首页> 外文期刊>Abdominal imaging. >Feasibility of CT scan-guided Tru-Cut serial liver biopsies to evaluate pharmacodynamic endpoints in patients with liver metastasis treated with experimental drugs.
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Feasibility of CT scan-guided Tru-Cut serial liver biopsies to evaluate pharmacodynamic endpoints in patients with liver metastasis treated with experimental drugs.

机译:CT扫描指导的Tru-Cut系列肝活检在评估用实验药物治疗的肝转移患者中药效学终点的可行性。

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摘要

We assessed the feasibility of using computed tomographically guided, Tru-Cut serial liver biopsies to perform pharmacodynamic studies in patients with liver metastasis who had been treated with experimental drugs. Twenty-three patients with liver metastasis were enrolled in two protocols for evaluation of the response to two new biologic drugs: a farnesyltransferase inhibitor and a tyrosine kinase inhibitor of the epidermal growth factor receptor. Computed tomographically guided Tru-Cut biopsies with an 18-gauge needle were performed. The procedure was performed at baseline and 2, 6, and 24 h after starting the administration of the drug. The procedures were scheduled on an outpatient basis. We obtained 271 samples (168 from metastatic lesions and 103 from surrounding normal liver tissue) from 23 patients. Biochemical determination of farnesyltransferase activity and different immunohistochemistry stainings (pEGRF, pMAPK, p27, Ki67, and apoptosis) of the signal transduction pathway were determined in each tissue sample, and all scheduled tissue assays were performed with the tissues obtained. Complete serial biopsies were performed in 20 patients. Three patients were excluded due to minor complications after the first biopsy. The morbidity rate in relation to the number of procedures was 1.1% (three of 271 samples). We found serial liver biopsies using Tru-Cut to be a safe and easy procedure. In our series, we could evaluate samples for molecular changes that influence the optimal dose, sequence, and schedule of the new antineoplastic agents.
机译:我们评估了使用计算机断层扫描指导的Tru-Cut系列肝活检在接受实验药物治疗的肝转移患者中进行药效学研究的可行性。 23位肝转移患者参加了两种方案,以评估对两种新生物药物的反应:法尼基转移酶抑制剂和表皮生长因子受体的酪氨酸激酶抑制剂。用18号针进行计算机断层扫描引导的Tru-Cut活检。该过程在开始给药后的基线,2、6和24小时进行。该程序按门诊安排。我们从23位患者中获得了271个样本(168个来自转移性病变,103个来自周围正常肝组织)。在每个组织样品中测定了法尼基转移酶活性的生化测定和信号转导途径的不同免疫组织化学染色(pEGRF,pMAPK,p27,Ki67和凋亡),并对获得的组织进行了所有预定的组织测定。对20例患者进行了完整的系列活检。首次活检后,由于轻微并发症而将三名患者排除在外。相对于手术数量的发病率是1.1%(271个样本中的三个)。我们发现使用Tru-Cut进行的肝活检是一种安全,简便的方法。在我们的系列中,我们可以评估样品的分子变化,这些变化会影响新抗肿瘤药的最佳剂量,顺序和时间表。

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