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脑内化疗:顺铂的慢性微量输注。

Intracerebral chemotherapy: chronic microinfusion of cisplatin.

作者信息

Kroin J S, Penn R D

出版信息

Neurosurgery. 1982 Mar;10(3):349-54. doi: 10.1227/00006123-198203000-00009.

Abstract

Cisplatin, a chemotherapeutic agent used to treat tumors in many parts of the body, does not reach brain tissue during systemic injection because of the blood-brain barrier and protein binding in the blood. To allow hydrophilic drugs, such as cisplatin, to reach brain neoplasms with minimal body toxicity, we tested chronic intracerebral microperfusion into the extracellular space of the brain in normal rats. Small stainless steel cannulas connected to osmotic minipumps were stereotactically placed in the midline cerebellum or frontal cortex, and cisplatin was pumped into the brain at the rate of 0.9 microgram/hour for periods of up to 7 days. Brain tissue was then analyzed for the total platinum content, at 1-mm intervals from the cannula tip, using atomic absorption spectroscopy. The results of the animal studies show that a platinum concentration of 2 ng/mg of tissue, wet weight, can be maintained over a 1-cm region of brain. If all of the extracellular platinum has remained in the active cisplatin form, then this would be equivalent to a drug concentration of 10 microM. Cisplatin at this constant level has been shown to have a therapeutic effect against various tumor lines in vitro. To extend these results to human brain neoplasms, we estimate that one cannula would be sufficient to treat a 1-cm tumor or a larger tumor that could be surgically reduced. For inoperable tumors of up to 2 cm in diameter, a multiple cannula system would be required to yield the 10 microM concentration throughout. For larger inoperable tumors, local infusion will not produce high enough drug levels. In conclusion, chronic intracerebral microinfusion can be used to produce adequate and sustained therapeutic drug levels over a considerable region of tissue without the problem of systemic toxicity.

摘要

顺铂是一种用于治疗身体许多部位肿瘤的化疗药物,在全身注射时由于血脑屏障和血液中的蛋白质结合作用,无法到达脑组织。为了使亲水性药物(如顺铂)能够以最小的身体毒性到达脑肿瘤部位,我们在正常大鼠中测试了向脑外间隙进行慢性脑内微量灌注的方法。将连接到渗透微型泵的小型不锈钢套管立体定向放置在小脑中线或额叶皮质,以0.9微克/小时的速率将顺铂泵入脑内,持续时间长达7天。然后使用原子吸收光谱法,从套管尖端开始,每隔1毫米分析脑组织中的总铂含量。动物研究结果表明,在1厘米的脑区域内可以维持2纳克/毫克组织湿重的铂浓度。如果所有细胞外铂都保持活性顺铂形式,那么这相当于10微摩尔/升的药物浓度。已证明处于这种恒定水平的顺铂在体外对各种肿瘤细胞系具有治疗作用。为了将这些结果推广到人类脑肿瘤,我们估计一根套管足以治疗直径1厘米的肿瘤或通过手术可以缩小的更大肿瘤。对于直径达2厘米的无法手术切除的肿瘤,需要一个多套管系统才能在整个肿瘤区域产生10微摩尔/升的浓度。对于更大的无法手术切除的肿瘤,局部灌注无法产生足够高的药物水平。总之,慢性脑内微量灌注可用于在相当大的组织区域内产生足够且持续的治疗药物水平,而不存在全身毒性问题。

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