Rydzewski Robert M, Burrill Leland, Mendonca Rohan, Palmer James T, Rice Mark, Tahilramani Ram, Bass Kathryn E, Leung Ling, Gjerstad Erik, Janc James W, Pan Lin
Department of Medicinal Chemistry, 180 Kimball Way, South San Francisco, California 94080, USA.
J Med Chem. 2006 May 18;49(10):2953-68. doi: 10.1021/jm058289o.
Beginning with the peptide sequence Cbz-Ile-Glu(OtBu)-Ala-Leu found in PSI (3), a series of vinyl sulfones (VS) were synthesized for evaluation as inhibitors of the chymotrypsin-like activity of the 20S proteasome. Variations at the key P3 position confirmed the importance of a long side chain capped with a hydrophobic group for optimal potency, consistent with a model of binding to the S3 subsite. The tert-butyl glutamic ester initially used at P3 gave plasma unstable, insoluble compounds and was replaced with the better isostere, N-beta-neopentyl asparagine. The inhibitors were shortened by replacing the N-terminal Cbz-isoleucine with a p-tosyl group without loss of potency. Small l-amino acids were used at P2, where d-substitution was not tolerated. The resulting optimized P4-P3-P2 sequence was grafted onto a novel proteasome inhibitor warhead, 2-keto-1,3,4-oxadiazoles (KOD), to produce reversible, subnanomolar proteasome inhibitors that were 1000-fold selective versus cathepsin B (CatB), cathepsin S (CatS), and trypsin-like as well as PGPH-like proteasome activity. A number of compounds in both the VS and the KOD series exhibited growth inhibitory effects against the human prostate cancer cell line PC3 at submicromolar concentrations.
从在PSI(3)中发现的肽序列Cbz-Ile-Glu(OtBu)-Ala-Leu开始,合成了一系列乙烯基砜(VS),作为20S蛋白酶体糜蛋白酶样活性抑制剂进行评估。关键P3位置的变化证实了带有疏水基团的长侧链对最佳效力的重要性,这与与S3亚位点结合的模型一致。最初在P3使用的叔丁基谷氨酸酯产生血浆不稳定、不溶性化合物,并用更好的电子等排体N-β-新戊基天冬酰胺取代。通过用对甲苯磺酰基取代N端的Cbz-异亮氨酸来缩短抑制剂,而不损失效力。在P2使用小的L-氨基酸,其中D-取代是不被容忍的。将得到的优化的P4-P3-P2序列嫁接到一种新型蛋白酶体抑制剂弹头2-酮-1,3,4-恶二唑(KOD)上,以产生可逆的、亚纳摩尔级的蛋白酶体抑制剂,其对组织蛋白酶B(CatB)、组织蛋白酶S(CatS)、胰蛋白酶样以及PGPH样蛋白酶体活性的选择性是1000倍。VS和KOD系列中的许多化合物在亚微摩尔浓度下对人前列腺癌细胞系PC3表现出生长抑制作用。
