATA[Victoria]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Muñoz]]></surname>
<given-names><![CDATA[Claudia]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Giraldo Arango]]></surname>
<given-names><![CDATA[Diana]]></given-names>
</name>
<xref ref-type="aff" rid="A02"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Lopera Restrepo]]></surname>
<given-names><![CDATA[Francisco]]></given-names>
</name>
<xref ref-type="aff" rid="A03"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Jaimes Barragán]]></surname>
<given-names><![CDATA[Fabián]]></given-names>
</name>
<xref ref-type="aff" rid="A03"/>
</contrib>
</contrib-group>
<aff id="A01">
<institution><![CDATA[,Universidad de Antioquia  ]]></institution>
<addr-line><![CDATA[Medellín ]]></addr-line>
<country>Colombia</country>
</aff>
<aff id="A02">
<institution><![CDATA[,Universidad de San Buenaventura  ]]></institution>
<addr-line><![CDATA[Medellín ]]></addr-line>
<country>Colombia</country>
</aff>
<aff id="A03">
<institution><![CDATA[,Universidad de Antioquia Facultad de Medicina Hospital Pablo Tobón Uribe]]></institution>
<addr-line><![CDATA[Medellín ]]></addr-line>
<country>Colombia</country>
</aff>
<pub-date pub-type="pub">
<day>00</day>
<month>04</month>
<year>2014</year>
</pub-date>
<pub-date pub-type="epub">
<day>00</day>
<month>04</month>
<year>2014</year>
</pub-date>
<volume>43</volume>
<numero>2</numero>
<fpage>113</fpage>
<lpage>122</lpage>
<copyright-statement/>
<copyright-year/>
<self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_arttext&amp;pid=S0034-74502014000200008&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_abstract&amp;pid=S0034-74502014000200008&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_pdf&amp;pid=S0034-74502014000200008&amp;lng=en&amp;nrm=iso"></self-uri><abstract abstract-type="short" xml:lang="es"><p><![CDATA[Introducción: Se ha señalado antes del diagna que el deterioro cognitivo comienza 20 años antes del diagnóstico de la demencia. Además de la edad, diversos factores médicos, socioeconómicos y conductuales pueden estar asociados al declive cognitivo. El objetivo de esta revisión sistemática es resumir la evidencia de factores de riesgo o protectores relacionados con el declive cognitivo en población menor de 65 años. Métodos: Se realizó una revisión sistemática mediante una estrategia de búsqueda en bases de datos MEDLINE y Embase, incluyendo estudios con diseño longitudinal que analizaran el efecto de factores protectores o de riesgo en el declive cognitivo de población adulta menor de 65 años. Resultados: Se incluyeron 22 estudios en la presente revisión. Factores como diabetes mellitus, hiperinsulinemia, sobrepeso u obesidad, síndrome metabólico, nivel educativo, actividad física, estimulación cognitiva, estado civil y calidad de la dieta podrían estar relacionados con el declive cognitivo antes de los 65 años. Conclusiones: Factores de riesgo cardiovasculares y de estilos de vida pueden estar asociados al declive cognitivo en menores de 65 años. Sin embargo, la calidad de la evidencia es baja.]]></p></abstract>
<abstract abstract-type="short" xml:lang="en"><p><![CDATA[Introduction: Cognitive decline could begin 20 years before the diagnosis of dementia. Besides age, several factors related to medical, socioeconomic, and behavioral and genetic condition may be associated with cognitive decline. The aim of this systematic review was to summarize evidence on the risk and protective factors for cognitive decline in people under 65 years old. Methods: A systematic review was conducted using a search strategy in MEDLINE and Embase, including longitudinal studies to analyze the effect of protective or risk factors on cognitive decline in a population under 65 years old. Results: A total of 22 studies were included in this review. Factors such as diabetes, hyperinsulinemia, overweight or obesity, metabolic syndrome, education, physical activity, cognitive stimulation, marital status and diet, could be related to cognitive decline before 65 years of age. Conclusions: Cardiovascular risk factors and lifestyle conditions may be associated with cognitive decline before 65 years of age. However, the quality of the evidence was low.]]></p></abstract>
<kwd-group>
<kwd lng="es"><![CDATA[Deterioro cognitivo]]></kwd>
<kwd lng="es"><![CDATA[Factores de riesgo]]></kwd>
<kwd lng="es"><![CDATA[Demencia]]></kwd>
<kwd lng="es"><![CDATA[Revisión sistemática]]></kwd>
<kwd lng="en"><![CDATA[Cognitive decline]]></kwd>
<kwd lng="en"><![CDATA[Risk factors]]></kwd>
<kwd lng="en"><![CDATA[Dementia]]></kwd>
<kwd lng="en"><![CDATA[Systematic review]]></kwd>
</kwd-group>
</article-meta>
</front><body><![CDATA[  <font face="verdana" size="2">     <p><B>Art&iacute;culo de revisi&oacute;n</B></p>     <p align="center"><font size="4"><b>Factores asociados con el declive cognitivo en poblaci&oacute;n menor de 65 a&ntilde;os. Una revisi&oacute;n sistem&aacute;tica</b></font></p>     <p align="center"><font size="3"><b>Factors Associated with Cognitive Decline in a Population Less than 65 Years Old. A Systematic Review</b></font></p>     <p align="center"><i><b>Daniel Camilo Aguirre-Acevedo</b></i><sup>a,*</sup>, <i><b>Eliana Henao</b></i><sup>a</sup>, <i><b>Victoria Tirado</b></i><sup>a</sup>, <i><b>Claudia Mu&ntilde;oz</b></i><sup>a</sup>, <i><b>Diana Giraldo Arango</b></i><sup>b</sup>, <i><b>Francisco Lopera Restrepo</b></i><sup>a,c</sup> y <i><b>Fabi&aacute;n Jaimes Barrag&aacute;n</b></i><sup>c</sup></p>     <p><Sup>a</Sup><I>Grupo de Neurociencias de Antioquia, Facultad de Medicina, Universidad de Antioquia, Medell&iacute;n, Colombia </I>    <br> <Sup>b</Sup><I>Facultad de Psicolog&iacute;a, Universidad de San Buenaventura, Medell&iacute;n, Colombia </I>    <br> <Sup>c</Sup><I>Grupo Acad&eacute;mico de Epidemiolog&iacute;a Cl&iacute;nica y Departamento de Medicina Interna, Facultad de Medicina, Universidad de Antioquia; Unidad de Investigaciones, Hospital Pablo Tob&oacute;n Uribe, Medell&iacute;n, Colombia </I></p>     <p><sup>*</sup>Author para correspondencia. Correo electr&oacute;nico: <a href="mailto:agua.dc@gmail.com">agua.dc@gmail.com</a> (D.C. Aguirre-Acevedo). <a href="http://dx.doi.org/10.1016/j.rcp.2014.02.009" target="_blank">http://dx.doi.org/10.1016/j.rcp.2014.02.009</a>.</p>     <p><I>Historia del art&iacute;culo: </I>Recibido el 23 de diciembre de 2013 Aceptado el 24 de febrero de 2014 <I>On-line </I>el 29 de mayo de 2014 </p> <hr>     ]]></body>
<body><![CDATA[<p><font size="3"><b>Resumen</b></font></p>     <p><I>Introducci&oacute;n:</I> Se ha se&ntilde;alado antes del diagna que el deterioro cognitivo comienza 20 a&ntilde;os antes del diagn&oacute;stico de la demencia. Adem&aacute;s de la edad, diversos factores m&eacute;dicos, socioecon&oacute;micos y conductuales pueden estar asociados al declive cognitivo. El objetivo de esta revisi&oacute;n sistem&aacute;tica es resumir la evidencia de factores de riesgo o protectores relacionados con el declive cognitivo en poblaci&oacute;n menor de 65 a&ntilde;os.    <br> <I>M&eacute;todos: </I>Se realiz&oacute; una revisi&oacute;n sistem&aacute;tica mediante una estrategia de b&uacute;squeda en bases de datos MEDLINE y Embase, incluyendo estudios con dise&ntilde;o longitudinal que analizaran el efecto de factores protectores o de riesgo en el declive cognitivo de poblaci&oacute;n adulta menor de 65 a&ntilde;os.    <br> <I>Resultados: </I>Se incluyeron 22 estudios en la presente revisi&oacute;n. Factores como diabetes mellitus, hiperinsulinemia, sobrepeso u obesidad, s&iacute;ndrome metab&oacute;lico, nivel educativo, actividad f&iacute;sica, estimulaci&oacute;n cognitiva, estado civil y calidad de la dieta podr&iacute;an estar relacionados con el declive cognitivo antes de los 65 a&ntilde;os.    <br> <I>Conclusiones: </I>Factores de riesgo cardiovasculares y de estilos de vida pueden estar asociados al declive cognitivo en menores de 65 a&ntilde;os. Sin embargo, la calidad de la evidencia es baja.</p>     <p><I><b>Palabras clave</b>: </I>Deterioro cognitivo, Factores de riesgo, Demencia, Revisi&oacute;n sistem&aacute;tica.</p> <hr>     <p><font size="3"><b>Abstract</b></font></p>     <p><I>Introduction: </I>Cognitive decline could begin 20 years before the diagnosis of dementia. Besides age, several factors related to medical, socioeconomic, and behavioral and genetic condition  may be associated with cognitive decline. The aim of this systematic review was to summarize evidence on the risk and protective factors for cognitive decline in people under 65 years old.    <br> <I>Methods: </I>A systematic review was conducted using a search strategy in MEDLINE and  Embase, including longitudinal studies to analyze the effect of protective or risk factors on cognitive decline in a population under 65 years old.    <br> <I>Results: </I>A total of 22 studies were included in this review. Factors such as diabetes, hyperinsulinemia, overweight or obesity, metabolic syndrome, education, physical activity, cognitive stimulation, marital status and diet, could be related to cognitive decline before 65 years of age.    ]]></body>
<body><![CDATA[<br> <I>Conclusions: </I>Cardiovascular risk factors and lifestyle conditions may be associated with cognitive decline before 65 years of age. However, the quality of the evidence was low.</p>     <p><b><I>Keywords: </I></b>Cognitive decline, Risk factors, Dementia, Systematic review.</p> <hr>     <p><b><font size="3">Introducci&oacute;n</font></b></p>     <p> Se ha se&ntilde;alado que el declive cognitivo comienza 20 a&ntilde;os antes del diagn&oacute;stico de la demencia<Sup>1,2</Sup>. Los individuos con declive cognitivo, a su vez, tienen mayor riesgo de demencia<Sup>3</Sup>. Se ha sugerido que factores de riesgo cardiovascular presentes antes de los 65 a&ntilde;os estar&iacute;an asociados con mayor riesgo de demencia<Sup>4</Sup>. M&aacute;s all&aacute; del efecto de la edad, la evidencia acerca de la relaci&oacute;n entre otros factores de riesgo y el declive cognitivo no es consistente y la calidad de los estudios es escasa<Sup>5</Sup>. Por otro lado, estudios transversales<Sup>6,7 </Sup>y longitudinales<Sup>8-11 </Sup>han indicado que factores cardiovasculares y gen&eacute;ticos podr&iacute;an estar relacionados con el declive cognitivo antes de los 65 a&ntilde;os. Esto es importante, dado que cerca de la mitad de los casos de enfermedad de Alzheimer (EA) podr&iacute;an ser atribuibles a factores de riesgo cardiovascular presentes varios a&ntilde;os antes del diagn&oacute;stico<Sup>12</Sup>, y se podr&iacute;an modificar con cambios en los estilos de vida o nuevas terapias preventivas. A&uacute;n no existe un tratamiento efectivo que disminuya el declive cognitivo; por esta raz&oacute;n, los estudios sobre factores asociados a dicho declive en poblaci&oacute;n menor de 65 a&ntilde;os son importantes por la oportunidad de desarrollar o implementar intervenciones preventivas farmacol&oacute;gicas o no farmacol&oacute;gicas<Sup>13</Sup>. No se han reportado revisiones sistem&aacute;ticas de estudios sobre factores asociados al declive cognitivo en poblaciones diferentes de adultos mayores. Por lo tanto, esta revisi&oacute;n sistem&aacute;tica tiene como objetivo determinar qu&eacute; factores m&eacute;dicos, sociales o conductuales y gen&eacute;ticos est&aacute;n relacionados con el declive cognitivo en poblaci&oacute;n menor de 65 a&ntilde;os.</p>     <p><font size="3"><b>Material y m&eacute;todos</b></font></p>     <p><I>Criterios de elegibilidad </I></p>     <p> Se dise&ntilde;&oacute; un protocolo siguiendo las gu&iacute;as de Cochrane para revisiones sistem&aacute;ticas y se utiliz&oacute; la gu&iacute;a de PRISMA<Sup>14 </Sup>para el actual reporte de resultados.</p>     <p>Se incluyeron estudios longitudinales realizados en poblaci&oacute;n menor de 65 a&ntilde;os que evaluaran las siguientes exposiciones, siguiendo la clasificaci&oacute;n propuesta por Plassman en 2010<Sup>3</Sup>: <I>a) </I>m&eacute;dicos: diabetes mellitus (DM), s&iacute;ndrome metab&oacute;lico (SM), hipertensi&oacute;n arterial (HTA), accidente cerebrovascular (ACV), hiperlipemia, homociste&iacute;na, trastornos del sue&ntilde;o, obesidad/&iacute;ndice de masa corporal (IMC), traumatismo craneoencef&aacute;lico (TEC), depresi&oacute;n, ansiedad y resiliencia; <I>b) </I>socioecon&oacute;micos y del comportamiento: factores en la infancia (residencia rural/urbana y factores ambientales), nivel educativo, ocupaci&oacute;n, coeficiente intelectual (CI), tabaquismo, alcohol, apoyo y redes sociales, estado civil y actividad f&iacute;sica; <I>c) </I>exposiciones a agentes t&oacute;xicos como pesticidas o poluci&oacute;n; <I>d) </I>gen&eacute;ticos: APOE&epsilon;4 y otros potenciales identificados en la b&uacute;squeda; <I>e) </I>nutricionales y dietarios: vitamina B, folato, otras vitaminas potenciales identificadas en la b&uacute;squeda, gingko-biloba, omega 3, consumo de frutas y vegetales, calor&iacute;as, hidratos de carbono, grasas y prote&iacute;nas, y <I>f</I>) medicamentos: estatinas, antihipertensivos, antiinflamatorios, esteroides gonadales, inhibidores de la colinesterasa y memantina.</p>     <p>Se incluyeron estudios en humanos menores de 65 a&ntilde;os, de cohortes prospectiva o retrospectiva y que evaluaran como desenlace la medici&oacute;n de una funci&oacute;n cognitiva espec&iacute;fica o general.</p>     <p>Se excluyeron los estudios realizados en pacientes con condiciones espec&iacute;ficas como DM, enfermedad renal, esquizofrenia, s&iacute;ndrome de Down, trastornos psic&oacute;ticos relacionados con abuso de sustancias, epilepsia y Parkinson, dise&ntilde;os de estudios transversales, desenlaces diferentes de las mediciones cognitivas y res&uacute;menes de congresos donde no se pudiera tener informaci&oacute;n completa y detallada de las caracter&iacute;sticas del estudio.</p>     ]]></body>
<body><![CDATA[<p><I>Fuentes de informaci&oacute;n y estrategia de b&uacute;squeda </I></p>     <p> Se realizaron b&uacute;squedas en bases de datos hasta octubre de 2013; en MEDLINE desde 1966 y en EMBASE desde 1974. La estrategia de b&uacute;squeda utilizada fue: cogni* AND (Decline OR impairment) AND Cohort study NOT ((schizophrenia&#91;mesh&#93; OR schizophrenia&#91;all fields&#93; OR "down syndrome"&#91;mesh&#93; OR "down syndrome"&#91;all fields&#93; OR "psychotic disorders"&#91;mesh&#93; OR "psychosis"&#91;all fields&#93; OR "substance-related disorders"&#91;MeSH Terms&#93; OR "substance abuse"&#91;all fields&#93; OR epilepsy&#91;mesh&#93; OR epilepsy&#91;all fields&#93; OR "seizure disorder"&#91;all fields&#93; OR "Parkinson disease"&#91;mesh&#93; OR "Parkinson disease"&#91;all fields&#93;) AND Limits: Humans, Adult: 19-44 years, Middle Aged: 4564 years. En EMBASE la estrategia de b&uacute;squeda fue: cogni* AND ('decline'/de OR impairment) AND (cohort OR longitudinal) NOT ('schizophrenia'/de OR Parkinson) AND &#91;adult&#93;/lim AND &#91;humans&#93;/lim.</p>     <p><I>Procedimientos de selecci&oacute;n </I></p>     <p> La selecci&oacute;n y el an&aacute;lisis de los estudios las realizaron en tres etapas cuatro revisores con formaci&oacute;n en Neuropsicolog&iacute;a (VT, CM, EH, DG) y un bioestad&iacute;stico con formaci&oacute;n en Epidemiolog&iacute;a (DC). En la primera etapa, se revisaron los t&iacute;tulos y los res&uacute;menes; en la segunda, los art&iacute;culos completos y en la tercera, se realizaron la extracci&oacute;n de los datos y la evaluaci&oacute;n de la calidad de los art&iacute;culos elegidos. Llevaron a cabo todas las etapas al menos dos revisores de manera independiente y se verificaron los resultados de cada etapa en reuniones de conjunto. Las discrepancias se resolvieron por consenso y/o por un revisor adicional.</p>     <p><I>Procedimientos de recolecci&oacute;n de la informaci&oacute;n </I></p>     <p> Los siguientes datos de los estudios se extrajeron a un formulario predise&ntilde;ado: n&uacute;mero de identificaci&oacute;n MED-LINE/Embase, primer a&ntilde;o, localizaci&oacute;n geogr&aacute;fica, dise&ntilde;o, n&uacute;mero de participantes, criterios de inclusi&oacute;n/exclusi&oacute;n, edad, sexo, nivel educativo, estado cognitivo basal, factor de riesgo estudiado, desenlace, tiempo desde la evaluaci&oacute;n de la exposici&oacute;n hasta la medici&oacute;n final del desenlace, control de variables de confusi&oacute;n, porcentaje de datos perdidos durante el seguimiento y resultados principales/secundarios.</p>     <p><I>Riesgo de sesgo en los estudios individuales </I></p>     <p> Dada la heterogeneidad de criterios para evaluar art&iacute;culos observacionales con dise&ntilde;os longitudinales, y  ante la carencia de gu&iacute;as claras sobre estudios de deterioro cognitivo, se adapt&oacute; la gu&iacute;a utilizada en la revisi&oacute;n de Plassman<Sup>3</Sup>.</p>     <p><I>Medidas de resumen y s&iacute;ntesis de los datos </I></p>     <p> Los estudios sobre deterioro cognitivo son heterog&eacute;neos con relaci&oacute;n a las poblaciones estudiadas, la medici&oacute;n de las exposiciones y los desenlaces que pueden ser categ&oacute;ricos (p. ej., DCL o demencia o estar por encima o por debajo de un punto de corte en la prueba neuropsicol&oacute;gica espec&iacute;fica) o continuos usando las puntuaciones brutas o estandarizadas (puntuaciones z). Adem&aacute;s, los estudios son heterog&eacute;neos con relaci&oacute;n a si se midi&oacute; una funci&oacute;n cognitiva espec&iacute;fica o en general y con relaci&oacute;n a los instrumentos de medici&oacute;n. Por tal raz&oacute;n, en este trabajo no se intent&oacute; realizar una s&iacute;ntesis cuantitativa de los resultados.</p>     ]]></body>
<body><![CDATA[<p><font size="3"><b>Resultados</b></font></p>     <p><I>Selecci&oacute;n art&iacute;culos </I></p>     <p> Se identificaron 8.071 registros, 4.163 en MEDLINE y 3.908 en Embase, de los que 1.116 estaban duplicados. Se hizo lectura completa de 123 estudios y, de estos, se inclueron 22 en la revisi&oacute;n (<a href="#f1">fig. 1</a>).</p>     <p align="center"><a name="f1"></a><img src="img/revistas/rcp/v43n2/v43n2a08f1.jpg"></p>     <p><I>Caracter&iacute;sticas de los estudios </I></p>     <p><I>Localizaci&oacute;n y tiempo de seguimiento </I></p>     <p>Todos los estudios ten&iacute;an un dise&ntilde;o longitudinal con al menos dos mediciones de las funciones cognitivas. Los pa&iacute;ses de origen de las investigaciones son Estados Unidos<Sup>8,11,15-18</Sup>, Pa&iacute;ses Bajos<Sup>9,10,19-24</Sup>, Reino Unido<Sup>25-29 </Sup>y Australia<Sup>30,31</Sup>. La mediana de seguimiento desde la primera hasta la &uacute;ltima evaluaci&oacute;n cognitiva fue 6 (2-20) a&ntilde;os.</p>     <p><I>Participantes </I></p>     <p>La mediana de participantes por estudio fue de 2.214 (18011.380). Todos los estudios excepto uno<Sup>16 </Sup>proven&iacute;an de cohortes ensambladas previamente: cuatro estudios de la cohorte ARIC<Sup>8,11,17,18</Sup>; cuatro de la Cohorte Whitehall II<Sup>9,10,23,24</Sup>; tres del Doetinchem Cohort Study<Sup>19,21,22</Sup>; dos del Maastricht  Aging Study (MAAS)<Sup>20,31</Sup>; dos de la cohorte VISAT<Sup>28,29</Sup>; dos de la British 1946 Birth Cohort<Sup>25,26</Sup>, uno del Longitudinal Assessment of Ageing in Women<Sup>30</Sup>; uno del Study of Women's Health Across the Nation (SWAN)<Sup>15</Sup>, y uno de The Medical Research Council National Survey of Health and Development (NSHD)<Sup>27</Sup>. La mediana de los promedios de edad en los estudios fue 49,5 (35-60) a&ntilde;os; la mediana del porcentaje de mujeres incluidas fue del 51% (23%-61%) y la del porcentaje de escolaridad alta fue del 33,4% (19,4%-58%).</p>     <p><I>Exposiciones </I></p>     ]]></body>
<body><![CDATA[<p>Se encontraron 12 estudios que evaluaron factores de tipo m&eacute;dico: DM<Sup>8,18,22</Sup>, hiperinsulinemia<Sup>17</Sup>,HTA<Sup>8,18</Sup>, hiperlipemia<Sup>8</Sup>, IMC<Sup>24,28</Sup>,ACV<Sup>18</Sup>, riesgo de ACV<Sup>9</Sup>,SM<Sup>9,18,24</Sup>, migr&ntilde;a<Sup>31 </Sup>y terapia de remplazo hormonal<Sup>30</Sup>, y un estudio evalu&oacute; el estado de salud general y su interacci&oacute;n con la educaci&oacute;n<Sup>20</Sup>.Delos factores sociales, econ&oacute;micos o conductuales, los estudios evaluaron el efecto de la educaci&oacute;n<Sup>20</Sup>, tabaquismo<Sup>8,18,19,25,27</Sup>, estado cognitivo en la adolescencia<Sup>26</Sup>, actividad laboral en horas laboradas<Sup>23 </Sup>y estimulaci&oacute;n cognitiva en el trabajo<Sup>29</Sup>, estatus socioecon&oacute;mico<Sup>10</Sup>, actividad f&iacute;sica<Sup>21,27 </Sup>y dieta<Sup>27</Sup>.En los factores gen&eacute;ticos, tres estudios evaluaron el efecto de APOE<sup>11,16,18</sup>.</p>     <p><b>Desenlaces</b></p>     <p> Los estudios fueron heterog&eacute;neos en cuanto a las pruebas utilizadas para la medici&oacute;n de las funciones cognitivas. Un estudio utiliz&oacute; el Examen Mental M&iacute;nimo (MMSE) como medida general<Sup>30 </Sup>y cuatro utilizaron puntuaciones compuestas<Sup>19,21,22,24</Sup>. Tambi&eacute;n se utilizaron pruebas que evaluaron memoria verbal<Sup>32,33</Sup>, memoria epis&oacute;dica, memoria visual<Sup>34,35</Sup>, lenguaje<Sup>34,36-40</Sup>, velocidad de procesamiento<Sup>41,42</Sup>, velocidad perceptual<Sup>43</Sup>, atenci&oacute;n<Sup>44-46</Sup>, funci&oacute;n ejecutiva<Sup>46-48</Sup>,  habilidades espaciales<Sup>41,49 </Sup>y perceptuales<Sup>50,51 </Sup>e inteligencia verbal<Sup>52 </Sup>y no verbal<Sup>53</Sup>.</p>     <p><I>Riesgo de sesgos en los estudios </I></p>     <p> Se encontr&oacute; potencial riesgo de sesgos de selecci&oacute;n en seis estudios<Sup>9,24-28 </Sup>y control incompleto de variables de confusi&oacute;n en 17<Sup>8-11,17,19-28,30,31</Sup>. La mediana de la p&eacute;rdida de seguimiento fue del 25% (16%-74%) y nueve estudios incluyeron solo a los participantes con informaci&oacute;n completa en las dos mediciones (basal/final)<Sup>9-11,17,23-25,27,30</Sup>.Tambi&eacute;n se presentaron sesgos de clasificaci&oacute;n en las exposiciones medidas por declaraci&oacute;n espont&aacute;nea<Sup>8-11,15-23,25-31,54</Sup> (<a href="#t1">tabla 1</a>).</p>     <p align="center"><a name="t1"></a><img src="img/revistas/rcp/v43n2/v43n2a08t1.jpg"></p>     <p><I>Medidas de resumen </I></p>     <p> Los estudios presentan heterogeneidad en la presentaci&oacute;n del resultado del declive cognitivo: diferencia de medias absoluta<Sup>8,11,17,23,27,54</Sup>,  estandarizada<Sup>19,21,22,26</Sup>, medici&oacute;n final ajustada por la medici&oacute;n basal<Sup>20,25</Sup>, p&eacute;rdida anual en puntos<Sup>9,16,18,24,29,31 </Sup>y de manera categ&oacute;rica como aparici&oacute;n de desenlaces mediante puntos de corte predefinidos<Sup>10,11,28,30</Sup>.</p>     <p><I>Resultados de los estudios individuales </I></p>     <p> La <a href="#t2">tabla 2</a> presenta los resultados generales de la asociaci&oacute;n de los factores m&eacute;dicos y el declive cognitivo. Factores como DM<Sup>8,18,22</Sup>, hiperinsulinemia<Sup>17</Sup>, IMC<Sup>24,28 </Sup>ySM<Sup>9,18 </Sup>mostraron asociaci&oacute;n con el declive en tareas de memoria verbal y lenguaje (fluidez verbal, fluidez fonol&oacute;gica, fluidez sem&aacute;ntica y vocabulario). El inicio temprano de la terapia de remplazo<Sup>30 </Sup>yun adecuado funcionamiento f&iacute;sico<Sup>20 </Sup>tendr&iacute;an un efecto protector contra el declive cognitivo.</p>     ]]></body>
<body><![CDATA[<p align="center"><a name="t2"></a><img src="img/revistas/rcp/v43n2/v43n2a08t2.jpg"></p>      <p>La <a href="#t3">tabla 3</a> presenta los resultados generales de la asociaci&oacute;n de los factores sociales, econ&oacute;micos o conductuales y el declive cognitivo. Mayor nivel educativo<Sup>20</Sup>, mejor nivel cognitivo en la adolescencia<Sup>26</Sup>, actividad f&iacute;sica<Sup>21,27</Sup>, estimulaci&oacute;n cognitiva dentro y fuera del trabajo<Sup>29</Sup>, estado civil (casado)<Sup>54 </Sup>y dieta<Sup>27 </Sup>tendr&iacute;an un efecto protector contra el declive en tareas de memoria verbal, lenguaje, velocidad de procesamiento y funci&oacute;n ejecutiva. La APOE&epsilon;4<Sup>11,16,18 </Sup>estar&iacute;a asociada con el declive cognitivo en tareas de memoria verbal, lenguaje, habilidades espaciales y perceptuales y funci&oacute;n ejecutiva.</p>     <p align="center"><a name="t3"></a><img src="img/revistas/rcp/v43n2/v43n2a08t3.jpg"></p>      <p>No se encontraron estudios que evaluaran el efecto de los siguientes factores: homociste&iacute;na, depresi&oacute;n/ansiedad, TCE, trastornos del sue&ntilde;o, resiliencia, residencia rural/urbana, apoyo y redes sociales, alcohol o exposici&oacute;n a agentes t&oacute;xicos.</p>     <p><b><font size="3">Discusi&oacute;n</font></b></p>       <p> La evidencia sobre factores asociados al declive cognitivo en poblaci&oacute;n menor de 65 a&ntilde;os es insuficiente. Hay pocos estudios que concluyan en la relaci&oacute;n de factores de riesgo cardiovascular, factores sociales, econ&oacute;micos o comporta-mentales con el declive cognitivo en esta poblaci&oacute;n. Algunas condiciones y antecedentes como la DM, la hiperinsulinemia, la obesidad, el SM, la enfermedad cerebrovascular, la educaci&oacute;n, la ocupaci&oacute;n, el estado civil y la presencia del polimorfismo APOE&epsilon;4 estar&iacute;an asociados con un mayor declive cognitivo en tareas de memoria verbal, velocidad de procesamiento, funci&oacute;n ejecutiva, atenci&oacute;n, razonamiento y fluidez sem&aacute;ntica y fonol&oacute;gica. Otros factores como la terapia de remplazo hormonal, la estimulaci&oacute;n cognitiva, la salud f&iacute;sica percibida, la actividad f&iacute;sica y la calidad de la dieta podr&iacute;an tener un efecto protector. No se encontraron estudios que evaluaran el efecto en el declive cognitivo antes de los 65 a&ntilde;os de otros factores como homociste&iacute;na, depresi&oacute;n/ansiedad, TCE, trastornos del sue&ntilde;o, resiliencia, residencia rural/urbana, apoyo y redes sociales, alcohol o exposici&oacute;n a agentes t&oacute;xicos. La evidencia sobre el efecto de estos factores en otras poblaciones de estudio de m&aacute;s edad tampoco ha sido concluyente<Sup>5</Sup>.</p>     <p>A pesar de la escasa evidencia en poblaci&oacute;n menor de 65 a&ntilde;os, estudios recientes han mostrado la relaci&oacute;n entre factores de riesgo cardiovascular evaluados en la etapa adulta joven o de mediana edad y el deterioro cognitivo </p>     <p>o la demencia presentes en la etapa de adultos mayores (&gt;65 a&ntilde;os). Estos estudios muestran que factores de riesgo como DM<Sup>55,56</Sup>, obesidad<Sup>24,55-57</Sup>, HTA<Sup>55,58</Sup>, altas concentraciones de colesterol<Sup>56,58</Sup>, escasa actividad f&iacute;sica<Sup>55 </Sup>y tabaquismo<Sup>58 </Sup>aumentan el riesgo de declive cognitivo o demencia. Hay varias razones potenciales de que la evidencia del declive cognitivo en poblaci&oacute;n menor de 65 a&ntilde;os sea escasa o no concluyente; algunas de ellas se han discutido previamente en el contexto metodol&oacute;gico de la investigaci&oacute;n sobre factores de riesgo en esta condici&oacute;n<Sup>59-61</Sup>. Las caracter&iacute;sticas reales de la poblaci&oacute;n en riesgo, o los sesgos de selecci&oacute;n, estaban presentes o no se pudo evaluarlas en algunos estudios debido a la falta de claridad en los criterios de exclusi&oacute;n, la inadecuada descripci&oacute;n de las cohortes y la carencia de informaci&oacute;n acerca del estado cognitivo inicial y otras caracter&iacute;sticas basales. El sesgo de supervivencia tambi&eacute;n pudo darse en numerosos estudios, dado que las p&eacute;rdidas de seguimiento estuvieron en entre el 14 y el 74%. Este efecto del &laquo;desgaste&raquo; de la cohorte presente en los estudios de declive cognitivo se ha estudiado anteriormente<Sup>62-66 </Sup>y se constituye en una importante debilidad metodol&oacute;gica; dado que se ha demostrado que los participantes que se retiran del estudio tienen un nivel cognitivo menor, menos educaci&oacute;n, peor estado de salud (mayor frecuencia de factores de riesgo cardiovasculares), mayor frecuencia de tabaquismo y menos actividad f&iacute;sica que los que terminan<Sup>67-69</Sup>, lo que subestimar&iacute;a el declive cognitivo observado en la cohorte. Del mismo modo, se reportan estudios cuyos an&aacute;lisis fueron realizados &uacute;nicamente con los participantes con informaci&oacute;n completa en las dos mediciones (basal/final) y que igualmente ten&iacute;an mejor desempe&ntilde;o cognitivo basal o mejor estado de salud que los que no fueron incluidos. Los m&eacute;todos de selecci&oacute;n de los participantes tambi&eacute;n pueden estar asociados con las caracter&iacute;sticas demogr&aacute;ficas y el nivel cognitivo basal, como apunta un estudio reciente<Sup>70</Sup>, en el que los participantes provenientes de una muestra seleccionada por conveniencia ten&iacute;an mejor rendimiento cognitivo, m&aacute;s educaci&oacute;n, mayor probabilidad de estar casado y menor probabilidad de historia familiar de demencia que aquellos cuya selecci&oacute;n fue probabil&iacute;stica.</p>      <p>Por otro lado, la medici&oacute;n de la funci&oacute;n cognitiva es un proceso complejo y con m&uacute;ltiples miradas potenciales. Algunos estudios utilizan medidas compuestas y otros, medidas de funciones cognitivas espec&iacute;ficas, con variables continuas  o categ&oacute;ricas. Las pruebas neuropsicol&oacute;gicas empleadas para el diagn&oacute;stico, la clasificaci&oacute;n y el seguimiento de la demencia presentan efectos piso y techo en los extremos de menor y mayor expresi&oacute;n de manifestaciones cl&iacute;nicas y pueden no ser sensibles al declive cognitivo, es decir, ser incapaces de detectarlo, en periodos precl&iacute;nicos. La utilizaci&oacute;n de puntuaciones compuestas<Sup>59 </Sup>puede ser &uacute;til para reducir los problemas de efecto piso o techo y el efecto del aprendizaje<Sup>71</Sup>. Sin embargo, la construcci&oacute;n de estas puntuaciones no es simple y pueden existir varias versiones o modelos; por ejemplo, en algunos casos se utiliza la suma ponderada o no ponderada de las pruebas que conforman la bater&iacute;a neuropsicol&oacute;gica.</p>     <p>Esta revisi&oacute;n tiene varias limitaciones: nuestro objetivo era establecer un declive cognitivo y sus factores asociados antes de los 65 a&ntilde;os. Por lo tanto, no se incluyeron estudios que midieran la exposici&oacute;n antes de los 65 a&ntilde;os, pero los desenlaces se midieron hasta la etapa adulta mayor. Dichos estudios muestran que la exposici&oacute;n a factores relacionados con estilos de vida, factores de riesgo cardiovascular o APOE&epsilon;4 incrementan el riesgo de declive cognitivo, deterioro cognitivo leve o demencia despu&eacute;s de los 65 a&ntilde;os. Estos estudios se habr&iacute;an podido incluir si se asume que la p&eacute;rdida cognitiva es lineal, es decir, constante a trav&eacute;s de los a&ntilde;os. Sin embargo, hay alguna evidencia de que dicha p&eacute;rdida no es constante<Sup>72,73 </Sup>y que la velocidad del deterioro cognitivo puede cambiar a&ntilde;os antes de presentarse los s&iacute;ntomas claros de demencia. Otra limitaci&oacute;n estar&iacute;a relacionada con un posible sesgo de publicaci&oacute;n al no consultar otras fuentes como literatura gris, trabajos presentados en eventos o contacto con los autores.</p>     ]]></body>
<body><![CDATA[<p><font size="3"><b>Conclusiones</b></font></p>     <p> Algunos factores de riesgo relacionados con la salud cardiovascular y los estilos de vida pueden estar asociados al declive cognitivo en menores de 65 a&ntilde;os. Sin embargo, se encontraron pocos estudios con dise&ntilde;o y conducci&oacute;n adecuados para sustentar la evidencia de cada uno de los factores reportados en la literatura. Entender c&oacute;mo estos factores influyen en el riesgo de declive cognitivo es importante para intentar reducir el riesgo de demencia en la etapa adulta. Los estudios futuros se deben realizar considerando las limitaciones metodol&oacute;gicas que no permiten estimar el efecto subyacente de los factores protectores o de riesgo del declive cognitivo en la poblaci&oacute;n general.</p>     <p><b>Financiaci&oacute;n</b></p>     <p> Este estudio fue financiado por el comit&eacute; para el desarrollo de la investigaci&oacute;n. CODI-Proyecto: Tasa de p&eacute;rdida cognitiva en la enfermedad de Alzheimer familiar por mutaci&oacute;n E280A en PS1: Estudio longitudinal 1995-2013 Antioquia. Colombia, mediana Cuant&iacute;a 2011-Universidad de Antioquia acta 609, Agosto de 2011. Beca programa doctorados nacionales No. 528 a&ntilde;o 2011, Departamento Administrativo de Ciencia, Tecnolog&iacute;a e Innovaci&oacute;n, Colciencias.</p>     <p><b>Conflicto de intereses</b></p>     <p> Los autores manifiestan que no tienen conflictos de intereses en este art&iacute;culo.</p> <hr>     <p><font size="3"><b>Bibliograf&iacute;a</b></font></p>     <!-- ref --><p>1. Elias MF, Beiser A, Wolf PA, Au R, White RF, D'Agostino RB.      The preclinical phase of alzheimer disease: A 22-year      prospective study of the Framingham Cohort. 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