125I-碘-α-甲基-L-酪氨酸在结肠癌细胞 DLD-1 中的摄取：天然氨基酸和氨基酸类似物药物的特征及抑制作用。

Uptake of 3-[125I]iodo-alpha-methyl-L-tyrosine into colon cancer DLD-1 cells: characterization and inhibitory effect of natural amino acids and amino acid-like drugs.

机构信息

Department of Radiological Sciences, Ibaraki Prefectural University of Health Sciences, Ami-machi, Inashiki-gun, Ibaraki 300-0394, Japan.

出版信息

Nucl Med Biol. 2010 Feb;37(2):197-204. doi: 10.1016/j.nucmedbio.2009.10.011. Epub 2009 Nov 26.

DOI:10.1016/j.nucmedbio.2009.10.011

PMID:20152719

Abstract

INTRODUCTION

We examined 3-[(123)I]iodo-alpha-methyl-L-tyrosine ([(123)I]IMT) uptake and inhibition by amino acids and amino acid-like drugs in the human DLD-1 colon cancer cell line, to discuss correlation between the inhibition effect and structure.

METHODS

Expression of relevant neutral amino acid transporters was examined by real-time PCR with DLD-1 cells. The time course of [(125)I]IMT uptake, contributions of transport systems, concentration dependence and inhibition effects by amino acids and amino acid-like drugs (1 mM) on [(125)I]IMT uptake were examined.

RESULTS

Expression of system L (4F2hc, LAT1 and LAT2), system A (ATA1, ATA2) and system ASC (ASCT1) was strongly detected; system L (LAT3, LAT4) and MCT8 were weakly detected; and B(0)AT was not detected. [(125)I]IMT uptake in DLD-1 cells involved Na(+)-independent system L primarily and Na(+)-dependent system(s). Uptake of [(125)I]IMT in Na(+)-free buffer followed Michaelis-Menten kinetics, with a K(m) of 78 microM and V(max) of 333 pmol/10(6) cells per minute. Neutral D- and L-amino acids with branched or aromatic large side chains inhibited [(125)I]IMT uptake. Tyrosine analogues, tryptophan analogues, L-phenylalanine and p-halogeno-L-phenylalanines, and gamma amino acids [including 3,4-dihydroxy-L-phenylalanine (L-DOPA), DL-threo-beta-(3,4-dihydroxyphenyl)serine (DOPS), 4-[bis(2-chloroethyl)amino]-L-phenylalanine and 1-(aminomethyl)-cyclohexaneacetic acid] strongly inhibited [(125)I]IMT uptake, but L-tyrosine methyl ester and R(+)/S(-)-baclofen weakly inhibited uptake. The substrates of system ASC and A did not inhibit [(125)I]IMT uptake except L-serine and D/L-cysteine.

CONCLUSIONS

[(125)I]IMT uptake in DLD-1 cells involves mostly LAT1 and its substrates' (including amino acid-like drugs derived from tyrosine, tryptophan and phenylalanine) affinity to transport via LAT1. Whether transport of gamma amino acid analogues is involved in LAT1 depends on the structure of the group corresponding to the amino acid residue. Beta-hydroxylation may confer reduction of transport affinity of tyrosine analogues via LAT1.

摘要

简介

我们研究了 3-[(123)I]碘-α-甲基-L-酪氨酸 ([(123)I]IMT) 在人 DLD-1 结肠癌细胞系中的摄取和被氨基酸和氨基酸样药物抑制的情况，以讨论抑制作用与结构之间的关系。

方法

通过实时 PCR 检测 DLD-1 细胞中相关中性氨基酸转运体的表达。研究了 [(125)I]IMT 摄取的时间过程、转运系统的贡献、浓度依赖性以及氨基酸和氨基酸样药物 (1 mM) 对 [(125)I]IMT 摄取的抑制作用。

结果

强烈检测到系统 L (4F2hc、LAT1 和 LAT2)、系统 A (ATA1、ATA2) 和系统 ASC (ASCT1) 的表达；系统 L (LAT3、LAT4) 和 MCT8 的表达较弱；B(0)AT 则没有检测到。DLD-1 细胞中的 [(125)I]IMT 摄取主要涉及不依赖于 Na(+)的系统 L 和依赖于 Na(+)的系统。在无 Na(+)缓冲液中，[(125)I]IMT 的摄取遵循米氏动力学，K(m)为 78 μM，V(max)为 333 pmol/10(6)个细胞/分钟。具有支链或芳香大侧链的中性 D-和 L-氨基酸抑制 [(125)I]IMT 的摄取。酪氨酸类似物、色氨酸类似物、L-苯丙氨酸和对卤代-L-苯丙氨酸以及γ-氨基酸[包括 3,4-二羟基-L-苯丙氨酸 (L-DOPA)、DL-苏氨酸-β-(3,4-二羟基苯基)丝氨酸 (DOPS)、4-[双(2-氯乙基)氨基]-L-苯丙氨酸和 1-(氨甲基)-环己烷乙酸]强烈抑制 [(125)I]IMT 的摄取，但 L-酪氨酸甲酯和 R(+)/S(-)-巴氯芬则较弱。除 L-丝氨酸和 D/L-半胱氨酸外，ASC 和 A 的底物不抑制 [(125)I]IMT 的摄取。

结论

DLD-1 细胞中的 [(125)I]IMT 摄取主要涉及 LAT1 及其底物（包括来自酪氨酸、色氨酸和苯丙氨酸的氨基酸样药物）通过 LAT1 的亲和力进行转运。γ-氨基酸类似物的转运是否涉及 LAT1 取决于与氨基酸残基相对应的基团的结构。β-羟化作用可能降低 LAT1 对酪氨酸类似物的转运亲和力。