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Expression and Characterization of Recombinant Rat Acyl-CoA Synthetases 1, 4, and 5
Inhibition by triacsins and troglitazone of long chain fatty acid incorporation into cellular lipids suggests the existence of inhibitor-sensitive and -resistant acyl-CoA synthetases (ACS, EC 6.2.1.3 ) that are linked to specific metabolic pathways. In order to test this hypothesis, we cloned and pu...
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| Published in: | The Journal of biological chemistry 2001-01, Vol.276 (27), p.24667-24673 |
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| Main Authors: | , , |
| Format: | Article |
| Language: | English |
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| Online Access: | Get full text |
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| Summary: | Inhibition by triacsins and troglitazone of long chain fatty acid incorporation into cellular lipids suggests the existence
of inhibitor-sensitive and -resistant acyl-CoA synthetases (ACS, EC 6.2.1.3 ) that are linked to specific metabolic pathways. In order to test this hypothesis, we cloned and purified rat ACS1, ACS4,
and ACS5, the isoforms present in liver and fat cells, expressed the isoforms as ACS-Flag fusion proteins in Escherichia coli, and purified them by Flag affinity chromatography. The Flag epitope at the C terminus did not alter the kinetic properties
of the enzyme. Purified ACS1-, 4-, and 5-Flag isoforms differed in their apparent K
m values for ATP, thermolability, pH optima, requirement for Triton X-100, and sensitivity to N -ethylmaleimide and phenylglyoxal. The ACS inhibitor triacsin C strongly inhibited ACS1 and ACS4, but not ACS5. The thiazolidinedione
(TZD) insulin-sensitizing drugs and peroxisome proliferator-activated receptor γ (PPARγ) ligands, troglitazone, rosiglitazone,
and pioglitazone, strongly and specifically inhibited only ACS4, with an IC 50 of less than 1.5 μ m . Troglitazone exhibited a mixed type inhibition of ACS4. α-Tocopherol, whose ring structure forms the non-TZD portion of
troglitazone, did not inhibit ACS4, indicating that the thiazolidine-2,4-dione moiety is the critical component for inhibition.
A non-TZD PPARγ ligand, GW1929, which is 7-fold more potent than rosiglitazone, inhibited ACS1 and ACS4 poorly with an IC 50 of greater than 50 μ m , more than 100-fold higher than was required for rosiglitazone, thereby demonstrating the specificity of TZD inhibition.
Further, the PPARα ligands, clofibrate and GW4647, and various xenobiotic carboxylic acids known to be incorporated into complex
lipids had no effect on ACS1, -4, or -5. These results, together with previous data showing that triacsin C and troglitazone
strongly inhibit triacylglycerol synthesis compared with other metabolic pathways, suggest that ACS1 and ACS4 catalyze the
synthesis of acyl-CoAs used for triacylglycerol synthesis and that lack of inhibition of a metabolic pathway by triacsin C
does not prove lack of acyl-CoA involvement. The results further suggest the possibility that the insulin-sensitizing effects
of the thiazolidinedione drugs might be achieved, in part, through direct interaction with ACS4 in a PPARγ-independent manner. |
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| ISSN: | 0021-9258 1083-351X |
| DOI: | 10.1074/jbc.M010793200 |