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Asymmetric organelle inheritance predicts human blood stem cell fate
Author(s) -
Dirk Loeffler,
Florin Schneiter,
Weijia Wang,
Arne Wehling,
Tobías Kull,
Claudia Lengerke,
Markus G. Manz,
Timm Schroeder
Publication year - 2021
Publication title -
blood
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.515
H-Index - 465
eISSN - 1528-0020
pISSN - 0006-4971
DOI - 10.1182/blood.2020009778
Subject(s) - stem cell , biology , cell division , haematopoiesis , asymmetric cell division , microbiology and biotechnology , hematopoietic stem cell , mitochondrion , organelle , cell fate determination , cell , blood cell , cell cycle , cytokinesis , genetics , gene , transcription factor
Understanding human hematopoietic stem cell fate control is important for its improved therapeutic manipulation. Asymmetric cell division, the asymmetric inheritance of factors during division instructing future daughter cell fates, was recently described in mouse blood stem cells. In human blood stem cells, the possible existence of asymmetric cell division remained unclear because of technical challenges in its direct observation. Here, we use long-term quantitative single-cell imaging to show that lysosomes and active mitochondria are asymmetrically inherited in human blood stem cells and that their inheritance is a coordinated, nonrandom process. Furthermore, multiple additional organelles, including autophagosomes, mitophagosomes, autolysosomes, and recycling endosomes, show preferential asymmetric cosegregation with lysosomes. Importantly, asymmetric lysosomal inheritance predicts future asymmetric daughter cell-cycle length, differentiation, and stem cell marker expression, whereas asymmetric inheritance of active mitochondria correlates with daughter metabolic activity. Hence, human hematopoietic stem cell fates are regulated by asymmetric cell division, with both mechanistic evolutionary conservation and differences to the mouse system.

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