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首页> 外文期刊>Dalton transactions: An international journal of inorganic chemistry >Technetium-99m complexes of L-arginine derivatives for targeting amino acid transporters
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Technetium-99m complexes of L-arginine derivatives for targeting amino acid transporters

机译:用于靶向氨基酸转运蛋白的L-精氨酸衍生物的Technetium-99m络合物

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摘要

Although relevant from the clinical point of view, radiotracers targeting cationic amino acid transporters are relatively unexplored and, in particular, no metal-based radiotracers are known. The rare examples of complexes recognized by amino acid transporters, namely by the Na+-independent neutral L-type amino acid transporter 1 (LAT1), are Tc-99m(I)/Re(I) compounds. Herein, we describe conjugates comprising a pyrazolyl-diamine chelating unit and the cationic amino acid L-arginine (L-Arg) linked by a propyl (L-1) or hexyl linker (L-2),which allowed the preparation of stable complexes of the type fac-[Tc-99m(CO) 3(k(3)-L)]+ (Tc1, L = L-1; Tc2, L = L-2) and of the respective surrogates Re1 and Re2. Interestingly, complex Tc2 exhibited moderate levels of time-dependent internalization in three human tumoural cell lines, with approximately 3% of total applied activity internalized, corresponding to 21% of the cell-associated activity. A putative mechanism of retention in the cytoplasm of cells could be the interaction of the complex with inducible nitric oxide synthase (iNOS), which is the enzyme responsible for the catalytic oxidation of L-Arg to citrulline and nitric oxide. However, the surrogate complex Re2 does not recognize iNOS, as demonstrated by the in vitro assays with purified iNOS and in studies with lipopolysaccharide(LPS)-activated macrophages. Preliminary mechanistic studies suggest that the internalization of Tc2 is linked to the cationic amino acid transporters, namely system y(+). This finding might open the way towards the development of novel families of metal-based radiotracers for probing metabolically active cancer cells.
机译:虽然与临床观点相关,但靶向阳离子氨基酸转运蛋白的放射性反射体相对未探测,特别是没有已知金属基质的放射体制物。氨基酸转运蛋白识别的络合物的罕见实例,即由Na + -Indepentent中性L型氨基酸转运蛋白1(LAT1)是TC-99M(I)/ Re(I)化合物。在此,我们描述包含通过丙基(L-1)或己基接头(L-2)连接的吡唑基 - 二胺螯合单元和阳离子氨基酸L-精氨酸(L-ARG),其允许制备稳定的配合物IC-[TC-99M(CO)3(K(3)-L)] +(TC1,L = L-1; TC2,L = L-2)和相应的代理RE1和RE2。有趣的是,复杂的TC2在三种人胎儿细胞系中表现出适度的时间依赖性内化,其中约3%的施加活性的内化,相当于细胞相关活性的21%。在细胞的细胞质中的留住机制可以是复合物与诱导型一氧化氮合酶(InOS)的相互作用,这是负责L-Arg催化氧化至瓜氨酸和一氧化氮的酶。然而,替代复合Re2不识别INO,如体外测定用纯化的InOS和用脂多糖(LPS) - 活化的巨噬细胞的研究证明。初步机械研究表明,TC2的内化与阳离子氨基酸转运蛋白相关,即系统Y(+)。这一发现可能对探测代谢活性癌细胞的金属基质基于基于金属基质的新颖家族的发展可能开辟道路。

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    Univ Lisbon Ctr Ciencias &

    Tecnol Nucl Inst Super Tecn Estr Nacl 10 Km 139-7 P-2695066 Bobadela Lrs Portugal;

    Univ Lisbon Ctr Ciencias &

    Tecnol Nucl Inst Super Tecn Estr Nacl 10 Km 139-7 P-2695066 Bobadela Lrs Portugal;

    Univ Lisbon Ctr Ciencias &

    Tecnol Nucl Inst Super Tecn Estr Nacl 10 Km 139-7 P-2695066 Bobadela Lrs Portugal;

    Univ Lisbon Ctr Ciencias &

    Tecnol Nucl Inst Super Tecn Estr Nacl 10 Km 139-7 P-2695066 Bobadela Lrs Portugal;

    Univ Lisbon Ctr Ciencias &

    Tecnol Nucl Inst Super Tecn Estr Nacl 10 Km 139-7 P-2695066 Bobadela Lrs Portugal;

    Univ Lisbon Ctr Ciencias &

    Tecnol Nucl Inst Super Tecn Estr Nacl 10 Km 139-7 P-2695066 Bobadela Lrs Portugal;

    Univ Lisbon Ctr Ciencias &

    Tecnol Nucl Inst Super Tecn Estr Nacl 10 Km 139-7 P-2695066 Bobadela Lrs Portugal;

    Univ Lisbon Ctr Ciencias &

    Tecnol Nucl Inst Super Tecn Estr Nacl 10 Km 139-7 P-2695066 Bobadela Lrs Portugal;

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  • 正文语种 eng
  • 中图分类 化学 ; 无机化学 ;
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