Synthetic nucleosides and nucleotides. 43. Inhibition of vertebrate telomerases by carbocyclic oxetanocin g (C.OXT-G) triphosphate analogues and influence of C.OXT-G treatment on telomere length in human HL60 cells.

Yamaguchi T; Saneyoshi M; Takahashi H; Hirokawa S; Amano R; Liu X; Inomata M; Maruyama T

首页> 外文期刊>Nucleosides, nucleotides and nucleic acids >Synthetic nucleosides and nucleotides. 43. Inhibition of vertebrate telomerases by carbocyclic oxetanocin g (C.OXT-G) triphosphate analogues and influence of C.OXT-G treatment on telomere length in human HL60 cells.

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Synthetic nucleosides and nucleotides. 43. Inhibition of vertebrate telomerases by carbocyclic oxetanocin g (C.OXT-G) triphosphate analogues and influence of C.OXT-G treatment on telomere length in human HL60 cells.

机译：合成核苷和核苷酸。 43.碳环氧etanocin g（C.OXT-G）三磷酸类似物对脊椎动物端粒酶的抑制作用以及C.OXT-G处理对人HL60细胞端粒长度的影响。

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Telomerase, responsible for telomere synthesis, is expressed in approximately 90% of human tumor cells but seldom in normal somatic cells. In this study, inhibition by carbocyclic oxetanocin G triphosphate (C. OXT-GTP) and its analogues was investigated in order to clarify the susceptibility of telomerase to various nucleotide analogues. C. OXT-GTP competitively inhibited telomerase activity with respect to dGTP However, C. OXT-GTP had a potent inhibitory effect on DNA polymerase alpha. It was examined whether the nucleoside (C. OXT-G) was able to alter telomere length in cultured human HL60 cells. Contrary to expectation, long-term treatment with 10 microM C. OXT-G was found to cause telomere lengthening.

机译：负责端粒合成的端粒酶在约90％的人类肿瘤细胞中表达，但在正常的体细胞中很少表达。在这项研究中，为了阐明端粒酶对各种核苷酸类似物的敏感性，研究了碳环氧杂环丁烷三磷酸G（C. OXT-GTP）及其类似物的抑制作用。 C.OXT-GTP相对于dGTP竞争性地抑制了端粒酶的活性。但是，C.OXT-GTP对DNA聚合酶α具有有效的抑制作用。检查了核苷（C. OXT-G）是否能够改变培养的人HL60细胞的端粒长度。与预期相反，发现用10 microM C. OXT-G长期治疗可导致端粒延长。

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《Nucleosides, nucleotides and nucleic acids》 |2006年第6期|共13页
作者
Yamaguchi T; Saneyoshi M; Takahashi H; Hirokawa S; Amano R; Liu X; Inomata M; Maruyama T;
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正文语种 eng
中图分类基础医学;
关键词
Carbon ion; oxetanocin G; Telomere; Human; Length; 端粒;

机译：碳离子;氧杂环丁菌素G;端粒;人类;长度;端粒;

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1. Synthetic nucleosides and nucleotides. 43. Inhibition of vertebrate telomerases by carbocyclic oxetanocin g (C.OXT-G) triphosphate analogues and influence of C.OXT-G treatment on telomere length in human HL60 cells. [J] . Yamaguchi T, Saneyoshi M, Takahashi H, Nucleosides, nucleotides and nucleic acids . 2006,第4a6期

机译：合成核苷和核苷酸。 43.碳环氧etanocin g（C.OXT-G）三磷酸类似物对脊椎动物端粒酶的抑制作用以及C.OXT-G处理对人HL60细胞端粒长度的影响。
2. 3 '-Azido-2 ',3 '-dideoxynucleoside 5 '-triphosphates inhibit telomerase activity in vitro, and the corresponding nucleosides cause telomere shortening in human HL60 cells [J] . Liu XH, Takahashi H, Harada Y, Nucleic Acids Research . 2007,第21期

机译：3'-Azido-2'，3'-二脱氧核苷5'-三磷酸在体外抑制端粒酶活性，相应的核苷导致人HL60细胞端粒缩短
3. 3′-Azido-2′,3′-dideoxynucleoside 5′-triphosphates inhibit telomerase activity in vitro, and the corresponding nucleosides cause telomere shortening in human HL60 cells [J] . Hazuki Takahashi, Mineo Saneyoshi, Toyofumi Yamaguchi, Nucleic acids research . 2007,第21期

机译：3'-azido-2'，3'-二脱氧核苷5'-三磷酸抑制体外端粒酶活性，相应的核苷导致人HL60细胞中的端粒缩短
4. 3′-Azido-2′3′-dideoxynucleoside 5′-triphosphates inhibit telomerase activity in vitro and the corresponding nucleosides cause telomere shortening in human HL60 cells [O] . Xiaohong Liu, Hazuki Takahashi, Yoko Harada, 2007

机译：3-叠氮基-23-二脱氧核苷5-三磷酸在体外抑制端粒酶活性相应的核苷导致人HL60细胞端粒缩短
5. 3′-Azido-2′,3′-dideoxynucleoside 5′-triphosphates inhibit telomerase activity in vitro, and the corresponding nucleosides cause telomere shortening in human HL60 cells [O] . Liu, Xiaohong, Takahashi, Hazuki, Harada, Yoko, 2007

机译：3'-叠氮基-2'，3'-双脱氧核苷5'-三磷酸在体外抑制端粒酶活性，相应的核苷导致人HL60细胞端粒缩短

Synthetic nucleosides and nucleotides. 43. Inhibition of vertebrate telomerases by carbocyclic oxetanocin g (C.OXT-G) triphosphate analogues and influence of C.OXT-G treatment on telomere length in human HL60 cells.

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