Modeling rare genetic disease with patient-derived induced pluripotent stem cells: reassessment of the minimum numbers of lines needed.

IF 4.9 2区医学 Q1 CELL & TISSUE ENGINEERING

Stem Cells Translational Medicine Pub Date : 2025-07-24 DOI:10.1093/stcltm/szaf032

Ashok R Dinasarapu, Diane J Sutcliffe, Lauren Grychowski, Erkin Ozel, Anika Thite, Jasper E Visser, Ellen J Hess, Sharon M Kolk, H A Jinnah

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引用次数: 0

Abstract

Induced pluripotent stem cells (iPSCs) are widely used to model human genetic diseases. The most common strategy involves collecting cells from relevant individuals and then reprogramming them into iPSCs. This strategy is very powerful, but finding enough individuals with a specific genetic disease can be challenging, especially since most are rare. In addition, making numerous iPSC lines is time-consuming and expensive. As a result, most studies have included relatively small numbers of iPSC lines, sometimes from the same individual. Considering the experimental variability obtained using different iPSC lines, there has been great interest in delineating the most efficient number of lines needed to achieve a robust and reproducible result. Several recommendations have been published, although most conclusions have been based on methods where experimental variance from individual cases is difficult to separate from technical issues related to the preparation of iPSCs. The current study used gene expression profiles determined by RNA sequencing (RNAseq) to empirically evaluate the impact of the number of unique individuals and the number of replicate iPSC lines from each individual for modeling Lesch-Nyhan disease (LND). This disease is caused by mutations in the HPRT1 gene, which encodes the enzyme hypoxanthine-guanine phosphoribosyltransferase. Results for detecting disease-relevant changes in gene expression depended on the analytical method employed, and whether or not statistical procedures were used to address multiple iPSC lines from the same individual. In keeping with prior studies, the best results were obtained with iPSC lines from 3-4 unique individuals per group. In contrast to prior studies, results were improved with 2 lines per individual, without statistical corrections for duplicate lines from the same individual. In the current study where all lines were produced in parallel using the same methods, most variance in gene expression came from technical factors unrelated to the individual from whom the iPSC lines were prepared.

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用患者来源的诱导多能干细胞模拟罕见遗传疾病：重新评估所需的最小细胞系数量。

诱导多能干细胞（iPSCs）被广泛用于人类遗传疾病的建模。最常见的策略包括从相关个体收集细胞，然后将其重新编程为iPSCs。这种策略非常强大，但找到足够多的患有特定遗传疾病的个体可能具有挑战性，特别是因为大多数都是罕见的。此外，制造大量的iPSC系既耗时又昂贵。因此，大多数研究只包括相对较少数量的iPSC系，有时来自同一个体。考虑到使用不同的iPSC系获得的实验变异性，人们对描述获得稳健和可重复结果所需的最有效的系数非常感兴趣。已经发表了几项建议，尽管大多数结论所依据的方法很难将个别病例的实验差异与与制备多能干细胞有关的技术问题区分开来。目前的研究使用由RNA测序（RNAseq）确定的基因表达谱来经验评估独特个体的数量和来自每个个体的重复iPSC系的数量对Lesch-Nyhan病（LND）建模的影响。这种疾病是由编码次黄嘌呤-鸟嘌呤磷酸核糖基转移酶的HPRT1基因突变引起的。检测疾病相关基因表达变化的结果取决于所采用的分析方法，以及是否使用统计程序来处理来自同一个体的多个iPSC系。与先前的研究一致，每组3-4个独特个体的iPSC系获得最佳结果。与先前的研究相比，每个个体2个品系的结果得到了改善，同一个体的重复品系没有统计学上的修正。在目前的研究中，所有系都是用相同的方法平行生产的，基因表达的大多数差异来自与制备iPSC系的个体无关的技术因素。

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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来源期刊

Stem Cells Translational Medicine CELL & TISSUE ENGINEERING-

CiteScore

12.90

自引率

3.30%

发文量

140

审稿时长

6-12 weeks

期刊介绍： STEM CELLS Translational Medicine is a monthly, peer-reviewed, largely online, open access journal. STEM CELLS Translational Medicine works to advance the utilization of cells for clinical therapy. By bridging stem cell molecular and biological research and helping speed translations of emerging lab discoveries into clinical trials, STEM CELLS Translational Medicine will help move applications of these critical investigations closer to accepted best patient practices and ultimately improve outcomes. The journal encourages original research articles and concise reviews describing laboratory investigations of stem cells, including their characterization and manipulation, and the translation of their clinical aspects of from the bench to patient care. STEM CELLS Translational Medicine covers all aspects of translational cell studies, including bench research, first-in-human case studies, and relevant clinical trials.