Abstract

The potential chemotherapeutic properties coupled to photochemical transitions make the family of fac-[Re(CO)₃(N,N)X]^0/+ (N,N = a bidentate diimine such as 2,2′-bipyridine (bpy); X = halide, H₂O, pyridine derivatives, PR₃, etc.) complexes of special interest. We have investigated reactions of the aqua complex fac-[Re(CO)₃(bpy)(H₂O)](CF₃SO₃) (1) with potential anticancer activity with the amino acid l-cysteine (H₂Cys), and its derivative N-acetyl-l-cysteine (H₂NAC), as well as the tripeptide glutathione (H₃A), under physiological conditions (pH 7.4, 37 °C), to model the interaction of 1 with thiol-containing proteins and enzymes, and the impact of such coordination on its photophysical properties and cytotoxicity. We report the syntheses and characterization of fac-[Re(CO)₃(bpy)(HCys)]·0.5H₂O (2), Na(fac-[Re(CO)₃(bpy)(NAC)]) (3), and Na(fac-[Re(CO)₃(bpy)(HA)])·H₂O (4) using extended X-ray absorption spectroscopy, IR and NMR spectroscopy, electrospray ionization spectrometry, as well as the crystal structure of {fac-[Re(CO)₃(bpy)(HCys)]}₄·9H₂O (2 + 1.75 H₂O). The emission spectrum of 1 displays a variance in Stokes shift upon coordination of l-cysteine and N-acetyl-l-cysteine. Laser excitation at λ = 355 nm of methanol solutions of 1–3 was followed by measuring their ability to produce singlet oxygen (¹O₂) using direct detection methods. The cytotoxicity of 1 and its cysteine-bound complex 2 was assessed using the MDA-MB-231 breast cancer cell line, showing that the replacement of the aqua ligand on 1 with l-cysteine significantly reduced the cytotoxicity of the Re(I) tricarbonyl complex. Probing the cellular localization of 1 and 2 using X-ray fluorescence microscopy revealed an accumulation of 1 in the nuclear and/or perinuclear region, whereas the accumulation of 2 was considerably reduced, potentially explaining its reduced cytotoxicity.

Graphic abstract

Replacing the aqua ligand with cysteine in the antitumor active fac-[Re(CO)₃(bpy)(H₂O)](CF₃SO₃) complex significantly reduced its cellular accumulation and cytotoxicity against the MDA-MB-213 breast cancer cell line, shifted its maximum emission to considerably higher energies, and decreased its fluorescence quantum yield.

中文翻译：

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Re（I）三羰基复合物与半胱氨酸及其衍生物结合的细胞毒性，细胞定位和光物理特性。

摘要

与光化学转变相关的潜在化学治疗特性使fac- [Re（CO）₃（N，N）X] ^{0 / +}家族（N，N  =二齿二亚胺，例如2,2'-联吡啶（bpy）; X =卤化物，H ₂ O，吡啶衍生物，PR ₃等）特别重要的配合物。我们已经研究了水族复合物fac- [Re（CO）₃（bpy）（H ₂ O）]（CF ₃ SO ₃）（1）与氨基酸l-半胱氨酸（H ₂ Cys）具有潜在抗癌活性的反应。，及其派生词N-乙酰基-1-半胱氨酸（H ₂ NAC）以及三肽谷胱甘肽（H ₃ A）在生理条件（pH 7.4，37°C）下模拟1与含硫醇的蛋白质和酶的相互作用，以及这种配位对其光物理性质和细胞毒性的影响。我们报道了fac- [Re（CO）₃（bpy）（HCys）]·0.5H ₂ O（2），Na（fac- [Re（CO）₃（bpy）（NAC）]）的合成与表征3）和Na（fac- [Re（CO）₃（bpy）（HA）]）·H ₂ O（4）的扩展X射线吸收光谱，IR和NMR光谱，电喷雾电离光谱以及{ fac- [Re（CO）₃（bpy）（HCys）]} ₄ ·9H ₂ O（2  + 1.75 H ₂ O）。的发射光谱1个显示在根据协调斯托克斯位移方差升-半胱氨酸和Ñ乙酰基升-半胱氨酸。在激光激发λ  = 355的甲醇溶液中的纳米1 - 3，随后通过测量它们，以产生单线态氧的能力（¹ Ò ₂）使用直接检测方法。的细胞毒性1和它的半胱氨酸结合的复合物2用的是MDA-MB-231乳腺癌细胞系进行评估，显示出替代的AQUA配体1与升-半胱氨酸显著降低了Re的细胞毒性（I）三羰基复杂。使用X射线荧光显微镜探测1和2的细胞定位，发现在核和/或核周区域中有1的积累，而2的积累却大大减少了，这可能解释了其细胞毒性的降低。

图形摘要

抗肿瘤活性fac- [Re（CO）₃（bpy）（H ₂ O）]（CF ₃ SO ₃）复合物中的半胱氨酸取代水配体显着降低了其对MDA-MB-213乳腺癌的细胞蓄积和细胞毒性细胞系，将其最大发射转移到更高的能量，并降低了其荧光量子产率。