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J. Biol. Chem., Vol. 261, Issue 18, 8213-8217, Jun, 1986
Evidence for multiple condensing enzymes in rat hepatic microsomes catalyzing the condensation of saturated, monounsaturated, and polyunsaturated acyl coenzyme A
MR Prasad, MN Nagi, D Ghesquier, L Cook and DL Cinti
The condensation of palmitoyl-CoA with malonyl-CoA by rat hepatic
microsomes was competitively inhibited by myristoyl-CoA, whereas it was
noncompetitively inhibited by palmitoleoyl and gamma-linolenoyl-CoA.
Furthermore, the condensation of palmitoleoyl-CoA with malonyl-CoA was also
noncompetitively inhibited by gamma-linolenoyl-CoA. Replacement of normal
diet by a fat-free high carbohydrate diet resulted in 8-, 2.5-, and
2.3-fold increases in the condensation rates of both palmitoyl- and
myristoyl-CoA, palmitoleoyl-CoA, and gamma-linolenoyl-CoA, respectively. On
the other hand, administration of di-(2- ethylhexyl)phthalate (DEHP)
resulted in a 2-fold stimulation of the condensation activities with
myristoyl- and palmitoyl-CoA, while those with palmitoleoyl- and
gamma-linolenoyl-CoA decreased to about 83 and 63%, respectively. Similar
results following dietary changes or DEHP administration were obtained for
total elongation activities. Finally condensation activities of 16:0, 16:1,
and gamma-18:3 CoA were differently affected by the proteolytic enzyme,
chymotrypsin. The competitive substrate studies, those of dietary and DEHP
administration, and the differential action of chymotrypsin strongly
suggest the existence of at least three discrete condensing enzymes
catalyzing the condensation of saturated, monounsaturated, and
polyunsaturated acyl-CoAs. These studies also indicate that the
condensation reaction is the regulating and rate-limiting step of the fatty
acid chain elongation system.

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Copyright © 1986 by the American Society for Biochemistry and Molecular Biology.
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