晚期癌症患者长期静脉输注羟基脲：一项I期试验。

Long-term intravenous hydroxyurea infusions in patients with advanced cancer. A phase I trial.

作者信息

Blumenreich M S, Kellihan M J, Joseph U G, Lalley K A, Sherrill E J, Sullivan D M, Hamm J T, Gentile P S, Sheth S P, Seeger J

机构信息

Department of Medicine, University of Louisville School of Medicine, Kentucky.

出版信息

Cancer. 1993 May 1;71(9):2828-32. doi: 10.1002/1097-0142(19930501)71:9<2828::aid-cncr2820710924>3.0.co;2-p.

DOI:10.1002/1097-0142(19930501)71:9<2828::aid-cncr2820710924>3.0.co;2-p

PMID:7682153

Abstract

BACKGROUND

Hydroxyurea is an S-phase specific drug. Constant exposure of tumor cells with a low S-phase fraction to the agent may result in improved cell kill. Because of its short half-life, a continuous intravenous infusion may result in better tumor exposure than intake by mouth. The goal of this trial was to find the longest tolerable duration of a continued intravenous infusion of hydroxyurea (HU) given at escalating doses.

METHODS

Eligible patients had histologically confirmed cancer without effective alternate therapy, normal blood counts, liver and kidney function. After giving informed consent, the infusion began via a permanent indwelling catheter utilizing a portable pump. Dose levels (in g/m2/d) were 0.5 for level I, 1.0 for level II, 1.66 for level III, and 2.5 for level IV.

RESULTS

Fourteen patients were entered. Five were men. Median age was 56 years of age (range: 32-67), median performance status 1 (range: 0-2). Diagnoses were as follows: colorectal cancer, seven; unknown primary site, three; breast cancer, two; melanoma, one; and adenoid-cystic carcinoma, one. Nine patients were pretreated with chemotherapy. Three patients were entered per dose level, except on level I, were five were entered. The mean duration of infusion was 12 weeks on level I, 5 weeks on II, 3 on III, 1 on IV. Toxicity included leukopenia below 2.0 K/mm3 in one patient each on levels III and IV, thrombocytopenia below 100 K/mm3 in one patient each on levels II and IV, and stomatitis in three patients (one on level II and two on IV). This toxicity was dose limiting. One patient on level III, with an unknown primary, had an objective response. HU levels were measured by a modification of the Fabricius-Rajewsky method. Mean plasma levels in micrograms per milliliter (SEM) were as follows: level I, 3.6 (0.23); level II, 5.1 (0.57); level III, 10.1 (1.55); and level IV, 16.7 (one point). Fetal hemoglobin rose two-fold and five-fold in two patients on level I after 9 and 16 weeks on therapy, respectively.

CONCLUSIONS

HU as a continuous intravenous infusion is well tolerated; the maximum duration of therapy is related inversely with the dose given. No major antitumor activity was seen. The greatest interest in the drug rests in its future use as a modulator and radiation potentiator. The increase in hemoglobin F was of interest and may be important in the treatment of sickle cell disease.

摘要

背景

羟基脲是一种S期特异性药物。持续将处于低S期比例的肿瘤细胞暴露于该药物下可能会提高细胞杀伤效果。由于其半衰期较短，持续静脉输注可能比口服能使肿瘤接触到更好的药物浓度。本试验的目的是找出递增剂量持续静脉输注羟基脲（HU）的最长可耐受时间。

方法

符合条件的患者经组织学确诊患有癌症且无有效的替代治疗方案，血常规、肝肾功能正常。在获得知情同意后，通过使用便携式泵经永久性留置导管开始输注。剂量水平（克/平方米/天）：I级为0.5，II级为1.0，III级为1.66，IV级为2.5。

结果

纳入14例患者。5例为男性。中位年龄为56岁（范围：32 - 67岁），中位体能状态评分为1分（范围：0 - 2分）。诊断如下：结直肠癌7例；原发部位不明3例；乳腺癌2例；黑色素瘤1例；腺样囊性癌1例。9例患者曾接受过化疗。除I级有5例患者外，每个剂量水平纳入3例患者。I级的平均输注持续时间为12周，II级为5周，III级为3周，IV级为1周。毒性反应包括III级和IV级各有1例患者白细胞计数低于2.0×10³/mm³，II级和IV级各有1例患者血小板计数低于100×10³/mm³，3例患者出现口腔炎（II级1例，IV级2例）。这种毒性反应限制了剂量。III级的1例原发部位不明的患者有客观反应。通过改良的法布里修斯 - 拉耶夫斯基方法测量HU水平。平均血浆水平（微克/毫升，标准误）如下：I级为3.6（0.23）；II级为5.1（0.57）；III级为10.1（1.55）；IV级为16.7（单个数据点）。I级的2例患者在治疗9周和16周后胎儿血红蛋白分别升高了两倍和五倍。