Here we elucidate the effect of Alzheimer disease (AD)-predisposing genetic backgrounds, APOE4, PSEN1ÎE9, and APPswe, on functionality of human microglia-like cells (iMGLs). We present a physiologically relevant high-yield protocol for producing iMGLs from induced pluripotent stem cells. Differentiation is directed with small molecules through primitive erythromyeloid progenitors to re-create microglial ontogeny from yolk sac. The iMGLs express microglial signature genes and respond to ADP with intracellular Ca(2+) release distinguishing them from macrophages. Using 16 iPSC lines from healthy donors, AD patients and isogenic controls, we reveal that the APOE4 genotype has a profound impact on several aspects of microglial functionality, whereas PSEN1ÎE9 and APPswe mutations trigger minor alterations. The APOE4 genotype impairs phagocytosis, migration, and metabolic activity of iMGLs but exacerbates their cytokine secretion. This indicates that APOE4 iMGLs are fundamentally unable to mount normal microglial functionality in AD.
PSEN1ÎE9, APPswe, and APOE4 Confer Disparate Phenotypes in Human iPSC-Derived Microglia.
PSEN1ΔE9、APPswe 和 APOE4 赋予人类 iPSC 衍生小胶质细胞不同的表型
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作者:Konttinen Henna, Cabral-da-Silva Mauricio E Castro, Ohtonen Sohvi, Wojciechowski Sara, Shakirzyanova Anastasia, Caligola Simone, Giugno Rosalba, Ishchenko Yevheniia, Hernández Damián, Fazaludeen Mohammad Feroze, Eamen Shaila, Budia Mireia Gómez, Fagerlund Ilkka, Scoyni Flavia, Korhonen Paula, Huber Nadine, Haapasalo Annakaisa, Hewitt Alex W, Vickers James, Smith Grady C, Oksanen Minna, Graff Caroline, Kanninen Katja M, Lehtonen Sarka, Propson Nicholas, Schwartz Michael P, Pébay Alice, Koistinaho Jari, Ooi Lezanne, Malm Tarja
| 期刊: | Stem Cell Reports | 影响因子: | 5.100 |
| 时间: | 2019 | 起止号: | 2019 Oct 8; 13(4):669-683 |
| doi: | 10.1016/j.stemcr.2019.08.004 | 种属: | Human |
| 研究方向: | 细胞生物学 | ||
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