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一种新型 LC-MS/MS 生物分析方法在大鼠体内研究有前景的含哌嗪抗肿瘤原型化合物 (LQFM018) 的药代动力学。

Preclinical pharmacokinetics of a promising antineoplastic prototype piperazine-containing compound (LQFM018) in rats by a new LC-MS/MS bioanalytical method.

机构信息

Center of Studies and Research Toxic-Pharmacological, School of Pharmacy, Federal University of Goias, Goiania, Goias, Brazil.

Institute of Biological Sciences, Federal University of Goias, Goiania, Goias, Brazil.

出版信息

J Chromatogr B Analyt Technol Biomed Life Sci. 2023 May 15;1223:123710. doi: 10.1016/j.jchromb.2023.123710. Epub 2023 Apr 12.

DOI:10.1016/j.jchromb.2023.123710
PMID:37068313
Abstract

LQFM018 is a novel antineoplastic prototype, showing an expressive drug-triggered K562 leukemic cells death mechanism, through necroptotic signaling. Due to its promising effect, this study aimed to evaluate the pharmacokinetics of LQFM018 in rats, using a new validated bioanalytical LC-MS/MS-based method. Chromatographic column was an ACE® C18 (100 mm × 4.6 mm, 5 µm) eluted by a mobile phase composed of ammonium acetate 2 mM and formic acid 0.025%:methanol (50:50, v/v), under flow of 1.2 mL/min and injection volume of 3.0 µL. LQFM018 was extracted from rat plasma by a simple liquid-liquid method, using MTBE solvent. Rats were administered intraperitoneally at LQFM018 100 mg/kg dose and blood samples were collect at times of 0, 1, 2, 3, 4, 5, 6, 7, 8, and 9 h. Bioanalytical-LC-MS/MS-based method was rapid, high throughput and sensitive with a good linearity ranging from 10 (LLOQ) to 15000 ng/mL, besides precise and accurate, ranging of 0.8-7.3% and 96.8-107.6%, respectively. The prototype LQFM018 was rapid and well absorbed, and highly distributed, apparently due to its high lipid solubility. These features are primordial for an anticancer agent in the treatment of deep tumors, such as bone marrow neoplasms, in which the drug might permeate easily tissue barriers. Also, LQFM018 has demonstrated a high clearance, according to a low tin rats, indicating a relative fast elimination phase related to a possible intense hepatic biotransformation. These information support further studies to establish new understands on pharmacokinetics of promising antineoplastic prototype LQFM018 from preclinical and clinical evaluations.

摘要

LQFM018 是一种新型抗肿瘤原型药物,通过坏死信号显示出表达药物触发的 K562 白血病细胞死亡机制。由于其有前景的效果,本研究旨在使用新验证的基于 LC-MS/MS 的生物分析方法来评估 LQFM018 在大鼠中的药代动力学。色谱柱为 ACE® C18(100mm×4.6mm,5μm),流动相由 2mM 乙酸铵和 0.025%甲酸:甲醇(50:50,v/v)组成,流速为 1.2mL/min,进样体积为 3.0μL。LQFM018 从大鼠血浆中通过简单的液液萃取方法提取,使用 MTBE 溶剂。大鼠以 LQFM018 100mg/kg 剂量腹腔给药,在 0、1、2、3、4、5、6、7、8 和 9h 时采集血样。基于生物分析的 LC-MS/MS 方法快速、高通量、灵敏,线性范围为 10(LLOQ)至 15000ng/mL,精密度和准确度分别为 0.8-7.3%和 96.8-107.6%。原型 LQFM018 吸收迅速、分布广泛,显然是由于其高脂溶性。这些特征对于治疗深层肿瘤(如骨髓肿瘤)的抗癌药物非常重要,因为药物可能容易渗透组织屏障。此外,LQFM018 的清除率很高,根据低锡大鼠的结果,表明与可能强烈的肝生物转化相关的相对快速消除相。这些信息支持进一步研究,以从临床前和临床评估中建立对有前途的抗肿瘤原型 LQFM018 的药代动力学的新认识。

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