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The metallobiochemistry of ultratrace levels of platinum group elements in the rat

机译:大鼠体内痕量铂族元素超痕量的金属叶化学

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The use of platinum, palladium and rhodium (Platinum Group Elements - PGEs) and the possibility of exposure to their ultratrace levels is increasing. In fact, the exponential development of metallic PGE-based nanoparticles (<100 nm in size) opens extraordinary perspectives in the areas of electrocatalysts and catalytic converters, magnetic nanopowders, polymer membranes, cancer therapy, coatings, plastics, nanofibres and textiles. Like other metal-based nanoparticles, exposure to PGEs nanoparticles may result in a release of ultratrace amounts of Pt, Pd, Rh ions in the body whose metabolic fate and toxicity still need to be evaluated. Furthermore, PGEs can act as allergic sensitizers by acting as haptens and inducing both type I and IV allergic reactions. In this work we studied the in vivo metabolic patterns of ultratrace levels of potent allergens and sensitizers PGE halogenated salts. Pt-191, Pd-103 and Rh-101m radioisotopes were prepared via cyclotron irradiation and used for radiolabelling (Na2PtCl4)-Pt-191, (Na2PdCl4)-Pd-103 and (Na2RhCl6)-Rh-101m salts. These anionic chlorocomplexes were intraperitoneally injected into rats (114 ng Pt kg(-1) bodyweight; 24 ng Pd kg(-1) b.w.; 16 ng Rh kg(-1) b.w.). At 16 h post-exposure, PGEs were poorly but significantly retained in all tissues analysed. Kidneys, spleen, adrenal gland, liver, pancreas and small intestine were the organs with the highest Pt, Pd, Rh concentrations. In the blood 30-35% of Pd-103 and Pt-191 and 10% of (101)mRh were recovered in the plasma, mainly bound to albumin and to a less extent to transferrin. The hepatic and renal intracellular distribution showed the highest recovery of Pt-191, Pd-103 and (101)mRh in the nuclear fraction (liver) and in the cytosol (kidney). Chromatographic separation and ultrafiltration experiments on kidney and liver cytosols showed the strong ability of biochemical macromolecules to bind Pt-191, Pd-103 and (101)mRh, and being responsible for the retention of the three elements in the body. The link to macromolecules is the basis for the sensitizing capacity of PGEs.
机译:铂,钯和铑(铂族元素-PGEs)的使用以及暴露于其超痕量水平的可能性正在增加。实际上,基于金属PGE的纳米颗粒(尺寸小于100 nm)的指数化发展为电催化剂和催化转化器,磁性纳米粉,聚合物膜,癌症治疗,涂料,塑料,纳米纤维和纺织品等领域开辟了非凡的前景。像其他基于金属的纳米粒子一样,暴露于PGEs纳米粒子可能会导致人体中痕量Pt,Pd,Rh离子释放超痕量,其代谢命运和毒性仍需要评估。此外,PGE可通过充当半抗原并诱导I型和IV型过敏反应而充当过敏性敏化剂。在这项工作中,我们研究了强效过敏原和敏化剂PGE卤化盐超痕量水平的体内代谢模式。通过回旋辐射制备Pt-191,Pd-103和Rh-101m放射性同位素,并将其用于放射性标记(Na2PtCl4)-Pt-191,(Na2PdCl4)-Pd-103和(Na2RhCl6)-Rh-101m盐。将这些阴离子氯配合物腹膜内注射到大鼠体内(体重114 ng Pt kg(-1);体重24 ng Pd kg(-1);体重16 ng Rh kg(-1))。暴露后16 h,PGEs较差,但在所有分析的组织中均明显保留。肾脏,脾脏,肾上腺,肝脏,胰腺和小肠是Pt,Pd,Rh浓度最高的器官。在血液中,血浆中回收了30-35%的Pd-103和Pt-191和10%的(101)mRh,主要结合白蛋白,但很少结合转铁蛋白。肝和肾细胞内分布显示核部分(肝)和细胞质(肾脏)中Pt-191,Pd-103和(101)mRh的回收率最高。肾脏和肝脏细胞质的色谱分离和超滤实验表明,生化大分子具有强大的结合Pt-191,Pd-103和(101)mRh的能力,并负责将这三种元素保留在体内。与大分子的联系是PGE敏化能力的基础。

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