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Influence on antiproliferative activity of structural modification and conjugation of gonadotropin‐releasing hormone (GnRH) analogues

机译:促性腺激素释放激素(GnRH)类似物对结构修饰和缀合的抗增殖活性的影响

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摘要

The effect of various GnRH analogues, and their conjugates on proliferation, clonogenicity and cell cycle phase distribution of MCF‐7 and Ishikawa human cancer cell lines was studied. GnRH‐III, a sea lamprey GnRH analogue reduced cell proliferation by 35% and clonogenicity by 55%. Structural modifications either decreased, or did not alter biological activity. Conjugation of GnRH analogues including MI‐1544, MI‐1892, and GnRH‐III with poly(N‐vinylpyrrolidone‐co‐maleic acid) (P) through a tetrapeptide spacer GFLG(X) substantially increased the inhibitory effect of the GnRH analogues. The conjugate P‐X‐GnRH‐III induced significant accumulation of cells in the G2/M phase; from 8% to 15.6% at 24 h and 9.8% to 15% at 48 h. It was concluded that conjugation of various GnRH analogues substantially enhanced their antiproliferative activity, strongly reduced cell clonogenicity and retarded cell progression through the cell division cycle at the G2/M phase.
机译:研究了各种GnRH类似物及其结合物对MCF-7和Ishikawa人类癌细胞系增殖,克隆形成和细胞周期阶段分布的影响。 GnRH-III,一种海七rey的GnRH类似物,可使细胞增殖降低35%,成克隆性降低55%。结构修饰要么降低,要么不改变生物活性。通过四肽间隔子GFLG(X)将GnRH类似物(包括MI-1544,MI-1892和GnRH-III)与聚(N-乙烯基吡咯烷酮-马来酸)(P)结合,可大大提高GnRH类似物的抑制作用。结合物P‐X‐GnRH‐III诱导了G2 / M期细胞的大量积聚;从24小时的8%降至15.6%和在48小时的9.8%至15%。结论是,各种GnRH类似物的结合显着增强了它们的抗增殖活性,大大降低了细胞的克隆形成性,并通过了G2 / M期的细胞分裂周期阻碍了细胞的进程。

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