基于纳米粒子的新型基因疗法 npFOXF1 对肺泡毛细血管发育不良伴肺静脉错位症野生型小鼠的安全性证明

IF 5.3 Q1 MEDICINE, RESEARCH & EXPERIMENTAL Biologics : Targets & Therapy Pub Date : 2023-03-20 eCollection Date: 2023-01-01 DOI:10.2147/BTT.S400006
Fatemeh Kohram, Zicheng Deng, Yufang Zhang, Abid A Al Reza, Enhong Li, Olena A Kolesnichenko, Samriddhi Shukla, Vladimir Ustiyan, Jose Gomez-Arroyo, Anusha Acharya, Donglu Shi, Vladimir V Kalinichenko, Alan P Kenny
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摘要

简介肺泡毛细血管发育不良伴肺静脉错位(ACDMPV)是一种致命的先天性疾病,是由于肺血管内皮细胞缺乏 FOXF1,导致肺泡毛细血管形态发生异常、肺静脉错位和肺叶发育紊乱。受影响的新生儿通常在出生后数天至数周内出现紫绀、严重呼吸困难、肺动脉高压和死亡。目前还没有治疗 ACDMPV 的方法,不过卡利尼琴科实验室(Kalinichenko lab)最近的一项小鼠研究表明,纳米颗粒给药可提高存活率并重建正常的肺泡-毛细血管结构。本研究的目的是调查静脉注射表达 FOXF1 的 PEI-PEG 纳米颗粒(npFOXF1)的安全性,这是我们治疗 ACDMPV 的开创性方法。方法:npFOXF1 已经构建、验证,随后通过眶后注射对出生后第 14 天(P14)的小鼠进行单剂量给药。在出生后第 16 天(P16)和出生后第 21 天(P21)监测生化、血清和组织学安全性:结果:经过治疗,我们没有观察到小鼠死亡,小鼠的一般状况也没有发现明显的异常。P16和P21的血清化学、全血和组织学毒性检测均未发现异常:总之,npFOXF1 具有很好的安全性,结合之前的疗效研究,npFOXF1 可被视为人类新生儿 ACDMPV 的理想候选疗法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Demonstration of Safety in Wild Type Mice of npFOXF1, a Novel Nanoparticle-Based Gene Therapy for Alveolar Capillary Dysplasia with Misaligned Pulmonary Veins.

Introduction: Alveolar Capillary Dysplasia with Misaligned Pulmonary Veins (ACDMPV) is a fatal congenital disease resulting from a pulmonary vascular endothelial deficiency of FOXF1, producing abnormal morphogenesis of alveolar capillaries, malpositioned pulmonary veins and disordered development of lung lobes. Affected neonates suffer from cyanosis, severe breathing insufficiency, pulmonary hypertension, and death typically within days to weeks after birth. Currently, no treatment exists for ACDMPV, although recent murine research in the Kalinichenko lab demonstrates nanoparticle delivery improves survival and reconstitutes normal alveolar-capillary architecture. The aim of the present study is to investigate the safety of intravenous administration of FOXF1-expressing PEI-PEG nanoparticles (npFOXF1), our pioneering treatment for ACDMPV.

Methods: npFOXF1 was constructed, validated, and subsequently administered in a single dose to postnatal day 14 (P14) mice via retro-orbital injection. Biochemical, serologic, and histologic safety were monitored at postnatal day 16 (P16) and postnatal day 21 (P21).

Results: With treatment we observed no lethality, and the general condition of mice revealed no obvious abnormalities. Serum chemistry, whole blood, and histologic toxicity was assayed on P16 and P21 and revealed no abnormality.

Discussion: In conclusion, npFOXF1 has a very good safety profile and combined with preceding studies showing therapeutic efficacy, npFOXF1 can be considered as a good candidate therapy for ACDMPV in human neonates.

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来源期刊
Biologics : Targets & Therapy
Biologics : Targets & Therapy MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
8.30
自引率
0.00%
发文量
22
审稿时长
16 weeks
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