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锝-99m 甲氧基异丁基异腈在显示谷胱甘肽相关耐药性的人乳腺癌细胞系中的摄取。

Technetium-99m sestamibi uptake in human breast carcinoma cell lines displaying glutathione-associated drug-resistance.

作者信息

Kabasakal L, Ozker K, Hayward M, Akansel G, Griffith O, Isitman A T, Hellman R, Collier D

机构信息

Department of Nuclear Medicine and Biochemistry, Medical College of Wisconsin, Milwaukee, USA.

出版信息

Eur J Nucl Med. 1996 May;23(5):568-70. doi: 10.1007/BF00833393.

Abstract

An in vitro study was designed to evaluate the uptake of sestamibi (MIBI) in P-glycoprotein (Pgp) and glutathione-associated (GSH) multidrug-resistant (MDR) cell lines. MIBI uptake was studied in various human breast carcinoma cell lines, i.e. in wild-type (MCF7/wt) cells, in adriamycin-resistant (MCF7/adr) cells which express Pgp and in melphalan-resistant (MCF7/mph) cells with increased levels of GSH. The effects of buthiomine sulphoximine (BSO) and verapamil on MIBI uptake were also studied in the MCF7/mph and MCF7/adr cells respectively. The cells were incubated for 1 h with a dose of 0.1 MBq thallium-201 and technetium-99m MIBI. Both MIBI and 201Tl uptakes were higher for MCF7/mph cells than for the other cells studied. The mean MIBI uptake in MCF7/adr cells was significantly lower than that in MCF7/wt cells (1.9%+/-0.5% vs 3. 1%.0.6%; P <0.01). Verapamil treatment increased the MIBI uptake in MCF7/adr cells (to 2.6%.0.3%; P <0.05). Treatment of MCF7/mph cells with BSO resulted in a significant reduction in GSH content (from 243.2+/-81.1 nmol/mg protein to 17.6+/-4.4 nmol/mg protein; P <0. 001). However, MIBI uptake in BSO-treated and untreated MCF7/mph cells was similar (4.43%+/-0.5% and 5.93%+/-1.7%, respectively; P >0. 1). This study suggests that the uptake of MIBI is not diminished by glutathione-associated drug resistance and that MIBI uptake in a tumour sample does not necessarily indicate that a cancer is sensitive to drugs.

摘要

设计了一项体外研究,以评估司他莫司(MIBI)在P - 糖蛋白(Pgp)和谷胱甘肽相关(GSH)多药耐药(MDR)细胞系中的摄取情况。在各种人乳腺癌细胞系中研究了MIBI摄取,即野生型(MCF7/wt)细胞、表达Pgp的阿霉素耐药(MCF7/adr)细胞和谷胱甘肽水平升高的美法仑耐药(MCF7/mph)细胞。还分别在MCF7/mph和MCF7/adr细胞中研究了丁硫氨酸亚砜胺(BSO)和维拉帕米对MIBI摄取的影响。将细胞与剂量为0.1 MBq的铊 - 201和锝 - 99m MIBI孵育1小时。MCF7/mph细胞的MIBI和201Tl摄取均高于所研究的其他细胞。MCF7/adr细胞中的平均MIBI摄取显著低于MCF7/wt细胞(1.9%±0.5%对3.1%±0.6%;P<0.01)。维拉帕米处理增加了MCF7/adr细胞中的MIBI摄取(至2.6%±0.3%;P<0.05)。用BSO处理MCF7/mph细胞导致谷胱甘肽含量显著降低(从243.2±81.1 nmol/mg蛋白质降至17.6±4.4 nmol/mg蛋白质;P<0.001)。然而,BSO处理和未处理的MCF7/mph细胞中的MIBI摄取相似(分别为4.43%±0.5%和5.93%±1.7%;P>0.1)。这项研究表明,谷胱甘肽相关的耐药性不会降低MIBI的摄取,并且肿瘤样本中的MIBI摄取不一定表明癌症对药物敏感。

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