Design and structure-activity relationships of ether-linked alkylides: Hybrids of 3-O-descladinosyl macrolides and quinolone motifs

IF 4.5 2区医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Bioorganic Chemistry Pub Date : 2024-08-10 DOI:10.1016/j.bioorg.2024.107712

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Abstract

Ketolides (3-keto) such as TE-802 and acylides (3-O-acyl) like TEA0929 are ineffective against constitutively resistant pathogens harboring erythromycin ribosomal methylation (erm) genes. Following our previous work on alkylides (3-O-alkyl), we explored the structure–activity relationships of hybrids combining (R/S) 3-descladinosyl erythromycin with 6/7-quinolone motifs, featuring extended ether-linked spacers, with a focus on their efficacy against pathogens bearing constitutive erm gene resistance. Optimized compounds 17a and 31f not only reinstated efficacy against inducibly resistant pathogens but also demonstrated significantly augmented activities against constitutively resistant strains of Streptococcus pneumoniae and Streptococcus pyogenes, which are typically refractory to existing C-3 modified macrolides. Notably, hybrid 31f (coded ZN-51) represented a pioneering class of agents distinguished by its dual modes of action, with ribosomes as the primary target and topoisomerases as the secondary target. As a novel chemotype of macrolide-quinolone hybrids, alkylide 31f is a valuable addition to our armamentarium against macrolide-resistant bacteria.

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醚键烷基化合物的设计和结构-活性关系：3-O-descladinosyl 大环内酯与喹诺酮基团的混合物。

TE-802 等酮苷类化合物（3-酮基）和 TEA0929 等酰基类化合物（3-O-酰基）对携带红霉素核糖体甲基化（erm）基因的组成型耐药性病原体无效。继之前关于烷基化物（3-O-烷基）的研究之后，我们探索了 3-去甲萘基红霉素与 6/7-quinolone 基团（R/S）杂交化合物的结构-活性关系，这些杂交化合物具有延长的醚键间隔，重点研究了它们对带有组成型 erm 基因抗性的病原体的疗效。优化后的化合物 17a 和 31f 不仅恢复了对诱导性耐药病原体的疗效，而且还显著增强了对组成型耐药肺炎链球菌和化脓性链球菌菌株的活性，这些菌株通常对现有的 C-3 改性大环内酯类药物难于耐受。值得注意的是，杂交种 31f（代号 ZN-51）是一类具有双重作用模式的先锋药物，其主要作用靶点是核糖体，次要作用靶点是拓扑异构酶。作为大环内酯-喹诺酮类杂交化合物的一种新型化学类型，烷基化物 31f 是我们对付大环内酯类耐药细菌的一个重要补充。

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来源期刊

Bioorganic Chemistry 生物-生化与分子生物学

CiteScore

9.70

自引率

3.90%

发文量

679

审稿时长

31 days

期刊介绍： Bioorganic Chemistry publishes research that addresses biological questions at the molecular level, using organic chemistry and principles of physical organic chemistry. The scope of the journal covers a range of topics at the organic chemistry-biology interface, including: enzyme catalysis, biotransformation and enzyme inhibition; nucleic acids chemistry; medicinal chemistry; natural product chemistry, natural product synthesis and natural product biosynthesis; antimicrobial agents; lipid and peptide chemistry; biophysical chemistry; biological probes; bio-orthogonal chemistry and biomimetic chemistry. For manuscripts dealing with synthetic bioactive compounds, the Journal requires that the molecular target of the compounds described must be known, and must be demonstrated experimentally in the manuscript. For studies involving natural products, if the molecular target is unknown, some data beyond simple cell-based toxicity studies to provide insight into the mechanism of action is required. Studies supported by molecular docking are welcome, but must be supported by experimental data. The Journal does not consider manuscripts that are purely theoretical or computational in nature. The Journal publishes regular articles, short communications and reviews. Reviews are normally invited by Editors or Editorial Board members. Authors of unsolicited reviews should first contact an Editor or Editorial Board member to determine whether the proposed article is within the scope of the Journal.