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类视黄醇特异性结合蛋白将类视黄醇特异性摄取到人类早幼粒细胞白血病细胞HL-60中:可能是真正的类视黄醇受体。

Specific uptake of retinoids into human promyelocytic leukemia cells HL-60 by retinoid-specific binding protein: possibly the true retinoid receptor.

作者信息

Hashimoto Y, Kagechika H, Kawachi E, Shudo K

机构信息

Faculty of Pharmaceutical Sciences, University of Tokyo.

出版信息

Jpn J Cancer Res. 1988 Apr;79(4):473-83. doi: 10.1111/j.1349-7006.1988.tb01616.x.

Abstract

The uptake of all-trans-retinoic acid (RA) and two new retinoids [4-(5,6,7,8-tetrahydro-5,5,8,8-tetramethyl-2-naphthalenylcarbamoyl )benzoic acid (Am80) and (E)-4-[3-(3,5-di-tert-butylphenyl)-3-oxo-1-propenyl]benzoic acid (Ch55)] by HL-60 human promyelocytic leukemia cells was investigated. For the investigation, [3H]RA and [3H]Am80 with high specific radioactivities (more than 50 Ci/mmol) were used. [3H]Am80 was prepared by hydrogenolysis of the corresponding chlorinated derivative of Am80 with tritium gas. The retinoids RA, Am80 and Ch55 were efficiently taken up by HL-60 cells, and induced differentiation of the cells into mature granulocytes. The specific bindings (uptake) of RA, Am80 and Ch55 (the bindings inhibited competitively by the other two retinoids) by HL-60 cells were due to a newly detected binding protein. The protein that bound specifically to RA appeared identical to that which bound specifically to Am80 by high-performance liquid chromatography (HPLC), and was named retinoid-specific binding protein (RSBP). One HL-60 cell was found to contain about 1500 molecules of RSBP distributed between the nuclear fraction and cytosolic fraction in proportions of about 4:1. The bindings of the three retinoids (RA, Am80 and Ch55) to RSBP (i.e., formation of retinoid-RSBP complexes) greatly enhanced the affinity of RSBP for the nuclei. The apparent molecular weight of RSBP was estimated to be 95,000 daltons by size exclusion HPLC. The association constants (Ka) of RSBP were calculated to be 2.4 X 10(10) M-1 for RA and 4.4 X 10(10) M-1 for Am80 from Scatchard plots. The bindings of RA, Am80 and Ch55 to RSBP were mutually competitive, indicating that the binding sites for RA, Am80 and Ch55 were identical. The very high affinities of these retinoids for RSBP (Ka's of the order of 10(10) M-1) correspond to the effective concentrations of these retinoids in HL-60 cell culture medium for induction of differentiation of the cells. The mutually competitive bindings of these retinoids strongly support the idea that RSBP is the true receptor of retinoids.

摘要

研究了全反式维甲酸(RA)以及两种新型维甲酸[4-(5,6,7,8-四氢-5,5,8,8-四甲基-2-萘基甲酰基)苯甲酸(Am80)和(E)-4-[3-(3,5-二叔丁基苯基)-3-氧代-1-丙烯基]苯甲酸(Ch55)]被HL-60人早幼粒细胞白血病细胞摄取的情况。为进行该研究,使用了具有高比放射性(超过50 Ci/mmol)的[3H]RA和[3H]Am80。[3H]Am80通过用氚气对Am80相应的氯化衍生物进行氢解制备。维甲酸RA、Am80和Ch55能被HL-60细胞有效摄取,并诱导细胞分化为成熟粒细胞。HL-60细胞对RA、Am80和Ch55的特异性结合(摄取)(这种结合可被另外两种维甲酸竞争性抑制)是由于一种新检测到的结合蛋白。通过高效液相色谱(HPLC)发现,与RA特异性结合的蛋白似乎与与Am80特异性结合的蛋白相同,该蛋白被命名为维甲酸特异性结合蛋白(RSBP)。发现一个HL-60细胞含有约1500个RSBP分子,它们以约4:1的比例分布在核组分和胞质组分之间。这三种维甲酸(RA、Am80和Ch55)与RSBP的结合(即形成维甲酸-RSBP复合物)极大地增强了RSBP对细胞核的亲和力。通过尺寸排阻HPLC估计RSBP的表观分子量为95,000道尔顿。根据Scatchard图计算,RSBP与RA的缔合常数(Ka)为2.4×10(10) M-1,与Am80的缔合常数为4.4×10(10) M-1。RA、Am80和Ch55与RSBP的结合相互竞争,表明RA、Am80和Ch55的结合位点相同。这些维甲酸对RSBP的极高亲和力(Ka约为10(10) M-1)与它们在HL-60细胞培养基中诱导细胞分化的有效浓度相对应。这些维甲酸的相互竞争结合有力地支持了RSBP是维甲酸真正受体的观点。

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