Rational design of Rhizopus oryzae lipase with modified stereoselectivity toward triradylglycerols

Abstract: The binding site of sn-1(3)-regioselective Rhizopus oryzae lipase (ROL) has been engineered to change the stereoselectivity of hydrolysis of triacylglycerol substrates and analogs. Two types of prochiral triradylglycerols were considered: 'flexible' substrates with ether, benzylether or ester groups, and 'rigid' substrates with amide or phenyl groups, respectively, in the sn-2 position. The molecular basis of sn-1(3) stereoselectivity of ROL was investigated by modeling the interactions between substrates and … Show more

“…[10,15,19,20,34] The results for secondary alcohols are in accordance with complementary methods which model enantioselectivity in hydrolasecatalyzed reactions by evaluating the free energy of enzyme-substrate complexes. [21,35] Small changes in structure lead to small changes in enantioselectivity Intuitively, one would expect that homologous enzymes have identical enantiopreference as it was observed for…”

“…by switching from L-to D-tartrate in the Sharpless-epoxidation [39] by a simple and general rule. [16,17] Changes of enantiopreference by point mutations in the substrate binding site have also been observed for lipases, [15] phosphotriesterases, [41] lactate dehydrogenases, [42] and alcohol dehydrogenases. [43] Thus, our results support the general idea that enantiopreference is not an inherent property of an enzyme but can be tuned by protein engineering.…”

“…Several attempts to vary enantioselectivity of esterases and lipases by directed evolution, [11][12][13] and by rational protein engineering were successful. [14,15] The latter method also yields insight into the molecular mechanism of enantiorecognition. X-ray structures of several lipases and esterases complexed with chiral substrate analogous inhibitors are available.…”

A Molecular Mechanism of Enantiorecognition of Tertiary Alcohols by Carboxylesterases

“…[10,15,19,20,34] The results for secondary alcohols are in accordance with complementary methods which model enantioselectivity in hydrolasecatalyzed reactions by evaluating the free energy of enzyme-substrate complexes. [21,35] Small changes in structure lead to small changes in enantioselectivity Intuitively, one would expect that homologous enzymes have identical enantiopreference as it was observed for…”

“…by switching from L-to D-tartrate in the Sharpless-epoxidation [39] by a simple and general rule. [16,17] Changes of enantiopreference by point mutations in the substrate binding site have also been observed for lipases, [15] phosphotriesterases, [41] lactate dehydrogenases, [42] and alcohol dehydrogenases. [43] Thus, our results support the general idea that enantiopreference is not an inherent property of an enzyme but can be tuned by protein engineering.…”

“…Several attempts to vary enantioselectivity of esterases and lipases by directed evolution, [11][12][13] and by rational protein engineering were successful. [14,15] The latter method also yields insight into the molecular mechanism of enantiorecognition. X-ray structures of several lipases and esterases complexed with chiral substrate analogous inhibitors are available.…”

A Molecular Mechanism of Enantiorecognition of Tertiary Alcohols by Carboxylesterases

“…As shown previously, docking methods are generally reliable and able to correctly predict stereopreference [5,22,23]. However, problems occur when energy-based scoring strategies are used to rank substrates [24].…”

Structural basis of stereoselectivity in Candida rugosa lipase-catalyzed hydrolysis of secondary alcohols

“…This hypothesis was tested replacing Leu258 either by the smaller amino acids alanine and serine or by the bulky phenylalanine. According to the model, the ROL Leu258Phe exhibited an increased sn-3 stereoselectivity toward triacylglycerol analogs with rigid and/or bulky sn-2 substituents adjacent to C2 of glycerol, while Leu258Ala and Leu258Ser substitutions decreased the sn-3 stereoselectivity or even reversed it (see section 6 for more details) [71]. Combining both rigidity and bulkiness of the sn-2 substituent, hydrolysis of ROL Leu258Phe toward the benzoylamide substrate revealed the most significant increase in stereoselectivity as compared to ROL wild type (E was 195 and 15, respectively, at 50 % conversion; Fig.…”

Molecular basis of lipase stereoselectivity