Chen Johnson, Balmaceda Casilda, Bruce Jeffrey N, Sisti Michael B, Huang May, Cheung Ying Kuen K, McKhann Guy M, Goodman Robert R, Fine Robert L
Experimental Therapeutics Program, Division of Medical Oncology, College of Physicians and Surgeons of Columbia University, New York, NY 10032, USA.
J Neurooncol. 2006 Jan;76(1):85-92. doi: 10.1007/s11060-005-4171-7.
P-glycoprotein (Pgp) mediates, in part, resistance to natural product chemotherapy drugs which constitute over half of the available drugs for cancer treatment. Tamoxifen (TAM) enhances intracellular deposition of natural product chemotherapy in human cell lines by inhibition of Pgp. Pgp is highly expressed in the choroid plexus and is thought to be a key component of the blood-cerebrospinal fluid barrier (BCSFB). We conducted a prospective, randomized study to assess if Pgp inhibition by TAM alters deposition of paclitaxel in cerebrospinal fluid (CSF).
Ten patients with either primary or metastatic brain tumors were randomized to: paclitaxel alone (175 mg/m2/IV) or a course of TAM (160 mg/m2 PO BID on Days 1-5) followed by paclitaxel (175 mg/m2/IV on Day 5). CSF and plasma samples were obtained following paclitaxel infusion; paclitaxel and TAM concentrations were measured by high-performance liquid chromatography assays.
Paclitaxel was detected in the CSF of six of the 10 patients. Peak CSF paclitaxel concentrations of the paclitaxel and paclitaxel-TAM groups ranged between 3.5-57.4 and 2.3-24.6 nM, respectively. Though there was a 2.4-fold higher mean CSF paclitaxel concentration and a 3.7-fold higher median peak CSF:plasma paclitaxel ratio for those who received paclitaxel alone as compared to combined paclitaxel-TAM, it was not statistically significant (P = 0.22). In one patient enrolled to both arms, higher CSF concentrations of paclitaxel and higher paclitaxel CSF: plasma ratios were observed when given paclitaxel alone.
The trend towards lower paclitaxel CSF concentrations when given with TAM is consistent with the published finding that Pgp's localization in the endothelial cells of the choroid plexus works in an opposite direction and keeps drugs in the CSF. Thus, agents which inhibit Pgp, such as TAM, may increase efflux of Pgp substrates out of the BCSFB and may paradoxically lower CSF concentrations of natural product chemotherapy drugs. Conceptually, this finding implies that the Pgp in the BBB and BCSFB keeps natural toxins such as paclitaxel, from entering the brain (BBB) and, if they do enter the brain, keeps them in the CSF (BCSFB) where they may be less harmful than if they re-entered the brain. Thus, our work supports this novel idea and adds to the understanding of the functions of the BCSFB.
P-糖蛋白(Pgp)部分介导了对天然产物化疗药物的耐药性,这类药物占现有癌症治疗药物的一半以上。他莫昔芬(TAM)通过抑制Pgp增强了天然产物化疗药物在人细胞系中的细胞内沉积。Pgp在脉络丛中高度表达,被认为是血脑脊髓液屏障(BCSFB)的关键组成部分。我们进行了一项前瞻性随机研究,以评估TAM对Pgp的抑制作用是否会改变紫杉醇在脑脊液(CSF)中的沉积。
10例原发性或转移性脑肿瘤患者被随机分为两组:单独使用紫杉醇(175mg/m²静脉注射)或先接受一个疗程的TAM(第1 - 5天,每日两次,每次160mg/m²口服),然后在第5天使用紫杉醇(175mg/m²静脉注射)。在紫杉醇输注后采集CSF和血浆样本;通过高效液相色谱法测定紫杉醇和TAM的浓度。
10例患者中有6例在CSF中检测到紫杉醇。紫杉醇组和紫杉醇 - TAM组的CSF紫杉醇峰值浓度分别在3.5 - 57.4 nM和2.3 - 24.6 nM之间。虽然单独使用紫杉醇的患者平均CSF紫杉醇浓度比联合使用紫杉醇 - TAM的患者高2.4倍,CSF与血浆紫杉醇峰值中位数之比高3.7倍,但差异无统计学意义(P = 0.22)。在同时参与两组的一名患者中,单独使用紫杉醇时观察到CSF中紫杉醇浓度更高,且CSF与血浆中紫杉醇的比值更高。
与TAM联合使用时紫杉醇CSF浓度降低的趋势与已发表的研究结果一致,即Pgp在脉络丛内皮细胞中的定位起相反作用,使药物保留在CSF中。因此,抑制Pgp的药物,如TAM,可能会增加Pgp底物从BCSFB流出,反而可能降低天然产物化疗药物的CSF浓度。从概念上讲,这一发现意味着血脑屏障(BBB)和BCSFB中的Pgp可防止紫杉醇等天然毒素进入大脑(BBB),并且如果它们进入大脑,会将其保留在CSF(BCSFB)中,在CSF中它们可能比重新进入大脑时危害更小。因此,我们的研究支持了这一新颖观点,并增进了对BCSFB功能的理解。
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