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锌(II)和铜(II)配合物增强了抗菌肽 3 的抗菌活性,但对抗菌肽 1 和 2 的抗菌活性没有增强作用。

Zn(II) and Cu(II) Coordination Enhances the Antimicrobial Activity of Piscidin 3, but Not That of Piscidins 1 and 2.

机构信息

Faculty of Chemistry, University of Wroclaw, ul. F. Joliot-Curie 14, 50-383 Wroclaw, Poland.

Screening of Biological Activity Assays and Collection of Biological Material Laboratory, Wroclaw Medical University Biobank, Faculty of Pharmacy, Wroclaw Medical University, ul. Borowska 211a, 50-556 Wroclaw, Poland.

出版信息

Inorg Chem. 2024 Jul 15;63(28):12958-12968. doi: 10.1021/acs.inorgchem.4c01659. Epub 2024 Jul 1.

Abstract

Piscidins, antimicrobial peptides isolated from fish, are potent against a variety of human pathogens; they show minimum inhibitory concentration values comparable to those of commercially used antimicrobials. Piscidins 1 and 2 are generally more effective than piscidin 3 when applied alone; the contrary is observed for their metal complexes: Zn(II) and Cu(II) coordination does not enhance the efficacy of piscidins 1 and 2, while a moderate enhancement is observed for piscidin 3. All three piscidins bind Cu(II) in a so-called albumin-like binding mode, while for Zn(II) complexes, two coordination modes are observed: piscidins 1 and 2 bind Zn(II) by imidazole nitrogens from His4, His11, and His17 side chains; piscidin 3 coordinates Zn(II) by His3, His4, and His11 imidazole nitrogens and additionally supports the interaction, formed by carbonyl oxygen from His4. Most likely, the high antimicrobial activity of piscidin complexes is due to neither the stability of their complexes nor the change in their secondary structure. Copper(II) complexes with piscidins 1 and 2 can form hydroxyl radicals, which could be responsible for the antimicrobial membrane damaging activity of these complexes. Clearly, a different mechanism (most likely an intercellular targeted one) is observed for piscidin 3 metal complexes; in most cases, the coordination of Cu(II) and Zn(II) enhances the antimicrobial potency of piscidin 3, showing that not only piscidin 3 alone but also its metal complexes have a different mode of action than piscidins 1 and 2.

摘要

从鱼类中分离出的抗菌肽——鱼素,对多种人类病原体具有强大的抑制作用;其最小抑菌浓度值与商业上使用的抗生素相当。单独使用时,鱼素 1 和 2 通常比鱼素 3 更有效;而它们的金属配合物则相反:Zn(II)和 Cu(II)的配位并没有增强鱼素 1 和 2 的功效,而对鱼素 3 则观察到适度的增强。这三种鱼素都以所谓的白蛋白结合模式结合 Cu(II),而对于 Zn(II)配合物,则观察到两种配位模式:鱼素 1 和 2 通过 His4、His11 和 His17 侧链的咪唑氮结合 Zn(II);鱼素 3 通过 His3、His4 和 His11 的咪唑氮结合 Zn(II),并额外支持由 His4 的羰基氧形成的相互作用。很可能,鱼素配合物的高抗菌活性既不是由于其配合物的稳定性,也不是由于其二级结构的变化。鱼素 1 和 2 与铜(II)的配合物可以形成羟基自由基,这可能是这些配合物具有抗菌膜破坏活性的原因。显然,鱼素 3 金属配合物观察到不同的机制(很可能是细胞内靶向机制);在大多数情况下,Cu(II)和 Zn(II)的配位增强了鱼素 3 的抗菌效力,表明不仅是鱼素 3 本身,而且其金属配合物的作用模式与鱼素 1 和 2 不同。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/459a/11256756/92af5b1e5280/ic4c01659_0001.jpg

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