Zoological Institute - Structural Biology, Kiel University 24118, Kiel, Germany.
Pharmaceutical Institute - Medicinal Chemistry, Kiel University 24118, Kiel, Germany.
J Med Chem. 2024 Oct 24;67(20):18090-18097. doi: 10.1021/acs.jmedchem.4c01148. Epub 2024 Oct 13.
-Hydroxyurea has been known since the 1960s as an antiproliferative drug and is used both in oncology and for treatment of hematological disorders such as sickle cell anemia where very high daily doses are administered. It is assumed that the cellular effect of -hydroxyurea is caused by inhibition of ribonucleotide reductase, while alternative mechanisms, e.g., generation of nitric oxide, have also been proposed. Despite its many therapeutic applications, the metabolism of hydroxyurea is largely unexplored. The major elimination pathway of -hydroxyurea is the reduction to urea. Since the mitochondrial amidoxime reducing component (mARC) is known for its -reductive activity, we investigated the reduction of NHU by this enzyme system. This study presents and evidence that this reductive biotransformation is specifically mediated by the mARC1. Inactivation by mARC1 is a possible explanation for the high doses of NHU required for treatment.
羟脲自 20 世纪 60 年代以来一直作为一种抗增殖药物而为人所知,它既用于肿瘤学,也用于治疗镰状细胞贫血等血液疾病,在这些疾病中,每天给予非常高的剂量。人们认为 -羟脲的细胞作用是由核昔酸还原酶的抑制引起的,而其他机制,例如一氧化氮的产生,也已经被提出。尽管羟脲有许多治疗应用,但它的代谢过程在很大程度上仍未被探索。-羟脲的主要消除途径是还原为尿素。由于线粒体酰胺氧化还原成分(mARC)以其 -还原活性而闻名,我们研究了该酶系统对 NHU 的还原。本研究提供了 和 证据表明,这种还原生物转化是由 mARC1 特异性介导的。mARC1 的失活可能是治疗需要高剂量 NHU 的原因之一。
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