Systemic Toxicity of Recombinant Adeno-Associated Virus Gene Therapy Vectors.

IF 1.4 4区 医学 Q3 PATHOLOGY Toxicologic Pathology Pub Date : 2024-11-22 DOI:10.1177/01926233241298892
Basel T Assaf
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Abstract

Recombinant adeno-associated virus (rAAV) vectors have emerged as a promising tool for gene therapy. However, the systemic administration of rAAV vectors is not without risks, particularly for dose levels >1 × 1014 viral genome per kilogram of body weight (vg/kg). rAAV-associated toxicities can variably manifest either acutely or in a delayed manner. Acute toxicities often present shortly after administration and can include severe immune responses, hepatotoxicity, and thrombotic microangiopathy (TMA). Delayed toxicities, on the other hand, may emerge weeks to months post-treatment, potentially involving chronic liver damage or prolonged immune activation. Thrombotic microangiopathy is often associated with complement activation and endothelial damage. The activation of the complement system can additionally trigger a cascade of inflammatory responses, exacerbating systemic toxicity. While many of these toxicities are reversible with appropriate medical intervention, there have been instances where the adverse effects were severe enough to lead to fatalities. Both human and animal studies have reported these adverse effects, highlighting the critical importance of thorough preclinical testing. However, a differential toxicity profile associated with systemic AAV administration exists between humans and nonhuman primates (NHPs), in which certain toxicities reported in humans are yet to be observed in NHPs, and vice versa. This review aims to explore the recent literature on systemic rAAV toxicities, focusing on dose levels, the role of the complement activation pathway, endothelial injury, TMA, hepatotoxicity, and the bidirectional translational safety profiles from both human and animal studies.

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重组腺相关病毒基因疗法载体的全身毒性。
重组腺相关病毒(rAAV)载体已成为一种前景广阔的基因治疗工具。然而,rAAV 载体的全身给药并非没有风险,尤其是当剂量水平大于每公斤体重 1 × 1014 病毒基因组(vg/kg)时。急性毒性通常在用药后不久出现,可包括严重的免疫反应、肝毒性和血栓性微血管病(TMA)。而延迟毒性则可能在治疗后数周至数月出现,可能涉及慢性肝损伤或长期免疫激活。血栓性微血管病通常与补体激活和内皮损伤有关。补体系统的激活还会引发一系列炎症反应,加剧全身毒性。虽然这些毒性中的许多在适当的医疗干预下是可逆的,但也有不良反应严重到导致死亡的情况。人类和动物研究都曾报告过这些不良反应,这凸显了全面临床前试验的极端重要性。然而,人与非人灵长类动物(NHPs)之间存在着与全身性 AAV 给药相关的不同毒性特征,其中某些在人身上报告的毒性尚未在 NHPs 身上观察到,反之亦然。本综述旨在探讨有关全身性 rAAV 毒性的最新文献,重点关注剂量水平、补体激活途径的作用、内皮损伤、TMA、肝毒性以及人类和动物研究的双向转化安全性概况。
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来源期刊
Toxicologic Pathology
Toxicologic Pathology 医学-病理学
CiteScore
4.70
自引率
20.00%
发文量
57
审稿时长
6-12 weeks
期刊介绍: Toxicologic Pathology is dedicated to the promotion of human, animal, and environmental health through the dissemination of knowledge, techniques, and guidelines to enhance the understanding and practice of toxicologic pathology. Toxicologic Pathology, the official journal of the Society of Toxicologic Pathology, will publish Original Research Articles, Symposium Articles, Review Articles, Meeting Reports, New Techniques, and Position Papers that are relevant to toxicologic pathology.
期刊最新文献
Toxicologic Pathology Forum*: Opinion on Assessing and Communicating Adversity for Implantable Medical Devices. Systemic Toxicity of Recombinant Adeno-Associated Virus Gene Therapy Vectors. Session 4: mRNA and Self-Amplifying RNA (saRNA): Opportunities for Disease Prevention and Therapy. Opinion on the Importance of Sharing Toxicologic Pathology Data for Educational and/or Scientific Purposes. Historical Control Background Incidence of Spontaneous Nonneoplastic Lesions of Sprague Dawley Rats in 104-Week Carcinogenicity Studies.
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