<?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>1794-1237</journal-id>
<journal-title><![CDATA[Revista EIA]]></journal-title>
<abbrev-journal-title><![CDATA[Revista EIA]]></abbrev-journal-title>
<issn>1794-1237</issn>
<publisher>
<publisher-name><![CDATA[Escuela de ingenieria de Antioquia]]></publisher-name>
</publisher>
</journal-meta>
<article-meta>
<article-id>S1794-12372007000100009</article-id>
<title-group>
<article-title xml:lang="es"><![CDATA[INMUNOSENSORES PIEZOELÉCTRICOS: REVISION GENERAL Y SU APLICACIÓN EN EL ANÁLISIS DE PESTICIDAS]]></article-title>
</title-group>
<contrib-group>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Ocampo]]></surname>
<given-names><![CDATA[Aquiles]]></given-names>
</name>
<xref ref-type="aff" rid="A01"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[March]]></surname>
<given-names><![CDATA[Carmen]]></given-names>
</name>
<xref ref-type="aff" rid="A02"/>
</contrib>
<contrib contrib-type="author">
<name>
<surname><![CDATA[Montoya]]></surname>
<given-names><![CDATA[Ángel]]></given-names>
</name>
<xref ref-type="aff" rid="A03"/>
</contrib>
</contrib-group>
<aff id="A01">
<institution><![CDATA[,Gibec y Gabis  ]]></institution>
<addr-line><![CDATA[ ]]></addr-line>
</aff>
<aff id="A02">
<institution><![CDATA[,Universidad Politécnica de Valencia  ]]></institution>
<addr-line><![CDATA[ ]]></addr-line>
</aff>
<aff id="A03">
<institution><![CDATA[,Instituto de Investigación e Innovación en Biotecnología  ]]></institution>
<addr-line><![CDATA[ ]]></addr-line>
</aff>
<pub-date pub-type="pub">
<day>00</day>
<month>06</month>
<year>2007</year>
</pub-date>
<pub-date pub-type="epub">
<day>00</day>
<month>06</month>
<year>2007</year>
</pub-date>
<numero>7</numero>
<fpage>97</fpage>
<lpage>110</lpage>
<copyright-statement/>
<copyright-year/>
<self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_arttext&amp;pid=S1794-12372007000100009&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_abstract&amp;pid=S1794-12372007000100009&amp;lng=en&amp;nrm=iso"></self-uri><self-uri xlink:href="http://www.scielo.org.co/scielo.php?script=sci_pdf&amp;pid=S1794-12372007000100009&amp;lng=en&amp;nrm=iso"></self-uri><abstract abstract-type="short" xml:lang="es"><p><![CDATA[En este artículo se presenta una revisión bibliográfica de los aspectos más relevantes en el desarrollo de inmunosensores, acompañada de algunos de los resultados experimentales en una aplicación en análisis del plaguicida Carbaril que ilustra la metodología analítica y los resultados esperados. El inmunosensor de microbalanza de cristal de cuarzo (QCM), más conocido como inmunosensor piezoeléctrico, es un sistema analítico que contiene un inmunorreactivo como componente biológico, un transductor de cristal de cuarzo con un antígeno, un conjugado o un anticuerpo inmovilizado en su superficie, acoplado a un sistema de procesamiento de información. Debido a su simplicidad, conveniencia, bajo costo, exactitud, estabilidad y respuesta en tiempo real, este dispositivo se ha vuelto cada vez más importante, especialmente para análisis de materiales en biomedicina, alimentos, medio ambiente y veterinaria.]]></p></abstract>
<abstract abstract-type="short" xml:lang="en"><p><![CDATA[A bibliographic review about the main aspects concerning the development of immunosensors is presented in this article, as well as some of the experimental results in an application in the analysis of carbaryl plaguicide that illustrates the analytical methodology and the expected results. The quartz crystal microbalance immunosensor (QCM), known as piezoelectric immunosensor, is an analytical system which combines an immunoreagent as the biologic component, a quartz crystal transducer with an immobilized antigen or antibody on its surface, coupled to an information processing system. Due to its simplicity, convenience, low cost, accuracy, stability, and real time response, this device has become very important, especially for material analysis in biomedicine, food, environment, and veterinary.]]></p></abstract>
<kwd-group>
<kwd lng="es"><![CDATA[inmunosensores]]></kwd>
<kwd lng="es"><![CDATA[piezoelectricidad]]></kwd>
<kwd lng="es"><![CDATA[QCM]]></kwd>
<kwd lng="es"><![CDATA[pesticidas]]></kwd>
<kwd lng="en"><![CDATA[immunosensors]]></kwd>
<kwd lng="en"><![CDATA[piezoelectricity]]></kwd>
<kwd lng="en"><![CDATA[QCM]]></kwd>
<kwd lng="en"><![CDATA[pesticides]]></kwd>
</kwd-group>
</article-meta>
</front><body><![CDATA[  <font face="verdana" size="2">     <p align="center"><b><font size="4">INMUNOSENSORES PIEZOEL&Eacute;CTRICOS: REVISION GENERAL Y SU APLICACI&Oacute;N EN EL</font></b> <font size="4"><b>AN&Aacute;LISIS DE PESTICIDAS</b></font></p>     <p align="center">&nbsp;</p>     <p><b>Aquiles Ocampo<sup>*</sup>, Carmen March<sup>**</sup>, &Aacute;ngel Montoya<sup>***</sup></b></p>     <p>* Ph.D. en Ingenier&iacute;a Qu&iacute;mica. Investigador de los grupos GPC, Gibec y Gabis. EIA.</p>     <p>** Doctora en Ciencias Biol&oacute;gicas. Instituto de Investigaci&oacute;n e Innovaci&oacute;n en Biotecnolog&iacute;a, Universidad Polit&eacute;cnica de Valencia (UPV).</p>     <p>*** Doctor en Ciencias Qu&iacute;micas. Instituto de Investigaci&oacute;n e Innovaci&oacute;n en Biotecnolog&iacute;a, UPV</p>     <p>Art&iacute;culo recibido 23-III-2007. Aprobado 25-V-2007</p>     <p>  Discusi&oacute;n abierta hasta diciembre de 2007</p> <hr />     <p><b><font size="3">RESUMEN</font></b></p>     ]]></body>
<body><![CDATA[<p>En este art&iacute;culo se presenta una revisi&oacute;n bibliogr&aacute;fica de los aspectos m&aacute;s relevantes en el desarrollo de inmunosensores, acompa&ntilde;ada de algunos de los resultados experimentales en una aplicaci&oacute;n en an&aacute;lisis del plaguicida Carbaril que ilustra la metodolog&iacute;a anal&iacute;tica y los resultados esperados. El inmunosensor de microbalanza de cristal de cuarzo (QCM), m&aacute;s conocido como inmunosensor piezoel&eacute;ctrico, es un sistema anal&iacute;tico que contiene un inmunorreactivo como componente biol&oacute;gico, un transductor de cristal de cuarzo con un ant&iacute;geno, un conjugado o un anticuerpo inmovilizado en su superficie, acoplado a un sistema de procesamiento de informaci&oacute;n. Debido a su simplicidad, conveniencia, bajo costo, exactitud, estabilidad y respuesta en tiempo real, este dispositivo se ha vuelto cada vez m&aacute;s importante, especialmente para an&aacute;lisis de materiales en biomedicina, alimentos, medio ambiente y veterinaria.</p> </font>     <p><font size="2" face="verdana"><b><font size="3">PALABRAS CLAVE:</font></b> inmunosensores; piezoelectricidad; QCM; pesticidas.</font></p> <font face="verdana" size="2"> <hr />     <p><b><font size="3">ABSTRACT</font></b></p>     <p>A bibliographic review about the main aspects concerning the development of immunosensors is presented in this article, as well as some of the experimental results in an application in the analysis of carbaryl plaguicide that illustrates the analytical methodology and the expected results. The quartz crystal microbalance immunosensor (QCM), known as piezoelectric immunosensor, is an analytical system which combines an immunoreagent as the biologic component, a quartz crystal transducer with an immobilized antigen or antibody on its surface, coupled to an information processing system. Due to its simplicity, convenience, low cost, accuracy, stability, and real time response, this device has become very important, especially for material analysis in biomedicine, food, environment, and veterinary.</p> </font>     <p><font size="2" face="verdana"><b><font size="3">KEY WORDS:</font></b> immunosensors; piezoelectricity; QCM; pesticides.</font></p> <font face="verdana" size="2"> <hr />     <p><b><font size="3">1. INTRODUCCI&Oacute;N</font></b></p>     <p>Un biosensor es un dispositivo anal&iacute;tico constituido por un componente biol&oacute;gico tal como una enzima, un anticuerpo o una c&eacute;lula, que es inmovilizado en un elemento de reconocimiento, el cual est&aacute; comunicado con un sistema de transducci&oacute;n que transforma la se&ntilde;al bioqu&iacute;mica en el&eacute;ctrica cuantificable. La <a href="#f1">figura 1</a> muestra un esquema de los componentes fundamentales de un biosensor [1].</p>     <p>    <center><a name="f1"><img src="img/revistas/eia/n7/n7a09f1.jpg" /></a></center> </p>     <p>Un inmunosensor es un biosensor en el cual el componente biol&oacute;gico es un inmunorreactivo. Cuando el analito es una mol&eacute;cula peque&ntilde;a, se requiere realizar un proceso adicional para lograr la reacci&oacute;n inmune con una mol&eacute;cula similar llamada hapteno. Generalmente el elemento objetivo es el ant&iacute;geno (el analito o el hapteno) y el anticuerpo se adhiere al receptor, aunque en algunos casos se obtiene una mejor respuesta cuando el analito, o una forma modificada de &eacute;l, se adhiere al receptor.</p>     ]]></body>
<body><![CDATA[<p>El inmunosensor piezoel&eacute;ctrico usa una mi-crobalanza de cristal de cuarzo (QCM) como un transductor altamente preciso y estable que contiene un cristal de cuarzo con un ant&iacute;geno, un conjugado o un anticuerpo inmovilizado en su superficie [2]. La tecnolog&iacute;a QCM utiliza un detector sensible a la masa formado por un cristal piezoel&eacute;ctrico oscilante de cuarzo que resuena a una frecuencia fundamental, propiedad que le ha permitido su uso en biosensores basados en afinidad [3, 4]. La operaci&oacute;n de resonadores piezoel&eacute;ctricos en fase l&iacute;quida incluye cambios de la frecuencia de la masa y efectos inducidos por el cambio de la densidad o de la viscosidad de la capa l&iacute;quida circundante [5, 6].</p>     <p>Un gran n&uacute;mero de estudios recientes han demostrado prometedoras aplicaciones de los inmuno-sensores piezoel&eacute;ctricos en la realizaci&oacute;n de an&aacute;lisis en muchos campos, tales como el alimentario, bio-m&eacute;dico, veterinario y medioambiental. Representan una herramienta conveniente para la determinaci&oacute;n r&aacute;pida y simple de virus, prote&iacute;nas, bacterias y otras c&eacute;lulas, &aacute;cidos nucleicos y mol&eacute;culas peque&ntilde;as como drogas, hormonas y pesticidas [7-9].</p>     <p>Existen reportes donde se propone la aplicaci&oacute;n de inmunosensores en an&aacute;lisis de materiales para la industria y las oficinas gubernamentales, tales como cerveza, concentraci&oacute;n de micotoxinas en muestras de cereales y de alimentos, detecci&oacute;n temprana de materiales peligrosos como g&eacute;rmenes o materiales de guerra qu&iacute;mica, drogas il&iacute;citas y explosivos, con prop&oacute;sitos de seguridad, por ejemplo, en aeropuertos [10, 11].</p>     <p>En el &aacute;rea de biomedicina se presenta una clara oportunidad de mejorar sus procesos, bajando el tiempo y el costo de los an&aacute;lisis. Se destacan casos como la determinaci&oacute;n de prote&iacute;nas urinarias como marcadores para la nefropat&iacute;a de la diabetes [12], la inmunoglobulina IgM y la prote&iacute;na C-reactiva [13]; c&eacute;lulas humanas tales como T-linfocitos [14], eritrocitos [15]; bacterias tales como <i>Escherichia coli</i> [16, 17], estafilococos <i>aureus </i>[18, 19], <i>tyfimurium </i>de salmonelas [20] y legionella pneum&oacute;fila [21]; drogas como coca&iacute;na en los fluidos corporales [22] y metan-fetamina en la orina humana [23]; virus como los de herpes humano [24], hepatitis [25] y VIH [26], virus &Eacute;bola [27] y ant&iacute;geno carcino-embrionario [28].</p>     <p>Los usos veterinarios propuestos incluyen la detecci&oacute;n del virus de la peste porcina africana (ASF) [29], ant&iacute;geno del gusano adulto (AWA) en la detecci&oacute;n del <i>Schistosoma japonicum </i>en la infecci&oacute;n de los conejos [30, 31] y de <i>Salmonella enteritidis </i>en los pollos [20].</p>     <p>Los inmunosensores basados en diferentes transductores son herramientas de amplias posibilidades para la supervisi&oacute;n de los agentes contaminadores org&aacute;nicos [2, 32-34]. Han encontrado uso en &aacute;reas extensamente variadas tales como herbicidas en el agua potable [35], concentraci&oacute;n de dioxinas en muestras ambientales reales [36, 37], atrazina [38, 39], herbicida 2,4-D [40] y bifenilos policlorinados (PCB) [41], entre otros.</p>     <p>Las secciones siguientes presentan una descripci&oacute;n general de los modelos que soportan el funcionamiento de los inmunosensores piezoel&eacute;ctricos, de las etapas envueltas en la producci&oacute;n e inmovilizaci&oacute;n de los inmunorreactivos y tambi&eacute;n una ilustraci&oacute;n de la manera como se lleva a cabo la caracterizaci&oacute;n de un inmunosensor.</p>     <p><b><font size="3">2. EL INMUNOSENSOR PIEZOEL&Eacute;CTRICO COMO M&Eacute;TODO ANAL&iacute;TICO PARA EL AN&Aacute;LISIS DE</font></b> <font size="3"><b>PESTICIDAS</b></font></p>     <p>El uso de cristales piezoel&eacute;ctricos como elementos transductores en el desarrollo de inmunosensores microgravim&eacute;tricos tiene su origen en los trabajos de Sauerbrey a finales de la d&eacute;cada de los sesenta [42]. Sus estudios demostraron que, en ciertas condiciones, la variaci&oacute;n de la frecuencia de resonancia de un cristal piezoel&eacute;ctrico ten&iacute;a un comportamiento lineal con la densidad de masa superficial depositada sobre &eacute;l. La sensibilidad de esta variaci&oacute;n para cristales de cuarzo AT vibrantes en modo de cizalla es proporcional al cuadrado de la frecuencia de resonancia, <i>f</i>, seg&uacute;n la siguiente expresi&oacute;n:</p>     <p>    ]]></body>
<body><![CDATA[<center>&Delta;f / (&Delta;&rho;<sub>s</sub>) = -2,269 . 10<sup>-15</sup> f<sup> 2</sup> (Hz cm<sup>2</sup> ng<sup>-1</sup>)</center> </p>     <p>donde &Delta;&rho;<sub>s</sub> es el incremento de masa por unidad de superficie activa del sensor.</p>     <p>Por lo tanto, para un cristal de cuarzo AT de 10 MHz, la sensibilidad es de 0,23 Hz cm<sup>2</sup> ng<sup>-1</sup>. Esto significa sensibilidades superficiales de masa de 0,4 ng/cm y 40 ng/cm<sup>2</sup> para variaciones m&iacute;nimas detectables (VMD) de frecuencia de 0,1 y 10 Hz respectivamente. Estas VMD son t&iacute;picas en sistemas de microbalanza de cuarzo en medios gaseosos y en medios l&iacute;quidos respectivamente.</p>     <p>Estos datos indican que en estado gaseoso un sensor microgravim&eacute;trico de cuarzo AT y frecuencia de resonancia 10 MHz es capaz de detectar la depositaci&oacute;n de mol&eacute;culas monoat&oacute;micas sobre su superficie. Por otra parte, en medio l&iacute;quido la sensibilidad es suficiente para detectar la adherencia de pr&aacute;cticamente cualquier mol&eacute;cula de peso superior a 2500 daltons, distribuida de modo uniforme sobre la superficie activa del sensor. Sin embargo, esta sensibilidad de masa es inespec&iacute;fica y la relaci&oacute;n lineal entre la variaci&oacute;n de frecuencia y de densidad superficial de masa obtenida por Sauerbrey s&oacute;lo es v&aacute;lida cuando la masa depositada sobre el cristal es lo suficientemente fina o r&iacute;gida para asegurar que sus propiedades viscoel&aacute;sticas no afectan la variaci&oacute;n de frecuencia.</p>     <p>El entorno l&iacute;quido afecta tambi&eacute;n la frecuencia de resonancia del cristal [6]. Sin embargo, se ha demostrado [43] que si el medio en que se halla inmerso el sensor puede considerarse semiinfinito (normalmente se expone s&oacute;lo una cara del sensor al entorno de ensayo), es decir, no se producen reflexiones de la onda ac&uacute;stica, la variaci&oacute;n de frecuencia del resonador corresponde a la suma de las contribuciones debidas al l&iacute;quido y a la capa de recubrimiento. En consecuencia, si las caracter&iacute;sticas de densidad y viscosidad del medio fluido, que por lo general puede considerarse newtoniano, se mantienen constantes, la variaci&oacute;n de frecuencia sigue el mismo comportamiento lineal establecido por Sauerbrey, siempre que la capa de recubrimiento pueda considerarse r&iacute;gida.</p>     <p>Los m&eacute;todos anal&iacute;ticos existentes para la determinaci&oacute;n de pesticidas organofosforados y N-metil carbamatos son complejos y generalmente no disponibles, sobre todo para los compuestos m&aacute;s polares. La baja estabilidad t&eacute;rmica de estos compuestos hace inapropiada la t&eacute;cnica de cromatograf&iacute;a de gases y convierte la cromatograf&iacute;a l&iacute;quida HPLC como la m&aacute;s apropiada para su determinaci&oacute;n. Aunque el m&eacute;todo es adecuado, requiere procedimientos de extracci&oacute;n y limpieza y con frecuencia exige etapas de derivaci&oacute;n y concentraci&oacute;n para obtener la sensibilidad requerida [44-46]. Debido a estas limitaciones de las metodolog&iacute;as convencionales, las t&eacute;cnicas inmunoqu&iacute;micas, y entre ellas los inmunosensores piezoel&eacute;ctricos, est&aacute;n ganando una aceptaci&oacute;n creciente como m&eacute;todos alternativos o complementarios para el an&aacute;lisis de pesticidas.</p>     <p><b><font size="3">3. PREPARACI&Oacute;N DE REACTIVOS Y ANTICUERPOS</font></b></p>     <p>La generaci&oacute;n acertada de anticuerpos espec&iacute;ficos y los an&aacute;lisis de sensibilidad hacia una mol&eacute;cula peque&ntilde;a dependen en alto grado del dise&ntilde;o apropiado de los haptenos para hacer posible su inmovilizaci&oacute;n y an&aacute;lisis. Las mol&eacute;culas peque&ntilde;as, como las de pesticidas, drogas, etc., son generalmente no inmunog&eacute;nicas, o sea que no provocan una respuesta inmune, a menos que est&eacute;n unidas con algunas macromol&eacute;culas tales como prote&iacute;nas. Esto implica una modificaci&oacute;n de estas sustancias para unirse con macromol&eacute;culas (portadoras) para hacer as&iacute; un complejo o conjugado estable del portador-hapteno. El hapteno debe ser tan similar como sea posible al analito, manteniendo sus caracter&iacute;sticas estructurales principales, grupos qu&iacute;micos y distribuci&oacute;n electr&oacute;nica [47-50].</p>     <p>Es dif&iacute;cil predecir cu&aacute;l hapteno es te&oacute;ricamente el m&aacute;s apropiado para un analito particular y, adem&aacute;s, si este hapteno se comportar&aacute; adecuadamente en los ensayos, como se discutir&aacute; m&aacute;s adelante. Si se emplea la tecnolog&iacute;a del anticuerpo monoclonal, debe realizarse una selecci&oacute;n cuidadosa del hapteno, para aprovechar las diferentes caracter&iacute;sticas de los anticuerpos eventualmente obtenidos [51-54].</p>     <p>El dise&ntilde;o del hapteno es, por lo tanto, un paso determinante en el desarrollo de los inmunoensayos para las mol&eacute;culas peque&ntilde;as, porque el hapteno es el responsable de determinar las caracter&iacute;sticas del reconocimiento del anticuerpo [55-57]. Para explorar el n&uacute;mero m&aacute;ximo de posibilidades para obtener anticuerpos de buena calidad, se suele recomendar la s&iacute;ntesis de varios haptenos con diferentes brazos espaciadores obtenidos por medio de diversas cadenas moleculares [58-60].</p>     ]]></body>
<body><![CDATA[<p>La <a href="#f2">figura 2</a> muestra la estrategia de s&iacute;ntesis realizada en el Instituto de Investigaci&oacute;n e Innovaci&oacute;n en Bioingenier&iacute;a de la Universidad Polit&eacute;cnica de Valencia (UPV), Espa&ntilde;a, para el hapteno CNH utilizado en el an&aacute;lisis de un insecticida modelo, el carbaril [61]. Fue basada en los procedimientos de s&iacute;ntesis industrial del propio insecticida.</p>     <p>    <center><a name="f2"><img src="img/revistas/eia/n7/n7a09f2.jpg" /></a></center> </p>     <p>La s&iacute;ntesis del &aacute;cido 6-[[(1-<i>naftiloxi)carbonil] amino]hexanoico </i>(CNH) fue un proceso en dos etapas: la primera fue la s&iacute;ntesis de 1-naftil cloroformato, que fue obtenido a partir del 1-naftol e hidr&oacute;xido de sodio para obtener un radical intermedio, el cual tratado con fosgeno (COCl<sub>2</sub>) produjo, despu&eacute;s de purificar, el cloroformato como un aceite amarillo claro; la segunda etapa fue la s&iacute;ntesis del CNH a partir del cloroformato obtenido antes y &aacute;cido aminohexa-noico disuelto en hidr&oacute;xido de sodio y tratado con una soluci&oacute;n de dioxano y luego purificado, como se describe en [61].</p>     <p>La preparaci&oacute;n de anticuerpos contra hap-tenos, dise&ntilde;ada para aplicaciones especiales tales como pesticidas y bifenilos policlorinados (PCB), se basa en el enlace covalente del hapteno a una prote&iacute;na (portador) y la inmunizaci&oacute;n de animales con los inmun&oacute;genos sintetizados. El enlace qu&iacute;mico del hapteno a una prote&iacute;na determina el car&aacute;cter de la especificidad del anticuerpo. Una gran cantidad de haptenos conjugados a prote&iacute;nas han sido utilizados para el desarrollo de anticuerpos. Actualmente, la ingenier&iacute;a de anticuerpos y la producci&oacute;n de anticuerpos recombinantes son campos muy prometedores para la investigaci&oacute;n y sus aplicaciones [62-66].</p>     <p>El desarrollo de inmunoensayos requiere la producci&oacute;n de anticuerpos para los analitos y su incorporaci&oacute;n en los distintos tipos y procedimientos de an&aacute;lisis, por lo general inmunoensayos enzim&aacute;ti-cos en fase s&oacute;lida (ELISA). La generaci&oacute;n acertada de anticuerpos espec&iacute;ficos y sensibles a una mol&eacute;cula peque&ntilde;a depende de un dise&ntilde;o apropiado de los haptenos, la inmunizaci&oacute;n y el procedimiento de an&aacute;lisis. A este respecto, sigue siendo imprevisible c&oacute;mo los haptenos se presentan al sistema inmune, por lo que es recomendable examinar varias estructuras hapt&eacute;nicas [55, 59]. Particularmente, la detecci&oacute;n de un grupo de compuestos de estructura similar puede lograrse a menudo mediante la s&iacute;ntesis juiciosa de los inmun&oacute;genos o conjugados hapteno-prote&iacute;na para exponer al m&aacute;ximo las caracter&iacute;sticas comunes a todos los miembros del grupo y a la vez reducir al m&iacute;nimo la presentaci&oacute;n de diferencias estructurales al sistema inmune [56].</p>     <p>Una vez que los inmun&oacute;genos del analito est&eacute;n preparados, la discusi&oacute;n se presenta sobre si obtener anticuerpos policlonales o monoclonales. Los anticuerpos policlonales son producidos usando procedimientos tradicionales de inmunizaci&oacute;n, con conejos, cabras, ovejas y cerdos. Los anticuerpos policlonales, especialmente de conejos, son reactivos ampliamente utilizados en an&aacute;lisis inmunoqu&iacute;mico, aunque una de sus principales desventajas estriba en el hecho de que no es posible producir especificidad id&eacute;ntica del anticuerpo incluso en dos animales de la misma especie. Por otra parte, el uso de anticuerpos monoclonales est&aacute; limitado por la dificultad en el manejo de la tecnolog&iacute;a del hibridoma resultante. Aun as&iacute;, si se requiere una fuente ilimitada de un tipo solo y homog&eacute;neo de anticuerpo, la opci&oacute;n es la tecnolog&iacute;a monoclonal. Adem&aacute;s, los inmunorreactivos estandarizados pueden facilitar la aceptaci&oacute;n de inmunoensayos en el laboratorio anal&iacute;tico asegurando una fuente a largo plazo de kits con un funcionamiento definido [59, 67, 68].</p>     <p>El procedimiento para producir los anticuerpos monoclonales es similar para diversos analitos; en particular para el insecticida modelo carbaril se ejecutaron los pasos siguientes [66]: (1) inmunizaci&oacute;n de las ratonas adultas de 8-10 semanas, (2) fusi&oacute;n celular de los linfocitos del bazo de la ratona con c&eacute;lulas del mieloma, (3) selecci&oacute;n de los anticuerpos de alta afinidad secretados por los clones de hibri-doma, que fueron expandidos y criopreservados en nitr&oacute;geno l&iacute;quido y (4) purificaci&oacute;n de los anticuerpos monoclonales y almacenaje a 4 <sup>o</sup>C como precipitados de sulfato de amonio. La afinidad y la especificidad de los anticuerpos monoclonales producidos para el insecticida modelo carbaril se caracteriz&oacute; usando procedimientos de ELISA de anticuerpo inmovilizado o de conjugado inmovilizado [66, 69, 70].</p>     <p>La selecci&oacute;n y la clonaci&oacute;n del hibridoma es uno de los pasos b&aacute;sicos en el desarrollo de anticuerpos monoclonales. Un m&eacute;todo com&uacute;n usado en el laboratorio de la UPV fue el siguiente: ocho a diez d&iacute;as despu&eacute;s de la fusi&oacute;n celular, los sobrenadantes de cultivo fueron seleccionados por la presencia de anticuerpos que reconocieron el analito. La selecci&oacute;n consisti&oacute; en la ejecuci&oacute;n simult&aacute;nea de un ELISA no competitivo y un ELISA competitivo indirecto, para probar la capacidad de los anticuerpos de unirse al conjugado proteico del hapteno inmunizante y de reconocer el analito, respectivamente. Los hibridomas seleccionados fueron clonados y los clones estables productores de anticuerpos fueron expandidos y criopreservados en nitr&oacute;geno l&iacute;quido.</p>     <p><b><font size="3">4. INMOVILIZACI&Oacute;N DE</font></b> <font size="3"><b>INMMUNORREACTIVOS</b></font></p>     ]]></body>
<body><![CDATA[<p>La inmovilizaci&oacute;n de biomol&eacute;culas en un sustrato es fundamental para asegurar el funcionamiento del sensor, debido a su papel en la especificidad, sensibilidad, reproducibilidad y capacidad de reciclaje. Los m&eacute;todos para inmovilizar biomol&eacute;culas divulgados en la literatura son adsorci&oacute;n f&iacute;sica, atrapamiento dentro de una membrana, pel&iacute;culas de Langmuir-Blodgett (LB) y enlace covalente en el soporte. Cada m&eacute;todo tiene sus propias caracter&iacute;sticas y limitaciones, aunque el enlace covalente es el m&aacute;s empleado, porque proporciona la carga superficial estable m&aacute;s alta [71-73].</p>     <p>Algunos de los requisitos que debe satisfacer un proceso de inmovilizaci&oacute;n son los siguientes: (1) retenci&oacute;n de la actividad biol&oacute;gica de las biomol&eacute;-culas despu&eacute;s de la inmovilizaci&oacute;n sobre la superficie del sensor; (2) enlace reproducible, duradero y estable con el sustrato, frente a las variaciones de pH, temperatura, fuerza i&oacute;nica y a la naturaleza qu&iacute;mica del microambiente; y (3) localizaci&oacute;n de las biomol&eacute;-culas de manera uniforme, densa y orientada. Entre todos los m&eacute;todos, el enlace covalente satisface la mayor parte de estos requisitos, aunque en ocasiones tiene algunas limitaciones, entre ellas p&eacute;rdida de actividad de biomol&eacute;culas [72].</p>     <p>Monocapa autoensamblada (SAM) es el nombre general dado a la tecnolog&iacute;a que proporciona el m&eacute;todo para generar pel&iacute;culas monomoleculares (monocapas) de mol&eacute;culas biol&oacute;gicas en una variedad de sustratos. La formaci&oacute;n de tales sistemas de monocapa es muy vers&aacute;til, permitiendo el desarrollo <i>in vitro </i>de las biosuperficies que pueden mimetizar los procesos moleculares naturales en el proceso de reconocimiento [74].</p>     <p>Los tioles y los sulfuros son de particular inter&eacute;s ante todo debido a su adsorci&oacute;n qu&iacute;mica espont&aacute;nea en la superficie de oro, lo que da una organizaci&oacute;n regular y elevada estabilidad t&eacute;rmica, mec&aacute;nica y qu&iacute;mica. Los tioles y los sulfuros con cadena larga son m&aacute;s estables t&eacute;rmicamente; se ha propuesto que su adsorci&oacute;n a la superficie procede por dos m&eacute;todos: (1) disociaci&oacute;n i&oacute;nica y (2) formaci&oacute;n de radical, &eacute;sta m&aacute;s probable [75].</p>     <p>Debido a la estabilidad, la orientaci&oacute;n y la capacidad para funcionalizar los grupos terminales de las mol&eacute;culas, las SAM de los &aacute;cidos mercaptoalca-noicos pueden ofrecer un m&eacute;todo muy conveniente y simple para la inmovilizaci&oacute;n de biomol&eacute;culas en la superficie del electrodo de oro, siendo por ello muy utilizadas en el desarrollo de biosensores, facilitando a las prote&iacute;nas y las enzimas la transferencia de electrones directamente con la superficie del electrodo, mientras que mantienen sus actividades fisiol&oacute;gicas [76-78].</p>     <p>La inmovilizaci&oacute;n del conjugado para el an&aacute;lisis del insecticida modelo carbaril se llev&oacute; a cabo previamente seg&uacute;n se ha descrito [70] y se ilustra en la <a href="#f3">figura 3</a>, cortes&iacute;a de Laura M. Lechuga (IMM-CSIC, Madrid, Espa&ntilde;a). El conjugado prote&iacute;na-hapteno, BSA-CNH, fue inmovilizado en la superficie del sensor mediante la formaci&oacute;n de monocapas autoensambladas (SAM), que proporcionan el enlace covalente de los derivados del analito a la superficie funcionalizada de una manera controlada. Para formar la SAM, una soluci&oacute;n de alcanotiol o de &aacute;cido mercaptoundecanoico se dej&oacute; reaccionar por adsorci&oacute;n sobre la superficie del electrodo de oro del sensor [70]. Los grupos carbox&iacute;licos se activaron mediante reacci&oacute;n con un reactivo intermedio N-hidroxisuccinimida (NHS) usando una mezcla de carbodiimida (EDC) y NHS en agua. En la reacci&oacute;n la EDC convierte el &aacute;cido carbox&iacute;lico en el &eacute;ster de N-hidroxisuccinimida, que puede unirse covalente-mente a los grupos amino libres de los conjugados de BSA-hapteno.</p>     <p>    <center>   <font face="verdana" size="2"><a name="f3"><img src="img/revistas/eia/n7/n7a09f3.jpg" /></a></font> </center> </p>     <p>El conjugado BSA-hapteno fue inmovilizado en una soluci&oacute;n salina de tamp&oacute;n fosfato (PBS). Luego se agreg&oacute; etanolamina para eliminar los conjugados no covalentemente unidos a la capa y desactivar todos los NHS-&eacute;steres que no reaccionaron y que quedaban como residuo en la superficie del sensor. Este procedimiento asegur&oacute; que s&oacute;lo quedaran en la superficie del sensor los derivados covalentemente unidos al analito.</p>     <p>Para prevenir la desnaturalizaci&oacute;n de la prote&iacute;na, reducir el ocultamiento est&eacute;rico y tambi&eacute;n para mejorar la bioactividad de una prote&iacute;na inmovilizada, los investigadores han propuesto el uso de monocapas autoensambladas mixtas (MSAM) de alcanotioles sobre oro. Las MSAM generalmente se forman por coadsorci&oacute;n de mezclas de dos tioles constituidos por un tiolato con un grupo funcional principal (como un &aacute;cido carbox&iacute;lico) a baja fracci&oacute;n molar y de otro tiolato diluyente de alta fracci&oacute;n molar [79, 80]. El segundo tiol reduce primero la concentraci&oacute;n superficial de los grupos funcionales y reduce as&iacute; a un m&iacute;nimo el ocultamiento est&eacute;rico, la desnaturalizaci&oacute;n parcial de la prote&iacute;na y las interacciones no espec&iacute;ficas que pueden producir se&ntilde;ales de interferencia [79]. Tambi&eacute;n el tiolato diluyente puede actuar para orientar las caracter&iacute;sticas fisicoqu&iacute;micas globales de la frontera de separaci&oacute;n (tales como su car&aacute;cter hidrof&oacute;bico/hidrof&iacute;lico). La caracterizaci&oacute;n de las superficies cubiertas con MSAM sigue siendo tema de numerosos estudios [81].</p>     ]]></body>
<body><![CDATA[<p>El uso de MSAM puede controlar las propiedades qu&iacute;micas, estructurales y biol&oacute;gicas de la prote&iacute;na inmovilizada. Esta capacidad de controlar las caracter&iacute;sticas superficiales en el nivel de nanoes-cala, incluyendo la abundancia, el tipo y distribuci&oacute;n espacial (normal y lateral) de los sitios del grupo funcional extremo, facilitar&aacute; los esfuerzos de desarrollar biomateriales biocompatibles, biosensores y electr&oacute;nica molecular. El control de las caracter&iacute;sticas de la superficie de nanoescala permite ajustar el microambiente superficial para ajustarse a las formas distintas y las funcionalidades superficiales de biomol&eacute;culas. De hecho, las MSAM han mostrado ya comportamientos interesantes de la adsorci&oacute;n con la variaci&oacute;n en la composici&oacute;n superficial de los grupos funcionales extremos [82].</p>     <p><b><font size="3">5.   CARACTERIZACI&Oacute;N DE UN INMUNOSENSOR</font></b></p>     <p>La etapa final en el desarrollo de un inmu-nosensor es su caracterizaci&oacute;n. Se presenta a continuaci&oacute;n un ejemplo pr&aacute;ctico del desarrollo de un biosensor piezoel&eacute;ctrico para el an&aacute;lisis del pesticida modelo carbaril [83]. El inmunosensor piezoel&eacute;ctrico que trabaja en el modo microgravim&eacute;trico para la determinaci&oacute;n de mol&eacute;culas org&aacute;nicas peque&ntilde;as, tales como pesticidas, sigue un procedimiento anal&iacute;tico para la detecci&oacute;n muy similar al esquema presentado en la <a href="#f4">figura 4</a>.</p>     <p>    <center><a name="f4"><img src="img/revistas/eia/n7/n7a09f4.jpg" /></a></center> </p>     <p><b>El transductor piezoel&eacute;ctrico y el sistema</b> <b>de medida. </b>Los cristales del cuarzo obtenidos por corte AT recubiertos con oro de 9-10 MHz (0,167 mm de espesor, 5 mm de di&aacute;metro y 0,196 cm<sup>2</sup> de &aacute;rea activa) fueron adquiridos en International Crystal Manufacturing Company, Inc., Oklahoma, EE. UU. Una vez qu&iacute;micamente funcionalizado, el cristal pie-zoel&eacute;ctrico de cuarzo fue colocado y sellado en una celda de arnita con dos anillos de nitrilo. Solamente una de las caras del cristal estar&aacute; en contacto con los reactivos durante los an&aacute;lisis.</p>     <p>La celda fue incluida en el sistema de flujo, controlado a su vez mediante una bomba perist&aacute;ltica. Las medidas de la frecuencia y de la resistencia durante los an&aacute;lisis se realizaron en un equipo de microbalanza de cristal de cuarzo para investigaci&oacute;n (RQCM) de Maxtek, Inc. Este instrumento es un sistema que proporciona la medida de los efectos de variaci&oacute;n en la masa del cristal y se basa en la t&eacute;cnica de la cancelaci&oacute;n de la capacitancia y se dise&ntilde;a para los usos de la investigaci&oacute;n. Un esquema del sistema completo de la medici&oacute;n se muestra en la <a href="#f5">figura 5</a>.</p>     <p>    <center><a name="f5"><img src="img/revistas/eia/n7/n7a09f5.jpg" /></a></center> </p>     <p><b>An&aacute;lisis de datos. </b>Las curvas patr&oacute;n normalizadas se obtuvieron trazando la disminuci&oacute;n de la frecuencia contra el logaritmo de la concentraci&oacute;n del analito. Los puntos experimentales se adaptaron a la ecuaci&oacute;n log&iacute;stica de cuatro variables:</p>     ]]></body>
<body><![CDATA[<p>    <center>y = D + (A-D)/[I + (x/C)<sup>B</sup>]</center> </p>     <p>donde A es el asint&oacute;tico m&aacute;ximo (se&ntilde;al m&aacute;xima en la ausencia del analito, Sm&aacute;x), B es la pendiente de la curva en el punto de inflexi&oacute;n (relacionado con la concentraci&oacute;n del analito que da un 50% de inhibici&oacute;n de Sm&aacute;x: C, I<sub>50</sub>) y D es el m&iacute;nimo asint&oacute;tico (se&ntilde;al del fondo).</p>     <p><b>Procedimiento del inmunoensayo. </b>Los inmunoensayos desarrollados para la determinaci&oacute;n del insecticida fueron pruebas de inhibici&oacute;n basadas en el procedimiento de conjugado inmovilizado, en el cual el hapteno conjugado fue inmovilizado covalentemente sobre la superficie del sensor. Para los an&aacute;lisis de inhibici&oacute;n, una cantidad fija del anticuerpo monoclonal respectivo fue mezclada con soluciones patr&oacute;n del analito, y la mezcla se bombe&oacute; sobre la superficie del sensor. Puesto que los analitos inhiben la uni&oacute;n del anticuerpo a los conjugados inmovilizados respectivos, el aumento en las concentraciones del analito reducir&aacute; el decremento de frecuencia del sensor piezoel&eacute;ctrico.</p>     <p>Se prepararon diversas concentraciones patr&oacute;n del insecticida mediante diluciones seriadas en dimetilformamida (DMF). Los patrones fueron mezclados con una concentraci&oacute;n fija del anticuerpo monoclonal, LIB-CNH45. Las soluciones del analito-anticuerpo fueron incubadas por una hora a temperatura ambiente y despu&eacute;s inyectadas sobre la superficie del sensor. La frecuencia de resonancia del cristal piezoel&eacute;ctrico se registr&oacute; en tiempo real mientras ocurr&iacute;a el enlace entre el anticuerpo libre y el conjugado inmovilizado. Terminado cada ensayo, la regeneraci&oacute;n de la superficie del biosensor se realiz&oacute; usando &aacute;cido clorh&iacute;drico diluido para romper la asociaci&oacute;n anticuerpo-analito. Las curvas patr&oacute;n representativas del ensayo se obtuvieron como promedio de varias curvas patr&oacute;n individuales, previamente normalizadas, expresando la disminuci&oacute;n de la frecuencia provocada por cada concentraci&oacute;n patr&oacute;n como el porcentaje de la m&aacute;xima respuesta (disminuci&oacute;n de la frecuencia obtenida en ausencia del analito).</p>     <p><b>Determinaciones del pesticida. </b>La finalidad &uacute;ltima de un inmunosensor es siempre poder determinar la concentraci&oacute;n de un pesticida en muestras problema. Como era de esperar, en el caso del carbaril que se est&aacute; ilustrando, las se&ntilde;ales de frecuencia proporcionadas por el sensor como respuesta a las diferentes concentraciones del pesticida siguieron curvas de calibraci&oacute;n t&iacute;picas de los ensayos de inhibici&oacute;n, de forma sigmoidea decreciente, similares a la mostrada en la <a href="#f6">figura 6</a>. Estas curvas se obtuvieron mediante el ajuste de los puntos experimentales a la ecuaci&oacute;n log&iacute;stica de cuatro variables ya mencionada. Las curvas se normalizaron expresando el valor de la absorbancia Inc F como (Inc F)/ (Inc F<sub>0</sub>)*100, donde Inc F<sub>0</sub> es la absorbancia indicada a una concentraci&oacute;n cero de insecticida. La misma ecuaci&oacute;n permite tambi&eacute;n obtener el valor de la I<sub>50</sub>, que se define como la concentraci&oacute;n de analito que reduce la se&ntilde;al del an&aacute;lisis al 50% de la m&aacute;xima. Este valor se utiliza habitualmente como una predicci&oacute;n de la sensibilidad del inmunosensor, de tal modo que los valores menores que I<sub>50</sub> indican mayor sensibilidad. En el caso del carbaril la I<sub>50</sub> se situ&oacute; alrededor de 25 ppb, mientras que el l&iacute;mite de predicci&oacute;n del ensayo (LOD) se calcul&oacute; como 7 ppb.</p>     <p>    <center><a name="f6"><img src="img/revistas/eia/n7/n7a09f6.jpg" /></a></center> </p>     <p><b>Reutilizaci&oacute;n del sensor. </b>Para este pesticida los cristales piezoel&eacute;ctricos funcionalizados con el conjugado inmovilizado pudieron ser reutilizados por m&aacute;s de cien veces, con reducciones leves de la se&ntilde;al m&aacute;xima y sin p&eacute;rdidas significativas de sensibilidad. El tiempo total requerido para un ciclo completo de an&aacute;lisis, incluyendo la regeneraci&oacute;n, fue de alrededor de 20 min.</p>     <p><b><font size="3">6. CONCLUSI&Oacute;N</font></b></p>     ]]></body>
<body><![CDATA[<p>Los inmunosensores piezoel&eacute;ctricos pueden considerarse ya como una t&eacute;cnica inmunoqu&iacute;mica alterna, en algunos casos comparable a otras bien establecidas como ELISA. En contraste con las t&eacute;cnicas ELISA que requieren la marcaci&oacute;n de los reactivos y tardan unas dos horas por ensayo, esta t&eacute;cnica puede ser automatizada, no utiliza marcadores y los resultados de los an&aacute;lisis se pueden obtener en pocos minutos. En contrapartida, hoy por hoy es necesario realizar los an&aacute;lisis muestra a muestra. Por tanto, todav&iacute;a se precisa mucho esfuerzo de investigaci&oacute;n para optimizar las t&eacute;cnicas de inmovilizaci&oacute;n y asegurar la regeneraci&oacute;n del sensor, as&iacute; como para obtener sensibilidades comparables a las t&eacute;cnicas ELISA y poder implementar el an&aacute;lisis simult&aacute;neo de muchas muestras. No obstante, las t&eacute;cnicas de inmunoensayo microgravim&eacute;trico deben considerarse como alternativas, de gran valor en muchos casos, a las actualmente establecidas.</p>     <p><b><font size="3">AGRADECIMIENTOS</font></b></p>     <p>Los autores agradecen al subprograma Petra II del programa Alfa II por su soporte financiero. Tambi&eacute;n agradecen el soporte de la Universidad Polit&eacute;cnica de Valencia (UPV) y la Escuela de Ingenier&iacute;a de Antioquia (EIA).</p>     <p><b><font size="3">REFERENCIAS</font></b></p>     <!-- ref --><p>1. Ortega Ortiz, F. Biosensores y biochips: Herramientas para el diagn&oacute;stico y la terap&eacute;utica. 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