Of biological membranes prevents transport of most solutes between the cytosol and the extra cellular environment and between the cytosol and the interior of organelles. Cellular homeostasis therefore relies upon integral membrane proteins allowing selective trans-membrane movement of solutes and information. The essential physiological role of membrane protein activity is visualized by the fact that approximately 60 [2] of all approved drugs are targeting a membrane protein. Despite 1655472 of this, by August 2012 25033180 the number of unique membrane protein structures has only reached 355 [http:// blanco.biomol.uci.edu/Membrane_Proteins_xtal.html] which is extremely low compared to the more than 54,000 structures available through the Protein Data Bank [http:/www.rcsb.org/ pdb/home/home.do]. Only 102 of these membrane proteins are from eukaryots including 36 of human origin. Heterologously expressed protein has been the starting point for seven of the structures [3,4,5,6,7,8]. For essentially all membrane proteins theirdensity in natural tissue is so low that purification on the milligram scale required for crystallization attempts is excluded. Access to purified membrane proteins is further complicated by the observation that the expression systems that successfully delivered more than 90 of proteins used for solving the structures for water soluble proteins, have failed in producing the required densities of recombinant membrane proteins. The reason for this is probably a general failure of cells to cope with high level expression of recombinant membrane embedded proteins [9,10]. Very few examples are found in literature on heterologous expression of eukaryotic membrane proteins to a level where large-scale purification is straight forward or even possible [11,12]. Aquaporins constitute a family of physiologically very important integral membrane proteins that are found in all three kingdoms, eubacteria, archaea and eukaryotes [13]. In human thirteen members of the aquaporin family have been identified [14]. As protein channels they all allow for passive transport of water [15] while some isoforms show additional permeability for small solutes like urea [16], glycerol [16], arsenite [17], antimonite [17], boric acid [18], silicic acid [19], nitrate [20], ammonia [21], hydrogen peroxide [22], carbon dioxide [23] or nitric oxide [24]. HumanHigh Level Human Aquaporin Production in YeastAquaporin-1 (hAQP1) is a 269 amino acids long protein with six transmembrane segments. hAQP1 provides the HA-1077 biological activity plasma membranes of erythrocytes and proximal tubules of the kidney with a high water permeability allowing water to be transported along an osmotic gradient. The physiologically important function of AQP1 is underscored by the finding that AQP1 knock-out mice [25] and humans [26] with defective AQP1suffer from marked polyurea and show low urinary osmolality. AQP1 also plays an important role in choroid plexus epithelium [27] where it facilitates secretion of cerebrospinal fluid and intracranial pressure regulation [28]. AQP1 has been suggested to be involved in a number of pathophysiological conditions including migrane with aura [29], human renal disorders [30] and tumor angiogenesis [31] making it an interesting drug FGF-401 site target. All human Aquaporins have been heterologously expressed, primarily in Xenopus oocytes for characterization of their transport specificity. The highest reported production of hAQP1was obtained in Pichia pastoris [32] and reached 90 mg per l.Of biological membranes prevents transport of most solutes between the cytosol and the extra cellular environment and between the cytosol and the interior of organelles. Cellular homeostasis therefore relies upon integral membrane proteins allowing selective trans-membrane movement of solutes and information. The essential physiological role of membrane protein activity is visualized by the fact that approximately 60 [2] of all approved drugs are targeting a membrane protein. Despite 1655472 of this, by August 2012 25033180 the number of unique membrane protein structures has only reached 355 [http:// blanco.biomol.uci.edu/Membrane_Proteins_xtal.html] which is extremely low compared to the more than 54,000 structures available through the Protein Data Bank [http:/www.rcsb.org/ pdb/home/home.do]. Only 102 of these membrane proteins are from eukaryots including 36 of human origin. Heterologously expressed protein has been the starting point for seven of the structures [3,4,5,6,7,8]. For essentially all membrane proteins theirdensity in natural tissue is so low that purification on the milligram scale required for crystallization attempts is excluded. Access to purified membrane proteins is further complicated by the observation that the expression systems that successfully delivered more than 90 of proteins used for solving the structures for water soluble proteins, have failed in producing the required densities of recombinant membrane proteins. The reason for this is probably a general failure of cells to cope with high level expression of recombinant membrane embedded proteins [9,10]. Very few examples are found in literature on heterologous expression of eukaryotic membrane proteins to a level where large-scale purification is straight forward or even possible [11,12]. Aquaporins constitute a family of physiologically very important integral membrane proteins that are found in all three kingdoms, eubacteria, archaea and eukaryotes [13]. In human thirteen members of the aquaporin family have been identified [14]. As protein channels they all allow for passive transport of water [15] while some isoforms show additional permeability for small solutes like urea [16], glycerol [16], arsenite [17], antimonite [17], boric acid [18], silicic acid [19], nitrate [20], ammonia [21], hydrogen peroxide [22], carbon dioxide [23] or nitric oxide [24]. HumanHigh Level Human Aquaporin Production in YeastAquaporin-1 (hAQP1) is a 269 amino acids long protein with six transmembrane segments. hAQP1 provides the plasma membranes of erythrocytes and proximal tubules of the kidney with a high water permeability allowing water to be transported along an osmotic gradient. The physiologically important function of AQP1 is underscored by the finding that AQP1 knock-out mice [25] and humans [26] with defective AQP1suffer from marked polyurea and show low urinary osmolality. AQP1 also plays an important role in choroid plexus epithelium [27] where it facilitates secretion of cerebrospinal fluid and intracranial pressure regulation [28]. AQP1 has been suggested to be involved in a number of pathophysiological conditions including migrane with aura [29], human renal disorders [30] and tumor angiogenesis [31] making it an interesting drug target. All human Aquaporins have been heterologously expressed, primarily in Xenopus oocytes for characterization of their transport specificity. The highest reported production of hAQP1was obtained in Pichia pastoris [32] and reached 90 mg per l.