Stereoselective Conjugation of Prostaglandin A2 and Prostaglandin J2 with Glutathione, Catalyzed by the Human Glutathione S-Transferases A1-1, A2-2, M1a-1a, and P1-1

Abstract

Prostaglandins containing an α,β-unsaturated keto group, such as prostaglandin A₂ (PGA₂) and prostaglandin J₂ (PGJ₂), inhibit cell proliferation. These cyclopentenone prostaglandins may be conjugated with GSH chemically or enzymatically via glutathione S-transferases, and this has been suggested to result in inhibition of the antiproliferative mode of action. In the present study, the role of the major human GSTs in the conjugation of PGA₂ and PGJ₂ with GSH was investigated with purified enzymes, i.e., the Alpha-class enzymes GST A1-1 and GST A2-2, the Mu-class enzyme GST M1a-1a, and the Pi-class enzyme GST P1-1. The GSH conjugates were separated from the parent compound by HPLC and identified by fast atom bombardment mass spectrometry and ¹H-NMR. Two GSH conjugates were found for both PGA₂ and PGJ₂, the R- and S-GSH conjugates of both prostaglandins. Incubation experiments with PGA₂ and PGJ₂ (70−600 μM) clearly showed the role of individual GSTs in the conjugation of PGA₂ and PGJ₂. Compared to the chemical reaction, enzyme activities towards PGA₂ were up to 5.4 times as high (GSTA1-1) at the lowest concentration (70 μM), while at the highest concentration (600 μM) enzyme activities were up to 3.0 times as high (GST P1-1). For PGJ₂, enzyme activities were up to 4.3 (GSTM1a-1a, 70 μM) and up to 3.1 (GSTM1a-1a, 600 μM) times as high. As expected, similar amounts of the R- and S-conjugates of both prostaglandins were found in the chemical reaction. Striking stereoselectivities in conjugating activities were observed for GST A1-1 and GST P1-1. GST A1-1 favors the formation of the R-GSH conjugates of both prostaglandins. GST P1-1 showed a clear selectivity with regard to the formation of the S-GSH conjugate of PGA₂. However, this selectivity was not found for the formation of the S-GSH conjugate of PGJ₂. GSTM1a-1a showed no stereoselectivity with regard to the GSH conjugation of both PGA₂ and PGJ₂. GSTA2-2 only showed some minor formation of the R-GSH conjugate of PGJ₂. The possible implications of the observed stereoselectivity on the effects of PGA₂ and PGJ₂ are discussed.