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研究药物LM985(黄酮乙酸酯)和LM975(黄酮乙酸)抗癌活性所涉及的因素。

Factors involved in the anti-cancer activity of the investigational agents LM985 (flavone acetic acid ester) and LM975 (flavone acetic acid).

作者信息

Bibby M C, Double J A, Phillips R M, Loadman P M

出版信息

Br J Cancer. 1987 Feb;55(2):159-63. doi: 10.1038/bjc.1987.32.

Abstract

LM985 has been shown previously to hydrolyse to flavone acetic acid (LM975) in mouse plasma and to produce significant anti-tumour effects in transplantable mouse colon tumours (MAC). It has undergone Phase I clinical trials and dose limiting toxicity was acute reversible hypotension. Substantially higher doses of LM975 can be given clinically without dose limiting toxicity. We have investigated the activity of LM975 against a panel of MAC tumours and also the in vitro cytotoxicity of both LM985 and LM975 in two cell lines derived from MAC tumours. LM985 is considerably more cytotoxic than LM975 in vitro but increased length of exposure to LM975 results in improved activity. Single in vivo injection of LM975 showed no activity against the ascitic tumour MAC 15A, moderate activity against the s.c. poorly differentiated tumour MAC 13 and produced a significant growth delay in the well differentiated MAC 26. These latter responses were considerably enhanced by repeated injection 7 days later. Pharmacokinetic studies in mice following i.p. injection of LM985 demonstrated rapid degradation of LM985 to LM975 in the peritoneum. Length of exposure as well as drug concentration appear important factors in determining anti-tumour responses.

摘要

先前已证明,LM985在小鼠血浆中可水解为黄酮乙酸(LM975),并对可移植的小鼠结肠肿瘤(MAC)产生显著的抗肿瘤作用。它已进行了I期临床试验,剂量限制性毒性为急性可逆性低血压。临床上可以给予剂量高得多的LM975而无剂量限制性毒性。我们研究了LM975对一组MAC肿瘤的活性,以及LM985和LM975在源自MAC肿瘤的两种细胞系中的体外细胞毒性。在体外,LM985的细胞毒性比LM975大得多,但延长LM975的暴露时间会提高其活性。LM975单次体内注射对腹水肿瘤MAC 15A无活性,对皮下低分化肿瘤MAC 13有中等活性,并使高分化的MAC 26肿瘤生长显著延迟。7天后重复注射可显著增强后者的反应。腹腔注射LM985后对小鼠进行的药代动力学研究表明,LM985在腹膜内迅速降解为LM975。暴露时间和药物浓度似乎是决定抗肿瘤反应的重要因素。

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