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               <dc:title>Design and characterization of genetically engineered zebrafish aquaporin-3 mutants highly permeable to the cryoprotectant ethylene glycol</dc:title>
               <dc:creator>Chauvigné, François</dc:creator>
               <dc:creator>Lubzens, Esther</dc:creator>
               <dc:creator>Cerdà, Joan</dc:creator>
               <dc:contributor>Producció Animal</dc:contributor>
               <dc:contributor>Aqüicultura</dc:contributor>
               <dc:description>Background: Increasing cell membrane permeability to water and cryoprotectants is critical for the successful&#xd;
cryopreservation of cells with large volumes. Artificial expression of water-selective aquaporins or aquaglyceroporins&#xd;
(GLPs), such as mammalian aquaporin-3 (AQP3), enhances cell permeability to water and cryoprotectants, but it is&#xd;
known that AQP3-mediated water and solute permeation is limited and pH dependent. To exploit further the&#xd;
possibilities of using aquaporins in cryobiology, we investigated the functional properties of zebrafish (Danio rerio) GLPs.&#xd;
Results: Water, glycerol, propylene glycol and ethylene glycol permeability of zebrafish Aqp3a, -3b, -7, -9a, -9b,&#xd;
-10a and -10b, and human AQP3, was examined. Expression in Xenopus laevis oocytes indicated that the&#xd;
permeability of DrAqp3a and -3b to ethylene glycol was higher than for glycerol or propylene glycol under&#xd;
isotonic conditions, unlike other zebrafish GLPs and human AQP3, which were more permeable to glycerol. In&#xd;
addition, dose-response experiments and radiolabeled ethylene glycol uptake assays suggested that oocytes&#xd;
expressing DrAqp3b were permeated by this cryoprotectant more efficiently than those expressing AQP3. Water&#xd;
and ethylene glycol transport through DrAqp3a and -3b were, however, highest at pH 8.5 and completely&#xd;
abolished at pH 6.0. Point mutations in the DrAqp3b amino acid sequence rendered two constructs, DrAqp3bT85A showing higher water and ethylene glycol permeability at neutral and alkaline pH, and DrAqp3b-H53A/G54H/&#xd;
T85A, no longer inhibited at acidic pH but less permeable than the wild type. Finally, calculation of permeability&#xd;
coefficients for ethylene glycol under concentration gradients confirmed that the two DrAqp3b mutants were&#xd;
more permeable than wild-type DrAqp3b and/or AQP3 at neutral pH, resulting in a 2.6- to 4-fold increase in the&#xd;
oocyte intracellular concentration of ethylene glycol.&#xd;
Conclusion: By single or triple point mutations in the DrAqp3b amino acid sequence, we constructed one mutant&#xd;
with enhanced ethylene glycol permeability and another with reduced pH sensitivity. The DrAqp3b and the two&#xd;
mutant constructs may be useful for application in cryobiology.</dc:description>
               <dc:date>2025-10-22T11:30:25Z</dc:date>
               <dc:date>2025-10-22T11:30:25Z</dc:date>
               <dc:date>2011-04-08</dc:date>
               <dc:type>info:eu-repo/semantics/article</dc:type>
               <dc:identifier>Chauvigné, François, Esther Lubzens, and Joan J. Cerdà. 2011. “Design and Characterization of Genetically Engineered Zebrafish Aquaporin-3 Mutants Highly Permeable to the Cryoprotectant Ethylene Glycol.” BMC Biotechnology 11 (1): 34. doi: 10.1186/1472-6750-11-34</dc:identifier>
               <dc:identifier>1472-6750</dc:identifier>
               <dc:identifier>http://hdl.handle.net/20.500.12327/2989</dc:identifier>
               <dc:identifier>https://doi.org/10.1186/1472-6750-11-34</dc:identifier>
               <dc:language>eng</dc:language>
               <dc:relation>BMC Biotechnology</dc:relation>
               <dc:relation>MEC/ /AGL2007-60262/ES/MECANISMOS MOLECULARES IMPLICADOS EN LA REGULACION DE AQUAPORINAS EN EL OOCITO DE PECES MARINOS Y APLICACIONES PARA LA CRIOPRESERVACION DE GAMETOS FEMENINOS EN ACUICULTURA/ACU</dc:relation>
               <dc:relation>EC/FP6/35995/EU/Integrated analyses of aquaporin structure and function/AQUA(GLYCERO)PORINS</dc:relation>
               <dc:rights>http://creativecommons.org/licenses/by/4.0/</dc:rights>
               <dc:rights>info:eu-repo/semantics/openAccess</dc:rights>
               <dc:rights>Attribution 4.0 International</dc:rights>
               <dc:publisher>BMC</dc:publisher>
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