Hay Michael P, Pchalek Karin, Pruijn Frederik B, Hicks Kevin O, Siim Bronwyn G, Anderson Robert F, Shinde Sujata S, Phillips Victoria, Denny William A, Wilson William R
Auckland Cancer Society Research Centre, Faculty of Medical and Health Sciences, The University of Auckland, New Zealand.
J Med Chem. 2007 Dec 27;50(26):6654-64. doi: 10.1021/jm701037w. Epub 2007 Dec 6.
Tirapazamine (TPZ) and related 1,2,4-benzotriazine 1,4 dioxides (BTOs) are selectively toxic under hypoxia, but their ability to kill hypoxic cells in tumors is generally limited by their poor extravascular transport. Here we show that removing hydrogen bond donors by replacing the 3-NH2 group of TPZ with simple alkyl groups increased their tissue diffusion coefficients as measured in multicellular layer cultures. This advantage was largely retained using solubilizing 3-alkylaminoalkyl substituents provided these were sufficiently lipophilic at pH 7.4. The high reduction potentials of such compounds resulted in rates of metabolism too high for optimal penetration into hypoxic tissue, but electron-donating 6- and 7-substituents moderated metabolism. Pharmacokinetic/pharmacodynamic model-guided screening was used to select BTOs with optimal extravascular transport and hypoxic cytotoxicity properties for evaluation against HT29 human tumor xenografts in combination with radiation. This identified four novel 3-alkyl BTOs providing greater clonogenic killing of hypoxic cells than TPZ at equivalent host toxicity, with the 6-morpholinopropyloxy-BTO 22 being 3-fold more active.
替拉扎明(TPZ)及相关的1,2,4-苯并三嗪1,4-二氧化物(BTOs)在缺氧条件下具有选择性毒性,但其在肿瘤中杀死缺氧细胞的能力通常受限于其血管外转运能力较差。在此我们表明,通过用简单烷基取代TPZ的3-NH₂基团来去除氢键供体,可提高其在多细胞层培养物中测得的组织扩散系数。使用增溶的3-烷基氨基烷基取代基时,若这些取代基在pH 7.4时具有足够的亲脂性,则这一优势在很大程度上得以保留。此类化合物的高还原电位导致代谢速率过高,不利于其最佳渗透进入缺氧组织,但供电子的6-和7-取代基可减缓代谢。药代动力学/药效学模型指导的筛选用于选择具有最佳血管外转运和缺氧细胞毒性特性的BTOs,以评估其与放疗联合用于对抗HT29人肿瘤异种移植的效果。这确定了四种新型3-烷基BTOs,在同等宿主毒性下,它们对缺氧细胞的克隆源性杀伤作用比TPZ更强,其中6-吗啉丙氧基-BTO 22的活性高3倍。
Zotero 插件