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BNP7787是一种新型的铂类相关毒性防护剂,在人肿瘤异种移植模型中不影响顺铂或卡铂的疗效。

BNP7787, a novel protector against platinum-related toxicities, does not affect the efficacy of cisplatin or carboplatin in human tumour xenografts.

作者信息

Boven E, Verschraagen M, Hulscher T M, Erkelens C A M, Hausheer F H, Pinedo H M, van der Vijgh W J F

机构信息

Department of Medical Oncology, Vrije Universiteit Medical Centre, De Boelelaan 1117, Amsterdam, The Netherlands.

出版信息

Eur J Cancer. 2002 May;38(8):1148-56. doi: 10.1016/s0959-8049(02)00036-9.

Abstract

BNP7787 (2',2'-dithio-bis-ethane sulphonate sodium), a water-soluble disulphide, is chemically and mechanistically different from other sulphur-containing chemoprotective agents. Presently, BNP7787 is under investigation for its protective properties with regard to the side-effects of platinum compounds. In this study, we evaluated BNP7787, mesna and amifostine for their effects on the antitumour activity of platinum compounds. Continuous exposure to BNP7787 did not affect the antiproliferative effects of cisplatin or carboplatin, but the efficacy of both compounds was reduced in the presence of mesna in vitro in two human ovarian cancer cell lines. BNP7787 or amifostine combined with cisplatin or carboplatin given in standard schedules for the treatment of nude mice bearing well-established OVCAR-3 xenografts did not interfere with platinum-induced inhibition of tumour growth. Of interest, BNP7787 or amifostine co-administered with carboplatin was significantly more effective than carboplatin alone (P<0.01). In the presence of amifostine, doses of cisplatin and carboplatin could be safely increased by factors of 1.6 and 1.5, respectively. Unlike in a previous study of BNP7787 in tumour-bearing rats, BNP7787 did not protect against additional weight loss following treatment with higher doses of cisplatin in OVCAR-3-bearing mice. Pharmacokinetics of (mixed) disulphides including BNP7787 and extractable mesna in deproteinised plasma revealed a rapid disappearance of BNP7787 and an AUC(5-60) value of mesna 9-fold lower than that calculated after an equivalent dose of mesna by weight. We can conclude that BNP7787 does not interfere with the antitumour activity of platinum compounds in vitro and in vivo. Clinical trials are underway to evaluate the protection of normal tissues by BNP7787 when combined with cisplatin.

摘要

BNP7787(2',2'-二硫代双乙烷磺酸钠)是一种水溶性二硫化物,在化学性质和作用机制上与其他含硫化学保护剂不同。目前,BNP7787正在接受关于其对铂类化合物副作用的保护特性的研究。在本研究中,我们评估了BNP7787、美司钠和氨磷汀对铂类化合物抗肿瘤活性的影响。持续暴露于BNP7787并不影响顺铂或卡铂的抗增殖作用,但在两种人卵巢癌细胞系中,体外存在美司钠时,这两种化合物的疗效均降低。按照治疗已建立的OVCAR-3异种移植裸鼠的标准方案,将BNP7787或氨磷汀与顺铂或卡铂联合使用,并不干扰铂诱导的肿瘤生长抑制。有趣的是,BNP7787或氨磷汀与卡铂联合给药比单独使用卡铂显著更有效(P<0.01)。在存在氨磷汀的情况下,顺铂和卡铂的剂量可分别安全地增加1.6倍和1.5倍。与之前在荷瘤大鼠中对BNP7787的研究不同,在携带OVCAR-3的小鼠中,BNP7787不能预防高剂量顺铂治疗后的额外体重减轻。在脱蛋白血浆中,包括BNP7787和可提取美司钠在内的(混合)二硫化物的药代动力学显示,BNP7787迅速消失,美司钠的AUC(5 - 60)值比按等重量等效剂量美司钠计算的值低9倍。我们可以得出结论,BNP7787在体外和体内均不干扰铂类化合物的抗肿瘤活性。目前正在进行临床试验,以评估BNP7787与顺铂联合使用时对正常组织的保护作用。

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