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通过包入离子交换微球降低阿霉素的毒性:一项使用大鼠肝肿瘤模型的治疗研究。

Reduced toxicity of adriamycin by incorporation into ion exchange microspheres: a therapeutic study using a rat liver tumour model.

作者信息

Codde J P, Burton M A, Kelleher D K, Archer S G, Gray B N

机构信息

University Department of Surgery, Royal Perth Hospital, Western Australia.

出版信息

Anticancer Res. 1990 Nov-Dec;10(6):1715-8.

PMID:2285247
Abstract

A comparison of the systemic toxicity and therapeutic efficacy of adriamycin carrying microspheres with conventional chemotherapeutic use of adriamycin was performed using a rat liver tumour model. The drug-microspheres were administered via the gastro-duodenal artery for delivery to the liver, whilst similar quantities of free adriamycin were given by systemic intravenous or regional intra-arterial routes. Significant leukopenia, thrombocytopenia and mortality were observed in the systemically treated free drug group (P less than 0.05) with a similar trend for for myelosuppression occurring in the intra-arterial free drug group. The adriamycin-microsphere group showed no toxic side-effects despite retarding tumour growth by similar amounts to the other drug modalities. This work demonstrates a large potential for the use of adriamycin carrying ion-exchange microspheres in the treatment of human malignancy.

摘要

使用大鼠肝肿瘤模型,对携带阿霉素的微球与阿霉素常规化疗应用的全身毒性和治疗效果进行了比较。药物微球通过胃十二指肠动脉给药以输送至肝脏,同时通过全身静脉或局部动脉途径给予等量的游离阿霉素。全身治疗的游离药物组观察到显著的白细胞减少、血小板减少和死亡率(P小于0.05),动脉内游离药物组也出现了类似的骨髓抑制趋势。阿霉素微球组尽管肿瘤生长的延缓程度与其他药物方式相似,但未显示出毒副作用。这项研究表明携带阿霉素的离子交换微球在治疗人类恶性肿瘤方面具有巨大潜力。

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