Sharma Kamalesh K, Wang Zhu, Motola Daniel L, Cummins Carolyn L, Mangelsdorf David J, Auchus Richard J
Division of Endocrinology and Metabolism, Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX 75390, USA.
Mol Endocrinol. 2009 May;23(5):640-8. doi: 10.1210/me.2008-0415. Epub 2009 Feb 5.
The nuclear hormone receptor DAF-12 from Caenorhabditis elegans is activated by dafachronic acids, which derive from sterols upon oxidation by DAF-9, a cytochrome P450. DAF-12 activation is a critical checkpoint in C. elegans for acquisition of reproductive competence and for entry into adulthood rather than dauer diapause. Previous studies implicated the (25S)-Delta(7)-dafachronic acid isomer as the most potent compound, but the (25S)-Delta(4)-isomer was also identified as an activator of DAF-12. To explore the tolerance of DAF-12 for structural variations in the ligand and to enable further studies requiring large amounts of ligands for DAF-12 and homologs in other nematodes, we synthesized (25R)- and (25S)-isomers of five dafachronic acids differing in A/B-ring configurations. Both the (25S)- and (25R)-Delta(7)-dafachronic acids are potent transcriptional activators in a Gal4-transactivation assay using HEK-293 cells, with EC(50) values of 23 and 33 nm, respectively, as are (25S)- and (25R)-Delta(4)-dafachronic acids, with EC(50) values of 23 and 66 nm, respectively. The (25S)- and (25R)-Delta(5)-isomers were much less potent, with EC(50) values approaching 1000 nm, and saturated 5alpha- and 5beta-dafachronic acids showed mostly intermediate potencies. Rescue assays using daf- 9-null mutants confirmed the results from transactivation experiments, but this in vivo assay accentuated the greater potencies of the (25S)-epimers, particularly for the (25S)-Delta(7)-isomer. We conclude that DAF-12 accommodates a large range of structural variation in ligand geometry, but (25S)-Delta(7)-dafachronic acid is the most potent and probably biologically relevant isomer. Potency derives more from the A/B-ring configuration than from the stereochemistry at C-25.
秀丽隐杆线虫的核激素受体DAF-12由二氢蜕皮酸激活,二氢蜕皮酸由细胞色素P450 DAF-9氧化甾醇产生。DAF-12的激活是秀丽隐杆线虫获得生殖能力以及进入成年期而非滞育期的关键检查点。先前的研究表明,(25S)-Δ⁷-二氢蜕皮酸异构体是最有效的化合物,但(25S)-Δ⁴-异构体也被鉴定为DAF-12的激活剂。为了探索DAF-12对配体结构变化的耐受性,并为进一步研究提供大量用于DAF-12及其他线虫同源物的配体,我们合成了A/B环构型不同的五种二氢蜕皮酸的(25R)-和(25S)-异构体。在使用HEK-293细胞的Gal4反式激活试验中,(25S)-和(25R)-Δ⁷-二氢蜕皮酸都是有效的转录激活剂,EC₅₀值分别为23和33 nM,(25S)-和(25R)-Δ⁴-二氢蜕皮酸也是如此,EC₅₀值分别为23和66 nM。(25S)-和(25R)-Δ⁵-异构体的效力要低得多,EC₅₀值接近1000 nM,饱和的5α-和5β-二氢蜕皮酸大多表现出中等效力。使用daf-9基因敲除突变体的拯救试验证实了反式激活实验的结果,但这种体内试验突出了(25S)-差向异构体的更高效力,特别是对于(25S)-Δ⁷-异构体。我们得出结论:DAF-12能适应配体几何结构的大范围结构变化,但(25S)-Δ⁷-二氢蜕皮酸是最有效的且可能是生物学上相关的异构体。效力更多地源于A/B环构型而非C-25处的立体化学。
