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利用HTSCA和CFU-C检测法鉴定出两种新的氨基酸酰胺类2-氯乙基亚硝脲同系物,与卡莫司汀相比,它们对人胶质瘤的体外活性有所增强。

Utilization of the HTSCA and CFU-C assay to identify two new 2-chloroethylnitrosourea congeners of amino acid amides with increased in vitro activity against human glioma compared with BCNU.

作者信息

Panasci L C, Dufour M, Chevalier L, Isabel G, Lazarus P, McQuillan A, Arbit E, Brem S, Feindel W

出版信息

Cancer Chemother Pharmacol. 1985;14(2):156-9. doi: 10.1007/BF00434356.

Abstract

AspCNU and SarCNU are two amino acid amide congeners (L-asparaginamide and sarcosinamide congeners) of chloroethylnitrosoureas. The in vitro myelotoxicity of these agents compared with BCNU at 1-8 micrograms/ml was determined in bone marrow cells from normal volunteers in the CFU-C assay. AspCNU and SarCNU were significantly (P less than 0.05) less myelotoxic than BCNU at equivalent microgram concentrations. SarCNU or AspCNU at 3 micrograms/ml demonstrate equivalent in vitro myelotoxicity to BCNU 1 microgram/ml. We used the human tumor stem cell assay (HTSCA) to investigate in vitro antitumor activity. We obtained four specimens of malignant glioma and one specimen of meningioma from patients not previously treated with chemotherapy. AspCNU and SarCNU were significantly (P less than 0.05) more active than BCNU at 1-3 micrograms/ml concentrations in the HTSCA in all four malignant glioma specimens. In the one meningioma specimen, BCNU was significantly (P less than 0.05) more active than either AspCNU or SarCNU at all concentrations studied. These results suggest that AspCNU or SarCNU at doses that should produce less myelotoxicity than BCNU may be more active than BCNU against gliomas.

摘要

天冬氨酸氮芥(AspCNU)和肌氨酸氮芥(SarCNU)是氯乙基亚硝脲的两种氨基酸酰胺类似物(L-天冬酰胺和肌氨酸酰胺类似物)。在CFU-C试验中,在正常志愿者的骨髓细胞中测定了这些药物在1-8微克/毫升浓度下与卡莫司汀(BCNU)相比的体外骨髓毒性。在等效微克浓度下,AspCNU和SarCNU的骨髓毒性明显低于BCNU(P<0.05)。3微克/毫升的SarCNU或AspCNU表现出与1微克/毫升的BCNU等效的体外骨髓毒性。我们使用人肿瘤干细胞试验(HTSCA)来研究体外抗肿瘤活性。我们从未接受过化疗的患者身上获得了4份恶性胶质瘤标本和1份脑膜瘤标本。在所有4份恶性胶质瘤标本中,在HTSCA中,1-3微克/毫升浓度的AspCNU和SarCNU比BCNU活性明显更高(P<0.05)。在1份脑膜瘤标本中,在所有研究浓度下,BCNU比AspCNU或SarCNU活性明显更高(P<0.05)。这些结果表明,与BCNU相比,AspCNU或SarCNU在产生更低骨髓毒性的剂量下对胶质瘤的活性可能更高。

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