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Extra-hepatic isozymes from the CYP1 and CYP2 families as potential chemotherapeutic targets.

机译:CYP1和CYP2家族的肝外同工酶作为潜在的化学治疗靶标。

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Cytochrome P450 isozymes (CYPs) from the CYP1 and CYP2 families located primarily in extra-hepatic tissues represent ideal candidates for chemotherapeutic drug development because: 1.) They are usually involved in the metabolism of endogenous substrates that are important for cell homeostasis and growth 2.) The over-expression of certain CYPs has been reported in various malignancies 3.) There has been much clinical success with inhibitors of CYPs involved in hormone synthesis. The most ideal candidates for chemotherapeutic drug development will be discussed in terms of their biological importance and relevant substrates. This review will focus on: 1.) CYP1A1 and CYP1B1 from the CYP1 family because of the dual role these enzymes play in the bioactivation of known carcinogens and endogenous compounds. 2.) The targeting of CYPs in hypoxic environments as a therapeutic strategy. 3.) CYP2J2 and its role in the metabolism of arachidonic acid to epoxyeicosatrienoic acids and angiogenesis will also be examined. While much progress has been made towards understanding the role of CYPs in extrahepatic tissue, future studies focused on the development of selective inhibitors coupled with appropriate delivery systems that would target the tumor micro-environments could lead to significant advancement in chemotherapeutic strategies.
机译:来自CYP1和CYP2家族的细胞色素P450同工酶(CYP)主要位于肝外组织中,是化学疗法药物开发的理想候选者,因为:1.)它们通常参与内源性底物的代谢,而内源性底物对于细胞的稳态和生长很重要2 。)在各种恶性肿瘤中都有某些CYP的过度表达的报道。3.)涉及激素合成的CYP抑制剂在临床上取得了很多成功。化疗药物开发的最理想候选者将根据其生物学重要性和相关底物进行讨论。这篇综述将侧重于:1.)CYP1家族的CYP1A1和CYP1B1,因为这些酶在已知致癌物和内源性化合物的生物活化中起双重作用。 2.)在低氧环境中以CYP为靶点作为治疗策略。 3.)还将研究CYP2J2及其在花生四烯酸代谢为环氧二十碳三烯酸的代谢中的作用以及血管生成。尽管在了解CYP在肝外组织中的作用方面已取得了很大进展,但未来的研究集中在选择性抑制剂的开发以及靶向肿瘤微环境的合适递送系统上,可能会导致化疗策略的显着进步。

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