Depletion of TP53 in Human Pluripotent Stem Cells Triggers Malignant-Like Behavior.

IF 3.2 3区生物学 Q3 MATERIALS SCIENCE, BIOMATERIALS Advanced biology Pub Date : 2025-01-06 DOI:10.1002/adbi.202400538

Joaquin Montilla-Rojo, Thomas F Eleveld, Marnix van Soest, Sanne Hillenius, Dennis M Timmerman, Ad J M Gillis, Bernard A J Roelen, Christine L Mummery, Leendert H J Looijenga, Daniela C F Salvatori

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Abstract

Human pluripotent stem cells (hPSCs) tend to acquire genetic aberrations upon culture in vitro. Common aberrations are mutations in the tumor suppressor TP53, suspected to confer a growth-advantage to the mutant cells. However, their full impact in the development of malignant features and safety of hPSCs for downstream applications is yet to be elucidated. Here, TP53 is knocked out in hPSCs using CRISPR-Cas9 and compared them with isogenic wild-type hPSCs and human germ cell tumor lines as models of malignancy. While no major changes in proliferation, pluripotency, and transcriptomic profiles are found, mutant lines display aberrations in some of the main chromosomal hotspots for genetic abnormalities in hPSCs. Additionally, enhanced clonogenic and anchorage-free growth, alongside resistance to chemotherapeutic compounds is observed. The results indicate that common TP53-depleting mutations in hPSCs, although potentially overlooked by standard analyses, can impact their behavior and safety in a clinical setting.

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人类多能干细胞中TP53的缺失引发恶性样行为。

人多能干细胞（hPSCs）在体外培养过程中容易出现遗传畸变。常见的畸变是肿瘤抑制因子TP53的突变，被怀疑赋予突变细胞生长优势。然而，它们对恶性特征发展的全面影响以及下游应用hPSCs的安全性尚未阐明。在这里，使用CRISPR-Cas9敲除hPSCs中的TP53，并将其与等基因野生型hPSCs和人类生殖细胞肿瘤系作为恶性肿瘤模型进行比较。虽然在增殖、多能性和转录组谱方面没有发现重大变化，但突变系在hPSCs的一些主要遗传异常的染色体热点上表现出畸变。此外，观察到克隆性和无锚定生长增强，以及对化疗化合物的耐药性。结果表明，尽管标准分析可能忽略了hPSCs中常见的tp53耗尽突变，但它可以影响它们在临床环境中的行为和安全性。

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