1-α-羟基维生素D2在促黄体生成素β亚基标签转基因小鼠中的毒性及剂量反应研究
Toxicity and dose-response studies of 1-alpha hydroxyvitamin D2 in LH-beta-tag transgenic mice.
作者信息
Dawson Daniel G, Gleiser Joel, Zimbric Michele L, Darjatmoko Soesiawaiti R, Lindstrom Mary J, Strugnell Stephen A, Albert Daniel M
机构信息
Department of Ophthalmology and Visual Sciences, University of Wisconsin School of Medicine, Madison, Wisconsin, USA.
出版信息
Ophthalmology. 2003 Apr;110(4):835-9. doi: 10.1016/S0161-6420(02)01934-6.
PURPOSE
To determine the effectiveness of a vitamin D analog, 1alpha-hydroxyvitamin D(2) (1alpha-OH-D(2)), in inhibiting retinoblastoma in a transgenic retinoblastoma model (LHbeta-Tag mouse) and to evaluate its toxicity.
DESIGN
Experimental study using an animal (LHbeta-Tag transgenic mouse) randomized (controlled) trial.
PARTICIPANTS AND CONTROLS
Two hundred seventeen LHbeta-Tag transgene-positive 8- to 10-week-old mice total; 179 drug-treated animals, 38 control animals.
METHODS
Mice were fed a vitamin D- and calcium-restricted diet and were randomized to treatment groups receiving control (vehicle), or 0.1, 0.3, 0.5, or 1.0 micro g/day of 1alpha-OH-D(2) via oral gavage 5 times weekly for 5 weeks. Body weight was measured at the start of treatment and twice weekly during treatment. Animals were euthanized on the last day of treatment. The eyes were enucleated, processed histologically, and serially sectioned. Representative sections from the superior, middle, and inferior regions of each globe were examined microscopically and tumor areas were measured using Optimas software. Serum was collected for serum calcium levels. Kidneys were removed for histologic processing and were analyzed microscopically for kidney calcification.
MAIN OUTCOME MEASURES
Mean tumor area was measured to determine drug effectiveness. Toxicity was assessed by survival, weight loss over the treatment period, serum calcium, and kidney calcification.
RESULTS
The mean tumor size in each 1alpha-OH-D(2) group was smaller than controls (all P values < 0.02): control, 90,248 micro m(2); 0.1 micro g, 31,545 micro m(2); 0.3 micro g, 16,750 micro m(2); 0.5 micro g, 30,245 micro m(2); and 1.0 micro g, 16,049 micro m(2). No dose-dependent response curve was evident. The survival percentage for each group was as follows: control, 97%; 0.1 micro g, 91%; 0.3 micro g, 88%; 0.5 micro g, 70%; and 1.0 micro g, 63%. Mortality was higher in the 0.5- micro g and 1.0- micro g doses (P values < 0.01) compared with other treatment groups and with the control group. Serum calcium levels were significant in all treatment groups compared with controls (all P values < 0.0001).
CONCLUSIONS
In the LHbeta-Tag mouse, 1alpha-OH-D(2) inhibits retinoblastoma with no significant increase in mortality in lower doses (0.1-0.3 micro g). 1alpha-OH-D(2) has approval by the Food and Drug Administration as an investigative drug for cancer treatment, and has shown efficacy with low toxicity in adult cancer trials. 1alpha-OH-D(2) meets the criteria for human clinical trials.
目的
确定维生素D类似物1α-羟基维生素D₂(1α-OH-D₂)在转基因视网膜母细胞瘤模型(LHβ-Tag小鼠)中抑制视网膜母细胞瘤的有效性,并评估其毒性。
设计
使用动物(LHβ-Tag转基因小鼠)随机(对照)试验的实验研究。
参与者和对照组
总共217只LHβ-Tag转基因阳性8至10周龄小鼠;179只药物治疗动物,38只对照动物。
方法
给小鼠喂食低维生素D和钙的饮食,并随机分为治疗组,分别接受对照(赋形剂),或通过每周5次口服灌胃给予0.1、0.3、0.5或1.0μg/天的1α-OH-D₂,持续5周。在治疗开始时测量体重,并在治疗期间每周测量两次。在治疗的最后一天对动物实施安乐死。摘除眼球,进行组织学处理并连续切片。使用Optimas软件对每个眼球的上、中、下区域的代表性切片进行显微镜检查并测量肿瘤面积。收集血清以检测血清钙水平。摘除肾脏进行组织学处理,并进行显微镜检查以分析肾脏钙化情况。
主要观察指标
测量平均肿瘤面积以确定药物有效性。通过生存率、治疗期间的体重减轻、血清钙和肾脏钙化来评估毒性。
结果
每个1α-OH-D₂组的平均肿瘤大小均小于对照组(所有P值<0.02):对照组为90248μm²;0.1μg组为31545μm²;0.3μg组为16750μm²;0.5μg组为30245μm²;1.0μg组为16049μm²。未观察到明显的剂量依赖性反应曲线。每组的生存率如下:对照组为97%;0.1μg组为91%;0.3μg组为88%;0.5μg组为70%;1.0μg组为63%。与其他治疗组和对照组相比,0.5μg和1.0μg剂量组的死亡率更高(P值<0.01)。与对照组相比,所有治疗组的血清钙水平均有显著差异(所有P值<0.0001)。
结论
在LHβ-Tag小鼠中,1α-OH-D₂可抑制视网膜母细胞瘤,低剂量(0.1 - 0.3μg)时死亡率无显著增加。1α-OH-D₂已获得美国食品药品监督管理局批准作为癌症治疗的研究性药物,并且在成人癌症试验中显示出低毒性的疗效。1α-OH-D₂符合人体临床试验的标准。
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