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遗传疾病与治疗

Genetic Disease and Therapy.

机构信息

Medical Scientist Training Program, University of California, San Francisco, California 94143, USA; email:

Department of Microbiology and Immunology and Diabetes Center, University of California, San Francisco, California 94143, USA.

出版信息

Annu Rev Pathol. 2021 Jan 24;16:145-166. doi: 10.1146/annurev-pathmechdis-012419-032626.

Abstract

Genetic diseases cause numerous complex and intractable pathologies. DNA sequences encoding each human's complexity and many disease risks are contained in the mitochondrial genome, nuclear genome, and microbial metagenome. Diagnosis of these diseases has unified around applications of next-generation DNA sequencing. However, translating specific genetic diagnoses into targeted genetic therapies remains a central goal. To date, genetic therapies have fallen into three broad categories: bulk replacement of affected genetic compartments with a new exogenous genome, nontargeted addition of exogenous genetic material to compensate for genetic errors, and most recently, direct correction of causative genetic alterations using gene editing. Generalized methods of diagnosis, therapy, and reagent delivery into each genetic compartment will accelerate the next generations of curative genetic therapies. We discuss the structure and variability of the mitochondrial, nuclear, and microbial metagenomic compartments, as well as the historical development and current practice of genetic diagnostics and gene therapies targeting each compartment.

摘要

遗传性疾病会导致许多复杂且棘手的病理。人类的复杂性和许多疾病风险的 DNA 序列编码包含在线粒体基因组、核基因组和微生物宏基因组中。这些疾病的诊断已经围绕着下一代 DNA 测序的应用而统一起来。然而,将特定的遗传诊断转化为靶向的遗传治疗仍然是一个核心目标。迄今为止,遗传治疗已经分为三大类:用新的外源基因组大量替代受影响的遗传区室,非靶向地添加外源遗传物质来补偿遗传错误,以及最近,使用基因编辑直接纠正致病遗传改变。将诊断、治疗和试剂递送至每个遗传区室的通用方法将加速下一代治愈性遗传治疗的发展。我们讨论了线粒体、核和微生物宏基因组区室的结构和变异性,以及针对每个区室的遗传诊断和基因治疗的历史发展和当前实践。

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