Egorin M J, Sigman L M, Van Echo D A, Forrest A, Whitacre M Y, Aisner J
Cancer Res. 1987 Jan 15;47(2):617-23.
Hexamethylene bisacetamide (HMBA), a potent differentiating agent, was tested in patients with refractory, solid tumors. Twenty patients received 25 evaluable courses. HMBA was given by continuous i.v. infusion for 5 consecutive days with courses repeated every 4 wk, provided there was acceptable, reversible toxicity. The starting dose was 4.8 g/m2/day for 5 days with escalations in subsequent cohorts of patients to 43.2 g/m2/day for 5 days. The patients included 12 females and eight males with median age of 56 yr (range 35 to 75 yr) and a median performance status of 80% (range, 60 to 100%). All except two patients had received prior chemotherapy, radiation therapy, or both. Metabolic acidosis and neurotoxicity, consisting of agitation, hallucinations, confusion, and alteration of consciousness, were dose dependent and dose limiting. The one patient treated with 43.2 m/m2/day became acidotic, agitated, and disoriented but recovered to his previous mental and electrolyte status by 8 days after the end of the HMBA infusion. One patient treated with 33.6 g/m2/day became severely acidotic (pH 7.07) and obtunded and also developed myocardial and cerebral infarctions during the HMBA infusion. The other two patients treated with 33.6 g/m2/day became mildly agitated during drug infusion. Six patients were treated at 24 g/m2/day without neurotoxicity. Transient renal insufficiency was seen in the two patients with severe neurotoxicity and in three other patients. Dose-related, mild to moderate nausea and vomiting were observed in ten patients. Four patients developed cutaneous herpes infections during treatment. White blood cell depression was not dose related, and at 24 g/m2/day, the median white blood cell nadir was 4,500/microliter (range, 2,000 to 7,900/microliter). Thrombocytopenia was dose related. At 24 g/m2/day, the median platelet count nadir was 207,000/microliter (range, 66,000 to 542,000/microliter). No objective tumor regressions were noted. HMBA pharmacokinetics was studied at all dosages. Plasma and urine samples from 20 patients were analyzed by gas-liquid chromatography for parent compound. HMBA plasma steady-state concentrations (Css) were achieved in all patients by 12 to 24 h into infusion. Once Css was achieved, daily variation was generally less than or equal to 10% from the mean Css. HMBA plasma Css increased linearly with dose, but there was variation in the Css achieved in individual patients at each dose. Doses of 24 to 33.6 g/m2/day consistently produced plasma HMBA Css of 1 to 2 mM matching concentrations required for differentiation in vitro.(ABSTRACT TRUNCATED AT 400 WORDS)
己二酰双乙酰胺(HMBA)是一种有效的分化诱导剂,已在难治性实体瘤患者中进行了试验。20例患者接受了25个可评估疗程的治疗。HMBA通过静脉持续输注给药,连续5天,每4周重复一个疗程,前提是毒性可接受且可逆。起始剂量为4.8 g/m²/天,持续5天,随后各批次患者剂量逐步增加至43.2 g/m²/天,持续5天。患者包括12名女性和8名男性,中位年龄56岁(范围35至75岁),中位体能状态为80%(范围60至100%)。除两名患者外,所有患者均接受过先前的化疗、放疗或两者皆有。代谢性酸中毒和神经毒性,包括躁动、幻觉、意识模糊和意识改变,呈剂量依赖性且为剂量限制性毒性。接受43.2 m/m²/天治疗的1例患者出现酸中毒、躁动和定向障碍,但在HMBA输注结束后8天恢复到之前的精神和电解质状态。接受33.6 g/m²/天治疗的1例患者在HMBA输注期间出现严重酸中毒(pH 7.07)和意识不清,还发生了心肌梗死和脑梗死。另外两名接受33.6 g/m²/天治疗的患者在药物输注期间出现轻度躁动。6例患者接受24 g/m²/天治疗,未出现神经毒性。两名严重神经毒性患者和另外三名患者出现短暂性肾功能不全。10例患者观察到与剂量相关的轻至中度恶心和呕吐。4例患者在治疗期间发生皮肤疱疹感染。白细胞减少与剂量无关,在24 g/m²/天剂量下,白细胞计数最低点的中位数为4500/微升(范围2000至7900/微升)。血小板减少与剂量相关。在24 g/m²/天剂量下,血小板计数最低点的中位数为207,000/微升(范围66,000至542,000/微升)。未观察到客观的肿瘤消退。在所有剂量下均对HMBA的药代动力学进行了研究。通过气液色谱法分析了20例患者的血浆和尿液样本中的母体化合物。所有患者在输注12至24小时后达到HMBA血浆稳态浓度(Css)。一旦达到Css,每日波动通常比平均Css低或等于10%。HMBA血浆Css随剂量呈线性增加,但每个剂量下个体患者达到的Css存在差异。24至33.6 g/m²/天的剂量持续产生1至2 mM的血浆HMBA Css,与体外分化所需浓度相符。(摘要截取自400字)
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