膀胱癌特异性溶瘤腺病毒的致畸毒性评价在小鼠上。

Teratogenic Toxicity Evaluation of Bladder Cancer-Specific Oncolytic Adenovirus on Mice.

机构信息

Gansu Nephro-Urological Clinical Center, Key Laboratory of Urological Diseases, Gansu Province (Lanzhou University), Institute of Urology, The Second Hospital of Lanzhou University, Lanzhou730000, China.

Center of Medical Experiments, School of Basic Medical Sciences, Lanzhou University, Gansu Province, Lanzhou730000, China.

出版信息

Curr Gene Ther. 2021;21(2):160-166. doi: 10.2174/1566523220999201217161258.

DOI:10.2174/1566523220999201217161258

PMID:33334289

Abstract

BACKGROUND

In our previous studies, we had demonstrated the efficiency and specificity of constructed bladder tissue-specific adenovirus Ad-PSCAE-UPII-E1A-AR (APU-EIA-AR) on bladder cancer. The virus biodistribution and body toxicity in nude mice have also been investigated. However, the safety of the bladder cancer-specific oncolytic adenovirus on fetal mice and F1 mice should be under intense investigation.

OBJECTIVE

In order to evaluate the teratogenic toxicity of bladder cancer-specific oncolytic adenovirus APU-EIA-AR on mice, in this study, we investigated the fetal mice weight, fetal body length and tail length, fetal skeleton development, as well as the F1 mice weight, growth curve, and major organ pathology. These teratogenic toxicity data of bladder tissue-specific adenovirus Ad-PSCAE- UPII-E1A-AR (AD) would provide safe information prior to embarking on clinical trials.

METHODS

On the sixth day of being fertilized, the pregnant mice began to be intramuscularly administrated with AD (1×10VP, 1×10VP, 1×10VP) every other day for ten days. The pregnant mice were then divided into two groups. One group was euthanized on the seventeenth day; the fetal mice were taken out, and the bone structure of the infants was observed. The other group was observed until natural childbirth. The Filial Generation (F1) is fed for 30 days; the variations in the growth progress and development were assessed. The mice were then euthanized; The tissues from major organs were harvested and observed under the microscope.

RESULTS

In the process of teratogenic toxicity test, the Placenta weight, fetal mice weight, body length, and a tail length of mice fetal in adenovirus treated group did not reveal any alteration. Meanwhile, comparing with the PBS group, there is no obvious change in the skeleton of fetal mice treated with adenovirus. During the development process of F1 mice treated with adenovirus, the changes in mice weight show statistical significance. However, in the progress of the growth curve, this difference is not very obvious. Furthermore, the pathological section showed no obvious alteration in major organs.

CONCLUSION

Our study demonstrated that bladder cancer-specific adenovirus Ad-PSCAE-UPII- E1A-AR appears safe in pregnant mice without any discernable effects on fetal mice and F1 development. Hence, it is relatively safe for tumor gene therapy.

摘要

背景

在我们之前的研究中，我们已经证明了构建的膀胱组织特异性腺病毒 Ad-PSCAE-UPII-E1A-AR（APU-EIA-AR）在膀胱癌中的效率和特异性。还研究了病毒在裸鼠中的体内分布和全身毒性。然而，膀胱癌特异性溶瘤腺病毒在胎鼠和 F1 鼠中的安全性应受到严格的研究。

目的

为了评估膀胱癌特异性溶瘤腺病毒 APU-EIA-AR 对小鼠的致畸毒性，本研究中，我们研究了胎鼠体重、胎鼠体长和尾长、胎鼠骨骼发育以及 F1 鼠体重、生长曲线和主要器官病理学。这些膀胱组织特异性腺病毒 Ad-PSCAE-UPII-E1A-AR（AD）的致畸毒性数据将为开展临床试验提供安全信息。

方法

受精第 6 天，妊娠小鼠开始每隔一天肌肉注射 AD（1×10VP、1×10VP、1×10VP），连续 10 天。然后将妊娠小鼠分为两组。一组在第 17 天处死；取出胎鼠，观察胎儿骨骼结构。另一组观察至自然分娩。子一代（F1）饲养 30 天；评估生长进展和发育的变化。然后处死小鼠；收获主要器官组织并在显微镜下观察。