<?xml version="1.0" encoding="UTF-8"?><?xml-stylesheet type="text/xsl" href="static/style.xsl"?><OAI-PMH xmlns="http://www.openarchives.org/OAI/2.0/" xmlns:xsi="http://www.w3.org/2001/XMLSchema-instance" xsi:schemaLocation="http://www.openarchives.org/OAI/2.0/ http://www.openarchives.org/OAI/2.0/OAI-PMH.xsd"><responseDate>2026-04-13T00:10:56Z</responseDate><request verb="GetRecord" identifier="oai:www.recercat.cat:2072/482739" metadataPrefix="mets">https://recercat.cat/oai/request</request><GetRecord><record><header><identifier>oai:recercat.cat:2072/482739</identifier><datestamp>2025-04-03T12:06:17Z</datestamp><setSpec>com_2072_98</setSpec><setSpec>col_2072_378192</setSpec></header><metadata><mets xmlns="http://www.loc.gov/METS/" xmlns:xlink="http://www.w3.org/1999/xlink" xmlns:xsi="http://www.w3.org/2001/XMLSchema-instance" xmlns:doc="http://www.lyncode.com/xoai" ID="&#xa;&#x9;&#x9;&#x9;&#x9;DSpace_ITEM_2072-482739" TYPE="DSpace ITEM" PROFILE="DSpace METS SIP Profile 1.0" xsi:schemaLocation="http://www.loc.gov/METS/ http://www.loc.gov/standards/mets/mets.xsd" OBJID="&#xa;&#x9;&#x9;&#x9;&#x9;hdl:2072/482739">
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                     <mods:roleTerm type="text">author</mods:roleTerm>
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                  <mods:namePart>Molín, Jéssica</mods:namePart>
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               <mods:name>
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                     <mods:roleTerm type="text">author</mods:roleTerm>
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                  <mods:namePart>José-López, Roberto</mods:namePart>
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               <mods:name>
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                  <mods:namePart>Ramírez, Gustavo A.</mods:namePart>
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               <mods:name>
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                     <mods:roleTerm type="text">author</mods:roleTerm>
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                  <mods:namePart>Pumarola i Batlle, Martí</mods:namePart>
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                  <mods:dateAccessioned encoding="iso8601">2025-04-03T12:06:17Z</mods:dateAccessioned>
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               <mods:identifier type="uri">http://hdl.handle.net/2072/482739</mods:identifier>
               <mods:abstract>PTEN is a critical tumor suppressor gene that plays a vital role in regulating cell proliferation, migration, and survival. The loss of PTEN function, either by genetic alterations or decreased protein expression, is frequent in human gliomas and has been correlated with tumor progression, grade, therapeutic resistance, and decreased overall survival in patients with glioma. This study investigates the immunohistochemical expression of PTEN in canine gliomas to evaluate possible alterations, as those reported in human gliomas. Our research demonstrates for the first time a variable reduction in PTEN protein expression in high-grade canine gliomas, particularly in astrocytomas. These observations are in line with those reported in human gliomas and provide a rationale for future studies regarding abnormalities in PTEN expression and PI3K/Akt/mTor pathway in canine gliomas, to evaluate its prognostic and therapeutic implications. Phosphatase and tensin homolog (PTEN) is a critical tumor suppressor gene with a vital role in regulating cell proliferation, migration, and survival. The loss of PTEN function, either by genetic alterations or decreased protein expression, is frequent in human gliomas and has been correlated with tumor progression, grade, therapeutic resistance, and decreased overall survival in patients with glioma. While different genetic mutations in PTEN gene have been occasionally reported in canine gliomas, no alterations in protein expression have been reported. This study investigates the immunohistochemical expression of PTEN in canine gliomas to evaluate possible alterations, as those reported in human gliomas. Immunohistochemical PTEN expression and pattern distribution were analyzed in 37 spontaneous canine gliomas. Among gliomas, 52.6% cases showed high PTEN expression and 48.6% displayed reduced (13.5%) or highly reduced (35.1%) immunopositivity. Most oligodendrogliomas showed high expression (73.7%), while the majority of astrocytomas (69.2%) showed a reduced or highly reduced expression. A reduced PTEN expression was mostly associated with a heterogeneous loss of PTEN immunopositivity. These observations are in line with those reported in human gliomas and provide a rationale for future studies regarding abnormalities in PTEN expression and PI3K/Akt/mTor pathway in canine gliomas, to evaluate its prognostic and therapeutic implications.</mods:abstract>
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               <mods:accessCondition type="useAndReproduction">open access Aquest document està subjecte a una llicència d'ús Creative Commons. Es permet la reproducció total o parcial, la distribució, la comunicació pública de l'obra i la creació d'obres derivades, fins i tot amb finalitats comercials, sempre i quan es reconegui l'autoria de l'obra original. https://creativecommons.org/licenses/by/4.0/</mods:accessCondition>
               <mods:subject>
                  <mods:topic>Astrocytoma</mods:topic>
               </mods:subject>
               <mods:subject>
                  <mods:topic>Dog</mods:topic>
               </mods:subject>
               <mods:subject>
                  <mods:topic>High grade</mods:topic>
               </mods:subject>
               <mods:subject>
                  <mods:topic>Immunohistochemistry</mods:topic>
               </mods:subject>
               <mods:subject>
                  <mods:topic>Oligodendroglioma</mods:topic>
               </mods:subject>
               <mods:subject>
                  <mods:topic>PTEN</mods:topic>
               </mods:subject>
               <mods:subject>
                  <mods:topic>PI3K/Akt/mTor</mods:topic>
               </mods:subject>
               <mods:subject>
                  <mods:topic>Signaling pathways</mods:topic>
               </mods:subject>
               <mods:subject>
                  <mods:topic>Undefined glioma</mods:topic>
               </mods:subject>
               <mods:titleInfo>
                  <mods:title>Immunohistochemical Expression of PTEN in Canine Gliomas</mods:title>
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               <mods:genre>Article</mods:genre>
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