硼替佐米抑制哺乳动物碳酸酐酶。
Bortezomib inhibits mammalian carbonic anhydrases.
作者信息
Supuran Claudiu T
机构信息
Università degli Studi di Firenze, Dipartimento Neurofarba, Sezione di Scienze Farmaceutiche e Nutraceutiche, Via U. Schiff 6, 50019 Sesto Fiorentino, Florence, Italy.
出版信息
Bioorg Med Chem. 2017 Oct 1;25(19):5064-5067. doi: 10.1016/j.bmc.2016.10.023. Epub 2016 Oct 19.
We investigated the carbonic anhydrase (CA, EC 4.2.1.1) inhibitory activity of the clinically used antitumor agent bortezomib, a marketed proteasome inhibitor, against all the catalytically active mammalian isoforms CA I-VII, IX, XII-XV. Bortezomib effectively inhibited all these CAs in the micromolar range. hCA II, the physiologically dominant cytosolic isoform showed the highest affinity for the drug, with a K of 1.16μM. The cytosolic slow isoform hCA I was also effectively inhibited, with a K of 1.29μM, whereas the next best affinity was observed for the membrane-anchored form mCA XV, with a K of 2.68μM, followed by two transmembrane isoforms, hCA IX and XIV (Ks of 3.28-3.38μM). The remaining cytosolic (CA III, VII and XIII), membrane-anchored (CA IV), mitochondrial (CA VA, VB), transmembrane (CA XII) and secreted (CA VI) isoforms were slightly less inhibited by bortezomib compared to isoforms discussed above, with Ks ranging between 4.38 and 8.45μM. These data may shed some light on possible side effects and novel antitumor mechanisms of action of this drug.
我们研究了临床使用的抗肿瘤药物硼替佐米(一种已上市的蛋白酶体抑制剂)对所有具有催化活性的哺乳动物同工型碳酸酐酶(CA,EC 4.2.1.1)I-VII、IX、XII-XV的抑制活性。硼替佐米在微摩尔范围内有效抑制所有这些碳酸酐酶。生理上占主导地位的胞质同工型hCA II对该药物表现出最高亲和力,K值为1.16μM。胞质慢同工型hCA I也被有效抑制,K值为1.29μM,而膜锚定形式mCA XV的亲和力次之,K值为2.68μM,随后是两种跨膜同工型hCA IX和XIV(K值为3.28 - 3.38μM)。与上述同工型相比,其余的胞质同工型(CA III、VII和XIII)、膜锚定同工型(CA IV)、线粒体同工型(CA VA、VB)、跨膜同工型(CA XII)和分泌同工型(CA VI)受硼替佐米的抑制作用稍弱,K值在4.38至8.45μM之间。这些数据可能为该药物可能的副作用和新的抗肿瘤作用机制提供一些线索。
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