Brody S L, Metzger M, Danel C, Rosenfeld M A, Crystal R G
Pulmonary Branch, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, MD 20892.
Hum Gene Ther. 1994 Jul;5(7):821-36. doi: 10.1089/hum.1994.5.7-821.
Recombinant human adenovirus (Ad) vectors are leading candidates for human gene therapy for cystic fibrosis (CF) based on demonstration of efficient transfer of exogenous genes to rodent respiratory epithelium in vivo and human respiratory cells in vitro. The safety of Ad-mediated gene transfer to the respiratory epithelium and acute (up to 21 days) clinical responses to airway delivery of a replication-deficient recombinant, E1-, E3- Ad type 5-based vector containing the human cystic fibrosis transmembrane conductance regulator cDNA (AdCFTR) were evaluated in rhesus monkeys. Airway delivery of an Ad vector with the lacZ marker gene demonstrated beta-galactosidase expression in epithelial cells. Animals administered intratracheal AdCFTR demonstrated human CFTR cDNA expression in airway epithelial cells. Animals administered AdCFTR intranasal, and 24 hr later, intrabronchial [2 x 10(7) to 5 x 10(10) plaque-forming units (pfu), n = 12], in a fashion similar to a proposed human protocol, or only intrabronchial (10(11) pfu, n = 3), had no significant changes in clinical parameters compared to vehicle controls (n = 6). Microscopic analysis of the lung by necropsy or bronchoalveolar lavage demonstrated a dose-dependent increase in inflammatory cells, primarily lymphocytes, in the area where AdCFTR was delivered, which persisted for at least 2 months in some animals. Serum anti-Ad type 5 neutralizing antibody titers did not rise and shed Ad was not detected. The presence of AdCFTR DNA, analyzed by the polymerase chain reaction (PCR), was not detected in organs outside the lung. These data demonstrate that AdCFTR is well tolerated in non-human primates, although there is dose-dependent inflammation in the lung not clinically apparent.(ABSTRACT TRUNCATED AT 250 WORDS)
重组人腺病毒(Ad)载体是用于囊性纤维化(CF)基因治疗的主要候选物,这是基于其在体内将外源基因有效转移至啮齿动物呼吸道上皮以及在体外转移至人呼吸道细胞的相关证明。在恒河猴中评估了Ad介导的基因转移至呼吸道上皮的安全性以及对气道递送含有人囊性纤维化跨膜传导调节因子cDNA的复制缺陷型重组E1 -、E3 - 5型腺病毒载体(AdCFTR)的急性(长达21天)临床反应。携带lacZ标记基因的Ad载体经气道递送后,在上皮细胞中显示出β - 半乳糖苷酶表达。经气管内给予AdCFTR的动物在气道上皮细胞中显示出人类CFTR cDNA表达。以类似于拟议的人体方案的方式经鼻内给予AdCFTR,24小时后再经支气管给予[2×10⁷至5×10¹⁰空斑形成单位(pfu),n = 12],或仅经支气管给予(10¹¹ pfu,n = 3),与载体对照(n = 6)相比,临床参数无显著变化。通过尸检或支气管肺泡灌洗对肺进行显微镜分析表明,在AdCFTR递送区域,炎症细胞(主要是淋巴细胞)呈剂量依赖性增加,在一些动物中这种情况持续至少2个月。血清抗5型腺病毒中和抗体滴度未升高,且未检测到脱落的腺病毒。通过聚合酶链反应(PCR)分析,在肺外器官中未检测到AdCFTR DNA的存在。这些数据表明,AdCFTR在非人灵长类动物中耐受性良好,尽管肺部存在剂量依赖性炎症,但在临床上并不明显。(摘要截断于250字)
